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LSM14B controls oocyte mRNA storage and stability to ensure female fertility.

Li-Ying ShanYu TianWen-Xiang LiuHai-Tao FanFeng-Guo LiWen-Juan LiuAng LiWei ShenQing-Yuan SunYong-Bin LiuYang ZhouTeng Zhang
Published in: Cellular and molecular life sciences : CMLS (2023)
Controlled mRNA storage and stability is essential for oocyte meiosis and early embryonic development. However, how to regulate mRNA storage and stability in mammalian oogenesis remains elusive. Here we showed that LSM14B, a component of membraneless compartments including P-body-like granules and mitochondria-associated ribonucleoprotein domain (MARDO) in germ cell, is indispensable for female fertility. To reveal loss of LSM14B disrupted primordial follicle assembly and caused mRNA reduction in non-growing oocytes, which was concomitant with the impaired assembly of P-body-like granules. 10× Genomics single-cell RNA-sequencing and immunostaining were performed. Meanwhile, we conducted RNA-seq analysis of GV-stage oocytes and found that Lsm14b deficiency not only impaired the maternal mRNA accumulation but also disrupted the translation in fully grown oocytes, which was closely associated with dissolution of MARDO components. Moreover, Lsm14b-deficient oocytes reassembled a pronucleus containing decondensed chromatin after extrusion of the first polar body, through compromising the activation of maturation promoting factor, while the defects were restored via WEE1/2 inhibitor. Together, our findings reveal that Lsm14b plays a pivotal role in mammalian oogenesis by specifically controlling of oocyte mRNA storage and stability.
Keyphrases
  • single cell
  • rna seq
  • binding protein
  • high throughput
  • germ cell
  • genome wide
  • dna damage
  • cell death
  • body mass index
  • ionic liquid
  • resting state
  • young adults
  • weight loss
  • weight gain