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The Potent Adjuvant Activity of Archaeosomes Correlates to the Recruitment and Activation of Macrophages and Dendritic Cells In Vivo

机译:古细菌的有效佐剂活性与体内巨噬细胞和树突状细胞的招募和活化有关。

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The unique glycerolipids of Archaea can be formulated into vesicles (archaeosomes) with potent adjuvant activity. We studied the effect of archaeosomes on APCs to elucidate the mechanism(s) of adjuvant action. Exposure of J774A.1 macrophages to archaeosomes in vitro resulted in up-regulation of B7.1, B7.2, and MHC class II molecules to an extent comparable to that achieved with LPS. Similarly, incubation of bone marrow-derived DCs with archaeosomes resulted in enhanced expression of MHC class II and B7.2 molecules. In contrast, conventional liposomes made from ester phospholipids failed to modulate the expression of these activation markers. APCs treated with archaeosomes exhibited increased TNF production and functional ability to stimulate allogenic T cell proliferation. More interestingly, archaeosomes enhanced APC recruitment and activation in vivo. Intraperitoneal injection of archaeosomes into mice led to recruitment of Mac1α+, F4/80+ and CD11c+ cells. The expression of MHC class II on the surface of peritoneal cells was also enhanced. Furthermore, peritoneal cells from archaeosome-injected mice strongly enhanced allo-T cell proliferation and cytokine production. The ability of archaeosome-treated APCs to stimulate T cells was restricted to Mac1αhigh, B220? cells in the peritoneum. These Mac1αhigh cells in the presence of GM-CSF gave rise to both F4/80+ (macrophage) and CD11c+ (dendritic) populations. Overall, the activation of APCs correlated to the ability of archaeosomes to induce strong humoral, T helper, and CTL responses to entrapped Ag. Thus, the recruitment and activation of professional APCs by archaeosomes constitutes an efficient self-adjuvanting process for induction of Ag-specific responses to encapsulated Ags.
机译:古生菌的独特甘油脂可以配制成具有有效佐剂活性的囊泡(古生菌体)。我们研究了古细菌对APC的影响,以阐明佐剂作用的机制。 J774A.1巨噬细胞在体外暴露于古细菌导致B7.1,B7.2和MHC II类分子的上调至与LPS相当的程度。同样,将骨髓来源的DC与古细菌一起孵育会导致II类MHC和B7.2分子表达增强。相反,由酯磷脂制成的常规脂质体不能调节这些活化标志物的表达。用古细菌处理的APC表现出增加的TNF产生和刺激同种异体T细胞增殖的功能能力。更有趣的是,古细菌增强了体内APC的募集和激活。向小鼠腹膜内注射古细菌导致Mac1α+,F4 / 80 +和CD11c +细胞募集。 MHC II类在腹膜细胞表面的表达也得到增强。此外,来自注射古细菌的小鼠的腹膜细胞强烈增强了同种异体T细胞的增殖和细胞因子的产生。经古细菌处理的APC刺激T细胞的能力仅限于Mac1αhigh,B220?腹膜中的细胞。在GM-CSF存在的情况下,这些Mac1α高细胞同时导致F4 / 80 +(巨噬细胞)和CD11c +(树突状细胞)种群的出现。总体而言,APC的激活与古细菌诱导强烈的体液,T辅助物和CTL对捕获的Ag的反应能力有关。因此,古细菌对专业APC的募集和激活构成了一种有效的自佐剂过程,用于诱导对封装的Ag的Ag特异性反应。

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