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人类基因组中快速进化的非编码序列。

Fast-evolving noncoding sequences in the human genome.

作者信息

Bird Christine P, Stranger Barbara E, Liu Maureen, Thomas Daryl J, Ingle Catherine E, Beazley Claude, Miller Webb, Hurles Matthew E, Dermitzakis Emmanouil T

机构信息

The Wellcome Trust Sanger Institute, Wellcome Trust Genome Campus, Hinxton, CB10 1SA, UK.

出版信息

Genome Biol. 2007;8(6):R118. doi: 10.1186/gb-2007-8-6-r118.

Abstract

BACKGROUND

Gene regulation is considered one of the driving forces of evolution. Although protein-coding DNA sequences and RNA genes have been subject to recent evolutionary events in the human lineage, it has been hypothesized that the large phenotypic divergence between humans and chimpanzees has been driven mainly by changes in gene regulation rather than altered protein-coding gene sequences. Comparative analysis of vertebrate genomes has revealed an abundance of evolutionarily conserved but noncoding sequences. These conserved noncoding (CNC) sequences may well harbor critical regulatory variants that have driven recent human evolution.

RESULTS

Here we identify 1,356 CNC sequences that appear to have undergone dramatic human-specific changes in selective pressures, at least 15% of which have substitution rates significantly above that expected under neutrality. The 1,356 'accelerated CNC' (ANC) sequences are enriched in recent segmental duplications, suggesting a recent change in selective constraint following duplication. In addition, single nucleotide polymorphisms within ANC sequences have a significant excess of high frequency derived alleles and high F(ST) values relative to controls, indicating that acceleration and positive selection are recent in human populations. Finally, a significant number of single nucleotide polymorphisms within ANC sequences are associated with changes in gene expression. The probability of variation in an ANC sequence being associated with a gene expression phenotype is fivefold higher than variation in a control CNC sequence.

CONCLUSION

Our analysis suggests that ANC sequences have until very recently played a role in human evolution, potentially through lineage-specific changes in gene regulation.

摘要

背景

基因调控被认为是进化的驱动力之一。尽管蛋白质编码DNA序列和RNA基因在人类谱系中经历了近期的进化事件,但据推测,人类与黑猩猩之间巨大的表型差异主要是由基因调控的变化而非蛋白质编码基因序列的改变所驱动。脊椎动物基因组的比较分析揭示了大量进化上保守但非编码的序列。这些保守的非编码(CNC)序列很可能包含驱动近期人类进化的关键调控变异。

结果

在此,我们鉴定出1356个CNC序列,它们似乎在选择压力下经历了显著的人类特异性变化,其中至少15%的替换率明显高于中性预期。这1356个“加速CNC”(ANC)序列在近期的片段重复中富集,表明重复后选择约束发生了近期变化。此外,相对于对照组,ANC序列内的单核苷酸多态性有显著过量的高频衍生等位基因和高F(ST)值,表明加速和正选择在人类群体中是近期发生的。最后,ANC序列内大量的单核苷酸多态性与基因表达的变化相关。ANC序列中变异与基因表达表型相关的概率比对照CNC序列中的变异高五倍。

结论

我们的分析表明,直到最近,ANC序列可能通过基因调控的谱系特异性变化在人类进化中发挥了作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/08de/2394770/2b30277b5e70/gb-2007-8-6-r118-1.jpg

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