Islet Biology Laboratory, Centre for Biomolecular Interactions Bremen 28355, University of Bremen, Leobener Strasse NW2, Rm. B2080, 28359 Bremen, Germany.
J Biol Chem. 2011 May 13;286(19):17144-55. doi: 10.1074/jbc.M110.210526. Epub 2011 Mar 10.
The transcription factor PDX1 plays a critical role during β-cell development and in glucose-induced insulin gene transcription in adult β-cells. Acute glucose exposure leads to translocalization of PDX1 to the nucleoplasm, whereas under conditions of oxidative stress, PDX1 shuttles from the nucleus to the cytosol. Here we show that cytosolic PDX1 expression correlated with β-cell failure in diabetes. In isolated islets from patients with type 2 diabetes and from diabetic mice, we found opposite regulation of insulin and PDX1 mRNA; insulin was decreased in diabetes, but PDX1 was increased. This suggests that elevated PDX1 mRNA levels may be insufficient to regulate insulin. In diabetic islets, PDX1 protein was localized in the cytosol, whereas in non-diabetic controls, PDX1 was in the nucleus. In contrast, overexpression of either IL-1 receptor antagonist or shuttling-deficient PDX1 restored β-cell survival and function and PDX1 nuclear localization. Our results show that nuclear localization of PDX1 is essential for a functional β-cell and provides a novel mechanism of the protective effect of IL-1 receptor antagonist on β-cell survival and function.
转录因子 PDX1 在 β 细胞发育和成人 β 细胞葡萄糖诱导胰岛素基因转录中发挥关键作用。急性葡萄糖暴露导致 PDX1 向核质转位,而在氧化应激条件下,PDX1 从核穿梭到细胞质。在这里,我们表明细胞质 PDX1 表达与糖尿病中的 β 细胞衰竭相关。在来自 2 型糖尿病患者和糖尿病小鼠的分离胰岛中,我们发现胰岛素和 PDX1 mRNA 的相反调节;在糖尿病中胰岛素减少,但 PDX1 增加。这表明升高的 PDX1 mRNA 水平可能不足以调节胰岛素。在糖尿病胰岛中,PDX1 蛋白位于细胞质中,而在非糖尿病对照中,PDX1 位于核内。相比之下,IL-1 受体拮抗剂的过表达或穿梭缺陷 PDX1 的过表达恢复了 β 细胞的存活和功能,并使 PDX1 核定位。我们的结果表明,PDX1 的核定位对于功能性 β 细胞是必不可少的,并提供了 IL-1 受体拮抗剂对 β 细胞存活和功能的保护作用的新机制。
