人类不等交换的同源性要求。
Homology requirements for unequal crossing over in humans.
作者信息
Metzenberg A B, Wurzer G, Huisman T H, Smithies O
机构信息
Laboratory of Genetics, University of Wisconsin, Madison 53706.
出版信息
Genetics. 1991 May;128(1):143-61. doi: 10.1093/genetics/128.1.143.
To gain insight into mechanisms of unequal homologous recombination in vivo, genes generated by homologous unequal crossovers in the human beta-globin gene cluster were examined by nucleotide sequencing and hybridization experiments. The naturally occurring genes studied included one delta-beta Lepore-Baltimore fusion gene, one delta-beta Lepore-Hollandia fusion gene, 12 delta-beta Lepore-Boston genes, one A gamma-beta fusion Kenya gene, one A gamma-G gamma fusion (the central gene of a triplication) and one G gamma-A gamma fusion. A comparison of the nucleotide sequences of three Lepore-Boston genes indicates that they were derived from at least two independent homologous but unequal crossover events, although the crossovers occurred within the same 58-bp region. Nine additional Lepore-Boston genes from individuals of various ethnic origins were shown, by hybridization to specific oligonucleotide probes, to have been generated by a crossover in the same region as the sequenced genes. Evidence for gene conversion accompanying a homologous unequal crossover event was found in only one case (although some of the single nucleotide differences observed in other genes in this study may be related to the crossover events in ways that we do not presently understand). Thus, as judged by this limited sample, concurrent gene conversions are not commonly associated with homologous but unequal exchange in humans in vivo. Classification of the recombinant chromosomes by their polymorphic restriction sites in the beta-globin gene cluster indicated that the Lepore-Boston genes are found in at least six different haplotype backgrounds. Therefore the total number of independent examples in this study is at least 6, and at most 12. We have shown that in at least six cases of genes that have arisen by homologous but unequal crossing over in vivo, each event occurred in a relatively extensive region of uninterrupted identity between the parental genes. This preference cannot be explained by a mechanism whereby crossovers occur at random within misaligned related but not identical genes. In general, crossovers occur in regions that are among the largest available stretches of identity for a particular pair of mismatched genes. Our data are in agreement with those of other types of studies of homologous recombination, and support the idea that sequence identity, rather than general homology, is a critical factor in homologous recombination.
为深入了解体内不等同源重组的机制,通过核苷酸测序和杂交实验对人类β-珠蛋白基因簇中同源不等交换产生的基因进行了研究。所研究的天然存在的基因包括一个δ-β Lepore-巴尔的摩融合基因、一个δ-β Lepore-霍兰迪亚融合基因、12个δ-β Lepore-波士顿基因、一个Aγ-β融合肯尼亚基因、一个Aγ-Gγ融合基因(三倍体的中心基因)和一个Gγ-Aγ融合基因。对三个Lepore-波士顿基因的核苷酸序列比较表明,尽管交换发生在相同的58个碱基对区域内,但它们至少源自两个独立的同源但不等的交换事件。通过与特定寡核苷酸探针杂交显示,来自不同种族个体的另外九个Lepore-波士顿基因是在与已测序基因相同的区域内通过交换产生的。仅在一个案例中发现了伴随同源不等交换事件的基因转换证据(尽管在本研究中其他基因中观察到的一些单核苷酸差异可能以我们目前尚不清楚的方式与交换事件有关)。因此,根据这个有限的样本判断,在人类体内,并发基因转换通常与同源但不等的交换无关。通过β-珠蛋白基因簇中多态性限制位点对重组染色体进行分类表明,Lepore-波士顿基因存在于至少六种不同的单倍型背景中。因此,本研究中独立实例的总数至少为6个,最多为12个。我们已经表明,在至少六个体内由同源但不等交换产生的基因案例中,每个事件都发生在亲本基因之间相对广泛的不间断同源区域内。这种偏好不能用一种机制来解释,即交换在错配的相关但不相同的基因内随机发生。一般来说,交换发生在特定一对错配基因中最大的可用同源区域内。我们的数据与同源重组的其他类型研究的数据一致,并支持序列同源性而非一般同源性是同源重组关键因素的观点。
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