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XPD – the lynchpin of NER: Molecule, Gene, Polymorphisms and role in Colorectal Carcinogenesis

机译:XPD – NER的关键:分子,基因,多态性及其在结直肠癌发生中的作用

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In mammals the bulky DNA adduct lesions known to result in deleterious phenotypes are acted upon and removed from the genomic DNA by nucleotide excision repair (NER) pathway. TFIIH multi-protein complex with its important helicase –Xeroderma Pigmentosum Protein (XPD) serves as the pivotal factor for opening up of the damaged lesion DNA site and carry out the repair process. The initial damage verification step of the TFIIH is in part dependent upon the helicase activity of XPD. Besides, XPD is also actively involved in the initiation steps of transcription and in the regulation of the cell cycle and apoptosis. In this review, we will be exploring the new insights in scientific research on the functioning of the NER pathway, the role of TFIIH as the central complex of NER, the pivotal helicase XPD as the lynchpin of NER and the effects of various single nucleotide polymorphisms (SNPs) of XPD oin its functioning and their consequent role in colorectal carcinogenesis.
机译:在哺乳动物中,已知导致有害表型的庞大的DNA加合物损伤通过核苷酸切除修复(NER)途径作用于基因组DNA并从基因组DNA中去除。 TFIIH多蛋白复合物及其重要的解旋酶–黑皮病色素蛋白(XPD)是打开受损病变DNA位点并进行修复过程的关键因素。 TFIIH的初始损坏验证步骤部分取决于XPD的解旋酶活性。此外,XPD还积极参与转录的起始步骤以及细胞周期和凋亡的调控。在这篇综述中,我们将探索有关NER途径的功能,TFIIH作为NER的中央复合体的作用,关键解旋酶XPD作为NER的关键基因以及各种单核苷酸多态性的影响的科学研究的新见解。 XPD(SNP)具有其功能及其在结直肠癌发生中的作用。

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