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首页> 外文期刊>American journal of transplantation: official journal of the American Society of Transplantation and the American Society of Transplant Surgeons >Cotransplantation of preactivated mesenchymal stem cells improves intraportal engraftment of islets by inhibiting liver natural killer cells in mice
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Cotransplantation of preactivated mesenchymal stem cells improves intraportal engraftment of islets by inhibiting liver natural killer cells in mice

机译:通过抑制小鼠的肝脏天然杀伤细胞来改善失活的间充质干细胞的分枝杆菌改善了胰岛的内瓣

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The activation of natural killer (NK) cells in the liver inhibits engraftment of intraportally transplanted islets. We attempted to modulate the activity of NK cells by cotransplanting mesenchymal stem cells (MSCs) with islets in mice. We first investigated the ability of MSCs to secrete prostaglandin E2 , a predominant inhibitor of NK cell function, in various combinations of inflammatory cytokines. Notably, we found that prostaglandin E2 production was partially delayed in MSCs activated by inflammatory cytokines in vitro, whereas liver NK cells were activated early after islet transplant in vivo. Accordingly, preactivated MSCs, but not naive MSCs, substantially suppressed the expression of activation markers in liver NK cells after cotransplant with islets. Similarly, cotransplant with preactivated MSCs, but not naive MSCs, markedly improved the survival of islet grafts. These results highlight MSC cotransplant as an effective and clinically feasible method for enhancing engraftment efficiency.
机译:肝脏中的自然杀伤(NK)细胞的激活抑制了内腔移植胰岛的植入。我们试图通过Cotroanspranting间充质干细胞(MSC)用小鼠中的胰岛调节NK细胞的活性。我们首先研究了MSCs分泌前列腺素E2,炎症细胞因子的各种组合中分泌前列腺素E2,是NK细胞功能的主要抑制剂。值得注意的是,我们发现前列腺素E2生产在体外炎症细胞因子激活的MSC中部分延迟,而肝脏NK细胞在体内胰岛移植后早期激活。因此,预活化的MSCs,但不是幼稚的MSCs,基本上抑制了肝脏肝脏在胰岛胰岛后肝脏NK细胞中活化标志物的表达。类似地,具有预活性MSC的COTAsplant,但不是幼稚的MSCs,显着改善了胰岛移植物的存活率。这些结果突出了MSC COTRASPLANT作为提高植入效率的有效和临床可行的方法。

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