趋化因子受体靶向可有效将抗原导向主要组织相容性复合体I类途径,并引发抗原特异性CD8+T细胞反应。
Chemokine receptor targeting efficiently directs antigens to MHC class I pathways and elicits antigen-specific CD8+ T-cell responses.
作者信息
Schiavo Roberta, Baatar Dolgor, Olkhanud Purevdorj, Indig Fred E, Restifo Nicholas, Taub Dennis, Biragyn Arya
机构信息
Laboratory of Immunology, Gerontology Research Center, National Institute on Aging, National Institutes of Health, Baltimore, MD 21224, USA.
出版信息
Blood. 2006 Jun 15;107(12):4597-605. doi: 10.1182/blood-2005-08-3207. Epub 2006 Mar 2.
Abstract
Chemokines are key controllers of cell trafficking and are involved in numerous pathologic and inflammatory conditions. However, the fate of a chemokine ligand, once it is endocytosed with its receptor, remains obscure. Here, using chemokine-tumor antigen fusion constructs, we demonstrate for the first time that chemokines are internalized to early/late endosomal and lysosomal compartments through a clathrin-dependent process and subsequently delivered to the cytosol for proteasomal processing, facilitating efficient cross-presentation to the TAP-1-dependent MHC class I processing pathway. These data not only elucidate the intracellular fate of chemokine ligands upon receptor uptake, but also demonstrate the superior carrier potency of chemokines for delivering self-antigens to both class I and II processing pathways to induce CD8(+) and CD4(+) T-cell responses.
摘要
趋化因子是细胞转运的关键调控因子,参与多种病理和炎症状态。然而,趋化因子配体一旦与其受体一起被内吞,其命运仍不清楚。在此,我们使用趋化因子 - 肿瘤抗原融合构建体,首次证明趋化因子通过网格蛋白依赖性过程被内化到早期/晚期内体和溶酶体区室,随后被递送至细胞质进行蛋白酶体加工,促进向TAP - 1依赖性MHC I类加工途径的有效交叉呈递。这些数据不仅阐明了趋化因子配体在受体摄取后的细胞内命运,还证明了趋化因子在将自身抗原递送至I类和II类加工途径以诱导CD8(+)和CD4(+) T细胞反应方面具有卓越的载体效能。
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