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首页> 外文期刊>International Journal of Cancer =: Journal International du Cancer >Do founder mutations characteristic of some cancer sites also predispose to pancreatic cancer?
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Do founder mutations characteristic of some cancer sites also predispose to pancreatic cancer?

机译:创始人突变是否有一些癌症遗址的特征也易于胰腺癌?

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摘要

Understanding of the etiology and risk of pancreatic cancer (PaCa) is still poorly understood. This study evaluated the prevalence of 10 Polish founder mutations in four genes among PaCa patients and assessed their possible association with the risk of disease in Poland. In the study 383 PaCa patients and 4,000 control subjects were genotyped for founder mutations in: BRCA1 (5382insC, 4153de1A, C61G), CHEK2 (1100delC, IVS2 + IG>A, de15395, I157T), NBS1 (657de15) and PALB2 (509 510delGA, 172 175delTTGT). A statistically significant association between the 657de15 mutation and an increased risk of pancreatic cancer was observed for N851 gene. The Slavic N8S1 gene mutation (657delACAAA) was detected in 8 of 383 (2.09%) unselected cases compared with 22 of 4,000 (0.55%) controls (OR: 3.80, p = 0.002). The PALB2 509 510delGA and 172 175delTTGT mutations combined were seen in 2 (0.52%) unselected cases of PaCa and in 8 (0.20%) of 4,000 controls (OR: 2.61, p = 0.49). For BRCA1, the three mutations combined were detected in 4 of 383 (1.04%) PaCa patients and in 17 of 4,000 (0.42%) controls (OR: 2.46, p = 0.20). CHEK2 mutations were not associated with the risk of pancreatic cancer (OR: 1.11, p = 0.72). The founder mutation in NB51 (657del5) was associated with an increased risk of PaCa in heterozygous carriers, indicating that this mutation appears to predispose to cancer of the pancreas. By identifying pancreatic cancer risk groups, founder mutation testing in Poland should be considered for people at risk for PaCa.
机译:理解胰腺癌(PACA)的病因和风险仍然很差。本研究评估了PACA患者中四种基因中的10种波兰创始人突变的患病率,并评估了波兰疾病风险的可能性。在该研究中,Paca患者和4,000名对照受试者进行了基因分型:BRCA1(5382辛,4153DE1A,C61G),CheK2(1100DelC,IVS2 + Ig> A,DE15395,I157T),NBS1(657DE15)和PALB2(509 510delga ,172 175delttgt)。对于N851基因,观察到657DE15突变与胰腺癌的风险增加之间的统计学意义。在383(2.09%)未选择的病例中检测到血浆N8S1基因突变(657DELACAA),与22例为4,000(0.55%)对照(或:3.80,P = 0.002)。 PALB2 509 510Delga和172175ddelttgt突变在PACA的2(0.52%)未选择的情况下组合,8(0.20%)4,000对照(或:2.61,P = 0.49)。对于BRCA1,组合的三种突变在383名(1.04%)PACA患者中检测到,其中17例(0.42%)对照(或:2.46,P = 0.20)。 Chek2突变与胰腺癌的风险无关(或:1.11,p = 0.72)。 NB51(657del5)中的创始人突变与杂合载体中PACA的风险增加有关,表明该突变似乎易于胰腺癌。通过鉴定胰腺癌风险群体,波兰的创始人突变检测应考虑有冒险的人对PACA的风险。

著录项

  • 来源
  • 作者单位

    Pomeranian Med Univ Int Hereditary Canc Ctr Dept Genet &

    Pathol Polabska 4 PL-70115 Szczecin;

    Univ Newcastle Fac Hlth Sch Biomed Sci Discipline Med Genet Callaghan NSW 2308 Australia;

    Pomeranian Med Univ Int Hereditary Canc Ctr Dept Genet &

    Pathol Polabska 4 PL-70115 Szczecin;

    Pomeranian Med Univ Int Hereditary Canc Ctr Dept Genet &

    Pathol Polabska 4 PL-70115 Szczecin;

    Pomeranian Med Univ Int Hereditary Canc Ctr Dept Genet &

    Pathol Polabska 4 PL-70115 Szczecin;

    Minist Internal Affairs &

    Adm Div Heath Care Lab Endoscopy Jagiellonska 44 PL-70382 Szczecin;

    Pomeranian Med Univ Int Hereditary Canc Ctr Dept Genet &

    Pathol Polabska 4 PL-70115 Szczecin;

    Pomeranian Med Univ Int Hereditary Canc Ctr Dept Genet &

    Pathol Polabska 4 PL-70115 Szczecin;

    Pomeranian Med Univ Dept Gen &

    Oncol Surg Al Powstancow Wlkp 72 PL-70111 Szczecin Poland;

    Pomeranian Med Univ Int Hereditary Canc Ctr Dept Genet &

    Pathol Polabska 4 PL-70115 Szczecin;

    Pomeranian Med Univ Int Hereditary Canc Ctr Dept Genet &

    Pathol Polabska 4 PL-70115 Szczecin;

    Pomeranian Med Univ Int Hereditary Canc Ctr Dept Genet &

    Pathol Polabska 4 PL-70115 Szczecin;

    Pomeranian Med Univ Int Hereditary Canc Ctr Dept Genet &

    Pathol Polabska 4 PL-70115 Szczecin;

  • 收录信息
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 肿瘤学;
  • 关键词

    pancreatic cancer; founder mutations; NBS1 gene; cancer risk;

    机译:胰腺癌;创始人突变;NBS1基因;癌症风险;

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