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前沿:给予肾移植受者的人调节性巨噬细胞的免疫后果和迁移。

Cutting Edge: Immunological consequences and trafficking of human regulatory macrophages administered to renal transplant recipients.

机构信息

Laboratory for Transplantation Research, Department of Surgery, University Hospital Regensburg, Regensburg 93053, Germany.

出版信息

J Immunol. 2011 Sep 1;187(5):2072-8. doi: 10.4049/jimmunol.1100762. Epub 2011 Jul 29.

Abstract

Regulatory macrophages (M regs) were administered to two living-donor renal transplant recipients. Both patients were minimized to low-dose tacrolimus monotherapy within 24 wk of transplantation and subsequently maintained excellent graft function. After central venous administration, most M regs remained viable and were seen to traffic from the pulmonary vasculature via the blood to liver, spleen, and bone marrow. By 1 y posttransplantation, both patients displayed patterns of peripheral blood gene expression converging upon the IOT-RISET signature. Furthermore, both patients maintained levels of peripheral blood FOXP3 and TOAG-1 mRNA expression within the range consistent with nonrejection. It is concluded that M regs warrant further study as a potential immune-conditioning therapy for use in solid-organ transplantation. The results of this work are being used to inform the design of The ONE Study, a multinational clinical trial of immunomodulatory cell therapy in renal transplantation.

摘要

两名活体供肾移植受者接受了调节性巨噬细胞(Mregs)治疗。两名患者在移植后 24 周内均被减至低剂量他克莫司单药治疗,随后保持了良好的移植物功能。静脉内给药后,大多数 Mregs 仍然存活,并从肺血管通过血液转移到肝脏、脾脏和骨髓。移植后 1 年,两名患者的外周血基因表达模式均趋于 IOT-RISET 特征。此外,两名患者的外周血 FOXP3 和 TOAG-1 mRNA 表达水平均保持在非排斥反应范围内。因此,Mregs 作为实体器官移植中潜在的免疫调节治疗方法值得进一步研究。这项工作的结果正在被用于为 The ONE 研究提供信息,这是一项关于免疫调节细胞治疗在肾移植中的多国临床试验。

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