Melanocyte and gonad activity as potential severity modifying factors in C3H/HeJ mouse alopecia areata

被引:20
|
作者
McElwee, KJ
Silva, K
Beamer, WG
King, LE
Sundberg, JP
机构
[1] Jackson Lab, Bar Harbor, ME 04609 USA
[2] Vanderbilt Univ, Dept Dermatol, Nashville, TN USA
关键词
autoimmune disease; disease susceptibility; mouse model;
D O I
10.1034/j.1600-0625.2001.100605.x
中图分类号
R75 [皮肤病学与性病学];
学科分类号
100206 ;
摘要
Circumstantial evidence has previously suggested gonad derived steroid hormones and melanogenesis related antigens may modify human alopecia areata (AA). AA-like hair loss can be induced in C3H/HeJ mice after skin allografts from spontaneous AA-affected mice. This inducible model was used to evaluate hormones and hair follicle melanocyte presence as disease-severity modifiers. Ten females and 9 mates were gonadectomized and received AA-affected allografts. All gonadectomized mice had 2-4 weeks delay in AA onset relative to non-gonadectomized controls. Two females and 4 males failed to develop any AA by 25 weeks after grafting. The experiment was repeated with gonadectomized female and male mice plus non-gonadectomized mice subcutaneously implanted with silastic capsules containing 80 mug 17 beta estradiol or 10 mg 5 alpha dihydrotestosterone, respectively. Five of 11 ovariectomized and 9 of 11 non-ovariectomized, estradiol supplemented females developed AA with extremely rapid progression. Three of 8 castrated, but none of 11 non-castrated, dihydrotestosterone-supplemented males expressed AA. In a separate study, 14 mice were freeze-branded, producing white hair on the dorsal lumbar region, and later received full-thickness allografts. Thirteen mice developed patchy pigmented and non-pigmented hair loss. One mouse developed diffuse, pigmented hair loss, but with white hair survival persisting 25 weeks after grafting. The results suggest that gonadal steroid hormones can modulate C3H/HeJ mouse AA where estradiol promoted rapid progression of AA while dihydrotestosterone increased resistance to AA onset. In general, both pigmented and non-pigmented C3H/HeJ mouse hair is susceptible to AA. Murine AA susceptibility and severity clearly involves an interplay between genetic and epigenetic factors.
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页码:420 / 429
页数:10
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