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How to use an article about genetic association: B: Are the results of the study valid?

机译:如何使用有关遗传关联的文章:B:研究结果是否有效?

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In the first article of this series, we reviewed the basic genetics concepts necessary to understand genetic association studies. In this second article, we enumerate the major issues in judging the validity of these studies, framed as critical appraisal questions. Was the disease phenotype properly defined and accurately recorded by someone blind to the genetic information? Have any potential differences between disease and nondisease groups, particularly ethnicity, been properly addressed? In genetic studies, one potential cause of spurious associations is differences between cases and controls in ethnicity, a situation termed population stratification. Was measurement of the genetic variants unbiased and accurate? Methods for determining DNA sequence variation are not perfect and may have some measurement error. Do the genotype proportions observe Hardy-Weinberg equilibrium? This simple mathematic rule about the distribution of genetic groups may be one way to check for errors in reading DNA information. Have the investigators adjusted their inferences for multiple comparisons? Given the thousands of genetic markers tested in genome-wide association studies, the potential for false-positive and false-negative results is much higher than in traditional medical studies, and it is particularly important to look for replication of results.
机译:在本系列的第一篇文章中,我们回顾了理解遗传关联研究所必需的基本遗传学概念。在第二篇文章中,我们列举了评判这些研究有效性的主要问题,这些问题被视为关键的评估问题。对遗传信息不了解的人是否正确定义并准确记录了疾病表型?疾病和非疾病人群之间,尤其是种族之间的潜在差异是否得到适当解决?在遗传学研究中,造成虚假关联的一个潜在原因是病例与对照种族之间的差异,这种情况被称为人口分层。遗传变异的测量是否公正且准确?确定DNA序列变异的方法并不完美,可能会有一些测量误差。基因型比例是否遵守Hardy-Weinberg平衡?关于遗传基团分布的简单数学规则可能是检查读取DNA信息错误的一种方法。研究者是否已针对多个比较调整其推论?鉴于在全基因组关联研究中测试了成千上万种遗传标记,因此假阳性和假阴性结果的潜力远高于传统医学研究,寻找结果的重复尤为重要。

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