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对人类黑色素瘤细胞中 POU3F2/BRN2 启动子占据的全基因组分析揭示 Kitl 是一个新的调控靶基因。

Genome-wide analysis of POU3F2/BRN2 promoter occupancy in human melanoma cells reveals Kitl as a novel regulated target gene.

机构信息

Institut de Génétique et de Biologie Moléculaire et Cellulaire, CNRS/INSERM/UDS, Illkirch Cédex, France.

出版信息

Pigment Cell Melanoma Res. 2010 Jun;23(3):404-18. doi: 10.1111/j.1755-148X.2010.00697.x. Epub 2010 Mar 17.

Abstract

POU3F2 is a POU-Homeodomain transcription factor expressed in neurons and melanoma cells. In melanoma lesions, cells expressing high levels of POU3F2 show enhanced invasive and metastatic capacity that can in part be explained by repression of Micropthalmia-associated Transcription Factor (MITF) expression via POU3F2 binding to its promoter. To identify other POU3F2 target genes that may be involved in modulating the properties of melanoma cells, we performed ChIP-chip experiments in 501Mel melanoma cells. 2108 binding loci located in the regulatory regions of 1700 potential target genes were identified. Bioinformatic and experimental assays showed the presence of known POU3F2-binding motifs, but also many AT-rich sequences with only partial similarity to the known motifs at the occupied loci. Functional analysis indicates that POU3F2 regulates the stem cell factor (Kit ligand, Kitl) promoter via a cluster of four closely spaced binding sites located in the proximal promoter. Our results suggest that POU3F2 may regulate the properties of melanoma cells via autocrine KIT ligand signalling.

摘要

POU3F2 是一种在神经元和黑色素瘤细胞中表达的 POU-Homeodomain 转录因子。在黑色素瘤病变中,表达高水平 POU3F2 的细胞表现出增强的侵袭和转移能力,这在一定程度上可以通过 POU3F2 结合其启动子来抑制小眼畸形相关转录因子(MITF)的表达来解释。为了鉴定其他可能参与调节黑色素瘤细胞特性的 POU3F2 靶基因,我们在 501Mel 黑色素瘤细胞中进行了 ChIP-chip 实验。鉴定出位于 1700 个潜在靶基因的调控区域的 2108 个结合位点。生物信息学和实验分析表明,在被占据的位点存在已知的 POU3F2 结合基序,但也存在许多与已知基序只有部分相似的富含 AT 的序列。功能分析表明,POU3F2 通过位于近端启动子中的四个紧密间隔的结合位点簇来调节干细胞因子(Kit 配体,Kitl)启动子。我们的结果表明,POU3F2 可能通过自分泌 KIT 配体信号来调节黑色素瘤细胞的特性。

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