G protein-coupled receptor inhibition of beta-cell electrical excitability and insulin secretion depends on Na/K ATPase activation
Authors
Dickerson
MT
Matthew T
,
Dadi
PK
Prasanna K
,
Zaborska
KE
Karolina E
,
Nakhe
AY
Arya Y
,
Schaub
CM
Charles M
,
Dobson
JR
Jordyn R
,
Wright
NM
Nicole M
,
Lynch
JC
Joshua C
,
Scott
CF
Claire F
,
Robinson
LD
Logan D
,
Jacobson
DA
David A
.
Nature communications. 2022 10 29; 13(1).
6461
Nature communications. 2022 10 29; 13(1).
6461
Abstract
G-coupled somatostatin or α2-adrenergic receptor activation stimulated β-cell NKA activity, resulting in islet Ca fluctuations. Furthermore, intra-islet paracrine activation of β-cell G-GPCRs and NKAs by δ-cell somatostatin secretion slowed Ca oscillations, which decreased insulin secretion. β-cell membrane potential hyperpolarization resulting from G-GPCR activation was dependent on NKA phosphorylation by Src tyrosine kinases. Whereas, β-cell NKA function was inhibited by cAMP-dependent PKA activity. These data reveal that NKA-mediated β-cell membrane potential hyperpolarization is the primary and conserved mechanism for G-GPCR control of electrical excitability, Ca handling, and insulin secretion.