Role of Molecular Chaperonin CCT and Its Co-Chaperone PhLP1 in the Assembly of mTOR Complexes

Dhavale, Madhura Vinayak

01 August 2017

mTOR is the central kinase in biochemical pathways that regulate cellular growth, protein synthesis and cell survival. Deregulation of mTOR signaling results in uncontrolled cell proliferation and hence is implicated in various cancers and autoimmune diseases. mTOR functions through two distinct signaling complexes, called mTORC1 and mTORC2. CCT is a cytosolic chaperonin that assists in folding of several protein substrates. In these studies, we have identified two components of the mTOR complexes, mLST8 and Raptor, as substrates of CCT. We have performed biochemical and signaling studies which indicate that CCT is involved in assembly and signaling of mTOR complexes by folding β-propeller domains of mLST8 and Raptor. We have also obtained high resolution structural information of the mLST8-CCT complex by cryo-EM and mass spectrometric cross-linking. Moreover, we have explored the role of PhLP1 as a co-chaperone for CCT in the assembly of mTOR complexes. Interestingly, we found that PhLP1 plays very different roles in the case of mLST8 and Raptor. While PhLP1 participate in assembly of mLST8 into mTOR complexes, it facilitates degradation of Raptor. These biochemical data, combined with structural information, can be used to design small molecules that modulate mTOR signaling by affecting the formation of intact mTOR complexes.

mTOR

mLST8

Raptor

CCT

cryo-EM

Chaperones

Chemistry

Chaperone-Mediated Folding and Assembly of β-Propeller Proteins into Cellular Signaling Complexes

Plimpton, Rebecca L

01 December 2014

G protein signaling depends on the ability of the individual subunits of the G protein heterotrimer to assemble into a functional complex. Formation of the G protein βγ (Gβγ) dimer is particularly challenging because it is an obligate dimer in which the individual subunits are unstable on their own. Recent studies have revealed an intricate chaperone system that brings the Gβ and Gγ subunits together. This system includes the cytosolic chaperonin containing TCP-1 (CCT) and a co-chaperone phosducin-like protein 1 (PhLP1). Two key intermediates in the Gβγ assembly process, the Gβ-CCT and the PhLP1-Gβ-CCT complexes, were isolated and their structures determined by cryo-electron microscopy, chemical cross-linking coupled with mass spectrometry, and unnatural amino acid cross-linking. These structures show that Gβ interacts with CCT in a near-native state through interactions of the Gγ-binding region of Gβ with the CCTγ subunit. PhLP1 binding stabilizes the Gβ β-propeller, disrupting interactions with CCT and releasing a PhLP1-Gβ dimer for assembly with Gγ. We also investigated the role of CCT and PhLP1 in folding and assembling mTOR complexes, which regulate cell growth through phosphorylation. We found that the β-propeller protein mLST8 and one of its binding partners called raptor, which is a large protein in which one domain forms a β-propeller, both bind to CCT. PhLP1 forms a ternary complex with mLST8 and CCT and may play a co-chaperone role. Depletion of PhLP1 or CCT reduces assembly of mTOR complexes in the cell. Collectively, this report reveals diversity in the contributions of CCT to the formation of protein complexes in signaling pathways and presents a molecular mechanism of Gβ folding by CCT and PhLP1.

G protein

chaperone

PhLP1

mLST8

cryo-EM

cross-linking

XL-MS

Biochemistry

Chemistry