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地中海贫血与疟疾:再探讨

Thalassaemia and malaria, revisited.

作者信息

Weatherall D J

机构信息

Institute of Molecular Medicine, University of Oxford, John Radcliffe Hospital, U.K. janet.watt%

出版信息

Ann Trop Med Parasitol. 1997 Oct;91(7):885-90. doi: 10.1080/00034989760653.

Abstract

Haldane's attractive hypothesis that the high gene frequencies for thalassaemia in the Mediterranean population may have resulted from heterozygote advantage in regions where Plasmodium falciparum malaria was common in the past has been extremely difficult to verify at the population or experimental level. However, the molecular era has provided some powerful new tools to attack this old problem. It is now clear that the thalassaemias are the commonest monogenic diseases in man, with a broad distribution throughout the Mediterranean, Middle East, Indian sub-continent and South-east Asia. All these populations have specific types of thalassaemia mutations which, presumably, have arisen locally and been expanded by selection together with drift and founder effect. Recent work indicates that alpha thalassaemia provides protection against severe malaria. Quite unexpectedly at least some of this protection may be mediated by rendering very young children more susceptible to both P. vivax and P. falciparum malaria; such early immunization may provide some protection against the disease in later life.

摘要

霍尔丹提出了一个颇具吸引力的假说,即地中海人群中高频率的地中海贫血基因可能源于过去恶性疟原虫疟疾常见地区的杂合子优势,但这一假说在人群或实验层面极难得到验证。然而,分子时代提供了一些强大的新工具来攻克这个老问题。现在很清楚,地中海贫血是人类最常见的单基因疾病,广泛分布于地中海、中东、印度次大陆和东南亚地区。所有这些人群都有特定类型的地中海贫血突变,据推测,这些突变是在当地产生的,并通过选择以及漂变和奠基者效应得以扩展。最近的研究表明,α地中海贫血能提供针对严重疟疾的保护。至少有一些保护作用可能是通过使幼儿更容易感染间日疟原虫和恶性疟原虫来介导的,这相当出人意料;这种早期免疫可能会在以后的生活中为预防该疾病提供一些保护。

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