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在小鼠模型中,角膜非感染性炎症和同种异体致敏中,眼表面抗原呈递细胞亚群的时间依赖性系列变化是不同的。

Time-Dependent Serial Changes of Antigen-Presenting Cell Subsets in the Ocular Surface Are Distinct between Corneal Sterile Inflammation and Allosensitization in a Murine Model.

机构信息

Laboratory of Ocular Regenerative Medicine and Immunology, Biomedical Research Institute, Seoul National University Hospital, 103 Daehak-ro, Jongno-gu, Seoul 03080, Korea.

Department of Ophthalmology, College of Medicine, Chung-Ang University, 102 Heukseok-ro, Dongjak-gu, Seoul 06973, Korea.

出版信息

Cells. 2021 Aug 26;10(9):2210. doi: 10.3390/cells10092210.

Abstract

The kinetics of antigen-presenting cells (APCs) vary depending on their resident tissues and the manner of immunization. We investigated the long-term changes in mature APC and T-cell subsets over 4 weeks in the ocular surface in murine models of corneal quiescent or potent sterile inflammation, and allosensitization using partial (PT), syngeneic (Syn), and allogeneic (Allo) corneal transplantation. In PT, CD11bCD11cMHCIICD86 cells increased until 4 weeks with an increase in IFNγ T cells. In Syn, both CD11bCD11cMHCIICD86 and CD11bCD11cMHCIICD86 APC subsets increased until 4 weeks with a brief increase in CD69 T cells at 2 weeks. In Allo, CD11bCD11cMHCIICD86 and CD11bCD11cMHCIICD86 APC subsets increased until 4 weeks, and an early increase in CD69 T cells was observed at 2 weeks followed by a late increase in IFNγ T cells at 4 weeks. The frequency of the IFNγ T cell subset was positively correlated with the frequency of the CD11bCD11cMHCIICD86 subset, indicating the existence of APC-T cell interaction in the ocular surface. Together, the results indicate that allosensitization in mature APCs leads to T-cell activation in the ocular surface, whereas sterile inflammation merely induces a brief and non-specific T-cell activation in the ocular surface.

摘要

抗原提呈细胞(APCs)的动力学因驻留组织和免疫方式而异。我们研究了角膜静止或有效无菌性炎症以及部分(PT)、同基因(Syn)和同种异体(Allo)角膜移植的小鼠模型中,眼表中成熟 APC 和 T 细胞亚群在 4 周内的长期变化。在 PT 中,CD11bCD11cMHCIICD86 细胞增加,直到第 4 周,IFNγ T 细胞增加。在 Syn 中,CD11bCD11cMHCIICD86 和 CD11bCD11cMHCIICD86 APC 亚群均增加,直到第 4 周,第 2 周 CD69 T 细胞短暂增加。在 Allo 中,CD11bCD11cMHCIICD86 和 CD11bCD11cMHCIICD86 APC 亚群增加,直到第 4 周,第 2 周 CD69 T 细胞早期增加,第 4 周 IFNγ T 细胞晚期增加。IFNγ T 细胞亚群的频率与 CD11bCD11cMHCIICD86 亚群的频率呈正相关,表明眼表存在 APC-T 细胞相互作用。综上所述,结果表明同种异体致敏导致成熟 APC 中的 T 细胞活化,而无菌性炎症仅在眼表面引起短暂的非特异性 T 细胞活化。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/15ac/8467177/b368b4134edd/cells-10-02210-g001.jpg

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