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白发早生中黑色素生成标志物的表达:一项横断面研究。

Melanogenesis Markers Expression in Premature Graying of Hair: A Cross-Sectional Study.

作者信息

Pss Ranugha, Madhunapantula Subbarao V, Betkerur Jayadev B, Bovilla Venugopal R, Shastry Veeranna

机构信息

Department of Dermatology, JSS Medical College, JSSAHER, Mysore, India.

Department of Biochemistry, JSS Medical College, JSSAHER, Mysore, India.

出版信息

Skin Pharmacol Physiol. 2022;35(3):180-186. doi: 10.1159/000520172. Epub 2021 Oct 26.

Abstract

BACKGROUND

Studies on mice and aging human hair follicles provide compelling evidence that graying of hair results from premature differentiation of melanocyte stem cells in the niche/bulge.

OBJECTIVE

The aim of this study was to analyze whether differentiation of melanocyte stem cells is responsible for premature graying of hair (PGH).

METHODS

Twenty-five patients with PGH (n = 25) attending the dermatology department were recruited. Five unpigmented and 5 pigmented hairs were obtained per patient by separating individual follicles after 1 mm punch biopsies. The hairs were dissected at a distance of 2 mm from the bulb to separate the stem cells (upper segment - US) from the melanocytes (lower segment - LS). RNA was extracted from hair follicle US and LS, and expression of GP100, tyrosinase (TYR), and tyrosinase-related protein-1 (TYRP1) genes was quantified using Qiagen one-step RT-PCR kit.

RESULTS

We found melanogenesis gene expression in both temporary (US) and permanent (LS) segments of unpigmented and pigmented hair follicles. When compared between the US and LS of white hair, the expression of TYR and GP100 was much higher in US than LS, suggestive of melanogenesis in the bulge. Similarly, when compared between white and black US, the expression of all 3 genes was higher in white US than black US, although not statistically significant.

LIMITATIONS

Low samples size and lack of data pertaining to the expression of genes at protein level are the limitations of current study.

CONCLUSION

Even though this pilot study data yielded key information about the expression of GP100, TYR, and TYRP-1 at the mRNA level, further studies quantifying the expression of these genes at protein level are needed to provide additional clues to further address the results in detail.

摘要

背景

对小鼠和衰老人类毛囊的研究提供了令人信服的证据,表明头发变白是由于毛囊微环境/隆突区黑素细胞干细胞的过早分化所致。

目的

本研究旨在分析黑素细胞干细胞的分化是否是头发过早变白(PGH)的原因。

方法

招募了25名到皮肤科就诊的PGH患者(n = 25)。在1毫米钻孔活检后,通过分离单个毛囊,每名患者获取5根无色素毛发和5根有色素毛发。从距毛囊球部2毫米处将毛发解剖,以将干细胞(上段-US)与黑素细胞(下段-LS)分离。从毛囊的上段和下段提取RNA,并使用Qiagen一步法RT-PCR试剂盒对GP100、酪氨酸酶(TYR)和酪氨酸酶相关蛋白-1(TYRP1)基因的表达进行定量。

结果

我们在无色素和有色素毛囊的临时(上段)和永久(下段)部分均发现了黑素生成基因的表达。白发上段和下段相比,上段中TYR和GP100的表达远高于下段,提示隆突区有黑素生成。同样,白发上段和黑发上段相比,所有3个基因的表达在白发上段中均高于黑发上段,尽管无统计学意义。

局限性

样本量少以及缺乏蛋白质水平基因表达的数据是本研究的局限性。

结论

尽管这项初步研究数据产生了关于GP100、TYR和TYRP-1在mRNA水平表达的关键信息,但仍需要进一步研究在蛋白质水平定量这些基因的表达,以提供更多线索,进一步详细分析结果。

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