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Dendritic Cell Therapies in Transplantation Revisited: Deletion of Recipient DCs Deters the Effect of Therapeutic DCs

机译:重新研究移植中的树突状细胞疗法:收件人DC的删除会阻止DC的治疗效果

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摘要

A critical goal in transplantation is the achievement of donor-specific tolerance, minimizing the use of immunosuppressants. Dendritic cells (DCs) are antigen (Ag) presenting cells (APCs) with capability to promote immunity or tolerance. The immune-regulatory properties of DCs have been exploited for generation of tolerogenic/immunosuppressive (IS) DCs that, when transfer systemically, prolong allograft survival in murine models. Surprisingly, the in vivo mechanisms of therapies based on (donor- or recipient-derived) ISDCs in transplantation remain unknown, given that previous studies investigated their effects in vitro, or ex vivo after transplantation. Since once injected, ISDCs are short-lived and transfer Ag to recipient APCs, we assessed the role of recipient DCs by depleting them at the time of ISDC-therapy in a mouse model of cardiac transplantation. The results indicate that, contrary to the accepted paradigm, systemically administered ISDCs reduce the alloresponse and prolong allograft survival, not by themselves, but through conventional DCs (cDCs) of the recipient. These findings raise doubts on the advantages of the currently used ISDC-therapies, since the immune-regulatory properties of the injected ISDC do not seem to be functionally relevant in vivo, and the quiescent/pro-tolerogenic status of cDCs may be compromised in patients with end-stage diseases that require transplantation.
机译:移植的关键目标是实现供体特异性耐受,从而最大程度地减少免疫抑制剂的使用。树突细胞(DC)是具有增强免疫力或耐受能力的抗原(Ag)呈递细胞(APC)。 DC的免疫调节特性已被用于产生致耐受性/免疫抑制(IS)DC,当系统转移时,DC可延长小鼠模型中同种异体移植的存活时间。出乎意料的是,鉴于以前的研究已经研究了它们在体外或离体后的作用,因此在移植中基于(供体或受体来源的)ISDC的疗法的体内机制仍然未知。由于一旦注射,ISDC的寿命很短,并将Ag转移至受体APC,我们通过在心脏移植小鼠模型中进行ISDC治疗时消耗受体DC来评估受体DC的作用,从而评估了受体DC的作用。结果表明,与公认的范式相反,全身施用的ISDC减少了过敏反应并延长了同种异体移植的存活时间,这不是靠它们自己而是通过接受者的常规DC(cDC)。这些发现使人们对目前使用的ISDC治疗的优势产生怀疑,因为注射的ISDC的免疫调节特性在体内似乎与功能不相关,并且患者中cDC的静止/致耐受性状态可能受到损害患有需要移植的晚期疾病。

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