Frontiers in alopecia areata pathobiology research

Gilhar, Amos; Laufer-Britva, Rimma; Keren, Aviad; Paus, Ralf

doi:10.1016/j.jaci.2019.08.035

Cited by 65 publications

(70 citation statements)

References 148 publications

(256 reference statements)

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“…This supports the concept that pathological mast cell‐T cell interactions may contribute to the pathogenesis of human AA, perhaps particularly so in atopic individuals 6,44,179 . Recent experiments have demonstrated that the AA phenotype can also be triggered by non–antigen‐specific innate lymphocytes such as type 1 innate lymphoid cells 44,284 . Therefore, besides mast cells, several innate and adaptive immune cell lineages may be functionally important in AA pathogenesis.…”

Section: Hair Follicle Immune Privilege Collapse As a Prerequisite Fosupporting

confidence: 74%

“…Mast cells strikingly switch from an immunoinhibitory phenotype and infrequent interactions with CD8 + T cells to a profoundly pro‐inflammatory phenotype and greatly enhanced interactions with CD8 + lymphocytes, and—highly unusual for mast cells—even proliferate around lesional HFs in situ 179 . This supports the concept that pathological mast cell‐T cell interactions may contribute to the pathogenesis of human AA, perhaps particularly so in atopic individuals 6,44,179 . Recent experiments have demonstrated that the AA phenotype can also be triggered by non–antigen‐specific innate lymphocytes such as type 1 innate lymphoid cells 44,284 .…”

Section: Hair Follicle Immune Privilege Collapse As a Prerequisite Fomentioning

confidence: 54%

“…The literature reveals that there are different NK and NKT subsets including regulatory ones 324,325 . Collectively, these studies indicate that multiple cell types may have roles in AA aetiology by breaking the delicate balance between scalp skin‐resident memory T cells versus immune cells with regulatory effects 44 …”

Section: Hair Follicle Immune Privilege Collapse As a Prerequisite Fomentioning

confidence: 96%

“…Compelling functional evidence for the existence of HF IP has not only been provided long ago by Billingham 21,22 but also in mutant mice overexpressing non‐HF antigens (e.g. 39 ) as well as by the observation that AA does not occur without HF IP collapse 4,6,33,43,44 …”

Section: Basic Immune Privilege Conceptsmentioning

confidence: 99%

“…Using a humanized mouse model of AA, Gilhar and colleagues have provided further functional evidence for this concept: The injection of large numbers of autologous IL‐2‐stimulated (activated) CD56 + and NKG2D + cells (T cells, NK and NKT cells) from healthy donors into healthy human scalp skin transplanted onto SCID/beige mice suffices to induce a clinical phenocopy of AA in the skin transplants 278 . Hence, AA should be viewed as a HF response pattern, for whose initiation a genuine autoimmune response pattern is only one of several distinct options (Figure 3; Table 3, 1a‐c) 4,6,33,44 …”

Section: Hair Follicle Immune Privilege Collapse As a Prerequisite Fomentioning

confidence: 99%

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Hair follicle immune privilege and its collapse in alopecia areata

Bertolini

McElwee

Gilhar

et al. 2020

Experimental Dermatology

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168

157

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Anagen stage hair follicles (HFs) exhibit “immune privilege (IP)” from the level of the bulge downwards to the bulb. Both passive and active IP mechanisms protect HFs from physiologically undesired immune responses and limit immune surveillance. IP is relative, not absolute, and is primarily based on absent, or greatly reduced, intra‐follicular antigen presentation via MHC class I and II molecules, along with prominent expression of “no danger” signals like CD200 and the creation of an immunoinhibitory signalling milieu generated by the secretory activities of HFs. Perifollicular mast cells, Tregs and other immunocytes may also contribute to HF IP maintenance in healthy human skin. Collapse of anagen hair bulb IP is an essential prerequisite for the development of alopecia areata (AA). In AA, lesional HFs are rapidly infiltrated by NKG2D + T cells and natural killer (NK) cells, while perifollicular mast cells acquire a profoundly pro‐inflammatory phenotype and interact with autoreactive CD8+ T cells. Using animal models, significant functional evidence has accumulated that demonstrates the dominance of the immune system in AA pathogenesis. Purified CD8+T‐cell and NK cell populations alone, which secrete fγ, suffice to induce the AA phenotype, while CD4+T‐cells aggravate it, and Tregs and iNKT cells may provide relative protection against AA development. While IP collapse may be induced by exogenous agents, inherent IP deficiencies might confer increased susceptibility to AA for some individuals. Thus, a key goal for effective AA management is the re‐establishment of a functional HF IP, which will also provide superior protection from disease relapse.

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Section: Hair Follicle Immune Privilege Collapse As a Prerequisite Fosupporting

confidence: 74%

Section: Hair Follicle Immune Privilege Collapse As a Prerequisite Fomentioning

confidence: 54%

Section: Hair Follicle Immune Privilege Collapse As a Prerequisite Fomentioning

confidence: 96%

Section: Basic Immune Privilege Conceptsmentioning

confidence: 99%

Section: Hair Follicle Immune Privilege Collapse As a Prerequisite Fomentioning

confidence: 99%

See 3 more Smart Citations

Hair follicle immune privilege and its collapse in alopecia areata

Bertolini

McElwee

Gilhar

et al. 2020

Experimental Dermatology

Self Cite

168

157

View full text Add to dashboard Cite

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Acquired Disorders of Hair

Harries,

Holmes,

McMichael

et al. 2024

Rook's Textbook of Dermatology

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This chapter reviews acquired hair disorders, including common scarring and non‐scarring alopecia presentations, conditions characterised by excessive body hair growth and acquired hair shaft disorders. We also describe the biology of normal hair follicles, including structure, hair cycle control and immunity, to better understand the mechanisms underlying these conditions. We present methods for clinical assessment, recommended investigation and management of each disease, and present summaries of frequently used therapeutics and cosmetic options employed when treating these problems.

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Platelet‐rich plasma in the treatment of alopecia areata after COVID‐19 vaccination

Teng¹,

Chen²

2023

Clinical Case Reports

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Key Clinical Message Alopecia areata may develop in patients after COVID‐19 vaccination. Platelet‐rich plasma (PRP) has an outstanding anti‐inflammatory effect and could be an alternative treatment for alopecia patients who are refractory or intolerant to corticosteroids. Abstract A 34‐year‐old female with no systemic illness presented with non‐scarring hair loss after the second COVID‐19 vaccination shot 4 weeks ago. The hair loss worsened and progressed to severe alopecia areata. We started double‐spin PRP therapy. Her hair recovered completely after six courses of PRP treatment.

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Frontiers in alopecia areata pathobiology research

Cited by 65 publications

References 148 publications

Hair follicle immune privilege and its collapse in alopecia areata

Hair follicle immune privilege and its collapse in alopecia areata

Acquired Disorders of Hair

Platelet‐rich plasma in the treatment of alopecia areata after COVID‐19 vaccination

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