Proteome-wide solubility and thermal stability profiling reveals distinct regulatory roles for ATP

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作者
Sindhuja Sridharan
Nils Kurzawa
Thilo Werner
Ina Günthner
Dominic Helm
Wolfgang Huber
Marcus Bantscheff
Mikhail M. Savitski
机构
[1] Genome Biology Unit,
[2] European Molecular Biology Laboratory,undefined
[3] Cellzome,undefined
[4] A GSK company,undefined
[5] Candidate for joint PhD degree from EMBL and Heidelberg University,undefined
[6] Faculty of Biosciences,undefined
[7] Proteomics Core Facility,undefined
[8] European Molecular Biology Laboratory,undefined
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Adenosine triphosphate (ATP) plays fundamental roles in cellular biochemistry and was recently discovered to function as a biological hydrotrope. Here, we use mass spectrometry to interrogate ATP-mediated regulation of protein thermal stability and protein solubility on a proteome-wide scale. Thermal proteome profiling reveals high affinity interactions of ATP as a substrate and as an allosteric modulator that has widespread influence on protein complexes and their stability. Further, we develop a strategy for proteome-wide solubility profiling, and discover ATP-dependent solubilization of at least 25% of the insoluble proteome. ATP increases the solubility of positively charged, intrinsically disordered proteins, and their susceptibility for solubilization varies depending on their localization to different membrane-less organelles. Moreover, a few proteins, exhibit an ATP-dependent decrease in solubility, likely reflecting polymer formation. Our data provides a proteome-wide, quantitative insight into how ATP influences protein structure and solubility across the spectrum of physiologically relevant concentrations.
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