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The proteomic investigation reveals interaction of mdig protein with the machinery of DNA double-strand break repair

机译:蛋白质组学研究揭示了mdig蛋白与DNA双链断裂修复机制的相互作用

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摘要

To investigate how mineral dust-induced gene (mdig, also named as mina53, MINA, or NO52) promotes carcinogenesis through inducing active chromatin, we performed proteomics analyses for the interacting proteins that were co-immunoprecipitated by anti-mdig antibody from either the lung cancer cell line A549 cells or the human bronchial epithelial cell line BEAS-2B cells. On SDS-PAGE gels, three to five unique protein bands were consistently observed in the complexes pulled-down by mdig antibody, but not the control IgG. In addition to the mdig protein, several DNA repair or chromatin binding proteins, including XRCC5, XRCC6, RBBP4, CBX8, PRMT5, and TDRD, were identified in the complexes by the proteomics analyses using both Orbitrap Fusion and Orbitrap XL nanoESI-MS/MS in four independent experiments. The interaction of mdig with some of these proteins was further validated by co-immunoprecipitation using antibodies against mdig and its partner proteins, respectively. These data, thus, provide evidence suggesting that mdig accomplishes its functions on chromatin, DNA repair and cell growth through interacting with the partner proteins.
机译:为了研究矿物质粉尘诱导基因(mdig,也称为mina53,MINA或NO52)如何通过诱导活性染色质促进癌变,我们对蛋白质相互作用的蛋白质组学进行了蛋白质组学分析,所述相互作用的蛋白被来自任一肺部的抗mdig抗体共同免疫沉淀癌细胞系A549细胞或人支气管上皮细胞系BEAS-2B细胞。在SDS-PAGE凝胶上,在通过mdig抗体而非对照IgG下拉的复合物中始终观察到三到五个独特的蛋白带。使用Orbitrap Fusion和Orbitrap XL nanoESI-MS / MS通过蛋白质组学分析,在复合物中鉴定了除mdig蛋白外的几种DNA修复或染色质结合蛋白,包括XRCC5,XRCC6,RBBP4,CBX8,PRMT5和TDRD。在四个独立的实验中通过分别使用针对mdig的抗体及其伴侣蛋白的共免疫沉淀,进一步验证了mdig与其中一些蛋白质的相互作用。因此,这些数据提供了证据,表明mdig通过与伴侣蛋白相互作用来完成其对染色质,DNA修复和细胞生长的功能。

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