用MIN-6细胞建立小鼠胰岛移植模型。

IF 1.9 4区 医学 Q3 ENDOCRINOLOGY & METABOLISM
Islets Pub Date : 2020-07-03 Epub Date: 2020-06-22 DOI:10.1080/19382014.2020.1763719
Douglas O Sobel, Barath Ramasubramanian, Larry Mitnaul
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引用次数: 4

摘要

永生化细胞是产生胰岛素的细胞的丰富来源。尽管MIN-6细胞在体外具有与正常胰岛相似的特性,但MIN-6细胞在体内的使用尚未得到充分的描述。本研究研究了MIN-6移植和排斥反应的小鼠体内模型。用Matrigel或HyStem-C水凝胶对MIN-6细胞进行皮下移植可以降低裸鼠的血糖,因此是体内MIN-6细胞的良好基质。NOD小鼠是很好的移植受体,因为它们对MIN-6细胞有最好的排斥反应。BalbC、Black Webster、Swiss Black、C3H和NOD小鼠的MLR反应与平均血糖反应相关,表明同种异体差异在细胞排斥反应中的重要性。环孢素给药3天对MIN-6细胞排斥反应无抑制作用,6天可短暂性降低血糖,每日给药可长期抑制排斥反应。裸小鼠的动态葡萄糖耐量(GTT)研究表明,移植的MIN-6细胞在控制血糖方面接近但不如正常胰岛有效,并且随着时间的推移,MIN-6细胞中胰岛素释放的血糖设定点降低到低血糖水平。为了避免低血糖,我们评估了MIN-6细胞辐照的效果。然而,辐照只能延缓低血糖的发展,而不能改变胰岛素释放的最终葡萄糖设定点。总之,我们已经建立了一种使用皮下MIN-6细胞进行β细胞移植的小鼠模型,该模型可以用作研究减轻免疫排斥的方法的工具。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Characterization of a mouse model of islet transplantation using MIN-6 cells.

Immortalized beta cells are an abundant source of insulin-producing cells. Although MIN-6 cells have similar characteristics as normal islets in vitro, the in vivo use of MIN-6 cells has not been fully described. This study characterizes in vivo mouse models of MIN-6 transplantation and rejection. Subcutaneous (sc) transplantation of MIN-6 cells in either Matrigel or HyStem-C hydrogels reduced blood sugars in nude mice and thus are good matrices for MIN-6 cells in vivo. NOD mice are good transplant recipients since they best rejected MIN-6 cells. MLR responses from BalbC, Black Webster, Swiss Black, C3H, and NOD mice correlated with mean blood glucose response suggesting the importance of allogeneic differences in the rejection of cells. Three days of cyclosporine administration caused no inhibition of MIN-6 cell rejection and 6 days resulted in a transient decrease in blood glucose, while daily administration inhibited rejection long term. Kinetic glucose tolerance (GTT) studies in nude mice demonstrated transplanted MIN-6 cells are close but not as effective as normal islets in controlling blood glucose and blood glucose set point for insulin release in MIN-6 cells decreases to hypoglycemic levels over time. To avoid hypoglycemia, the effect of MIN-6 cell irradiation was assessed. However, irradiation only delayed the development of hypoglycemia, not altering the final glucose set point for insulin release. In conclusion, we have characterized a mouse model for beta-cell transplantation using subcutaneous MIN-6 cells that can be used as a tool to study approaches to mitigate immune rejection.

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来源期刊
Islets
Islets ENDOCRINOLOGY & METABOLISM-
CiteScore
3.30
自引率
4.50%
发文量
10
审稿时长
>12 weeks
期刊介绍: Islets is the first international, peer-reviewed research journal dedicated to islet biology. Islets publishes high-quality clinical and experimental research into the physiology and pathology of the islets of Langerhans. In addition to original research manuscripts, Islets is the leading source for cutting-edge Perspectives, Reviews and Commentaries. Our goal is to foster communication and a rapid exchange of information through timely publication of important results using print as well as electronic formats.
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