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Publication : Organization and dynamics of the cortical complexes controlling insulin secretion in β-cells.

First Author  Noordstra I Year  2022
Journal  J Cell Sci Volume  135
Issue  3 PubMed ID  35006275
Mgi Jnum  J:325465 Mgi Id  MGI:7278948
Doi  10.1242/jcs.259430 Citation  Noordstra I, et al. (2022) Organization and dynamics of the cortical complexes controlling insulin secretion in beta-cells. J Cell Sci 135(3):jcs259430
abstractText  Insulin secretion in pancreatic beta-cells is regulated by cortical complexes that are enriched at the sites of adhesion to extracellular matrix facing the vasculature. Many components of these complexes, including bassoon, RIM, ELKS and liprins, are shared with neuronal synapses. Here, we show that insulin secretion sites also contain the non-neuronal proteins LL5beta (also known as PHLDB2) and KANK1, which, in migrating cells, organize exocytotic machinery in the vicinity of integrin-based adhesions. Depletion of LL5beta or focal adhesion disassembly triggered by myosin II inhibition perturbed the clustering of secretory complexes and attenuated the first wave of insulin release. Although previous analyses in vitro and in neurons have suggested that secretory machinery might assemble through liquid-liquid phase separation, analysis of endogenously labeled ELKS in pancreatic islets indicated that its dynamics is inconsistent with such a scenario. Instead, fluorescence recovery after photobleaching and single-molecule imaging showed that ELKS turnover is driven by binding and unbinding to low-mobility scaffolds. Both the scaffold movements and ELKS exchange were stimulated by glucose treatment. Our findings help to explain how integrin-based adhesions control spatial organization of glucose-stimulated insulin release.
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