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RNA 解旋酶 D1PAS1 可解决 R 环问题,并形成复合物,用于小鼠粗线期 piRNA 的生物发生,这对于雄性生育力是必需的。

RNA helicase D1PAS1 resolves R-loops and forms a complex for mouse pachytene piRNA biogenesis required for male fertility.

机构信息

Laboratory of Cellular and Developmental Biology, NIDDK, National Institutes of Health, Bethesda, MD 20892, USA.

出版信息

Nucleic Acids Res. 2024 Oct 28;52(19):11973-11994. doi: 10.1093/nar/gkae712.

Abstract

During meiosis, RNA polymerase II transcribes pachytene piRNA precursors with unusually long and unspliced transcripts from discrete autosomal loci in the mouse genome. Despite the importance of piRNA for male fertility and a well-defined maturation process, the transcriptional machinery remains poorly understood. Here, we document that D1PAS1, an ATP-dependent RNA helicase, is critical for pachytene piRNA expression from multiple genomic loci and subsequent translocation into the cytoplasm to ensure mature piRNA biogenesis. Depletion of D1PAS1 in gene-edited mice results in the accumulation of R-loops in pachytene spermatocytes, leading to DNA-damage-induced apoptosis, disruption of piRNA biogenesis, spermatogenic arrest, and male infertility. Transcriptome, genome-wide R-loop profiling, and proteomic analyses document that D1PAS1 regulates pachytene piRNA transcript elongation and termination. D1PAS1 subsequently forms a complex with nuclear export components to ensure pachytene piRNA precursor translocation from the nucleus to the cytoplasm for processing into small non-coding RNAs. Thus, our study defines D1PAS1 as a specific transcription activator that promotes R-loop unwinding and is a critical factor in pachytene piRNA biogenesis.

摘要

在减数分裂过程中,RNA 聚合酶 II 从小鼠基因组中离散的常染色体基因座转录具有异常长和未剪接转录物的粗线期 piRNA 前体。尽管 piRNA 对雄性生育力很重要,并且有明确的成熟过程,但转录机制仍知之甚少。在这里,我们证明 D1PAS1,一种 ATP 依赖性 RNA 解旋酶,对于来自多个基因组基因座的粗线期 piRNA 表达以及随后转入细胞质以确保成熟 piRNA 生物发生至关重要。在基因编辑的小鼠中耗尽 D1PAS1 会导致粗线期精母细胞中 R 环的积累,导致 DNA 损伤诱导的细胞凋亡、piRNA 生物发生的破坏、精子发生停滞和雄性不育。转录组、全基因组 R 环分析和蛋白质组学分析表明,D1PAS1 调节粗线期 piRNA 转录物的延伸和终止。D1PAS1 随后与核输出成分形成复合物,以确保粗线期 piRNA 前体从细胞核转移到细胞质进行加工成小非编码 RNA。因此,我们的研究将 D1PAS1 定义为一种特定的转录激活因子,它促进 R 环解旋,是粗线期 piRNA 生物发生的关键因素。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/25ff/11514495/a8e7f094ac75/gkae712figgra1.jpg

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