Polymorphisms in GLTSCR1 and ERCC2 are associated with the development of oligodendrogliomas

少突胶质瘤 ERCC2型 单核苷酸多态性 等位基因 单倍型 外显子 基因型 胶质瘤 杂合子丢失 遗传学 医学 SNP公司 生物 肿瘤科 基因 星形细胞瘤
作者
Ping Yang,Thomas M. Kollmeyer,Kristin Buckner,William R. Bamlet,Karla V. Ballman,Robert B. Jenkins
出处
期刊:Cancer [Wiley]
卷期号:103 (11): 2363-2372 被引量:65
标识
DOI:10.1002/cncr.21028
摘要

Abstract BACKGROUND Deletions of 19q have been associated with gliomas, especially oligodendrogliomas. In addition, cases with oligodendrogliomas with the 19q deletion have been observed to have a better survival compared with cases without the 19q deletion. The authors have previously described a 150‐kilobase minimal deletion region in gliomas that maps to 19q13.33 and contains 3 novel candidate genes ( GLTSCR1 , EHD2 , and GLTSCR2 ). METHODS The authors performed an association study using 141 cases with gliomas (61 cases with astrocytomas, 40 cases with oligodendrogliomas, 40 cases with mixed oligoastrocytomas) and 108 general controls. They evaluated 7 single nucleotide polymorphisms (SNPs) in 6 genes within and nearby the minimal 19q deletion region ( ERCC2 , RAI , ASE‐1 , ERCC1 , GLTSCR1 , and LIG1 ). RESULTS The prevalence of a germline GLTSCR1 ‐exon‐1 T allele (SNP rs1035938) was 40% in cases with oligodendrogliomas compared with 27% in controls ( P = 0.029), and the prevalence of an ERCC2‐exon‐22 T allele (SNP rs1052555) was 35% in cases with oligodendrogliomas compared with 18% in controls ( P = 0.043). One high‐risk and 1 low‐risk haplotype were associated with oligodendroglioma development ( P = 0.003 and 0.026, respectively). Cases with oligodendrogliomas with the 19q deletion had a significantly higher frequency of the GLTSCR1 ‐exon‐1 T allele compared with cases without the 19q deletion ( P = 0.01). It was noteworthy that cases with gliomas who were homozygous for the GLTSCR1 ‐exon‐1 T allele had a significantly better survival: 77% and 68% survival at 2 and 5 years compared with 56% and 34% for other genotypes ( P = 0.02, log‐rank test). Multivariable analysis identified grade, age, and the GLTSCR1 ‐exon‐1 and ERCC2‐exon‐22 genotypes as independent predictors for survival. CONCLUSIONS These results suggested that alterations in GLTSCR1 (or a closely linked gene) were associated with the development and progression of oligodendroglioma. Cancer 2005. © 2005 American Cancer Society.

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