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脂多糖激活的树突状细胞分泌白细胞介素-10或白细胞介素-12,这严重依赖于相对于纯化树突状细胞培养开始的刺激时间。

Secretion of interleukin-10 or interleukin-12 by LPS-activated dendritic cells is critically dependent on time of stimulus relative to initiation of purified DC culture.

作者信息

Jiang Hui-Rong, Muckersie Elizabeth, Robertson Marie, Xu Heping, Liversidge Janet, Forrester John V

机构信息

Department of Ophthalmology, University of Aberdeen Medical School Foresterhill, Scotland, United Kingdom.

出版信息

J Leukoc Biol. 2002 Nov;72(5):978-85.

Abstract

Dendritic cells (DC) are key regulators of adaptive immunity with the potential to induce T cell activation/immunity or T cell suppression/tolerance. DC are themselves induced by "maturation" signals such as bacterial lipopolysaccharide (LPS). We demonstrate here that LPS can stimulate DC to display similar maturation phenotypes but to differentiate toward an interleukin (IL)-10(high)- or IL-12(high)-secretor profile depending on the timing of maturation signal induction. Immediate/early administration of LPS induced purified bone marrow-derived DC (BMDC) to differentiate as IL-10(high)IL-12(low)-secreting cells, termed early DC (eDC). Conversely, delayed administration of LPS altered the DC cytokine profile to IL-10(low)IL-12(high), termed later DC (lDC). The presence of IL-4 enhanced the yield and maturation of BMDC but inhibited LPS-induced IL-10 production by eDC. In contrast, interferon-gamma reduced the yield of DC but promoted the level of LPS-induced IL-10 production by lDC. Our data provide new evidence that ex vivo manipulation and the cytokine environment regulate DC maturation status and cytokine-secretor phenotype with implications for the control of T cell differentiation and function via DC-based immunotherapeutic strategies.

摘要

树突状细胞(DC)是适应性免疫的关键调节因子,具有诱导T细胞激活/免疫或T细胞抑制/耐受的潜力。DC自身由诸如细菌脂多糖(LPS)等“成熟”信号诱导产生。我们在此证明,LPS可刺激DC呈现相似的成熟表型,但根据成熟信号诱导的时间,可分化为白细胞介素(IL)-10高分泌型或IL-12高分泌型。立即/早期给予LPS可诱导纯化的骨髓来源DC(BMDC)分化为IL-10高分泌、IL-12低分泌细胞,称为早期DC(eDC)。相反,延迟给予LPS会使DC细胞因子谱变为IL-10低分泌、IL-12高分泌,称为晚期DC(lDC)。IL-4的存在可提高BMDC的产量和成熟度,但会抑制eDC中LPS诱导的IL-10产生。相比之下,干扰素-γ会降低DC的产量,但会促进lDC中LPS诱导的IL-10产生水平。我们的数据提供了新的证据,即体外操作和细胞因子环境可调节DC的成熟状态和细胞因子分泌表型,这对通过基于DC的免疫治疗策略控制T细胞分化和功能具有重要意义。

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