| Literature DB >> 27720452 |
Erik McShane1, Celine Sin2, Henrik Zauber1, Jonathan N Wells3, Neysan Donnelly4, Xi Wang1, Jingyi Hou1, Wei Chen1, Zuzana Storchova5, Joseph A Marsh3, Angelo Valleriani2, Matthias Selbach6.
Abstract
Do young and old protein molecules have the same probability to be degraded? We addressed this question using metabolic pulse-chase labeling and quantitative mass spectrometry to obtain degradation profiles for thousands of proteins. We find that >10% of proteins are degraded non-exponentially. Specifically, proteins are less stable in the first few hours of their life and stabilize with age. Degradation profiles are conserved and similar in two cell types. Many non-exponentially degraded (NED) proteins are subunits of complexes that are produced in super-stoichiometric amounts relative to their exponentially degraded (ED) counterparts. Within complexes, NED proteins have larger interaction interfaces and assemble earlier than ED subunits. Amplifying genes encoding NED proteins increases their initial degradation. Consistently, decay profiles can predict protein level attenuation in aneuploid cells. Together, our data show that non-exponential degradation is common, conserved, and has important consequences for complex formation and regulation of protein abundance.Entities:
Keywords: aneuploidy; bioorthogonal amino acid tagging; gene copy-number alterations; metabolic labeling; posttranslational control; protein complex assembly; protein degradation; proteomics; pulse chase experiment; trisomy
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Year: 2016 PMID: 27720452 DOI: 10.1016/j.cell.2016.09.015
Source DB: PubMed Journal: Cell ISSN: 0092-8674 Impact factor: 41.582