The contraceptive vaginal ring is a small, flexible, polymer-based device inserted into the vagina by the user, which continuously releases a combination of synthetic progestin (etonogestrel) and estrogen (ethinylestradiol) through the vaginal mucosa to prevent pregnancy primarily by inhibiting ovulation, thickening cervical mucus to impede sperm migration, and thinning the endometrial lining to reduce implantation potential.[1] This localized delivery method results in lower systemic hormone exposure compared to oral contraceptives while maintaining steady serum levels.[2]First developed through research beginning in the 1970s, the vaginal ring gained commercial availability in the early 2000s with the approval of NuvaRing by regulatory bodies such as the FDA in 2001, marking a significant advancement in user-controlled hormonal contraception that requires no daily dosing.[3] Clinical trials have established its efficacy, with perfect-use Pearl Indices as low as 0.65 to 1.0 pregnancies per 100 woman-years, comparable to combined oral contraceptives, and high user acceptability due to ease of insertion, minimal interference with daily activities, and improved cycle control over pills.[1][2]Despite these benefits, empirical data from post-marketing surveillance and comparative studies indicate risks including vaginal irritation, discharge, headaches, nausea, and a venous thromboembolism incidence similar to that of combined oral contraceptives, underscoring the need for careful patient selection excluding those with contraindications like smoking over age 35 or history of thrombotic events.[1][2] Newer iterations, such as the reusable segesterone acetate/ethinylestradiol ring approved in 2018, extend options but share analogous hormonal risk profiles based on mechanistic similarities.30289-X/fulltext) Overall, the device's defining characteristics lie in its balance of convenience, efficacy, and localized administration, supported by randomized controlled trials demonstrating superior adherence potential over daily methods.[2]
History
Early development
The initial research into vaginal rings as intravaginal hormone delivery systems emerged in the early 1970s, building on siliconeelastomer materials like Silastic for controlled drug diffusion. The first clinical study, published in 1970, tested cylindrical silicone rubber rings impregnated with medroxyprogesterone acetate in regularly menstruating women to evaluate contraceptive effects through sustained progestin release.[4] These prototypes leveraged the polymer's ability to allow hormones to diffuse gradually from an impregnated matrix, enabling local absorption via the vaginal epithelium without requiring frequent dosing.[5]Subsequent 1970s investigations focused on empirical validation of release kinetics and bioavailability, demonstrating that intravaginal administration bypassed hepatic first-pass metabolism, resulting in more consistent systemic hormone levels than oral routes.[6] For example, early pharmacokinetic evaluations of progestin-loaded rings revealed steady daily release rates—such as 3-5 mg of medroxyprogesterone acetate over initial trial periods—correlating with measurable serum concentrations and ovulation suppression in animal and limited human models.[7] The World Health Organization concurrently prototyped rings incorporating progesterone, norethisterone, or norgestrel, prioritizing diffusion-controlled mechanisms to achieve prolonged, zero-order release profiles independent of vaginal pH or fluid variations.[6]By the 1980s, research shifted toward human feasibility trials, refining silicone-based designs to optimize epithelial permeation and minimize variability in hormone flux, with studies confirming absorption rates sufficient for therapeutic steady-state levels over weeks.[8] These efforts underscored the causal role of the vaginal mucosa's vascularity in facilitating direct hormone entry into circulation, supported by in vitro diffusion assays and serial plasma sampling that quantified bioavailability advantages over gastrointestinal delivery.[5]
Commercial approvals and milestones
The etonogestrel/ethinyl estradiol vaginal ring, marketed as NuvaRing by Organon, received initial marketing authorization in the Netherlands on February 14, 2001, marking the first commercial approval for a combined hormonal contraceptive ring in Europe.[9] The U.S. Food and Drug Administration (FDA) approved NuvaRing on October 3, 2001, establishing it as the inaugural combined estrogen-progestin vaginal ring available for contraception.[10] Subsequent mutual recognition procedures facilitated approvals across additional European Union countries, with expansions noted in territories including the United Kingdom, Estonia, Hungary, Latvia, Lithuania, and the Slovak Republic by 2007.[11]In 2018, the FDA approved Annovera (segesterone acetate/ethinyl estradiol), a reusable vaginal ring designed for up to one year of use, representing a milestone in extended-duration contraceptive options. This was followed in 2019 by the FDA approval of EluRyng on December 11, the first generic equivalent to NuvaRing, enhancing accessibility through competition.[12]A significant regulatory milestone occurred in 2013 when NuvaRing's labeling was updated to warn of elevated venous thromboembolism risks compared to certain other contraceptives, prompted by post-marketing data and litigation.[13] In 2014, manufacturer Merck settled approximately 2,200 lawsuits alleging inadequate warnings about blood clot risks for $100 million, influencing ongoing safety communications without altering approval status.[14]By the 2010s, clinical studies reported high user acceptability for vaginal rings, with a pooled prevalence of 85.6% favorable experiences among actual users, indicating growing preference among women seeking discreet, user-controlled long-acting contraception in surveyed demographics.[15]
Mechanism of action
Drug delivery system
The vaginal ring operates as a matrix-based sustained-release drug deliverysystem, utilizing a flexible polymer matrix composed of ethylene-vinyl acetate (EVA) copolymers to embed and control the release of hormones such as etonogestrel and ethinyl estradiol.[16][5] These copolymers, typically with 9% and 28% vinyl acetate content, provide rate-controlling properties that facilitate diffusion of the active agents.[16] The ring's physical structure features an outer diameter of 54 mm and a cross-sectional diameter of 4 mm, enabling comfortable intravaginal placement while maintaining structural integrity over the usage period. Drug release from the EVA matrix follows principles of passive diffusion, where hormones partition from the polymer into the surrounding vaginal fluid and subsequently absorb across the mucosal epithelium.[5] This process approximates zero-order kinetics, designed to deliver consistent daily doses—such as 120 μg of etonogestrel and 15 μg of ethinyl estradiol in combined contraceptive formulations—over three weeks, minimizing fluctuations in plasma concentrations compared to bolus dosing.[16][19] The release rate is influenced by factors including polymer composition, drug loading, and ring geometry, with surface drug initially dissolving rapidly before transitioning to matrix-controlled diffusion.[5]Compared to oral systemic delivery, the vaginal ring's localized administration bypasses gastrointestinal tract degradation and hepatic first-pass metabolism, enabling lower overall hormone doses to achieve therapeutic plasma levels through direct absorption by the vaginal epithelium.[20][21] This pharmacokinetic advantage results in reduced ethinyl estradiol exposure—approximately 35-50% lower than equivalent oral contraceptives—while preserving efficacy, as evidenced by steady-state serum concentrations that support ovulation suppression.[21][22] Such design principles enhance bioavailability efficiency and potentially mitigate dose-related side effects associated with higher systemic burdens in traditional routes.[20]
Hormonal effects on reproduction
The progestin component, such as etonogestrel released from combined vaginal rings, primarily exerts its contraceptive effect by suppressing the mid-cycle gonadotropin surge, thereby inhibiting follicle-stimulating hormone (FSH) and luteinizing hormone (LH) secretion from the anterior pituitary gland. This disruption prevents ovarian follicular development and maturation, resulting in the absence of ovulation.[2][23] In clinical studies evaluating etonogestrel/ethinylestradiol vaginal rings, ovulation was completely inhibited during the standard three-week insertion period, with no follicular growth exceeding 13 mm observed via ultrasound monitoring.[24][23]Additionally, etonogestrel alters cervical mucus composition, increasing its viscosity and forming a thick, impenetrable barrier that impedes sperm penetration and transport into the upper reproductive tract.[25] This local effect complements ovulation suppression, enhancing overall contraceptive reliability independent of systemic ovarian inhibition.[2]The estrogen component, typically ethinylestradiol, contributes to endometrial transformation by promoting a thin, decidualized lining that is less conducive to implantation, while also stabilizing the endometrium to minimize unscheduled bleeding.[26] Together, the steady release of these hormones mimics the constant progestin-dominant state of the luteal phase, overriding the natural hypothalamic-pituitary-ovarian axis feedback loops that drive the menstrual cycle.[25] Empirical data from pharmacokinetic and pharmacodynamic trials confirm that these combined hormonal actions sustain reproductive suppression throughout the usage cycle, with no ovulation resumption during continuous ring placement up to five weeks in controlled evaluations.[23][27]
Types
Combined estrogen-progestin rings
Combined estrogen-progestin vaginal rings incorporate both a progestin and ethinyl estradiol (EE) into a flexible silicone or copolymer matrix, enabling controlled transvaginal release of hormones over an extended period. These devices achieve steady systemic absorption, bypassing first-pass hepatic metabolism for potentially reduced side effects compared to oral counterparts.[28]NuvaRing consists of 11.7 mg etonogestrel (ENG), a progestin derived from desogestrel, and 2.7 mg EE embedded in an ethylene vinylacetate copolymer. It releases an average of 0.120 mg ENG and 0.015 mg EE daily during 21 days of continuous vaginal insertion, followed by a 7-day removal interval. Pharmacokinetic data from early development studies demonstrate near-complete bioavailability for ENG (>90%) and approximately 56% for EE via vaginal absorption, with consistent serum levels maintained throughout use. The U.S. Food and Drug Administration (FDA) approved NuvaRing on October 29, 2001.[29][25][28]Annovera, a reusable combined ring, contains 103 mg segesterone acetate (SGA, formerly nestorone), a potent progestin, and 17.4 mg EE in a silicone-based matrix. It delivers daily averages of 0.15 mg SGA and 0.013 mg EE, supporting 13 cycles of 21-day insertion and 7-day removal, after which the ring is washed and stored dry at room temperature. Stability testing confirms hormone release consistency across cycles without refrigeration. The FDA approved Annovera on August 10, 2018.[30][31]30265-7/fulltext)EluRyng, the first generic equivalent to NuvaRing, matches its formulation with 11.7 mg ENG and 2.7 mg EE, releasing equivalent daily doses. Bioequivalence was established through pharmacokinetic studies showing 90% confidence intervals for key parameters (AUC and C_max) within FDA acceptance limits of 80-125%. The FDA granted approval on December 11, 2019. Empirical absorption and stabilitydata from generic development align with the originator product.[12][32]
Progestin-only and alternative rings
Progestin-only vaginal rings release a progestogen such as progesterone or synthetic analogs without estrogen, thereby avoiding estrogen-associated risks like increased venous thromboembolism incidence observed in combined formulations.[33] These rings leverage progestogen's effects on cervical mucus thickening, endometrial thinning, and variable ovulation suppression to achieve contraception, with pharmacokinetic profiles enabling steady local absorption and lower systemic exposure compared to oral methods.[7]The progesterone vaginal ring (PVR), releasing approximately 10 mg of natural progesterone daily, is designed specifically for lactating women starting from six weeks postpartum, where it extends lactational amenorrhea when breastfeeding occurs at least four times daily.[34] Clinical trials in breastfeeding populations have reported cumulative one-year pregnancy rates below 2 per 100 women, with no disruption to milk production or infant growth, attributing efficacy to synergistic reinforcement of breastfeeding-induced hormonal inhibition.00350-1/abstract)[35] The PVR, marketed as Progering in select countries including parts of Latin America since 2013, is used continuously for three to four months per insertion, with removal only for hygiene, and demonstrates acceptability due to its non-interference with nursing.[36][37]Nestorone (segestaone)-only vaginal rings, delivering 100-200 μg daily, have undergone phase II and III trials showing ovulation suppression in over 95% of cycles across diverse populations, with steady-state serum levels achieved within days and sustained for 90-180 days per ring.[38][39] These prototypes target broader use beyond lactation, offering extended duration to improve compliance, though as of 2023, they remain investigational without FDA approval, pending further long-term safety data on bleeding patterns and bone density.[40]Early levonorgestrel-releasing rings, such as WHO prototypes emitting 20 μg daily, suppressed ovulation in pharmacokinetic studies of menstruating women, reducing plasma progesterone to follicular-phase levels (<1 ng/mL) throughout continuous use, with no pregnancies in small cohorts over 3-6 months.[41] Alternative formulations incorporate novel progestins like trimegestone (50 μg daily release), where phase I trials confirmed complete ovulation inhibition via luteinizing hormone surge blockade, comparable to combined rings but without estrogen, and with potential for monthly replacement to manage irregular bleeding.[42] Research into lower-dose variants, such as reduced etonogestrel prototypes, explores minimized progestogenic side effects like weight gain, while maintaining efficacy through optimized polymer matrices for consistent release rates of 50-100 μg daily.[33]
Non-contraceptive applications
Vaginal rings have been developed for hormone replacement therapy in postmenopausal women, particularly to address genitourinary syndrome of menopause (GSM), which includes symptoms such as vaginal dryness, atrophy, dyspareunia, and urinary urgency.[43] Estring, an estradiol-releasing ring containing 2 mg of estradiol that delivers approximately 7.5 micrograms per day over 90 days, is approved for treating moderate to severe vulvar and vaginal atrophy due to estrogen deficiency.[44] A multicenter study involving 175 women demonstrated that Estring significantly improved urogenital symptoms, with maturation index scores increasing by 24.5% after one year and minimal systemic estrogen exposure, confirming its efficacy and safety for long-term local therapy.[45]Randomized controlled trials (RCTs) support the use of low-dose vaginal estradiol rings for GSM relief, showing reductions in vaginal pH, improved epithelial integrity, and alleviation of dryness and painful intercourse without substantial endometrial proliferation or systemic hormone elevations.[43] A meta-analysis of 18 RCTs further indicated that intravaginal estrogen therapies, including rings, effectively mitigate postmenopausal vaginal atrophy and associated vaginitis, with standardized mean differences favoring treatment over placebo for symptom scores.[46] These local effects stem from direct tissue absorption, minimizing risks compared to oral estrogens.[47]Beyond hormone therapy, vaginal rings deliver antiretrovirals for HIV prevention as microbicides. The dapivirine ring, a silicone matrix containing 25 mg of the non-nucleoside reverse transcriptase inhibitor dapivirine, is designed for monthly self-insertion and release to prevent HIV-1 acquisition in women.[48] In the ASPIRE Phase III trial (MTN-020), involving over 2,600 participants in sub-Saharan Africa from 2011 to 2015, the ring reduced HIV-1 incidence by 27% overall (95% CI: 1-46) in intention-to-treat analysis, with higher efficacy (61%) among highly adherent users confirmed via residual drug levels.[48] The IPM Ring Study similarly reported a 37% reduction (95% CI: 21-50), establishing the ring's protective effect through sustained local drug concentrations in vaginal tissues.[49]Emerging applications include longer-duration dapivirine rings; a 2024 trial demonstrated a 3-month formulation achieving superior drug release profiles over the 1-month version, supporting potential for extended-use HIV pre-exposure prophylaxis.[50] Limited evidence also explores rings for dysmenorrhea relief, with one trial evaluating progestin-releasing prototypes for reducing primary dysmenorrhea severity independent of contraceptive intent.[51] These non-contraceptive uses highlight the ring's versatility as a sustained-release platform for targeted vaginal pharmacotherapy.
Usage
Insertion and removal procedures
The vaginal ring is designed for self-insertion by the user, typically performed in a comfortable position such as squatting, standing with one leg elevated, or lying down. Users should first wash their hands thoroughly with soap and water to minimize infection risk. The flexible ring is then compressed between the thumb and forefinger into a folded shape resembling a tampon, and gently inserted into the vagina using the same hand, aiming for the upper vaginal area behind the pubic bone. The exact position within the vagina does not affect efficacy, as hormone release occurs uniformly via transvaginal absorption regardless of precise placement.[52][53]Removal follows a similar self-managed process: after washing hands, the user inserts a lubricated finger into the vagina, hooks it under the ring's lower rim, and gently pulls downward and outward until the ring is expelled. For reusable rings such as Annovera, the retrieved device should be cleaned with mild soap and warm water, patted dry with a clean towel, and stored in its provided case at room temperature (20–25°C) to preserve material integrity for up to 13 cycles.[31][54]Studies indicate that unintended expulsion occurs in approximately 2–20% of users, with partial expulsions (where the ring slips partially out) reported at up to 19.8% and complete expulsions at around 7% in some cohorts; risks are higher with shallow insertion or during activities like tampon use or intercourse, but can be mitigated by ensuring deeper placement during insertion. Manufacturer protocols emphasize checking the ring's position periodically by touch to detect early slippage.[1][55]
Cycle management and compliance
The standard cycle for combined estrogen-progestin vaginal rings, such as NuvaRing, involves insertion on day 1 of the menstrual cycle (or days 2-5 if starting later), continuous wear for 21 days, followed by removal for a 7-day hormone-free interval to allow withdrawal bleeding, after which a new ring is inserted to maintain suppression of ovulation and endometrial buildup.[53][56] This regimen aligns hormone release with cyclic fluctuations to replicate natural menstrual patterns while preventing pregnancy. Extended or continuous use is possible under medical supervision to reduce bleeding frequency, but the 21/7 schedule remains the default for most users to optimize cycle control.[57]Compliance with vaginal ring use benefits from its monthly dosing, which demands less frequent action than daily pills, leading to reported 6-month continuation rates of 91% in comparative trials against oral contraceptives.[58] Real-world adherence is higher among motivated users, such as those in structured clinical settings or with strong method preference, though overall rates vary by demographic factors like age and education.[55] Key challenges include forgetting to replace the ring promptly after the 7-day break, which disrupts continuous protection, and occasional expulsion or migration requiring manual checks.[59]The ring's discreet design—small, flexible, and positioned high in the vagina—typically avoids detection by partners during intercourse, supporting uninterrupted sexual activity without mandatory disclosure and thereby enhancing user confidence and adherence.[60] Studies indicate that dissatisfaction with sensation or minor discomfort contributes to non-adherence in a subset of users, but the method's simplicity fosters superior compliance over alternatives requiring daily recall.[61] Tracking apps or reminders can mitigate forgetfulness, particularly for the replacement step.[62]
Effectiveness
Failure rates and influencing factors
The contraceptive vaginal ring exhibits a low failure rate under perfect use, defined as consistent and correct insertion, retention for three weeks, removal for one week, and timely reinsertion without extensions beyond three hours for activities like intercourse. Phase III clinical trials for etonogestrel/ethinyl estradiol rings (e.g., NuvaRing) reported Pearl Indices of 0.65 to 1.3 pregnancies per 100 woman-years in intent-to-treat analyses approximating perfect compliance.[63][64] This translates to an annual failure rate of approximately 0.3% to 1%.[2]In typical use, incorporating real-world inconsistencies such as prolonged ring removal (>3 hours), incorrect timing of cycles, or accidental expulsion, the annual failure rate increases to 7-9%.[65][2]User error accounts for the majority of these failures, with studies indicating that rings left out beyond recommended limits elevate ovulation risk due to hormone level fluctuations.[1]Body mass index (BMI) exceeding 30 kg/m² does not substantially diminish efficacy, as pharmacokinetic data show sustained therapeutic serum concentrations of etonogestrel and ethinyl estradiol in obese users comparable to those with normal BMI.[66] Gastrointestinal disturbances like vomiting or diarrhea minimally affect absorption, given the ring's intravaginal delivery bypassing first-pass metabolism.[67] Most antibiotics lack interaction with ring-released hormones, though rifampin induces metabolism and requires alternative contraception.[68][69]Adolescents experience higher typical-use failure rates, up to 12% annually, largely from adherence challenges including inconsistent insertion/removal and lower method familiarity compared to adults.[70][71]
Empirical data from studies
In phase III clinical trials for the NuvaRing, which involved over 2,000 women across North American and European sites, the method failure rate under perfect use conditions ranged from 0.4 to 1.6 pregnancies per 100 woman-years, with a pooled Pearl Index of 0.77 (95% CI: 0.37–1.40) in integrated analyses of compliant users.[3][72] Comparative trials against combined oral contraceptives reported intent-to-treat Pearl Indices of 0.25 for NuvaRing versus 0.99 for pills per 100 woman-years, indicating similar overall efficacy when accounting for adherence differences.[73]Meta-analyses and pooled data from multiple studies confirm that combined hormonal vaginal rings achieve effectiveness comparable to oral contraceptives, with perfect-use pregnancy rates typically under 1 per 100 woman-years, though real-world typical-use rates vary by population.[74] North American trials consistently show higher failure rates than European counterparts—e.g., up to 1.6 versus below 0.65 per 100 woman-years—attributed to differences in user demographics, education levels, and compliance rather than inherent method flaws.[3]For the Annovera ring, phase III open-label trials encompassing 2,308 women aged 18–40 demonstrated sustained efficacy over 13 cycles, with a cumulative one-year pregnancy rate of 2.9% under typical use and no evident decline in protection across cycles when used as directed (21 days in, 7 days out).[75][76] Prolonged ring removals exceeding 2 hours correlated with elevated risks, yielding adjusted rates of 2.11 pregnancies per 100 woman-years in compliant subgroups.[77]
Study/Product
Design
Population/ Duration
Perfect-Use Pearl Index (pregnancies/100 woman-years)
The combined hormonal vaginal ring inhibits ovulation through steady release of etonogestrel and ethinylestradiol, thereby reducing the risk of functional ovarian cysts relative to non-users, as ovulation suppression prevents follicular development into cysts.[78] Cohort studies of hormonal contraceptive users, including those with combined methods akin to the vaginal ring, confirm lower incidence of benign ovarian cysts with prolonged use.[79]Use of hormonal contraceptives like the vaginal ring markedly lowers the overall risk of ectopic pregnancy by preventing conception, with current users exhibiting reduced rates compared to non-users in population-based analyses.[80] If failure occurs, the adjusted risk among pregnancies remains low due to endometrial thinning and cervical mucus changes that impede implantation.[81]The device enhances menstrual regulation by stabilizing the endometrial lining, resulting in lighter and shorter withdrawal bleeding during the ring-free week. Non-comparative studies report that after three cycles, 42% of users experience decreased blood loss and 39% note shorter bleeding duration.[73]Dysmenorrhea prevalence declines significantly, from 42% pretreatment to 26% after three months in observational data.[73]In women with heavy menstrual bleeding, randomized controlled trials demonstrate substantial reductions in blood loss, with Pictorial Blood Loss Assessment Chart (PBAC) scores falling by 59-69% over three cycles versus baseline, comparable to oral alternatives.[82][83] Cycle control improves, yielding higher rates of predictable withdrawal-only bleeding (up to 83% by cycle three) and fewer breakthrough episodes than combined oral contraceptives.[82][73]
Other physiological advantages
The etonogestrel component in common combined vaginal rings, derived from desogestrel, exhibits anti-androgenic properties that suppress sebaceous gland activity and reduce sebum production, leading to decreased acne severity in users compared to baseline or certain progestin-based oral contraceptives.[84] Observational data indicate vaginal ring users report lower odds of acne (OR 0.23 versus levonorgestrel/ethinylestradiol users; OR 0.18 versus drospirenone/ethinylestradiol) attributable to stable hormone delivery minimizing androgen fluctuations.[84]Hormonal stabilization from continuous progestin and estrogen release may alleviate premenstrual syndrome symptoms such as mood disturbances and irritability by suppressing cyclic hormone variations, though direct randomized trials on vaginal rings are lacking and benefits are inferred from broader combined hormonal contraceptive effects.[85]In young women, vaginal rings promote positive bone turnover, with prospective studies showing preserved or increased bone mineral density at lumbar spine and hip sites after 24 months of use, contrasting transient losses seen with some progestin-only methods due to the estrogen component counteracting resorption.[86] This effect stems from estrogen's role in osteoblast stimulation and reduced osteoclast activity, yielding similar outcomes to transdermal patches without oral first-pass metabolism impacts.[86]Long-term use of combined hormonal contraceptives, including vaginal rings, correlates with reduced ovarian cancer incidence in observational cohorts, with a 30% risk reduction after 5 years of exposure persisting up to 30 years post-discontinuation; relative risk approximates 0.70 per 5 years of use, driven by ovulation suppression limiting epithelial inclusions and inflammation.[87] Absolute risk reductions remain modest given ovarian cancer's low baseline incidence (about 12 per 100,000 women annually), and causality is supported by dose-response patterns across delivery modes.[87][88]
Risks and side effects
Common adverse reactions
The most frequently reported local adverse reactions associated with the combined hormonal vaginal ring, such as NuvaRing, involve vaginal irritation, discharge, and vaginitis, occurring in 1-14% of users across clinical trials.[89][73] Vaginal discomfort and leucorrhea are also common, with incidences typically ranging from 5-10% in comparative studies against oral contraceptives.[90] Ring expulsion, often linked to improper placement or defecation, affects 2-6% of users, though rates up to 20% have been noted in acceptability surveys.[91][92]Mild systemic effects mirror those of combined oral contraceptives, including headache (up to 26% in some cohorts), nausea (5-10%), and breast tenderness (4-10%).[93][94] These symptoms are generally transient and resolve within the first few cycles, with hormonal side effects reported in under 10% of subjects in phase III trials.[95]Overall, adverse reactions prompt discontinuation in 13-15% of users within the first year, primarily due to vaginal symptoms or device-related issues rather than systemic effects.[89][96] Continuation rates remain comparable to oral methods when local tolerability improves with user experience.[73]
Serious health risks including VTE
The vaginal ring, delivering ethinyl estradiol and a progestin such as etonogestrel, carries an elevated risk of venous thromboembolism (VTE), encompassing deep vein thrombosis and pulmonary embolism, attributable to estrogen-mediated procoagulant effects on factors like fibrinogen and resistance to activated protein C. Large-scale observational data indicate an incidence of approximately 9 per 10,000 woman-years among users, versus 2-3 per 10,000 in non-users of hormonal contraception.[97][1] This rate aligns with or exceeds that of low-dose combined oral contraceptives (COCs), particularly levonorgestrel-containing formulations, with relative risks for non-oral combined methods like the ring estimated at 6.5-7.9 times the baseline.[98][99]Arterial thrombotic events, including ischemic stroke and myocardial infarction, also show increased incidence with vaginal ring use, driven by estrogen's promotion of endothelial dysfunction and platelet aggregation. A 2025 Danish nationwide cohort analysis reported adjusted incidence rate ratios of 2.4 (95% CI 1.5-3.7) for stroke and 3.8 for myocardial infarction relative to non-use, surpassing risks with second-generation COCs and underscoring higher hazards for non-oral delivery systems.[100][101] Absolute event rates remain low—typically under 5 per 10,000 woman-years—yet the causal link persists across registries, with first-pass hepatic metabolism bypassed in vaginal administration potentially amplifying systemic estrogen exposure.[102]Estrogen in the ring formulation causally contributes to gallbladder disease via heightened hepatic cholesterol synthesis and biliary stasis, yielding relative risks of 1.5-2 for cholecystitis or cholelithiasis compared to non-users.[103][104]Hypertension risk elevates modestly, with estrogen stimulating angiotensinogen production; cohort evidence links combined hormonal methods to new-onset or exacerbated blood pressure rises, particularly exceeding 140/90 mmHg thresholds in susceptible individuals.[105]These risks intensify with modifiable and demographic factors: smoking synergistically doubles VTE odds via endothelial damage; age over 35 years correlates with 2-3 fold higher arterial event rates; and obesity (BMI ≥30 kg/m²) amplifies VTE incidence by impairing fibrinolysis, as quantified in Danish registry cohorts tracking over 1 million women.[98][106] Contraindications thus emphasize avoidance in those with these amplifiers to mitigate absolute event probabilities.
Comparisons with other contraceptives
Versus oral hormonal methods
The vaginal ring and combined oral contraceptives (COCs) exhibit comparable contraceptive efficacy, with typical-use failure rates of approximately 7% for both methods and perfect-use failure rates below 1%.[65] Head-to-head trials have demonstrated equivalent ovulation suppression between the two, supporting their parity in preventing follicular development.[22] The ring's monthly insertion schedule enhances compliance compared to daily pill ingestion, particularly among users prone to forgetfulness; in a study of college women, perfect compliance at three months was higher with the ring (though both methods yielded high satisfaction).[107]Vaginal administration of hormones via the ring bypasses gastrointestinal absorption and hepatic first-pass metabolism, resulting in lower systemic exposure to ethinylestradiol (EE) and more consistent serum levels relative to COCs, which undergo daily hepatic processing.[20] This pharmacokinetic profile may reduce gastrointestinal side effects associated with oral dosing, as hormones are absorbed directly into the systemic circulation without liver metabolism altering their bioavailability.[73]Regarding health outcomes, the ring often provides superior cycle control, with fewer instances of breakthrough bleeding and spotting than COCs in comparative studies.[108] Venous thromboembolism (VTE) risk with the ring is similar to that of COCs, neither substantially increased nor decreased, based on observational data and guidelines from reproductive medicine societies.[109]
Versus long-acting reversible contraceptives
The vaginal ring, typically requiring self-insertion and monthly replacement or removal, exhibits a typical-use failure rate of 7-9% in the first year, substantially higher than the less than 1% typical-use failure rate observed for long-acting reversible contraceptives (LARCs) such as intrauterine devices (IUDs) and subdermal implants.[110][111] This disparity arises from the user-dependent nature of ring placement and adherence, contrasted with the provider-inserted, "set-and-forget" mechanism of LARCs, which minimizes discontinuation due to non-compliance.[112] Empirical data from cohort studies confirm LARC superiority in effectiveness, with failure rates remaining below 1% even among adolescents and young adults, populations prone to inconsistent use of shorter-acting methods like the ring.[71]Duration of action further differentiates the methods: standard etonogestrel/ethinylestradiol rings like NuvaRing provide protection for 21 days followed by a 7-day removal interval, necessitating repeated user intervention, whereas levonorgestrel IUDs (e.g., Mirena) and etonogestrel implants (e.g., Nexplanon) offer 3-8 years and 3-5 years of continuous efficacy, respectively, promoting higher long-term adherence without frequent healthcare visits.[113][112] Both categories achieve rapid reversibility upon discontinuation, with fertility return typically within days to weeks, though LARCs may involve a brief post-removal adjustment period comparable to rings.[114]Health profiles vary notably: estrogen-progestin rings confer venous thromboembolism (VTE) risks akin to combined oral contraceptives (3-9 per 10,000 woman-years), exceeding those of progestin-only implants or levonorgestrel IUDs (lower systemic exposure) and absent in copper IUDs.[114] Rings obviate the insertion pain, cramping, or vasovagal episodes reported in 10-20% of IUD placements, alongside rare perforation (1-2 per 1,000 insertions), but introduce localized vaginal adverse effects like discharge or irritation in up to 10% of users, versus IUD expulsion risks of 2-10% in the first year.[2][112] Thus, rings may suit individuals preferring non-procedural options despite elevated hormonal risks, while LARCs excel for those prioritizing minimal maintenance and sustained efficacy.[114]
Controversies and criticisms
Safety concerns and regulatory scrutiny
In 2014, Merck, the manufacturer of NuvaRing (a vaginal ring containing etonogestrel and ethinyl estradiol), agreed to a $100 million settlement resolving over 2,000 lawsuits alleging that the device increased the risk of venous thromboembolism (VTE) events such as deep vein thrombosis and pulmonary embolism, with plaintiffs claiming inadequate warnings about these risks compared to other combined hormonal contraceptives.[14][13] Observational data from cohort studies have indicated that users of vaginal rings experience a VTE incidence rate approximately 6.5 times higher than non-users of hormonal contraception, though absolute risks remain low at around 9-12 events per 10,000 woman-years among young, otherwise healthy users, prompting debates over whether relative risks were sufficiently communicated relative to baseline population rates of 1-5 per 10,000.[98]Critics, including patient advocacy groups and litigators, have argued that promotional materials for vaginal rings like NuvaRing underemphasized absolute VTE risks—potentially 1 in 1,000 for younger users annually—while highlighting convenience over causal links to higher estrogen exposure via first-pass avoidance in the liver, which may elevate clotting factors more than oral equivalents.[115] Pro-life organizations have raised ethical concerns about the hormonal mechanisms of such devices, contending that progestin components can alter endometrial lining and potentially disrupt implantation of fertilized embryos, framing dependency on synthetic hormones as promoting a disconnect from natural fertility cycles without full disclosure of these post-fertilization effects.[116][117]Regulatory bodies have responded with enhanced scrutiny; the U.S. Food and Drug Administration (FDA) mandates a boxed warning on all combined hormonal contraceptives, including vaginal rings, for increased cardiovascular risks like VTE, particularly in smokers over 35 or those with predisposing factors, with label updates emphasizing discontinuation four weeks pre-surgery to mitigate perioperative clot risks.[118][119] Defenders, including manufacturers and some clinical guidelines, counter that absolute VTE incidences are comparable to or lower than those during pregnancy (up to 20-fold higher relative risk), with overall benefits in preventing unintended pregnancies—estimated at 0.65 per 100 woman-years failure rate—outweighing harms for low-risk populations when individual factors are assessed.[120][2] These positions underscore ongoing tensions between empirical risk data and interpretive frameworks, with peer-reviewed analyses affirming no definitive superiority in VTE hazard over second-generation oral contraceptives but calling for personalized risk-benefit evaluations.[121]
Debates on risk communication and promotion
Critics of vaginal ring promotion argue that marketing materials, often produced by pharmaceutical companies like Merck for NuvaRing, prioritize convenience and user-independent dosing over comprehensive disclosure of potential hormonal effects, such as transient suppression of ovarian reserve markers that may mimic reduced fertility during use.[122] Empirical data from cohort studies indicate no permanent impairment to long-term fertility post-discontinuation, with conception rates returning to baseline within months akin to other hormonal methods, yet some patient reports and qualitative reviews highlight unresolved concerns about hormone accumulation from repeated cycles, prompting calls for longitudinal studies to quantify any subtle cumulative impacts beyond short-term trials.[123][124][1]In clinical settings, inadequate counseling on non-adherence risks—such as ring removal for hygiene or intercourse—correlates with higher discontinuation rates, with one study of 803 users reporting 16% early termination due to ring-related issues including expulsion and tolerability problems.[125] Peer-reviewed analyses emphasize that thorough pre-insertion education reduces such events, as users unprepared for side effects like mood alterations or perceived weight gain (reported in up to 5-10% of cases leading to cessation) exhibit 20-30% lower continuation at one year compared to informed cohorts.[126][127] Despite manufacturer labels acknowledging these effects, discontinuation data from 2023-2025 post-marketing surveillance underscore verifiable user exits for these reasons, challenging claims of negligible impact in promotional narratives.[128]Diverse viewpoints intensify the debate: conservative commentators, including figures like those cited in analyses of social media trends, critique the normalization of hormonal methods as eroding natural fertility cycles and amplifying mental health risks through estrogen-progestin interference, attributing under-discussed discontinuations to causal mood disruptions overlooked in autonomy-focused public health campaigns.[129] In contrast, reproductive health advocates stress evidence-based promotion of access, arguing that overemphasis on rare long-term unknowns deters uptake among women seeking reliable contraception, though both sides cite the need for balanced informed consent protocols to mitigate biases in source selection—such as academia's tendency to favor efficacy data from industry-funded trials.[130] Recent empirical reviews post-2023 recommend enhanced labeling for vascular risks, informed by updated VTE incidence data showing 1.5-2 times higher odds versus low-dose pills, to align communication with causal risk profiles rather than convenience alone.[13][55]
Recent developments
Innovations in formulations and delivery
The segesterone acetate (SA) and ethinyl estradiol (EE) vaginal ring, known as Annovera, incorporates a reusable siliconeelastomer formulation designed for 13 cycles of use, releasing 150 mcg SA and 13 mcg EE daily to achieve sustained contraception over one year. This lower EE dose (13 mcg/day versus 15 mcg/day in etonogestrel/EE rings) reduces systemic estrogen exposure while maintaining efficacy, with pharmacokinetic studies confirming progestin serum levels exceeding 100 pmol/L across 364 days and minimal degradation in hormone release rates due to the matrix's thermal stability, eliminating refrigeration needs.[1][131]Longer-duration delivery systems have advanced with a 90-day ring formulation combining SA (200 mcg/day) and natural estradiol (E2, 200 mcg/day), avoiding synthetic EE to potentially lower venous thromboembolism risks; in vivo data show stable E2 levels above 40 pg/mL for ovulation suppression without hypoestrogenism, demonstrating improved pharmacokinetic consistency over extended wear.[132]Material innovations include silicone-urethane copolymers for 3D-printed rings, enabling precise hormone loading (e.g., 14-40 mg etonogestrel and 3.5-10 mg EE) and controlled release over 90 days as an alternative to ethylene-vinyl acetate, with enhanced mechanical stability under accelerated conditions (40°C/75% RH) to reduce degradation and support personalized sizing for comfort.[133] FDA guidance in 2023 for generic SA/EE rings further facilitates refinements in low-estrogen delivery.[134]
Ongoing research and 2023-2025 updates
A 2023 analysis of the multipurpose prevention technologies (MPTs) pipeline emphasized progress in vaginal rings that integrate contraception with HIV and STI prevention, including formulations combining tenofovir for antiviral activity and levonorgestrel for ovulation suppression, with ongoing preclinical and early clinical evaluations demonstrating sustained release over 90 days.[135] Clinical trials reported in the same year tested dual-purpose rings delivering tenofovir and levonorgestrel, showing protective concentrations against HIV and herpes simplex virus while providing contraceptive efficacy, though challenges with adherence and side effects persisted among participants.[136]In 2024, development of next-generation intravaginal rings advanced with innovations like clip-on polymer systems enabling lower hormone doses; for instance, CLIPLOW rings achieved etonogestrel and ethinylestradiol release at reduced levels compared to standard products like NuvaRing, aiming to minimize systemic exposure while sustaining local effects for 90 days, as validated in pharmacokinetic models.[133] These efforts target improved tolerability and reduced adverse events through precise dosing control, with high-dose variants (CLIPHIGH) outperforming benchmarks in hormone delivery duration.[137]A December 2024 Danish registry study quantified ischemic stroke risks with combined hormonal contraceptives, finding vaginal rings associated with a 1.79-fold increased incidence rateratio (95% CI, 1.11–2.89) versus non-use, comparable to the 1.77-fold risk (95% CI, 1.62–1.93) for oral combined methods, though limited data on patches highlighted needs for further non-oral comparisons.[138] This has spurred reevaluations of riskstratification, particularly for women with comorbidities, as contemporary formulations maintain elevated absolute risks despite lower estrogen doses.[138] A February 2025 analysis extended these findings to myocardial infarction, confirming persistent cardiovascular signals with ring use and advocating enhanced patient-specific counseling on delivery method differences.[139]