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首页> 外文期刊>Toxicologic pathology >Quantitative histopathological assessment of retardation of islets of Langerhans degeneration in rosiglitazone-dosed obese ZDF rats using combined insulin and collagens (I and III) immunohistochemistry with automated image analysis and statistical modeling
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Quantitative histopathological assessment of retardation of islets of Langerhans degeneration in rosiglitazone-dosed obese ZDF rats using combined insulin and collagens (I and III) immunohistochemistry with automated image analysis and statistical modeling

机译:使用组合胰岛素和胶原蛋白(I和III)免疫组化与自动图像分析和统计建模ranglitazoneedodeSzdF大鼠兰氏菌剂ZDF大鼠胰岛胰岛胰岛胰岛胰岛稀释性的定量组织病理学评估

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摘要

Islets of Langerhans represent a heterogeneous population in insulin resistant and diabetic animals and humans as histological appearances and function vary substantially. Mathematical representation that reflects this morphological diversity will assist in assessment of degeneration and regeneration, enabling comparisons between species, strains, and experimental investigations. Our investigative approach used a model of islet degeneration in diabetic male obese Zucker Diabetic Fatty (ZDF) rats and evaluated its prevention using rosiglitazone treatment. Immunohistochemical staining (insulin and collagens I/III) with automated image analysis reliably measured numbers, area, clustering, and staining intensity of β-cells and degree of islet fibrosis. Finite mixture mathematical modeling for the joint probability distribution of seven islet parameters to represent islet numerical data variation provided an automatic procedure for islet category allocations as normal or abnormal. Allocations for obese ZDF controls and rosiglitazone-treated animals were significantly different, with no significant difference between the latter and lean ZDF controls, indicative of differences within islet populations of individual animals, between lean and obese rat strains and following drug treatment. Islet morphology showed clear association with mathematical characterization. Information on islet morphology obtained by histopathological assessment of single pancreatic tissue sections was confirmed by this method showing drug-induced retardation of islet of Langerhans degeneration.
机译:Langerhans的胰岛代表了胰岛素抗性和糖尿病动物的异质人群,人类作为组织学外观和功能显着变化。反映这种形态多样性的数学表示将有助于评估退化和再生,从而能够在物种,菌株和实验研究之间进行比较。我们的调查方法使用了糖尿病雄性肥胖痘痘糖尿病脂肪(ZDF)大鼠的胰岛退化模型,并使用Rosiglitazone治疗评估预防。免疫组织化学染色(胰岛素和胶原I / III)具有自动图像分析,可靠地测量β-细胞的数量,面积,聚类和染色强度和胰岛纤维化程度。有限的混合物数学建模对于七个胰岛参数的联合概率分布,表示胰岛数值数据变化提供了胰岛类别分配的自动过程,正常或异常。肥胖ZDF对照和罗格列唑酮治疗的动物的分配显着不同,后者和瘦ZDF对照之间没有显着差异,表明瘦肉和肥胖大鼠菌株和药物治疗后胰岛素群体内的胰岛群体。胰岛素形态表现出明确的数学表征。通过该方法证实了通过单一胰腺组织切片的组织病理学评估获得的胰岛形态的信息,显示出含有药物诱导的朗格汉斯退化的胰岛胰岛素的延迟。

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