胰岛细胞特异性敲除心钠肽受体鸟苷酸环化酶 A 加速肥胖诱导的小鼠葡萄糖不耐受。
β Cell-specific deletion of guanylyl cyclase A, the receptor for atrial natriuretic peptide, accelerates obesity-induced glucose intolerance in mice.
机构信息
Institute of Physiology, University of Würzburg, Röntgenring 9, 97070, Würzburg, Germany.
Department of Biotechnology and Biophysics, University of Würzburg, Am Hubland, 97074, Würzburg, Germany.
出版信息
Cardiovasc Diabetol. 2018 Jul 17;17(1):103. doi: 10.1186/s12933-018-0747-3.
BACKGROUND
The cardiac hormones atrial (ANP) and B-type natriuretic peptides (BNP) moderate arterial blood pressure and improve energy metabolism as well as insulin sensitivity via their shared cGMP-producing guanylyl cyclase-A (GC-A) receptor. Obesity is associated with impaired NP/GC-A/cGMP signaling, which possibly contributes to the development of type 2 diabetes and its cardiometabolic complications. In vitro, synthetic ANP, via GC-A, stimulates glucose-dependent insulin release from cultured pancreatic islets and β-cell proliferation. However, the relevance for systemic glucose homeostasis in vivo is not known. To dissect whether the endogenous cardiac hormones modulate the secretory function and/or proliferation of β-cells under (patho)physiological conditions in vivo, here we generated a novel genetic mouse model with selective disruption of the GC-A receptor in β-cells.
METHODS
Mice with a floxed GC-A gene were bred to Rip-Cre mice, thereby deleting GC-A selectively in β-cells (β GC-A KO). Weight gain, glucose tolerance, insulin sensitivity, and glucose-stimulated insulin secretion were monitored in normal diet (ND)- and high-fat diet (HFD)-fed mice. β-cell size and number were measured by immunofluorescence-based islet morphometry.
RESULTS
In vitro, the insulinotropic and proliferative actions of ANP were abolished in islets isolated from β GC-A KO mice. Concordantly, in vivo, infusion of BNP mildly enhanced baseline plasma insulin levels and glucose-induced insulin secretion in control mice. This effect of exogenous BNP was abolished in β GC-A KO mice, corroborating the efficient inactivation of the GC-A receptor in β-cells. Despite this under physiological, ND conditions, fasted and fed insulin levels, glucose-induced insulin secretion, glucose tolerance and β-cell morphology were similar in β GC-A KO mice and control littermates. However, HFD-fed β GC-A KO animals had accelerated glucose intolerance and diminished adaptative β-cell proliferation.
CONCLUSIONS
Our studies of β GC-A KO mice demonstrate that the cardiac hormones ANP and BNP do not modulate β-cell's growth and secretory functions under physiological, normal dietary conditions. However, endogenous NP/GC-A signaling improves the initial adaptative response of β-cells to HFD-induced obesity. Impaired β-cell NP/GC-A signaling in obese individuals might contribute to the development of type 2 diabetes.
背景
心脏激素心房(ANP)和 B 型利钠肽(BNP)通过其共同的 cGMP 产生鸟苷酸环化酶-A(GC-A)受体调节动脉血压并改善能量代谢和胰岛素敏感性。肥胖与 NP/GC-A/cGMP 信号转导受损有关,这可能导致 2 型糖尿病及其心血管代谢并发症的发生。在体外,合成的 ANP 通过 GC-A 刺激培养的胰岛和β细胞的葡萄糖依赖性胰岛素释放和增殖。然而,体内全身葡萄糖稳态的相关性尚不清楚。为了剖析内源性心脏激素是否在体内(病理)生理条件下调节β细胞的分泌功能和/或增殖,我们在此生成了一种新型遗传小鼠模型,该模型选择性地在β细胞中破坏 GC-A 受体。
方法
将带有 floxed GC-A 基因的小鼠与 Rip-Cre 小鼠交配,从而选择性地在β细胞中敲除 GC-A(β GC-A KO)。在正常饮食(ND)和高脂肪饮食(HFD)喂养的小鼠中监测体重增加、葡萄糖耐量、胰岛素敏感性和葡萄糖刺激的胰岛素分泌。通过基于免疫荧光的胰岛形态计量学测量β细胞大小和数量。
结果
在体外,ANP 的胰岛素促分泌和增殖作用在β GC-A KO 小鼠分离的胰岛中被消除。与此一致,在体内,BNP 的输注轻度增强了对照小鼠的基础血浆胰岛素水平和葡萄糖诱导的胰岛素分泌。在β GC-A KO 小鼠中,外源性 BNP 的这种作用被消除,证实了β细胞中 GC-A 受体的有效失活。尽管在生理、ND 条件下,空腹和进食后的胰岛素水平、葡萄糖诱导的胰岛素分泌、葡萄糖耐量和β细胞形态在β GC-A KO 小鼠和对照同窝仔鼠中相似。然而,HFD 喂养的β GC-A KO 动物的葡萄糖耐量加速受损,适应性β细胞增殖减少。
结论
我们对β GC-A KO 小鼠的研究表明,在生理、正常饮食条件下,心脏激素 ANP 和 BNP 不会调节β细胞的生长和分泌功能。然而,内源性 NP/GC-A 信号可改善β细胞对 HFD 诱导的肥胖的初始适应性反应。肥胖个体中β细胞 NP/GC-A 信号转导受损可能导致 2 型糖尿病的发生。
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