Proteomic Profiling of Unannotated Microproteins in Human Placenta Reveals XRCC6P1 as a Potential Negative Regulator of Translation

Qiong Li, Fanrong Liu, Xiaoyu Ma, Feifei Chen, Ziying Yi, Yangyang Du, Anxin Huang, Chenyang Zhao, Da Wang, Yanran Chen, Xiongwen Cao

Research output: Contribution to journalArticlepeer-review

Abstract

Ribosome profiling and mass spectrometry have revealed thousands of previously unannotated small and alternative open reading frames (sm/alt-ORFs) that are translated into micro/alt-proteins in mammalian cells. However, their prevalence across human tissues and biological roles remains largely undefined. The placenta is an ideal model for identifying unannotated microproteins and alt-proteins due to its considerable protein diversity that is required to sustain fetal development during pregnancy. Here, we profiled unannotated microproteins and alt-proteins in human placental tissues from preeclampsia patients or healthy individuals by proteomics, identified 52 unannotated microproteins or alt-proteins, and demonstrated that five microproteins can be translated from overexpression constructs in a heterologous cell line, although several are unstable. We further demonstrated that one microprotein, XRCC6P1, associates with translation initiation factor eIF3 and negatively regulates translation when exogenously overexpressed. Thus, we revealed a hidden sm/alt-ORF-encoded proteome in the human placenta, which may advance the mechanism studies for placenta development as well as placental disorders such as preeclampsia.

Original languageEnglish
Pages (from-to)4005-4013
Number of pages9
JournalJournal of Proteome Research
Volume23
Issue number9
DOIs
StatePublished - 6 Sep 2024

Keywords

  • XRCC6P1
  • alternative protein
  • eIF3
  • human placenta
  • microprotein
  • preeclampsia
  • translation
  • unannotated protein

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