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Determination of Optimal Sample Size for Quantification of β-Cell Area Amyloid Area and β-Cell Apoptosis in Isolated Islets

机译:确定定量胰岛中β-细胞面积淀粉样蛋白面积和β-细胞凋亡的最佳样本量

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摘要

Culture of isolated rodent islets is widely used in diabetes research to assess different endpoints, including outcomes requiring histochemical staining. As islet yields during isolation are limited, we determined the number of islets required to obtain reliable data by histology. We found that mean values for insulin-positive β-cell area/islet area, thioflavin S-positive amyloid area/islet area and β-cell apoptosis do not vary markedly when more than 30 islets are examined. Measurement variability declines as more islets are quantified, so that the variability of the coefficient of variation (CV) in human islet amyloid polypeptide (hIAPP) transgenic islets for β-cell area/islet area, amyloid area/islet area and β-cell apoptosis are 13.20% ± 1.52%, 10.03% ± 1.76% and 6.78% ± 1.53%, respectively (non-transgenic: 7.65% ± 1.17% β-cell area/islet area and 8.93% ± 1.56% β-cell apoptosis). Increasing the number of islets beyond 30 had marginal effects on the CV. Using 30 islets, 6 hIAPP-transgenic preparations are required to detect treatment effects of 14% for β-cell area/islet area, 30% for amyloid area/islet area and 23% for β-cell apoptosis (non-transgenic: 9% for β-cell area/islet area and 45% for β-cell apoptosis). This information will be of value in the design of studies using isolated islets to examine β cells and islet amyloid.
机译:分离的啮齿动物胰岛的培养被广泛用于糖尿病研究,以评估不同的终点,包括需要组织化学染色的结果。由于隔离过程中胰岛的产量有限,我们通过组织学确定了获得可靠数据所需的胰岛数量。我们发现,当检查超过30个胰岛时,胰岛素阳性β细胞面积/胰岛面积,硫代黄素S阳性淀粉样蛋白面积/胰岛面积和β细胞凋亡的平均值没有明显变化。随着更多胰岛的量化,测量变异性下降,因此人类胰岛淀粉样多肽(hIAPP)转基因胰岛中的变异系数(CV)对于β细胞面积/胰岛面积,淀粉样蛋白面积/胰岛面积和β细胞凋亡的变异性分别为13.20%±1.52%,10.03%±1.76%和6.78%±1.53%(非转基因:β细胞面积/胰岛面积为7.65%±1.17%和8.93%±1.56%细胞凋亡)。将胰岛数量增加到30以上会对CV产生边际影响。使用30个胰岛,需要6种hIAPP转基因制剂才能检测到治疗效果,分别为β细胞面积/胰岛面积14%,淀粉样蛋白区域/胰岛面积30%和β细胞凋亡23%(非转基因:9% β细胞面积/胰岛面积的百分比为45%(β细胞凋亡的百分比)。该信息在使用分离的胰岛检查β细胞和胰岛淀粉样蛋白的研究设计中具有价值。

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