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Analysis of mtDNA variation in African populations reveals the most ancient of all human continent-specific haplogroups.

机译:对非洲人群中mtDNA变异的分析揭示了人类大陆特定单倍群中最古老的。

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摘要

mtDNA sequence variation was examined in 140 Africans, including Pygmies from Zaire and Central African Republic (C.A.R.) and Mandenkalu, Wolof, and Pular from Senegal. More than 76% of the African mtDNAs (100% of the Pygmies and 67.3% of the Senegalese) formed one major mtDNA cluster (haplogroup L) defined by an African-specific HpaI site gain at nucleotide pair (np) 3592. Additional mutations subdivided haplogroup L into two subhaplogroups, each encompassing both Pygmy and Senegalese mtDNAs. A novel 12-bp homoplasmic insertion in the intergenic region between tRNA(Tyr) and cytochrome oxidase I (COI) genes was also observed in 17.6% of the Pygmies from C.A.R. This insertion is one of the largest observed in human mtDNAs. Another 25% of the Pygmy mtDNAs harbored a 9-bp deletion between the cytochrome oxidase II (COII) and tRNA(Lys) genes, a length polymorphism previously reported in non-African populations. In addition to haplogroup L, other haplogroups were observed in the Senegalese. These haplogroups were more similar to those observed in Europeans and Asians than to haplogroup L mtDNAs, suggesting that the African mtDNAs without the HpaI np 3592 site could be the ancestral types from which European and Asian mtDNAs were derived. Comparison of the intrapopulation sequence divergence in African and non-African populations confirms that African populations exhibit the largest extent of mtDNA variation, a result that further supports the hypothesis that Africans represent the most ancient human group and that all modern humans have a common and recent African origin. The age of the total African variation was estimated to be 101,000-133,000 years before present (YBP), while the age of haplogroup L was estimated at 98,000-130,000 YBP. These values substantially exceed the ages of all Asian- and European-specific mtDNA haplogroups.
机译:在140名非洲人中检查了mtDNA序列变异,包括来自扎伊尔和中非共和国(C.A.R.)的P格米人以及来自塞内加尔的Mandenkalu,Wolof和Pular。超过76%的非洲mtDNA(100%的y格米人和67.3%的塞内加尔人)形成了一个主要的mtDNA簇(单倍型L),该簇由非洲特异性HpaI位点在核苷酸对(np)3592处定义。其他突变被细分。 L单倍群L分为两个亚单倍群,每个亚倍群都包含P格米和塞内加尔mtDNA。在C.A.R.的17.族侏儒中,在tRNA(Tyr)和细胞色素氧化酶I(COI)基因之间的基因间区域中也发现了新的12 bp同质插入。该插入是人类mtDNA中观察到的最大插入之一。 25格米人mtDNA的另外25%在细胞色素氧化酶II(COII)和tRNA(Lys)基因之间隐藏了9 bp的缺失,这是以前在非非洲人群中报道的一种长度多态性。除了单倍群L,在塞内加尔人中还观察到其他单倍群。这些单倍群与在欧洲人和亚洲人中观察到的相似,而不是与单倍体L mtDNA相似,这表明没有HpaI np 3592位点的非洲mtDNA可能是欧洲和亚洲mtDNA的祖先类型。比较非洲和非非洲人口的种群内序列差异,证实非洲人口表现出最大程度的mtDNA变异,这一结果进一步支持了以下假设:非洲人代表最古老的人类群体,而所有现代人类都有共同的和最近的非洲血统。非洲总变异的年龄估计为现世前的101,000-133,000年(YBP),而单倍体L的年龄估计为98,000-130,000 YBP。这些值大大超过了所有亚洲和欧洲特定的mtDNA单倍群的年龄。

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