Pharmacologic and genetic approaches define human pancreatic β cell mitogenic targets of DYRK1A inhibitors.

Adolescent Adult Aged Cell Proliferation / drug effects Female Gene Expression Glycogen Synthase Kinase 3 / genetics Harmine / metabolism Humans Insulin-Secreting Cells / metabolism Insulinoma Male Middle Aged Mitogens / metabolism Phosphorylation Protein Kinase Inhibitors / pharmacology Protein Serine-Threonine Kinases / drug effects Protein-Tyrosine Kinases / drug effects Young Adult Dyrk Kinases

Beta cells Diabetes Endocrinology Metabolism

Journal

JCI insight

ISSN: 2379-3708

Titre abrégé: JCI Insight

Pays: United States

ID NLM: 101676073

Informations de publication

Date de publication:
16 01 2020

Historique:

received: 13 08 2019

accepted: 04 12 2019

pubmed: 11 12 2019

medline: 11 5 2021

entrez: 11 12 2019

Statut: epublish

Résumé

Small molecule inhibitors of dual specificity, tyrosine phosphorylation-regulated kinase 1A (DYRK1A), including harmine and others, are able to drive human β cell regeneration. While DYRK1A is certainly a target of this class, whether it is the only or the most important target is uncertain. Here, we employ a combined pharmacologic and genetic approach to refine the potential mitogenic targets of the DYRK1A inhibitor family in human islets. A combination of human β cell RNA sequencing, DYRK1A inhibitor kinome screens, pharmacologic inhibitors, and targeted silencing of candidate genes confirms that DYRK1A is a central target. Surprisingly, however, DYRK1B also proves to be an important target: silencing DYRK1A results in an increase in DYRK1B. Simultaneous silencing of both DYRK1A and DYRK1B yields greater β cell proliferation than silencing either individually. Importantly, other potential kinases, such as the CLK and the GSK3 families, are excluded as important harmine targets. Finally, we describe adenoviruses that are able to silence up to 7 targets simultaneously. Collectively, we report that inhibition of both DYRK1A and DYRK1B is required for induction of maximal rates of human β cell proliferation, and we provide clarity for future efforts in structure-based drug design for human β cell regenerative drugs.

Identifiants

DOI: 10.1172/jci.insight.132594 PMID: 31821176 PMC: PMC7030849

pubmed: 31821176

pii: 132594

doi: 10.1172/jci.insight.132594

pmc: PMC7030849

doi:

pii:

Substances chimiques

Mitogens 0

Protein Kinase Inhibitors 0

Harmine 4FHH5G48T7

Protein-Tyrosine Kinases EC 2.7.10.1

Protein Serine-Threonine Kinases EC 2.7.11.1

Glycogen Synthase Kinase 3 EC 2.7.11.26

Types de publication

Journal Article Research Support, N.I.H., Extramural Research Support, Non-U.S. Gov't

Langues

eng

Sous-ensembles de citation

Subventions

Organisme : NIDDK NIH HHS

ID : R01 DK116904

Pays : United States

Organisme : NIDDK NIH HHS

ID : R01 DK116873

Pays : United States

Organisme : NIDDK NIH HHS

ID : U24 DK098085

Pays : United States

Organisme : NIDDK NIH HHS

ID : P30 DK020541

Pays : United States

Organisme : NIDDK NIH HHS

ID : R01 DK105015

Pays : United States

Organisme : NIDDK NIH HHS

ID : UC4 DK104211

Pays : United States

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Pharmacologic and genetic approaches define human pancreatic β cell mitogenic targets of DYRK1A inhibitors.

Journal

Informations de publication

Résumé

Identifiants

Substances chimiques

Types de publication

Langues

Sous-ensembles de citation

Subventions

Références

Auteurs

Courtney Ackeifi (C)

Ethan Swartz (E)

Kunal Kumar (K)

Hongtao Liu (H)

Suebsuwong Chalada (S)

Esra Karakose (E)

Donald K Scott (DK)

Adolfo Garcia-Ocaña (A)

Roberto Sanchez (R)

Robert J DeVita (RJ)

Andrew F Stewart (AF)

Peng Wang (P)

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Classifications MeSH