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人类抑制性受体免疫球蛋白样转录物2增强CD11b+Gr1+髓源性抑制细胞,后者可促进同种异体移植物的长期存活。

Human inhibitory receptor immunoglobulin-like transcript 2 amplifies CD11b+Gr1+ myeloid-derived suppressor cells that promote long-term survival of allografts.

作者信息

Zhang Wei, Liang Siyuan, Wu Juan, Horuzsko Anatolij

机构信息

Department of Medicine, Center for Molecular Chaperone/Radiobiology and Cancer Virology, Medical College of Georgia, Augusta, GA, USA.

出版信息

Transplantation. 2008 Oct 27;86(8):1125-34. doi: 10.1097/TP.0b013e318186fccd.

Abstract

BACKGROUND

The expression of human leukocyte antigen (HLA)-G during allogeneic recognition is associated with better graft acceptance. The inhibitory receptor immunoglobulin-like transcript (ILT)-2 is expressed on activated T cells and serves to shut down T-cell activation, culminating in T-cell death, or induction of anergy. One of the potential mechanisms in the immunosuppressive accomplishment of HLA-G-ILT2 interactions involves the expansion of myeloid-derived suppressor cells (MDSCs). The potential of MDSCs in transplantation has not yet been exploited.

METHODS

(1) Detailed phenotypic characteristics, immunosuppressive potential of MDSCs expanded by means of inhibitory receptor ILT2 and its ligands, and allogeneic transplant-activated MDSCs were obtained in mice. (2) Oligo- and real-time pathway-specific polymerase chain reaction arrays were performed to characterize ILT2-specific MDSCs. (3) Skin allograft survival after adoptive transfer of MDSCs was studied.

RESULTS

Engagement of ILT2 receptors, especially by HLA-G, expanded the population of MDSCs with enhanced suppressive activity. Adoptive transfer of MDSCs generated by ILT2 receptor and its ligands prolonged graft survival in recipients of allogeneic skin transplant. We have proposed pathways for enhancement of immunosuppressive activities and expansion of MDSCs by ILT2 and HLA-G.

CONCLUSIONS

Our results suggest that induction of MDSCs using ILT2 inhibitory receptor/HLA-G ligand may be an attractive strategy for preventing rejection of immunogenic organs or tissues in clinical transplantation.

摘要

背景

在同种异体识别过程中,人类白细胞抗原(HLA)-G的表达与更好的移植物接受相关。抑制性受体免疫球蛋白样转录物(ILT)-2在活化的T细胞上表达,用于终止T细胞活化,最终导致T细胞死亡或诱导无反应性。HLA-G与ILT-2相互作用实现免疫抑制的潜在机制之一涉及髓系来源的抑制细胞(MDSC)的扩增。MDSC在移植中的潜力尚未得到开发。

方法

(1)在小鼠中获得了通过抑制性受体ILT2及其配体扩增的MDSC的详细表型特征、免疫抑制潜力以及同种异体移植激活的MDSC。(2)进行寡核苷酸和实时通路特异性聚合酶链反应阵列以表征ILT2特异性MDSC。(3)研究了MDSC过继转移后皮肤同种异体移植物的存活情况。

结果

ILT2受体的结合,特别是被HLA-G结合,扩大了具有增强抑制活性的MDSC群体。由ILT2受体及其配体产生的MDSC过继转移延长了同种异体皮肤移植受体中移植物的存活时间。我们提出了通过ILT2和HLA-G增强免疫抑制活性和扩大MDSC的途径。

结论

我们的结果表明,使用ILT2抑制性受体/HLA-G配体诱导MDSC可能是临床移植中预防免疫原性器官或组织排斥的一种有吸引力的策略。

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