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Clinically applicable GABA receptor positive allosteric modulators promote ß-cell replication

机译:临床上可应用的GABA受体阳性变构调节剂促进ß细胞复制

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摘要

A key goal of diabetes research is to develop treatments to safely promote human ß-cell replication. It has recently become appreciated that activation of γ-aminobutyric acid receptors (GABA-Rs) on ß-cells can promote their survival and replication. A number of positive allosteric modulators (PAMs) that enhance GABA’s actions on neuronal GABAA-Rs are in clinical use. Repurposing these GABAA-R PAMs to help treat diabetes is theoretically appealing because of their safety and potential to enhance the ability of GABA, secreted from ß-cells, or exogenously administered, to promote ß-cell replication and survival. Here, we show that clinically applicable GABAA-R PAMs can increase significantly INS-1 ß-cell replication, which is enhanced by exogenous GABA application. Furthermore, a GABAA-R PAM promoted human islet cell replication in vitro. This effect was abrogated by a GABAA-R antagonist. The combination of a PAM and low levels of exogenous GABA further increased human islet cell replication. These findings suggest that PAMs may potentiate the actions of GABA secreted by islet ß-cells on GABAA-Rs and provide a new class of drugs for diabetes treatment. Finally, our findings may explain a past clinical observation of a GABAA-R PAM reducing HbA1c levels in diabetic patients.
机译:糖尿病研究的一个关键目标是开发能够安全促进人ß细胞复制的疗法。最近已经认识到,β细胞上的γ-氨基丁酸受体(GABA-Rs)的激活可以促进其存活和复制。临床上正在使用许多能增强GABA对神经元GABAA-R作用的正性变构调节剂(PAM)。重新使用这些GABAA-R PAM来帮助治疗糖尿病在理论上很有吸引力,因为它们的安全性和潜力可以增强从ß细胞分泌或外源给药的GABA促进ß细胞复制和存活的能力。在这里,我们表明临床上可应用的GABAA-R PAM可以显着增加INS-1ß细胞的复制,而外源GABA的应用可以增强这种复制。此外,GABAA-R PAM在体外促进人胰岛细胞复制。 GABAA-R拮抗剂消除了这种作用。 PAM和低水平的外源性GABA的组合进一步提高了人类胰岛细胞的复制。这些发现表明,PAMs可能增强胰岛β细胞分泌的GABA在GABAA-Rs上的作用,并为糖尿病治疗提供一类新的药物。最后,我们的发现可能解释了GABAA-R PAM降低糖尿病患者HbA1c水平的以往临床观察。

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