Dickgreber Nina, Stoitzner Patrizia, Bai Yan, Price Kylie M, Farrand Kathryn J, Manning Kristy, Angel Catherine E, Dunbar P Rod, Ronchese Franca, Fraser John D, Bäckström B Thomas, Hermans Ian F
Malaghan Institute of Medical Research, Wellington, New Zealand.
J Immunol. 2009 Feb 1;182(3):1260-9. doi: 10.4049/jimmunol.182.3.1260.
An efficient pathway of cross-presentation common to a range of dendritic cell (DC) populations was identified by targeting Ag to MHC class II molecules. This finding was achieved by conjugating Ag to M1, which is a modified version of the superantigen streptococcal mitogenic exotoxin Z-2 that binds to MHC class II molecules but cannot directly stimulate T cells. M1 conjugates were efficiently presented to CD4(+) and CD8(+) T cells by bone marrow-derived DC and Langerhans cells in vitro. Whereas nonconjugated Ag was preferentially cross-presented by splenic CD8alpha(+) DC in vivo, M1-conjugated Ag was cross-presented by all dendritic subtypes assessed. Potent effector T cell responses with antitumor activity were elicited when M1 conjugates were injected together with an adjuvant. This method of Ag delivery has significant potential in therapeutic applications.
通过将抗原靶向主要组织相容性复合体(MHC)II类分子,确定了一系列树突状细胞(DC)群体共有的有效交叉呈递途径。这一发现是通过将抗原与M1偶联实现的,M1是超抗原链球菌促有丝分裂外毒素Z-2的修饰版本,它能与MHC II类分子结合,但不能直接刺激T细胞。M1偶联物在体外被骨髓来源的DC和朗格汉斯细胞有效地呈递给CD4(+)和CD8(+) T细胞。在体内,未偶联的抗原优先由脾脏CD8α(+) DC交叉呈递,而M1偶联的抗原则由所有评估的树突状细胞亚型交叉呈递。当M1偶联物与佐剂一起注射时,会引发具有抗肿瘤活性的强效效应T细胞反应。这种抗原递送方法在治疗应用中具有巨大潜力。
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