Pervasive Protein Thermal Stability Variation during the Cell Cycle
Author(s) -
Isabelle Becher,
Amparo AndrésPons,
Natalie Romanov,
Frank Stein,
Maike Schramm,
Florence Baudin,
Dominic Helm,
Nils Kurzawa,
André Mateus,
MarieTherese Mackmull,
Athanasios Typas,
Christoph W. Müller,
Peer Bork,
Martin Beck,
Mikhail M. Savitski
Publication year - 2018
Publication title -
cell
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 26.304
H-Index - 776
eISSN - 1097-4172
pISSN - 0092-8674
DOI - 10.1016/j.cell.2018.03.053
Subject(s) - biology , variation (astronomy) , cell cycle , protein stability , cell cycle protein , microbiology and biotechnology , stability (learning theory) , evolutionary biology , cell , genetics , physics , machine learning , astrophysics , computer science
Quantitative mass spectrometry has established proteome-wide regulation of protein abundance and post-translational modifications in various biological processes. Here, we used quantitative mass spectrometry to systematically analyze the thermal stability and solubility of proteins on a proteome-wide scale during the eukaryotic cell cycle. We demonstrate pervasive variation of these biophysical parameters with most changes occurring in mitosis and G1. Various cellular pathways and components vary in thermal stability, such as cell-cycle factors, polymerases, and chromatin remodelers. We demonstrate that protein thermal stability serves as a proxy for enzyme activity, DNA binding, and complex formation in situ. Strikingly, a large cohort of intrinsically disordered and mitotically phosphorylated proteins is stabilized and solubilized in mitosis, suggesting a fundamental remodeling of the biophysical environment of the mitotic cell. Our data represent a rich resource for cell, structural, and systems biologists interested in proteome regulation during biological transitions.
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