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CD8 高表达 CD56+ T 细胞是活动性白塞氏葡萄膜炎患者的细胞毒性效应细胞。

CD8brightCD56+ T cells are cytotoxic effectors in patients with active Behcet's uveitis.

作者信息

Ahn Jae Kyoun, Chung Hum, Lee Dong-sup, Yu Young Suk, Yu Hyeong Gon

机构信息

Department of Ophthalmology, Seoul National University College of Medicine, Seoul Artificial Eye Center, Seoul National University Hospital Clinical Research Institute, Seoul, Korea.

出版信息

J Immunol. 2005 Nov 1;175(9):6133-42. doi: 10.4049/jimmunol.175.9.6133.

Abstract

Behçet's uveitis, characterized by chronic recurrent uveitis and obliterating retinal vasculitis, frequently causes bilateral blindness. Intraocular infiltration of TCRalphabeta+CD8brightCD56+ cells was a distinct feature in Behçet's uveitis. However, phenotypic natures and effector functions of the cells have remained elusive. This study was conducted to determine phenotypic and functional characteristics and cytotoxic mechanisms of CD8brightCD56+ T cells in Behçet's uveitis. CD11b+CD27-CD62L- phenotypes of CD8brightCD56+ T cells were increased in patients with active Behçet's uveitis compared with inactive Behcet's patients and normal controls. Interestingly, CD45RAdimCD45RO- phenotypes were expanded, and CD94 expression was markedly up-regulated in contrast to the down-regulation of NKG2D. Furthermore, these subsets were polarized to produce IFN-gamma and contained high amounts of preformed intracellular perforin while exclusively expressing surface FasL upon PI stimulation. Moreover, the cytolytic functions of freshly isolated CD8brightCD56+ T cells were up-regulated against both K562 (NK-sensitive) and Raji (NK-resistant) cells, which were effectively inhibited by perforin inhibitor (concanamycin A). Their cytolytic activity against HUVECs was also increased and was effectively suppressed by Fas ligand inhibitor (brefeldin A) and partly by perforin inhibitor. Furthermore, cytolytic functions of PMA and ionomycin-stimulated CD8brightCD56+ T cells against HUVECs were greatly enhanced, by pretreatment of recombinant human IFN-gamma on HUVECs. Therefore, CD8brightCD56+ T cells in Behçet's uveitis are characterized by cytotoxic effector phenotypes with functional NK receptors and function as strong cytotoxic effectors through both Fas ligand-dependent and perforin-dependent pathways.

摘要

白塞氏葡萄膜炎以慢性复发性葡萄膜炎和闭塞性视网膜血管炎为特征,常导致双眼失明。TCRαβ⁺CD8brightCD56⁺细胞的眼内浸润是白塞氏葡萄膜炎的一个显著特征。然而,这些细胞的表型性质和效应功能仍不清楚。本研究旨在确定白塞氏葡萄膜炎中CD8brightCD56⁺T细胞的表型和功能特征以及细胞毒性机制。与非活动性白塞氏病患者和正常对照相比,活动性白塞氏葡萄膜炎患者中CD8brightCD56⁺T细胞的CD11b⁺CD27⁻CD62L⁻表型增加。有趣的是,CD45RAdimCD45RO⁻表型扩大,与NKG2D的下调相反,CD94表达明显上调。此外,这些亚群极化产生IFN-γ,含有大量预先形成的细胞内穿孔素,同时在PI刺激下仅表达表面FasL。此外,新鲜分离的CD8brightCD56⁺T细胞对K562(NK敏感)和Raji(NK耐药)细胞的细胞溶解功能上调,穿孔素抑制剂( concanamycin A)可有效抑制这种上调。它们对HUVECs的细胞溶解活性也增加,Fas配体抑制剂(布雷菲德菌素A)可有效抑制,穿孔素抑制剂部分抑制。此外,通过重组人IFN-γ预处理HUVECs,PMA和离子霉素刺激的CD8brightCD56⁺T细胞对HUVECs的细胞溶解功能大大增强。因此,白塞氏葡萄膜炎中的CD8brightCD56⁺T细胞具有带有功能性NK受体的细胞毒性效应表型,并通过Fas配体依赖性和穿孔素依赖性途径发挥强大的细胞毒性效应。

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