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非裔美国人的线粒体DNA常常与在多个非洲族群中发现的线粒体DNA相匹配。

African-American mitochondrial DNAs often match mtDNAs found in multiple African ethnic groups.

作者信息

Ely Bert, Wilson Jamie Lee, Jackson Fatimah, Jackson Bruce A

机构信息

Department of Biological Sciences, University of South Carolina, Columbia, South Carolina, 29208, USA.

出版信息

BMC Biol. 2006 Oct 12;4:34. doi: 10.1186/1741-7007-4-34.

DOI:10.1186/1741-7007-4-34
PMID:17038170
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1618861/
Abstract

BACKGROUND

Mitochondrial DNA (mtDNA) haplotypes have become popular tools for tracing maternal ancestry, and several companies offer this service to the general public. Numerous studies have demonstrated that human mtDNA haplotypes can be used with confidence to identify the continent where the haplotype originated. Ideally, mtDNA haplotypes could also be used to identify a particular country or ethnic group from which the maternal ancestor emanated. However, the geographic distribution of mtDNA haplotypes is greatly influenced by the movement of both individuals and population groups. Consequently, common mtDNA haplotypes are shared among multiple ethnic groups. We have studied the distribution of mtDNA haplotypes among West African ethnic groups to determine how often mtDNA haplotypes can be used to reconnect Americans of African descent to a country or ethnic group of a maternal African ancestor. The nucleotide sequence of the mtDNA hypervariable segment I (HVS-I) usually provides sufficient information to assign a particular mtDNA to the proper haplogroup, and it contains most of the variation that is available to distinguish a particular mtDNA haplotype from closely related haplotypes. In this study, samples of general African-American and specific Gullah/Geechee HVS-I haplotypes were compared with two databases of HVS-I haplotypes from sub-Saharan Africa, and the incidence of perfect matches recorded for each sample.

RESULTS

When two independent African-American samples were analyzed, more than half of the sampled HVS-I mtDNA haplotypes exactly matched common haplotypes that were shared among multiple African ethnic groups. Another 40% did not match any sequence in the database, and fewer than 10% were an exact match to a sequence from a single African ethnic group. Differences in the regional distribution of haplotypes were observed in the African database, and the African-American haplotypes were more likely to match haplotypes found in ethnic groups from West or West Central Africa than those found in eastern or southern Africa. Fewer than 14% of the African-American mtDNA sequences matched sequences from only West Africa or only West Central Africa.

CONCLUSION

Our database of sub-Saharan mtDNA sequences includes the most common haplotypes that are shared among ethnic groups from multiple regions of Africa. These common haplotypes have been found in half of all sub-Saharan Africans. More than 60% of the remaining haplotypes differ from the common haplotypes at a single nucleotide position in the HVS-I region, and they are likely to occur at varying frequencies within sub-Saharan Africa. However, the finding that 40% of the African-American mtDNAs analyzed had no match in the database indicates that only a small fraction of the total number of African haplotypes has been identified. In addition, the finding that fewer than 10% of African-American mtDNAs matched mtDNA sequences from a single African region suggests that few African Americans might be able to trace their mtDNA lineages to a particular region of Africa, and even fewer will be able to trace their mtDNA to a single ethnic group. However, no firm conclusions should be made until a much larger database is available. It is clear, however, that when identical mtDNA haplotypes are shared among many ethnic groups from different parts of Africa, it is impossible to determine which single ethnic group was the source of a particular maternal ancestor based on the mtDNA sequence.

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c051/1618861/11b30e13ce87/1741-7007-4-34-2.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c051/1618861/8858cf2a9f38/1741-7007-4-34-1.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c051/1618861/11b30e13ce87/1741-7007-4-34-2.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c051/1618861/8858cf2a9f38/1741-7007-4-34-1.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c051/1618861/11b30e13ce87/1741-7007-4-34-2.jpg
摘要

背景

线粒体DNA(mtDNA)单倍型已成为追溯母系血统的常用工具,多家公司向公众提供此项服务。众多研究表明,人类mtDNA单倍型可用于可靠地识别单倍型起源的大陆。理想情况下,mtDNA单倍型还可用于识别母系祖先来自的特定国家或族群。然而,mtDNA单倍型的地理分布受到个体和群体迁移的极大影响。因此,常见的mtDNA单倍型在多个族群中共享。我们研究了西非族群中mtDNA单倍型的分布,以确定mtDNA单倍型能够多频繁地用于将非裔美国人与其非洲母系祖先的国家或族群重新联系起来。线粒体DNA高变区I(HVS-I)的核苷酸序列通常提供足够信息,以将特定的mtDNA归入适当的单倍群,并且它包含了大部分可用于区分特定mtDNA单倍型与密切相关单倍型的变异。在本研究中,将一般非裔美国人样本和特定的古拉/吉奇HVS-I单倍型与两个来自撒哈拉以南非洲的HVS-I单倍型数据库进行比较,并记录每个样本的完全匹配发生率。

结果

当对两个独立的非裔美国人样本进行分析时,超过一半的采样HVS-I mtDNA单倍型与多个非洲族群共享的常见单倍型完全匹配。另外40%与数据库中的任何序列都不匹配,不到10%与来自单个非洲族群的序列完全匹配。在非洲数据库中观察到单倍型的区域分布差异,非裔美国人的单倍型更有可能与西非或中西部非洲族群中发现的单倍型匹配,而不是与东非或南非发现的单倍型匹配。不到14%的非裔美国人mtDNA序列仅与西非或仅与中西部非洲的序列匹配。

结论

我们的撒哈拉以南mtDNA序列数据库包含了非洲多个地区族群共享的最常见单倍型。这些常见单倍型在所有撒哈拉以南非洲人中的一半中被发现。其余单倍型中超过60%在HVS-I区域的单个核苷酸位置与常见单倍型不同,并且它们可能在撒哈拉以南非洲以不同频率出现。然而,分析的40%非裔美国人mtDNA在数据库中没有匹配项这一发现表明,仅识别出了非洲单倍型总数的一小部分。此外,不到10%的非裔美国人mtDNA与来自单个非洲地区的mtDNA序列匹配这一发现表明,很少有非裔美国人能够将其mtDNA谱系追溯到非洲的特定地区,能够将其mtDNA追溯到单个族群的人甚至更少。然而,在有更大的数据库之前不应得出确凿结论。然而,很明显,当许多来自非洲不同地区的族群共享相同的mtDNA单倍型时,不可能根据mtDNA序列确定哪个单一族群是特定母系祖先的来源。

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