Insulin granule morphology and crinosome formation in mice lacking the pancreatic β cell-specific phogrin (PTPRN2) gene
We recently reported that phogrin, also known as IA-2β or PTPRN2, forms a complex with the insulin receptor in pancreatic β cells upon glucose stimulation and stabilizes insulin receptor substrate 2. In β cells of systemic phogrin gene knockout ( IA-2β −/− ) mice, impaired glucose-induced insulin se...
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Veröffentlicht in: | Histochemistry and cell biology 2024-03, Vol.161 (3), p.223-238 |
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Sprache: | eng |
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Zusammenfassung: | We recently reported that phogrin, also known as IA-2β or PTPRN2, forms a complex with the insulin receptor in pancreatic β cells upon glucose stimulation and stabilizes insulin receptor substrate 2. In β cells of systemic phogrin gene knockout (
IA-2β
−/−
) mice, impaired glucose-induced insulin secretion, decreased insulin granule density, and an increase in the number and size of lysosomes have been reported. Since phogrin is expressed not only in β cells but also in various neuroendocrine cells, the precise impact of phogrin expressed in β cells on these cells remains unclear. In this study, we performed a comprehensive analysis of morphological changes in
RIP-Cre
+/−
Phogrin
flox/flox
(
βKO
) mice with β cell-specific phogrin gene knockout. Compared to control
RIP-Cre
+/−
Phogrin
+
/
+
(
Ctrl
) mice, aged
βKO
mice exhibited a decreased density of insulin granules, which can be categorized into three subtypes. While no differences were observed in the density and size of lysosomes and crinosomes, organelles involved in insulin granule reduction, significant alterations in the regions of lysosomes responding positively to carbohydrate labeling were evident in young
βKO
mice. These alterations differed from those in
Ctrl
mice and continued to change with age. These electron microscopic findings suggest that phogrin expression in pancreatic β cells plays a role in insulin granule homeostasis and crinophagy during aging, potentially through insulin autocrine signaling and other mechanisms. |
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ISSN: | 0948-6143 1432-119X |
DOI: | 10.1007/s00418-023-02256-8 |