首页> 美国卫生研究院文献>Molecular Medicine >Amyloid formation in response to beta cell stress occurs in vitro but not in vivo in islets of transgenic mice expressing human islet amyloid polypeptide.
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Amyloid formation in response to beta cell stress occurs in vitro but not in vivo in islets of transgenic mice expressing human islet amyloid polypeptide.

机译:响应β细胞应激的淀粉样蛋白的形成发生在体外而不是体内在表达人胰岛淀粉样蛋白多肽的转基因小鼠的胰岛中发生。

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摘要

BACKGROUND: Human, but not mouse, islet amyloid polypeptide (IAPP) is amyloidogenic. Transgenic mice overexpressing human IAPP in the beta cells of the islets of Langerhans should be useful in identifying factors important for the deposition of IAPP as insoluble amyloid fibrils. MATERIALS AND METHODS: Transgenic mice expressing human IAPP were examined using several experimental models for the production of persistent hyperglycemia, as well as for the overstimulation and/or inhibition of beta cell secretion. Obesity was induced by aurothioglucose. Persistent hyperglycemia was produced by long-term administration of glucocorticosteroids or by partial pancreatectomy. Inhibition of normal beta cell exocytosis by diazoxide administration, with or without concurrent dexamethasone injections, was carried out to increase crinophagy of secretory granules. The human IAPP gene was also introduced into the ab and ob mouse models for diabetes. Finally, isolated islets cultivated in vitro at high glucose concentration were also examined. RESULTS: No amyloid deposits were found in the pancreata of any of the animals, either by light microscopy after Congo red staining or by electron microscopy after immunogold labeling with antibodies specific for human IAPP. Aurothioglucose treatment resulted in increased numbers of granules in the beta cell and the appearance of large lysosomal bodies without amyloid. However, islets from db and ob mice expressing human IAPP cultivated in vitro in the presence of glucocorticosteroid and/or growth hormone, were found to contain extracellular amyloid deposits reacting with antibodies to human IAPP. CONCLUSIONS: Oversecretion of human IAPP or increased crinophagy are not sufficient for amyloid formation. This indicates that other factors must influence amyloid deposition; one such factor may be the local clearance of IAPP.
机译:背景:人类而非小鼠的胰岛淀粉样多肽(IAPP)具有淀粉样原性。在朗格罕岛的胰岛β细胞中过表达人IAPP的转基因小鼠可用于鉴定对于IAPP沉积为不溶性淀粉样原纤维的重要因素。材料和方法:使用几种实验模型检查了表达人IAPP的转基因小鼠的持续性高血糖的产生,以及对β细胞分泌的过度刺激和/或抑制。肥胖是由金硫葡糖引起的。长期服用糖皮质激素或部分胰腺切除术可产生持续性高血糖症。通过有或没有同时地塞米松注射的二氮嗪给药抑制正常β细胞胞吐作用,以增加分泌颗粒的吞噬作用。人的IAPP基因也被引入了糖尿病的ab和ob小鼠模型中。最后,还检查了体外以高葡萄糖浓度培养的胰岛。结果:通过刚果红染色后的光学显微镜或免疫金标记人IAPP抗体后的电子显微镜,在任何动物的胰腺中均未发现淀粉样蛋白沉积。硫代葡萄糖处理导致β细胞中颗粒数量增加,并且出现了没有淀粉样蛋白的较大溶酶体。但是,发现在存在糖皮质激素和/或生长激素的条件下体外培养表达人IAPP的db和ob小鼠的胰岛含有与人IAPP抗体反应的细胞外淀粉样蛋白沉积物。结论:人IAPP的过度分泌或增加的吞噬作用不足以形成淀粉样蛋白。这表明其他因素也必须影响淀粉样蛋白的沉积。此类因素之一可能是IAPP的当地许可。

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