仓鼠胰腺癌模型胰岛激素分泌的早期变化。

J Permert, M Herrington, K Kazakoff, P M Pour, T E Adrian
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引用次数: 0

摘要

糖尿病常与胰腺癌相关,其特点是血浆中几种胰岛激素水平升高,并伴有明显的胰岛素抵抗。亚全胰切除术后糖尿病状态和胰岛素敏感性均有改善。在仓鼠胰腺癌模型中也发现糖耐量受损,但关于胰岛功能的数据相互矛盾。为了进一步研究胰腺癌早期发展过程中胰岛的功能和分泌,我们在使用导管细胞特异性致癌物BOP诱导肿瘤后12周和27周,测量了血浆、胰腺组织和分泌素刺激的胰岛淀粉样多肽(IAPP)的浓度。BOP后12周,血浆胰高血糖素水平显著升高。在BOP后27周,而不是12周,观察到夸张的血糖反应和伴随的高胰岛素血症。血浆IAPP浓度在27周时升高,但胰高血糖素或生长抑素没有升高。bop处理的仓鼠在27周时IAPP的组织浓度显著降低。在调查的两个时间点中,两组的胰液中激素浓度均无差异。研究表明,胰岛激素的变化伴随着仓鼠胰腺模型胰腺肿瘤的早期发展。激素变化和明显的胰岛素抵抗类似于胰腺癌患者的代谢变化。
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Early changes in islet hormone secretion in the hamster pancreatic cancer model.

The diabetic state that is seen at a high frequency in association with pancreatic cancer is characterized by elevated plasma levels of several islet hormones and by marked insulin resistance. Both the diabetic state and insulin sensitivity improve after tumor removal by sub-total pancreatectomy. Impaired glucose tolerance has also been found in the hamster pancreatic cancer model, but conflicting data regarding islet function have been reported. In order to further investigate islet function and secretion during early development of pancreatic cancer, we measured the concentrations of insulin, glucagon, somatostatin, and islet amyloid polypeptide (IAPP) in plasma, pancreatic tissue, and secretin-stimulated pancreatic juice at 12 and 27 weeks after the ductal-cell-specific carcinogen, BOP had been used to induce tumors in Syrian golden hamsters. At 12 weeks after BOP, plasma glucagon levels were significantly increased. An exaggerated plasma-glucose response and concomitant hyperinsulinemia were observed at 27 but not 12 weeks after BOP. Plasma IAPP concentrations, but not glucagon or somatostatin, were elevated at 27 weeks. Tissue concentrations of IAPP were substantially reduced in BOP-treated hamsters at 27 weeks. No differences in hormone concentrations were seen in pancreatic juice from the two groups at either of the two time points investigated. The study showed that islet hormone changes accompany the early development of pancreatic tumors in the hamster pancreatic model. The hormone changes and apparent insulin resistance resemble the metabolic changes found in humans with pancreatic cancer.

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