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简明综述:中枢神经系统中同种异体和异种细胞移植物的固有和适应性免疫识别。

Concise Review: Innate and Adaptive Immune Recognition of Allogeneic and Xenogeneic Cell Transplants in the Central Nervous System.

机构信息

Laboratory of Experimental Hematology, Faculty of Medicine and Health Sciences, University of Antwerp, Antwerp, Belgium.

Vaccine and Infectious Disease Institute (Vaxinfectio), Faculty of Medicine and Health Sciences, University of Antwerp, Antwerp, Belgium.

出版信息

Stem Cells Transl Med. 2017 May;6(5):1434-1441. doi: 10.1002/sctm.16-0434. Epub 2017 Feb 28.

Abstract

Over the last 30 years, numerous allogeneic and xenogeneic cell grafts have been transplanted into the central nervous system (CNS) of mice and men in an attempt to cure neurological diseases. In the early studies, human or porcine embryonic neural cells were grafted in the striatum of animals or patients in an attempt to replace lost neurons. Although the immune-privileged status of the brain as a recipient organ was widely accepted, it rapidly became evident that CNS-grafted allogeneic and xenogeneic cells could be recognized and rejected by the immune system, resulting in poor neural graft survival and limited functional recovery. Since then, the CNS transplantation field has witnessed a sharp rise in the number of studies in which allogeneic and xenogeneic neural or mesenchymal stem cells (NSCs or MSCs, respectively) are transplanted, predominantly aiming at providing trophic stimulation and promoting endogenous repair of the brain. Interestingly, in many recent NSC and MSC-based publications functional improvement was used as the principal measure to evaluate the success of cell transplantation, while the fate of transplanted cells remained largely unreported. In this review, we first attempt to understand why primary neural cell isolates were largely substituted for NSCs and MSCs in cell grafting studies. Next, we review the current knowledge on the immune mechanisms involved in the recognition and rejection of allogeneic and xenogeneic cellular grafts in the CNS. Finally, we propose strategies to reduce graft immunogenicity and to improve graft survival in order to design improved cell-based CNS therapies. Stem Cells Translational Medicine 2017;6:1434-1441.

摘要

在过去的 30 年中,人们尝试将许多同种异体和异种细胞移植到小鼠和人类的中枢神经系统(CNS)中,以治疗神经疾病。在早期的研究中,人们将人或猪胚胎神经细胞移植到动物或患者的纹状体中,试图替代丢失的神经元。尽管大脑作为受体器官具有免疫豁免特权的地位得到了广泛认可,但很快就发现,中枢神经系统移植的同种异体和异种细胞会被免疫系统识别和排斥,导致神经移植物的存活和功能恢复有限。从那时起,中枢神经系统移植领域见证了大量研究的兴起,这些研究主要将同种异体和异种神经或间充质干细胞(分别为 NSCs 或 MSCs)移植,旨在提供营养刺激并促进大脑的内源性修复。有趣的是,在许多最近的 NSC 和 MSC 为基础的出版物中,功能改善被用作评估细胞移植成功的主要指标,而移植细胞的命运在很大程度上仍未得到报道。在这篇综述中,我们首先尝试了解为什么在细胞移植研究中,主要使用原代神经细胞分离物替代 NSCs 和 MSCs。接下来,我们回顾了目前关于中枢神经系统中同种异体和异种细胞移植物的识别和排斥所涉及的免疫机制的知识。最后,我们提出了降低移植物免疫原性和提高移植物存活率的策略,以设计改进的基于细胞的中枢神经系统治疗方法。《干细胞转化医学》2017 年;6:1434-1441.

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4d8b/5442707/8ba3e277d635/SCT3-6-1434-g001.jpg

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