| Article ID | Journal | Published Year | Pages | File Type |
|---|---|---|---|---|
| 8645310 | Gene | 2018 | 7 Pages |
Abstract
Non-homologous end joining (NHEJ) pathway has pivotal role in repair of double-strand DNA breaks that may lead to carcinogenesis. XRCC4 is one of the essential proteins of this pathway and single-nucleotide polymorphisms (SNPs) of this gene are reported to be associated with cancer risks. In our study, we first used computational approaches to predict the damaging variants of XRCC4 gene. Tools predicted rs79561451 (S110P) nsSNP as the most deleterious SNP. Along with this SNP, we analysed other two SNPs (rs3734091 and rs6869366) to study their association with breast cancer in population of West India. Variant rs3734091 was found to be significantly associated with breast cancer while rs6869366 variant did not show any association. These SNPs may influence the susceptibility of individuals to breast cancer in this population.
Keywords
Psicamplification-refractory mutation systemSIFTDDGSNPsNon-synonymous single nucleotide polymorphismsNCBIPDBNHEJHMMHWEBERARMSnsSNPsProtein ANalysis THrough Evolutionary RelationshipsDNA repairHardy–Weinberg equilibriumbase excision repairGibbs free energy changeBreast cancerReliability indexnon-homologous end-joiningconfidence intervalpolymorphism phenotypingHidden Markov modelSorting Intolerant From Tolerantodds ratioVariantPANTHERProtein Data BankPolyPhenSingle nucleotide polymorphisms
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Authors
Preety K. Singh, Kinnari N. Mistry, Haritha Chiramana, Dharamshi N. Rank, Chaitanya G. Joshi,