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瘦素在非肥胖糖尿病小鼠和CD-1小鼠胰岛中的免疫组织化学显示:在胰高血糖素细胞中的共定位及其在糖尿病发病时的减弱。

Immunohistochemical demonstration of leptin in pancreatic islets of non-obese diabetic and CD-1 mice: co-localization in glucagon cells and its attenuation at the onset of diabetes.

作者信息

Reddy S, Lau E M, Ross J M

机构信息

School of Biological Sciences, Department of Paediatrics, University of Auckland, Auckland, New Zealand.

出版信息

J Mol Histol. 2004 Jun;35(5):511-9. doi: 10.1023/b:hijo.0000045963.10002.4b.

Abstract

Leptin is a 16 kD polypeptide hormone produced predominantly by white adipose tissue and exerts profound effects on food intake and energy balance. More recent studies have shown extra sites of leptin production in human and rodent tissues and have ascribed additional roles for the hormone, e.g., in immune and reproductive functions. A role for the hormone has also been implicated in insulin-dependent diabetes mellitus in the non-obese diabetic (NOD) mouse. However, whether leptin originates from islet cells of the mouse is not known. Here dual-label immunohistochemistry was employed to examine leptin expression in islet cells, and its distribution and cellular sources in pancreatic sections of female NOD/Ak and CD-1 mice of various ages. For comparison, leptin immunolabelling was examined in adult pancreatic sections from male NOD/Ak CD-1, Balb/c and FVB/N mice and female severe combined immunodeficient CB. 17 mice. Pancreatic tissues from adult female guinea pig, sheep and cattle and neonatal pigs were also studied. Our results show that in the day 1 NOD and CD-1 mice, leptin immunolabelling was observed in selective glucagon cells within the developing islets while at days 15 and 22, it became more intense and co-incident. This pattern of staining was maintained at days 40, 90, 150 and 250. In the female NOD mouse, leptin was absent in intra-islet immune cells. Its expression was variable in islets from male NOD and CD-1 mice. In spontaneously diabetic female NOD mice and following acceleration of diabetes with cyclophosphamide, despite the persistence of strong immunolabelling for glucagon in the re-distributed alpha cells, leptin expression was either absent, diminished or present in only a proportion of alpha cells. The reduction in leptin labelling was often associated with diabetic islets which had insulitis in association with only a small number of residual beta cells. Leptin expression was absent in guinea pig, ovine, bovine and neonatal porcine islet cells, despite the expression of intensely labelled glucagon cells. The present results demonstrate leptin co-localization in glucagon cells of the mouse islet. Its expression diminishes in the presence of inadequate insulin. Leptin produced within the mouse islet may have bi-directional influences on leptin and insulin regulation and may play local functions in islet development and metabolism.

摘要

瘦素是一种主要由白色脂肪组织产生的16 kD多肽激素,对食物摄入和能量平衡具有深远影响。最近的研究表明,在人类和啮齿动物组织中存在瘦素产生的额外部位,并赋予了该激素其他作用,例如在免疫和生殖功能方面。该激素在非肥胖糖尿病(NOD)小鼠的胰岛素依赖型糖尿病中也被认为发挥了作用。然而,瘦素是否源自小鼠的胰岛细胞尚不清楚。在此,采用双重免疫组织化学方法检查瘦素在胰岛细胞中的表达,以及其在不同年龄的雌性NOD/Ak和CD-1小鼠胰腺切片中的分布和细胞来源。作为比较,在成年雄性NOD/Ak CD-1、Balb/c和FVB/N小鼠以及雌性严重联合免疫缺陷CB.17小鼠的胰腺切片中检查瘦素免疫标记。还研究了成年雌性豚鼠、绵羊和牛以及新生猪的胰腺组织。我们的结果表明,在出生第1天的NOD和CD-1小鼠中,在发育中的胰岛内的选择性胰高血糖素细胞中观察到瘦素免疫标记,而在第15天和第22天,其变得更加明显且同时出现。这种染色模式在第40、90、150和250天得以维持。在雌性NOD小鼠中,胰岛内免疫细胞中不存在瘦素。其在雄性NOD和CD-1小鼠的胰岛中的表达存在差异。在自发糖尿病雌性NOD小鼠以及用环磷酰胺加速糖尿病进程后,尽管重新分布的α细胞中胰高血糖素的强免疫标记持续存在,但瘦素表达要么缺失、减少,要么仅在一部分α细胞中存在。瘦素标记的减少通常与伴有少量残余β细胞的胰岛炎的糖尿病胰岛相关。尽管存在强烈标记的胰高血糖素细胞的表达,但在豚鼠、绵羊、牛和新生猪的胰岛细胞中不存在瘦素表达。目前的结果证明瘦素在小鼠胰岛的胰高血糖素细胞中共定位。在胰岛素不足的情况下其表达减少。小鼠胰岛内产生的瘦素可能对瘦素和胰岛素调节具有双向影响,并可能在胰岛发育和代谢中发挥局部作用。

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