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ABO blood groups and pancreatic cancer risk and survival: results from the PANcreatic Disease ReseArch (PANDoRA) consortium.

机译:ABO血型和胰腺癌的风险与生存:胰腺疾病研究小组(PANDoRA)联盟的结果。

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摘要

There is strong epidemiologic evidence indicating that common genetic variability could be implicated in pancreatic cancer risk and, to date, various loci have been proposed. In particular, there is increasing evidence of the involvement of ABO gene variability and pancreatic cancer risk. In a large multicentric study of 1,028 pancreatic ductal adenocarcinoma cases and 2,257 controls in the context of the PANcreatic Disease ReseArch (PANDoRA) consortium, we investigated the suggested association with increased risk for carriers of single nucleotide polymorphisms (SNPs) determining the A or B allele in comparison with the O allele, which encodes for a non-functional enzyme. Since glycosyltransferase activity, encoded by ABO, is higher for the A1 variant compared with the A2 variant, we investigated the hypothesis that A1 carriers were at an increased risk of pancreatic cancer. In our analysis, carriers of the A1 were indeed at greater risk of developing the disease. In addition, we investigated the possible influence that genetic variability at the ABO locus may have in pancreatic cancer survival, but we observed no effect in our population.
机译:有强大的流行病学证据表明,常见的遗传变异可能与胰腺癌的风险有关,迄今为止,已经提出了多种基因座。特别是,越来越多的证据表明ABO基因变异与胰腺癌风险有关。在一项针对胰腺癌ReseArch(PANDoRA)财团的1,028例胰管腺癌病例和2,257例对照的大型多中心研究中,我们调查了与确定A或B等位基因的单核苷酸多态性(SNP)携带者的风险增加之间的相关性。与编码非功能性酶的O等位基因相比。由于A1变体比A2变体由ABO编码的糖基转移酶活性更高,因此我们研究了A1携带者罹患胰腺癌的风险增加的假设。在我们的分析中,A1携带者确实有更大的患病风险。此外,我们调查了ABO位点的遗传变异性可能对胰腺癌存活的影响,但未观察到对人群的影响。

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