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髓系树突状细胞分化过程中表面II类主要组织相容性复合体蛋白的构象变化伴随着溶酶体MIIC的结构改变。

Conformational variation of surface class II MHC proteins during myeloid dendritic cell differentiation accompanies structural changes in lysosomal MIIC.

作者信息

Potolicchio Ilaria, Chitta Sriram, Xu Xiaonan, Fonseca Dora, Crisi Giovanna, Horejsi Vaclav, Strominger Jack L, Stern Lawrence J, Raposo Graca, Santambrogio Laura

机构信息

Department of Pathology Albert Einstein College of Medicine, New York, NY 10461, USA.

出版信息

J Immunol. 2005 Oct 15;175(8):4935-47. doi: 10.4049/jimmunol.175.8.4935.

DOI:10.4049/jimmunol.175.8.4935
PMID:16210595
Abstract

Dendritic cells (DC), uniquely among APC, express an open/empty conformation of MHC class II (MHC-II) proteins (correctly folded molecules lacking bound peptides). Generation and trafficking of empty HLA-DR during DC differentiation are investigated here. HLA-DR did not fold as an empty molecule in the endoplasmic reticulum/trans-Golgi network, did not derived from MHC/Ii complexes trafficking to the cell surface, but was generated after invariant chain degradation within lysosomal-like MHC-II rich compartments (MIIC). In pre-DC, generated from monocytes cultured in the presence of GM-CSF, Lamp-1(+)MHC-II(+) compartments are predominantly electron dense and, in these cells, empty MHC-II molecules accounts for as much as 20% of total surface HLA-DR. In immature DC, generated in presence of GM-CSF and IL-4, empty HLA-DR reside in multilamellar MIIC, but are scarcely observed at the cell surface. Thus, the morphology/composition of lysosomal MIIC at different DC maturational stages appear important for surface egression or intracellular retention of empty HLA-DR. Ag loading can be achieved for the fraction of empty HLA-DR present in the "peptide-receptive" form. Finally, in vivo, APC-expressing surface empty HLA-DR were found in T cell areas of secondary lymphoid organs.

摘要

树突状细胞(DC)在抗原呈递细胞中独具特色,其表达的MHC II类(MHC-II)蛋白呈开放/空的构象(即正确折叠但缺乏结合肽的分子)。本文研究了DC分化过程中空的HLA-DR的产生和转运情况。HLA-DR并非在内质网/反式高尔基体网络中折叠为空分子,也并非源自转运至细胞表面的MHC/Ii复合物,而是在富含MHC-II的溶酶体样区室(MIIC)内恒定链降解后产生的。在由存在GM-CSF的单核细胞培养生成的前体DC中,Lamp-1(+)MHC-II(+)区室主要为电子致密区,在这些细胞中,空的MHC-II分子占总表面HLA-DR的20%。在存在GM-CSF和IL-4的情况下生成的未成熟DC中,空的HLA-DR存在于多层MIIC中,但在细胞表面几乎观察不到。因此,不同DC成熟阶段溶酶体MIIC的形态/组成对于空的HLA-DR的表面逸出或细胞内保留似乎很重要。对于以“肽接受性”形式存在的空HLA-DR部分,可以实现抗原加载。最后,在体内,在二级淋巴器官的T细胞区域发现了表达表面空HLA-DR的抗原呈递细胞。

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