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通过在斑马鱼中筛选标记的三嗪文库,鉴定F1F0线粒体ATP酶作为调节皮肤色素沉着的靶点。

Identification of the F1F0 mitochondrial ATPase as a target for modulating skin pigmentation by screening a tagged triazine library in zebrafish.

作者信息

Jung Da-Woon, Williams Darren, Khersonsky Sonya M, Kang Tae-Wook, Heidary Noushin, Chang Young-Tae, Orlow Seth J

机构信息

Department of Chemistry, New York University, New York, NY 10003, USA.

出版信息

Mol Biosyst. 2005 May;1(1):85-92. doi: 10.1039/b417765g. Epub 2005 Mar 8.

Abstract

A triazine-based combinatorial library of small molecules was screened in zebrafish to identify compounds that produced interesting phenotypes. One compound (of 1536 screened) induced a dramatic increase in the pigmentation of early stage zebrafish embryos. This compound, PPA, was also found to increase pigmentation in cultured mammalian melanocytes. The cellular target was identified as the mitochondrial F1F0-ATP synthase (ATPase) by affinity chromatography. Oligomycin, a small molecule known to inhibit the mitochondrial ATPase, competed with PPA for its cellular target in melanocytes. In addition, PPA was shown to alter the membrane potential of mitochondria, consistent with inhibition of the mitochondrial ATPase. Thus, PPA has been successfully used as a chemical probe in a forward chemical genetic approach to establish a link between the phenotype and the protein. The results attest to the power of screening small molecule libraries in zebrafish as a means of identifying mammalian targets and suggest the mitochondrial ATPase as a target for modulating pigmentation in both melanocytes and melanoma cells.

摘要

在斑马鱼中筛选了一个基于三嗪的小分子组合文库,以鉴定产生有趣表型的化合物。在所筛选的1536种化合物中,有一种化合物可使斑马鱼早期胚胎的色素沉着显著增加。这种化合物,即PPA,还被发现可增加培养的哺乳动物黑素细胞中的色素沉着。通过亲和色谱法确定细胞靶点为线粒体F1F0 - ATP合酶(ATP酶)。寡霉素是一种已知可抑制线粒体ATP酶的小分子,它在黑素细胞中与PPA竞争其细胞靶点。此外,PPA被证明可改变线粒体的膜电位,这与线粒体ATP酶的抑制作用一致。因此,PPA已成功用作正向化学遗传学方法中的化学探针,以建立表型与蛋白质之间的联系。结果证明了在斑马鱼中筛选小分子文库作为鉴定哺乳动物靶点的一种手段的有效性,并表明线粒体ATP酶是调节黑素细胞和黑色素瘤细胞色素沉着的一个靶点。

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