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上位性与β地中海贫血表型筛选的敏感性

Epistasis and the sensitivity of phenotypic screens for beta thalassaemia.

作者信息

Penman Bridget S, Gupta Sunetra, Weatherall David J

机构信息

Department of Zoology, University of Oxford, Oxford, UK.

出版信息

Br J Haematol. 2015 Apr;169(1):117-28. doi: 10.1111/bjh.13241. Epub 2014 Dec 17.

Abstract

Genetic disorders of haemoglobin, particularly the sickle cell diseases and the alpha and beta thalassaemias, are the commonest inherited disorders worldwide. The majority of affected births occur in low-income and lower-middle income countries. Screening programmes are a vital tool to counter these haemoglobinopathies by: (i) identifying individual carriers and allowing them to make informed reproductive choices, and (ii) generating population level gene-frequency estimates, to help ensure the optimal allocation of public health resources. For both of these functions it is vital that the screen performed is suitably sensitive. One popular first-stage screening option to detect carriers of beta thalassaemia in low-income countries is the One Tube Osmotic Fragility Test (OTOFT). Here we introduce a population genetic framework within which to quantify the likely sensitivity and specificity of the OTOFT in different epidemiological contexts. We demonstrate that interactions between the carrier states for beta thalassaemia and alpha thalassaemia, glucose-6-phosphate dehydrogenase deficiency and Southeast Asian Ovalocytosis have the potential to reduce the sensitivity of OTOFTs for beta thalassaemia heterozygosity to below 70%. Our results therefore caution against the widespread application of OTOFTs in regions where these erythrocyte variants co-occur.

摘要

血红蛋白的遗传性疾病,尤其是镰状细胞病以及α和β地中海贫血,是全球最常见的遗传性疾病。大多数受影响的新生儿出生在低收入和中低收入国家。筛查项目是对抗这些血红蛋白病的重要工具,其作用包括:(i)识别个体携带者并让他们做出明智的生育选择,以及(ii)生成人群层面的基因频率估计值,以帮助确保公共卫生资源的优化分配。对于这两项功能而言,所进行的筛查具有适当的敏感性至关重要。在低收入国家,一种用于检测β地中海贫血携带者的常见一级筛查方法是单管渗透脆性试验(OTOFT)。在此,我们引入一个群体遗传框架,用于量化OTOFT在不同流行病学背景下可能的敏感性和特异性。我们证明,β地中海贫血与α地中海贫血、葡萄糖-6-磷酸脱氢酶缺乏症以及东南亚椭圆形红细胞增多症的携带者状态之间的相互作用,有可能将OTOFT检测β地中海贫血杂合性的敏感性降低至70%以下。因此,我们的结果提醒人们,在这些红细胞变异同时出现的地区,不要广泛应用OTOFT。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/aff3/4383351/b986933c1fc2/bjh0169-0117-f1.jpg

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