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黑素皮质素1受体亚型对组成性和紫外线诱导的皮肤色素沉着的调节。

Regulation of constitutive and UVR-induced skin pigmentation by melanocortin 1 receptor isoforms.

作者信息

Rouzaud Francois, Costin Gertrude-E, Yamaguchi Yuji, Valencia Julio C, Berens Werner F, Chen Kevin G, Hoashi Toshihiko, Böhm Markus, Abdel-Malek Zalfa A, Hearing Vincent J

机构信息

Laboratory of Cell Biology, National Cancer Institute, National Institutes of Health, Bethesda, Maryland, USA.

出版信息

FASEB J. 2006 Sep;20(11):1927-9. doi: 10.1096/fj.06-5922fje. Epub 2006 Jul 28.

Abstract

Melanin synthesized by epidermal melanocytes protects the skin against UVR-induced DNA damage and skin cancer. Exposure to UVR increases the synthesis of the photoprotective eumelanin on activation of MC1R, a melanoma susceptibility gene. We studied the expression of MC1R under UVR and alpha-MSH stimulation in skin of different ethnic origins and in melanocytes of various pigmentary levels. This study identifies and characterizes a novel MC1R isoform (MC1R350) generated by alternative splicing of the classically known MC1R (MC1R317). We demonstrate that the melanin content of melanocytes shows a significant positive correlation with MC1R317 levels but correlates inversely with the amount of MC1R350, suggesting that this latter isoform could act as a negative regulator of melanin synthesis. We confirmed that hypothesis by showing that while MC1R317 signaling significantly increases the expression of MITF and tyrosinase, two key factors in the melanin synthesis pathway, MC1R350 dramatically hampers their expression. In the skin, we show that UVR does not increase MC1R350 expression but does significantly increase MC1R317. Taken together, our results strongly suggest that MC1R350 acts as a negative regulator of skin pigmentation and demonstrate for the first time that MC1R isoform-specific expression is closely related to skin pigmentation and photoprotection.

摘要

由表皮黑素细胞合成的黑色素可保护皮肤免受紫外线辐射诱导的DNA损伤和皮肤癌。暴露于紫外线会增加光保护真黑素的合成,这一过程由黑素瘤易感基因MC1R的激活所介导。我们研究了不同种族来源皮肤以及不同色素水平黑素细胞在紫外线和α-促黑素刺激下MC1R的表达情况。本研究鉴定并表征了一种由经典的MC1R(MC1R317)通过可变剪接产生的新型MC1R异构体(MC1R350)。我们发现,黑素细胞的黑色素含量与MC1R317水平呈显著正相关,但与MC1R350的量呈负相关,这表明后一种异构体可能作为黑色素合成的负调节因子。我们通过实验证实了这一假设,即MC1R317信号显著增加了黑色素合成途径中的两个关键因子MITF和酪氨酸酶的表达,而MC1R350则显著抑制它们的表达。在皮肤中,我们发现紫外线不会增加MC1R350的表达,但会显著增加MC1R317的表达。综上所述,我们的结果有力地表明MC1R350作为皮肤色素沉着的负调节因子,并且首次证明MC1R异构体特异性表达与皮肤色素沉着和光保护密切相关。

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