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4-deoxypyridoxine improves the viability of isolated pancreatic islets ex vivo

机译:4-deoxypyridoxine提高离体胰岛的离体活力

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The successful islet transplantation, for the treatment of type 1 diabetes, depends on the quantity and the quality of transplanted islets. Previously, it has reported that the significant loss of isolated islet mass could be prevented by sphingolipid metabolite, sphinogosine-1-phophate (S1P). This study was performed to elucidate whether the beneficial effects of S1P maintaining isolated pancreatic islets ex vivo are mimicked by modulation of intracellular S1P. We tested the in vitro effect of various agents that modulate intracellular S1P levels in insulinoma cell lines and isolated islets to compare their anti-apoptotic effects with that of S1P. As results, we discovered that 4-deoxypyridoxine (DOP), which inhibits the degradation of intracellular S1P by inhibiting S1P lyase (SPL) activity, minimized the chemically induced apoptosis of insulinoma cell lines as S1P did. Also, supplementation of DOP in the culture media protected the regression of isolated islets that have been maintained ex vivo at least for 18 h providing the evidence of increasing viability of isolated islets with DOP, which impaired SPL activity. In conclusion, these results suggest that the application of SPL inhibitors could be considered as a supplement for the maintenance of viable islets isolated from donor sources in the process of islet transplantation.
机译:用于治疗1型糖尿病的成功胰岛移植取决于所移植胰岛的数量和质量。以前,有报道说,鞘脂代谢产物1-磷酸鞘氨醇(S1P)可以防止离体胰岛的大量损失。进行这项研究是为了阐明通过调节细胞内S1P是否可以模仿S1P维持离体胰岛离体的有益作用。我们测试了调节胰岛素瘤细胞系和分离的胰岛中细胞内S1P水平的各种药物的体外作用,以比较它们与S1P的抗凋亡作用。结果,我们发现通过抑制S1P裂解酶(SPL)活性抑制细胞内S1P降解的4-deoxypyridoxine(DOP)像S1P一样使胰岛素瘤细胞系的化学诱导凋亡最小化。同样,在培养基中补充DOP可以保护离体的胰岛的退化,而离体的胰岛在体外至少维持了18小时,这提供了DOP分离的胰岛的生存能力增加的证据,这损害了SPL活性。总之,这些结果表明,在胰岛移植过程中,可以将SPL抑制剂的应用视为维持从供体来源分离的存活胰岛的补充。

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