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美洲原住民和太平洋岛屿人群中JC病毒的亚洲基因型:病毒进化和人类迁徙的标志物

Asian genotypes of JC virus in Native Americans and in a Pacific Island population: markers of viral evolution and human migration.

作者信息

Agostini H T, Yanagihara R, Davis V, Ryschkewitsch C F, Stoner G L

机构信息

Neurotoxicology Section, National Institute of Neurological Disorders and Stroke, National Institutes of Health, Bethesda, MD 20892, USA.

出版信息

Proc Natl Acad Sci U S A. 1997 Dec 23;94(26):14542-6. doi: 10.1073/pnas.94.26.14542.

Abstract

The human polyomavirus JC (JCV) causes the central nervous system demyelinating disease progressive multifocal leukoencephalopathy. Previously, we showed that 40% of Caucasians in the United States excrete JCV in the urine as detected by PCR. We have now studied 68 Navaho from New Mexico, 25 Flathead from Montana, and 29 Chamorro from Guam. By using PCR amplification of a fragment of the VP1 gene, JCV DNA was detected in the urine of 45 (66%) Navaho, 14 (56%) Flathead, and 20 (69%) Chamorro. Genotyping of viral DNAs in these cohorts by cycle sequencing showed predominantly type 2 (Asian), rather than type 1 (European). Type 1 is the major type in the United States and Hungary. Type 2 can be further subdivided into 2A, 2B, and 2C. Type 2A is found in China and Japan. Type 2B is a subtype related to the East Asian type, and is now found in Europe and the United States. The large majority (56-89%) of strains excreted by Native Americans and Pacific Islanders were the type 2A subtype, consistent with the origin of these strains in Asia. These findings indicate that JCV infection of Native Americans predates contact with Europeans, and likely predates migration of Amerind ancestors across the Bering land bridge around 12,000-30,000 years ago. If JCV had already differentiated into stable modern genotypes and subtypes prior to first settlement, the origin of JCV in humans may date from 50,000 to 100,000 years ago or more. We conclude that JCV may have coevolved with the human species, and that it provides a convenient marker for human migrations in both prehistoric and modern times.

摘要

人类多瘤病毒JC(JCV)可引发中枢神经系统脱髓鞘疾病——进行性多灶性白质脑病。此前,我们发现,通过聚合酶链反应(PCR)检测,美国40%的高加索人尿液中可排出JCV。我们现在对来自新墨西哥州的68名纳瓦霍人、来自蒙大拿州的25名平头印第安人以及来自关岛的29名查莫罗人进行了研究。通过对VP1基因片段进行PCR扩增,在45名(66%)纳瓦霍人、14名(56%)平头印第安人以及20名(69%)查莫罗人的尿液中检测到了JCV DNA。通过循环测序对这些队列中的病毒DNA进行基因分型显示,主要为2型(亚洲型),而非1型(欧洲型)。1型是美国和匈牙利的主要类型。2型可进一步细分为2A、2B和2C。2A型在中国和日本被发现。2B型是与东亚型相关的一个亚型,现在在欧洲和美国被发现。美洲原住民和太平洋岛民排出的毒株绝大多数(56 - 89%)为2A型亚型,这与这些毒株起源于亚洲一致。这些发现表明,美洲原住民感染JCV的时间早于与欧洲人接触的时间,而且很可能早于约12000 - 30000年前美洲印第安祖先跨越白令陆桥的迁徙时间。如果JCV在首次定居之前就已经分化为稳定的现代基因型和亚型,那么JCV在人类中的起源时间可能可追溯到50000至100000年前或更久以前。我们得出结论,JCV可能与人类共同进化,并且它为史前和现代的人类迁徙提供了一个便利的标记。

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