In utero pulse injection of isotopic amino acids quantifies protein turnover rates during murine fetal development

Josue Baeza, Barbara E. Coons, Zongtao Lin, John Riley, Mariel Mendoza, William H. Peranteau, Benjamin A. Garcia

Research output: Contribution to journalArticlepeer-review

Abstract

Protein translational control is critical for ensuring that the fetus develops correctly and that necessary organs and tissues are formed and functional. We developed an in utero method to quantify tissue-specific protein dynamics by monitoring amino acid incorporation into the proteome after pulse injection. Fetuses of pregnant mice were injected with isotopically labeled lysine and arginine via the vitelline vein at various embyonic days, and organs and tissues were harvested. By analyzing the nascent proteome, unique signatures of each tissue were identified by hierarchical clustering. In addition, the quantified proteome-wide turnover rates were calculated between 3.81E−5 and 0.424 h−1. We observed similar protein turnover profiles for analyzed organs (e.g., liver vs. brain); however, their distributions of turnover rates vary significantly. The translational kinetic profiles of developing organs displayed differentially expressed protein pathways and synthesis rates, which correlated with known physiological changes during mouse development.

Original languageEnglish
Article number100713
JournalCell Reports Methods
Volume4
Issue number2
DOIs
StatePublished - Feb 26 2024

Keywords

  • CP: Developmental biology
  • CP: Molecular biology
  • fetal development
  • in utero injection
  • protein turnover
  • proteomics
  • pulse labeling

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