Unraveling Verapamil's Multidimensional Role in Diabetes Therapy: From β-Cell Regeneration to Cholecystokinin Induction in Zebrafish and MIN6 Cell-Line Models

揭示维拉帕米在糖尿病治疗中的多维作用:从β细胞再生到斑马鱼和MIN6细胞系模型中的胆囊收缩素诱导

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作者:Hossein Arefanian ,Ashraf Al Madhoun ,Fatema Al-Rashed ,Fawaz Alzaid ,Fatemah Bahman ,Rasheeba Nizam ,Mohammed Alhusayan ,Sumi John ,Sindhu Jacob ,Michayla R Williams ,Nermeen Abukhalaf ,Steve Shenouda ,Shibu Joseph ,Halemah AlSaeed ,Shihab Kochumon ,Anwar Mohammad ,Lubaina Koti ,Sardar Sindhu ,Mohamed Abu-Farha ,Jehad Abubaker ,Thangavel Alphonse Thanaraj ,Rasheed Ahmad ,Fahd Al-Mulla

Abstract

This study unveils verapamil's compelling cytoprotective and proliferative effects on pancreatic β-cells amidst diabetic stressors, spotlighting its unforeseen role in augmenting cholecystokinin (CCK) expression. Through rigorous investigations employing MIN6 β-cells and zebrafish models under type 1 and type 2 diabetic conditions, we demonstrate verapamil's capacity to significantly boost β-cell proliferation, enhance glucose-stimulated insulin secretion, and fortify cellular resilience. A pivotal revelation of our research is verapamil's induction of CCK, a peptide hormone known for its role in nutrient digestion and insulin secretion, which signifies a novel pathway through which verapamil exerts its therapeutic effects. Furthermore, our mechanistic insights reveal that verapamil orchestrates a broad spectrum of gene and protein expressions pivotal for β-cell survival and adaptation to immune-metabolic challenges. In vivo validation in a zebrafish larvae model confirms verapamil's efficacy in fostering β-cell recovery post-metronidazole infliction. Collectively, our findings advocate for verapamil's reevaluation as a multifaceted agent in diabetes therapy, highlighting its novel function in CCK upregulation alongside enhancing β-cell proliferation, glucose sensing, and oxidative respiration. This research enriches the therapeutic landscape, proposing verapamil not only as a cytoprotector but also as a promoter of β-cell regeneration, thereby offering fresh avenues for diabetes management strategies aimed at preserving and augmenting β-cell functionality. Keywords: MIN6 cells; calcium channel blocker; diabetes mellitus; verapamil; zebrafish; β-cells.

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