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人T细胞的TCR激活可诱导携带TCR/CD3/ζ复合体的外泌体产生。

TCR activation of human T cells induces the production of exosomes bearing the TCR/CD3/zeta complex.

作者信息

Blanchard Nicolas, Lankar Danielle, Faure Florence, Regnault Armelle, Dumont Céline, Raposo Graça, Hivroz Claire

机构信息

Institut National de la Santé et de la Recherche Médicale, Unité 520, Institut Curie, Paris, France.

出版信息

J Immunol. 2002 Apr 1;168(7):3235-41. doi: 10.4049/jimmunol.168.7.3235.

DOI:10.4049/jimmunol.168.7.3235
PMID:11907077
Abstract

We show in this study that human T cells purified from peripheral blood, T cell clones, and Jurkat T cells release microvesicles in the culture medium. These microvesicles have a diameter of 50-100 nm, are delimited by a lipidic bilayer membrane, and bear TCR beta, CD3epsilon, and zeta. This microvesicle production is regulated because it is highly increased upon TCR activation, whereas another mitogenic signal, such as PMA and ionomycin, does not induce any release. T cell-derived microvesicles also contain the tetraspan protein CD63, suggesting that they originate from endocytic compartments. They contain adhesion molecules such as CD2 and LFA-1, MHC class I and class II, and the chemokine receptor CXCR4. These transmembrane proteins are selectively sorted in microvesicles because CD28 and CD45, which are highly expressed at the plasma membrane, are not found. The presence of phosphorylated zeta in these microvesicles suggests that the CD3/TCR found in the microvesicles come from the pool of complexes that have been activated. Proteins of the transduction machinery, tyrosine kinases of the Src family, and c-Cbl are also observed in the T cell-derived microvesicles. Our data demonstrate that T lymphocytes produce, upon TCR triggering, vesicles whose morphology and phenotype are reminiscent of vesicles of endocytic origin produced by many cell types and called exosomes. Although the exact content of T cell-derived exosomes remains to be determined, we suggest that the presence of TCR/CD3 at their surface makes them powerful vehicles to specifically deliver signals to cells bearing the right combination of peptide/MHC complexes.

摘要

我们在本研究中表明,从外周血中纯化的人T细胞、T细胞克隆和Jurkat T细胞在培养基中释放微泡。这些微泡直径为50 - 100纳米,由脂质双层膜界定,并带有TCRβ、CD3ε和ζ链。这种微泡产生是受调控的,因为在TCR激活时其产量会大幅增加,而另一种促有丝分裂信号,如佛波酯(PMA)和离子霉素,不会诱导任何释放。T细胞衍生的微泡还含有四跨膜蛋白CD63,表明它们起源于内吞区室。它们含有黏附分子,如CD2和淋巴细胞功能相关抗原-1(LFA-1)、MHC I类和II类分子以及趋化因子受体CXCR4。这些跨膜蛋白在微泡中被选择性分选,因为在质膜上高表达的CD28和CD45未被发现。这些微泡中存在磷酸化的ζ链,表明微泡中的CD3/TCR来自已被激活的复合物池。在T细胞衍生的微泡中也观察到转导机制的蛋白质、Src家族的酪氨酸激酶和c-Cbl。我们的数据表明,T淋巴细胞在TCR触发时产生的囊泡,其形态和表型让人联想到许多细胞类型产生的内吞起源的囊泡,即外泌体。尽管T细胞衍生的外泌体的确切成分仍有待确定,但我们认为其表面存在TCR/CD3使其成为强大的载体,能够将信号特异性地传递给带有正确肽/MHC复合物组合的细胞。

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J Immunol. 2002 Apr 1;168(7):3235-41. doi: 10.4049/jimmunol.168.7.3235.
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