An Excess of G over C Nucleotides in Mutagenesis of Human Genetic Diseases

被引:0
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作者
Li Xiao
Wanping Sun
Jia Zhang
Yanping Zhou
Linling Chen
Hanlin Gao
Pierre Sirois
Kai Li
机构
[1] Soochow University,Department of Molecular Diagnostics, College of Pharmacy
[2] The Second Affiliated Hospital of Soochow University,Department of Molecular Medicine Center
[3] Genomics Institute of the Novartis Research Foundation,Department of Molecular Diagnostics
[4] City of Hope National Medical Center,CHUL Research Center
[5] Laval University,undefined
来源
Molecular Biotechnology | 2011年 / 48卷
关键词
Genetic disease; Mutagenesis; Single nucleotide substitution; Strand bias; Factor IX;
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摘要
Strand asymmetries in DNA evolution, including indel and single nucleotide substitutions, were reported in prokaryotes. Recently, an excess of G>A over C>T substitutions in hemophilia B patients was recognized in our molecular diagnostic practices. Further analysis demonstrated biased point mutations between sense and antisense strands when unique changes in factor IX were counted. Similar mutation spectra of factor IX and the HGMD prompted us to speculate that the excess of G>A over C>T may be present in genes other than factor IX. Data from nine genes (each has ≥100 missense mutations) retrieved from HGMD, international factor IX database, and Dr. Sommer’s lab database in the City of Hope National Medical Center, Duarte, CA, USA were analyzed for their point mutation spectra. Similar to factor IX, all genes selected in this study have biased G>A over C>T unique mutations when nonsense mutations were excluded. The biased missense point mutations were recently convincingly documented by the statistic data of categorized missense mutation in HGMD. The consistence of the genetic observation and the genomic data from HGMD strongly indicate that biased point mutations, possibly a phenotypic selection, are more widespread than previously thought. The biased mutations have immediate clinical impact in molecular diagnostics.
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页码:1 / 6
页数:5
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