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Frontal Fibrosing Alopecia

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Last Update: June 7, 2024.

Continuing Education Activity

Frontal fibrosing alopecia results in a retraction of the frontal implantation line of the scalp. This cicatricial alopecia involves the frontal line and can extend to the preauricular and retroauricular regions of the scalp. In the advanced stages of the disease, the contrast is evident between the alopecic area, where the skin is pale and devoid of follicular openings, and the rest of the forehead, which is hyperpigmented with signs of solar elastosis. The implantation line has an unusual appearance due to the disappearance of all hair follicles.

This activity reviews the epidemiology, genetics, clinical presentation, and management of frontal fibrosing alopecia, equipping clinicians to improve patient care for this condition. Sometimes, an erythema or perifollicular papules are apparent in the active stages of the disease and on the edges of the alopecic zone. Alopecia may extend to the occipital or parietal implantation line and may form circular patterns. Frontal fibrosing alopecia is a special form of lichen planopilaris affecting the frontal area in women, most often after menopause. The description of the condition in humans is recent, and the recognition of family cases is newly described.

Objectives:

  • Determine the histopathological features of frontal fibrosing alopecia based on physical examination findings.
  • Compare the physical examination findings commonly observed in patients with frontal fibrosing alopecia.
  • Implement the treatment plan for frontal fibrosing alopecia guided by the pattern of hair loss.
  • Collaborate with dermatologists, endocrinologists, and other healthcare professionals to optimize multidisciplinary care for patients with frontal fibrosing alopecia.
Access free multiple choice questions on this topic.

Introduction

Frontal fibrosing alopecia is a type of hair loss identified by Kossarden in 1994. The condition is characterized by band-like cicatricial alopecia of the frontotemporal zone of the scalp. Signs of perifollicular inflammation are apparent at the edge of the hairy region, with associated eyebrow alopecia and involvement of axillary, pubic, facial, and hairy lesions of the limbs. Histopathological examination shows a lymphocytic infiltrate around the isthmus and infundibulum, associated with a decrease in the number of follicles replaced by fibrosis.[1] Frontal fibrosing alopecia is a special form of lichen planopilaris affecting the frontal area in women, most often after menopause. The description in humans is recent, and the recognition of cases in families is newly described (see Image. Frontal Fibrosing Alopecia).

Etiology

The mechanism of the disease is still unclear. Family cases are increasingly reported, which suggests a genetic factor. Environmental factors, including dioxin-like substances in the food of animal origin, drugs, sun exposure, sunscreens, and viral infections, could be the trigger in genetically predisposed patients.[2]

Epidemiology

The incidence of frontal fibrosing alopecia is increasing in Europe, the United States, and Japan. Frontal fibrosing alopecia mainly affects women after menopause, typically around the age of 60.[3] However, instances have been documented in premenopausal women, with the youngest reported case aged 21, and rarely in men.[4] Men are mainly affected when genetic factors are involved. Among African women, frontal fibrosing alopecia is often associated with traction alopecia that worsens the progression of the disease. Japanese women have less severe forms compared to European women.[5]

Pathophysiology

Frontal fibrosing alopecia is a special form of lichen planopilaris. Affected follicles may express a specific antigen to induce a T-lymphocyte immune response. Drug-induced lichen planopilaris has been documented with the use of certain medications, such as β-blockers and nonsteroidal anti-inflammatory drugs. In contrast, some drugs, such as angiotensin-converting enzyme inhibitors, have a protective role.[6] No drug-induced cases of frontal fibrosing alopecia have been described to date.

Many cases of frontal fibrosing alopecia have been reported after surgery, such as hair transplantation or facial lifting.[7] A Koebner phenomenon or the loss of the immune privilege of the follicle could explain this. The occurrence after menopause is in favor of a hormonal factor. The efficacy of anti-androgens, reported by some authors, favors this hypothesis.[8][9] However, the condition affects men and premenopausal women with normal hormonal balances. Hormone replacement therapy does not affect the course of the disease.[10]

Histopathology

In a series of 20 cases of frontal fibrosing alopecia, Vaisse et al confirmed the stereotypical clinical aspects of this disease.[11] Therefore, the diagnosis is exclusively clinical. In complex cases, a histological examination is useful. The examination demonstrates perifollicular lymphocytic infiltrate, apoptotic cells in the outer epithelial sheath, and perifollicular fibrosis followed by the destruction of the follicle, replaced by a nonspecific vertical fibrous band. More apoptosis and fewer inflammatory infiltrates occur in frontal fibrosing alopecia compared to lichen planopilaris.[12] The inflammatory infiltrates simultaneously affect the terminal, intermediate, and vellus hair, regardless of the hair cycle phase.

In the advanced stages of the disease, the histological aspect is not specific, showing cicatricial alopecia in all the affected areas.[13] Direct cutaneous immunofluorescence is often negative in frontal fibrosing alopecia. In contrast, the testing may reveal immunoglobulin M (IgM)-positive colloidal antibodies more rarely in IgA or C3 in 40% of lichen planopilaris cases.

History and Physical

Frontal fibrosing alopecia results in a retraction of the frontal implantation line of the scalp. This cicatricial alopecia involves the frontal line and can extend to the preauricular and retroauricular regions of the scalp. In the advanced stages of the disease, the contrast is evident between the alopecic area, where the skin is pale and devoid of follicular openings, and the rest of the forehead, which is hyperpigmented with signs of solar elastosis. The implantation line has an unusual appearance due to the disappearance of all hair follicles. Isolated hair, however, is observed in the affected areas. Erythema or perifollicular papules are present in the active stages of the disease and on the edges of the alopecic zone.

In some cases, alopecia may extend to the occipital or parietal implantation line and may form circular patterns.[14] The hair pull test is positive on the edges of affected areas during the active stages. The hair pull test is positive without clinical evidence of inflammation. Pruritus is rare in frontal fibrosing alopecia, unlike lichen planopilaris. Burns and pains are typically non-existent. Total or partial eyebrow alopecia affects 81% of patients with Kossard and 100% of the more recent series.[13][15] This eyebrow injury may precede frontal alopecia. The involvement of axillary, pubic, and limb regions has been documented, along with eyelashes.[16] Therefore, frontal fibrosing alopecia is a generalized hair condition close to the Graham Little-Piccardi-Lassueur syndrome, which combines cicatricial alopecia of the scalp and axillary and pubic alopecia.[17]

Evaluation

In a patient with frontal fibrosing alopecia, dermoscopy reveals the following signs:

  • The disappearance of follicular orifices and discrete peri-follicular desquamation
  • Marked perifollicular hyperkeratosis, more visible without immersion 
  • Perifollicular erythema is more visible with non-contact dermatoscopy
  • The disappearance of the follicular openings, which is not easy to highlight [18]

Special examination of the frontal line is required, especially during the initial stages of the disease.

Treatment / Management

No treatment is fully effective in frontal fibrosing alopecia. The absence of controlled trials and the potential for spontaneous resolution in frontal fibrosing alopecia necessitate caution before confirming treatment efficacy. No standardized criteria are available for measuring treatment effectiveness. Objective criteria include the hair count, a photographic evaluation, or measuring the distance between the glabella and the frontotemporal line. Price developed a severity score of the lichen planopilaris (LPPAI: Lichen Planopilaris Activity Index) but evaluates pain, burns, and pruritus, often absent in the frontal fibrosing alopecia. The LPP develops slowly; this is necessary to affirm the effectiveness of treatment 2 years after follow-up with standardized photographs and accounts of hair on marked areas.[19][20][21]

Potent local corticosteroids are insufficient to halt the progression of alopecia in 93% of cases, in some isolated stabilization cases, and sometimes in combination with minoxidil (2% or 5%). Intralesional corticosteroids provide an improvement in almost 60% of patients using intralesional injections of triamcinolone acetonide (10 mg/mL). The risk is to worsen atrophy. The efficiency is much better on the eyebrows, with 80% of patients experiencing partial or total regrowth after intralesional triamcinolone injections in the early stages.[22] Minoxidil is ineffective, except in cases with associated androgenic alopecia. Synthetic antimalarials, such as hydroxychloroquine or chloroquine, are ineffective in several series. Price reports an improvement in LPPAI in 73% of cases after 6 months of hydroxychloroquine in 16 patients with frontal fibrosing alopecia, but this improvement is considered crucial in only 36% of patients. Price, in the same series, treated 4 patients with doxycycline, with improvement in half of the patients after 6 months of treatment.[11] 

The most promising outcomes are achieved with 5-α-reductase inhibitors, finasteride, and dutasteride. Stabilization was observed in 4 out of 8 patients treated with finasteride at a dosage of 2.5 mg per day and minoxidil 2% for 18 months. Similarly, stabilization was noted in a patient treated with dutasteride at a dosage of 0.5 mg per day for 6 months with topical pimecrolimus for 3 months.[23] Frontal fibrosing alopecia is often associated with androgenic alopecia. 5ARI and minoxidil can improve androgenic alopecia, but they falsely suggest an improvement.

Topical tacrolimus, used alone, is ineffective and difficult on the scalp. Oral ciclosporin and mycophenolate mofetil have been proposed in lichen planopilaris with some efficiency, but a high recurrence rate is reported.[24][25] The number of cases of frontal fibrosing alopecia treated with ciclosporin or mycophenolate mofetil reported in the literature is too low to conclude, and adverse effects limit the use of these treatments. However, some consider ciclosporin as a future treatment. No indication of the use of hormone replacement therapy is indicated to improve frontal fibrosing alopecia. The condition can stabilize spontaneously.

Frontal fibrosing alopecia is a good indication of hair transplants because of its slow evolution. A recent publication on 3 grafted cases shows good growth of the grafts after 2 years, followed by the disappearance of more than 50% of the grafts after 3 years.[26] Signs of active disease are observed on the remaining grafts. Therefore, hair grafts may be considered for patients with stabilized disease, preferably after performing test grafts with a follow-up of at least 3 years.[27]

Differential Diagnosis

Androgenic alopecia most often affects the anterior borderline; intermediate hair and hairy duvet persist on this anterior border. No scarring or peri-follicular inflammation is apparent. The eyebrows are spared. The biopsy, when performed, highlights the miniaturization of the follicles. A sudden onset of frontal fibrosing alopecia affecting the eyebrows and the occipital areas can be confused with alopecia areata. Scarring alopecia is not obvious in the early stages. Dermoscopy is helpful in this case, revealing exclamation mark hair, black dots, yellow dots, and pigtail hairs.[28]

Chronic lupus erythematosus may lead to plaque-like frontal scarring, but a destructive pigment is absent in frontal fibrosing alopecia, diffuse hyperkeratosis, and diffuse erythema. Some women have high frontal implantation of familial origin, characterized by early-onset, non-cicatricial, normal eyebrows, and no perifollicular erythema, aiding in correct diagnosis.[29] Traction alopecia is common in women.[30] The persistence of anterior frontal hair is in favor of this diagnosis. Looking for sliding ducts along the traction zone represents a strong argument for diagnosing traction alopecia.

Prognosis

Alopecia can affect half of the scalp, often called crown alopecia. The progression of the disease is variable among patients, ranging from 0.2 to 2 cm per year without treatment or, on average, 0.9 mm per month. The final degree of alopecia before stabilization is difficult to predict.

Complications

Complications of frontal fibrosing alopecia extend beyond cosmetic concerns, encompassing psychosocial distress due to visible alopecia and the potential for irreversible scarring leading to permanent hair loss. In addition, frontal fibrosing alopecia is associated with ocular and facial involvement, including eyebrow loss, periorbital erythema, and cicatricial ectropion. Beard hair loss has recently been reported in patients.[31] The diagnosis often necessitates a multidisciplinary approach involving dermatologists, endocrinologists, and, occasionally, ophthalmologists to manage the condition comprehensively and address the diverse manifestations.[32]

Deterrence and Patient Education

Deterrence and patient education are pivotal in managing frontal fibrosing alopecia due to its challenging nature and limited treatment options. Educating patients about the progressive nature of frontal fibrosing alopecia, potential complications, and available treatment modalities is essential for fostering realistic expectations and enhancing treatment adherence. Emphasizing the importance of early detection and intervention can help mitigate disease progression and minimize irreversible scarring.

Furthermore, educating patients about potential triggers or exacerbating factors, such as sun exposure and certain skincare products, can enable them to make informed lifestyle choices to mitigate disease activity. Deterrence strategies may involve advocating for regular monitoring by dermatologists and prompt evaluation of new hair loss or changes in the frontal hairline or eyebrows. Collaborative efforts between clinicians and patients are crucial for optimizing outcomes and enhancing the quality of life in patients with frontal fibrosing alopecia.[33]

Enhancing Healthcare Team Outcomes

Frontal fibrosing alopecia is a relatively common disorder characterized by band-like cicatricial alopecia of the frontotemporal zone of the scalp. This condition often presents with signs of perifollicular inflammation at the edge of the hairy region, with associated eyebrow alopecia and the potential involvement of axillary, pubic, facial, and hairy lesions of the limbs.

Although the condition has no specific treatment, clinicians, including nurse practitioners, physician assistants, and primary care clinicians, should collaborate with dermatologists for expert guidance in managing the condition. Dermatology nurses play a vital role in this collaborative effort by providing patient education, monitoring treatment outcomes, and facilitating communication between patients and dermatologists. Pharmacists also contribute significantly by reviewing prescribed medications, identifying and managing potential drug interactions, and educating patients about possible adverse effects. Unfortunately, the prognosis for patients with frontal fibrosing alopecia is often poor, with many experiencing a significant degree of hair loss despite treatment efforts.

Review Questions

Frontal Fibrosing Alopecia

Figure

Frontal Fibrosing Alopecia. This cicatricial alopecia involves the frontal line and can extend to the preauricular and retroauricular regions of the scalp. DermNet New Zealand

References

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Disclosure: Hasnain Syed declares no relevant financial relationships with ineligible companies.

Disclosure: Safa Idoudi declares no relevant financial relationships with ineligible companies.

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