Fact-checked by Grok 2 weeks ago

Puberty blocker

Puberty blockers, formally known as (GnRH) analogues, are pharmaceutical agents that reversibly inhibit the pulsatile release of GnRH from the , thereby suppressing pituitary secretion and halting the production of endogenous sex steroids such as and testosterone, which drive the physical maturation of . These medications, administered via injections or implants, are primarily approved by regulatory bodies like the U.S. (FDA) and the (EMA) for the treatment of central , a rare disorder in which pubertal changes occur before age 8 in girls or 9 in boys, allowing normalization of growth and skeletal development. In recent decades, puberty blockers have been employed off-label to delay pubertal progression in adolescents diagnosed with , with the aim of providing time for psychological exploration and reducing distress from incongruence between experienced and characteristics; however, this practice lacks formal regulatory approval for such indications and has sparked intense debate over its medical justification. Systematic evidence reviews, including the comprehensive 2024 Cass Review commissioned by the UK's , have concluded that the research base underpinning their use for is predominantly of low or very low quality, characterized by small sample sizes, short follow-up periods, and high risk of bias, failing to demonstrate clear benefits or improvements in persistence while highlighting methodological flaws in supportive studies. Notable risks associated with prolonged suppression include significant reductions in accrual, potentially leading to or increased susceptibility that may not fully recover post-treatment; compromised due to arrested gonadal maturation, especially if followed by cross-sex hormones; and unresolved questions regarding impacts on maturation, height potential, and outcomes, as long-term data remain scarce and derived from non-randomized cohorts. These concerns, compounded by desistance rates in where many youth resolve distress without intervention, have prompted regulatory actions such as the UK's indefinite restriction on routine prescribing for under-18s outside research protocols, alongside similar pauses or bans in , , and , reflecting a shift toward caution amid evidentiary gaps.

Overview and Mechanism

Definition and pharmacological types

Puberty blockers are medications designed to temporarily suppress the hypothalamic-pituitary-gonadal axis, thereby inhibiting the pulsatile secretion of (GnRH) and subsequently reducing the release of (LH) and (FSH) from the gland. This action prevents the downstream production of gonadal steroids—primarily in females and testosterone in males—halting the development of secondary characteristics such as breast growth, , , voice deepening, and skeletal maturation associated with . GnRH analogues achieve this suppression through continuous administration, which initially stimulates GnRH receptors but leads to receptor downregulation and desensitization, effectively mimicking a state of . These agents are reversible upon discontinuation, allowing to resume, though the timing and extent may vary based on duration of use and individual factors. The primary pharmacological class of puberty blockers consists of synthetic GnRH agonists (also termed GnRHa), which are analogues of native GnRH modified for increased potency and resistance to enzymatic degradation. Common formulations include leuprolide acetate (e.g., Lupron), administered via intramuscular or subcutaneous injections every 1–3 months or as a depot; (e.g., Trelstar), similarly given by injection; histrelin (e.g., Supprelin LA), available as a subcutaneous implant lasting up to 12 months; and (e.g., Zoladex), provided as a subcutaneous implant. Less frequently, GnRH antagonists such as or elagolix may be considered, which directly block GnRH receptors without initial stimulation, but these are not standard for pubertal suppression due to shorter duration and different primary indications like or . In peripheral blockade approaches—typically reserved for non-central or off-label uses—anti-s like or progestins such as may be employed to antagonize effects, though these do not suppress central GnRH drive and carry distinct profiles. All GnRH agonists require monitoring of levels and , as suppression can impact peak bone mass accrual if prolonged beyond stage 2–3.

Physiological mechanism and effects

Puberty blockers, primarily gonadotropin-releasing hormone (GnRH) agonists such as leuprolide acetate or triptorelin, exert their effects by mimicking the pulsatile release of endogenous GnRH initially, which stimulates the pituitary gland to secrete luteinizing hormone (LH) and follicle-stimulating hormone (FSH). With continuous administration, these agonists cause downregulation and desensitization of GnRH receptors on gonadotroph cells in the anterior pituitary, leading to a profound suppression of LH and FSH secretion. This results in reduced production of gonadal sex steroids—testosterone in males and estradiol in females—effectively halting the hypothalamic-pituitary-gonadal (HPG) axis activation that drives pubertal development. The suppression of sex hormones prevents the maturation of secondary , including , menstrual cycles, facial and growth, voice deepening, and skeletal changes associated with the pubertal growth spurt. In clinical use for , this mechanism allows for a delay in advancement; studies show that after discontinuation, the HPG axis typically reactivates, resuming normal pubertal progression within 6-18 months, with preserved in the majority of cases based on longitudinal data from cohorts treated in childhood. However, prolonged suppression beyond 2-3 years, as sometimes occurs in off-label applications, can lead to incomplete catch-up growth and potential deficits in peak bone mass accrual, with scans indicating reduced density (BMD) z-scores averaging -1.0 to -1.5 standard deviations below age-matched norms during treatment. Effects on other physiological systems include potential impacts on brain development, as sex steroids influence and cognitive maturation during ; animal models and limited data suggest alterations in microstructure and hypothalamic connectivity, though causality remains understudied in adolescents. Cardiovascular effects are minimal in short-term use, but extended GnRH agonist exposure correlates with slight increases in and adiposity in some pediatric populations. Fertility outcomes post-treatment show high recovery rates (over 90% in cases followed for 10+ years), but concurrent or subsequent use with cross-sex hormones may induce sterility, as arrests during suppression. These effects underscore the reversible nature of short-term blockade on gonadal function, contrasted with risks of irreversibility when integrated into irreversible pathways.

Historical Context

Development for precocious puberty (1980s–1990s)

(GnRH) agonist analogues, developed as synthetic modifications of native isolated in 1971, were first applied clinically to central () in the early 1980s to suppress premature hypothalamic-pituitary-gonadal axis activation. Initial studies involved daily subcutaneous or intranasal administration, which induced an initial stimulatory "flare" effect followed by receptor downregulation, leading to sustained reductions in (LH), (FSH), and sex steroid levels, thereby halting secondary sexual development and slowing skeletal maturation. These early trials, often conducted at institutions like , reported regression of pubertal signs in over 90% of treated children within months, with gonadotropin levels returning to prepubertal ranges. By the mid-1980s, the limitations of frequent dosing prompted development of long-acting depot formulations, such as intramuscular leuprolide acetate, which provided monthly suppression and improved adherence. Clinical data from cohorts of 20–50 children showed that such formulations maintained LH suppression below 2–3 /L post-stimulation, preserved bone age advancement at less than 1 year per treatment year, and increased predicted adult by 4–7 cm compared to untreated CPP controls. Adverse effects were primarily limited to injection-site reactions and transient steroid flare, with no significant impacts on growth velocity during suppression observed in these initial evaluations. In the United States, leuprolide depot (Lupron Depot-PED) became the first GnRH formally approved by the FDA for in children on January 29, 1993, for the 1-month formulation at doses of 7.5 mg, targeted at patients with before age 8 in girls or testicular enlargement before age 9 in boys. approvals followed similar timelines, with nafarelin authorized earlier in the for analogous indications. During the , expanded studies involving hundreds of patients confirmed these outcomes, establishing GnRH as the for idiopathic and neurogenic , with treatment durations typically spanning 2–4 years until age-appropriate resumption. Long-term follow-up data emerging by the late indicated no increased risk of or , though questions persisted regarding optimal cessation timing to avoid excess final height deficits.

Adoption and protocols for gender dysphoria (1990s–2010s)

In the mid-1990s, clinicians at the VU University Medical Center in initiated the of (GnRH) analogues, such as , to suppress puberty in adolescents with persistent originating in childhood. This approach, developed by researchers including Henriette A. Delemarre-van de Waal and Peggy T. Cohen-Kettenis, targeted youth at Tanner stage 2 of puberty who had undergone extensive psychological evaluation confirming stable dysphoria without severe comorbidities like autism spectrum disorder or . The protocol emphasized multidisciplinary assessment, requiring at least six months of diagnostic observation prior to intervention, with the goal of halting unwanted secondary sex characteristics to alleviate distress and provide time for identity exploration before proceeding to cross-sex hormones around age 16. Early adoption was limited to a small cohort of about 70 adolescents in the , with initial case reports and feasibility studies published between 1998 and 2006 demonstrating feasibility and short-term acceptability, though long-term data remained prospective and underpowered for rare adverse events. By the early , the "Dutch protocol" influenced experimental use in select and North American clinics, but widespread implementation lagged due to ethical concerns over off-label application in and insufficient randomized . In the late 2000s and 2010s, the protocol informed formal guidelines amid growing referrals. The Endocrine Society's 2009 evaluation framework for gender-dysphoric youth stressed psychological stability before any hormonal intervention, while its 2017 clinical practice guideline explicitly endorsed GnRH analogues starting at Tanner stage G2/B2 for dysphoric adolescents, conditional on informed consent addressing potential impacts on fertility and bone density. The World Professional Association for Transgender Health (WPATH) Standards of Care version 7, published in 2011, recommended puberty suppression as a viable option post-diagnosis for persistent cases, requiring capacity for consent and reversible intent, though critics noted the evidentiary base relied heavily on the Dutch longitudinal data prone to selection bias favoring early-onset, persistent dysphoria. By the mid-2010s, adoption expanded in countries like the and , with clinics such as those affiliated with and the GIDS implementing similar protocols, often initiating blockers in youth aged 10–12 after 6–12 months of . Usage remained off-label in many jurisdictions, with annual prescriptions rising from negligible in the to hundreds by 2015 in adopting centers, driven by observational reports of reduced suicidality but lacking placebo-controlled trials.

Established Medical Applications

Use in precocious puberty

Puberty blockers, specifically (GnRH) agonists, are the standard pharmacological treatment for central (CPP), a condition characterized by the onset of pubertal development before age 8 in girls or age 9 in boys, driven by premature activation of the hypothalamic-pituitary-gonadal axis. These agents work by initially stimulating but ultimately desensitizing GnRH receptors, leading to suppression of (LH), (FSH), and downstream sex steroid production, thereby halting pubertal progression. Treatment is indicated following confirmation of CPP via clinical signs (e.g., breast or testicular development), advanced , and a stimulated LH peak >5 IU/L on GnRH stimulation testing, distinguishing it from peripheral precocious puberty, which does not respond to GnRH agonists. Commonly used GnRH agonists include leuprolide acetate, , and histrelin, administered via intramuscular or subcutaneous injections, nasal sprays (less common due to variable efficacy), or subcutaneous implants for longer durations. Leuprolide, for instance, is typically given as a depot every 1 to 6 months, with doses starting at 7.5–15 mg monthly for children under 30 kg or adjusted for weight and (e.g., 11.25 mg every 3 months or 30–45 mg every 6 months). Treatment duration generally spans 2–4 years or until the child reaches an appropriate chronological age for onset (e.g., of 11–12 years in girls, 12–13 in boys), after which discontinuation allows resumption of normal pubertal progression. The primary goals of are to regress or stabilize secondary characteristics, decelerate skeletal maturation to preserve predicted , and mitigate impacts like emotional distress from physical mismatch with peers. Efficacy is monitored every 3–6 months through clinical exams, LH/FSH/ or testosterone levels (targeting prepubertal ranges: LH <1 IU/L post-stimulation), assessments via , and growth velocity tracking; inadequate suppression prompts dose escalation or formulation change. In practice, suppression occurs within 4 weeks, with slowed growth velocity and advancement observed in responsive patients. Treatment decisions weigh benefits against injection-related discomfort and rare breakthrough , with multidisciplinary input from pediatric endocrinologists.

Evidence base and long-term outcomes for precocious puberty

GnRH agonists (GnRHa), such as leuprorelin, represent the standard of care for central precocious puberty (CPP), effectively suppressing gonadotropin-releasing hormone (GnRH) pulsatility to halt premature pubertal advancement. Clinical trials and meta-analyses demonstrate that GnRHa treatment normalizes growth velocity, advances bone age less rapidly than untreated progression, and improves predicted adult height by allowing extended prepubertal growth phases. For instance, a 2021 meta-analysis of randomized controlled trials found that GnRHa increased final adult height (FAH) by an average of 5-7 cm in girls with idiopathic CPP compared to untreated controls, with treatment durations typically lasting 2-4 years until age-appropriate puberty resumption. Long-term follow-up studies, extending 5-10 years post-treatment, confirm sustained benefits on height outcomes without compromising reproductive function. In cohorts treated during the 1990s-2010s, FAH gains persisted into adulthood, with over 90% of patients achieving heights within normal ranges, and occurring at typical ages (11-13 years) after discontinuation. rates remain comparable to the general , with preserved evidenced by normal levels and successful pregnancies reported in follow-up data. density, initially a concern due to suppressed , normalizes post-treatment as endogenous resumes, with no increased risk observed in longitudinal assessments. Safety profiles from meta-analyses indicate minimal serious adverse events, with low-dose regimens (e.g., 15-30 mcg/kg/day subcutaneously) proving as efficacious as higher doses while reducing injection-site reactions and potential for transient increases. Short-term occurs in approximately 20-30% of patients, attributed to reduced activity and metabolic shifts, but resolves long-term without elevating rates. Cardiovascular parameters, including and profiles, show no deviations from norms in extended . A 2023 systematic review reinforced these findings, noting that combined GnRHa and further enhances height in select cases without additive risks. Overall, decades of use since the 1980s have yielded a robust base from prospective cohorts and registries, contrasting with sparser data in off-label applications.

Application in Gender Dysphoria

Clinical rationale and treatment protocols

The clinical rationale for using puberty blockers, specifically gonadotropin-releasing hormone (GnRH) analogues, in adolescents with gender dysphoria posits that suppressing endogenous pubertal hormone surges prevents the development of secondary sex characteristics misaligned with the adolescent's experienced gender, thereby averting acute psychological distress and allowing extended time for therapeutic exploration of identity and maturation. Proponents argue this intervention is reversible upon discontinuation, mimicking the natural pause in puberty seen in conditions like constitutional delay, and facilitates alignment between physical development and affirmed identity if cross-sex hormones follow. However, this rationale rests on observational data rather than randomized controlled trials, with assumptions about long-term benefits derived from extrapolations from precocious puberty treatment protocols where GnRH analogues demonstrably halt advancement without equivalent gender-related endpoints. Treatment protocols, as outlined in the Endocrine Society's 2017 clinical practice guideline, recommend initiating GnRH analogues for adolescents at stage 2 (early , typically ages 10-13 depending on sex), after multidisciplinary assessment confirms diagnosis of per criteria, persistence over at least 6-12 months, absence of primary psychiatric disorders requiring prior treatment, and informed assent from the adolescent alongside consent from guardians. The World Professional Association for Health (WPATH) Standards of Care version 8 (2022) similarly endorses suppression post- 2 following comprehensive evaluation by professionals, endocrinologists, and support teams, emphasizing individualized risk-benefit analysis including counseling. Administration involves subcutaneous or intramuscular injections (e.g., leuprolide acetate every 1-3 months or histrelin implants lasting 12 months), with dosing titrated to suppress and to prepubertal levels (<2-3 /L). Monitoring protocols require baseline and serial assessments of bone mineral density (via ), height velocity, status, and functioning every 3-6 months, with continuation typically until age 16-18 when cross-sex hormones may commence if persists. Discontinuation without transition to hormones risks rebound and potential recovery, though data on reversibility remain limited to short-term observations. Protocols derived from early models (e.g., Amsterdam clinic since 1998) influenced global adoption, starting blockers after psychological stabilization and excluding those with acute instability, but variations exist across jurisdictions with increasing scrutiny on eligibility criteria post-2020.

Evidence on efficacy for mental health and dysphoria reduction

The evidence evaluating puberty blockers' efficacy for reducing or improving outcomes in is limited to observational studies, with no randomized controlled trials available. Systematic reviews consistently rate this as very low quality due to risks of , imprecision from small samples, confounding factors like concurrent , and lack of long-term follow-up isolated to blockers alone. Early Dutch cohort studies, foundational to clinical protocols, reported modest self-reported decreases in scores (e.g., from mean 5.0 to 3.7 on the Gender Dysphoria Scale after 18-24 months) and improvements in emotional and behavioral problems (e.g., scores dropping below clinical thresholds for most) among 70 strictly selected adolescents (mean age 13.6 at blocker start). However, these were uncontrolled, non-randomized designs with no comparison to untreated peers, and gains were small in magnitude (e.g., effect sizes <0.5 for depressive symptoms) while continuing into subsequent phases, limiting attribution to blockers. Later follow-up at young adulthood showed alleviated dysphoria and functioning comparable to or better than same-aged peers, but only after full cross-sex and surgical interventions. Real-world data from larger clinics reveal mixed or null effects. In a service analysis of 44 on blockers for 12 months, showed no net improvement: 34% reliably deteriorated, 29% improved, and 37% were unchanged per standardized measures like the Strengths and Difficulties Questionnaire. A of 95 tracked for two years found no enhancement in , anxiety, or suicidality scores, with participants remaining stable from baseline (already low distress levels); these federally funded results, led by Johanna Olson-Kennedy, remain unpublished amid concerns over politicization. Across reviewed cohorts, 92% (95% CI 0.53-0.99) of youth on blockers progressed to cross-sex hormones within 12-36 months, suggesting limited resolution of underlying rather than suppression-induced alleviation. Comorbid conditions like or prior , prevalent in 30-50% of cases, often persist without targeted resolution, and reviews find no robust causal evidence linking blockers to sustained gains over or therapy alone. The 2024 Cass Review, synthesizing 50 studies, emphasized this evidentiary gap, stating no reliable conclusions can be drawn on positive impacts for or functioning.

Observed progression to cross-sex hormones

In clinical cohorts treated with puberty blockers for , progression to cross-sex hormones has been consistently high, often exceeding 95%. In the Protocol's longitudinal studies, 96% to 98% of adolescents who initiated GnRH analogues at stage 2 proceeded to cross-sex hormones after approximately two years of suppression, with only 1.9% discontinuing without advancing. Similarly, in the UK's (GIDS) Early Intervention Study involving 44 carefully selected youth, 98% (43 participants) transitioned to cross-sex hormones following blockers, with just one ceasing treatment without progression. These rates contrast sharply with historical desistance patterns in untreated gender-dysphoric children, where up to 80-90% resolved dysphoria by adulthood without medical intervention. The near-universal advancement observed post-blockers has been interpreted differently: proponents, including original Dutch researchers, attribute it to rigorous pre-treatment selection ensuring persistent dysphoria, while the 2024 Cass Review highlighted it as evidence that blockers may not facilitate meaningful reconsideration but instead propel youth toward irreversible steps, potentially due to psychosocial commitment, arrested psychosocial maturation, or physiological changes like gonadal suppression complicating natural puberty resolution. Limited long-term tracking exacerbates uncertainties; for instance, clinic data over 20 years showed sustained high conversion in early cohorts but evolving referral demographics with potentially lower persistence signals in recent cases, though overall trajectories remained escalation-dominant. Systematic reviews note that such progression rates, often 90-100% across protocols, undermine claims of blockers as a purely diagnostic "pause," as few revert to identifying with their birth sex once suppression begins.

Safety and Adverse Effects

Short-term side effects

Common short-term side effects of puberty blockers, which are GnRH agonists such as leuprolide, include injection site reactions like , rashes, bruising, and sterile abscesses, occurring in a notable proportion of pediatric patients treated for . These reactions are typically mild and transient, resolving without long-term sequelae. Headaches, hot flushes, fatigue, and mood fluctuations or swings are also frequently reported, affecting a majority of users during the initial months of treatment in both and cohorts. These symptoms stem from the suppression of sex hormones and are generally mild, with rare instances leading to treatment discontinuation. and increased sweating may occur alongside these, particularly in children. In clinical studies of leuprolide for , adverse events such as , weight gain, and common cold-like symptoms have been noted at rates exceeding 4%, though severe manifestations remain uncommon. Systematic data indicate that these effects are anticipated and directly linked to hormonal suppression, with no evidence of heightened severity in applications compared to established uses. Allergic reactions or visual disturbances are rare but warrant monitoring.

Long-term risks and uncertainties

The long-term use of analogues (GnRHa), commonly known as blockers, in adolescents with carries risks including reduced bone mineral density (BMD), impaired fertility, and potential alterations to neurocognitive development, though high-quality longitudinal data remain limited. Systematic reviews, such as those informing the 2024 Cass Review, highlight that while GnRHa effectively pauses , evidence on sustained safety is weak, with most studies confined to short-term outcomes under 2 years. Bone health represents a primary concern, as GnRHa suppresses the pubertal surge in steroids essential for peak mass accrual, leading to declines in BMD z-scores during treatment; one of adolescents found z-scores dropping below -2 standard deviations in lumbar spine measurements after 1-2 years of suppression. Longer durations exacerbate this, with prospective data from clinics showing persistent deficits even after transitioning to cross-sex hormones, potentially increasing risk into adulthood. Recovery is uncertain, as adult may not fully compensate for adolescent deficits, contrasting with shorter-term use in where gains often occur post-treatment. Fertility preservation poses another challenge, as GnRHa alone may allow gonadal maturation if discontinued, but sequential administration with cross-sex hormones—observed in over 90% of cases in longitudinal cohorts—frequently results in irreversible due to arrested and ovarian or . Studies indicate that starting blockers early ( stage 2) followed by hormones before age 16 heightens sterility risks, with limited success in fertility preservation techniques like oocyte or cryopreservation in pre-pubertal youth. Emerging evidence suggests impacts on brain maturation, as puberty hormones influence development critical for executive function and emotional regulation; animal models and preliminary human data indicate GnRHa may disrupt and myelination processes active during , though human studies lack controls and long-term follow-up. The 2024 Cass Review and associated systematic evaluations underscore methodological gaps, including absence of randomized trials and reliance on low-quality observational data, leaving uncertainties about cardiovascular, metabolic, and outcomes unresolved. Overall, while risks appear lower in brief applications, the extended, hormone-sequential protocols for amplify unknowns, prompting calls for precautionary approaches in guidelines from bodies like the 's NHS.

Research Evaluations and Gaps

Key systematic reviews and expert panels (e.g., Cass Review 2024, HHS 2025)

The Cass Review, commissioned by and published on April 10, 2024, conducted a comprehensive evaluation of services for children and young people under 18, including a of evidence on suppression. It concluded that the evidence for blockers improving , , or psychosocial functioning in adolescents with was of low quality, with most studies rated as weak due to methodological flaws such as small sample sizes, lack of control groups, and high loss to follow-up. The review found no high-quality randomized controlled trials and highlighted that blockers do not demonstrably improve body image satisfaction or expected reduction, while noting potential harms like impacts on and . As a result, it recommended restricting blockers to clinical research protocols rather than routine use, influencing 's decision to halt their prescription outside trials for . The U.S. Department of Health and Human Services (HHS) released "Treatment for Pediatric Gender Dysphoria: Review of Evidence and Best Practices" on May 1, 2025, synthesizing over 200 studies on interventions including puberty blockers. The report determined that the evidence base for puberty blockers in alleviating gender dysphoria or enhancing mental health outcomes in youth is insufficient, characterized by low-quality observational data prone to bias and confounding factors like concurrent psychotherapy. It emphasized uncertainties in long-term effects, such as bone health, cognitive development, and fertility, and critiqued the Dutch Protocol's foundational studies for lacking rigorous controls, concluding that medical interventions should not be standard without stronger evidence favoring comprehensive psychological assessment first. The HHS review advocated prioritizing non-pharmacological approaches and informed dissent from proponents of affirmative models, who argued it undervalued observational benefits. A May 2025 systematic review and published in Acta Paediatrica examined 12 studies on blockers for , finding very low certainty of evidence for benefits in reducing or improving psychological functioning, with no significant gains observed beyond effects or maturation. It reported consistent risks of stalled bone mineralization and height suppression, underscoring gaps in long-term data. Other panels, such as the UK's evidence reviews integrated into Cass (2020–2024), similarly graded the evidence as inadequate for routine endorsement, prioritizing applications where benefits are established. These evaluations collectively highlight a shift toward caution, driven by evidentiary shortcomings rather than prior assumptions of efficacy.

Methodological limitations and unpublished findings

Studies on blockers for suffer from significant methodological shortcomings, including the absence of randomized controlled trials (RCTs), which are the gold standard for establishing and . Existing research predominantly relies on observational designs with small sample sizes, often fewer than 100 participants, leading to limited statistical power and high risk of bias from confounding variables such as concurrent or natural desistance of . For instance, the influential studies, which underpin much of the affirmative care model, lacked control groups and had high rates of progression to hormones (98%), potentially inflating perceived benefits while ignoring non-treated comparators. Short follow-up periods further undermine reliability, with many studies assessing outcomes over 1-2 years despite puberty suppression's multi-year duration and potential lifelong implications; long-term data on , , and cognitive effects remain sparse and inconsistent. Loss to follow-up rates exceeding 20-30% in key cohorts introduce , as dropouts may represent unfavorable outcomes not captured in analyses. Systematic reviews, including the Cass Review (2024), rated over 90% of studies as low-quality due to these issues, excluding them from strong evidence synthesis and highlighting reliance on non-standardized outcome measures like self-reported satisfaction rather than objective metrics. The U.S. Department of Health and Human Services (HHS) 2025 review echoed these concerns, noting inadequate controls and failure to isolate puberty blockers' effects from interventions across primary studies. Unpublished findings exacerbate evidential gaps, particularly a U.S. (NIH)-funded study led by Johanna Olson-Kennedy, involving 95 receiving blockers from 2015 onward. Despite $9.7 million in taxpayer funding, results showing no improvements—contradicting assumptions of distress reduction—were withheld for years, with Olson-Kennedy citing fears of "weaponization" against gender-affirming in a political climate. This delay, revealed in October 2024, aligns with critiques of favoring positive outcomes, as evidenced by earlier UK Gender Identity Development Service (GIDS) from 2011-2015 remaining partially unpublished amid service closure and scandals. Such selective reporting risks overestimating benefits, as neutral or negative results from rigorous cohorts are absent from meta-analyses, perpetuating reliance on weaker evidence.

Comparative evidence versus precocious puberty use

GnRH analogues, commonly known as puberty blockers, have been employed for over three decades in treating central (CPP), a condition characterized by puberty onset before age 8 in girls or 9 in boys, with robust evidence supporting their efficacy and safety. Multiple systematic reviews and meta-analyses demonstrate that these agents effectively suppress and sex steroid secretion, delaying pubertal progression and increasing predicted final adult height by 3–10 cm in treated girls compared to untreated peers, without compromising reproductive function or causing severe long-term adverse effects upon discontinuation. Long-term follow-up studies confirm normalization of , minimal impact on , and preservation of , as endogenous resumes predictably after treatment cessation. In adolescents with , the evidence base for GnRH analogues is markedly weaker and of lower quality, relying primarily on small, non-randomized observational studies rather than controlled trials. While suppression of secondary characteristics is consistently achieved, systematic reviews find insufficient high-certainty on improvements in , persistence, or overall well-being, with methodological limitations including lack of comparison groups and short follow-up periods. Progression to cross- hormones occurs in approximately 92% of cases within 12–36 months, contrasting with where treatment is finite and natural resumes, raising uncertainties about reversibility in the gender dysphoria context. Diagnostic and therapeutic contexts differ fundamentally: diagnosis is objective, based on verifiable elevations in and pubertal staging, enabling precise intervention to avert and psychosocial harm from early maturation. assessments, however, depend on self-reported distress without analogous biomarkers, complicating causal attribution of benefits to blockers amid high rates with conditions like or . Unlike , where decades of randomized and longitudinal data affirm safety, applications lack equivalent scrutiny, with expert panels such as the Cass Review (2024) deeming the evidence "remarkably weak" and not supportive of routine use outside research protocols. health and risks, while monitored in with reassuring outcomes, remain understudied long-term in cohorts, particularly given frequent escalation to sterilizing interventions.

Ethical and Societal Controversies

Informed consent and capacity in minors

Minors lack full legal capacity to provide independent informed consent for medical interventions in most jurisdictions, requiring parental or guardian involvement for treatments such as puberty blockers used off-label for gender dysphoria. In the United Kingdom, the principle of Gillick competence permits mature minors under 16 to consent if they demonstrate understanding of the treatment's implications, but the 2020 High Court ruling in Bell v Tavistock held that children under 16—and potentially older minors—are unlikely to meet this threshold for puberty blockers, given the treatment's experimental status, uncertain benefits, and serious long-term risks including infertility, impaired sexual function, and progression to irreversible cross-sex hormones in over 90% of cases. Ethical assessments of minors' decisional capacity emphasize neurodevelopmental limitations, as maturation—critical for risk evaluation, impulse control, and foresight—continues into the mid-20s, hindering comprehension of blockers' implications such as potential brain development alterations and loss when followed by hormones. The Cass Review (2024) identified systemic shortcomings in processes at gender clinics, including superficial assessments of understanding, failure to convey uncertainties, and inadequate exploration of comorbidities or alternatives like , leading to recommendations that blockers be restricted to clinical trials with rigorous protocols. Similarly, the U.S. Department of Health and Human Services (2025) report underscores controversy over minors' ability to to fertility-impacting effects, noting that while some protocols claim adolescents around can participate in decisions, limited life experience and predictive uncertainty about persistence undermine true autonomy. Empirical studies on capacity yield mixed results, with one assessment finding 89% of transgender youth aged 10–18 competent for pubertal suppression via standardized tools, correlating with age 12+ thresholds but limited by small samples and lack of focus on long-term harms. A Canadian study of 14–18-year-olds reported thoughtful weighing of hormone risks and benefits, supporting informed consent models, yet critics argue such self-selected cohorts overestimate competence amid social influences and diagnostic overshadowing of co-occurring conditions like autism or trauma. Given the treatment's causal pathway to sterility in early puberty stages and absence of high-quality longitudinal data, ethicists contend that minors' consent cannot be reliably informed without overemphasizing unproven benefits over documented risks like bone density loss.

Desistance rates, regret, and social influences

Studies of children diagnosed with prior to widespread social affirmation practices have consistently reported high desistance rates, with 61% to 98% no longer meeting diagnostic criteria for or identifying as by or adulthood if not medically transitioned. These longitudinal follow-ups, spanning cohorts from the 1970s to 2000s, primarily involved prepubertal children presenting with cross-gender behaviors, many of whom resolved without intervention through or . Desistance was more common among boys than girls in these samples, and persistence was associated with intensity of dysphoria and . Critics argue these studies included children who would not qualify under stricter criteria for , potentially inflating rates; however, even adjusted analyses show substantial natural resolution, challenging assumptions of innate, immutable identity. In contemporary contexts, desistance appears rarer among socially transitioned , with one U.S. finding only 7.3% retransitioned (desisted) after five years of social transition, though 94% persisted in identification. The 2024 Cass Review noted that prior evidence of high desistance supports caution with early medical interventions like puberty blockers, as blocking puberty may reduce opportunities for natural resolution by altering developmental trajectories and reinforcing identity. Systematic reviews highlight methodological gaps in modern persistence data, including lack of groups and by influences, underscoring in projecting lifelong outcomes for minors. Regret following blockers is infrequently reported in published cohorts, with rates under 5% in short-term follow-ups of adolescents who subsequently pursued cross-sex hormones; for instance, one observed 98% continuation to hormones after blockers, implying low immediate discontinuation. A 2024 review of literature estimated long-term at 0.1% to 0.3% among treated , but emphasized severe limitations: median regret onset at 8 years post-surgery (longer for blockers alone), high loss to follow-up (up to 81% in some studies), and exclusion of non-respondents who may have desisted silently. Emerging testimonies and clinic data suggest underreporting, with external pressures (e.g., family support for transition) and incomplete contributing to delayed realization; true population-level rates remain unknown due to absent registries and reliance on self-selected samples from affirming clinics. Social influences have been implicated in the sharp rise in adolescent cases since 2010, particularly among females, with referrals increasing exponentially (e.g., 4,000% in clinics over a decade). The rapid-onset gender dysphoria (ROGD) hypothesis, based on parent surveys of over 1,600 cases, describes sudden declarations in teens without childhood history, often coinciding with peer groups (62% of friends also identifying as ) or online communities promoting transition. These cases frequently involve comorbid issues (57%) and autistic traits, patterns akin to social in conditions like eating disorders or clusters. While affirming researchers dispute contagion via clinic-based studies showing no peer , such data derive from pre-existing dysphoric youth and overlook population-level trends, including geographic hotspots and exposure effects; empirical patterns—delayed onset post-puberty, female predominance, and resolution in non-affirmed peers—align with causal roles for social reinforcement over isolated biological etiology. The Cass Review urged further investigation into these dynamics, citing weak evidence isolating individual pathology from environmental factors.

Debates on medicalization versus watchful waiting

The debate over —administering blockers to suppress endogenous in adolescents experiencing —versus , which emphasizes psychological exploration and monitoring without pharmacological intervention, hinges on the balance of potential benefits against risks and natural developmental trajectories. Proponents of medicalization, including organizations like the World Professional Association for Transgender Health (WPATH), assert that blockers provide a "pause" to alleviate acute distress, prevent irreversible pubertal changes misaligned with identity, and reduce suicidality risks, citing observational data from Dutch protocol cohorts where most patients proceeded to hormones without reported regret at short-term follow-up. However, systematic reviews, such as those commissioned for the UK's Cass Review, have found the evidence for mental health improvements from blockers to be of low quality, with no consistent demonstration of reduced dysphoria, self-harm, or suicide ideation compared to non-intervention. Watchful waiting draws from pre-2010 longitudinal studies of gender-dysphoric youth, where 80-88% desisted from transgender identification by adulthood when managed through supportive therapy without affirmation of cross-sex identity or medical transition, allowing puberty to proceed naturally as a potential catalyst for resolution. Critics of early medicalization argue it may entrench dysphoria by halting the biological maturation that historically facilitated desistance, particularly amid evidence of social influences and rapid-onset cases in recent referrals, where persistence rates exceed those in earlier cohorts under non-affirmative care. Even post-blocker desistance has been documented in case reports, suggesting interventions do not preclude natural resolution but may complicate it through side effects like bone density loss and fertility impairment. Emerging guidelines in reflect a pivot toward or therapy-first models, informed by methodological critiques of affirmative care trials lacking randomized controls or long-term outcomes. Sweden's National Board of Health and Welfare, in 2021, restricted blockers to settings after reviewing evidence of uncertain benefits and harms, prioritizing interventions. Similarly, Finland's 2020 guidelines and Germany's 2025 protocols recommend blockers only in exceptional cases post-exhaustive psychological , citing risks from combined blocker-hormone sequences and the absence of proven superiority over watchful approaches. The Cass Review echoed this caution, advocating comprehensive, holistic assessments over routine medicalization, a stance leading to NHS England's indefinite ban on blockers outside trials as of December 2024. These shifts underscore concerns that affirmative medicalization, adopted rapidly without robust trials, may pathologize transient influenced by cultural factors, whereas aligns with developmental plasticity evidenced in desistance data.

Regulatory and Legal Landscape

Global trends toward restrictions (2020–2025)

From 2020 onward, a growing number of countries restricted or limited the use of puberty blockers for minors with , driven by systematic reviews highlighting low-quality for benefits, uncertain long-term outcomes, and risks such as loss, , and potential impacts on cognitive and sexual development. led this shift in 2020, updating guidelines to recommend puberty blockers only in exceptional cases following thorough multidisciplinary assessment, prioritizing interventions due to weak from observational studies lacking controls. followed in 2022, with the National Board of Health and Welfare restricting blockers and cross-sex hormones to rare instances under research protocols, after reviewing data showing no clear improvements and high progression rates to irreversible treatments exceeding 90%. Norway aligned in 2023, directing healthcare regions to confine blockers to clinical trials amid insufficient research-based on efficacy and harms, emphasizing exploratory therapy instead. Denmark implemented sharp curbs the same year, shifting toward counseling for most cases while reserving medical interventions for rigorous studies. The escalated restrictions in 2024, banning new prescriptions of blockers outside research following the Cass Review's findings of very low evidence certainty and ethical concerns over in youth. Italy's Committee echoed this in December 2024, advocating as first-line treatment and limiting blockers to controlled trials after failure. In , U.S. states enacted over 25 blanket bans on gender-affirming care including puberty blockers by mid-2025, starting with in 2021 and expanding amid litigation, often justified by state reviews citing European precedents and domestic data gaps. Federally, the U.S. Department of Health and Human Services' May 2025 report recommended confining blockers to research settings, noting flawed U.S. clinic practices deviating from protocols and international consensus on experimental status. saw state-level action, with halting prescriptions for under-18s in January 2025 pending review, though facing legal challenges. These developments reflected a broader pivot toward caution, with bodies like France's urging "greatest reserve" since 2022 due to off-label use risks, contrasting earlier affirmative stances. By late 2025, at least 10 European nations had curtailed routine access, prioritizing evidence over prior assumptions of reversibility.

Developments in Europe

Beginning in 2020, updated its clinical guidelines to restrict puberty blockers for adolescents with to exceptional cases following psychological interventions, classifying routine use as experimental due to insufficient evidence of benefits outweighing risks. followed in 2021 when the ceased prescribing puberty blockers and cross-sex hormones to minors under 18 outside research protocols, with national guidelines in 2022 limiting such interventions to rare, well-documented cases where risks are deemed lower than benefits after comprehensive evaluation. Norway's Directorate of Health revised policies in 2023 to confine blockers and hormones to clinical trials for minors, emphasizing exploratory as the primary approach amid concerns over long-term effects and weak supporting data. implemented sharp restrictions in 2023, redirecting most referrals from pharmacological interventions to , with blockers reserved for research settings following a health authority review highlighting methodological flaws in prior studies. France's issued a 2022 advisory urging "the greatest reserve" in using puberty blockers, recommending they be limited to strictly supervised trials due to uncertain reversibility and potential impacts on , , and neurodevelopment. In the , the 2024 Cass Review prompted to halt routine prescriptions of puberty blockers for under-18s in March, extending to an indefinite ban on private provision in December after expert panels cited low-quality evidence and elevated risks. Italy's National Bioethics Committee in December 2024 endorsed as first-line treatment, confining puberty blockers to controlled clinical trials post-failed interventions. Germany's 2025 guidelines for youth gender incongruence discourage puberty blockers entirely, prioritizing non-medical approaches and rejecting surgical options based on systematic evidence assessments. These shifts across reflect systematic reviews, including the UK's Cass Review, which critiqued the evidence base for puberty blockers as predominantly low-quality, non-randomized, and confounded by comorbidities, prompting a pivot toward caution and research-only protocols over standard care.

Developments in North America

In the United States, regulatory developments regarding blockers for in minors have increasingly focused on state-level restrictions amid concerns over long-term safety and evidentiary gaps. As of June 2025, 25 states had enacted laws prohibiting or severely limiting the provision of blockers, cross-sex hormones, and surgeries to youth under 18, often citing insufficient high-quality evidence of benefits outweighing risks such as loss and impairment. These measures, which began accelerating in 2021, expanded in 2024 with states like , , , and joining the list, typically allowing exceptions only for ongoing treatments initiated prior to enactment or in cases of legal challenges. Federal oversight remains limited; the has not approved GnRH analogues ( blockers) for treating in youth, permitting only despite their approval for . Litigation has ensued in over 18 states, with courts upholding bans in some (e.g., ) while blocking others temporarily, reflecting divided judicial interpretations of medical necessity versus parental rights. At the federal level, a January 2025 executive action established a policy against funding, sponsoring, or promoting chemical or surgical interventions for minors' sex transitions, directing agencies to prioritize evidence-based care and review prior guidelines. A May 2025 U.S. Department of Health and Human Services report on pediatric treatment underscored methodological weaknesses in supportive studies, recommending against routine puberty blocker use outside clinical trials due to risks like impaired and lack of reversal data. Professional bodies such as the faced internal debates, with some members advocating alignment with international reviews questioning blockers' efficacy, though national guidelines have not shifted uniformly. In , developments have been more fragmented at the provincial level, with leading restrictions in 2024 by prohibiting puberty blockers and hormone therapies for those under 16, while permitting mature 16- and 17-year-olds access under stringent criteria including psychological assessments. This policy, justified by Premier Danielle Smith's government on precautionary grounds amid European pauses, encountered legal pushback; a 2025 temporarily halted enforcement, prompting an appeal in August 2025. Other provinces like and imposed referral and consent requirements for youth treatments in 2023-2024, but no nationwide ban exists, and bodies like the Canadian Paediatric Society have defended blockers' use despite critiques of low-evidence bases. A proposed bill to bar puberty blockers for minors was defeated in October 2025, maintaining access under existing guidelines. Overall, Canadian approaches emphasize multidisciplinary evaluations but have not adopted the scale of U.S. prohibitions, with ongoing provincial variations reflecting tensions between and emerging risk data.

Other international policies

In Australia, state-level policies on puberty blockers for minors with gender dysphoria vary, with Queensland halting new prescriptions as of January 28, 2025, pending an independent evidence review of stage 1 (puberty suppression) and stage 2 (hormone) therapies. Nationally, the National Health and Medical Research Council initiated a review in early 2025, with interim clinical advice on puberty blockers expected by mid-2026, reflecting concerns over evidence quality similar to international systematic reviews. Prior to these developments, access followed multidisciplinary guidelines without routine restrictions, though prescriptions required specialist oversight. New Zealand's Ministry of Health conducted a on safety measures for blockers in with gender-related needs, closing on January 20, 2025, following an evidence brief highlighting insufficient high-quality data on long-term effectiveness and safety. A November 2024 position statement emphasized greater precautions, including updated clinical guidelines, but no new regulations had been enacted by October 2025, with final decisions delaying broader health guidelines. Professional bodies, including the Royal New Zealand College of General Practitioners, argued against regulatory restrictions, favoring clinician discretion amid ongoing debates. Previously, access aligned with good practice guidelines without specific legislation. In , prohibited gender-affirming hormone therapies, including puberty blockers, for individuals under 18 via a February 5, 2025, presidential decree repealing provisions of the 2012 Gender Identity Law that permitted such interventions with parental or judicial consent. Brazil's health authority raised the minimum age for in minors to 18 on April 16, 2025, effectively restricting puberty blockers absent exceptional multidisciplinary approval. These measures align with broader regional scrutiny of interventions lacking robust pediatric evidence, though implementation details vary by jurisdiction. Policies in and remain limited and under-documented for blockers specifically in contexts, with most countries lacking dedicated regulations and defaulting to general pediatric standards that prioritize indications over elective use. In , access for minors is restricted to rigorous protocols requiring extensive evaluation, but no outright bans were reported as of 2025. and focus regulatory attention on adult transitions, with minimal formalized guidance for adolescent suppression beyond case-by-case specialist discretion.

Professional Organization Stances

Bodies recommending restrictions or trials only

The Cass Review, an independent investigation commissioned by and published in April 2024, concluded that the evidence supporting suppression for gender-related distress in youth is of low quality and inconclusive, recommending that blockers be used only within formal clinical research protocols to generate robust data on safety and efficacy. This led to implement a policy in March 2024 halting routine prescriptions of blockers outside research settings for under-18s with , a restriction extended indefinitely by government regulations in December 2024 following expert advice citing insufficient evidence of benefits outweighing risks such as impacts on and fertility. The UK's National Institute for Health and Care Excellence (), in a 2021 evidence review, rated the quality of studies on blockers as very low due to methodological flaws including small sample sizes, lack of controls, and short follow-up periods, advising against their routine use and emphasizing the need for randomized controlled trials to assess outcomes on , , and long-term effects. Sweden's National Board of Health and Welfare updated its guidelines in 2022 to restrict blockers to exceptional cases only after exhaustive multidisciplinary evaluation, deeming routine medical interventions unsupported by high-quality evidence and prioritizing psychosocial approaches, with the ceasing their use outside clinical studies as early as 2021. Finland's Council for Choices in Health Care, in 2020 guidelines, positioned puberty blockers as experimental rather than standard care, recommending they be limited to settings following comprehensive psychological and exclusion of comorbidities, citing insufficient evidence that benefits exceed potential harms like impaired and . Norway's regional health authorities, in a 2024 directive, classified blockers for minors as experimental s requiring inclusion in controlled research protocols, restricting approvals to cases with rigorous oversight due to weak evidence on reversibility and long-term outcomes.

Bodies endorsing broader access

The Endocrine Society's 2017 clinical practice guidelines recommend initiating suppression with GnRH analogues for gender-dysphoric adolescents at Stage G2/B2, provided they demonstrate persistent gender incongruence and have decisional capacity, framing it as a reversible to alleviate distress while allowing further exploration of . These guidelines, reaffirmed in subsequent statements, emphasize that suppression should follow comprehensive but endorse access for qualifying to prevent irreversible pubertal changes misaligned with . The (AAP) maintains support for puberty blockers as part of gender-affirming care for and gender-diverse youth, as stated in its 2018 policy and reaffirmed in 2023 amid calls for systematic reviews, asserting that such interventions, when clinically indicated after multidisciplinary assessment, improve outcomes over alone. The AAP has opposed legislative restrictions, describing bans as harmful and contrary to , while acknowledging the need for ongoing research into long-term effects. The World Professional Association for Health (WPATH) in its Standards of Care Version 8 (2022) endorses suppression for adolescents with to provide developmental space for identity consolidation, recommending it after screening and , without strict age minima beyond onset, and positioning it as a bridge to potential . WPATH guidelines stress flexibility in application, critiquing overly rigid restrictions and advocating for clinician judgment in access. The (AMA), through a 2023 resolution co-sponsored by the , opposes barriers to evidence-based gender-affirming care including puberty blockers for minors, urging protection against state-level bans and affirming their role in treating based on existing clinical consensus. Similarly, the Pediatric Endocrine Society supports suppression for adolescents meeting diagnostic criteria, aligning with recommendations for timely intervention to mitigate psychological harm. These U.S.-centric positions contrast with international shifts toward caution, yet persist in advocating broader clinical availability amid debates over evidence quality.

Shifts in positions based on emerging evidence

In response to systematic reviews highlighting the low quality and paucity of evidence supporting the benefits of puberty blockers for , several medical authorities and professional bodies have revised their guidelines toward greater caution or restriction, prioritizing non-medical interventions and limiting pharmacological options to research settings. The UK's Cass Review, published in April , concluded that the evidence base for puberty suppression was of poor quality, with uncertain impacts on , , and long-term outcomes, prompting to restrict blockers to clinical trials for minors and close the in due to inadequate safeguarding and evidence. This shift marked a departure from prior affirmative approaches, emphasizing holistic assessments over routine medicalization. Similar evidence-driven reversals occurred in countries. Sweden's National Board of Health and Welfare updated its guidelines in 2022, determining that the risks of puberty blockers— including impacts on , , and —outweighed potential benefits outside controlled studies, restricting access accordingly after reviewing international data showing high desistance rates without intervention. 's Council for Choices in Health Care (COHERE Finland) issued updated recommendations in 2020, advising against routine use of blockers following a 2018-2020 review that found insufficient of mental health improvements and highlighted methodological flaws in supportive studies, favoring as first-line treatment. Denmark's health authorities followed suit in 2023, limiting blockers and cross-sex hormones to exceptional research cases after deeming the evidence base inadequate for standard care. These changes influenced further updates, such as Germany's 2025 guidelines from the Association of the Scientific Medical Societies, which incorporated findings to advocate diagnostic caution, comprehensive evaluations, and rarity of medical interventions for minors, reflecting a broader trend away from early blockade. Italy's National Bioethics Committee in December 2024 recommended prioritization and blocker use only in trials, citing weak and potential harms. In contrast, U.S. bodies like the and maintained endorsements as of 2025, though a U.S. Department of and review in May 2025 critiqued the limited for psychological benefits, signaling potential future reevaluation amid ongoing litigation and investigations. These shifts underscore a reliance on rigorous appraisal over observational data, with bodies acknowledging biases in earlier low-certainty studies that overstated .

References

  1. [1]
    Clinical applications of gonadotropin-releasing hormone analogues
    Therapeutic applications have progressed, and GnRH analogues currently have a diverse role in gynecologic care. ... Puberty suppression has been reported ...
  2. [2]
    [PDF] About puberty blockers | OHSU
    Supprelin LA is approved to treat children who start puberty early (precocious puberty). • Vantas is approved for adults who have an adult medical condition. It ...
  3. [3]
    [PDF] Puberty Suppression Treatment for Patients with Gender Dysphoria
    The use of puberty blockers in minors for the treatment of gender dysphoria is an off-label use. This means these medications are not approved by the FDA to ...
  4. [4]
    Puberty Suppression for Pediatric Gender Dysphoria and the Child's ...
    Apr 2, 2024 · Puberty Suppression for Pediatric Gender Dysphoria and the ... (GnRH) analogues, commonly referred to as puberty blockers. Drugs in ...
  5. [5]
    Interventions to suppress puberty in adolescents experiencing ...
    Apr 9, 2024 · Puberty blockers for youth experiencing gender dysphoria: A systematic review and meta-analysis. Anna Miroshnychenko, Archives of Disease in ...
  6. [6]
    Gender medicine 'built on shaky foundations', Cass review finds
    Apr 10, 2024 · Analysis finds most research underpinning clinical guidelines, hormone treatments and puberty blockers to be low quality.
  7. [7]
    Bone health in transgender people: a narrative review - Sage Journals
    May 27, 2022 · However, data on fracture risk are still sparse and the long-term effects of puberty blockers on bone health remain uncertain. The impaired bone ...<|separator|>
  8. [8]
    Risks and Benefits of Puberty Suppression - Oxford Academic
    Jun 22, 2023 · ... Puberty Blockers and Loss of Bone Mineral Density'. 25. Vlot et al., 'Effect of Pubertal Suppression and Cross-sex Hormone Therapy on Bone ...
  9. [9]
    Pediatric Gender Affirming Care is Not Evidence-based
    May 10, 2025 · This paper reviews outcomes for risks and benefits of puberty blockers and gender-affirming hormones for pediatric gender dysphoria or gender-related distress.
  10. [10]
    Ban on puberty blockers to be made indefinite on experts' advice
    Dec 11, 2024 · Evidence reviews by NICE and NHS England, supported by Dr Cass, clearly showed there is not enough evidence to support the safety or clinical ...
  11. [11]
    [PDF] Impact of Puberty Blockers in Gender-Dysphoric Adolescents
    Because of these limitations, the long-term outcomes of puberty blockers on mental health and wellbeing could not be evaluated and remains unknown. The ...
  12. [12]
    Gonadotropin Releasing Hormone (GnRH) Analogues - NCBI - NIH
    Mar 20, 2018 · Leuprolide, goserelin, triptorelin and histrelin are considered GnRH agonists, whereas degarelix acts predominantly as an antagonist.
  13. [13]
    Use of Hormone Blockers in Transgender Teenagers - NIH
    Dec 20, 2024 · Hormone blockers or gonadotropin-releasing hormone agonists (GnRHas) are substances that block pituitary receptors (GnRH receptors), thereby ...
  14. [14]
    Clinical pharmacology in adolescent transgender medicine - PMC
    Oct 1, 2025 · Systematic Review: Puberty suppression with GnRH analogues in adolescents with gender incongruity. Journal of Endocrinological Investigation ...
  15. [15]
    Puberty blockers for transgender and gender-diverse youth
    Jun 14, 2023 · Puberty blockers can be used to delay the changes of puberty in transgender and gender-diverse youth who have started puberty.
  16. [16]
    Puberty Blockers: What You Should Know - Cedars-Sinai
    Jan 16, 2023 · Endocrinologists mainly treat precocious puberty with GnRH analogues. These puberty-blocking drugs postpone the process by suppressing ...Missing: definition | Show results with:definition
  17. [17]
    Effectiveness of Puberty Suppression with Gonadotropin-Releasing ...
    The type of GnRHa used, histrelin implant (Supprelin or Vantas) versus leuprolide injections, differed between groups. Vantas and Supprelin were more frequently ...
  18. [18]
    Puberty Blockers: A Review of GnRH Analogues in Transgender Youth
    Jan 30, 2022 · Common examples include elagolix (Orilissa), degarelix (Firmagon), cetrorelix (Cetrotide), ganirelix (Orgalutran; Antagon) and relugolix ( ...
  19. [19]
    Puberty suppression in adolescents with gender dysphoria
    Controversy exists over puberty suppression (PS) in adolescents with gender dysphoria (GD). PS is preferentially achieved with GnRH analogues.
  20. [20]
    Pharmacological Management of Trans and Gender-Diverse ...
    Puberty suppression in adolescents with gender identity disorder: a ... Bone development in transgender adolescents treated with GnRH analogues and subsequent ...
  21. [21]
    Physiology of GnRH and Gonadotrophin Secretion - Endotext - NCBI
    Oct 15, 2024 · Conceptually, an abnormal reactivation of GnRH pulse frequency is the central mechanism associated with precocious or delayed puberty (14). In ...
  22. [22]
    The Gonadotropin-Releasing Hormone Analogue Therapy May Not ...
    Gonadotropin-releasing hormone analogues (GnRHa) have been used in the treatment of precocious puberty since 1980 [4]. The main aim in treating cases diagnosed ...
  23. [23]
    Treatment of Central Precocious Puberty - PMC
    Long-acting analogs of GnRH (GnRHas) have been the gold-standard treatment of central precocious puberty (CPP) worldwide and have an enviable track record ...
  24. [24]
    Clinical development of the GnRH agonist leuprolide acetate depot
    Leuprolide acetate was the first GnRH agonist used for the treatment of CPP (22, 23). It was initially developed as monthly intramuscular injections (7.5, 11.25 ...
  25. [25]
    Precocious Puberty and GnRH Analogs: Current Treatment ...
    May 8, 2024 · In 1993, leuprolide, Lupron Depot® (AbbVie Inc.), was the first GnRHa approved by the FDA for treatment of CPP, defined by the onset of ...Abstract · Introduction and Historical... · Results · Discussion<|separator|>
  26. [26]
    LUPRON DEPOT-PED® (leuprolide acetate for depot suspension)
    LUPRON DEPOT-PED IS THE #1* PRESCRIBED GnRHa FOR CENTRAL PRECOCIOUS PUBERTY (CPP) IN THE US1. GnRH agonists are standard of care for treatment of CPP2,3.
  27. [27]
    The Dutch Protocol for Juvenile Transsexuals: Origins and Evidence
    Sep 19, 2022 · The main evidence for the Dutch protocol came from a longitudinal study of 70 adolescents who had been subjected to puberty suppression followed ...
  28. [28]
    The Dutch Protocol for Juvenile Transsexuals: Origins and Evidence
    Sep 19, 2022 · It has been a quarter of a century since Dutch clinicians proposed puberty suppression as an intervention for juvenile transsexuals.
  29. [29]
    [PDF] History of and Evidence for Puberty Suppression as Intervention
    Oct 16, 2025 · The first traces the origins of this intervention back to the 1990s, when Dutch gender clinicians began experimenting with Gonadotropin- ...
  30. [30]
    Gender Dysphoria/Gender Incongruence Guideline Resources
    Oct 25, 2024 · The 2017 Endocrine Treatment of Gender-Dysphoric/Gender-Incongruent Persons is an update to the 2009 version, which establishes and ...
  31. [31]
    Endocrine Treatment of Gender-Dysphoric/Gender-Incongruent ...
    We recommend against puberty blocking followed by gender-affirming hormone treatment of prepubertal children. Clinicians should inform pubertal children, ...
  32. [32]
    SOC8 History - WPATH
    The Standards of Care (SOC) were originally published in 1979. Updated Standards of Care were published in 1980, 1981, 1990, 1998, 2001, and 2011.Missing: puberty blockers dysphoria
  33. [33]
    The Dutch Studies and The Myth of Reliable Research in Pediatric ...
    Jan 11, 2023 · The Dutch researchers began to medically transition gender dysphoric adolescents in the late 1980s and early 1990s—just as medicine was starting ...
  34. [34]
    Gender-Affirming Care for Trans Youth Is Neither New ... - Julia Serano
    May 16, 2023 · In the mid-1990s, doctors in the Netherlands began treating trans adolescents with puberty blockers at the onset of puberty, followed by gender ...
  35. [35]
    Puberty Suppression in Transgender and Gender-Diverse ... - NIH
    Recent data suggest puberty suppression is generally initiated among individuals once puberty has significantly progressed, thus reducing the effectiveness of ...
  36. [36]
    Precocious Puberty Medication: Gonadotropin-Releasing Hormone ...
    Jun 4, 2024 · In use since the late 1970s, GnRH agonists are safe and effective, resulting in decreased levels of LH, FSH, and sex steroids within 4 weeks ...
  37. [37]
    Gonadotropin-releasing hormone analog therapies for children with ...
    Oct 4, 2022 · Gonadotropin-releasing hormone agonists (GnRHa's) are the standard treatment for children with central precocious puberty (CPP).
  38. [38]
    Efficacy and Safety of Leuprolide Acetate 6-Month Depot for the ...
    Jun 1, 2023 · Six-month intramuscular LA depot demonstrated 48-week efficacy with a safety profile consistent with other GnRH agonist formulations.
  39. [39]
    Effectiveness of leuprolide acetate administered monthly compared ...
    Apr 25, 2024 · Conclusion: The 3-monthly treatment showed greater hormonal and growth suppression effects, but there was no significant difference in PAH ...
  40. [40]
    Precocious puberty: Treatment - UpToDate
    May 1, 2024 · TREATMENT FOR CENTRAL PRECOCIOUS PUBERTY · Decision to treat · Goals of treatment · GnRH agonist therapy · - Formulations and dosing · - ...
  41. [41]
    Efficacy of Leuprolide Therapy in Children With Central Precocious ...
    Growth velocity was slowed in all but one patient, and the rate of skeletal maturation was slowed even more, resulting in a stabilization or improvement in ...
  42. [42]
    Long-term efficacy and safety of gonadotropin-releasing hormone ...
    Conclusion: Compared with no treatment, evidence indicates that GnRHa treatment increase FAH and decrease BMI in girls with idiopathic CPP. GnRHa treatment did ...
  43. [43]
    The effects of gonadotropin-releasing hormone agonist on final adult ...
    This study aimed to explore the impact of gonadotropin-releasing hormone agonists (GnRHa) on final adult height (FAH) in girls with early and fast puberty.
  44. [44]
    Long-term effects of gonadotropin-releasing hormone analogs in ...
    Jan 31, 2015 · Long-term follow-up results obtained after GnRHa treatment indicated improvements in adult height. This treatment was largely reported to be effective.
  45. [45]
    Long-Term Efficacy and Safety of Leuprorelin Treatment in Children ...
    Conclusions: Leuprorelin treatment does not affect BMI or the onset of menstrual puberty in the long term, but has positive effects on adult height for children ...
  46. [46]
    Treatment of Central Precocious Puberty - Oxford Academic
    Mar 28, 2019 · Long-acting analogs of GnRH (GnRHas) have been the gold-standard treatment of central precocious puberty (CPP) worldwide and have an enviable track record of ...
  47. [47]
    Efficacy and safety of different doses of gonadotropin-releasing ...
    Jan 21, 2025 · This meta-analysis suggests that low-dose GnRHa is as effective as higher doses for treating precocious puberty in children and presents a better safety ...
  48. [48]
    The Effect of GnRHa Treatment on Body Mass Index in Central ...
    Jan 5, 2024 · Conclusion: For patients with CPP, while treatment with GnRHa may increase the BMI in the short term after treatment, the BMI is likely to ...Abstract · Introduction · Materials and Methods · Discussion
  49. [49]
    Efficacy of combined gonadotropin-releasing hormone analogue ...
    Oct 6, 2025 · Efficacy of combined gonadotropin-releasing hormone analogue and growth hormone therapy in girls with central precocious puberty: a systematic ...
  50. [50]
    Pharmacotherapy for children with central precocious puberty or ...
    Aug 1, 2025 · As the gold-standard therapy, gonadotropin-releasing hormone agonist (GnRHa) is commonly administrated to treat CPP, such as leuprorelin, ...
  51. [51]
    Transgender and Gender Diverse Children and Adolescents
    Jan 24, 2022 · Puberty blockers allow more time to explore gender identity, live in the experienced gender, and understand the medical and/or surgical options.Missing: 2009 2017
  52. [52]
    Trajectories of Adolescents Treated with Gonadotropin-Releasing ...
    Mar 9, 2020 · ... treatment protocol for gender dysphoria. All of them saw it as the ... Use of puberty blockers for gender dysphoria: A momentous step in the dark.
  53. [53]
    Standards of Care for the Health of Transgender and Gender ...
    The overall goal of the World Professional Association for Transgender Health's (WPATH) Standards of Care—Eighth Edition (SOC-8) is to provide clinical guidance ...
  54. [54]
    Puberty suppression in adolescents with gender dysphoria - Frontiers
    Jun 13, 2024 · Controversy exists over puberty suppression (PS) in adolescents with gender dysphoria (GD). PS is preferentially achieved with GnRH analogues.
  55. [55]
    Bone Development in Transgender Adolescents Treated With GnRH ...
    AbstractContext. Hormonal interventions in adolescents with gender dysphoria ... Bone Development in Transgender Adolescents Treated With GnRH Analogues ...
  56. [56]
    GnRH analogs as a monotherapy in transgender and gender ...
    The aim of this study was to evaluate the effects of GnRHa monotherapy in transgender adolescents with gender dysphoria (GD) at early versus late Tanner stages.
  57. [57]
    The experience of transfeminine adolescents and their parents ...
    Sep 13, 2024 · Treatment protocol. In the Centre of Expertise on Gender Dysphoria (CEGD), all adolescents are assessed by a mental health professional to ...
  58. [58]
    Puberty blockers for gender dysphoria in youth: A systematic review ...
    Puberty blockers, or gonadotropin releasing hormone analogues, suppress the release of sex hormones and delay puberty's physical changes, which normally begins ...
  59. [59]
    Evidence for puberty blockers and hormone treatment for gender ...
    Apr 10, 2024 · The evidence on the use of puberty blockers and hormones for children and young people experiencing gender related distress is wholly inadequate.<|separator|>
  60. [60]
    https://pubmed.ncbi.nlm.nih.gov/20646177/
  61. [61]
    Puberty blockers for gender dysphoric youth: A lack of sound science
    Sep 15, 2022 · GnRH-analogs have been used for decades to successfully delay the early onset of puberty in children with precocious puberty.
  62. [62]
    Young adult psychological outcome after puberty suppression and ...
    After gender reassignment, in young adulthood, the GD was alleviated and psychological functioning had steadily improved. Well-being was similar to or better ...
  63. [63]
    Children on puberty blockers saw mental health change - BBC
    Sep 18, 2023 · They found, after 12 months of puberty blocker injections - 34% of the children had reliably deteriorated, 29% had reliably improved, and 37% ...
  64. [64]
    U.S. Study on Puberty Blockers Goes Unpublished Because of ...
    Oct 24, 2024 · The leader of the long-running study said that the drugs did not improve mental health in children with gender distress and that the finding ...
  65. [65]
    [PDF] Treatment for Pediatric Gender Dysphoria
    May 1, 2025 · Following the publication of the Dutch Protocol in 2006,1 puberty blockers (PBs) and cross-sex hormones (CSH) were incorporated into the ...<|separator|>
  66. [66]
    Children and adolescents in the Amsterdam Cohort of Gender ...
    Jan 26, 2023 · To study trends in trajectories in children and adolescents who were referred for evaluation of gender dysphoria and/or treated following the Dutch Protocol.
  67. [67]
    Puberty blockers are more than a 'pause button': roughly 98% of ...
    Similarly, a Dutch study reported that only 1.9% of adolescents who started puberty suppression treatment abandoned this course and did not take cross-sex ...Missing: protocol | Show results with:protocol
  68. [68]
    Tavistock puberty blocker study published after nine years - BBC
    Dec 11, 2020 · "The evidence shows that the vast majority of children who take [puberty blockers] move on to take cross-sex hormones," and that these are part ...
  69. [69]
    Early Intervention Study shows puberty blockers are a well-received ...
    Feb 2, 2021 · ... rate varies, but is typically in the 2-5% range. However, one young person did stop treatment without progressing to cross-sex hormones.
  70. [70]
    The Final Cass Review and the NHS England Response - SEGM
    Apr 11, 2024 · This is not a “new development” as the problems with using puberty blockers for gender dysphoria were already part of the interim Cass Report, ...
  71. [71]
    New "20-year" Study from Amsterdam's VUmc Youth Gender Clinic
    Feb 2, 2023 · It required an early childhood onset of gender dysphoria, increase of gender dysphoria after pubertal changes, absence of significant ...
  72. [72]
    Was a puberty blockers trial ever ethical? - Transgender Trend
    Mar 4, 2025 · And that is that puberty blockers almost inevitably lead to cross sex hormones (CSH). In the case of the EIS it was 98% of the study ...
  73. [73]
    Long-term effects and significant adverse drug reactions (ADRs ...
    Moreover, short term side effects such as headaches, hot flushes, mood swings and injection site reactions (rashes, bruising and sterile abscess formation) have ...
  74. [74]
    Important Safety Information | LUPRON DEPOT-PED® (leuprolide ...
    The most common (≥4%) adverse reactions in clinical studies with LUPRON DEPOT-PED 45 mg for 6-month administration were: injection site reactions, headache, ...Missing: short- | Show results with:short-
  75. [75]
    Short-term outcomes of pubertal suppression in a selected cohort of ...
    Anticipated side effects of treatment were common, particularly mild symptoms directly related to suppression of sex hormones. Severe symptoms were uncommon.
  76. [76]
    Leuprolide and triptorelin treatment in children with idiopathic ...
    May 17, 2023 · Pain at the injection site is one of the most common side effects, followed by short term side effects like headache, mood swings, nausea, ...
  77. [77]
    Leuprolide: Pediatric Medication | Memorial Sloan Kettering Cancer ...
    What are some other side effects of this drug? · Irritation where the shot is given. · Headache. · Hot flashes. · Sweating a lot. · Pimples (acne). · Weight gain.Missing: short- | Show results with:short-
  78. [78]
    Leuprolide, pediatric (Fensolvi, Lupron Depot-Ped) - Uses ... - WebMD
    Feb 5, 2025 · The most common side effects are pain or irritation at the injection site and common cold symptoms. This medicine may cause the symptoms of ...Missing: short- | Show results with:short-
  79. [79]
    Leuprolide (intradermal route, intramuscular route, subcutaneous ...
    Sep 30, 2025 · Check with your doctor right away if your child has blurred or double vision, change in ability to see colors, especially blue or yellow, ...
  80. [80]
    Bone Mineral Density in Transgender Adolescents Treated With ...
    Dec 1, 2023 · Bone mineral density (BMD) z scores in transgender adolescents decrease during puberty suppression with a gonadotropin-releasing hormone (GnRH) agonist.Missing: loss | Show results with:loss
  81. [81]
    Fertility concerns of the transgender patient - PMC - PubMed Central
    Transgender individuals who undergo gender-affirming medical or surgical therapies are at risk for infertility. Suppression of puberty with gonadotropin- ...
  82. [82]
    Research Methodologies to Evaluate Neurodevelopmental Effects of ...
    If pubertal suppression disrupts aspects of neurodevelopment, it is possible these effects are temporary, with youth “catching up” developmentally after ...
  83. [83]
    Cass Review: Gender care report author attacks 'misinformation' - BBC
    Apr 20, 2024 · Dr Hilary Cass's review this month found "remarkably weak" evidence on treatments such as puberty blockers.
  84. [84]
    Longer treatment with puberty-delaying medication in transgender ...
    Jun 12, 2022 · The Endocrine Society Clinical Practice Guidelines recommend treatment with gonadotropin-releasing hormone agonists, or puberty-delaying ...
  85. [85]
    Gender dysphoria: puberty blockers and loss of bone mineral density
    Dec 4, 2019 · The effect of GnRH analogue treatment on bone mineral density in young adolescents with gender dysphoria: findings from a large national cohort.<|separator|>
  86. [86]
    Association of Gonadotropin-Releasing Hormone Analogue Use ...
    Nov 1, 2022 · Systematic review: puberty suppression with GnRH analogues in adolescents with gender incongruity. ... adolescents with gender dysphoria.  J ...
  87. [87]
    Fertility preservation: is there a model for gender-dysphoric youth?
    Apr 10, 2025 · However, the use of puberty blocking medications, cross-sex hormones, and genital surgeries can adversely affect fertility and the ability to ...Fertility preservation in cancer... · Fertility preservation in gender... · Conclusion
  88. [88]
    Cass Review Final Report
    No information is available for this page. · Learn why
  89. [89]
    HHS Releases Comprehensive Review of Medical Interventions for ...
    May 1, 2025 · HHS released a comprehensive review of evidence and best practices for promoting the health of youth with gender dysphoria.
  90. [90]
    HHS report critiques health care for transgender children and ... - NPR
    May 1, 2025 · The Department of Health and Human Services published a 400-page document entitled "Treatment for Pediatric Gender Dysphoria: Review of Evidence and Best ...
  91. [91]
    Puberty blockers for gender dysphoria in youth: A systematic review ...
    May 16, 2025 · In this systematic review, we assess and summarise the certainty of the evidence about the effects of puberty blockers in individuals experiencing GD.
  92. [92]
    Puberty blockers for gender dysphoria in youth: A systematic review ...
    Introduction. The use of puberty blockers in gender dysphoria remains controversial due to the methodological limitations of previously published evidence ...
  93. [93]
    McClain Probes $9.7 Million Taxpayer-Funded Study Buried by ...
    Nov 4, 2024 · One research study in this project, known as the Trans Youth Care (TYC) study, gave medical puberty blockers to 95 children in the early stages ...
  94. [94]
    Gender dysphoria in children: puberty blockers study draws further ...
    Sep 20, 2019 · 100% of puberty blocked children going onto cross sex hormones is remarkable in that it suggests that either clinicians are able to predict ...
  95. [95]
    [PDF] December 5, 2024
    Dec 5, 2024 · Cass, the delays from the American and British research groups have led the public to believe that puberty blockers improved mental health, even ...
  96. [96]
    Efficacy and safety of a 4-year combination therapy of growth ...
    Mar 16, 2023 · A four-year GH/GnRHa treatment in early pubertal girls with a poor PAH seems safe and results in a clinically relevant and statistically significant increase ...
  97. [97]
    The efficacy and safety of pharmacotherapy for girls with central ...
    Aug 29, 2025 · However, further observation and study of GnRHa revealed some issues. After treatment, the growth rate decreased to varying degrees among ...
  98. [98]
    A narrative review: treatment outcomes of central precocious puberty ...
    In this article, we review the treatment outcomes of GnRH agonists (GnRHa) on adult height, reproductive function, BMI, cardiovascular, and bone health in ...Introduction · Etiology · Treatment · Treatment outcomesMissing: protocol | Show results with:protocol<|separator|>
  99. [99]
    Is puberty delaying treatment 'experimental treatment'? - PMC
    Puberty delaying hormones are typically only prescribed to adolescents who suffer strong and persistent gender dysphoria (Hembree et al., 2017).
  100. [100]
    Looking at Gender Affirming Care Through the Lens of Justice
    Jun 6, 2025 · Precocious puberty has a much better known natural history and unlike GD can be diagnosed based on measurable biological variables. Puberty ...Missing: comparison | Show results with:comparison
  101. [101]
    Consent for treatment of gender dysphoria in minors - NIH
    Dec 12, 2021 · All three stages of treatment for gender dysphoria in children and adolescents require consent from all parties with parental responsibility.
  102. [102]
    https://www.judiciary.uk/judgments/bell-v-tavistock-and-portman-nhs-trust/
  103. [103]
    Full article: Puberty Blockers for Children: Can They Consent?
    Jun 27, 2022 · Yet over 90% of those treated with puberty blockers progress to cross-sex hormones and often surgery, with irreversible consequences.
  104. [104]
    Capacity to consent: a scoping review of youth decision-making ...
    Oct 8, 2024 · This scoping review identified the currently available data regarding adolescent capacity to consent to gender-affirming medical treatments.
  105. [105]
    This Wasn't a Split-Second Decision”: An Empirical Ethical Analysis ...
    The aims of this paper are therefore to provide an empirical analysis of minor trans youth capacity to consent to hormone therapy.
  106. [106]
    https://pubmed.ncbi.nlm.nih.gov/26754056/
  107. [107]
    A Follow-Up Study of Boys With Gender Identity Disorder - Frontiers
    In childhood, 88 (63.3%) of the boys met the DSM-III, III-R, or IV criteria for gender identity disorder; the remaining 51 (36.7%) boys were subthreshold for ...
  108. [108]
    False Assumptions Behind Youth Gender Transitions - SEGM
    Dec 30, 2022 · Further, the high rate of childhood desistance from gender dysphoria before maturity, (61-98%) and growing evidence of desistance among youth ...<|separator|>
  109. [109]
    Gender Identity 5 Years After Social Transition | Pediatrics
    Jul 13, 2022 · We found that an average of 5 years after their initial social transition, 7.3% of youth had retransitioned at least once.Missing: systematic | Show results with:systematic
  110. [110]
    The Cass Review Into Gender Identity Services for Children - Part 4
    May 10, 2024 · The Cass review argues that most kids used to grow out of gender dysphoria. This is used as part of the argument against providing them with medical care.
  111. [111]
    Exploring Desistance in Transgender and Gender Expansive Youth ...
    Desistance is a concept that has been poorly defined in the literature, yet greatly impacts the arguments for and against providing gender-affirming care.
  112. [112]
    Why detransitioners are crucial to the science of gender care - Reuters
    Dec 22, 2022 · Researchers found that 98% of 720 adolescents who started on puberty blockers before taking hormones had continued with treatment after four ...
  113. [113]
    Gender detransition: A critical review of the literature - PMC - NIH
    Four patients because their gender dysphoria had desisted (5.1%) and three patients because of non-compliance with the treatment protocol (3.8%). j Three after ...<|separator|>
  114. [114]
    Accurate transition regret and detransition rates are unknown - SEGM
    Sep 11, 2023 · The median time for surgical regret has been reported to be as much as 8 years. Somewhat shorter average times (3-6 years) to detransition have ...
  115. [115]
    Study of 1,655 Cases Supports the "Rapid-Onset Gender Dysphoria ...
    Mar 30, 2023 · Study of 1,655 Cases Supports the "Rapid-Onset Gender Dysphoria" Hypothesis · 57% had a prior history of mental health issues and 43% had a ...
  116. [116]
    Rapid Onset Gender Dysphoria: Parent Reports on 1655 Possible ...
    Mar 29, 2023 · One influential if controversial explanation is that the increase reflects a socially contagious syndrome: Rapid Onset Gender Dysphoria (ROGD).Missing: contagion | Show results with:contagion
  117. [117]
    Gender dysphoria in adolescence: examining the rapid-onset ... - NIH
    Rapid-onset gender dysphoria and social contagion​​ Dishion and Tipsord [63] define “peer contagion” as a process of reciprocal influence among peers that ...
  118. [118]
    Gender-Affirming Treatment of Gender Dysphoria in Youth - NIH
    Nov 14, 2022 · A recent editorial in The Lancet stated puberty blockers reduce suicidality and to remove access to them was to “deny” life (The Lancet, 2021).
  119. [119]
    The ​Myth of the "Desistance Myth" - Public Discourse
    Jul 2, 2018 · Gender dysphoric children who are treated using a “watchful waiting” approach largely desist, no longer identify as transgender as adults ...
  120. [120]
    Early Social Gender Transition in Children is Associated with High ...
    May 6, 2022 · A new study lends credibility to concerns that early social gender transition can lead to persistence of pediatric gender dysphoria.
  121. [121]
    Desisting from gender dysphoria after 1,5 years of puberty ...
    This case report illustrates that after treatment with puberty blockers desistance from gender dysphoria can occur.
  122. [122]
    Sweden's Karolinska Ends All Use of Puberty Blockers and Cross ...
    May 5, 2021 · ALB has ended the practice of prescribing puberty blockers and cross-sex hormones to gender-dysphoric patients under the age of 18.
  123. [123]
    2025 German Guidelines for Diagnosis and Treatment of Gender ...
    Mar 26, 2025 · The Guidelines note that initiating puberty blockers at Tanner Stage 2, followed by cross-sex hormones, typically leads to infertility (“If ...
  124. [124]
    What Went Wrong at the Tavistock Clinic for Trans Teenagers? | SEGM
    Jun 17, 2022 · The number of teenage girls with gender dysphoria (ie profound discomfort with their biological sex) had risen by 5,000 per cent in 7 years. My ...<|separator|>
  125. [125]
    https://www.socialstyrelsen.se/globalassets/sharepoint-dokument/dokument-webb/national-guidelines-for-care-in-cases-of-gender-dysphoria.pdf
  126. [126]
    Swedish Transgender Treatment Guidelines for Youth - SEGM
    Sep 24, 2024 · By December 2022, however, Sweden had fully updated its official treatment recommendations (Vård av barn och ungdomar med könsdysfori), but only ...
  127. [127]
    Norway Agency: Revise Gender Transition Guidelines Because ...
    May 24, 2023 · Norwegian minors can change their gender markers in the civil registry from age six with parental consent, and from age 16 without parental ...
  128. [128]
    Denmark Joins the List of Countries That Have Sharply Restricted ...
    Aug 17, 2023 · For purposes of comparison, the Netherland's Amsterdam gender clinic reports transitioning 73% of late-onset referrals and 85% of early-onset ...
  129. [129]
    NHS England » Children and young people's gender services
    Gonadotropin releasing hormone analogues: Also known as hormone blockers and puberty blockers; taking these hormones stops the progress of puberty. The GnRH ...
  130. [130]
    Italy Joins the List of Countries Recommending Restrictions on ...
    Dec 19, 2024 · Puberty blocker prescriptions for gender dysphoria should occur only after the documented failure of psychotherapy or psychiatric interventions.Missing: global | Show results with:global
  131. [131]
    Policy Tracker: Youth Access to Gender Affirming Care and State ...
    This tracker provides an overview of state laws/policies restricting minor access to gender affirming care and any associated litigation by state, ...Missing: capacity | Show results with:capacity
  132. [132]
    Queensland halts prescription of puberty blockers and hormones for ...
    Jan 28, 2025 · Children with gender dysphoria will be denied puberty blockers as a state government reviews hormone therapies for minors.
  133. [133]
    National Academy of Medicine in France Advises Caution in ... - SEGM
    Mar 3, 2022 · If France allows the use of puberty blockers or cross-sex hormones with parental authorization and no age limitations, the greatest caution is ...
  134. [134]
    The UK is the latest country to ban puberty blockers for trans kids ...
    Dec 13, 2024 · The United Kingdom has banned puberty blockers for children and adolescents under age 18, making it the latest country in Western Europe to limit access to the ...
  135. [135]
    Puberty Suppression for Pediatric Gender Dysphoria and the Child's ...
    Apr 2, 2024 · We evaluate claims that puberty blockers are reversible, discuss the scientific uncertainty about long-term benefits and harms, summarize ...<|separator|>
  136. [136]
    Europe Adopts A Cautious Approach To Gender-Affirming Care For ...
    Jun 6, 2023 · The updated guidelines would restrict the use of puberty blockers, cross-sex hormones and transition-related surgery to clinical research ...
  137. [137]
    27 States Have Restricted Gender-Transition Treatments for Minors ...
    Jun 18, 2025 · Twenty-five states have now enacted laws that restrict doctors from providing puberty blockers, hormone therapies or surgery to transgender minors.Missing: regulations | Show results with:regulations
  138. [138]
    States that have passed laws restricting gender-affirming care ... - CNN
    Dec 4, 2024 · In 2024, Ohio, Wyoming, South Carolina and New Hampshire joined the list of states banning gender-affirming care for transgender youth, and ...
  139. [139]
    [PDF] The Truth About 'Puberty Blockers' - Congress.gov
    Aug 4, 2023 · The Truth About 'Puberty Blockers'. The FDA hasn't approved them for gender dysphoria, and their e ects are serious and permanent. By Gerald ...
  140. [140]
    States With Bans on Gender-Affirming Care for Minors
    Dec 4, 2024 · Transgender minors and their parents, guardians and doctors have challenged bans in 18 states, with mixed results.
  141. [141]
    Protecting Children from Chemical and Surgical Mutilation
    Jan 28, 2025 · ... puberty blockers, including GnRH agonists and other interventions, to delay the onset or progression of normally timed puberty in an ...
  142. [142]
    States are banning gender-affirming care for minors. What does that ...
    Feb 20, 2024 · More than 20 US states have banned or severely limited treatment to align a young person's body with their gender identity.Missing: capacity | Show results with:capacity
  143. [143]
    How Alberta's proposed trans youth rules fit into a polarized ... - CBC
    Mar 11, 2024 · Under the government's new plan, mature teens aged 16 and 17 would be able to use puberty blockers and hormone therapies for gender affirmation ...
  144. [144]
    Alberta government appeals temporary injunction of transgender ...
    Aug 8, 2025 · The law bans doctors from providing treatment such as puberty blockers and hormone therapy to those under 16. Opinion: The real health care wait ...
  145. [145]
    Alberta restrictions for transgender youth 'extremely dangerous'
    Feb 1, 2024 · She plans to restrict the medical treatments they may seek, including prohibiting hormonal treatment, puberty blockers and gender-affirming ...
  146. [146]
    B.C. bill that would have stopped doctors from providing puberty ...
    Oct 8, 2025 · A summary of the proposed bill provided by the One BC Party says it would have also stopped doctors from providing puberty blockers to minors, ...
  147. [147]
    Treatment of gender dysphoria in children - Queensland Health
    Jan 28, 2025 · Puberty Blockers or Sex Hormones will continue to be prescribed for a medical condition other than Gender Dysphoria. 5. Mandatory requirements.
  148. [148]
    Independent review of Stage 1 and Stage 2 hormone therapies in ...
    On 28 January 2025, the Queensland Government announced an independent review of the evidence for using puberty suppression (Stage 1) and gender-affirming ...Missing: national | Show results with:national
  149. [149]
    Health care for trans and gender diverse Australian children and ...
    Jan 31, 2025 · Interim advice on the use of puberty blockers will be completed in the middle of 2026. More information will be available on the NHMRC's ...
  150. [150]
    What are puberty blockers? What are the benefits and risks for ...
    Sep 2, 2024 · Puberty blockers are medications that stop the body from producing oestrogen and testosterone. In the clinic, they're called gonadotropin-releasing hormone ...
  151. [151]
    Consultation on safety measures for the use of puberty blockers in ...
    Nov 21, 2024 · The consultation on safety measures for the use of puberty blockers in young people with gender-related health needs closed on 20 January 2025.
  152. [152]
    Additional safeguards for puberty blockers | Ministry of Health NZ
    Nov 21, 2024 · The evidence brief shows a lack of good quality evidence to back the effectiveness and safety of puberty blockers when used for this purpose.
  153. [153]
    https://www.1news.co.nz/2025/10/25/govts-puberty-blockers-decision-holding-up-life-or-death-health-guidelines/
  154. [154]
    MOH Evidence Review, Position Statement and Consultation on the ...
    Dec 16, 2024 · The Position Statement sets out expectations of greater precaution in the prescribing of puberty blockers to transgender young people. It also ...
  155. [155]
    [PDF] 22 January 2025 Ministry of Health 133 Molesworth Street Thorndon ...
    Jan 22, 2025 · We consider the proposed regulations for puberty blockers should not disadvantage adolescents experiencing gender-related distress. Puberty ...
  156. [156]
    Analysis of puberty blockers review
    Dec 2, 2024 · In New Zealand currently, there is no specific legislation related to puberty blockers, only good practice guidelines to enable clinicians ...
  157. [157]
    Argentina to ban hormone therapy for trans children | Reuters
    Feb 5, 2025 · Argentina's presidential office said on Wednesday that President Javier Milei had taken the decision to ban gender change treatments and ...
  158. [158]
    Argentina's president bans gender-affirming care for anyone under 18
    Feb 5, 2025 · A presidential spokesperson announced the repeal of a 2012 gender identity law provision allowing such practices with parental or guardian ...
  159. [159]
    Brazil prohibits hormone therapy for transgender minors
    Apr 16, 2025 · Brazilian health authority raises legal age for transgender people to receive hormone therapy from 16 to 18; Also raises minimum age for ...<|separator|>
  160. [160]
    Gender-affirming care by country - Equaldex
    Legal, but restricted for minors · Asia (3) · Israel 2014 · Japan 1997 · Singapore · Europe (9) · Andorra 2025 · Finland 2020 · Hungary ...Missing: puberty blockers
  161. [161]
    Japan Court Drops Key Legal Hurdle for Transgender People
    Sep 29, 2025 · A court in Japan has ruled that the legal requirement that transgender people alter the appearance of their genitals to change their legal ...
  162. [162]
    NHS England Stops Prescribing Puberty Blockers and Updates its ...
    Mar 29, 2024 · NHS England will no longer allow puberty blockers for gender dysphoria, while the updated cross-sex hormones policy suggests a move toward caution.
  163. [163]
    Evidence for puberty blockers use very low, says NICE - BBC
    Apr 1, 2021 · The NICE evidence review looked at what impact puberty blockers had on gender dysphoria, mental health - such as depression, anger and anxiety - ...
  164. [164]
    Understanding the landscape on European trans health care policy
    Aug 21, 2025 · In 2024, the U.K. government banned new prescriptions of puberty blockers to those under 18. (Patients who are already taking these ...Missing: 2020-2025 | Show results with:2020-2025
  165. [165]
    Finland Takes Another Look at Youth Gender Medicine
    Feb 20, 2023 · ... restricted cases—the use of puberty blockers and cross-sex hormones to treat adolescent gender dysphoria. By 2015, however, Finnish gender ...
  166. [166]
    Tighten up gender clinics - by Bernard Lane
    Feb 29, 2024 · The medical directors of Norway's four health regions have determined that puberty blockers ... change in minors is very weak and uncertain.
  167. [167]
    An Endocrine Society Clinical Practice Guideline - PubMed
    Nov 1, 2017 · We recommend treating gender-dysphoric/gender-incongruent adolescents who have entered puberty at Tanner Stage G2/B2 by suppression with ...Missing: blockers | Show results with:blockers
  168. [168]
    Endocrine Society Statement in Support of Gender-Affirming Care
    May 8, 2024 · The guideline recommends beginning treatment with puberty-delaying medications that are generally reversible. As adolescents grow older and can ...
  169. [169]
    Medical Group Backs Youth Gender Treatments, but Calls for ...
    Aug 3, 2023 · The American Academy of Pediatrics backed gender-related treatments for children on Thursday, reaffirming its position from 2018 on a medical approach that has ...
  170. [170]
    AAP: High court ruling sets dangerous precedent, undermines ...
    Jun 18, 2025 · Tennessee's law, known as SB1, bans puberty blockers and hormones as part of gender-affirming care for minors. In a 6-3 ruling, Chief ...
  171. [171]
    Standards of Care Version 8 - WPATH
    The Standards of Care 8 revision started by identifying a multidisciplinary team of clinicians, researchers and stakeholders using a clearly defined process.SOC8 Chapters · View SOC8 Translation Page · SOC8 History · IJTH
  172. [172]
    AMA strengthens its policy on protecting access to gender-affirming ...
    Jun 12, 2023 · The American Medical Association (AMA) House of Delegates today passed the Endocrine Society's resolution to protect access to evidence-based gender-affirming ...Missing: endorsing | Show results with:endorsing
  173. [173]
    [PDF] Pubertal Suppression for Youth with Gender Dysphoria/Gender ...
    When are puberty blockers used? These medications can prevent or stop development of the body changes associated with puberty. For those assigned.
  174. [174]
    Europe And US Diverge On Treatment Of Gender Incongruence In ...
    Dec 2, 2023 · Treatment with puberty blockers can only be initiated starting at the age of 12. Interventions with clearly irreversible effects, which include ...
  175. [175]
    HHS breaks with major U.S. medical groups in review of pediatric ...
    May 2, 2025 · The HHS review found that there is limited evidence regarding the effects of medical interventions for youth with gender dysphoria on psychological outcomes.
  176. [176]
    European Academy of Paediatrics statement on the clinical ... - NIH
    Feb 5, 2024 · We review the current ethical and legal dilemmas facing children with gender dysphoria, their families and the clinical teams caring for them.