Argonaute CSR-1A promotes H3K9me3 maintenance to protect somatic development in offspring

IF 13.1 2区 生物学 Q1 BIOCHEMISTRY & MOLECULAR BIOLOGY Nucleic Acids Research Pub Date : 2025-03-04 DOI:10.1093/nar/gkaf127
Di Rao, Dengfeng Li, Lili Li, Junchao Xue, Shikui Tu, En-Zhi Shen
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Abstract

Parental stress can be encoded into altered epigenetic information to influence their offspring. Concurrently, it is vital for the preservation of a parent's epigenetic information, despite environmental challenges, to ensure accurate inheritance by the next generation. Nevertheless, the complexities of this process and the specific molecular mechanisms involved are not yet fully understood. Here we report that Argonaute CSR-1A potentiates the recovery of histone H3 lysine 9 trimethylation (H3K9me3) in spermatocyte to secure the developmental competence of male offspring. CSR-1A employs its repetitive RG motif to engage with putative histone 3 lysine 9 (H3K9) methyltransferases SET-25 and -32, and helps to restore repressive H3K9me3 chromatin marks following heat-stress, protecting the late development of somatic cells in the progeny. Finally, among the genes regulated by CSR-1A, we identified dim-1, at which decreased H3K9me3 persists in the progeny, and RNAi of dim-1 mitigates the somatic defects associated with csr-1a loss under stress. Thus, CSR-1A coordinates a paternal epigenetic program that shields development from the influences of the paternal environment. We speculate that, driven by both natural environmental stressors and the unique characteristics of spermatogenic chromatin, the emergence of multiple RG motif-featured and spermatogenesis-specific CSR-1A and small RNA serves as a protective strategy to safeguard against variability in the orchestration of inherited developmental programs from the paternal lineage.
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Argonaute CSR-1A促进H3K9me3维持以保护后代的体细胞发育
父母的压力可以被编码成改变的表观遗传信息,从而影响他们的后代。同时,尽管面临环境挑战,保存父母的表观遗传信息对于确保下一代的准确遗传至关重要。然而,这一过程的复杂性和所涉及的具体分子机制尚未完全了解。在这里,我们报道了Argonaute CSR-1A增强了精母细胞中组蛋白H3赖氨酸9三甲基化(H3K9me3)的恢复,以确保雄性后代的发育能力。CSR-1A利用其重复RG基序与组蛋白3赖氨酸9 (H3K9)甲基转移酶SET-25和-32结合,帮助恢复热应激后抑制的H3K9me3染色质标记,保护后代体细胞的晚期发育。最后,在受CSR-1A调控的基因中,我们发现了dim-1,其H3K9me3的降低在后代中持续存在,并且dim-1的RNAi减轻了应激下CSR-1A缺失相关的体细胞缺陷。因此,CSR-1A协调父系表观遗传程序,保护发育免受父系环境的影响。我们推测,在自然环境压力因素和生精染色质独特特征的驱动下,多种RG基序特征和精子发生特异性的CSR-1A和小RNA的出现作为一种保护策略,以防止来自父系的遗传发育程序的变化。
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来源期刊
Nucleic Acids Research
Nucleic Acids Research 生物-生化与分子生物学
CiteScore
27.10
自引率
4.70%
发文量
1057
审稿时长
2 months
期刊介绍: Nucleic Acids Research (NAR) is a scientific journal that publishes research on various aspects of nucleic acids and proteins involved in nucleic acid metabolism and interactions. It covers areas such as chemistry and synthetic biology, computational biology, gene regulation, chromatin and epigenetics, genome integrity, repair and replication, genomics, molecular biology, nucleic acid enzymes, RNA, and structural biology. The journal also includes a Survey and Summary section for brief reviews. Additionally, each year, the first issue is dedicated to biological databases, and an issue in July focuses on web-based software resources for the biological community. Nucleic Acids Research is indexed by several services including Abstracts on Hygiene and Communicable Diseases, Animal Breeding Abstracts, Agricultural Engineering Abstracts, Agbiotech News and Information, BIOSIS Previews, CAB Abstracts, and EMBASE.
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