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人类蛋白质组中改变结构域的单核苷酸多态性及其对信号通路的影响。

Domain altering SNPs in the human proteome and their impact on signaling pathways.

机构信息

Center for Integrated Bioinformatics, Drexel University, Philadelphia, Pennsylvania, United States of America.

出版信息

PLoS One. 2010 Sep 23;5(9):e12890. doi: 10.1371/journal.pone.0012890.

Abstract

Single nucleotide polymorphisms (SNPs) constitute an important mode of genetic variations observed in the human genome. A small fraction of SNPs, about four thousand out of the ten million, has been associated with genetic disorders and complex diseases. The present study focuses on SNPs that fall on protein domains, 3D structures that facilitate connectivity of proteins in cell signaling and metabolic pathways. We scanned the human proteome using the PROSITE web tool and identified proteins with SNP containing domains. We showed that SNPs that fall on protein domains are highly statistically enriched among SNPs linked to hereditary disorders and complex diseases. Proteins whose domains are dramatically altered by the presence of an SNP are even more likely to be present among proteins linked to hereditary disorders. Proteins with domain-altering SNPs comprise highly connected nodes in cellular pathways such as the focal adhesion, the axon guidance pathway and the autoimmune disease pathways. Statistical enrichment of domain/motif signatures in interacting protein pairs indicates extensive loss of connectivity of cell signaling pathways due to domain-altering SNPs, potentially leading to hereditary disorders.

摘要

单核苷酸多态性(SNP)是人类基因组中观察到的重要遗传变异模式之一。大约有四千个 SNP 与遗传疾病和复杂疾病有关,而 SNP 只占人类基因组中一千万个 SNP 的一小部分。本研究关注的是位于蛋白质结构域上的 SNP,这些结构域是细胞信号转导和代谢途径中蛋白质连接的 3D 结构。我们使用 PROSITE 网络工具扫描了人类蛋白质组,识别出含有 SNP 结构域的蛋白质。我们发现,位于蛋白质结构域上的 SNP 在与遗传疾病和复杂疾病相关的 SNP 中高度富集。由于 SNP 的存在而导致结构域发生剧烈变化的蛋白质,甚至更有可能存在于与遗传疾病相关的蛋白质中。具有结构域改变 SNP 的蛋白质在细胞途径中构成高度连接的节点,如焦点粘连、轴突导向途径和自身免疫性疾病途径。相互作用蛋白对中结构域/基序特征的统计富集表明,由于结构域改变 SNP 的存在,细胞信号通路的连接广泛丢失,可能导致遗传疾病。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d062/2944825/ccf698251202/pone.0012890.g001.jpg

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