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利用小分子对黑色素生成进行剖析,确定 prohibitin 为一种调节因子。

Dissection of melanogenesis with small molecules identifies prohibitin as a regulator.

作者信息

Snyder Jane R, Hall Andrea, Ni-Komatsu Li, Khersonsky Sonya M, Chang Young-Tae, Orlow Seth J

机构信息

The Ronald O. Perelman Department of Dermatology, New York University, New York 10016, USA.

出版信息

Chem Biol. 2005 Apr;12(4):477-84. doi: 10.1016/j.chembiol.2005.02.014.

Abstract

Bioactive compounds can be used to selectively modulate gene function. We utilized a chemical genetic approach to dissect the mammalian pigmentation pathway and identify protein regulators. We screened a tagged library of 1170 small molecules in a cell-based assay and discovered a class of pigment-enhancing chemicals. From this class we characterized the small molecule melanogenin. Using melanogenin bound to an affinity matrix and amino acid sequencing, we identified the mitochondrial protein, prohibitin, as an intracellular binding target. Studies employing siRNA demonstrate that prohibitin is required for melanogenin to exert its propigmentary effects and reveal an unsuspected functional role for this protein in melanin induction. This represents a mechanism by which propigmentary signals are transduced and ultimately provides a potential target for the treatment of pigmentary disorders.

摘要

生物活性化合物可用于选择性调节基因功能。我们利用化学遗传学方法剖析哺乳动物色素沉着途径并鉴定蛋白质调节因子。我们在基于细胞的分析中筛选了一个包含1170种小分子的标记文库,发现了一类色素增强化学物质。从这类物质中,我们对小分子黑素原进行了表征。利用与亲和基质结合的黑素原和氨基酸测序,我们确定线粒体蛋白 prohibitin 为细胞内结合靶点。使用 siRNA 的研究表明,prohibitin 是黑素原发挥其促色素作用所必需的,并揭示了该蛋白在黑色素诱导中一个未曾预料到的功能作用。这代表了一种促色素信号转导的机制,并最终为色素紊乱的治疗提供了一个潜在靶点。

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