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髓源性抑制细胞增加并抑制移植物肠道上皮的供体反应性 T 细胞反应在肠移植患者中。

Myeloid-derived suppressor cells increase and inhibit donor-reactive T cell responses to graft intestinal epithelium in intestinal transplant patients.

机构信息

Transplant Center, Department of General Surgery, Digestive Disease & Surgery Institute, Cleveland Clinic, Cleveland, OH, USA.

Department of Immunology, Lerner Research Institute, Cleveland Clinic, Cleveland, OH, USA.

出版信息

Am J Transplant. 2018 Oct;18(10):2544-2558. doi: 10.1111/ajt.14718. Epub 2018 Apr 17.

DOI:10.1111/ajt.14718
PMID:29509288
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6127002/
Abstract

Recent advances in immunosuppressive regimens have decreased acute cellular rejection (ACR) rates and improved intestinal and multivisceral transplant (ITx) recipient survival. We investigated the role of myeloid-derived suppressor cells (MDSCs) in ITx. We identified MDSCs as CD33 CD11b lineage(CD3/CD56/CD19) HLA-DR cells with 3 subsets, CD14 CD15 (e-MDSCs), CD14 CD15 (M-MDSCs), and CD14 CD15 (PMN-MDSCs), in peripheral blood mononuclear cells (PBMCs) and mononuclear cells in the grafted intestinal mucosa. Total MDSC numbers increased in PBMCs after ITx; among MDSC subsets, M-MDSC numbers were maintained at a high level after 2 months post ITx. The MDSC numbers decreased in ITx recipients with ACR. MDSC numbers were positively correlated with serum interleukin (IL)-6 levels and the glucocorticoid administration index. IL-6 and methylprednisolone enhanced the differentiation of bone marrow cells to MDSCs in vitro. M-MDSCs and e-MDSCs expressed CCR1, -2, and -3; e-MDSCs and PMN-MDSCs expressed CXCR2; and intestinal grafts expressed the corresponding chemokine ligands after ITx. Of note, the percentage of MDSCs among intestinal mucosal CD45 cells increased after ITx. A novel in vitro assay demonstrated that MDSCs suppressed donor-reactive T cell-mediated destruction of donor intestinal epithelial organoids. Taken together, our results suggest that MDSCs accumulate in the recipient PBMCs and the grafted intestinal mucosa in ITx, and may regulate ACR.

摘要

免疫抑制方案的最新进展降低了急性细胞排斥(ACR)的发生率,并提高了肠和多器官移植(ITx)受者的存活率。我们研究了髓系来源的抑制细胞(MDSCs)在 ITx 中的作用。我们在外周血单核细胞(PBMCs)和移植肠黏膜的单核细胞中鉴定出 MDSCs 为 CD33 CD11b 谱系(CD3/CD56/CD19)HLA-DR 细胞,有 3 个亚群,CD14 CD15(e-MDSCs)、CD14 CD15(M-MDSCs)和 CD14 CD15(PMN-MDSCs)。ITx 后 PBMCs 中的总 MDSC 数量增加;在 MDSC 亚群中,M-MDSC 数量在 ITx 后 2 个月仍维持在高水平。ACR 的 ITx 受者 MDSC 数量减少。MDSC 数量与血清白细胞介素(IL)-6 水平和糖皮质激素给药指数呈正相关。IL-6 和甲泼尼龙在体外增强骨髓细胞向 MDSC 的分化。M-MDSCs 和 e-MDSCs 表达 CCR1、-2 和 -3;e-MDSCs 和 PMN-MDSCs 表达 CXCR2;ITx 后肠移植表达相应的趋化因子配体。值得注意的是,ITx 后肠黏膜 CD45 细胞中 MDSC 的比例增加。一种新的体外测定表明,MDSCs 抑制供体反应性 T 细胞介导的供体肠上皮类器官的破坏。综上所述,我们的研究结果表明,MDSCs 在 ITx 受者的 PBMC 和移植肠黏膜中积累,并可能调节 ACR。

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