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ABO糖基转移酶的常见变异与严重恶性疟原虫疟疾的易感性相关。

Common variation in the ABO glycosyltransferase is associated with susceptibility to severe Plasmodium falciparum malaria.

作者信息

Fry Andrew E, Griffiths Michael J, Auburn Sarah, Diakite Mahamadou, Forton Julian T, Green Angela, Richardson Anna, Wilson Jonathan, Jallow Muminatou, Sisay-Joof Fatou, Pinder Margaret, Peshu Norbert, Williams Thomas N, Marsh Kevin, Molyneux Malcolm E, Taylor Terrie E, Rockett Kirk A, Kwiatkowski Dominic P

机构信息

The Wellcome Trust Centre for Human Genetics, Roosevelt Drive, Oxford OX3 7BN, UK.

出版信息

Hum Mol Genet. 2008 Feb 15;17(4):567-76. doi: 10.1093/hmg/ddm331. Epub 2007 Nov 13.

Abstract

There is growing epidemiological and molecular evidence that ABO blood group affects host susceptibility to severe Plasmodium falciparum infection. The high frequency of common ABO alleles means that even modest differences in susceptibility could have a significant impact on the health of people living in malaria endemic regions. We performed an association study, the first to utilize key molecular genetic variation underlying the ABO system, genotyping >9000 individuals across three African populations. Using population- and family-based tests, we demonstrated that alleles producing functional ABO enzymes are associated with greater risk of severe malaria phenotypes (particularly malarial anemia) in comparison with the frameshift deletion underlying blood group O: case-control allelic odds ratio (OR), 1.2; 95% confidence interval (CI), 1.09-1.32; P = 0.0003; family-studies allelic OR, 1.19; 95% CI, 1.08-1.32; P = 0.001; pooled across all studies allelic OR, 1.18; 95% CI, 1.11-1.26; P = 2 x 10(-7). We found suggestive evidence of a parent-of-origin effect at the ABO locus by analyzing the family trios. Non-O haplotypes inherited from mothers, but not fathers, are significantly associated with severe malaria (likelihood ratio test of Weinberg, P = 0.046). Finally, we used HapMap data to demonstrate a region of low F(ST) (-0.001) between the three main HapMap population groups across the ABO locus, an outlier in the empirical distribution of F(ST) across chromosome 9 (approximately 99.5-99.9th centile). This low F(ST) region may be a signal of long-standing balancing selection at the ABO locus, caused by multiple infectious pathogens including P. falciparum.

摘要

越来越多的流行病学和分子证据表明,ABO血型会影响宿主对恶性疟原虫严重感染的易感性。常见ABO等位基因的高频率意味着,即使易感性存在适度差异,也可能对生活在疟疾流行地区的人们的健康产生重大影响。我们开展了一项关联研究,这是首次利用ABO系统潜在的关键分子遗传变异,对三个非洲人群中的9000多名个体进行基因分型。通过基于人群和家系的检测,我们证明,与O型血所基于的移码缺失相比,产生功能性ABO酶的等位基因与严重疟疾表型(尤其是疟疾贫血)的风险更高相关:病例对照等位基因优势比(OR)为1.2;95%置信区间(CI)为1.09 - 1.32;P = 0.0003;家系研究等位基因OR为1.19;9%置信区间为1.08 - 1.32;P = 0.001;所有研究汇总后的等位基因OR为1.18;95%置信区间为1.11 - 1.26;P = 2×10⁻⁷。通过分析家系三联体,我们发现了ABO基因座存在亲本来源效应的提示性证据。从母亲而非父亲遗传的非O单倍型与严重疟疾显著相关(温伯格似然比检验,P = 0.046)。最后,我们利用HapMap数据证明,在ABO基因座上,三个主要HapMap人群组之间存在一个低F(ST)区域(-0.001),这是9号染色体上F(ST)经验分布中的一个异常值(约第99.5 - 99.9百分位数)。这个低F(ST)区域可能是ABO基因座长期平衡选择的信号,是由包括恶性疟原虫在内的多种感染性病原体引起的。

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