Hubbry Logo
search
logo
Dermatofibroma avatar
Dermatofibroma
Dermatofibroma
current hub
2091811

Dermatofibroma

logo
Community Hub0 Subscribers
Read side by side
Dermatofibroma
View on Wikipedia
from Wikipedia
Dermatofibroma
Other namesDermal dendrocytoma,[1] Dermatofibroma,[2] Fibrous dermatofibroma,[2] Fibrous histiocytoma,[2] Fibroma simplex,[1] Nodular subepidermal fibrosis,[1] and Sclerosing hemangioma[1])
Histopathology of dermatofibroma, with basilar hyperpigmentation of the overlying epidermis (top right), and spindled fibroblasts with collagen entrapment. HE stain.
SpecialtyOncology Edit this on Wikidata

A dermatofibroma, or benign fibrous histiocytomas, is a benign nodule in the skin, typically on the legs, elbows or chest of an adult.[3] It is usually painless.[3]

It usually ranges from 0.2 to 2 cm in size but larger examples have been reported.[3] It typically results from mild trauma such as an insect bite.[3] Risk factors for developing multiple dermatofibromas include lupus, HIV, blood cancer and some medicines that weaken immunity.[3]

It is usually diagnosed by its appearance, but a biopsy may be required.[3] Other bumps such as granular cell tumor, melanoma, clear cell acanthoma and dermatofibrosis lenticularis disseminata may look similar.[3] Usually no treatment is needed.[3] It can remain unchanged for years but can resolve spontaneously.[3]

Signs and symptoms

[edit]

Dermatofibromas[4] are hard solitary slow-growing papules (rounded bumps) that appear in a variety of colours, usually brownish to tan. They are often elevated or pedunculated. A dermatofibroma is associated with the dimple sign; by applying lateral pressure, there is a central depression of the dermatofibroma. Although typical dermatofibromas cause little or no discomfort, itching and tenderness can occur. Dermatofibromas can be found anywhere on the body, but most often they are found on the legs and arms.[5] They occur more often in women; the male to female ratio is about 1:4.[6] The age group in which they most commonly occur is 20 to 45 years.

Some physicians and researchers believe dermatofibromas form as a reaction to previous injuries such as insect bites or thorn pricks.[6] They are composed of disordered collagen laid down by fibroblasts. Dermatofibromas are classed as benign skin lesions, meaning they are completely harmless, though they may be confused with a variety of subcutaneous tumours.[7] Deep penetrating dermatofibromas may be difficult to distinguish, even histologically, from rare malignant fibrohistocytic tumours like dermatofibrosarcoma protuberans.[8]

Dermatofibromas typically have a positive buttonhole sign, or central dimpling in the center.[9]

Diagnosis

[edit]

Immunohistochemical staining

[edit]
Neoplasm CD34[1] Stromelysin-3[10] Factor XIIIa[6]
Dermatofibroma - + +
Dermatofibrosarcoma protuberans + - -

See also

[edit]

References

[edit]
[edit]
Revisions and contributorsEdit on WikipediaRead on Wikipedia

Dermatofibroma

View on Grokipedia
from Grokipedia
Dermatofibroma, also known as fibrous histiocytoma, is a common benign cutaneous soft-tissue lesion characterized by firm subcutaneous nodules, typically measuring ≤1 cm in diameter.[1] These nodules most frequently appear on the extremities, particularly the lower legs, and are usually asymptomatic, though they may cause pruritus, tenderness, or pain in some cases.[2] A distinctive clinical feature is the "dimple sign," where lateral pressure on the lesion causes central invagination due to tethering of the overlying epidermis.[1] Epidemiologically, dermatofibromas affect individuals across all ages but are most prevalent between 20 and 50 years, with a notable female predominance (up to a 2:1 ratio).[1] They constitute approximately 3% of all skin biopsy specimens in dermatopathology practices and show no significant racial predilection.[2] The etiology remains unknown, but many cases are associated with prior local trauma, such as insect bites or minor injuries, suggesting a possible reactive process, though neoplastic origins involving clonal fibroblast proliferation have also been proposed.[1] Histologically, these lesions feature a dermal proliferation of spindle-shaped fibroblasts and histiocytes, often with trapped collagen bundles and a characteristic Grenz zone separating the lesion from the epidermis.[2] Diagnosis is primarily clinical based on the lesion's appearance, with confirmation via excisional biopsy if atypical features raise concern for malignancy; dermoscopy may reveal a central white patch surrounded by a peripheral pigmented network.[1] Treatment is generally unnecessary due to the benign nature, but symptomatic lesions or those mimicking melanoma may be excised, with low recurrence rates except in rare aggressive variants like cellular or aneurysmal subtypes.[2] Overall, dermatofibromas have an excellent prognosis, with spontaneous regression occasionally reported, and they pose no significant health risk.[1]

Background

Definition

Dermatofibroma, also known as fibrous histiocytoma or benign fibrous histiocytoma, is a common benign cutaneous soft-tissue lesion that typically presents as a firm subcutaneous nodule measuring ≤1 cm in diameter.[1] These lesions are composed of a localized proliferation of spindle-shaped fibroblasts and histiocytes within the dermis, often arranged in a storiform pattern.[3] A hallmark histological feature is the entrapment of collagen bundles at the lesion's periphery, which creates a characteristic radial extension of hyalinized collagen fibers into the surrounding dermis.[4] The cellular composition primarily involves fibroblastic and histiocytic elements, with variable amounts of inflammatory cells and hemosiderin deposition depending on the subtype.[1] Epidermal changes overlying the lesion, such as acanthosis and hyperpigmentation of the basal layer, are frequently observed, along with a Grenz zone of uninvolved papillary dermis separating the lesion from the epidermis.[3] Dermatofibroma is generally regarded as a reactive process, potentially triggered by minor trauma or insect bites, rather than a true neoplasm.[5] However, debate persists regarding its precise nature, with some evidence suggesting clonal fibroblast proliferation indicative of neoplastic potential, while others emphasize its self-limited, non-aggressive behavior.[1] This distinction underscores the lesion's benign prognosis, with rare instances of local recurrence following incomplete excision but no metastatic capability.[3]

Epidemiology

Dermatofibroma is one of the most common benign cutaneous lesions, accounting for approximately 3% of all skin biopsy specimens in dermatopathology laboratories.[1] The exact incidence remains difficult to quantify due to its typically asymptomatic presentation and the tendency for many cases to go undiagnosed or unreported without medical consultation.[1] This underreporting is exacerbated by the lesion's benign nature, which often leads to incidental discovery rather than proactive evaluation.[1] The condition affects individuals across all age groups, though it is most prevalent in adults aged 20 to 50 years.[6] Studies indicate that around 80% of biopsied cases occur in patients between 20 and 49 years old.[2] There is a notable female predominance, with women affected up to twice as frequently as men.[7] No significant racial or geographic variations are reported, suggesting that dermatofibroma occurs equally across ethnicities and worldwide populations.[7] Multiple lesions are observed in approximately 10% of cases, frequently appearing in clusters on the lower extremities.[1]

Etiology and Pathophysiology

Etiology

The etiology of dermatofibroma remains largely unknown, though it is widely regarded as a benign reactive process triggered by minor external insults to the skin.[1] While many cases develop spontaneously, associations have also been reported with immunosuppression (e.g., in HIV patients), pregnancy, and altered immune states. Local trauma is identified in only about 20% of cases.[1] Common associations include local trauma, such as insect bites, splinters, superficial puncture wounds, or injections, which may initiate a localized proliferative response in the dermis.[1] Some cases have been linked to arthropod assaults or episodes of folliculitis, supporting the hypothesis of a reactive hyperplasia in response to these insults.[8] No confirmed genetic or hereditary factors have been identified for the development of typical dermatofibromas, distinguishing them from more aggressive fibrohistiocytic tumors.[1] Rare reports of familial clustering, such as eruptive variants in association with atopic dermatitis, suggest possible hereditary influences in exceptional cases, though a missense mutation in the coagulation factor XIII-A subunit gene has been identified in cases of autosomal dominant multiple dermatofibromas; these are not established as a primary cause.[9][10] Hormonal influences have been speculated as a contributing factor, given the observed female predominance in occurrence, though this link remains unproven and unsupported by direct mechanistic evidence.[1]

Pathophysiology

Dermatofibroma arises from a benign proliferation of spindle-shaped fibroblasts and histiocytes within the dermis, frequently extending into the superficial subcutis to form a well-circumscribed nodular lesion.[1] This dermal accumulation of fibroblastic cells intermingled with histiocytic elements leads to the development of a firm, fibrous nodule that is typically confined to the reticular dermis.[2] A distinctive histopathological feature is the peripheral entrapment of collagen bundles, which radiate outward from the lesion's border, creating a spiculated margin that enhances the nodule's induration and resistance to deformation.[1] This collagen trapping represents a reactive fibrous response at the interface between the proliferating cells and surrounding stroma, contributing to the lesion's structural integrity without significant disruption of adjacent tissues.[2] The pathogenesis involves ongoing debate regarding whether dermatofibroma primarily represents a reactive process, often initiated by minor trauma such as insect bites or skin injury, or a low-grade neoplastic proliferation.[1][2] While some studies demonstrate clonality in the histiocytic component, suggestive of a neoplastic origin, the fibroblastic population frequently shows polyclonality, supporting a reactive etiology in most cases.[11][12] The pathogenesis remains debated, with evidence supporting both a reactive process, often initiated by minor trauma, and a low-grade neoplastic proliferation involving clonal fibroblast or histiocyte growth.[7] Lesions grow slowly over time due to the gradual deposition of extracellular matrix and fibrous tissue by the proliferating fibroblasts, rarely exceeding 1 cm in diameter.[1] In typical cases, there is no prominent vascular component or sustained inflammatory infiltrate, distinguishing the process from more aggressive fibrohistiocytic tumors.[2]

Clinical Features

Signs and Symptoms

Dermatofibromas typically present as slow-growing, firm papules or nodules that are reddish-brown or hyperpigmented, measuring 3 to 10 mm in diameter.[7][1] These lesions often have a smooth or slightly dimpled surface and may vary in color from pink to dark brown depending on skin tone and lesion age.[1] They occur more frequently in females.[1] The most common locations are the lower extremities, particularly the legs, followed by the arms and trunk, while involvement of the face or mucous membranes is rare.[7][13] Lesions are generally solitary but can be multiple in some individuals.[1] Although dermatofibromas are usually asymptomatic, they may cause pruritus (itching), tenderness, or pain upon lateral pressure in affected patients.[7][1] A distinctive clinical sign is the positive dimple sign (or pinch sign), elicited by laterally compressing the lesion, which produces a central depression due to its tethering to the underlying dermis.[1][7] These benign growths tend to persist indefinitely without spontaneous regression in most cases, remaining stable for years.[1]

Variants

Dermatofibromas exhibit several histological variants that deviate from the classic form, each characterized by distinct morphological features that can influence clinical presentation and diagnostic considerations. These variants maintain the benign nature of the lesion but may mimic other conditions, such as vascular tumors or melanomas, due to their atypical appearances. Recognition of these subtypes is essential for accurate diagnosis, as they often require histopathological confirmation to differentiate from malignant entities.[14] The cellular variant, comprising less than 5% of cases, displays increased cellularity with dense fascicles of spindle-shaped fibroblasts extending into the subcutis, contrasting with the more moderate proliferation in typical dermatofibromas. Clinically, it presents as a firm nodule predominantly on the extremities, with a higher risk of local recurrence following excision, reported in up to 26% of incompletely excised lesions.[15][16] In the aneurysmal variant, which accounts for about 1.7% of dermatofibromas, prominent hemorrhagic cystic spaces devoid of endothelial lining dissect through the fibrous stroma, potentially evolving from hemosiderotic changes and mimicking angiosarcoma. This subtype often arises after trauma and appears as a rapidly enlarging, bluish lesion prone to bleeding upon manipulation.[14][17] The epithelioid variant features large, rounded epithelioid cells with abundant eosinophilic cytoplasm and vesicular nuclei, comprising at least 50% of the cellular population, which can resemble melanoma cells histologically. Clinically, it manifests as an erythematous, polypoid nodule, most commonly on the lower extremities (60% of cases), with an epidermal collarette at the base.[14] Hemosiderotic dermatofibroma is marked by extensive iron deposition from prior hemorrhage, resulting in a blue-black coloration that distinguishes it from the typical brown hue of classic lesions. Histologically, it shows prominent hemosiderin-laden macrophages, small capillaries, and acanthosis, with a female predominance and frequent occurrence on the extremities.[14][17] The atypical, or pseudosarcomatous, variant exhibits pleomorphic spindle cells with hyperchromatic nuclei and increased mitotic activity, raising concerns for sarcoma despite its benign behavior and lack of metastatic potential in most cases. These lesions tend to be larger (average 3.2 cm) and may show irregular borders clinically, necessitating careful histopathological evaluation.[14] Finally, the atrophic variant presents as a depressed, scar-like patch with central umbilication, more prevalent in females (5:1 ratio) and often located above the waist. Histologically, it is defined by dermal thinning, sclerotic collagen bundles, and reduced cellularity, differing from the protuberant, firm classic form.[14][17]

Diagnosis

Clinical Evaluation

Clinical evaluation of dermatofibroma begins with a detailed patient history to assess potential etiological factors and lesion characteristics. Clinicians inquire about any preceding trauma, such as insect bites or minor injuries, which is reported in approximately 20% of cases.[1] The duration of the lesion is typically longstanding, spanning months to years, with slow growth and stability over time.[1] Patients may also express cosmetic concerns, particularly if the nodule is visible on exposed areas, though many lesions remain asymptomatic; occasional pruritus can prompt evaluation.[1] Physical examination focuses on visual inspection and palpation to confirm characteristic features. Lesions appear as firm, nontender cutaneous nodules, usually measuring less than 1 cm in diameter, with colors ranging from tan-pink to reddish-brown depending on age and pigmentation.[1] Palpation reveals a rubbery consistency, often larger than visible, and elicits the classic dimple sign—a central depression formed by lateral compression due to tethering of the lesion to the dermis.[1][18] High clinical suspicion arises in young adults, particularly women, presenting with nodules on the lower extremities.[18] Dermoscopy enhances diagnostic accuracy by revealing stereotypical patterns that distinguish dermatofibroma from mimics like melanoma. A central white scar-like patch is observed in about 57% of cases, with a peripheral delicate pigment network in approximately 51% or brown globules in approximately 42%.[19] These features, such as the peripheral pigment network with central hypopigmentation, provide a non-invasive clue for differentiation.[1][18] Routine imaging is not required for typical presentations, as clinical and dermoscopic findings suffice for diagnosis in most instances. Biopsy is reserved for atypical cases where doubt persists, such as rapid growth or unusual location.[1]

Histopathological Findings

Dermatofibromas are characterized histologically by a well-circumscribed dermal nodule composed of spindle-shaped fibrohistiocytic cells arranged in a storiform pattern, often with interspersed histiocytes, foam cells, and multinucleated giant cells.[1] The overlying epidermis typically shows hyperplasia, including acanthosis, hyperkeratosis, and elongated rete ridges that extend downward around the lesion, known as the "dirty feet" appearance.[1] At the periphery, collagen trapping is evident, where thick collagen bundles are entrapped by the tumor cells, contributing to the lesion's circumscription.[1] Immunohistochemically, dermatofibroma cells are positive for factor XIIIa, a marker of dermal dendrocytes, and CD68, indicating histiocytic differentiation.[1][20] They are typically negative for CD34, which helps distinguish them from dermatofibrosarcoma protuberans, and S100, ruling out neural neoplasms.[1][21] Certain variants exhibit distinct histopathological changes; for instance, the aneurysmal variant features prominent hemorrhage with blood-filled cystic spaces lacking endothelial lining, while hemosiderotic variants show abundant hemosiderin deposition.[22] Mitotic figures are rare in benign cases, and necrosis is absent, supporting the tumor's benign nature.[22][23] Diagnosis is confirmed via biopsy, with punch biopsy suitable for smaller lesions or when preservation of the epidermis is important, and excisional biopsy preferred for complete removal and evaluation in atypical presentations.[1][24]

Differential Diagnosis

Differentiating dermatofibroma from other cutaneous lesions is essential due to its benign nature contrasted with potentially malignant mimics, often requiring histopathological examination for confirmation.[1] Clinical features such as the characteristic firm nodule with a dimple sign upon lateral compression can provide initial clues, but overlap with other entities necessitates further evaluation.[1][25] Dermatofibrosarcoma protuberans (DFSP) is a key malignant mimic, presenting as a larger, more infiltrative plaque-like lesion that grows slowly and may lack the dimple sign.[1][26] Histologically, DFSP shows a more cellular spindle cell proliferation with deeper subcutaneous invasion and fat entrapment in a honeycomb pattern, unlike the superficial dermal involvement in dermatofibroma.[1] Immunohistochemistry (IHC) aids differentiation, with DFSP typically CD34-positive and factor XIIIa-negative, while dermatofibroma exhibits the opposite pattern; wider excision is required for DFSP management.[1] Kaposi sarcoma may resemble vascular variants of dermatofibroma, particularly in immunocompromised patients, appearing as reddish-purple patches or nodules with a vascular component.[1][26] Key distinguishing features include prominent vascularity and extravasated red blood cells on histology, often associated with human herpesvirus 8 (HHV-8) infection.[1] IHC confirms HHV-8 positivity, along with endothelial markers like CD31 and CD34, which are not characteristic of dermatofibroma.[1] Pigmented lesions such as intradermal nevus or melanoma can mimic darker variants of dermatofibroma, especially when symmetrically raised and brown.[25] However, nevi are typically softer without the firm consistency or dimple sign, while melanomas show asymmetry, irregular borders, and color variation on dermoscopy, often with an atypical pigment network.[25][26] Histology and IHC reveal S100 positivity in melanocytic lesions, contrasting with the fibroblastic markers in dermatofibroma.[1] Leiomyoma presents as a painful, firm dermal nodule, differing from the usually asymptomatic dermatofibroma.[25] It arises from smooth muscle and shows positivity for smooth muscle markers like desmin and smooth muscle myosin heavy chain on IHC, which are not expressed in dermatofibroma.[27] Scars or keloids may be confused with dermatofibroma due to their firm, raised appearance following trauma, but they lack a discrete nodule and dimple sign, often extending beyond the original injury site.[25] Keloids are hypertrophic and irregular, with a history of preceding injury, whereas dermatofibroma typically develops without such trauma.[25] In ambiguous cases, IHC panels and deeper biopsies are crucial to distinguish dermatofibroma from these mimics, ensuring accurate diagnosis and appropriate management.[1]

Management

Conservative Approaches

For most patients with typical, asymptomatic dermatofibromas, observation is the recommended conservative approach, as these benign lesions generally follow a stable course without intervention.[28][1] Reassurance regarding the harmless nature of the lesion is often sufficient, particularly since the majority remain unchanged over time.[29] In cases where pruritus or mild inflammation is present, topical corticosteroids, such as low-potency options like hydrocortisone or triamcinolone acetonide, can be applied to alleviate symptoms by reducing local irritation.[30][31] For more persistent itching, intralesional steroid injections using triamcinolone may help flatten the lesion slightly and diminish symptoms, though results vary.[28][29] Patient education plays a key role in conservative management, emphasizing the importance of avoiding trauma to the lesion, such as from scratching or tight clothing, to prevent irritation, ulceration, or apparent growth.[28] Individuals should be advised to monitor for any changes in size, color, or symptoms and seek medical evaluation if these occur.[1] If cosmetic appearance causes concern, non-invasive camouflage techniques, such as medical-grade makeup or self-tanning products, can be used to mask the lesion without structural alteration.[32] Routine follow-up is not required for stable lesions, but periodic self-examination is encouraged, with professional reassessment prompted only by notable changes, as spontaneous regression occurs rarely.[2][1]

Surgical and Other Interventions

Surgical excision is the primary intervention for dermatofibromas causing cosmetic concerns or symptoms such as pain or pruritus, involving complete removal of the lesion with narrow margins to minimize scarring.[3] This approach is particularly recommended for atypical variants, including cellular and aneurysmal types, due to their higher potential for incomplete resolution with less invasive methods.[15] Recurrence rates following standard excision are low, typically less than 5% for conventional dermatofibromas, though rates can reach 10-25% in cellular or aneurysmal variants depending on margin involvement.[33][34] Cryotherapy, utilizing liquid nitrogen to freeze small lesions in 1-2 cycles, serves as a minimally invasive option for superficial dermatofibromas when excision is not preferred.[35] It offers effective resolution in many cases but carries risks of hypopigmentation and blistering, particularly in darker skin types.[29] Recurrence is more common than with excision.[36] Laser therapy, including CO2 and pulsed-dye lasers, targets superficial lesions to ablate tissue and reduce vascularity, providing cosmetic benefits with potentially less scarring than traditional surgery.[3] Pulsed-dye laser at 595-600 nm has demonstrated clinical improvement in lesion appearance and symptoms, with good tolerability in small series.[37][38] CO2 laser ablation is suitable for facial or visible sites, though data on long-term efficacy remain limited.[39] Curettage combined with electrodesiccation involves scraping the lesion followed by cauterization to destroy residual tissue, reserved for select superficial or smaller dermatofibromas.[40] This method achieves adequate removal in appropriate cases but may result in higher recurrence compared to full excision, especially for deeper lesions.[3]

Prognosis

Long-term Outcomes

Dermatofibromas are benign cutaneous lesions with an excellent prognosis, exhibiting no malignant potential in the vast majority of cases.[1] These tumors typically demonstrate indolent behavior, remaining stable over many years without progression to malignancy.[1] Most lesions persist indefinitely, either unchanging or slowly enlarging, though spontaneous regression occurs rarely, potentially leaving hypopigmented patches on the skin.[1] Recurrence following complete surgical excision is rare, but may increase to approximately 20% in atypical variants such as cellular or aneurysmal types, particularly if removal is incomplete.[41] Dermatofibromas involve only the skin and do not produce systemic effects.[1] Reports of metastasis are extremely rare and confined to atypical cases, often involving larger lesions exceeding 3 cm, though such instances are debated as potential misdiagnoses of more aggressive entities like dermatofibrosarcoma protuberans.[1] Rare cases of malignant transformation, such as progression to high-grade sarcoma, have been reported in certain variants as of 2024.[42]

Complications

Dermatofibromas are typically benign and do not pose significant health risks, but rare lesion-related complications can occur, including ulceration and bleeding, particularly in the aneurysmal variant where the lesion is friable and contains blood-filled spaces prone to hemorrhage.[1][43] These issues may arise from trauma, such as shaving over the lesion or friction from clothing, leading to chronic irritation, tenderness, or minor pain in affected areas like the lower extremities.[7][29][44] Treatment-related complications are more commonly encountered, especially with surgical excision, which can result in infection, bleeding, scarring, or disfigurement, with the resulting scar sometimes more noticeable than the original lesion.[1] Cryotherapy, used for irritated lesions, may cause hypopigmentation due to melanocyte sensitivity to cold, while hypertrophic scars can develop post-surgery in susceptible individuals.[45][46] Although not a medical complication, the cosmetic appearance of dermatofibromas can lead to psychological distress or anxiety, prompting removal for aesthetic reasons.[29][44] Dermatofibromas carry no increased risk of malignant transformation to skin cancer.[1][29] Monitoring is recommended for any changes, such as rapid growth or ulceration, to rule out mimics like dermatofibrosarcoma protuberans.[1]

References

  1. Dermatofibroma - StatPearls - NCBI Bookshelf - NIH
  2. Dermatofibroma: Background, Pathophysiology, Etiology
  3. Dermatofibroma: Reappraisal and Updated Review - PMC
  4. Dermatofibroma (cutaneous fibrous histiocytoma) - Pathology Outlines
  5. Dermatofibroma (fibrous histiocytoma) pathology - DermNet
  6. Dermatofibroma (benign fibrous histiocytoma) - UpToDate
  7. Dermatofibroma (histiocytoma) - DermNet
  8. Clinicopathologic Analysis of Dermatofibroma: A Retrospective ... - NIH
  9. Familial Eruptive Dermatofibromas in Atopic Dermatitis - PubMed
  10. Dermatofibroma is a clonal proliferative disease - PubMed
  11. Dermatofibroma (Benign Fibrous Histiocytoma) - Basicmedical Key
  12. Dermatofibroma: Causes, images, and treatment - MedicalNewsToday
  13. https://doi.org/10.2147/CCID.S526191
  14. Clinicopathologic Review of 218 Cases of Cellular Dermatofibroma ...
  15. [PDF] Cellular dermatofibroma: A case report and review of the literature
  16. Variants of dermatofibroma--a histopathological study - PubMed
  17. Dermatofibroma, histiocytoma - Primary Care Dermatology Society
  18. Dermoscopy of Dermatofibromas: A Prospective Morphological ...
  19. Atypical Cutaneous Fibrous Histiocytoma: An Unusual and ... - NIH
  20. Dermatofibromas with Aberrant Expression of CD34 Protein - NIH
  21. Variants of dermatofibroma - a histopathological study - PMC
  22. Giant Hemosiderotic Dermatofibroma: A Case Report and Review of ...
  23. Atrophic Dermatofibroma: A Comprehensive Literature Review - PMC
  24. [PDF] Dermatofibroma: a curious tumor. - Jefferson Digital Commons
  25. Deciphering dermatofibromas: A confocal and dermoscopic ...
  26. Expression of Desmin and Smooth Muscle Myosin Heavy Chain in ...
  27. Dermatofibroma Treatment & Management - Medscape Reference
  28. Dermatofibroma (also known as histiocytoma)
  29. [PDF] Dermatofibroma
  30. Dermatofibroma Symptoms and Treatment Options - Triage
  31. Treatment of a symptomatic dermatofibroma with fractionated carbon ...
  32. Skin Camouflage - Newcastle Hospitals NHS Foundation Trust
  33. Cellular Dermatofibroma: Causes, Symptoms & Treatment
  34. Cellular dermatofibroma (fibrous histiocytoma): A challenging ...
  35. Cryosurgery for Common Skin Conditions - AAFP
  36. Cutaneous Cryosurgery for Common Skin Conditions - AAFP
  37. Dermatofibromas treated with pulsed dye laser - PubMed
  38. Treatment of dermatofibroma with a 600 nm pulsed dye laser
  39. Multiple dermatofibromas on face treated with carbon dioxide laser
  40. Common Benign Skin Tumors | AAFP
  41. Challenging Patterns of Atypical Dermatofibromas and Promising ...
  42. https://www.sciencedirect.com/science/article/pii/S2213576625001903
  43. Dermatofibroma Natural History: What Happens If Left Untreated
  44. Cutaneous Cryosurgery | AAFP
  45. Cryotherapy: Uses, Cautions, and Aftercare - DermNet
User Avatar
No comments yet.