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作为人类表皮色素沉着进化“驱动力”的屏障需求。

Barrier requirements as the evolutionary "driver" of epidermal pigmentation in humans.

机构信息

Dermatology Services, Veterans Affairs Medical Center, San Francisco, California, USA.

出版信息

Am J Hum Biol. 2010 Jul-Aug;22(4):526-37. doi: 10.1002/ajhb.21043.

DOI:10.1002/ajhb.21043
PMID:20209486
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3071612/
Abstract

Current explanations for the development of epidermal pigmentation during human evolution are not tenable as stand-alone hypotheses. Accordingly, we assessed instead whether xeric- and UV-B-induced stress to the epidermal permeability barrier, critical to survival in a terrestrial environment, could have "driven" the development of epidermal pigmentation. (1) Megadroughts prevailed in central Africa when hominids expanded into open savannahs [approximately 1.5-0.8 million years ago], resulting in sustained exposure to both extreme aridity and erythemogenic UV-B, correlating with genetic evidence that pigment developed approximately 1.2 million years ago. (2) Pigmented skin is endowed with enhanced permeability barrier function, stratum corneum integrity/cohesion, and a reduced susceptibility to infections. The enhanced function of pigmented skin can be attributed to the lower pH of the outer epidermis, likely due to the persistence of (more-acidic) melanosomes into the outer epidermis, as well as the conservation of genes associated with eumelanin synthesis and melanosome acidification (e.g., TYR, OCA2 [p protein], SLC24A5, SLC45A2, MATP) in pigmented populations. Five keratinocyte-derived signals (stem cell factor-->KIT; FOXn1-->FGF2; IL-1alpha, NGF, and p53) are potential candidates to have stimulated the sequential development of epidermal pigmentation in response to stress to the barrier. We summarize evidence here that epidermal interfollicular pigmentation in early hominids likely evolved in response to stress to the permeability barrier.

摘要

目前关于人类进化过程中表皮色素沉着形成的解释,作为独立的假说并不可行。因此,我们转而评估了干燥和 UV-B 对表皮渗透性屏障的应激是否可能“驱动”了表皮色素沉着的发展。(1)在人类进入开阔的热带稀树草原时,中部非洲曾盛行特大干旱[约 150 万至 80 万年前],导致人类持续暴露在极端干旱和致红斑的 UV-B 之下,这与大约 120 万年前色素形成的遗传证据相吻合。(2)色素沉着的皮肤具有增强的渗透性屏障功能、角质层完整性/内聚性和降低的感染易感性。色素沉着皮肤的增强功能可归因于外表皮的较低 pH 值,这可能是由于外表皮中存在(更酸性的)黑素小体,以及与真黑素合成和黑素小体酸化相关的基因的保留(例如,TYR、OCA2[p 蛋白]、SLC24A5、SLC45A2、MATP)。五种角质形成细胞衍生的信号(干细胞因子-->KIT;FOXn1-->FGF2;IL-1alpha、NGF 和 p53)可能是刺激表皮色素沉着在屏障应激下顺序发育的潜在候选者。我们在这里总结了证据,表明早期人类表皮毛囊间色素沉着可能是对渗透性屏障应激的进化反应。

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