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首页> 外文期刊>Interdisciplinary Sciences: Computational Life Sciences >In silico Prediction of Structure and Functions for Some Proteins of Male-Specific Region of the Human Y Chromosome
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In silico Prediction of Structure and Functions for Some Proteins of Male-Specific Region of the Human Y Chromosome

机译:在计算机上预测人Y染色体男性特定区域某些蛋白质的结构和功能

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摘要

Male-specific region of the human Y chromosome (MSY) comprises 95% of its length that is functionally active. This portion inherits in block from father to male offspring. Most of the genes in the MSY region are involved in male-specific function, such as sex determination and spermatogenesis; also contains genes probably involved in other cellular functions. However, a detailed characterization of numerous MSY-encoded proteins still remains to be done. In this study, 12 uncharacterized proteins of MSY were analyzed through bioinformatics tools for structural and functional characterization. Within these 12 proteins, a total of 55 domains were found, with DnaJ domain signature corresponding to be the highest (11%) followed by both FAD-dependent pyridine nucleotide reductase signature and fumarate lyase superfamily signature (9%). The 3D structures of our selected proteins were built up using homology modeling and the protein threading approaches. These predicted structures confirmed in detail the stereochemistry; indicating reasonably good quality model. Furthermore the predicted functions and the proteins with whom they interact established their biological role and their mechanism of action at molecular level. The results of these structure-functional annotations provide a comprehensive view of the proteins encoded by MSY, which sheds light on their biological functions and molecular mechanisms. The data presented in this study may assist in future prognosis of several human diseases such as Turner syndrome, gonadal sex reversal, spermatogenic failure, and gonadoblastoma.
机译:人Y染色体(MSY)的男性特定区域占其功能性活动长度的95%。从父亲到雄性后代,这部分都是遗传性的。 MSY区域中的大多数基因都与男性特定的功能有关,例如性别决定和精子发生;也包含可能参与其他细胞功能的基因。但是,许多MSY编码蛋白的详细表征仍有待完成。在这项研究中,通过生物信息学工具分析了MSY的12种未表征蛋白,以进行结构和功能表征。在这12种蛋白质中,共发现55个结构域,其中DnaJ结构域签名最高(11%),然后是FAD依赖性吡啶核苷酸还原酶签名和富马酸裂合酶超家族签名(9%)。我们选择的蛋白质的3D结构是使用同源性建模和蛋白质穿线方法构建的。这些预测的结构详细证实了立体化学。表示质量模型相当合理。此外,预测的功能以及与之相互作用的蛋白质在分子水平上确立了其生物学作用和作用机理。这些结构功能注释的结果提供了由MSY编码的蛋白质的全面视图,从而阐明了其生物学功能和分子机理。这项研究中提供的数据可能有助于某些人类疾病的未来预后,例如特纳综合征,性腺性逆转,生精功能衰竭和性腺母细胞瘤。

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