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Dopamine signalling in pancreatic islet cells and role in adaptations to metabolic stress.

J Pharm Pharmacol · 2024

Last updated 2026-05-28

In mice, a dopamine precursor called l-DOPA worsened blood sugar control and reduced insulin release triggered by glucose, a diabetes drug (exendin-4), and another nutrient (alanine). The study also found that diabetes or a high-fat diet increased the number of dopamine-producing cells in the pancreas, with some changes depending on the type of stress.

AI summary of the abstract below.

JournalJ Pharm Pharmacol, 2024
Citations3
Relative citation ratio0.80
NIH percentile43
Molecules
Conditions studied Type 2 Diabetes, Obesity

Abstract

OBJECTIVES: Dopamine and related receptors are evidenced in pancreatic endocrine tissue, but the impact on islet β-cell stimulus-secretion as well as (patho)physiological role are unclear. METHODS: The present study has evaluated islet cell signalling pathways and biological effects of dopamine, as well as alterations of islet dopamine in rodent models of diabetes of different aetiology. KEY FINDINGS: The dopamine precursor l-DOPA partially impaired glucose tolerance in mice and attenuated glucose-, exendin-4, and alanine-induced insulin secretion. The latter effect was echoed by the attenuation of glucose-induced [Ca2+]i dynamics and elevation of ATP levels in individual mouse islet cells. l-DOPA significantly decreased β-cell proliferation rates, acting predominantly via the D2 receptor, which was most abundant at the mRNA level. The administration of streptozotocin (STZ) or high-fat diet (HFD) in mice significantly elevated numbers of dopamine-positive islet cells, with HFD also increasing colocalization of dopamine with insulin. At the same time, colocalization of dopamine with glucagon was increased in STZ-treated and pregnant mice, but unaffected by HFD. CONCLUSION: These findings highlight a role for dopamine receptor signalling in islet cell biology adaptations to various forms of metabolic stress.

Verbatim abstract via PubMed 38652540 ↗