GLP-1 suppresses glucagon secretion in human pancreatic alpha-cells by inhibition of P/Q-type Ca2+ channels

Reshma Ramracheya; Caroline Chapman; Margarita Chibalina; Haiqiang Dou; Caroline Miranda; Alejandro González; Yusuke Moritoh; Makoto Shigeto; Quan Zhang; Matthias Braun; Anne Clark; Paul R Johnson; Patrik Rorsman; Linford J B Briant

doi:10.14814/phy2.13852

GLP-1 suppresses glucagon secretion in human pancreatic alpha-cells by inhibition of P/Q-type Ca²⁺ channels

Physiol Rep. 2018 Sep;6(17):e13852. doi: 10.14814/phy2.13852.

Authors

Reshma Ramracheya¹, Caroline Chapman¹, Margarita Chibalina¹, Haiqiang Dou², Caroline Miranda², Alejandro González¹, Yusuke Moritoh¹, Makoto Shigeto¹, Quan Zhang¹, Matthias Braun¹, Anne Clark¹, Paul R Johnson^{3

4}, Patrik Rorsman^{1

2

4}, Linford J B Briant^{1

5}

Affiliations

¹ Oxford Centre for Diabetes, Endocrinology and Metabolism, Radcliffe Department of Medicine, University of Oxford, Oxford, United Kingdom.
² Institute of Neuroscience and Physiology, Metabolic Research Unit, University of Göteborg, Göteborg, Sweden.
³ Nuffield Department of Surgery, University of Oxford, John Radcliffe Hospital, Oxford, United Kingdom.
⁴ NIHR Oxford Biomedical Research Centre, Oxford, United Kingdom.
⁵ Department of Computer Science, University of Oxford, Oxford, United Kingdom.

Abstract

Glucagon is the body's main hyperglycemic hormone, and its secretion is dysregulated in type 2 diabetes mellitus (T2DM). The incretin hormone glucagon-like peptide-1 (GLP-1) is released from the gut and is used in T2DM therapy. Uniquely, it both stimulates insulin and inhibits glucagon secretion and thereby lowers plasma glucose levels. In this study, we have investigated the action of GLP-1 on glucagon release from human pancreatic islets. Immunocytochemistry revealed that only <0.5% of the α-cells possess detectable GLP-1R immunoreactivity. Despite this, GLP-1 inhibited glucagon secretion by 50-70%. This was due to a direct effect on α-cells, rather than paracrine signaling, because the inhibition was not reversed by the insulin receptor antagonist S961 or the somatostatin receptor-2 antagonist CYN154806. The inhibitory effect of GLP-1 on glucagon secretion was prevented by the PKA-inhibitor Rp-cAMPS and mimicked by the adenylate cyclase activator forskolin. Electrophysiological measurements revealed that GLP-1 decreased action potential height and depolarized interspike membrane potential. Mathematical modeling suggests both effects could result from inhibition of P/Q-type Ca²⁺ channels. In agreement with this, GLP-1 and ω-agatoxin (a blocker of P/Q-type channels) inhibited glucagon secretion in islets depolarized by 70 mmol/L [K⁺ ]_o , and these effects were not additive. Intracellular application of cAMP inhibited depolarization-evoked exocytosis in individual α-cells by a PKA-dependent (Rp-cAMPS-sensitive) mechanism. We propose that inhibition of glucagon secretion by GLP-1 involves activation of the few GLP-1 receptors present in the α-cell membrane. The resulting small elevation of cAMP leads to PKA-dependent inhibition of P/Q-type Ca²⁺ channels and suppression of glucagon exocytosis.

Keywords: GLP-1, glucagon-like peptide 1; KATP, potassium ATP channel; SST, somatostatin; T2DM, Type 2 diabetes mellitus; cAMP, cyclic adenosine monophosphate.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Adult
Animals
Calcium Channel Blockers / pharmacology
Calcium Channels, P-Type / metabolism*
Calcium Channels, Q-Type / metabolism*
Cells, Cultured
Exocytosis
Female
Glucagon / metabolism*
Glucagon-Like Peptide 1 / pharmacology*
Glucagon-Secreting Cells / drug effects
Glucagon-Secreting Cells / metabolism*
Glucagon-Secreting Cells / physiology
Humans
Male
Membrane Potentials
Mice
Middle Aged

Substances

Calcium Channel Blockers
Calcium Channels, P-Type
Calcium Channels, Q-Type
Glucagon-Like Peptide 1
Glucagon

Abstract

Publication types

MeSH terms

Substances

Grants and funding