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Regulation of Oocyte mRNA Metabolism: A Key Determinant of Oocyte Developmental Competence.

Alison F ErmischJennifer R Wood
Published in: Advances in anatomy, embryology, and cell biology (2024)
The regulation of mRNA transcription and translation is uncoupled during oogenesis. The reason for this uncoupling is two-fold. Chromatin is only accessible to the transcriptional machinery during the growth phase as it condenses prior to resumption of meiosis to ensure faithful segregation of chromosomes during meiotic maturation. Thus, transcription rates are high during this time period in order to produce all of the transcripts needed for meiosis, fertilization, and embryo cleavage until the newly formed embryonic genome becomes transcriptionally active. To ensure appropriate timing of key developmental milestones including chromatin condensation, resumption of meiosis, segregation of chromosomes, and polar body extrusion, the translation of protein from transcripts synthesized during oocyte growth must be temporally regulated. This is achieved by the regulation of mRNA interaction with RNA binding proteins and shortening and lengthening of the poly(A) tail. This chapter details the essential factors that regulate the dynamic changes in mRNA synthesis, storage, translation, and degradation during oocyte growth and maturation.
Keyphrases
  • transcription factor
  • binding protein
  • gene expression
  • genome wide
  • dna damage
  • dna binding
  • pregnant women
  • dna methylation
  • oxidative stress
  • nitric oxide
  • protein protein
  • amino acid
  • nucleic acid
  • heat stress