Molecular Determinants and Signaling Effects of PKA RIα Phase Separation

Author:

Hardy Julia C.ORCID,Pool Emily H.ORCID,Bruystens Jessica G.H.,Zhou Xin,Li Qingrong,Zhou Daojia R.,Palay Max,Tan Gerald,Chen Lisa,Choi Jaclyn L.C.,Lee Ha Neul,Strack StefanORCID,Wang Dong,Taylor Susan S.,Mehta Sohum,Zhang JinORCID

Abstract

ABSTRACTSpatiotemporal regulation of intracellular signaling molecules, such as the 3’,5’-cyclic adenosine monophosphate (cAMP)-dependent protein kinase (PKA), ensures the specific execution of various cellular functions. Liquid-liquid phase separation (LLPS) of the ubiquitously expressed PKA regulatory subunit RIα was recently identified as a major driver of cAMP compartmentation and signaling specificity. However, the molecular determinants of RIα LLPS remain unclear. Here, we reveal that two separate dimerization interfaces combined with the cAMP-induced release of the PKA catalytic subunit (PKA-C) from the pseudosubstrate inhibitory sequence are required to drive RIα condensate formation in cytosol, which is antagonized by docking to A-kinase anchoring proteins. Strikingly, we find that the RIα pseudosubstrate region is critically involved in the formation of a non-canonical R:C complex, which serves to maintain low basal PKA activity in the cytosol by enabling the recruitment of active PKA-C to RIα condensates. Our results suggest that RIα LLPS not only facilitates cAMP compartmentation but also spatially restrains active PKA-C, thus highlighting the functional versatility of biomolecular condensates in driving signaling specificity.

Publisher

Cold Spring Harbor Laboratory

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