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一种与库鲁病暴露共定位的新型保护性朊病毒蛋白变体。

A novel protective prion protein variant that colocalizes with kuru exposure.

作者信息

Mead Simon, Whitfield Jerome, Poulter Mark, Shah Paresh, Uphill James, Campbell Tracy, Al-Dujaily Huda, Hummerich Holger, Beck Jon, Mein Charles A, Verzilli Claudio, Whittaker John, Alpers Michael P, Collinge John

机构信息

Medical Research Council Prion Unit, Department of Neurodegenerative Disease, University College London Institute of Neurology, United Kingdom.

出版信息

N Engl J Med. 2009 Nov 19;361(21):2056-65. doi: 10.1056/NEJMoa0809716.

Abstract

BACKGROUND

Kuru is a devastating epidemic prion disease that affected a highly restricted geographic area of the Papua New Guinea highlands; at its peak, it predominantly affected adult women and children of both sexes. Its incidence has steadily declined since the cessation of its route of transmission, endocannibalism.

METHODS

We performed genetic and selected clinical and genealogic assessments of more than 3000 persons from Eastern Highland populations, including 709 who participated in cannibalistic mortuary feasts, 152 of whom subsequently died of kuru.

RESULTS

Persons who were exposed to kuru and survived the epidemic in Papua New Guinea are predominantly heterozygotes at the known resistance factor at codon 129 of the prion protein gene (PRNP). We now report a novel PRNP variant--G127V--that was found exclusively in people who lived in the region in which kuru was prevalent and that was present in half of the otherwise susceptible women from the region of highest exposure who were homozygous for methionine at PRNP codon 129. Although this allele is common in the area with the highest incidence of kuru, it is not found in patients with kuru and in unexposed population groups worldwide. Genealogic analysis reveals a significantly lower incidence of kuru in pedigrees that harbor the protective allele than in geographically matched control families.

CONCLUSIONS

The 127V polymorphism is an acquired prion disease resistance factor selected during the kuru epidemic, rather than a pathogenic mutation that could have triggered the kuru epidemic. Variants at codons 127 and 129 of PRNP demonstrate the population genetic response to an epidemic of prion disease and represent a powerful episode of recent selection in humans.

摘要

背景

库鲁病是一种极具破坏性的流行性朊病毒疾病,曾影响巴布亚新几内亚高地一个高度受限的地理区域;在其流行高峰期,主要影响成年女性和儿童。自其传播途径——内源性食人行为停止后,其发病率稳步下降。

方法

我们对来自东部高地人群的3000多人进行了基因以及部分临床和系谱评估,其中包括709名参与食人丧葬盛宴的人,这些人中152人随后死于库鲁病。

结果

在巴布亚新几内亚接触过库鲁病并在疫情中存活下来的人,在朊病毒蛋白基因(PRNP)第129密码子处的已知抗性因子上主要为杂合子。我们现在报告一种新的PRNP变异体——G127V,该变异体仅在库鲁病流行地区的人群中发现,并且在PRNP第129密码子处为甲硫氨酸纯合子的、来自最高暴露地区的易感女性中有一半携带该变异体。尽管这个等位基因在库鲁病发病率最高的地区很常见,但在库鲁病患者和全球未接触过该病的人群中未发现。系谱分析显示,携带保护性等位基因的家系中库鲁病的发病率明显低于地理匹配的对照家庭。

结论

127V多态性是在库鲁病流行期间选择出的一种获得性朊病毒病抗性因子,而非可能引发库鲁病流行的致病突变。PRNP第127和129密码子处的变异体展示了人群对朊病毒病流行的遗传反应,代表了人类近期一次有力的选择事件。

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