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T-cell engineering by a chimeric T-cell receptor with antibody-type specificity for the HIV-1 gp120

机译:通过嵌合T细胞受体的T细胞工程,其具有针对HIV-1 gp120的抗体型特异性

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摘要

Immune-based approaches of cell therapy against viral pathogens such as the human immunodeficiency virus type 1 (HIV-1) could be of primary importance for the control of this viral infection. Here, we designed a chimeric cell surface receptor (105TCR) to provide primary human T-lymphocytes with antibody-type specificity for the HIV-1 envelope glycoprotein.\udThis receptor includes the single chain Fv domain of the neutralizing anti-gp120 human monoclonal antibody F105, CD8a hinge and the transmembrane and the cytoplasmic domains of TCRz. Our results show that 105TCR is expressed at the cellular surface and is capable of recognizing the HIV-1 envelope glycoprotein inducing highly efficient effector T-cell responses, including extracellular signal-regulated kinase phosphorylation and cytokine secretion. Moreover, human primary CD8+ T-lymphocytes transduced by oncoretroviral and lentiviral vectors containing the 105TCR gene are able to mediate in vitro-specific cytolysis of envelope-expressing cells and HIV-1-infected CD4+ T-lymphocytes. These findings suggest that 105TCR is particularly suited for in vivo efficacy studies.
机译:基于病毒的针对病毒病原体(例如人类免疫缺陷病毒1型(HIV-1))的细胞疗法可能对于控制这种病毒感染至关重要。在这里,我们设计了一种嵌合细胞表面受体(105TCR),以为人类T淋巴细胞提供针对HIV-1包膜糖蛋白的抗体类型特异性。\ ud该受体包括中和性抗gp120人类单克隆抗体的单链Fv结构域F105,CD8a铰链和TCRz的跨膜和胞质域。我们的结果表明105TCR在细胞表面表达,并且能够识别HIV-1包膜糖蛋白,诱导高效的效应T细胞反应,包括细胞外信号调节的激酶磷酸化和细胞因子的分泌。而且,由包含105TCR基因的抗核内转录病毒和慢病毒载体转导的人原代CD8 + T淋巴细胞能够介导表达包膜的细胞和HIV-1感染的CD4 + T淋巴细胞的体外特异性细胞溶解。这些发现表明105TCR特别适用于体内功效研究。

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