Expression of TNF-related apoptosis-inducing ligand (TRAIL) in keratinocytes mediates apoptotic cell death in allogenic T cells.

Kerstin Reimers, Christine Radtke, Claudia Y Choi, Christina Allmeling, Susanne Kall, Paul Kiefer, Thomas Muehlberger, Peter M Vogt
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引用次数: 4

Abstract

The objective of the present study was to evaluate the aptitude of TRAIL gene expression for inducing apoptosis in co-cultivated T-cells. This should allow preparing a strategy for the development of a durable, allogenic skin substitute based on the induction of an immune-privileged transplant. In order to counteract the significant potential of rejection in transplanted allogenic keratinocytes, we created a murine keratinocyte cell line which expressed TRAIL through stable gene transfer. The exogenic protein was localized on the cellular surface and was not found in soluble condition as sTRAIL. Contact to TRAIL expressing cells in co-culture induced cell death in sensitive Jurkat-cells, which was further intensified by lymphocyte activation. This cytotoxic effect is due to the induction of apoptosis. We therefore assume that the de-novo expression of TRAIL in keratinocytes can trigger apoptosis in activated lymphocytes and thus prevent the rejection of keratinocytes in allogenic, immune-privileged transplants.

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Abstract Image

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角质形成细胞中tnf相关凋亡诱导配体(TRAIL)的表达介导同种异体T细胞的凋亡细胞死亡。
本研究的目的是评估TRAIL基因表达诱导共培养t细胞凋亡的能力。这应该可以为开发一种基于诱导免疫特权移植的持久的同种异体皮肤替代品制定策略。为了抵消移植异体角化细胞的排斥反应,我们通过稳定的基因转移创造了一种表达TRAIL的小鼠角化细胞细胞系。外源蛋白定位于细胞表面,在可溶性条件下未发现sTRAIL。在共培养中与TRAIL表达细胞接触可诱导敏感jurkat细胞死亡,并通过淋巴细胞活化进一步加剧。这种细胞毒性作用是由于诱导细胞凋亡。因此,我们假设在角质形成细胞中去novo表达TRAIL可以触发活化淋巴细胞的凋亡,从而防止异体免疫特权移植中角质形成细胞的排斥反应。
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