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使用先天修复受体配体西比奈肽改善胰岛移植物功能。

Improvement of Islet Allograft Function Using Cibinetide, an Innate Repair Receptor Ligand.

机构信息

Division of Transplantation Surgery, CLINTEC, Karolinska Institutet, Stockholm, Sweden.

Department of Transplantation Surgery, Karolinska University Hospital Huddinge, Stockholm, Sweden.

出版信息

Transplantation. 2020 Oct;104(10):2048-2058. doi: 10.1097/TP.0000000000003284.

Abstract

BACKGROUND

During intraportal pancreatic islet transplantation (PITx), early inflammatory reactions cause an immediate loss of more than half of the transplanted graft and potentiate subsequent allograft rejection. Previous findings suggest that cibinetide, a selective innate repair receptor agonist, exerts islet protective and antiinflammatory properties and improved transplant efficacy in syngeneic mouse PITx model. In a stepwise approach toward a clinical application, we have here investigated the short- and long-term effects of cibinetide in an allogeneic mouse PITx model.

METHODS

Streptozotocin-induced diabetic C57BL/6N (H-2) mice were transplanted with 320 (marginal) or 450 (standard) islets from BALB/c (H-2) mice via the portal vein. Recipients were treated perioperative and thereafter daily during 14 d with cibinetide (120 µg/kg), with or without tacrolimus injection (0.4 mg/kg/d) during days 4-14 after transplantation. Graft function was assessed using nonfasting glucose measurements. Relative gene expressions of proinflammatory cytokines and proinsulin of the graft-bearing liver were assessed by quantitative polymerase chain reaction. Cibinetide's effects on dendritic cell maturation were investigated in vitro.

RESULTS

Cibinetide ameliorated the local inflammatory responses in the liver and improved glycemic control immediately after allogeneic PITx and significantly delayed the onset of allograft loss. Combination treatment with cibinetide and low-dose tacrolimus significantly improved long-term graft survival following allogeneic PITx. In vitro experiments indicated that cibinetide lowered bone-marrow-derived-immature-dendritic cell maturation and subsequently reduced allogeneic T-cell response.

CONCLUSIONS

Cibinetide reduced the initial transplantation-related severe inflammation and delayed the subsequent alloreactivity. Cibinetide, in combination with low-dose tacrolimus, could significantly improve long-term graft survival in allogeneic PITx.

摘要

背景

在门静脉内胰岛移植(PITx)过程中,早期炎症反应会导致移植的胰岛立即损失一半以上,并加剧随后的同种异体移植物排斥反应。先前的研究结果表明,选择性先天修复受体激动剂西比奈肽具有胰岛保护和抗炎特性,并能改善同种异体小鼠 PITx 模型中的移植效果。在向临床应用逐步推进的过程中,我们在此研究了西比奈肽在同种异体小鼠 PITx 模型中的短期和长期效果。

方法

链脲佐菌素诱导的糖尿病 C57BL/6N(H-2)小鼠通过门静脉接受来自 BALB/c(H-2)小鼠的 320(边缘)或 450(标准)个胰岛。受体在手术期间和术后每天接受西比奈肽(120μg/kg)治疗,在移植后第 4-14 天期间,每天还接受他克莫司(0.4mg/kg/d)注射。通过非空腹血糖测量评估移植物功能。通过定量聚合酶链反应评估携带移植物肝脏中促炎细胞因子和前胰岛素的相对基因表达。研究了西比奈肽对树突状细胞成熟的体外影响。

结果

西比奈肽改善了同种异体 PITx 后肝内局部炎症反应,改善了血糖控制,并显著延迟了同种异体移植物丢失的发生。西比奈肽与低剂量他克莫司联合治疗可显著改善同种异体 PITx 后的长期移植物存活率。体外实验表明,西比奈肽降低了骨髓来源的不成熟树突状细胞的成熟度,从而降低了同种异体 T 细胞的反应。

结论

西比奈肽减少了与移植相关的初始严重炎症,并延迟了随后的同种异体反应。西比奈肽与低剂量他克莫司联合使用可显著提高同种异体 PITx 的长期移植物存活率。

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