体内天然免疫原性热休克蛋白的细胞哨兵的鉴定。
Identification of the cellular sentinels for native immunogenic heat shock proteins in vivo.
机构信息
Department of Immunology, University of Pittsburgh, Pittsburgh, PA 15261;
出版信息
J Immunol. 2013 Oct 15;191(8):4456-65. doi: 10.4049/jimmunol.1300827. Epub 2013 Sep 18.
Abstract
Select members of the heat shock proteins (HSPs) family, such as gp96, elicit immune responses specific to their chaperoned peptides. Although immunologic effects of HSPs on APCs described to date have largely been demonstrated with cell lines or primary cells in culture, their collective responses in vitro have been consistent with priming immune responses. In this study, we examine the physiologically relevant APCs in mice that are targeted after vaccination with native, murine HSPs, and we characterize those cells. Gp96 accesses the subcapsular region of the draining lymph node, and it is internalized predominantly by CD11b(+) cells in this locale. Cells acquiring gp96 can transfer protective antitumor immunity to naive mice by actively cross-presenting gp96-chaperoned peptides and providing costimulation. Our studies illustrate how HSPs act to alert the immune system of cellular damage and will be of paramount importance in immunotherapy of patients with cancer and infectious disease.
摘要
选择热休克蛋白 (HSPs) 家族的成员,如 gp96,可引发针对其伴侣肽的特异性免疫反应。尽管迄今为止描述的 HSPs 对 APCs 的免疫作用在很大程度上是通过细胞系或原代细胞在培养中证明的,但它们在体外的总体反应与免疫原性一致。在这项研究中,我们研究了接种天然、鼠 HSP 后靶向的生理相关 APCs,并对这些细胞进行了表征。gp96 进入引流淋巴结的被膜下区域,并且它主要被该部位的 CD11b(+) 细胞内化。获得 gp96 的细胞可以通过主动交叉呈递 gp96 伴侣肽并提供共刺激来将保护性抗肿瘤免疫转移给幼稚小鼠。我们的研究说明了 HSPs 如何作用以提醒免疫系统细胞损伤,这对于癌症和传染病患者的免疫治疗将至关重要。
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