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果蝇中关键 DNA 修复基因家族的重复复制和多样化。

Recurrent Duplication and Diversification of a Vital DNA Repair Gene Family Across Drosophila.

机构信息

Department of Biology and Epigenetics Institute, University of Pennsylvania, Philadelphia, PA 19104, USA.

Department of Molecular Biology and Center for Regenerative Science and Medicine, University of Texas Southwestern Medical Center, Dallas, TX, USA.

出版信息

Mol Biol Evol. 2024 Jun 1;41(6). doi: 10.1093/molbev/msae113.

Abstract

Maintaining genome integrity is vital for organismal survival and reproduction. Essential, broadly conserved DNA repair pathways actively preserve genome integrity. However, many DNA repair proteins evolve adaptively. Ecological forces like UV exposure are classically cited drivers of DNA repair evolution. Intrinsic forces like repetitive DNA, which also imperil genome integrity, have received less attention. We recently reported that a Drosophila melanogaster-specific DNA satellite array triggered species-specific, adaptive evolution of a DNA repair protein called Spartan/MH. The Spartan family of proteases cleave hazardous, covalent crosslinks that form between DNA and proteins ("DNA-protein crosslink repair"). Appreciating that DNA satellites are both ubiquitous and universally fast-evolving, we hypothesized that satellite DNA turnover spurs adaptive evolution of DNA-protein crosslink repair beyond a single gene and beyond the D. melanogaster lineage. This hypothesis predicts pervasive Spartan gene family diversification across Drosophila species. To study the evolutionary history of the Drosophila Spartan gene family, we conducted population genetic, molecular evolution, phylogenomic, and tissue-specific expression analyses. We uncovered widespread signals of positive selection across multiple Spartan family genes and across multiple evolutionary timescales. We also detected recurrent Spartan family gene duplication, divergence, and gene loss. Finally, we found that ovary-enriched parent genes consistently birthed functionally diverged, testis-enriched daughter genes. To account for Spartan family diversification, we introduce a novel mechanistic model of antagonistic coevolution that links DNA satellite evolution and adaptive regulation of Spartan protease activity. This framework promises to accelerate our understanding of how DNA repeats drive recurrent evolutionary innovation to preserve genome integrity.

摘要

维持基因组完整性对于生物体的生存和繁殖至关重要。基本的、广泛保守的 DNA 修复途径积极地保护基因组完整性。然而,许多 DNA 修复蛋白是适应性进化的。紫外线暴露等生态力量通常被认为是 DNA 修复进化的驱动因素。像重复 DNA 这样的内在力量,也会危及基因组的完整性,但受到的关注较少。我们最近报道,一种果蝇特异性的 DNA 卫星阵列引发了一种称为 Spartan/MH 的 DNA 修复蛋白的物种特异性、适应性进化。Spartan 蛋白酶家族切割 DNA 和蛋白质之间形成的危险的共价交联(“DNA-蛋白质交联修复”)。鉴于 DNA 卫星无处不在且普遍进化迅速,我们假设卫星 DNA 的周转会刺激 DNA-蛋白质交联修复的适应性进化,不仅在单个基因中,而且在果蝇谱系之外。这一假设预测了 Spartan 基因家族在果蝇物种中的普遍多样化。为了研究果蝇 Spartan 基因家族的进化历史,我们进行了群体遗传学、分子进化、系统基因组学和组织特异性表达分析。我们在多个 Spartan 家族基因和多个进化时间尺度上发现了广泛的正选择信号。我们还检测到了 Spartan 家族基因重复、分化和基因丢失的反复出现。最后,我们发现卵巢丰富的亲本基因持续产生功能分化的、富含睾丸的子基因。为了解释 Spartan 家族的多样化,我们引入了一种新的拮抗协同进化的机制模型,将 DNA 卫星进化和 Spartan 蛋白酶活性的适应性调节联系起来。这个框架有望加速我们对 DNA 重复如何驱动反复出现的进化创新以维持基因组完整性的理解。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6414/11210505/c3f06d06456c/msae113f1.jpg

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