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Lysine ubiquitination and acetylation of human cardiac 20S proteasomes

  • Nobel Zong
  • , Peipei Ping
  • , Edward Lau
  • , Howard J.H. Choi
  • , Dominic C.M. Ng
  • , David Meyer
  • , Caiyun Fang
  • , Haomin Li
  • , Ding Wang
  • , Ivette M. Zelaya
  • , John R. Yates
  • , Maggie P.Y. Lam

Research output: Contribution to journalArticlepeer-review

Abstract

Purpose: Altered proteasome functions are associated with multiple cardiomyopathies. While the proteasome targets polyubiquitinated proteins for destruction, it itself is modifiable by ubiquitination. We aim to identify the exact ubiquitination sites on cardiac proteasomes and examine whether they are also subject to acetylations. Experimental design: Assembled cardiac 20S proteasome complexes were purified from five human hearts with ischemic cardiomyopathy, then analyzed by high-resolution MS to identify ubiquitination and acetylation sites. We developed a library search strategy that may be used to complement database search in identifying PTM in different samples. Results: We identified 63 ubiquitinated lysines from intact human cardiac 20S proteasomes. In parallel, 65 acetylated residues were also discovered, 39 of which shared with ubiquitination sites. Conclusion and clinical relevance: This is the most comprehensive characterization of cardiac proteasome ubiquitination to date. There are significant overlaps between the discovered ubiquitination and acetylation sites, permitting potential crosstalk in regulating proteasome functions. The information presented here will aid future therapeutic strategies aimed at regulating the functions of cardiac proteasomes.

Original languageEnglish (US)
Pages (from-to)590-594
Number of pages5
JournalProteomics - Clinical Applications
Volume8
Issue number7-8
DOIs
StatePublished - Aug 2014
Externally publishedYes

Keywords

  • 20S proteasome
  • Acetylation
  • PTM
  • Spectral library
  • Ubiquitination

ASJC Scopus subject areas

  • Clinical Biochemistry

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