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将抗原从内吞区室递送至胞质溶胶以进行交叉呈递仅限于早期未成熟树突状细胞。

The delivery of an antigen from the endocytic compartment into the cytosol for cross-presentation is restricted to early immature dendritic cells.

作者信息

Hotta Chie, Fujimaki Haruka, Yoshinari Masahiro, Nakazawa Masatoshi, Minami Mutsuhiko

机构信息

Department of Immunology, Yokohama City University School of Medicine, Yokohama, Japan.

出版信息

Immunology. 2006 Jan;117(1):97-107. doi: 10.1111/j.1365-2567.2005.02270.x.

Abstract

Dendritic cells (DCs) are the only antigen-presenting cell population having a cross-presentation capacity. For cross-presentation, however, the intracellular antigen-processing pathway and its regulatory mechanism have not been defined. Here we report the differences in cross-presentation ability among murine bone marrow-derived immature DC, early immature day8-DC and late immature day10-DC, and fully mature day10 + lipopolysaccharide DC. Day8-DCs and day10-DCs show an immature phenotypic profile but are different in morphology. Day8-DCs can internalize an abundant volume of exogenous soluble ovalbumin (OVA) and result in cross-presentation. In contrast, day10-DCs are not able to cross-present, although they maintain efficient macropinocytosis. Exogenously internalized OVA antigens are stored in the endocytic compartments. The endocytic compartments are temporarily maintained at mildly acidic pH in day8-DCs and are rapidly acidified in day10-DCs after uptake of antigens. We show that OVA antigens accumulated in the endocytic compartments move into the cytosol in day8-DCs but do not in day10-DCs. NH(4)Cl-treatment, which neutralizes the acidic endocytic compartments and/or delays endosomal maturation, restores day10-DCs for transport the stored OVA antigens from the endocytic compartments into the cytosol. Diphenyleneiodonium chloride-treatment, which acidifies the endocytic compartments, decreases an amount of transported OVA antigen into the cytosol in day8-DCs. These data indicate that only the early immature stage of DC interferes with endosomal maturation, even after uptake of exogenous antigens, and then transports the antigens into the cytosol.

摘要

树突状细胞(DCs)是唯一具有交叉呈递能力的抗原呈递细胞群体。然而,对于交叉呈递而言,细胞内抗原加工途径及其调控机制尚未明确。在此,我们报告了小鼠骨髓来源的未成熟DC、早期未成熟的第8天DC和晚期未成熟的第10天DC以及完全成熟的第10天+脂多糖DC之间交叉呈递能力的差异。第8天DC和第10天DC呈现未成熟的表型特征,但形态不同。第8天DC能够内化大量外源性可溶性卵清蛋白(OVA)并导致交叉呈递。相比之下,第10天DC虽然保持高效的巨胞饮作用,但无法进行交叉呈递。外源性内化的OVA抗原存储在内吞小室中。内吞小室在第8天DC中暂时维持在轻度酸性pH值,而在摄取抗原后第10天DC中迅速酸化。我们发现,在第8天DC中,积累在内吞小室中的OVA抗原会进入细胞质,而在第10天DC中则不会。NH(4)Cl处理可中和酸性内吞小室和/或延迟内体成熟,使第10天DC恢复将储存的OVA抗原从内吞小室转运到细胞质中的能力。二苯基碘鎓氯化物处理可酸化内吞小室,减少第8天DC中转运到细胞质中的OVA抗原量。这些数据表明,只有DC的早期未成熟阶段即使在摄取外源性抗原后也会干扰内体成熟,然后将抗原转运到细胞质中。

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