Computational and Structural Investigation of Deleterious Functional SNPs in Breast Cancer BRCA2 Gene 被引量：1

Computational and Structural Investigation of Deleterious Functional SNPs in Breast Cancer BRCA2 Gene

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摘要 In this work, we have analyzed the genetic variation that can alter the expression and the function in BRCA2 gene using computational methods. Out of the total 534 SNPs, 101 were found to be non synonymous (nsSNPs). Among the 7 SNPs in the untranslated region, 3 SNPs were found in 5′ and 4 SNPs were found in 3′ un-translated regions (UTR). Of the nsSNPs 20.7% were found to be damaging by both SIFT and PolyPhen server among the 101 nsSNPs investigated. UTR resource tool suggested that 2 SNPs in the 5′ UTR region and 4 SNPs in the 3′ UTR regions might change the protein expression levels. The mutation from asparagine to isoleucine at the position 3124 of the native protein of BRCA2 gene was most deleterious by both SIFT and PolyPhen servers. A structural analysis of this mutated protein and the native protein was made which had an RMSD value of 0.301 nm. Based on this work, we proposed that this most deleterious nsSNP with an SNPid rs28897759 is an important candidate for the cause of breast cancer by BRCA2 gene. In this work, we have analyzed the genetic variation that can alter the expression and the function in BRCA2 gene using computational methods. Out of the total 534 SNPs, 101 were found to be non synonymous （nsSNPs）. Among the 7 SNPs in the untranslated region, 3 SNPs were found in 5＇ and 4 SNPs were found in 3＇ un-translated regions （UTR）. Of the nsSNPs 20.7% were found to be damaging by both SIFT and PolyPben server among the 101 nsSNPs investigated. UTR resource tool suggested that 2 SNPs in the 5＇ UTR region and 4 SNPs in the 3＇ UTR regions might change the protein expression levels. The mutation from asparagine to isoleucine at the position 3124 of the native protein of BRCA2 gene was most deleterious by both SIFT and PolyPhen servers. A structural analysis of this mutated protein and the native protein was made which had an RMSD value of 0.301 nm. Based on this work, we proposed that this most deleterious nsSNP with an SNPid rs28897759 is an important candidate for the cause of breast cancer by BRCA2 gene.

作者 Rajasekaran R George Priya Doss Sudandiradoss C Ramanathan K Rituraj Purohit Rao Sethumadhavan

机构地区 School of Biotechnology

出处《生物工程学报》 CAS CSCD 北大核心 2008年第5期851-856,共6页 Chinese Journal of Biotechnology

关键词乳癌治疗方法临床分析基因 <i>BRCA2</i> gene breast cancer SIFT PolyPhen UTRscan modeled structure

分类号 R737.9 [医药卫生—肿瘤]

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Computational and Structural Investigation of Deleterious Functional SNPs in Breast Cancer BRCA2 Gene 被引量：1

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