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Genome‐wide association study of circulating folate one‐carbon metabolites

机译:循环叶酸单碳代谢物的基因组 - 宽协会研究

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摘要

Abstract Experimental, observational, and clinical trials support a critical role of folate one‐carbon metabolism (FOCM) in colorectal cancer (CRC) development. In this report, we focus on understanding the relationship between common genetic variants and metabolites of FOCM. We conducted a genome‐wide association study of FOCM biomarkers among 1,788 unaffected (without CRC) individuals of European ancestry from the Colon Cancer Family Registry. Twelve metabolites, including 5‐methyltetrahydrofolate, vitamin B 2 (flavin mononucleotide and riboflavin), vitamin B 6 (4‐pyridoxic acid, pyridoxal, and pyridoxamine), total homocysteine, methionine, S ‐adenosylmethionine, S ‐adenosylhomocysteine, cystathionine, and creatinine were measured from plasma using liquid chromatography‐mass spectrometry (LC‐MS) or LC‐MS/MS. For each individual biomarker, we estimated genotype array‐specific associations followed by a fixed‐effect meta‐analysis. We identified the variant rs35976024 (at 2p11.2 and intronic of ATOH8 ) associated with total homocysteine ( p = 4.9?×?10 ?8 ). We found a group of six highly correlated variants on chromosome 15q14 associated with cystathionine (all p ??5?×?10 ?8 ), with the most significant variant rs28391580 ( p = 2.8?×?10 ?8 ). Two variants (rs139435405 and rs149119426) on chromosome 14q13 showed significant ( p ??5?×?10 ?8 ) associations with S‐adenosylhomocysteine. These three biomarkers with significant associations are closely involved in homocysteine metabolism. Furthermore, when assessing the principal components (PCs) derived from seven individual biomarkers, we identified the variant rs12665366 (at 6p25.3 and intronic of EXOC2 ) associated with the first PC ( p = 2.3?×?10 ?8 ). Our data suggest that common genetic variants may play an important role in FOCM, particularly in homocysteine metabolism.
机译:摘要实验,观察和临床试验支持叶酸单碳代谢(FOCM)在结肠直肠癌(CRC)发育中的关键作用。在本报告中,我们专注于了解常见遗传变异与焦点代谢物之间的关系。我们在1,788年不受影响的基因组生物标志物中进行了一种基因组 - 群体生物标志物,从结肠癌家庭登记处欧洲祖先的欧洲血统的个人。 12种代谢物,包括5-甲基四氢脱落,维生素B 2(Flavin单核苷酸和核黄素),维生素B 6(4-吡吡氧基酸,吡哆醛和吡哆醛),总同型半胱氨酸,甲硫氨酸,S-淀粉酰甲基硫甲硫醚,S-andenylhomocysteine,胱硫脲和肌酐使用液相色谱 - 质谱(LC-MS)或LC-MS / MS从等离子体测量。对于每个生物标志物,我们估计了基因型阵列特异性关联,然后进行了固定效应元分析。我们鉴定了与总同型酮相关的variant rs35976024(在2p11.2和atoh8的内部inhorone)(p = 4.9?×10?8)。我们在与胱硫脲(所有Pααα×10?10?10)相关的染色体15Q14上发现了一组高度相关的变体(所有p?5?×10?8),具有最高的变体RS28391580(p = 2.8?×10?10)。染色体14Q13上的两个变体(RS139435405和RS149119426)显示出与S-腺瘤骨细胞的关联(p≤x≤5≤x≤10≤x≤10.×10〜10.)。这三个具有重要关联的生物标志物敏锐地参与同型胰岛素代谢。此外,当评估衍生自七个单独生物标志物的主要成分(PCS)时,我们识别与第一PC相关的变型RS12665366(在6p25.3和exoc2的内部)(p = 2.3?×10?10)。我们的数据表明,常见的遗传变异可能在焦点中发挥重要作用,特别是在同型半胱氨酸代谢中。

著录项

  • 来源
    《Genetic epidemiology.》 |2019年第8期|共16页
  • 作者单位

    Department of Preventive Medicine USC Norris Comprehensive Cancer Center Keck School of;

    Department of Clinical Pharmacy and Pharmaceutical Economics and Policy School of;

    Department of Medicine School of MedicineUniversity of North CarolinaChapel Hill North Carolina;

    Cedars‐Sinai Medical CenterSamuel Oschin Comprehensive Cancer InstituteLos Angeles California;

    Cedars‐Sinai Medical CenterSamuel Oschin Comprehensive Cancer InstituteLos Angeles California;

    Cedars‐Sinai Medical CenterSamuel Oschin Comprehensive Cancer InstituteLos Angeles California;

    Public Health Sciences DivisionFred Hutchinson Cancer Research CenterSeattle Washington;

    Public Health Sciences DivisionFred Hutchinson Cancer Research CenterSeattle Washington;

    Department of Population and Quantitative Health SciencesCase Western Reserve UniversityCleveland;

    Department of Clinical Pharmacy and Pharmaceutical Economics and Policy School of;

    Center for Public Health GenomicsUniversity of VirginiaCharlottesville Virginia;

    Department of Preventive Medicine USC Norris Comprehensive Cancer Center Keck School of;

  • 收录信息
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 流行病学与防疫;
  • 关键词

    colorectal cancer; epidemiology; folate; genome‐wide association analysis; one‐carbon metabolism;

    机译:结肠直肠癌;流行病学;叶酸;基因组关联分析;单碳代谢;

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