Location

Fox-Fordyce disease typically affects apocrine gland-rich areas of the body such as axillae, areolae, anogenital area and to a lesser extent the umbilicus, perineum and medial aspect of the upper thigh.[11] Less frequently affected locations include the lips, thorax, abdomen, and legs.[16] Bilateral skin involvement is typical.

Lesional Morphology

Primary lesions are 2 to 3 mm dome-shaped follicular or perifollicular papules that are typically characterized by distribution, although they can vary in color (skin-colored, yellow, reddish, violaceous). Their distribution is in crops around apocrine-gland dense areas (axillary, areolar, perianal, genital) that may appear linear when the skin becomes stretched. Associated features include hypotrichosis and hyperkeratosis, and excoriation marks secondary to scratching.

Chief Symptoms

FFD’s characteristic skin eruption is often associated with extreme pruritus, which worsens with hyperhidrosis, sweating, stress, and anxiety.

Chronic FFD may present as lichenified, thickened, coarse, hyperpigmented skin secondary to damage caused by scratching. Severe FFD may also demonstrate localized anhidrosis and brittle, sparse, or absent hair due to the subsequent destruction of the gland and associated hair follicle.

Clinical Course

The course of FFD is chronic relapsing and remitting, which may continue for years. The disease may improve as the affected glands become damaged, often with resulting local anhidrosis. FFD usually improves during pregnancy, and after menopause.

The diagnosis of Fox-Fordyce disease is by and large clinical. However, evaluation with the following methods is possible:

(1) Dermoscopy reveals hair follicle-centered papules, traumatized terminal hairs, and blackheads.[19]

(2) Histopathology - Biopsy from the papules reveal the changes detailed above (vide supra), with perifollicular foam cells pathognomonic of the condition.

(3) In vivo High-definition optical coherence tomography (HD-OCT) -  Axial/ slice images showed distinct epidermal lesions in the epidermis extending into the upper dermis. Intralesional dilated ductal structures surrounded by a dark rim indicative of fluid were visible in the en face images. Hyperrefractile (bright) lesions appeared on the skin surface on 3-dimensional reconstruction.[20][21] HD-OCT remains an experimental imaging technique for FFD.

Data is limited to case reports and small case series, precluding definitive recommendations on the best approach. Example of interventions that may be effective include methods to reduce inflammation, inhibit ductal occlusion, or reduce sweating as well as procedures that remove or destroy sweat glands.

First line: First-line treatments include topical and oral retinoids, topical benzoyl peroxide, topical clindamycin, intralesional or topical corticosteroids (TCS), topical calcineurin inhibitors (CNIs), and oral contraceptives [16]. These are the initial choices because of availability, easy administration, and low risk for serious side effects. There has been no establishment of optimal regimens. Recurrence is possible after discontinuing treatment.

• Low potency topical corticosteroids (TCS) are best (less risk of skin atrophy, striae, fissuring), usually twice daily until symptoms improve and then may decrease to daily use two to three times per week.
• Topical clindamycin twice daily. May see improvement in the first few weeks. The mechanism is unclear [22]
• Topical CNIs reduce inflammation akin to TCS without the risk of cutaneous atrophy. Both pimecrolimus and tacrolimus use have resulted in moderate to near-complete clearance.[23][24][25]
• Topical retinoids - Both tretinoin and adapalene are options. These are thought to reduce follicular occlusion and secondary ductal occlusion. Skin irritation is an issue. Patients may tolerate application every other day instead of daily may be better tolerated.[26][27]
• Oral isotretinoin has shown decent results in anecdotal reports.[28]

Second line and Novel Treatments

These are better for cases that are severe and/or refractory to the first-line therapies. These include:

Surgical excision, fractional lasers including 1550 nm erbium glass, pulsed dye laser, botulinum toxin, phototherapy, electrocoagulation, copper vapor, and CO laser, liposuction-assisted-curettage, and microwave technology.[29][30][31][32][33][34]

Although Fox-Fordyce disease is easily diagnosable by its typical clinical presentation and characteristic histopathology, certain conditions must be considerations in differential diagnoses:

• Folliculitis – erythematous papules and/or pustules; FFD does not have pustules
• Pseudofolliculitis – “ingrown hairs” - typically involving the lower shave-area of the neck in men and repeatedly waxed areas in women.
• Miliaria rubra or profunda – eccrine miliaria are vesicular or popular eruptions 2/2 occlusion of eccrine sweat glands. Unlike FFD, the above may occur in any site with eccrine glands.
• Milia – 1 to 2 mm epidermal inclusion cysts, usually on the face, usually white or yellow (used to distinguish from FFD papules)
• Granular parakeratosis – uncommon, hyperkeratotic brown-red papules that coalesce into plaques in intertriginous areas (axilla is most common). Pruritus is common.
• Syringomas – multiple 2 to 4 mm skin-colored, brown, or pink papules. Most common on periorbital skin, but may occur in intertriginous areas or other areas. May need a biopsy to distinguish from FFD. Histology reveals small collections of epithelial cells with central ducts in the superficial dermis.[35][36]
• Acanthosis nigricans – hyperpigmented velvety plaques that may have a papular appearance; occurs in intertriginous sites or skin folds, e.g., axillae or posterior neck.
• Graham-Little-Piccardi-Lasseur syndrome - characterized by lichen planopilaris and non-scarring alopecia of other parts of the body, typically axillae
• Darier's disease & Hailey-Hailey Disease [37]
• A pruritic generalized variant of Trichostasis spinulosa - It presents with typical involvement of the face, trunk (interscapular area) and the differential is the dermoscopic finding of multiple vellus hairs bundled in a funnel-like structure.[38]

Although at present, there is no published report, there is a hypothesis that fractionated microneedle radiofrequency may be an effective therapeutic option in Fox-Fordyce disease.[39] This concept has been extrapolated from the proven histopathological evidence of the efficacy of microneedle radiofrequency for the treatment of axillary hyperhidrosis.[40] Moreover, there are reports that micro-needling promotes the migration and proliferation of epidermal and dermal cells, especially keratinocytes and fibroblasts that release several growth factors that might result in a favorable transformation of the perifollicular cellular milieu and reduce pruritus.[41]

There is no definitive cure for Fox-Fordyce disease, but the symptomatic improvement to complete resolution has been reported with the treatment modalities mentioned before (vide supra).[22] Thus, the overall prognosis is decent.

Chronic Fox-Fordyce disease may present as lichenified, thickened, coarse, hyperpigmented skin secondary to damage caused by scratching. Severe FFD may also demonstrate localized anhidrosis and brittle, sparse, or absent hair due to the subsequent destruction of the gland and associated hair follicle.

Data on Fox-Fordyce disease is limited to case reports and small case series, precluding definitive recommendations on the best approach to management. Example of interventions that may be effective include methods to reduce inflammation, inhibit ductal occlusion, or reduce sweating as well as procedures that remove or destroy sweat glands. The patient may also be instructed to try reducing stress, avoiding humid climates, and avoiding occlusive clothing to offset the pruritus. 

Physicians often confuse Fordyce spots (FS) with Fox-Fordyce disease.

Fordyce spots are tiny (1 to 5 mm), slightly elevated yellowish or white papules which represent a variant of sebaceous glands that are visible without hair follicles and typically involve the vermilion border of the lips, buccal mucosa, glans or shaft of the penis, and the vulva in females. They are of no consequence, but patients often seek consultation owing to their concern about the lesions and for cosmetic purposes.

Fox-Fordyce disease is a rare skin disorder and often gets misdiagnosed. Most skin disorders initially present to the primary care provider or nurse practitioner. 

Coordinated care between primary care providers and those who specialize in dermatology will best serve the patient, as this is a difficult diagnosis to make if the practitioner is unfamiliar with the disease process and presentation. 

Moreover, since plastic surgeons, as well as practitioners of other specialties, perform LHR, their recognition of the development of pruritic papules representing FFD following multiple sessions of LHR requires reinforcement. 

After the clinician makes the diagnosis, the pharmacist should educate the patient on the different drug therapies available and their potential adverse effects. If untoward side effects arise, the pharmacist should report their concerns to the clinician. The nurse should provide patient education regarding the various cosmetic procedures available, and the need to avoid stress, intense exposure to light and sunlight. Clinicians should obtain informed consent before any treatment and not offer unrealistic patient expectations. Only through such an interprofessional team approach can outcomes be improved. [Level V]