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Transgenic Wuzhishan minipigs designed to express a dominant-negative porcine growth hormone receptor display small stature and a perturbed insulin/IGF-1 pathway

机译:设计用于表达显性负性猪生长激素受体的转基因五指山小型猪显示身材矮小和胰岛素/ IGF-1通路受干扰

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摘要

Growth hormone (GH) is an anabolic mitogen with widespread influence on cellular growth and differentiation as well as on glucose and lipid metabolism. GH binding to the growth hormone receptor (GHR) on hepatocytes prompts expression of insulin growth factor I (IGF-1) involved in nutritionally induced compensatory hyperplasia of pancreatic beta-cell islets and insulin release. A prolonged hyperactivity of the IGF-1/insulin axis in the face of insulinotropic nutrition, on the other hand, can lead to collapse of the pancreatic islets and glucose intolerance. Individuals with Laron syndrome carry mutations in the GHR gene resulting in severe congenital IGF-1 deficiency and elevated GH serum levels leading to short stature as well as perturbed lipid and glucose metabolism. However, these individuals enjoy a reduced prevalence of acne, cancer and possibly diabetes. Minipigs have become important biomedical models for human conditions due to similarities in organ anatomy, physiology, and metabolism relative to humans. The purpose of this study was to generate transgenic Wuzhishan minipigs by handmade cloning with impaired systemic GHR activity and assess their growth profile and glucose metabolism. Transgenic minipigs featuring overexpression of a dominant-negative porcine GHR (GHR(dm)) presented postnatal growth retardation and proportionate dwarfism. Molecular changes included elevated GH serum levels and mild hyperglycemia. We believe that this model may prove valuable in the study of GH functions in relation to cancer, diabetes and longevity.
机译:生长激素(GH)是一种合成代谢有丝分裂剂,对细胞的生长和分化以及葡萄糖和脂质代谢具有广泛的影响。 GH与肝细胞上的生长激素受体(GHR)的结合促使胰岛素生长因子I(IGF-1)的表达参与了营养诱导的胰岛β细胞胰岛代偿性增生和胰岛素释放。另一方面,面对促胰岛素营养,IGF-1 /胰岛素轴的过度活跃会导致胰岛的崩溃和葡萄糖耐受不良。患有Laron综合征的人在GHR基因中携带突变,导致严重的先天性IGF-1缺乏症和GH血清水平升高,导致身材矮小以及脂质和葡萄糖代谢紊乱。但是,这些人的痤疮,癌症和可能的糖尿病患病率降低。由于相对于人类的器官解剖结构,生理学和新陈代谢的相似性,小型猪已成为人类疾病的重要生物医学模型。这项研究的目的是通过手工克隆产生转基因的五指山小型猪,其系统性GHR活性受损,并评估其生长特性和葡萄糖代谢。以显性阴性猪GHR(GHR(dm))高表达为特征的转基因迷你猪表现出出生后发育迟缓和成比例的侏儒症。分子变化包括GH血清水平升高和轻度高血糖症。我们认为,该模型在与癌症,糖尿病和长寿有关的GH功能研究中可能被证明是有价值的。

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