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在实验性肾移植中,基于间充质干细胞的免疫调节治疗最适合且有效的给药途径是静脉内给药还是动脉内给药?

Which is the most suitable and effective route of administration for mesenchymal stem cell-based immunomodulation therapy in experimental kidney transplantation: endovenous or arterial?

作者信息

Zonta S, De Martino M, Bedino G, Piotti G, Rampino T, Gregorini M, Frassoni F, Dal Canton A, Dionigi P, Alessiani M

机构信息

Dipartimento di Scienze, Chirurgia Epatopancreatica, IRCCS Pol San Matteo, Chirurgiche Università di Pavia, Italy.

出版信息

Transplant Proc. 2010 May;42(4):1336-40. doi: 10.1016/j.transproceed.2010.03.081.

Abstract

Immunomodulating cell therapy represents a new perspective for the control of cellular immune responses that determine the occurrence of acute rejection (ACR) in allo-transplantation. Mesenchymal stem cells (MSC) demonstrate immunoregulatory effects by inactivating T-cell components that regulate tissue damage in transplantation models. The presumed mechanism of action is recruitment of cells by a cytokine network. The purpose of this study was to test which route of administration (intra-arterial vs intravenous) was the most effective route to achieve immunomodulating effects in experimental rat kidney transplantation. Transgenic Sprague-Dawley rats (SD) expressing the enhanced green fluorescent protein (EGFP) at the somatic level were used as MSC donors: Allogeneic Fischer to Lewis grafts (n = 4 per group) were performed in rats after bilateral nephrectomy. In Gr B, 3 x 10(6) MSCs were infused into the renal graft artery, whereas in Gr C, they were infused into the tail vein. The untreated Gr A were a control group. No immunosuppressive therapy was administered. The animals were sacrificed at day 7 postoperatively. Biochemical analysis for renal function, histological (Banff criteria) and immunohistological (anti-EGFP-Immunoglobulin) analysis were performed on the transplanted animals. In Gr B, functional recovery was more rapid (creatinine: Gr B vs Gr C, P < .05). The inflammatory infiltrate in the graft was less in Gr B vs Gr C, with preservation of tubules, arteries, and glomeruli (P < .01). Intra-arterial infusion of MSCs was more effective to control ACR.

摘要

免疫调节细胞疗法为控制细胞免疫反应提供了新的视角,而细胞免疫反应决定了同种异体移植中急性排斥反应(ACR)的发生。间充质干细胞(MSC)通过使调节移植模型中组织损伤的T细胞成分失活来发挥免疫调节作用。推测的作用机制是通过细胞因子网络募集细胞。本研究的目的是测试哪种给药途径(动脉内给药与静脉内给药)是在实验性大鼠肾移植中实现免疫调节作用的最有效途径。将在体细胞水平表达增强型绿色荧光蛋白(EGFP)的转基因Sprague-Dawley大鼠(SD)用作MSC供体:在双侧肾切除术后的大鼠中进行异基因Fischer到Lewis移植(每组n = 4)。在B组中,将3×10⁶个MSC注入肾移植动脉,而在C组中,将它们注入尾静脉。未治疗的A组为对照组。未给予免疫抑制治疗。在术后第7天处死动物。对移植动物进行肾功能生化分析、组织学(Banff标准)和免疫组织学(抗EGFP免疫球蛋白)分析。在B组中,功能恢复更快(肌酐:B组与C组相比,P <.05)。与C组相比,B组移植物中的炎性浸润较少,肾小管、动脉和肾小球得以保留(P <.01)。动脉内输注MSC对控制ACR更有效。

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