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In Silico Prediction of the Deleterious Effect of a Mutation: Proceed with Caution in Clinical Genetics

机译:在计算机模拟中预测突变的有害作用:在临床遗传学中应谨慎行事

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When a sequence variation is found in a candidate gene for a disease, it is important to establish whether this change is neutral or responsible for the observed disorders in a patient. To answer this question, in the absence of further experimental investigations, several simulation programs have been proposed to predict whether a nonsynonymous single-nucleotide polymorphism is likely to have or not have a deleterious effect on the phenotype. In this work, we tested two such programs, PolyPhen and SIFT, using two kinds of targets. The first ones concerned the products of the hemoglobin and glucose-6-phosphate dehydrogenase genes, which are abundantly documented. The second concerned two systems for which much less information is available: ( a ) the TNFRSF1A gene, implicated in tumor necrosis factor receptor-associated periodic syndrome, and ( b ) the MEFV gene, which is believed to be involved in familial Mediterranean fever. Our data suggest that, from a practical point of view, these programs should not be used to decide, in the absence of other tests or arguments, whether the sequence variation found in a patient is or is not responsible for the disease. The consequence of an erroneous prediction may be disastrous in the perspective of genetic counseling.
机译:当在疾病的候选基因中发现序列变异时,重要的是确定这种改变是中性的还是对患者中观察到的疾病负责。为了回答这个问题,在没有进一步的实验研究的情况下,已经提出了几种模拟程序来预测非同义的单核苷酸多态性是否可能对表型具有有害作用。在这项工作中,我们使用两种目标测试了两个这样的程序PolyPhen和SIFT。第一个涉及血红蛋白和葡萄糖-6-磷酸脱氢酶基因的产物,这些文献已被大量记载。第二个涉及两个系统,其可用信息少得多:(a)与肿瘤坏死因子受体相关的周期性综合征有关的TNFRSF1A基因,和(b)被认为与家族性地中海热有关的MEFV基因。我们的数据表明,从实际的角度来看,在没有其他测试或论据的情况下,不应使用这些程序来确定患者中发现的序列变异是否导致该疾病。从遗传咨询的角度来看,错误预测的后果可能是灾难性的。

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