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与其他 NHEJ 因子相比,DNA-PK 蛋白和 RNA 水平在所有高等灵长类动物中显著增加,但在原猴或其他哺乳动物中没有增加。

Compared to other NHEJ factors, DNA-PK protein and RNA levels are markedly increased in all higher primates, but not in prosimians or other mammals.

机构信息

RIKEN Center for Integrative Medical Sciences (IMS), Yokohama, Japan.

Department of Microbiology, Genetics, and Immunology, Michigan State University, East Lansing, MI 48824, USA.

出版信息

DNA Repair (Amst). 2024 Oct;142:103737. doi: 10.1016/j.dnarep.2024.103737. Epub 2024 Aug 8.

Abstract

The DNA dependent protein kinase (DNA-PK) initiates non-homologous recombination (NHEJ), the predominate DNA double-strand break (DSBR) pathway in higher vertebrates. It has been known for decades that the enzymatic activity of DNA-PK [that requires its three component polypeptides, Ku70, Ku80 (that comprise the DNA-end binding Ku heterodimer), and the catalytic subunit (DNA-PKcs)] is present in humans at 10-50 times the level observed in other mammals. Here, we show that the high level of DNA-PKcs protein expression appears evolutionarily in mammals between prosimians and higher primates. Moreover, the RNAs encoding the three component polypeptides of DNA-PK are present at similarly high levels in hominids, new-, and old-world monkeys, but expression of these RNAs in prosimians is ∼5-50 fold less, analogous to the levels observed in other non-primate species. This is reminiscent of the appearance of Alu repeats in primate genomes -- abundant in higher primates, but present at much lower density in prosimians. Alu repeats are well-known for their capacity to promote non-allelic homologous recombination (NAHR) a process known to be inhibited by DNA-PK. Nanopore sequence analyses of cultured cells proficient or deficient in DNA-PK revealed an increase of inter-chromosomal translocations caused by NAHR. Although the high levels of DNA-PK in primates may have many functions, we posit that high levels of DNA-PK may function to restrain deleterious NAHR events between Alu elements.

摘要

DNA 依赖性蛋白激酶(DNA-PK)启动非同源重组(NHEJ),这是高等脊椎动物中主要的 DNA 双链断裂(DSBR)途径。几十年来,人们已经知道,DNA-PK 的酶活性[需要其三个组成多肽,Ku70、Ku80(构成 DNA 末端结合 Ku 异二聚体)和催化亚基(DNA-PKcs)]在人类中的水平是其他哺乳动物的 10-50 倍。在这里,我们表明,在灵长类动物和高等灵长类动物之间的原猴中,DNA-PKcs 蛋白表达水平的高度进化。此外,编码 DNA-PK 三个组成多肽的 RNA 在人科、新猴和旧猴中同样高水平表达,但在原猴中这些 RNA 的表达水平降低了 5-50 倍,类似于在其他非灵长类物种中观察到的水平。这让人想起了 Alu 重复在灵长类基因组中的出现——在高等灵长类动物中丰富,但在原猴中密度要低得多。Alu 重复以其促进非等位基因同源重组(NAHR)的能力而闻名,而 DNA-PK 已知能抑制该过程。对具有或缺乏 DNA-PK 的培养细胞进行纳米孔测序分析,揭示了由 NAHR 引起的染色体间易位增加。虽然灵长类动物中高水平的 DNA-PK 可能具有许多功能,但我们假设高水平的 DNA-PK 可能有助于抑制 Alu 元件之间有害的 NAHR 事件。

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