The Structure of the R2TP Complex Defines a Platform for Recruiting Diverse Client Proteins to the HSP90 Molecular Chaperone System

Rivera-Calzada, Ángel; Pal, Mohinder; Muñoz-Hernández, Hugo; Luque‐Ortega, Juan Román; Gil, David; Degliesposti, Gianluca; Skehel, J. Mark; Prodromou, Chrisostomos; Pearl, Laurence H.; Llorca, Óscar

doi:10.1016/j.str.2017.05.016

Cited by 51 publications

(89 citation statements)

References 40 publications

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“…The N-terminal PIH domain of Pih1p/PIH1D1 binds a CK2-phosphorylation motif on Tel2p/TELO2, mediating recruitment of the TTT complex to R2TP 2 , 3 . Most recently, we have determined the cryo-EM structure of the intact yeast R2TP complex, in which a single Tah1p–Pih1p sub-complex binds a heterohexameric Rvb1–Rvb2 ring 24 , a finding subsequently confirmed by others 25 . In metazoan R2TP, the small (12 kDa) single-TPR domain protein Tah1p is replaced by the much larger (75 kDa) RPAP3/hSpagh whose N-terminal half contains a tandem pair of TPR domains that bind in concert to a single HSP90 dimer 2 .…”

Section: Introductionsupporting

confidence: 59%

“…The TPR domain of yeast Tah1p mediates interaction with the conserved MEEVD C-terminal tail peptide of HSP90 2 , 19 – 22 , while its C-terminal extension couples Tah1p to the CS-domain of Pih1p 2 , 21 . The central region of Pih1p mediates recruitment of Pih1p–Tah1p to the Rvb1p–Rvb2p heterohexameric ring 23 , 24 . The N-terminal PIH domain of Pih1p/PIH1D1 binds a CK2-phosphorylation motif on Tel2p/TELO2, mediating recruitment of the TTT complex to R2TP 2 , 3 .…”

Section: Introductionmentioning

confidence: 99%

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RPAP3 provides a flexible scaffold for coupling HSP90 to the human R2TP co-chaperone complex

et al. 2018

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The R2TP/Prefoldin-like co-chaperone, in concert with HSP90, facilitates assembly and cellular stability of RNA polymerase II, and complexes of PI3-kinase-like kinases such as mTOR. However, the mechanism by which this occurs is poorly understood. Here we use cryo-EM and biochemical studies on the human R2TP core (RUVBL1–RUVBL2–RPAP3–PIH1D1) which reveal the distinctive role of RPAP3, distinguishing metazoan R2TP from the smaller yeast equivalent. RPAP3 spans both faces of a single RUVBL ring, providing an extended scaffold that recruits clients and provides a flexible tether for HSP90. A 3.6 Å cryo-EM structure reveals direct interaction of a C-terminal domain of RPAP3 and the ATPase domain of RUVBL2, necessary for human R2TP assembly but absent from yeast. The mobile TPR domains of RPAP3 map to the opposite face of the ring, associating with PIH1D1, which mediates client protein recruitment. Thus, RPAP3 provides a flexible platform for bringing HSP90 into proximity with diverse client proteins.

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Section: Introductionsupporting

confidence: 59%

Section: Introductionmentioning

confidence: 99%

RPAP3 provides a flexible scaffold for coupling HSP90 to the human R2TP co-chaperone complex

et al. 2018

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“…1C). These include seven of the eight members of the Hsp90-R2TP-TTT super-complex (Rivera-Calzada et al, 2017) and one of its target clients, Nipped-A (also known as TRRAP) (Fig. 1C,E).…”

Section: Morgana Interacts With the Hsp90-r2tp-ttt Super-complex And mentioning

confidence: 99%

Drosophila Morgana is an Hsp90-interacting protein with a direct role in microtubule polymerisation

Palumbo

Tariq

Borgal

et al. 2020

Journal of Cell Science

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Morgana (Mora, also known as CHORD in flies) and its mammalian homologue, called CHORDC1 or CHP1, is a highly conserved cysteine and histidine-rich domain (CHORD)-containing protein that has been proposed to function as an Hsp90 co-chaperone. Morgana deregulation promotes carcinogenesis in both mice and humans while, in Drosophila, loss of mora causes lethality and a complex mitotic phenotype that is rescued by a human morgana transgene. Here, we show that Drosophila Mora localises to mitotic spindles and co-purifies with the Hsp90-R2TP-TTT supercomplex and with additional well-known Hsp90 co-chaperones. Acute inhibition of Mora function in the early embryo results in a dramatic reduction in centrosomal microtubule stability, leading to small spindles nucleated from mitotic chromatin. Purified Mora binds to microtubules directly and promotes microtubule polymerisation in vitro, suggesting that Mora directly regulates spindle dynamics independently of its Hsp90 co-chaperone role.

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“…In various chromatin-remodeling complexes such as INO80 and SRCAP, these ATPases form a scaffold that organizes the architecture of other subunits in the complex (Aramayo et al, 2018;Eustermann et al, 2018;Feng et al, 2018). RUVBL1 and RUVBL2 also interact with RPAP3 and PIH1D1 proteins to form the R2TP complex, a HSP90 co-chaperone involved in the assembly and maturation of some large complexes including RNA polymerase II and members of the Phosphatidylinositol 3-kinase-related kinase (PIKK) family such as ATR, ATM, SMG1 and mTOR (Houry et al, 2018;Martino et al, 2018;Maurizy et al, 2018;Munoz-Hernandez et al, 2019;Rivera-Calzada et al, 2017). In all these complexes, the DIIface of the RUVBL1-RUVBL2 ring is used as scaffold platform for the interaction with other proteins, which are recruited by the DII domains.…”

Section: Introductionmentioning

confidence: 99%

Regulation of RUVBL1-RUVBL2 AAA-ATPases by the nonsense-mediated mRNA decay factor DHX34, as evidenced by Cryo-EM

López-Perrote

Hug

González-Corpas

et al. 2020

Preprint

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Nonsense-mediated mRNA decay (NMD) is a surveillance pathway that degrades aberrant mRNAs and also regulates the expression of a wide range of physiological transcripts. RUVBL1 and RUVBL2 AAA-ATPases form an hetero-hexameric ring that is part of several macromolecular complexes such as INO80, SWR1 and R2TP. Interestingly, RUVBL1-RUVBL2 ATPase activity is required for NMD activation by an unknown mechanism. Here, we show that DHX34, an RNA helicase regulating NMD initiation, directly interacts with RUVBL1-RUVBL2 in vitro and in cells. Cryo-EM reveals that DHX34 induces extensive changes in the N-termini of every RUVBL2 subunit in the complex, stabilizing a conformation that does not bind nucleotide and thereby down-regulates ATP hydrolysis of the complex. Using ATPase-deficient mutants, we find that DHX34 acts exclusively on the RUVBL2 subunits. We propose a model, where DHX34 acts to couple RUVBL1-RUVBL2 ATPase activity to the assembly of factors required to initiate the NMD response.

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The Structure of the R2TP Complex Defines a Platform for Recruiting Diverse Client Proteins to the HSP90 Molecular Chaperone System

Cited by 51 publications

References 40 publications

RPAP3 provides a flexible scaffold for coupling HSP90 to the human R2TP co-chaperone complex

RPAP3 provides a flexible scaffold for coupling HSP90 to the human R2TP co-chaperone complex

Drosophila Morgana is an Hsp90-interacting protein with a direct role in microtubule polymerisation

Regulation of RUVBL1-RUVBL2 AAA-ATPases by the nonsense-mediated mRNA decay factor DHX34, as evidenced by Cryo-EM

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