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By protecting against cutaneous inflammation, epidermal pigmentation provided an additional advantage for ancestral humans

机译:通过防止皮肤发炎,表皮色素沉着为祖先人类提供了额外的优势

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Pigmentation evolved in ancestral humans to protect against toxic, ultraviolet B irradiation, but the question remains: “what is being protected?” Because humans with dark pigmentation display a suite of superior epidermal functions in comparison with their more lightly pigmented counterparts, we hypothesized and provided evidence that dark pigmentation evolved in Africa to support cutaneous function. Because our prior clinical studies also showed that a restoration of a competent barrier dampens cutaneous inflammation, we hypothesized that resistance to inflammation could have provided pigmented hominins with yet another, important evolutionary benefit. We addressed this issue here in two closely related strains of hairless mice, endowed with either moderate (Skh2/J) or absent (Skh1) pigmentation. In these models, we showed that (a) pigmented mice display a markedly reduced propensity to develop inflammation after challenges with either a topical irritant or allergen in comparison with their nonpigmented counterparts; (b) visible and histologic evidence of inflammation was paralleled by reduced levels of pro‐inflammatory cytokines (i.e., IL‐1α and INFα); (c) because depigmentation of Skh2/J mouse skin enhanced both visible inflammation and pro‐inflammatory cytokine levels after comparable pro‐inflammatory challenges, the reduced propensity to develop inflammation was directly linked to the presence of pigmentation; and (d) furthermore, in accordance with our prior work showing that pigment production endows benefits by reducing the surface pH of skin, acidification of albino (Skh1) mouse skin also protected against inflammation, and equalized cytokine levels to those found in pigmented skin. In summary, pigmentation yields a reduced propensity to develop inflammation, consistent with our hypothesis that dark pigmentation evolved in ancestral humans to provide a suite of barrier‐linked benefits that now include resistance to inflammation.
机译:色素沉着在祖先人类中进化出来,以防止有毒的紫外线B辐射,但问题仍然是:“什么受到保护?”由于深色色素的人与浅色色素的人相比显示出一系列优越的表皮功能,因此我们进行了假设并提供了证据,证明深色色素在非洲进化而来支持皮肤功能。因为我们先前的临床研究还表明,恢复有效屏障可以抑制皮肤炎症,所以我们假设对炎症的抵抗力可能为有色人参素提供了又一个重要的进化益处。我们在两个紧密相关的无毛小鼠品系中解决了这个问题,这些品系具有中度(Skh2 / J)或不存在(Skh1)的色素沉着。在这些模型中,我们表明(a)与无色素的小鼠相比,有色素的小鼠在受到局部刺激性或过敏原刺激后,发炎的趋势明显降低; (b)炎症的可见和组织学证据与促炎性细胞因子(即IL-1α和INFα)水平降低相平行; (c)由于在可比的促炎性攻击后,Skh2 / J小鼠皮肤的色素脱色同时增强了可见的炎症和促炎性细胞因子水平,因此发炎倾向的降低与色素沉着的存在直接相关; (d)此外,根据我们先前的研究表明,色素的产生通过降低皮肤的表面pH值而受益,白化病(Skh1)小鼠皮肤的酸化也可以防止发炎,并使细胞因子水平与有色素的皮肤相同。总而言之,色素沉着降低了发炎的倾向,这与我们的假设相一致,即我们的假设是,深色色素沉着在祖先的人类中进化,从而提供了一系列的屏障相关益处,现在包括抵抗炎症。

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