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首页> 外文期刊>Cell biochemistry and biophysics >Computational Identification of Pathogenic Associated nsSNPs and its Structural Impact in UROD Gene: A Molecular Dynamics Approach
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Computational Identification of Pathogenic Associated nsSNPs and its Structural Impact in UROD Gene: A Molecular Dynamics Approach

机译:致病性相关nsSNPs的计算鉴定及其在UROD基因中的结构影响:分子动力学方法

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Uroporphyrinogen decarboxylase is a cytosolic enzyme involved in the biosynthetic pathway of heme production. Decreased activity of this enzyme results in porphyria cutanea tarda and hepato erythropoietic porphyria. Nonsynonymous single nucleotide polymorphisms (nsSNPs) alter protein sequence and can cause disease. Identifying the deleterious nsSNPs that contribute to disease is an important task. We used five different in silico tools namely SIFT, PANTHER, PolyPhen2, SNPs&GO, and I-mutant3 to identify deleterious nsSNPs in UROD gene. Further, we used molecular dynamic (MD) approach to evaluate the impact of deleterious mutations on UROD protein structure. By comparing the results of all the five prediction results, we screened 35 (51.47 %) nsSNPs as highly deleterious. MD analysis results show that all the three L161Q, L282R, and I334T deleterious variants were affecting the UROD protein structural stability and flexibility. Our findings provide strong evidence on the effect of deleterious nsSNPs in UROD gene. A detailed MD study provides a new insight in the conformational changes occurred in the mutant structures of UROD protein.
机译:尿卟啉原脱羧酶是一种参与血红素产生生物合成途径的胞质酶。该酶的活性降低导致皮肤卟啉卟啉菌和肝红细胞生成性卟啉症。非同义的单核苷酸多态性(nsSNPs)会改变蛋白质序列,并可能导致疾病。鉴定导致疾病的有害nsSNP是一项重要任务。我们使用了五个不同的计算机软件工具,即SIFT,PANTHER,PolyPhen2,SNPs&GO和I-mutant3来鉴定UROD基因中有害的nsSNPs。此外,我们使用分子动力学(MD)方法来评估有害突变对UROD蛋白结构的影响。通过比较所有五个预测结果的结果,我们筛选出35种(51.47%)nsSNP具有高度有害性。 MD分析结果表明,所有三个L161Q,L282R和I334T有害变体均影响UROD蛋白的结构稳定性和柔韧性。我们的发现为UROD基因中有害的nsSNPs的作用提供了有力的证据。详细的MD研究为UROD蛋白突变结构中发生的构象变化提供了新的见解。

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