Guo Wei, Zhou Rong Miao, Wan Ling Ling, Wang Na, Li Yan, Zhang Xiao Juan, Dong Xiu Juan
Hebei Cancer Institute, The Fourth Hospital of Hebei Medical University, Jiankanglu 12, 050011 Shijiazhuang, Hebei, China.
J Cancer Res Clin Oncol. 2008 Feb;134(2):263-70. doi: 10.1007/s00432-007-0283-0. Epub 2007 Jul 26.
Inherited polymorphisms of DNA repair genes may contribute to variations in DNA repair capacity (DRC) and genetic susceptibility to different cancers. The aim of this study was to determine whether single nucleotide polymorphisms (SNPs) of xeroderma pigmentosum group A (XPA) and XPC can influence the risk of esophageal squamous cell carcinoma (ESCC).
In this report, one SNP of XPA and three SNPs of XPC were genotyped by polymerase-chain reaction (PCR) and PCR-restriction fragment length polymorphism (PCR-RFLP) assay in 327 ESCC patients and 612 healthy controls in a high incidence region of North China.
Family history of upper gastrointestinal cancers (UGIC) may increase the risk of developing ESCC. The overall genotype and allelotype distributions of XPA A23G in ESCC patients were significantly different from that in healthy controls (P < 0.05). The A/G + G/G genotype significantly decreased the risk of developing ESCC compared with A/A genotype. When stratified for family history of UGIC, compared with A/A genotype, A/G + G/G genotype significantly decreased the risk of ESCC in groups with negative history of UGIC. The overall genotype and allelotype distributions of XPC intron 9 PAT(+/-) and exon 15 Lys939Gln and exon 8 Val499Ala in ESCC patients were not significantly different from that in healthy controls (P > 0.05). When stratified for smoking status and UGIC family history, compared with A/A genotype, C/C genotype of exon 15 Lys939Gln significantly increased the risk of developing ESCC in non-smoker group.
We concluded that XPA23 polymorphism may be useful markers for identifying individuals at risk of developing ESCC. C/C genotype of XPC exon 15 may be one of the factors that affect the risk of developing ESCC in nonsmoking population in the high incidence region of China.
DNA修复基因的遗传性多态性可能导致DNA修复能力(DRC)的差异以及对不同癌症的遗传易感性。本研究的目的是确定A型着色性干皮病(XPA)和XPC的单核苷酸多态性(SNP)是否会影响食管鳞状细胞癌(ESCC)的风险。
在本报告中,采用聚合酶链反应(PCR)和PCR-限制性片段长度多态性(PCR-RFLP)分析对中国北方高发地区的327例ESCC患者和612例健康对照进行XPA的一个SNP和XPC的三个SNP基因分型。
上消化道癌(UGIC)家族史可能增加患ESCC的风险。ESCC患者中XPA A23G的总体基因型和等位基因分布与健康对照者显著不同(P<0.05)。与A/A基因型相比,A/G+G/G基因型显著降低了患ESCC的风险。按UGIC家族史分层时,与A/A基因型相比,A/G+G/G基因型在UGIC家族史阴性组中显著降低了ESCC的风险。ESCC患者中XPC内含子9 PAT(+/-)、外显子15 Lys939Gln和外显子8 Val499Ala的总体基因型和等位基因分布与健康对照者无显著差异(P>0.05)。按吸烟状况和UGIC家族史分层时,与A/A基因型相比,外显子15 Lys939Gln的C/C基因型在非吸烟组中显著增加了患ESCC的风险。
我们得出结论,XPA23多态性可能是识别ESCC发病风险个体的有用标志物。XPC外显子15的C/C基因型可能是影响中国高发地区非吸烟人群ESCC发病风险的因素之一。
