TY - JOUR
T1 - Pharmacoproteomics pinpoints HSP70 interaction for correction of the most frequent Wilson disease-causing mutant of ATP7B
AU - Concilli, Mafalda
AU - Petruzzelli, Raffaella
AU - Parisi, Silvia
AU - Catalano, Federico
AU - Sirci, Francesco
AU - Napolitano, Francesco
AU - Renda, Mario
AU - Galietta, Luis J.
AU - Di Bernardo, Diego
AU - Polishchuk, Roman S.
N1 - KAUST Repository Item: Exported on 2021-07-14
Acknowledgements: We thank Cathal Wilson for critical reading of the manuscript and acknowledge support from Telethon Institute of Genetics and Medicine bioinformatics and microscopy cores. This work was funded by Telethon, Italy, Grant TIGEM-CBDM9 (to R.S.P.); Consiglio Nazionale delle Ricerche/Russian Foundation for Basic Research Collaboration Program, Italy- Russia Grant 18-515-7811; PRIN-2017 (2017CH4RNP) (to S.P.); the Wilson Disease Association; Associazione Nazionale Malattia di Wilson; and a Veronesi Foundation Fellowship (to R.P.).
PY - 2020
Y1 - 2020
N2 - Pathogenic mutations in the copper transporterATP7Bhave been hypothesized to affect its protein interaction landscape contributing to loss of function and, thereby, to hepatic copper toxicosis in Wilson disease. Although targeting mutant interactomes was proposed as a therapeutic strategy, druggable interactors for rescue of ATP7B mutants remain elusive. Using proteomics, we found that the frequent H1069Q substitution promotes ATP7B interaction with HSP70, thus accelerating endoplasmic reticulum (ER) degradation of the mutant protein and consequent copper accumulation in hepatic cells. This prompted us to use an HSP70 inhibitor as bait in a bioinformatics search for structurally similar Food and Drug Administration-approved drugs. Among the hits, domperidone emerged as an effective corrector that recovered trafficking and function of ATP7B-H1069Q by impairing its exposure to the HSP70 proteostatic network. Our findings suggest that HSP70-mediated degradation can be safely targeted with domperidone to rescue ER-retained ATP7B mutants and, hence, to counter the onset of Wilson disease.
AB - Pathogenic mutations in the copper transporterATP7Bhave been hypothesized to affect its protein interaction landscape contributing to loss of function and, thereby, to hepatic copper toxicosis in Wilson disease. Although targeting mutant interactomes was proposed as a therapeutic strategy, druggable interactors for rescue of ATP7B mutants remain elusive. Using proteomics, we found that the frequent H1069Q substitution promotes ATP7B interaction with HSP70, thus accelerating endoplasmic reticulum (ER) degradation of the mutant protein and consequent copper accumulation in hepatic cells. This prompted us to use an HSP70 inhibitor as bait in a bioinformatics search for structurally similar Food and Drug Administration-approved drugs. Among the hits, domperidone emerged as an effective corrector that recovered trafficking and function of ATP7B-H1069Q by impairing its exposure to the HSP70 proteostatic network. Our findings suggest that HSP70-mediated degradation can be safely targeted with domperidone to rescue ER-retained ATP7B mutants and, hence, to counter the onset of Wilson disease.
UR - http://hdl.handle.net/10754/670173
UR - http://www.pnas.org/lookup/doi/10.1073/pnas.2006648117
UR - http://www.scopus.com/inward/record.url?scp=85098173281&partnerID=8YFLogxK
U2 - 10.1073/pnas.2006648117
DO - 10.1073/pnas.2006648117
M3 - Article
C2 - 33288711
SN - 0027-8424
VL - 117
SP - 32453
EP - 32463
JO - PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA
JF - PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA
IS - 51
ER -