Presenilin-1 controls glucose metabolism and identity of pancreatic beta cells

Zhanat Koshenov
Sandra Postic
Gabriela Schosiwohl
Savina van Amsterdam
Victoria Hois-Zelinka
Furkan E. Oflaz
Rene Rost
Oleksandra Tiapko
Benjamin Gottschalk
Martin Hirtl
Olaf G. Bachkoenig
Aigerim Koshenova
Yusuf C. Erdogan
Adlet Sagintayev
Anita Krnjic
Johannes U. Pfabe
Srdjan Sarikas
Bernhard Hochreiter
Juergen Gindlhuber
Matthias Schittmayer
Jelena Tadic
Barbara Ehall
Frank Madeo
Tobias Madl
Roland Malli
Ruth Birner-Gruenberger
Thomas Pieber
Tobias Eisenberg
Marjan Slak Rupnik
Wolfgang F. Graier

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Abstract

Presenilin 1 is an endoplasmic reticulum protein, most known for its role in pathogenesis of familial Alzheimer’s Disease (AD). Presenilin 1 has been attributed roles in intracellular calcium homeostasis in the brain, as well as in the pancreatic beta cells, where it has been shown to be fundamental for glucose-induced insulin secretion. Functional similarity of presenilin 1 in regulation of intracellular calcium homeostasis in the brain and pancreas prompted us to investigate a prevalent assumption that associates AD and diabetes mellitus. By examining pancreatic islets from AD model mice, we have found deficits in initial phase of glucose-induced calcium signaling and insulin secretion. Furthermore, these transgenic mice showed a tendency towards reduced expression of mature beta cell markers, which was even more pronounced in islets and beta cell lines with a transient knock down of presenilin 1. We demonstrate here that presenilin 1 controls beta cell glycolysis by regulating sub-cellular calcium homeostasis and, in doing so, contributes to preservation of beta cell identity.

Version published to 10.1101/2025.09.05.674426 on bioRxiv
Sep 5, 2025

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