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米诺环素通过抑制晚期小胶质细胞激活和 T 细胞募集促进脑内神经元移植的长期存活。

Minocycline promotes long-term survival of neuronal transplant in the brain by inhibiting late microglial activation and T-cell recruitment.

机构信息

INSERM, UMR, Nantes, France.

出版信息

Transplantation. 2010 Apr 15;89(7):816-23. doi: 10.1097/TP.0b013e3181cbe041.

DOI:10.1097/TP.0b013e3181cbe041
PMID:20216486
Abstract

BACKGROUND

Cell therapy in the brain is limited by the requirement of high doses of immunosuppressors that have harmful side effects, and often, it cannot prevent the ultimate rejection of the transplanted cells. Alternative treatments that replace or enable a reduction in the doses of usual immunosuppressors have to be found. In this regard, minocycline shows potential as therapeutic agent. This drug crosses the blood-brain barrier, has good safety records, and exhibits strong antiinflammatory effects.

METHODS

To study the impact of minocycline on the survival of intracerebral transplant, 400,000 porcine fetal neurons were transplanted into the striatum of rats treated daily with minocycline until sacrifice. Graft survival and immunologic reaction were evaluated by immunohistochemistry.

RESULTS

In the control groups, all the grafts were rejected at day 63, whereas healthy grafts exhibiting tyrosine hydroxylase neurons were observed in 40% of the treated rats. The low immunoreactivity for ED1 and R73 in treated rats when compared with the control groups suggests that minocycline promotes long-term survival of neuronal xenograft by inhibiting microglial activation and T-cell recruitment.

CONCLUSIONS

Our present data provide the first evidence of an effect of minocycline on the host immune response after neuronal transplantation into the brain. This observation raises new perspectives concerning the use of minocycline and provides basis for the development of safe and efficient immunosuppressive protocols for intracerebral transplantation.

摘要

背景

脑内细胞疗法受到需要大剂量免疫抑制剂这一限制,而免疫抑制剂具有有害的副作用,而且往往不能防止移植细胞的最终排斥。必须寻找替代治疗方法,以替代或减少常用免疫抑制剂的剂量。在这方面,米诺环素显示出作为治疗剂的潜力。这种药物可以穿过血脑屏障,具有良好的安全性记录,并具有很强的抗炎作用。

方法

为了研究米诺环素对脑内移植存活的影响,将 40 万个猪胎神经元移植到接受米诺环素治疗的大鼠纹状体中,直至处死。通过免疫组织化学评估移植物的存活和免疫反应。

结果

在对照组中,所有移植物在第 63 天被排斥,而在接受治疗的大鼠中,有 40%观察到酪氨酸羟化酶神经元的健康移植物。与对照组相比,治疗组 ED1 和 R73 的低免疫反应性表明,米诺环素通过抑制小胶质细胞激活和 T 细胞募集,促进神经元异种移植物的长期存活。

结论

我们目前的数据首次提供了米诺环素对脑内神经元移植后宿主免疫反应的影响的证据。这一观察结果为米诺环素的使用提供了新的视角,并为脑内移植的安全有效的免疫抑制方案的开发提供了依据。

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