首页> 外文期刊>Transplantation: Official Journal of the Transplantation Society >Isolation of regulatory T cells in the skin of a human hand-allograft, up to six years posttransplantation.
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Isolation of regulatory T cells in the skin of a human hand-allograft, up to six years posttransplantation.

机译:移植后长达六年的时间,在人手同种异体移植皮肤中分离调节性T细胞。

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BACKGROUND: A bilateral hand allotransplantation was performed in a patient six years ago. Whereas skin is known to be highly immunogenic, grafts have been well accepted up to now. Therefore, here we investigated the putative presence of regulatory T cells in the graft. METHODS: Skin biopsies were performed at different time points and analyzed by immunochemistry. T cells were initially expanded with interleukin (IL)-2. In the latter biopsy, skin was directly analyzed by reverse-transcriptase polymerase chain reaction without any culture. RESULTS: When tested against donor mononuclear cells, donor-primed skin T cells demonstrated unresponsiveness and inhibited donor-directed blood T cell alloresponse. Moreover, their T-cell receptor-Vbeta repertoire was skewed, in contrast to that of peripheral blood T cells. Retrospectively, nuclear FoxP3 expression in skin was measured by immunohistochemistry and was found positive at that time, but appeared to increase with time. This result was supported by the measurement of FoxP3 messenger RNA (mRNA) expression in the latter fresh biopsy, which showed higher levels than that of blood, together with no expression of perforin mRNA, but increased expression of transforming growth factor-beta and IL-10. No FoxP3 mRNA expression was found in the contralateral leg, due to the absence of T cell infiltrate. CONCLUSION: This study shows the presence of the FoxP3 marker, in a well accepted human composite tissue allograft, up to six years posttransplantation. Because a suppressive cytokinic profile was also detected intragraft, in the absence of perforin mRNA expression, our data suggest that regulatory T cells could play a role in the long-term survival of this allograft.
机译:背景:六年前在一名患者中进行了双侧同种异体手移植。尽管已知皮肤具有高度免疫原性,但迄今为止,移植物已被广泛接受。因此,这里我们研究了移植物中调节性T细胞的假定存在。方法:在不同时间点进行皮肤活检并通过免疫化学分析。 T细胞最初用白介素(IL)-2扩增。在后者的活检中,无需任何培养即可通过逆转录酶聚合酶链反应直接分析皮肤。结果:当针对供体单核细胞进行测试时,供体引发的皮肤T细胞表现出无反应性,并抑制了供体定向的血液T细胞的过敏反应。而且,与外周血T细胞相反,它们的T细胞受体-Vbeta库是偏斜的。回顾性地,通过免疫组织化学测量了皮肤中的核FoxP3表达,并且在那个时候发现它是阳性的,但是似乎随着时间增加。这一结果得到了后者新鲜活检中FoxP3信使RNA(mRNA)表达的测量的支持,该水平显示出比血液更高的水平,并且无穿孔素mRNA表达,但转化生长因子-β和IL- 10。由于没有T细胞浸润,在对侧腿中未发现FoxP3 mRNA表达。结论:这项研究表明,在移植后长达六年的时间里,FoxP3标记存在于公认的人类复合组织同种异体移植物中。因为在移植物中也检测到抑制性的细胞因子,所以在缺乏穿孔素mRNA表达的情况下,我们的数据表明调节性T细胞可能在同种异体移植物的长期存活中发挥作用。

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