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CD4 T cell help is required for primary CD8 T cell responses to vesicular antigen delivered to dendritic cells in vivo.

机译:对于体内CD8 T细胞对囊泡抗原的初级CD8 T细胞应答,需要CD4 T细胞帮助。

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摘要

Insight into the mechanisms by which dendritic cells (DC) present exogenous antigen to T cells is of major importance in the design of vaccines. We examined the effectiveness of free antigen as well as antigen with lipopolysaccharide, emulsified in complete Freund's adjuvant, and antigen encapsulated in liposomes in activating adoptively transferred antigen-specific CD4 and CD8 T cells. When contained in liposomes, 100- to 1000-fold lower antigen amounts were as efficient in inducing proliferation and effector functions of CD4 and CD8 T cells in draining lymph nodes as other antigen forms. CD11c(+)/CD11b(+)/CD205(mod)/CD8alpha(-) DC that captured liposomes were activated and presented this form of antigen in an MHC class I- and class II-restricted manner. CD4 T cells differentiated into Th1 and Th2 effector cells. Primary expansion and cytotoxic activity of CD8 T cells were CD4 T cell-dependent and required the transporter associated with antigen processing (TAP). Finally, adoptively transferred CD4 and CD8 T cells were not deleted after primary immunization and rapidly responded to a secondary immunization with antigen-containing liposomes. In conclusion, encapsulation of antigen in liposomes is an efficient way of delivering antigen to DC for priming of both CD4 and CD8 T cell responses. Importantly, primary CD8 T cell responses were CD4 T cell-dependent.
机译:洞察树突状细胞(DC)向T细胞呈递外源抗原的机制在疫苗设计中至关重要。我们研究了游离抗原以及含脂多糖的抗原(在完全弗氏佐剂中乳化)和包裹在脂质体内的抗原在激活过继转移的抗原特异性CD4和CD8 T细胞中的有效性。当包含在脂质体中时,较低的抗原量可在引流淋巴结中诱导CD4和CD8 T细胞的增殖和效应功能,其效率低至其他抗原形式的100至1000倍。捕获脂质体的CD11c(+)/ CD11b(+)/ CD205(mod)/ CD8alpha(-)DC被激活并以MHC I类和II类限制的方式呈递这种形式的抗原。 CD4 T细胞分化为Th1和Th2效应细胞。 CD8 T细胞的原代扩增和细胞毒性活性是CD4 T细胞依赖性的,需要与抗原加工(TAP)相关的转运蛋白。最后,过继转移的CD4和CD8 T细胞在初次免疫后不会缺失,并迅速对含抗原脂质体的二次免疫作出反应。总之,将抗原包封在脂质体中是将抗原递送至DC的有效方法,用于引发CD4和CD8 T细胞反应。重要的是,主要的CD8 T细胞反应是CD4 T细胞依赖性的。

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