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小鼠艾滋病中的CD4 T细胞无反应性:通过CD28共刺激以及添加白细胞介素-12不足以挽救无反应性CD4 T细胞。

CD4 T cell anergy in murine AIDS: costimulation via CD28 and the addition of IL-12 are not sufficient to rescue anergic CD4 T cells.

作者信息

Andrews C, Swain S L, Muralidhar G

机构信息

The Scripps Research Institute, La Jolla, CA 92037, USA.

出版信息

J Immunol. 1997 Sep 1;159(5):2132-8.

PMID:9278299
Abstract

Murine acquired immunodeficiency syndrome (MAIDS) is a fatal disease induced by a mixture of retroviruses known as BM5. It is characterized by splenomegaly, lymphadenopathy, hypergammaglobulinemia, loss of T and B cell function, and development of B cell lymphomas. As the disease progresses, by wk 8 of infection, CD4 T cell response to Ags and mitogens is severely curtailed and the CD4 T cell population becomes anergic. We examined responses of anergic CD4 T cells upon addition of a costimulatory signal (anti-CD28) and a cytokine (IL-12), which might help to restore the function of cells. We report that proliferation and cytokine production were restored in the early stages of infection by the strategies we tested, but not at later stages when anergy was well established. We also examined the effect of the same treatments on anergy of CD4 T cells from thymectomized, BM5-infected mice to determine whether the rescue seen was due to cells freshly derived from the thymus. We report that proliferation and cytokine production decreased in thymectomized mice even at wk 4 of infection, indicating that cells that are freshly derived from thymus are the ones responding to treatment. This study indicates that once anergy has been established in MAIDS, it cannot be reversed by providing costimulation via CD28 and IL-12. Anergy of CD4 T cells in MAIDS appears to be different from that seen in other systems, both in underlying cause and in the ability of the cells to revert to a normal state.

摘要

小鼠获得性免疫缺陷综合征(MAIDS)是一种由称为BM5的逆转录病毒混合物诱导的致命疾病。其特征为脾肿大、淋巴结病、高球蛋白血症、T和B细胞功能丧失以及B细胞淋巴瘤的发生。随着疾病进展,在感染第8周时,CD4 T细胞对抗原和丝裂原的反应严重减弱,且CD4 T细胞群体变得无反应性。我们研究了添加共刺激信号(抗CD28)和细胞因子(IL-12)时无反应性CD4 T细胞的反应,这可能有助于恢复细胞功能。我们报告称,通过我们测试的策略,在感染早期增殖和细胞因子产生得以恢复,但在无反应性充分确立的后期则不然。我们还研究了相同处理对胸腺切除、BM5感染小鼠CD4 T细胞无反应性的影响,以确定观察到的挽救是否归因于新来自胸腺的细胞。我们报告称,即使在感染第4周时,胸腺切除小鼠的增殖和细胞因子产生也会减少,表明新来自胸腺的细胞是对处理有反应的细胞。这项研究表明,一旦MAIDS中确立了无反应性,通过CD28和IL-12提供共刺激无法将其逆转。MAIDS中CD4 T细胞的无反应性在根本原因以及细胞恢复到正常状态的能力方面似乎与其他系统中所见不同。

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