Ilaria Righi , Daria Trabattoni , Lorenzo Rosso , Valentina Vaira , Mario Clerici
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引用次数: 0
摘要
免疫检查点(IC)分子在抗原呈递时调节免疫反应;不同 IC 分子之间的相互作用将导致刺激或挫败这种反应。肿瘤细胞会表达更多的抑制性 IC 分子,试图逃避免疫反应;目前已开发出能与抑制性 IC 分子结合的治疗药物,从而恢复肿瘤导向的免疫反应,改变一些癌症的预后。在实体器官移植(SOT)的情况下,刺激抑制性 IC 分子可能有利于防止排斥反应,在动物模型中获得的体内和体内结果表明确实如此。除了将 IgG Fc 片段与 CTLA-4 细胞外结构域相连的单克隆抗体(mAb)belatacept 外,尚未产生预防 SOT 排斥反应的新型治疗方法。我们回顾了 IC 分子在移植中所起作用的最新知识,相信创新研究将为控制实体器官移植中的排斥反应提供新的途径。
Immune checkpoint molecules in solid organ transplantation: A promising way to prevent rejection
Immune checkpoint (IC) molecules modulate immune responses upon antigen presentation; the interaction between different IC molecules will result in the stimulation or, rather, the thwarting of such responses. Tumor cells express increased amounts of inhibitory IC molecules in an attempt to evade immune responses; therapeutic agents have been developed that bind inhibitory IC molecules, restoring tumor-directed immune responses and changing the prognosis of a number of cancers. Stimulation of inhibitory IC molecules could be beneficial in preventing rejection in the setting of solid organ transplantation (SOT), and in vivo as well as in vivo results obtained in animal models show this to indeed to be the case. With the exception of belatacept, a monoclonal antibody (mAb) in which an IgG Fc fragment is linked to the extracellular domain of CTLA-4, this has not yet translated into the generation of novel therapeutic approaches to prevent SOT rejection. We provide a review of state-of-the art knowledge on the role played by IC molecules in transplantation, confident that innovative research will lead to new avenues to manage rejection in solid organ transplant.