Department of Biological Sciences, Korea Advanced Institute of Science and Technology, Daejeon, South Korea.
Neoplasia. 2009 Dec;11(12):1340-7. doi: 10.1593/neo.91132.
PTPRCAP (CD45-AP) is a positive regulator of protein tyrosine phosphatase PTPRC (CD45), which activates Src family kinases implicated in tumorigenesis. Single-nucleotide polymorphism (SNP) rs869736 located at position -309 of the PTPRCAP promoter was associated with susceptibility to diffuse-type gastric cancer in the current case-control study. The minor-allele homozygote was significantly associated with a 2.5-fold increased susceptibility to diffuse-type gastric cancer (P = .0021, n = 252), but not to intestinal-type (P = .30, n = 178), versus the major-allele homozygote, when comparing unrelated Korean patients with healthy controls (n = 406). Nine other SNPs were in nearly perfect linkage disequilibrium (r(2) >or= 0.97) with this SNP, exhibiting the same association, and spread out for 26 kb on chromosome 11q13.1 covering RPS6KB2, PTPRCAP, CORO1B, and GPR152. Among the four genes, however, only PTPRCAP expression was affected by haplotypes of the 10 SNPs. Endogenous transcript levels of PTPRCAP were linearly correlated with copy numbers (0, 1, and 2) of the risk-haplotype (P = .0060) in 12 lymphoblastoid cells derived from blood samples, but those of the other three genes were not. Furthermore, the cancer-risk, minor-allele T of rs869736 increased both promoter activity and specific nuclear protein-binding affinity than the nonrisk, major-allele G in luciferase reporter and electrophoretic mobility shift assays, respectively. Accordingly, the minor allele of rs869736 in the PTPRCAP promoter is associated with increased susceptibility to diffuse-type gastric cancer by increasing PTPRCAP expression, possibly leading to activation of the oncogenic Src family kinases.
PTPRCAP(CD45-AP)是蛋白酪氨酸磷酸酶 PTPRC(CD45)的正调控因子,可激活与肿瘤发生相关的Src 家族激酶。当前病例对照研究发现,位于 PTPRCAP 启动子 -309 位的单核苷酸多态性(SNP)rs869736 与弥漫型胃癌易感性相关。与主要等位基因纯合子相比,次要等位基因纯合子与弥漫型胃癌的易感性增加 2.5 倍显著相关(P =.0021,n = 252),但与肠型(P =.30,n = 178)无关,在比较 406 例无关韩国患者与健康对照者(n = 406)时。该 SNP 附近还有另外 9 个 SNP 处于近乎完美的连锁不平衡(r(2) >or= 0.97),表现出相同的关联,并分布在 11q13.1 染色体上的 26 kb 范围内,覆盖 RPS6KB2、PTPRCAP、CORO1B 和 GPR152。然而,在这四个基因中,只有 PTPRCAP 的表达受 10 个 SNP 单倍型的影响。在从血液样本中获得的 12 个淋巴母细胞系中,PTPRCAP 的内源性转录水平与风险单倍型(rs869736)的拷贝数(0、1 和 2)呈线性相关(P =.0060),而其他三个基因则没有。此外,rs869736 的癌症风险、次要等位基因 T 在荧光素酶报告和电泳迁移率变动分析中,分别比非风险、主要等位基因 G 增加了启动子活性和特定核蛋白结合亲和力。因此,PTPRCAP 启动子中的 rs869736 等位基因通过增加 PTPRCAP 表达与弥漫型胃癌易感性增加相关,可能导致致癌性 Src 家族激酶的激活。