β-cell insulin resistance plays a causal role in fat-induced β-cell dysfunction in vitro and in vivo

Endocrinology. 2024 Apr 5:bqae044. doi: 10.1210/endocr/bqae044. Online ahead of print.ABSTRACTIn the classical insulin target tissues liver, muscle and adipose tissue, chronically elevated levels of free fatty acids (FFA) impair insulin signaling. Insulin signaling molecules are also present in β-cells where they play a role in β-cell function. Therefore, inhibition of the insulin/IGF-1 pathway may be involved in fat-induced β-cell dysfunction. To address the role of β-cell insulin resistance in FFA-induced β-cell dysfunction we co-infused bisperoxovanadate (BPV) with oleate or olive oil for 48 h in rats. BPV, a tyrosine phosphatase inhibitor, acts as an insulin mimetic and is devoid of any antioxidant effect that could prevent β-cell dysfunction, unlike most insulin sensitizers. Following fat infusion, rats either underwent hyperglycemic clamps for assessment of β-cell function in vivo or islets were isolated for ex vivo assessment of glucose-stimulated insulin secretion (GSIS). We also incubated islets with oleate or palmitate and BPV for in vitro assessment of GSIS and Akt phosphorylation. Next, mice with β-cell specific deletion of PTEN (negative regulator of insulin signaling) and littermate controls were infused with oleate for 48 h, followed by hyperglycemic clamps or ex vivo evaluation of GSIS. In rat experiments, BPV protected against fat-induced impairment of β-cell function in vivo, ex vivo and in vitro. In mice, β-cell specific deletion of PTEN protected...
Source: Endocrinology - Category: Endocrinology Authors: Source Type: research