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Identification of Potential Drug Targets Implicated in Parkinsons Disease from Human Genome: Insights of Using Fused Domains in Hypothetical Proteins as Probes

机译:从人类基因组中确定与帕金森氏病有关的潜在药物靶标的鉴定:在假设蛋白中使用融合域作为探针的见解

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摘要

High-throughput genome sequencing has led to data explosion in sequence databanks, with an imbalance of sequence-structure-function relationships, resulting in a substantial fraction of proteins known as hypothetical proteins. Functions of such proteins can be assigned based on the analysis and characterization of the domains that they are made up of. Domains are basic evolutionary units of proteins and most proteins contain multiple domains. A subset of multidomain proteins is fused domains (overlapping domains), wherein sequence overlaps between two or more domains occur. These fused domains are a result of gene fusion events and their implication in diseases is well established. Hence, an attempt has been made in this paper to identify the fused domain containing hypothetical proteins from human genome homologous to parkinsonian targets present in KEGG database. The results of this research identified 18 hypothetical proteins, with domains fused with ubiquitin domains and having homology with targets present in parkinsonian pathway.
机译:高通量基因组测序已导致序列数据库中的数据爆炸,并且序列结构与功能之间的关系不平衡,从而导致相当大一部分蛋白质被称为假设蛋白质。可以基于对组成它们的结构域的分析和表征来分配这些蛋白的功能。域是蛋白质的基本进化单位,大多数蛋白质包含多个域。多结构域蛋白的一个子集是融合结构域(重叠结构域),其中两个或多个结构域之间发生序列重叠。这些融合结构域是基因融合事件的结果,它们在疾病中的含义已得到充分证实。因此,本文已尝试从人基因组中鉴定与KEGG数据库中存在的帕金森靶标同源的假设蛋白质的融合域。这项研究的结果确定了18种假设蛋白,这些蛋白的结构域与泛素结构域融合,并且与帕金森病途径中存在的靶标具有同源性。

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