PATL2突变影响人卵母细胞mRNA稳态和细胞周期调节中的蛋白相互作用。

IF 6.1 2区生物学 Q1 BIOCHEMISTRY & MOLECULAR BIOLOGY

Cell and Bioscience Pub Date : 2024-12-31 DOI:10.1186/s13578-024-01341-2

Yin-Li Zhang, Zhanhong Hu, Huifang Jiang, Jiamin Jin, Yan Zhou, Mengru Lai, Peipei Ren, Siya Liu, Ying-Yi Zhang, Yan Rong, Wei Zheng, Shen Zhang, Xiaomei Tong, Songying Zhang

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引用次数: 0

摘要

背景：卵母细胞成熟缺陷（OMD）和早期胚胎骤停是导致女性不育的主要原因。先前的研究已经将PATL2基因的双等位基因突变与OMD联系起来，但其潜在的机制在很大程度上仍然未知。结果：本研究发现了3个新突变（c.1201G b> T, c.1284delA和c.1613 + 2_1613 + 3insGT）和3个已报道的突变(c.1204C . > T, C . 1271t > C, C .223 - 14_223-2delCCCTCCTGTTCCA)在表现出OMD、卵母细胞死亡和早期胚胎停止的5个无亲缘关系个体的PATL2基因中的表达。RNA测序显示，PATL2突变降低了人生发囊泡（GV）卵母细胞中mRNA的储存，并阻碍了成熟和早期胚胎中mRNA的衰变。我们证明了人类卵母细胞中PATL2与CPEB1和TUT7相互作用以维持mRNA稳态。此外，我们观察到patl2突变的GV卵母细胞中CCNB1和CCNE1 mRNA水平降低，这可能与GV阻滞有关。利用野生型和突变的PATL2V401F/R402W变体，我们表征了PATL2的蛋白质相互作用组，确定了PATL2V401F/R402W变体的破坏主要影响细胞周期相关蛋白，包括CDC23， APC1和MAD2L1。PATL2与卵母细胞中CDC23的相互作用和稳定可能阐明突变诱导心肌梗死的机制。PALT2是mRNA高效翻译所必需的，它维持小鼠GV卵母细胞中CDC23、APC1和MAD2L1的蛋白水平。结论：PATL2可能分别通过与CPEB1和TUT7的相互作用，在调节人卵母细胞mRNA的积累和衰变中发挥关键作用。PATL2突变通过影响mRNA积累、mRNA翻译以及直接结合和稳定与细胞周期调节相关的蛋白，如CCNB1和CDC23，导致卵母细胞减数分裂缺陷。这项研究扩大了PATL2的突变谱，并为PATL2突变相关的卵母细胞成熟障碍的分子机制提供了新的见解。

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PATL2 mutations affect human oocyte maternal mRNA homeostasis and protein interactions in cell cycle regulation.

Background: Oocyte maturation defect (OMD) and early embryonic arrest result in female infertility. Previous studies have linked biallelic mutations in the PATL2 gene to OMD, yet the underlying mechanism remains largely unknown.

Results: This study uncovers three novel mutations (c.1201G > T, c.1284delA and c.1613 + 2_1613 + 3insGT) and three reported mutations (c.1204 C > T, c.1271T > C, c.223 - 14_223-2delCCCTCCTGTTCCA) in the PATL2 gene across five unrelated individuals exhibiting OMD, oocyte death, and early embryonic arrest. RNA sequencing revealed that PATL2 mutations decreased mRNA storage in human germinal vesicle (GV) oocytes and impeded mRNA decay during maturation and in early embryos. We demonstrate that PATL2 interacts with CPEB1 and TUT7 in human oocytes to maintain mRNA homeostasis. Additionally, we observed a reduction in CCNB1 and CCNE1 mRNA levels in PATL2-mutant GV oocytes, which may be linked to GV arrest. Employing both wild-type and mutated PATL2^V401F/R402W variants, we characterized the protein interactome of PATL2, identifying disruptions of PATL2^V401F/R402W variants predominantly affecting cell cycle-related proteins, including CDC23, APC1 and MAD2L1. PATL2's interaction with and stabilization of CDC23 in oocytes may elucidate the mechanisms behind the mutation-induced MI arrest. PALT2 is required for the efficient mRNA translation and it maintains the protein level of CDC23, APC1 and MAD2L1 in mouse GV oocyte.

Conclusion: PATL2 plays a critical role in regulating mRNA accumulation and decay in human oocytes, potentially through interactions with CPEB1 and TUT7, respectively. Mutations in PATL2 lead to oocyte meiosis defects by affecting the mRNA accumulation, mRNA translation, and direct binding to and stabilizing proteins related to cell cycle regulation, such as CCNB1 and CDC23. This study expands the mutational spectrum of PATL2 and provides new insights into the molecular mechanisms underlying PATL2 mutation-associated oocyte maturation disorders.

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来源期刊

Cell and Bioscience BIOCHEMISTRY & MOLECULAR BIOLOGY-

CiteScore

10.70

自引率

0.00%

发文量

187

审稿时长

>12 weeks

期刊介绍： Cell and Bioscience, the official journal of the Society of Chinese Bioscientists in America, is an open access, peer-reviewed journal that encompasses all areas of life science research.