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在内毒素和脂多糖存在的情况下,内毒素和脂多糖会刺激人T细胞在自体单核细胞存在的情况下增殖。

Endotoxin and lipid A stimulate proliferation of human T cells in the presence of autologous monocytes.

作者信息

Mattern T, Thanhäuser A, Reiling N, Toellner K M, Duchrow M, Kusumoto S, Rietschel E T, Ernst M, Brade H, Flad H D

机构信息

Borstel Research Institute, Germany.

出版信息

J Immunol. 1994 Oct 1;153(7):2996-3004.

PMID:7916368
Abstract

In this paper we describe a new activity of LPS and partial structures: the induction of DNA synthesis and lymphokine production of human T lymphocytes. The LPS-induced T cell proliferation is dose dependent and requires 100 to 10,000 ng/ml of LPS or synthetic lipid A (compound 506) for optimal stimulation. In contrast, the synthetic lipid A precursor Ia (compound 406) is not active but rather antagonizes LPS-induced proliferation. The proliferation is accompanied by the expression of mRNA for the Th1 cell-derived lymphokines IFN-gamma and IL-2, but not for the Th2 lymphokines IL-4, IL-5, or IL-10. Highly enriched T lymphocyte preparations with less than 0.1% monocytes are not stimulated by LPS, showing that monocytes are required for T cell proliferation. Reconstitution experiments show that only monocytes, but not B lymphocytes, are able to support induction of DNA synthesis. Separating LPS-stimulated monocytes from T lymphocytes by a membrane, permeable for cytokines but not for cells, abolishes T cell proliferation. Fixation of monocytes with paraformaldehyde also abrogates their accessory function for T cells. If the monocytes are preincubated for 2 h at 37 degrees C with LPS and then washed, they still are able to induce T cell proliferation in the absence of additional LPS. Our results indicate that human T cells respond in a monocyte-supported manner to LPS exposure by proliferation and lymphokine production. We hypothesize that this reactivity of T lymphocytes to LPS may be of clinical relevance.

摘要

在本文中,我们描述了脂多糖(LPS)的一种新活性及其部分结构:诱导人T淋巴细胞的DNA合成和淋巴因子产生。LPS诱导的T细胞增殖呈剂量依赖性,最佳刺激需要100至10,000 ng/ml的LPS或合成类脂A(化合物506)。相比之下,合成类脂A前体Ia(化合物406)无活性,反而拮抗LPS诱导的增殖。增殖伴随着Th1细胞衍生的淋巴因子IFN-γ和IL-2的mRNA表达,但不伴有Th2淋巴因子IL-4、IL-5或IL-10的mRNA表达。单核细胞含量低于0.1%的高度富集T淋巴细胞制剂不受LPS刺激,表明T细胞增殖需要单核细胞。重组实验表明,只有单核细胞而非B淋巴细胞能够支持DNA合成的诱导。用对细胞因子可通透但对细胞不可通透的膜将LPS刺激的单核细胞与T淋巴细胞分离,可消除T细胞增殖。用多聚甲醛固定单核细胞也会消除其对T细胞的辅助功能。如果单核细胞在37℃下与LPS预孵育2小时,然后洗涤,它们在没有额外LPS的情况下仍能诱导T细胞增殖。我们的结果表明,人T细胞通过增殖和淋巴因子产生以单核细胞支持的方式对LPS暴露作出反应。我们推测T淋巴细胞对LPS的这种反应性可能具有临床相关性。

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