Local activation of focal adhesion kinase orchestrates the positioning of presynaptic scaffold proteins and Ca2+ signalling to control glucose-dependent insulin secretion

Author:

Jevon Dillon1,Deng Kylie1ORCID,Hallahan Nicole1,Kumar Krish1,Tong Jason1ORCID,Gan Wan Jun1,Tran Clara2,Bilek Marcela234,Thorn Peter1ORCID

Affiliation:

1. Charles Perkins Centre, School of Medical Sciences, University of Sydney

2. School of Physics, University of Sydney

3. School of Aerospace, Mechanical and Mechatronic Engineering, University of Sydney

4. Sydney Nanoscience Institute, University of Sydney

Abstract

A developing understanding suggests that spatial compartmentalisation in pancreatic β cells is critical in controlling insulin secretion. To investigate the mechanisms, we have developed live-cell subcellular imaging methods using the mouse organotypic pancreatic slice. We demonstrate that the organotypic pancreatic slice, when compared with isolated islets, preserves intact β-cell structure, and enhances glucose-dependent Ca2+ responses and insulin secretion. Using the slice technique, we have discovered the essential role of local activation of integrins and the downstream component, focal adhesion kinase (FAK), in regulating β cells. Integrins and FAK are exclusively activated at the β-cell capillary interface and using in situ and in vitro models we show their activation both positions presynaptic scaffold proteins, like ELKS and liprin, and regulates glucose-dependent Ca2+ responses and insulin secretion. We conclude that FAK orchestrates the final steps of glucose-dependent insulin secretion within the restricted domain where β-cell contact the islet capillaries.

Funder

National Health and Medical Research Council

Sydney Medical School

Diabetes Australia Research Trust

Australian Research Council

Publisher

eLife Sciences Publications, Ltd

Subject

General Immunology and Microbiology,General Biochemistry, Genetics and Molecular Biology,General Medicine,General Neuroscience

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