4.8 Article

Codon identity regulates mRNA stability and translation efficiency during the maternal-to-zygotic transition

Journal

EMBO JOURNAL
Volume 35, Issue 19, Pages 2087-2103

Publisher

WILEY
DOI: 10.15252/embj.201694699

Keywords

codon optimality; decay; maternal-to-zygotic transition; translation; zebrafish

Funding

  1. Pew Fellows Program in Biomedical Sciences
  2. James Hudson Brown-Alexander Brown Coxe Postdoctoral Fellowship
  3. Swiss National Science Foundation [P2GEP3_148600]
  4. US National Institutes of Health [R21 HD073768, R01 HD081379 GM103789, R01 GM102251, R01 GM101108, GM081602, R01 HD081379, R01 GM37949, GM37951]
  5. Edward Mallinckrodt Jr. Foundation
  6. Pew Scholars Program in the Biomedical Sciences
  7. March of Dimes
  8. Yale Scholars Program
  9. Whitman fellowship funds
  10. [T32GM007499]
  11. Swiss National Science Foundation (SNF) [P2GEP3_148600] Funding Source: Swiss National Science Foundation (SNF)

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Cellular transitions require dramatic changes in gene expression that are supported by regulated mRNA decay and new transcription. The maternal-to-zygotic transition is a conserved developmental progression during which thousands of maternal mRNAs are cleared by post-transcriptional mechanisms. Although some maternal mRNAs are targeted for degradation by microRNAs, this pathway does not fully explain mRNA clearance. We investigated how codon identity and translation affect mRNA stability during development and homeostasis. We show that the codon triplet contains translation-dependent regulatory information that influences transcript decay. Codon composition shapes maternal mRNA clearance during the maternal-to-zygotic transition in zebrafish, Xenopus, mouse, and Drosophila, and gene expression during homeostasis across human tissues. Some synonymous codons show consistent stabilizing or destabilizing effects, suggesting that amino acid composition influences mRNA stability. Codon composition affects both polyadenylation status and translation efficiency. Thus, the ribosome interprets two codes within the mRNA: the genetic code which specifies the amino acid sequence and a conserved codon optimality code that shapes mRNA stability and translation efficiency across vertebrates.

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