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免疫健全大鼠体内的猪神经异种移植:扩增神经前体细胞移植后的免疫反应

Porcine neural xenografts in the immunocompetent rat: immune response following grafting of expanded neural precursor cells.

作者信息

Armstrong R J, Harrower T P, Hurelbrink C B, McLaughin M, Ratcliffe E L, Tyers P, Richards A, Dunnett S B, Rosser A E, Barker R A

机构信息

Cambridge Centre for Brain Repair, University of Cambridge, Forvie Site, Robinson Way, Cambridge CB2 2PY, UK.

出版信息

Neuroscience. 2001;106(1):201-16. doi: 10.1016/s0306-4522(01)00273-1.

Abstract

Intracerebral neural xenografts elicit a host immune response that results in their rapid rejection. This forms a key barrier to the therapeutic use of xenogeneic tissue transplantation for conditions such as Parkinson's disease. The current study sought to provide insight into the cellular components of donor cell suspensions that are important in stimulating the host rejection response and thereby to suggest rational manipulations of xenogeneic donor tissue that might ultimately enhance its clinical utility. The neural stem cell mitogens, epidermal growth factor and fibroblast growth factor-2, have been used to isolate and expand populations of primordial neural precursor cells from the embryonic pig brain. The immune response elicited by these cells on transplantation into the non-immunosuppressed rat has been fully characterised. In the first experiments, expanded neural precursors were grafted into the hemi-parkinsonian, non-immunosuppressed Sprague-Dawley rat and graft status and host response examined 10, 21, 35 and 60 days post-transplantation. While equivalent primary tissue grafts were completely eliminated at 35 days, grafts of expanded neural precursors with healthy neurofilament-positive projections were present at all time-points, and two large grafts remained even at 60 days. Some grafts appeared to elicit minimal host immune responses at the time-points they were examined, although most did appear to be undergoing a rejection process since a co-ordinated response involving host cytotoxic T-lymphocytes, microglia/macrophages, immunoglobulin M and complement could be demonstrated to varying degrees. Subsequent experiments went on to demonstrate further that expanded precursor populations and primary tissue suspensions differed in their immunogenic profile. Firstly, when primary tissue was injected intraperitoneally into immunocompetent rats a vigorous primary humoral response was generated. No such response was detected following injection of expanded neural precursors. Secondly, flow cytometric analysis revealed small but significant levels of class II porcine major histocompatibility complex expression in primary cell suspensions but no such expression in expanded precursor populations.The results of this study therefore demonstrate that the immunogenicity of porcine neural cell suspensions used for intracerebral grafting is reduced when neural stem cell mitogens are used to expand precursor cells. The implications of these findings in the development of novel xenogeneic cellular therapies for neurodegenerative conditions such as Parkinson's disease are discussed.

摘要

脑内神经异种移植会引发宿主免疫反应,导致其迅速被排斥。这成为了异种组织移植治疗帕金森病等疾病的关键障碍。当前研究旨在深入了解供体细胞悬液中在刺激宿主排斥反应方面起重要作用的细胞成分,从而提出对异种供体组织进行合理操作的建议,最终可能提高其临床应用价值。神经干细胞促分裂原,即表皮生长因子和成纤维细胞生长因子 -2,已被用于从胚胎猪脑中分离和扩增原始神经前体细胞群体。这些细胞移植到未免疫抑制的大鼠体内所引发的免疫反应已得到充分表征。在最初的实验中,将扩增的神经前体细胞移植到半帕金森病、未免疫抑制的斯普拉格 - 道利大鼠体内,并在移植后10、21、35和60天检查移植状态和宿主反应。虽然同等的原代组织移植在35天时被完全清除,但具有健康神经丝阳性突起的扩增神经前体细胞移植在所有时间点均存在,甚至在60天时仍有两个大的移植体。一些移植体在检查的时间点似乎引发了最小的宿主免疫反应,尽管大多数移植体似乎确实在经历排斥过程,因为涉及宿主细胞毒性T淋巴细胞、小胶质细胞/巨噬细胞、免疫球蛋白M和补体的协同反应在不同程度上可以得到证实。随后的实验进一步证明,扩增的前体细胞群体和原代组织悬液在免疫原性特征上存在差异。首先,当将原代组织腹腔内注射到有免疫能力的大鼠体内时,会产生强烈的初次体液反应。注射扩增的神经前体细胞后未检测到此类反应。其次,流式细胞术分析显示原代细胞悬液中有少量但显著水平的II类猪主要组织相容性复合体表达,而扩增的前体细胞群体中没有此类表达。因此,本研究结果表明,当使用神经干细胞促分裂原扩增前体细胞时,用于脑内移植的猪神经细胞悬液的免疫原性会降低。讨论了这些发现对开发针对帕金森病等神经退行性疾病的新型异种细胞疗法的意义。

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