Multiparameter phenotypic screening for endogenous TFEB and TFE3 translocation identifies novel chemical series modulating lysosome function

The accumulation of toxic protein aggregates in multiple neurodegenerative diseases is associated with defects in the macroautophagy/autophagy-lysosome pathway. The amelioration of disease phenotypes across multiple models of neurodegeneration can be achieved through modulating the master regulator...

Descripción completa

Detalles Bibliográficos
Autores principales: Carling, Phillippa J, Ryan, Brent J, McGuinness, William, Kataria, Shikha, Humble, Stewart W, Milde, Stefan, Duce, James A, Kapadia, Nirav, Zuercher, William J, Davis, John B., Di Daniel, Elena, Wade-Martins, Richard
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Taylor & Francis 2022
Materias:
Toolbox
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9851200/
https://www.ncbi.nlm.nih.gov/pubmed/35786165
http://dx.doi.org/10.1080/15548627.2022.2095834
_version_ 1784872355737108480
author Carling, Phillippa J
Ryan, Brent J
McGuinness, William
Kataria, Shikha
Humble, Stewart W
Milde, Stefan
Duce, James A
Kapadia, Nirav
Zuercher, William J
Davis, John B.
Di Daniel, Elena
Wade-Martins, Richard
author_facet Carling, Phillippa J
Ryan, Brent J
McGuinness, William
Kataria, Shikha
Humble, Stewart W
Milde, Stefan
Duce, James A
Kapadia, Nirav
Zuercher, William J
Davis, John B.
Di Daniel, Elena
Wade-Martins, Richard
author_sort Carling, Phillippa J
collection PubMed
description The accumulation of toxic protein aggregates in multiple neurodegenerative diseases is associated with defects in the macroautophagy/autophagy-lysosome pathway. The amelioration of disease phenotypes across multiple models of neurodegeneration can be achieved through modulating the master regulator of lysosome function, TFEB (transcription factor EB). Using a novel multi-parameter high-throughput screen for cytoplasmic:nuclear translocation of endogenous TFEB and the related transcription factor TFE3, we screened the Published Kinase Inhibitor Set 2 (PKIS2) library as proof of principle and to identify kinase regulators of TFEB and TFE3. Given that TFEB and TFE3 are responsive to cellular stress we have established assays for cellular toxicity and lysosomal function, critical to ensuring the identification of hit compounds with only positive effects on lysosome activity. In addition to AKT inhibitors which regulate TFEB localization, we identified a series of quinazoline-derivative compounds that induced TFEB and TFE3 translocation. A novel series of structurally-related analogs was developed, and several compounds induced TFEB and TFE3 translocation at higher potency than previously screened compounds. KINOMEscan and cell-based KiNativ kinase profiling revealed high binding for the PRKD (protein kinase D) family of kinases, suggesting good selectivity for these compounds. We describe and utilize a cellular target-validation platform using CRISPRi knockdown and orthogonal PRKD inhibitors to demonstrate that the activity of these compounds is independent of PRKD inhibition. The more potent analogs induced subsequent upregulation of the CLEAR gene network and cleared pathological HTT protein in a cellular model of proteinopathy, demonstrating their potential to alleviate neurodegeneration-relevant phenotypes. Abbreviations: AD: Alzheimer disease; AK: adenylate kinase; CLEAR: coordinated lysosomal expression and regulation; CQ: chloroquine; HD: Huntington disease; PD: Parkinson disease; PKIS2: Published Kinase Inhibitor Set 2; PRKD: protein kinase D; TFEB: transcription factor EB.
format Online
Article
Text
id pubmed-9851200
institution National Center for Biotechnology Information
language English
publishDate 2022
publisher Taylor & Francis
record_format MEDLINE/PubMed
spelling pubmed-98512002023-01-20 Multiparameter phenotypic screening for endogenous TFEB and TFE3 translocation identifies novel chemical series modulating lysosome function Carling, Phillippa J Ryan, Brent J McGuinness, William Kataria, Shikha Humble, Stewart W Milde, Stefan Duce, James A Kapadia, Nirav Zuercher, William J Davis, John B. Di Daniel, Elena Wade-Martins, Richard Autophagy Toolbox The accumulation of toxic protein aggregates in multiple neurodegenerative diseases is associated with defects in the macroautophagy/autophagy-lysosome pathway. The amelioration of disease phenotypes across multiple models of neurodegeneration can be achieved through modulating the master regulator of lysosome function, TFEB (transcription factor EB). Using a novel multi-parameter high-throughput screen for cytoplasmic:nuclear translocation of endogenous TFEB and the related transcription factor TFE3, we screened the Published Kinase Inhibitor Set 2 (PKIS2) library as proof of principle and to identify kinase regulators of TFEB and TFE3. Given that TFEB and TFE3 are responsive to cellular stress we have established assays for cellular toxicity and lysosomal function, critical to ensuring the identification of hit compounds with only positive effects on lysosome activity. In addition to AKT inhibitors which regulate TFEB localization, we identified a series of quinazoline-derivative compounds that induced TFEB and TFE3 translocation. A novel series of structurally-related analogs was developed, and several compounds induced TFEB and TFE3 translocation at higher potency than previously screened compounds. KINOMEscan and cell-based KiNativ kinase profiling revealed high binding for the PRKD (protein kinase D) family of kinases, suggesting good selectivity for these compounds. We describe and utilize a cellular target-validation platform using CRISPRi knockdown and orthogonal PRKD inhibitors to demonstrate that the activity of these compounds is independent of PRKD inhibition. The more potent analogs induced subsequent upregulation of the CLEAR gene network and cleared pathological HTT protein in a cellular model of proteinopathy, demonstrating their potential to alleviate neurodegeneration-relevant phenotypes. Abbreviations: AD: Alzheimer disease; AK: adenylate kinase; CLEAR: coordinated lysosomal expression and regulation; CQ: chloroquine; HD: Huntington disease; PD: Parkinson disease; PKIS2: Published Kinase Inhibitor Set 2; PRKD: protein kinase D; TFEB: transcription factor EB. Taylor & Francis 2022-07-25 /pmc/articles/PMC9851200/ /pubmed/35786165 http://dx.doi.org/10.1080/15548627.2022.2095834 Text en © 2022 The Author(s). Published by Informa UK Limited, trading as Taylor & Francis Group. https://creativecommons.org/licenses/by/4.0/This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0/ (https://creativecommons.org/licenses/by/4.0/) ), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Toolbox
Carling, Phillippa J
Ryan, Brent J
McGuinness, William
Kataria, Shikha
Humble, Stewart W
Milde, Stefan
Duce, James A
Kapadia, Nirav
Zuercher, William J
Davis, John B.
Di Daniel, Elena
Wade-Martins, Richard
Multiparameter phenotypic screening for endogenous TFEB and TFE3 translocation identifies novel chemical series modulating lysosome function
title Multiparameter phenotypic screening for endogenous TFEB and TFE3 translocation identifies novel chemical series modulating lysosome function
title_full Multiparameter phenotypic screening for endogenous TFEB and TFE3 translocation identifies novel chemical series modulating lysosome function
title_fullStr Multiparameter phenotypic screening for endogenous TFEB and TFE3 translocation identifies novel chemical series modulating lysosome function
title_full_unstemmed Multiparameter phenotypic screening for endogenous TFEB and TFE3 translocation identifies novel chemical series modulating lysosome function
title_short Multiparameter phenotypic screening for endogenous TFEB and TFE3 translocation identifies novel chemical series modulating lysosome function
title_sort multiparameter phenotypic screening for endogenous tfeb and tfe3 translocation identifies novel chemical series modulating lysosome function
topic Toolbox
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9851200/
https://www.ncbi.nlm.nih.gov/pubmed/35786165
http://dx.doi.org/10.1080/15548627.2022.2095834
work_keys_str_mv AT carlingphillippaj multiparameterphenotypicscreeningforendogenoustfebandtfe3translocationidentifiesnovelchemicalseriesmodulatinglysosomefunction
AT ryanbrentj multiparameterphenotypicscreeningforendogenoustfebandtfe3translocationidentifiesnovelchemicalseriesmodulatinglysosomefunction
AT mcguinnesswilliam multiparameterphenotypicscreeningforendogenoustfebandtfe3translocationidentifiesnovelchemicalseriesmodulatinglysosomefunction
AT katariashikha multiparameterphenotypicscreeningforendogenoustfebandtfe3translocationidentifiesnovelchemicalseriesmodulatinglysosomefunction
AT humblestewartw multiparameterphenotypicscreeningforendogenoustfebandtfe3translocationidentifiesnovelchemicalseriesmodulatinglysosomefunction
AT mildestefan multiparameterphenotypicscreeningforendogenoustfebandtfe3translocationidentifiesnovelchemicalseriesmodulatinglysosomefunction
AT ducejamesa multiparameterphenotypicscreeningforendogenoustfebandtfe3translocationidentifiesnovelchemicalseriesmodulatinglysosomefunction
AT kapadianirav multiparameterphenotypicscreeningforendogenoustfebandtfe3translocationidentifiesnovelchemicalseriesmodulatinglysosomefunction
AT zuercherwilliamj multiparameterphenotypicscreeningforendogenoustfebandtfe3translocationidentifiesnovelchemicalseriesmodulatinglysosomefunction
AT davisjohnb multiparameterphenotypicscreeningforendogenoustfebandtfe3translocationidentifiesnovelchemicalseriesmodulatinglysosomefunction
AT didanielelena multiparameterphenotypicscreeningforendogenoustfebandtfe3translocationidentifiesnovelchemicalseriesmodulatinglysosomefunction
AT wademartinsrichard multiparameterphenotypicscreeningforendogenoustfebandtfe3translocationidentifiesnovelchemicalseriesmodulatinglysosomefunction

Ejemplares similares