Extended regulation interface coupled to the allosteric network and disease mutations in the PP2A-B56δ holoenzyme

An increasing number of mutations associated with devastating human diseases are diagnosed by whole-genome/exon sequencing. Recurrent de novo missense mutations have been discovered in B56δ (encoded by PPP2R5D), a regulatory subunit of protein phosphatase 2A (PP2A), that cause intellectual disabilit...

Descripción completa

Detalles Bibliográficos
Autores principales: Wu, Cheng-Guo, Balakrishnan, Vijaya K., Parihar, Pankaj S., Konovolov, Kirill, Chen, Yu-Chia, Merrill, Ronald A, Wei, Hui, Carragher, Bridget, Sundaresan, Ramya, Cui, Qiang, Wadzinski, Brian E., Swingle, Mark R., Musiyenko, Alla, Honkanen, Richard, Chung, Wendy K., Suzuki, Aussie, Strack, Stefan, Huang, Xuhui, Xing, Yongna
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Cold Spring Harbor Laboratory 2023
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10103954/
https://www.ncbi.nlm.nih.gov/pubmed/37066309
http://dx.doi.org/10.1101/2023.03.09.530109
_version_ 1785025948220915712
author Wu, Cheng-Guo
Balakrishnan, Vijaya K.
Parihar, Pankaj S.
Konovolov, Kirill
Chen, Yu-Chia
Merrill, Ronald A
Wei, Hui
Carragher, Bridget
Sundaresan, Ramya
Cui, Qiang
Wadzinski, Brian E.
Swingle, Mark R.
Musiyenko, Alla
Honkanen, Richard
Chung, Wendy K.
Suzuki, Aussie
Strack, Stefan
Huang, Xuhui
Xing, Yongna
author_facet Wu, Cheng-Guo
Balakrishnan, Vijaya K.
Parihar, Pankaj S.
Konovolov, Kirill
Chen, Yu-Chia
Merrill, Ronald A
Wei, Hui
Carragher, Bridget
Sundaresan, Ramya
Cui, Qiang
Wadzinski, Brian E.
Swingle, Mark R.
Musiyenko, Alla
Honkanen, Richard
Chung, Wendy K.
Suzuki, Aussie
Strack, Stefan
Huang, Xuhui
Xing, Yongna
author_sort Wu, Cheng-Guo
collection PubMed
description An increasing number of mutations associated with devastating human diseases are diagnosed by whole-genome/exon sequencing. Recurrent de novo missense mutations have been discovered in B56δ (encoded by PPP2R5D), a regulatory subunit of protein phosphatase 2A (PP2A), that cause intellectual disabilities (ID), macrocephaly, Parkinsonism, and a broad range of neurological symptoms. Single-particle cryo-EM structures show that the PP2A-B56δ holoenzyme possesses closed latent and open active forms. In the closed form, the long, disordered arms of B56δ termini fold against each other and the holoenzyme core, establishing dual autoinhibition of the phosphatase active site and the substrate-binding protein groove. The resulting interface spans over 190 Å and harbors unfavorable contacts, activation phosphorylation sites, and nearly all residues with ID-associated mutations. Our studies suggest that this dynamic interface is close to an allosteric network responsive to activation phosphorylation and altered globally by mutations. Furthermore, we found that ID mutations perturb the activation phosphorylation rates, and the severe variants significantly increase the mitotic duration and error rates compared to the wild variant.
format Online
Article
Text
id pubmed-10103954
institution National Center for Biotechnology Information
language English
publishDate 2023
publisher Cold Spring Harbor Laboratory
record_format MEDLINE/PubMed
spelling pubmed-101039542023-04-15 Extended regulation interface coupled to the allosteric network and disease mutations in the PP2A-B56δ holoenzyme Wu, Cheng-Guo Balakrishnan, Vijaya K. Parihar, Pankaj S. Konovolov, Kirill Chen, Yu-Chia Merrill, Ronald A Wei, Hui Carragher, Bridget Sundaresan, Ramya Cui, Qiang Wadzinski, Brian E. Swingle, Mark R. Musiyenko, Alla Honkanen, Richard Chung, Wendy K. Suzuki, Aussie Strack, Stefan Huang, Xuhui Xing, Yongna bioRxiv Article An increasing number of mutations associated with devastating human diseases are diagnosed by whole-genome/exon sequencing. Recurrent de novo missense mutations have been discovered in B56δ (encoded by PPP2R5D), a regulatory subunit of protein phosphatase 2A (PP2A), that cause intellectual disabilities (ID), macrocephaly, Parkinsonism, and a broad range of neurological symptoms. Single-particle cryo-EM structures show that the PP2A-B56δ holoenzyme possesses closed latent and open active forms. In the closed form, the long, disordered arms of B56δ termini fold against each other and the holoenzyme core, establishing dual autoinhibition of the phosphatase active site and the substrate-binding protein groove. The resulting interface spans over 190 Å and harbors unfavorable contacts, activation phosphorylation sites, and nearly all residues with ID-associated mutations. Our studies suggest that this dynamic interface is close to an allosteric network responsive to activation phosphorylation and altered globally by mutations. Furthermore, we found that ID mutations perturb the activation phosphorylation rates, and the severe variants significantly increase the mitotic duration and error rates compared to the wild variant. Cold Spring Harbor Laboratory 2023-04-05 /pmc/articles/PMC10103954/ /pubmed/37066309 http://dx.doi.org/10.1101/2023.03.09.530109 Text en https://creativecommons.org/licenses/by-nc-nd/4.0/This work is licensed under a Creative Commons Attribution-NonCommercial-NoDerivatives 4.0 International License (https://creativecommons.org/licenses/by-nc-nd/4.0/) , which allows reusers to copy and distribute the material in any medium or format in unadapted form only, for noncommercial purposes only, and only so long as attribution is given to the creator.
spellingShingle Article
Wu, Cheng-Guo
Balakrishnan, Vijaya K.
Parihar, Pankaj S.
Konovolov, Kirill
Chen, Yu-Chia
Merrill, Ronald A
Wei, Hui
Carragher, Bridget
Sundaresan, Ramya
Cui, Qiang
Wadzinski, Brian E.
Swingle, Mark R.
Musiyenko, Alla
Honkanen, Richard
Chung, Wendy K.
Suzuki, Aussie
Strack, Stefan
Huang, Xuhui
Xing, Yongna
Extended regulation interface coupled to the allosteric network and disease mutations in the PP2A-B56δ holoenzyme
title Extended regulation interface coupled to the allosteric network and disease mutations in the PP2A-B56δ holoenzyme
title_full Extended regulation interface coupled to the allosteric network and disease mutations in the PP2A-B56δ holoenzyme
title_fullStr Extended regulation interface coupled to the allosteric network and disease mutations in the PP2A-B56δ holoenzyme
title_full_unstemmed Extended regulation interface coupled to the allosteric network and disease mutations in the PP2A-B56δ holoenzyme
title_short Extended regulation interface coupled to the allosteric network and disease mutations in the PP2A-B56δ holoenzyme
title_sort extended regulation interface coupled to the allosteric network and disease mutations in the pp2a-b56δ holoenzyme
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10103954/
https://www.ncbi.nlm.nih.gov/pubmed/37066309
http://dx.doi.org/10.1101/2023.03.09.530109
work_keys_str_mv AT wuchengguo extendedregulationinterfacecoupledtotheallostericnetworkanddiseasemutationsinthepp2ab56dholoenzyme
AT balakrishnanvijayak extendedregulationinterfacecoupledtotheallostericnetworkanddiseasemutationsinthepp2ab56dholoenzyme
AT pariharpankajs extendedregulationinterfacecoupledtotheallostericnetworkanddiseasemutationsinthepp2ab56dholoenzyme
AT konovolovkirill extendedregulationinterfacecoupledtotheallostericnetworkanddiseasemutationsinthepp2ab56dholoenzyme
AT chenyuchia extendedregulationinterfacecoupledtotheallostericnetworkanddiseasemutationsinthepp2ab56dholoenzyme
AT merrillronalda extendedregulationinterfacecoupledtotheallostericnetworkanddiseasemutationsinthepp2ab56dholoenzyme
AT weihui extendedregulationinterfacecoupledtotheallostericnetworkanddiseasemutationsinthepp2ab56dholoenzyme
AT carragherbridget extendedregulationinterfacecoupledtotheallostericnetworkanddiseasemutationsinthepp2ab56dholoenzyme
AT sundaresanramya extendedregulationinterfacecoupledtotheallostericnetworkanddiseasemutationsinthepp2ab56dholoenzyme
AT cuiqiang extendedregulationinterfacecoupledtotheallostericnetworkanddiseasemutationsinthepp2ab56dholoenzyme
AT wadzinskibriane extendedregulationinterfacecoupledtotheallostericnetworkanddiseasemutationsinthepp2ab56dholoenzyme
AT swinglemarkr extendedregulationinterfacecoupledtotheallostericnetworkanddiseasemutationsinthepp2ab56dholoenzyme
AT musiyenkoalla extendedregulationinterfacecoupledtotheallostericnetworkanddiseasemutationsinthepp2ab56dholoenzyme
AT honkanenrichard extendedregulationinterfacecoupledtotheallostericnetworkanddiseasemutationsinthepp2ab56dholoenzyme
AT chungwendyk extendedregulationinterfacecoupledtotheallostericnetworkanddiseasemutationsinthepp2ab56dholoenzyme
AT suzukiaussie extendedregulationinterfacecoupledtotheallostericnetworkanddiseasemutationsinthepp2ab56dholoenzyme
AT strackstefan extendedregulationinterfacecoupledtotheallostericnetworkanddiseasemutationsinthepp2ab56dholoenzyme
AT huangxuhui extendedregulationinterfacecoupledtotheallostericnetworkanddiseasemutationsinthepp2ab56dholoenzyme
AT xingyongna extendedregulationinterfacecoupledtotheallostericnetworkanddiseasemutationsinthepp2ab56dholoenzyme

Ejemplares similares