Fact-checked by Grok 2 weeks ago

Poikiloderma

Poikiloderma is a descriptive term in referring to a characteristic characterized by the triad of cutaneous (thinning of the skin), telangiectasias (dilated small blood vessels), and reticulated pigmentation changes, including both and , often presenting in a mottled or net-like pattern. This skin manifestation can arise from diverse etiologies and is classified into acquired and congenital forms, with the former often linked to environmental factors such as chronic (UV) radiation exposure from , which damages dermal structures and fibers, leading to the classic appearance. Acquired poikiloderma may also result from therapy, chemical photosensitizers (e.g., certain fragrances in perfumes), or iatrogenic causes like following transplantation. In contrast, congenital or inherited poikiloderma typically stems from genetic mutations affecting , telomere maintenance, or integrity, often presenting in infancy or early childhood with as an early feature. Among the most common acquired variants is poikiloderma of Civatte, a benign, predominantly affecting fair-skinned individuals, particularly postmenopausal women, and manifesting as reddish-brown, reticulated patches on the sides of the neck, upper chest, and sometimes cheeks, sparing the submental area due to natural shading. It is primarily caused by cumulative sun exposure combined with hormonal influences, and while usually asymptomatic, it can cause cosmetic distress with rare sensations of burning or pruritus. Inherited forms include Rothmund-Thomson syndrome (RTS), an autosomal recessive disorder due to mutations in the RECQL4 gene, featuring early-onset poikiloderma alongside , skeletal abnormalities, and increased risk of ; dyskeratosis congenita (DC), linked to biology defects, which adds nail dystrophy, oral leukoplakia, and bone marrow failure; and poikiloderma with (PN), caused by USB1 gene mutations, involving recurrent infections from low neutrophil counts. Other notable genetic syndromes encompass (XP), (BS), Kindler syndrome (KS), and hereditary fibrosing poikiloderma with tendon contractures, myopathy, and pulmonary fibrosis (POIKTMP). Poikiloderma can also appear in systemic conditions like or (poikilodermatous ), where it signals underlying pathology. Diagnosis generally relies on clinical examination, with histopathological confirmation via skin biopsy showing epidermal atrophy, dilated vessels, and pigment incontinence if needed to differentiate from mimics such as actinic damage, lupus erythematosus, or parapsoriasis. Management focuses on addressing the underlying cause: strict sun protection with broad-spectrum SPF 30+ sunscreen and protective clothing is essential for all types to prevent progression, while cosmetic improvement in acquired cases like poikiloderma of Civatte may involve topical retinoids, hydroquinone for pigmentation, or vascular lasers such as pulsed dye laser or intense pulsed light (IPL) therapy. In inherited syndromes, multidisciplinary care is critical, including genetic counseling, monitoring for malignancies (e.g., skin cancers in XP or RTS), and supportive treatments like growth factors for neutropenia in PN. Overall, while poikiloderma itself is not life-threatening, its presence warrants evaluation for associated systemic involvement to guide appropriate intervention.

Introduction

Definition

Poikiloderma is a descriptive term in referring to a distinctive characterized by the triad of cutaneous (thinning of the skin), telangiectasias (dilated small blood vessels), and reticulated pigmentation changes, including both (lightened areas) and (darkened areas), which together produce a mottled or variegated appearance. This clinical pattern reflects chronic alterations in the skin's structure and color, often resulting in a reticular network of affected areas. The term "poikiloderma" originates from words "poikilos," meaning spotted, mottled, or varied, and "derma," meaning , aptly capturing the heterogeneous, patchwork-like quality of the lesions. The specific acquired form known as poikiloderma of Civatte was first described in by dermatologist Achille Civatte, who identified the pattern in sun-exposed areas of the neck and upper chest. Importantly, poikiloderma does not represent a single entity but serves as a morphological descriptor for a reaction pattern that can arise in diverse etiologies, including genetic, inflammatory, and environmental factors. This distinction underscores its role as a sign rather than a , commonly observed on sun-exposed surfaces.

Clinical Features

Poikiloderma manifests as a of cutaneous , telangiectasias, and reticulated pigmentation changes, resulting in a mottled appearance of . leads to thinning and increased fragility, making prone to easy bruising or tearing, while telangiectasias present as prominent, dilated superficial blood vessels resembling fine red threads. Pigmentation alterations include irregular brownish hyperpigmented patches interspersed with pale hypopigmented areas, forming a net-like or reticulate pattern. These features predominantly affect sun-exposed regions, such as the face, neck, and V-shaped area of the upper chest, often in a symmetrical distribution that spares shaded areas like the submental region. The condition may initially appear as confluent reddish-brown patches with subtle , progressing to more pronounced vascular and pigmentary abnormalities over time. Secondary symptoms are variable; approximately half of affected individuals report mild itching, burning, or flushing sensations, though many remain beyond cosmetic dissatisfaction from the visible discoloration and texture changes. Progression typically evolves from initial and fine scaling in early stages to established poikilodermatous features over months to years, with a mean diagnostic delay of about 6 years in common acquired forms. In advanced or severe presentations, xerosis (dry, rough skin) may develop, and non-healing ulcers can occur, particularly in syndromic associations like Rothmund-Thomson syndrome.

Classification

Congenital Poikiloderma

Congenital poikiloderma refers to inherited forms of the , primarily manifesting as part of multisystem genetic syndromes with early-onset skin changes and associated extracutaneous features. These syndromes exhibit various inheritance patterns, including autosomal recessive, X-linked recessive, and autosomal dominant, and arise from mutations disrupting , telomere maintenance, or immune function, leading to poikilodermatous lesions that typically emerge in infancy or . Unlike acquired poikiloderma, which develops later in life due to external factors, congenital variants present within the first few years and often involve systemic complications. Rothmund-Thomson syndrome (RTS) is a classic example, caused by biallelic mutations in the RECQL4 gene, which encodes a DNA helicase involved in replication and repair. Affected individuals typically develop and erythematous patches on the cheeks and in infancy (around 3-6 months), progressing to characteristic poikiloderma on the face, , and limbs by . The poikiloderma spreads centrifugally, with telangiectasias, , and pigmentation changes becoming prominent. RTS carries an elevated risk of skin cancers, such as , and , underscoring the need for vigilant monitoring. The estimated incidence is less than 1 in 1,000,000 births, with fewer than 500 cases reported worldwide. Dyskeratosis congenita (), encompassing a spectrum of telomere biology disorders, results from mutations in genes such as DKC1, TERT, or TERC that impair elongation and maintenance. Poikiloderma in often begins in early childhood on the neck, upper trunk, and extremities, accompanied by nail dystrophy (e.g., ridging and splitting) and oral . Progression involves reticulated hyper- and with , and affected patients face significant risks of failure (in up to 80% of cases) and skin malignancies. prevalence is estimated at 1 in 1,000,000, with diverse ethnic representation due to multiple causative genes. Poikiloderma with neutropenia (PN), also known as Clericuzio-type PN, stems from biallelic mutations in the USB1 gene (formerly C16orf57), which encodes an affecting U6 snRNA processing and immune function. The condition presents with poikiloderma starting at 6-12 months, initially on the face and before extending to the limbs and , alongside chronic leading to recurrent bacterial infections. Nail hyperkeratosis and are common, with progression marked by inflammatory flares and increased susceptibility to skin infections. Fewer than 100 cases have been documented globally. Other congenital forms of poikiloderma include (XP), an autosomal recessive disorder caused by mutations in genes (e.g., XPA-XPG), leading to extreme and poikiloderma on sun-exposed areas alongside high risk; (BS), autosomal recessive due to BLM helicase mutations, featuring , facial poikiloderma, growth retardation, and cancer predisposition; Kindler syndrome (KS), autosomal recessive from FERMT1 mutations affecting kindlin-1, with early blistering, , and progressive poikiloderma with mucosal involvement; and hereditary fibrosing poikiloderma with tendon contractures, , and (POIKTMP), autosomal dominant caused by FAM111B mutations, presenting with early poikiloderma, joint contractures, muscle weakness, and potential lung .

Acquired Poikiloderma

Acquired poikiloderma refers to non-inherited forms of the condition arising from external triggers or secondary to underlying diseases, typically manifesting in adulthood. Unlike congenital variants, these cases often present with later onset and may be reversible upon removal of the inciting factor or management of the associated disease. A common subtype is poikiloderma of Civatte, a benign, form induced by prolonged sun exposure, primarily affecting the sides of the and cheeks in middle-aged or menopausal individuals. It features reticulated erythematous-brown patches with telangiectasias and pigmentary changes, characteristically sparing the submental area due to reduced exposure there. Another notable subtype is poikilodermatous , a variant of characterized by poikilodermatous patches involving more than 50% of the body surface, often in a "bathing suit" distribution on the trunk and extremities. Histologically, it shows atypical CD4+ or CD8+ T-lymphocytes with epidermotropism, epidermal , and dilated dermal vessels. Other associations include drug-induced poikiloderma, such as from agents like hydroxyurea used in myeloproliferative disorders, which can cause poikilodermatous changes through mechanisms involving atrophy and dyspigmentation. Post-radiation poikiloderma occurs as a late complication of radiotherapy, presenting with , telangiectasias, and mottled pigmentation confined to the irradiated field, typically emerging months to years after exposure due to microvascular damage. Iatrogenic poikiloderma can also occur in chronic following transplantation. Additionally, it can develop secondary to diseases, including and systemic sclerosis (), where poikilodermatous lesions often appear on sun-exposed areas as part of the inflammatory process. These acquired forms generally exhibit adult onset, with lesions that are often asymmetric or localized to sites of exposure or injury, distinguishing them from the more diffuse, early-life presentations in congenital poikiloderma. In poikilodermatous , epidermotropism by atypical lymphocytes is a key feature, and the condition may progress to erythroderma in some cases, though it carries a relatively favorable compared to classic .

Epidemiology

Prevalence and Demographics

Poikiloderma is a rare dermatological condition, with congenital forms being exceptionally uncommon. Rothmund-Thomson syndrome, a prototypical congenital poikiloderma, has an unknown exact prevalence but is estimated at less than 1 in 1,000,000 individuals, based on approximately 300 to 500 cases reported globally in the medical literature. Other congenital forms, such as dyskeratosis congenita and poikiloderma with neutropenia, are similarly rare, with estimated prevalences of approximately 1 in 1,000,000 and less than 1 in 1,000,000, respectively, and fewer than 500 and 100 cases reported worldwide. Acquired forms of poikiloderma are more frequently encountered in clinical settings. Poikiloderma of Civatte, the most common acquired variant, has been estimated to affect about 1.4% of patients attending clinics. Poikiloderma vasculare atrophicans, often linked to early-stage , represents a rarer subtype, comprising roughly 1-2% of all cases. Demographically, acquired poikiloderma predominantly impacts fair-skinned individuals, with females comprising 68% of reported cases of poikiloderma of Civatte. The condition typically manifests in middle-aged to elderly adults, with a mean diagnostic age of 47.8 years for women and 61.7 years for men, particularly among those with chronic outdoor sun exposure. Geographically, poikiloderma of Civatte shows higher prevalence in regions with abundant , such as sunny climates or areas at higher altitudes, where levels contribute to increased occurrence among susceptible populations.

Risk Factors

Poikiloderma, particularly its acquired forms, is influenced by a range of modifiable and non-modifiable risk factors that predispose individuals to its development. to (UV) from represents the primary environmental risk factor, especially for Poikiloderma of Civatte, where cumulative sun damage leads to dermal , , and pigmentation changes over time. from therapeutic sources, such as for malignancies, can also induce poikiloderma as a late through microvascular injury and in treated areas. Additionally, extreme or injuries may contribute to localized poikilodermatous changes by damaging skin vasculature and . Photosensitizing agents, including certain drugs like thiazide diuretics and topical irritants in or perfumes, exacerbate UV-induced damage, heightening susceptibility in exposed individuals. Demographic factors play a significant role, with fair types classified as Fitzpatrick I-II conferring greater vulnerability due to reduced protection against UV radiation. In Poikiloderma of Civatte, female gender increases risk, attributed to hormonal influences such as decline during , which may alter cutaneous vasculature and responsiveness to environmental stressors. Age is another key non-modifiable factor, as the condition typically emerges in the fourth to fifth decades following prolonged cumulative exposures. Disease-related risk factors include underlying autoimmune conditions, where poikiloderma manifests as a cutaneous feature; for instance, , , and predispose affected individuals through chronic inflammation and photosensitivity. Malignancies, particularly cutaneous lymphomas such as , are associated with poikilodermatous presentations due to lymphoproliferative involvement of the skin. Prior cancer therapies, including , further elevate risk by directly impairing skin integrity in irradiated fields.

Etiology and Pathogenesis

Causes

Poikiloderma arises from a variety of congenital and acquired etiologies, with genetic mutations predominantly underlying the congenital forms and external or inflammatory triggers responsible for most acquired cases. Congenital poikiloderma is caused by germline mutations in genes critical for , telomere maintenance, and cellular integrity. In Rothmund-Thomson syndrome, biallelic mutations in the RECQL4 gene, which encodes a involved in replication and repair, disrupt genomic stability and lead to early-onset poikiloderma. Dyskeratosis congenita results from mutations in multiple genes, including DKC1 on the that encodes dyskerin, a protein essential for function and telomere elongation, causing progressive poikilodermatous skin changes. Other specific genetic causes include poikiloderma with neutropenia, linked to biallelic mutations in USB1 (also known as C16orf57), which encodes a 3' to 5' exoribonuclease involved in processing. Hereditary fibrosing poikiloderma with tendon contractures, myopathy, and stems from heterozygous mutations in FAM111B, encoding a that regulates protein degradation. Kindler syndrome, another congenital form, is due to mutations in FERMT1, which codes for kindlin-1, a protein necessary for adhesion and integrity. Acquired poikiloderma typically develops secondary to environmental exposures, iatrogenic interventions, inflammatory processes, or rarely neoplastic infiltration. Chronic (UV) and visible light exposure induces , manifesting as poikiloderma of Civatte through cumulative damage to dermal , , and vasculature in sun-exposed areas like the and chest. In , an autoimmune , poikiloderma emerges from immune-mediated vascular injury and inflammation, often worsened by UV light on photoexposed sites such as the upper back and shoulders. Iatrogenic causes include chronic radiation dermatitis following therapy for malignancies, where high-dose exposure leads to persistent , , and pigmentary mottling in treated fields. Certain medications, such as hydroxyurea used in myeloproliferative disorders and topical or systemic corticosteroids, can also trigger poikilodermatous changes via direct toxicity to and fibroblasts. Neoplastic etiologies are uncommon but include poikilodermatous , a variant characterized by atypical lymphocytic infiltration of the , resulting in the triad of , pigmentation alterations, and . Infectious triggers are rare, though acrodermatitis chronica atrophicans from infection can present with poikiloderma-like features due to spirochetal invasion of dermal structures. These etiologic factors initiate poikiloderma by promoting vascular dilation, degradation, and dysregulation in the .

Pathophysiological Mechanisms

Poikiloderma arises from a complex interplay of cellular and molecular processes that disrupt , often triggered by environmental exposures such as (UV) radiation. These mechanisms converge to produce the characteristic triad of , , and pigmentary changes through damage to the , , and vascular structures. Vascular changes in poikiloderma primarily stem from endothelial damage in the superficial dermal vessels, leading to the formation of telangiectasias. Chronic insults, including UV exposure, induce the expression of matrix metalloproteinases (MMPs), particularly MMP-1 and MMP-3, which degrade type I and III in the surrounding capillaries. This degradation weakens vascular support, resulting in persistent dilation and visible telangiectatic networks. Endothelial cells also exhibit hydropic degeneration and increased permeability, further contributing to the reticular pattern of vascular observed in affected skin. Pigmentary alterations result from injury to the basal layer of the , causing melanin incontinence and subsequent hyper- and . Damage to basal leads to vacuolar degeneration and release of granules into the , where they are phagocytosed by melanophages, producing mottled pigmentation. In photo-induced cases, (ROS) generated by UV radiation exacerbate this process by oxidizing melanocytes and promoting uneven synthesis and distribution, amplifying the reticulate dyschromia. Atrophic features involve progressive epidermal thinning and dermal remodeling driven by chronic inflammation. Persistent lymphocytic infiltration in the upper triggers release, promoting through excessive deposition and fragmentation, while simultaneously inhibiting epidermal to cause . In genetic forms of poikiloderma, defective mechanisms, such as dysfunction, impair the resolution of UV-induced DNA lesions, amplifying cumulative damage and accelerating these inflammatory and fibrotic processes.

Diagnosis

Clinical Evaluation

Clinical evaluation of poikiloderma begins with a detailed history to distinguish congenital from acquired forms and identify potential underlying causes. In congenital cases, such as Rothmund-Thomson syndrome, onset typically occurs in early infancy, often with initial on the cheeks between the 3rd and 6th months of life, accompanied by a family history suggestive of autosomal recessive inheritance and heightened leading to exacerbated skin changes with sun exposure. Associated symptoms may include , sparse hair, juvenile cataracts, skeletal abnormalities, and fatigue related to systemic involvement. For acquired poikiloderma, such as poikiloderma of Civatte, history reveals later onset in adulthood, often in peri-menopausal women, with significant chronic sun exposure on the neck and upper chest, typically without a family history suggestive of genetic inheritance, and potential links to topical irritants like perfumes or systemic conditions such as , where fatigue and muscle weakness may be prominent. Physical examination focuses on inspecting sun-exposed areas for the classic triad of telangiectasias, mottled hypo- and , and cutaneous , which may present in a reticular pattern sparing the submental area in acquired forms. In congenital variants, poikiloderma often affects the face, extremities, and buttocks while sparing the trunk, with additional findings like sparse hair or skeletal deformities. Wood's lamp examination can enhance visualization of subtle pigmentation patterns, aiding in delineating hypo- and hyperpigmented areas under ultraviolet light. Severity assessment may employ tools like the Cutaneous Disease Area and Severity Index (CDASI) when poikiloderma accompanies dermatomyositis, with the damage score (0-32 total) assessing poikiloderma across 15 body areas. Differential diagnosis requires distinguishing poikiloderma from conditions with overlapping features, such as chronic actinic damage (which lacks early onset and systemic associations), (typically facial, hormonally influenced, and without atrophy or telangiectasias), and (characterized by pruritic, violaceous papules rather than reticulate pigmentation). Other considerations include dermatomyositis-specific poikiloderma (with heliotrope rash) or (with pruritus and progression to plaques). Confirmation may involve if clinical findings are equivocal.

Histopathological Findings

Histopathological examination of skin biopsies from poikiloderma lesions reveals characteristic features that confirm the and distinguish it from mimics. Common findings include epidermal with flattening of the rete ridges, vacuolar () degeneration of the basal layer, and occasional apoptotic . In the , there is often incontinence, evidenced by melanophages in the superficial layers, alongside a mild perivascular lymphocytic infiltrate. Dilated, ectatic capillaries in the papillary correspond to the clinical telangiectasias observed. These microscopic changes support the clinical suspicion of poikiloderma identified during evaluation. In congenital forms, such as Rothmund-Thomson syndrome, biopsies may additionally show and rare dyskeratotic cells in affected areas. Special stains enhance characterization of specific etiologies. For ultraviolet radiation-associated acquired poikiloderma, such as poikiloderma of Civatte, elastic tissue stains (e.g., Verhoeff-van Gieson) consistently demonstrate solar elastosis, with amorphous, basophilic degeneration of elastic fibers in the papillary dermis present in nearly all cases. In poikilodermatous , an acquired variant, reveals atypical + or + T-lymphocytes with epidermotropism, often forming a band-like infiltrate at the dermoepidermal junction; CD3 positivity with focal loss of CD7 supports the lymphoid nature. Ancillary tests are crucial for etiological clarification. , including sequencing of the RECQL4 , is recommended for suspected congenital poikiloderma to identify biallelic pathogenic variants confirming diagnoses like Rothmund-Thomson . For cases raising concern for underlying cutaneous , such as poikilodermatous , on lesional tissue or peripheral blood can assess T-cell clonality, complementing histopathological and molecular studies like TCR rearrangement.

Management

Treatment Approaches

Treatment of poikiloderma is primarily symptomatic and tailored to the underlying and specific subtype, as no curative therapy exists for most forms. Broad-spectrum sunscreens with high and strict sun avoidance are essential to prevent exacerbation of pigmentation changes, telangiectasias, and , particularly in photosensitive variants like poikiloderma congenitale. Topical emollients, such as bland moisturizers, help manage and maintain , reducing discomfort in affected areas. For vascular components, laser therapies offer targeted relief. Pulsed dye laser (PDL) effectively reduces telangiectasias in poikiloderma of Civatte, with studies showing significant improvement in redness and mottling after multiple sessions using fluences up to 50% higher than traditional settings. (IPL) or ablative fractional lasers address both vascular and pigmentary elements, providing safe clearance of poikilodermatous lesions with minimal downtime. Cause-specific interventions focus on managing associated conditions. In dermatomyositis-related poikiloderma, systemic immunosuppressants like combined with corticosteroids (e.g., prednisolone at 1 mg/kg/day) improve cutaneous manifestations, including poikilodermatous rashes, by targeting autoimmune inflammation. For poikilodermatous , a rare variant, 308-nm therapy combined with topical corticosteroids has shown promising improvement in in a 2025 case report after multiple sessions. In dyskeratosis congenita, where poikiloderma accompanies bone marrow failure, allogeneic serves as the definitive treatment for hematologic complications, though it carries risks and is not primarily for skin symptoms. Emerging therapies aim to mitigate implicated in poikiloderma . Research on congenital forms like Kindler syndrome suggests potential for topical antioxidants, such as , to reduce UV-induced (ROS) and damage in cellular models, though further clinical validation is required.

Prognosis and Complications

The of poikiloderma varies significantly depending on the underlying subtype, influencing treatment selection, with skin manifestations often remaining primarily cosmetic and non-progressive in milder forms such as certain presentations of poikiloderma congenitale (PC), where changes are confined to the skin without systemic involvement. In contrast, congenital forms like Rothmund-Thomson syndrome (RTS) carry a guarded outlook due to an elevated risk of malignancies, including in approximately 30% of affected individuals, typically diagnosed at a age of 11 years. in RTS is generally normal in the absence of malignancy, though complications such as metastatic cancers can lead to premature death. Complications in poikiloderma encompass both dermatologic and systemic sequelae, with chronic ulceration and secondary bacterial infections arising from atrophic skin changes and recurrent trauma in subtypes like . Malignant transformation is a notable risk, particularly in chronic or acquired cases, as well as in , where dysfunction predisposes to head and neck s and other solid tumors. Systemic issues in include bone marrow failure leading to in up to 90% of cases, alongside and increased susceptibility to . In , recurrent sinopulmonary infections can progress to , while rare instances of and further complicate the course. Ongoing monitoring is essential for optimizing outcomes, involving annual dermatologic examinations for early detection of skin cancers and prompt evaluation for skeletal abnormalities in RTS if symptoms suggestive of osteosarcoma emerge. Cancer screening protocols, including regular ophthalmologic assessments for cataracts and hematologic surveillance in DC and PN, help mitigate risks of progression. Recent advances in early neutropenia management in PN, through supportive measures like prophylactic antibiotics, have contributed to improved survival by reducing infection-related morbidity. Prognosis is also influenced by adherence to multidisciplinary care.

References

  1. [1]
    Inherited skin disorders presenting with poikiloderma - PubMed
    Mar 19, 2021 · Poikiloderma is a skin condition that combines atrophy, telangiectasia, and macular pigment changes (hypo- as well as hyperpigmentation).
  2. [2]
    Poikiloderma - an overview | ScienceDirect Topics
    Poikiloderma is a combination of linear telangiectasia, mottled hyperpigmentation/depigmentation, and superficial atrophy in a reticular pattern.
  3. [3]
    Acquired poikiloderma: proposed classification and ... - PubMed
    Jul 28, 2012 · "Poikiloderma" is a morphologic and descriptive term referring to a combination of cutaneous atrophy, telangiectasia, and varied macular ...
  4. [4]
    Poikiloderma of Civatte: What It Is, Causes, Treatment
    Poikiloderma of Civatte is a skin condition that appears as mottled, reddish-brown patches usually on the sides of your neck, upper chest and cheeks.Missing: reliable sources
  5. [5]
    Poikiloderma (Concept Id: C0392777) - NCBI
    Poikiloderma refers to a patch of skin with (1) reticulated hypopigmentation and hyperpigmentation, (2) wrinkling secondary to epidermal atrophy, ...
  6. [6]
    Poikiloderma of Civatte - DermNet
    The term 'poikiloderma' refers to a skin change with atrophy where hypopigmentation/hyperpigmentation changes and dilation of the fine blood vessels ( ...Missing: reliable | Show results with:reliable
  7. [7]
    Poikiloderma Vasculare Atrophicans: A Distinct Clinical Entity? - PMC
    Poikiloderma is characterized generally by erythema, atrophy, telangiectasias, hypo, and hyperpigmentation in a reticulate pattern. It is usually considered a ...
  8. [8]
    Diagnosis and Differential Diagnosis of Poikiloderma of Civatte
    Poikiloderma of Civatte (PC) is a rather common benign dermatosis of the neck and face, mainly affecting fair-skinned individuals, especially postmenopausal ...Missing: definition | Show results with:definition
  9. [9]
    Poikiloderma of Civatte: a clinical and epidemiological study - PubMed
    Almost half of the patients (46%) were symptomatic (itching, burning and 'flushing'). The mean duration from onset to diagnosis was 6.2 years according to the ...
  10. [10]
    Clericuzio-type poikiloderma with neutropenia and leg ulceration - NIH
    Skin ulcers that are slow to heal are associated with PN. However, a link between PG and Clericuzio-type poikiloderma has not been documented before. Of ...Missing: xerosis | Show results with:xerosis
  11. [11]
    Poikiloderma Congenitale - StatPearls - NCBI Bookshelf - NIH
    It is characterized by early-onset facial poikiloderma and associated with clinical features, including short stature, sparse scalp hair, absent or sparse ...
  12. [12]
    Dyskeratosis Congenita and Related Telomere Biology Disorders
    Nov 12, 2009 · Dyskeratosis congenita and related telomere biology disorders (DC/TBD) are caused by impaired telomere maintenance resulting in short or very short telomeres.Clinical Characteristics · Differential Diagnosis · Management · Genetic Counseling
  13. [13]
    Mutations in RECQL4 cause a subset of cases of Rothmund ...
    We report that three RTS patients carried two types of compound heterozygous mutations in RECQL4. The fact that the mutated alleles were inherited from the ...
  14. [14]
    Rothmund-Thomson syndrome: MedlinePlus Genetics
    Aug 1, 2013 · Poikiloderma congenitale of Rothmund-Thomson; RTS. Additional ... mutations in the RECQL4 gene in Rothmund-Thomson syndrome. J Natl ...
  15. [15]
    Rothmund-Thomson syndrome, a disorder far from solved - Frontiers
    Nov 9, 2023 · Mutations in RECQL4 cause a subset of cases of Rothmund-Thomson syndrome. ... Rothmund-Thomson syndrome, RECQL4, ANAPC1, DNA2, CRIPT, poikiloderma.
  16. [16]
    Rothmund-Thomson syndrome - Orphanet
    The prevalence is unknown, but around 500 cases have been reported so far. Clinical description. The skin is usually normal at birth. Erythema develops on the ...
  17. [17]
    Dyskeratosis congenita and telomere biology disorders - PMC
    Dec 9, 2022 · Dyskeratosis congenita (DC) and related telomere biology disorders (TBDs) comprise a heterogeneous group of illnesses caused by germline mutations resulting in ...
  18. [18]
    Disease progression and clinical outcomes in telomere biology ...
    Mar 24, 2022 · Dyskeratosis congenita related telomere biology disorders (DC/TBDs) are characterized by very short telomeres caused by germline pathogenic ...<|separator|>
  19. [19]
    Entry - #604173 - POIKILODERMA WITH NEUTROPENIA; PN - OMIM
    Poikiloderma with neutropenia (PN) is an autosomal recessive syndrome characterized by poikiloderma, hyperkeratotic nails, generalized hyperkeratosis on palms ...
  20. [20]
    Poikiloderma with Neutropenia - PubMed
    Feb 22, 2024 · Poikiloderma with neutropenia (PN) is characterized by an inflammatory eczematous rash (appears at ages 6-12 months) followed by post-inflammatory poikiloderma.
  21. [21]
    Poikiloderma with Neutropenia - SpringerLink
    Jun 18, 2021 · Poikiloderma with neutropenia (PN) is an ultra-rare autosomal recessive genodermatosis with fewer than 200 patients reported in the literature.
  22. [22]
    Acquired poikiloderma: Proposed classification and diagnostic ...
    Aug 7, 2025 · 2 Poikiloderma can be caused by acquired disorders ( Table 2); most of them are inflammatory or neoplastic. 3 However, it is also a key symptom ...Missing: scleroderma | Show results with:scleroderma
  23. [23]
    Diagnosis and differential diagnosis of Poikiloderma of Civatte
    Jan 31, 2023 · Introduction: Poikiloderma of Civatte (PC) is a common, acquired, chronic, benign poikiloderma of the neck and face, most commonly affecting ...
  24. [24]
    Poikilodermatous mycosis fungoides: A study of its ... - ResearchGate
    Aug 7, 2025 · Poikilodermatous mycosis fungoides (MF) is a rare clinical variant of patch-stage MF and is characterized by deep-red or brownish plaques with ...
  25. [25]
    [PDF] Poikiloderma: Differential Diagnosis & Treatment
    Iatrogenic causes: 1. Drugs: corticosteroids and hydroxyurea. 2. Radiotherapy. 7. Neoplastic causes: 1. Poikilodermatous mycosis fungoides. 2. Poikilodermatous ...Missing: subtypes | Show results with:subtypes
  26. [26]
    Inflammatory Skin Conditions Associated With Radiotherapy
    The condition presents with poikiloderma, hyper- or hypopigmented areas, atrophy, and telangiectasia (Fig. 1). Probably related to microvascular damage, ...Review · Skin Conditions Induced... · Skin Conditions Triggered Or...
  27. [27]
    A Long Journey of Poikilodermatous Erythroderma to ... - NIH
    “Poikiloderma” in dermatology is a descriptive term used for combination of cutaneous atrophy, telangiectasia, hypo or hyperpigmented macules giving mottled ...Missing: definition symptoms reliable sources
  28. [28]
    Rothmund-Thomson Syndrome - GeneReviews® - NCBI Bookshelf
    Jun 4, 2020 · The prevalence of skin cancers in individuals with RTS is estimated from the literature to be 5%. Skin cancer can occur at any age, although it ...Clinical Characteristics · Differential Diagnosis · Management · Genetic Counseling
  29. [29]
    A Rare Case of Poikilodermatous Mycosis Fungoides - PMC - NIH
    There are numerous variants of MF, among which poikilodermatous MF is a rare variant constituting 1%–2% of the total cases.[2] Herein, we report one such rare ...
  30. [30]
    Poikiloderma Of Civatte - Causes, Symptoms, Diagnosis, Treatment ...
    Apr 25, 2025 · Geographic Location: Individuals living in sunny climates or at higher altitudes are at increased risk due to higher UV radiation levels.Missing: distribution | Show results with:distribution
  31. [31]
    (PDF) Poikilodermatous changes on the forearms of a woman ...
    May 20, 2025 · ... prevalence is likely higher, especially among fair-. skinned populations living in sunny climates.2. Poikiloderma of Civatte (PC) most often ...
  32. [32]
    Poikiloderma of Civatte - Dermatology Advisor
    Mar 13, 2019 · Poikiloderma of Civatte is a combination of linear telangiectasia, reticulate hyperpigmentation and slight atrophy occurring most commonly in sun-exposed areas.Are You Confident Of The... · Figure 1 · Optimal Therapeutic Approach...
  33. [33]
    Inflammatory Skin Conditions Associated With Radiotherapy
    Another name for sclerodermiform-like panniculitis after radiation is sclerosing postirradiation panniculitis. This uncommon form of panniculitis presents as a ...
  34. [34]
    Reduce Redness and Texture from Poikiloderma
    Poikiloderma ... It's most often caused by chronic sun exposure, but can also be linked to hormonal shifts, radiation therapy, or certain autoimmune conditions.
  35. [35]
    Dyskeratosis Congenita - StatPearls - NCBI Bookshelf - NIH
    Patients with graft-versus-host disease have poikiloderma, and mucosal changes are lichen planus-like. There are also a few variants of DKC that have ...
  36. [36]
    The Role of Genetic Testing in Hereditary Poikiloderma - NIH
    Genetic testing through whole exosome and direct Sanger sequencing identified a novel homozygous missense mutation c. 623A>G, p.
  37. [37]
    Mutations in FAM111B Cause Hereditary Fibrosing Poikiloderma ...
    In conclusion, we have demonstrated that mutations in FAM111B cause HFP with tendon contracture, myopathy, and pulmonary fibrosis. Our findings identify FAM111B ...Missing: acquired | Show results with:acquired
  38. [38]
    Unique Dermatological and Systemic Manifestations in a Classic ...
    May 27, 2025 · It is an autosomal recessive disorder caused by mutations in the FERMT1 gene, which encodes the protein kindlin-1, located on chromosome 20p12.3 ...Missing: acquired | Show results with:acquired
  39. [39]
    Dermatomyositis: Myositis and the Skin - HSS
    Poikiloderma, a discoloration of the skin resulting from the combination of dilated blood vessels, hyperpigmentation, hypopigmentation, and mild skin thinning.
  40. [40]
    [PDF] Poikiloderma: Differential Diagnosis and Treatment - Hilaris Publisher
    Poikiloderma is one of the diagnostic cutaneous signs for chronic GVHD and is often present on the face and trunk during sclerodermoid phase of the disease. 3.Missing: subtypes | Show results with:subtypes
  41. [41]
    Role of Matrix Metalloproteinases in Photoaging and ...
    Jun 2, 2016 · MMPs are responsible for degrading the extracellular matrix (ECM) proteins such as collagen, fibronectin, elastin, and proteoglycans, contributing to ...
  42. [42]
    Poikiloderma of Civatte: A Histopathological and Ultrastructural Study
    Mar 9, 2007 · Background: Poikiloderma of the face and neck (Civatte) has not been studied in depth for decades, especially as far as the histopathology ...
  43. [43]
    Skin abnormalities in disorders with DNA repair defects, premature ...
    Poikiloderma consists of three features: hyper- and hypopigmentation ... The DNA repair-deficient diseases reviewed here are rare genetic disorders ...Cockayne Syndrome · Rothmund-Thomson Syndrome · Recql4 In Dna Repair<|control11|><|separator|>
  44. [44]
    https://pmc.ncbi.nlm.nih.gov/articles/PMC3853004/
  45. [45]
    Wood lamp skin examination - DermNet
    Aug 8, 2014 · A Wood lamp is used to identify the extent of pigmented or depigmented patches and to detect fluorescence.Missing: poikiloderma | Show results with:poikiloderma
  46. [46]
    Evaluation of reliability, validity, and responsiveness of the CDASI ...
    Total scores range from 0-28, 0-17 for activity and 0-11 for damage. Neither activity nor damage is scored by percentage of body surface area involvement.
  47. [47]
    Dermatologic Look-Alikes: Hyperpigmented Patches on Face and ...
    Oct 17, 2024 · First described by French dermatologist Achille Civatte in 1923, poikiloderma of Civatte is widely recognized as photoaging— a long-term ...
  48. [48]
    https://pmc.ncbi.nlm.nih.gov/articles/PMC4926402/
  49. [49]
    Poikiloderma with Neutropenia - GeneReviews® - NCBI Bookshelf
    Oct 26, 2017 · Clinical characteristics. Poikiloderma with neutropenia (PN) is characterized by an inflammatory eczematous rash (appears at ages 6-12 ...
  50. [50]
    Treatment of poikiloderma of Civatte using a redesigned pulsed dye ...
    Nov 27, 2018 · This study demonstrates the safety and effectiveness of a new pulsed‐dye laser with a 15 mm spot and 50% higher fluences for the treatment of poikiloderma of ...
  51. [51]
    Treatment of Poikiloderma of Civatte with ablative fractional laser ...
    In this prospective study, AFP was both safe and effective for the treatment of the vascular, pigmentary and textural components of PC.
  52. [52]
    Erythroderma and extensive poikiloderma – a rare initial ... - NIH
    Mar 24, 2018 · She was started on orally administered prednisolone 1 mg/kg per day with methotrexate 10 mg once a week and had a good response to treatment ...
  53. [53]
    Successful Treatment of Poikilodermatous Mycosis Fungoides with ...
    Feb 12, 2025 · Successful Treatment of Poikilodermatous Mycosis Fungoides with 308-nm Excimer Laser Open Access ; Received: January 11 2025 ; Accepted: February ...
  54. [54]
    UV-B-induced cutaneous inflammation and prospects for antioxidant ...
    One reasonable therapeutic approach emerging from our results is the antioxidant treatment, which could avoid downstream effects of ROS, like additional DNA and ...