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Functional and morphological study of cultured pancreatic islets treated with cyclosporine

机译:环孢菌素处理的胰岛的功能和形态研究

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Cyclosporine A (CsA)., a potent immunosuppressive drug, has been found to induce glucose intolerance through its toxic effect on the endocrine pancreas. It is not exactly known whether CsA has a direct effect on the endocrine pancreas or induces its effect indirectly. The present study was therefore undertaken to examine the function and morphology of isolated pancreatic islets when they are directly exposed in vitro to CsA. Pancreatic islets were isolated from adult male Lewis rats using collagenase ductal perfusion technique. The islets were separated with the discontinuous Ficoll gradient technique and further purified by hand picking of the non-islet tissue. The islets were cultured in RPMI-1640, pH 7.4 and maintained at 37 癈 in a humid atmosphere of 5% (v/v) carbon dioxide in air. Cyclosporine was added to the culture medium to give a final concentration of 1 jig/ml (therapeutic dose), 5 jig/ml (toxic dose), or vehicle (control). Islets were harvested at 1, 4 and 10 days of culture and processed for functional or histological study. The functional study of the islets cultured with 1 fig/ml CsA showed insulin and C-peptide contents similar to those of the control islets. The islets cultured with 5 ug/ml CsA showed a marked decrease in insulin and C-peptide contents. Glucose-dependent insulin release was variable. C-peptide release was lower than that of the control following both the therapeutic and toxic doses of CsA. Phase contrast microscopy showed that the islets cultured with 1mug/ml CsA were mostly normal looking with a well-defined regular periphery; a few islets had ill-defined or irregular peripheries. The islets cultured with 5 ug/ml CsA had ill-defined irregular peripheries at 1 day, and were dense and forming clumps at 4 and 10 days following culture. There was a decrease in the islet number following the therapeutic dose; the decrease was more following the toxic dose of CsA. The islet diameters increased after the therapeutic dose, but slightly decreased following the toxic dose of CsA. Islets showed a weakly positive immunoperoxidase reaction for insulin that was weaker following the toxic dose of CsA. It is concluded that CsA has a direct effect on B-cells that was proved by the functional and morphological changes seen in the pancreatic islets cultured in vitro. 500B-cells; C-peptide; Culture; Cycfosporine; Histology; Immunohistochemistry; Insulin; Islets of Langerhans; Morphology; Pancreas; Rat
机译:已经发现环孢菌素A(CsA)是一种有效的免疫抑制药物,它通过对内分泌胰腺的毒性作用诱导葡萄糖耐受不良。尚不清楚CsA对内分泌胰腺有直接作用还是间接引起其作用。因此,进行本研究以检查分离的胰岛在体外直接暴露于CsA时的功能和形态。使用胶原酶导管灌注技术从成年雄性Lewis大鼠中分离出胰岛。用不连续的Ficoll梯度技术分离胰岛,并通过手工挑选非胰岛组织进一步纯化。将胰岛在RPMI-1640,pH 7.4中培养,并在空气中5%(v / v)二氧化碳的潮湿气氛中保持在37℃。将环孢菌素添加到培养基中,使其终浓度为1夹具/毫升(治疗剂量),5夹具/毫升(毒性剂量)或溶媒(对照)。在培养的第1、4和10天收获胰岛,并进行功能或组织学研究。用1 Fig / ml CsA培养的胰岛的功能研究表明,胰岛素和C肽含量与对照胰岛相似。用5 ug / ml CsA培养的胰岛显示胰岛素和C肽含量明显降低。葡萄糖依赖性胰岛素释放是可变的。在治疗剂量和有毒剂量的CsA后,C-肽的释放均低于对照。相差显微镜显示,以1ug / ml CsA培养的胰岛外观基本正常,外围轮廓清晰。少数胰岛周围不清晰或不规则。用5 ug / ml CsA培养的胰岛在第1天具有不确定的不规则外围,并且在培养后第4天和第10天密集且形成团块。治疗剂量后胰岛数目减少; CsA的毒性剂量后下降幅度更大。胰岛直径在治疗剂量后增加,但在有毒剂量的CsA后略有减小。胰岛显示出对胰岛素的弱阳性免疫过氧化物酶反应,该反应在有毒剂量的CsA后减弱。结论是CsA对B细胞具有直接作用,这在体外培养的胰岛中见到的功能和形态变化已得到证实。 500B电池; C肽文化;环孢霉素组织学免疫组织化学;胰岛素;朗格罕岛形态学;胰腺;鼠

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