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Cytomegalovirus prevents antigen presentation by blocking the transport of peptide-loaded major histocompatibility complex class I molecules into the medial-Golgi compartment

机译：巨细胞病毒可通过阻止载有肽的主要组织相容性复合物I类分子转运至高尔基体内侧来阻止抗原呈递

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Selective expression of murine cytomegalovirus (MCMV) immediate-early (IE) genes leads to the presentation by the major histocompatibility complex (MHC) class I molecule Ld of a peptide derived from MCMV IE protein pp89 (Reddehase, M.J., J. B. Rothbard, and U.H. Koszinowski. 1989. Nature (Lond.). 337:651). Characterization of endogenous antigenic peptides identified the pp89 peptide as the nonapeptide 168YPHFMPTNL176 (del Val, M., H.-J. Schlicht, T. Ruppert, M.J. Reddehase, and U.H. Koszinowski. 1991. Cell. 66:1145). Subsequent expression of MCMV early genes prevents presentation of pp89 (del Val, M., K. Munch, M.J. Reddehase, and U.H. Koszinowski. 1989. Cell. 58:305). We report on the mechanism by which MCMV early genes interfere with antigen presentation. Expression of the IE promoter-driven bacterial gene lacZ by recombinant MCMV subjected antigen presentation of beta-galactosidase to the same control and excluded antigen specificity. The Ld-dependent presence of naturally processed antigenic peptides also in nonpresenting cells located the inhibitory function subsequent to the step of antigen processing. The finding that during the E phase of MCMV gene expression the MHC class I heavy chain glycosylation remained in an Endo H-sensitive form suggested a block within the endoplasmic reticulum/cis-Golgi compartment. The failure to present antigenic peptides was explained by a general retention of nascent assembled trimolecular MHC class I complexes. Accordingly, at later stages of infection a significant decrease of surface MHC class I expression was seen, whereas other membrane glycoproteins remained unaffected. Thus, MCMV E genes endow this virus with an effective immune evasion potential. These results also indicate that the formation of the trimolecular complex of MHC class I heavy chain, beta 2-microglobulin, and the finally trimmed peptide is completed before entering the medial-Golgi compartment.

机译：鼠巨细胞病毒（MCMV）即早（IE）基因的选择性表达导致主要组织相容性复合体（MHC）I类分子Ld呈现MCMV IE蛋白pp89（Reddehase，MJ，JB Rothbard和UH Koszinowski。1989. Nature（Lond。）。337：651）。内源性抗原肽的鉴定将pp89肽鉴定为九肽168YPHFMPTNL176（del Val，M.，H.-J.Schlicht，T.Ruppert，M.J.Reddehase，和U.H.Koszinowski.1991.Cell.66：1145）。 MCMV早期基因的后续表达阻止了pp89的表达（del Val，M.，K.Munch，M.J.Reddehase和U.H.Koszinowski.1989.Cell.58：305）。我们报告了MCMV早期基因干扰抗原呈递的机制。通过重组MCMV IE启动子驱动的细菌基因lacZ的表达使β-半乳糖苷酶的抗原呈递达到相同的对照，并排除了抗原特异性。天然加工的抗原肽的Ld依赖性存在也位于抗原加工步骤之后的抑制功能的非递呈细胞中。在MCMV基因表达的E期中，MHC I类重链糖基化仍以Endo H敏感的形式存在的发现表明，内质网/顺式高尔基体中存在一个阻滞。呈递抗原肽的失败是由于新生组装的三分子MHC I类复合物的总体保留所致。因此，在感染的后期，观察到I类表面MHC表达明显降低，而其他膜糖蛋白仍不受影响。因此，MCMV E基因赋予该病毒有效的免疫逃避潜力。这些结果还表明，MHC I类重链，β2-微球蛋白的三分子复合物的形成以及最后修饰的肽在进入内侧-高尔基体之前完成。

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1. Cytomegalovirus prevents antigen presentation by blocking the transport of peptide-loaded major histocompatibility complex class I molecules into the medial-Golgi compartment. [J] . M del Val, H Hengel, H H?cker, The Journal of Experomental Medicine . 1992,第3期

机译：CytomeGalovirus通过阻止肽加载的主要组织相容性复合体Is分子传输到内侧 - 高尔基室中来防止抗原呈递。
2. A SYNTHETIC RANDOM BASIC COPOLYMER WITH PROMISCUOUS BINDING TO CLASS II MAJOR HISTOCOMPATIBILITY COMPLEX MOLECULES INHIBITS T-CELL PROLIFERATIVE RESPONSES TO MAJOR AND MINOR HISTOCOMPATIBILITY ANTIGENS IN VITRO AND CONFERS THE CAPACITY TO PREVENT MUR [J] . Schlegel PG., Chen YF., Chen J., Proceedings of the National Academy of Sciences of the United States of America . 1996,第10期

机译：一种与II类主要组织相容性复杂结合的合成随机基本共聚物，可抑制T细胞对主要和次要的组织相容性抗原的体外反应，并赋予其预防能力
3. Human cytomegalovirus blocks interferon-gamma stimulated up-regulation of major histocompatibility complex class I expression and the class I antigen processing machinery. [J] . Miller DM, Zhang Y, Rahill BM, Transplantation: Official Journal of the Transplantation Society . 2000,第4期

机译：人类巨细胞病毒可阻断干扰素-γ刺激的主要组织相容性复合物I类表达和I类抗原加工机制的上调。
4. Prediction and Rule Extraction of Major Histocompatibility Complex Class II Epitopes by Logic Minimization [C] . C. Aguilar-Bonavides, R. Cruz-Cano, C. Lanzas International Conference on Bioinformatics and Computational Biology . 2014

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5. The binding and presentation of peptide antigens by class I major histocompatibility molecules. [D] . Huczko, Eric Lee. 1997

机译：Ⅰ类主要组织相容性分子对肽抗原的结合和呈递。
6. Cytomegalovirus prevents antigen presentation by blocking the transport of peptide-loaded major histocompatibility complex class I molecules into the medial-Golgi compartment [O] . 1992

机译：巨细胞病毒可通过阻止载有肽的主要组织相容性复合物I类分子转运至高尔基体内侧来阻止抗原呈递
7. Cytomegalovirus prevents antigen presentation by blocking the transport of peptide-loaded major histocompatibility complex class I molecules into the medial-Golgi compartment [O] . Del Val Margarita, Hengel Hartmut, Häcker Hans, 1992

机译：巨细胞病毒通过阻断载有肽的主要组织相容性复合物I类分子转运到内侧 - 高尔基体区来阻止抗原呈递
8. Apoptosis Use Case: In Silico Evaluation of a Library of Small Molecule Pharmacophore Models for Blocking the Formation of SEB-Major Histocompatibility Class II Complexes [R] . Hammamieh, R. 2007

机译：细胞凋亡用例：用于阻断sEB-主要组织相容性II类复合物形成的小分子药效团模型的silico评价

Cytomegalovirus prevents antigen presentation by blocking the transport of peptide-loaded major histocompatibility complex class I molecules into the medial-Golgi compartment

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