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首页> 外文期刊>American Journal of Pathology: Official Publication of the American Association of Pathologists >Pancreatic and Islet Remodeling in Cystic Fibrosis Transmembrane Conductance Regulator (CFTR) Knockout Ferrets
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Pancreatic and Islet Remodeling in Cystic Fibrosis Transmembrane Conductance Regulator (CFTR) Knockout Ferrets

机译:囊性和胰岛重塑在囊性纤维化跨膜电导调节器(CFTR)敲除雪貂

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In cystic fibrosis (CF), there is early destruction of the exocrine pancreas, and this results in a unique form of diabetes that affects approximately half of adult CF individuals. An animal model of cystic fibrosis-related diabetes has been developed in the ferret, which progresses through phases of glycemic abnormalities because of islet remodeling during and after exocrine destruction. Herein, we quantified the pancreatic histopathological changes that occur during these phases. There was an increase in percentage ductal, fat, and islet area in CF ferrets over time compared with age-matched wild-type controls. We also quantified islet size, shape, islet cell composition, cell proliferation (Ki-67), and expression of remodeling markers (matrix metalloprotease-7, desmin, and a-smooth muscle actin). Pancreatic ducts were dilated with scattered proliferating cells and were surrounded by activated stellate cells, indicative of tissue remodeling. The timing of islet and duct proliferation, stellate cell activation, and matrix remodeling coincided with the previously published stages of glycemic crisis and inflammation. This mapping of remodeling events in the CF ferret pancreas provides insights into early changes that control glycemic intolerance and subsequent recovery during the evolution of CF pancreatic disease.
机译:在囊性纤维化(CF)中,外分泌胰腺早期破坏,这导致独特的糖尿病形式,这些糖尿病会影响成人CF个体的一半。在雪貂中开发了一种囊性纤维化相关糖尿病的动物模型,其通过血糖异常的阶段进行了血糖异常的阶段,因为在外分泌破坏期间和之后的胰岛重塑。在此,我们量化了在这些阶段发生的胰腺组织病理学变化。与年龄匹配的野生型对照相比,CF雪貂中的导管百分比,脂肪和胰岛面积增加。我们还量化了胰岛尺寸,形状,胰岛细胞组合物,细胞增殖(Ki-67)和重塑标记物的表达(基质金属蛋白酶-7,Desmin和A-平滑肌肌动蛋白)。用散射增殖细胞扩张胰管,并被活化的星状细胞包围,指示组织重塑。胰岛和管道增殖,星状细胞活化和基质重塑的时序与先前公布的血糖危机和炎症的阶段吻合。 CF雪貂胰腺中重塑事件的这种映射提供了对在CF胰腺疾病演变期间控制血糖不耐受和随后恢复的早期变化的见解。

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