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淋巴结基质细胞强烈影响免疫反应抑制。

Lymph node stromal cells strongly influence immune response suppression.

机构信息

Institute of Functional and Applied Anatomy, Hannover Medical School, Hannover, Germany.

出版信息

Eur J Immunol. 2011 Mar;41(3):624-33. doi: 10.1002/eji.201040681. Epub 2011 Jan 18.

Abstract

Many pathogens are initially encountered in the gut, where the decision is made to mount an immune response or induce tolerance. The mesentric lymph node (mLN) has been shown to be involved in immune response and much more in oral tolerance induction. Furthermore, using an in vivo transplantation model, we showed recently that lymph node (LN) stromal cells can affect T-cell function and influence the IgA response by supporting a site-specific environment. To elucidate the importance of LN stromal cells for tolerance induction, mLN or peripheral LN were transplanted into mice (mLNtx or pLNtx) and oral tolerance was induced via ovalbumin. A reduced delayed-type hypersensitivity (DTH) response was detected in pLNtx compared to mLNtx mice. Reduced IL-10 expression, reduced percentages of Tregs, and increased proportions of B cells were identified within the pLNtx. The increase of B cells resulted in a specific immunoglobulin production undetectable in mLNtx. Moreover, transferred IgG(+) cells of tolerized peripheral LN induced a strong reduction of the delayed-type hypersensitivity response, whereas CD4(+) cells were less efficient. Thus, stromal cells have a high impact on creating a unique environment. Furthermore, the environment of pLNtx induces a tolerogenic phenotype by B-cell accumulation and antibody production.

摘要

许多病原体最初在肠道中被遇到,在那里决定是否产生免疫反应或诱导耐受。肠系膜淋巴结(mLN)已被证明参与免疫反应,而在口服耐受诱导中则更为重要。此外,我们最近使用体内移植模型表明,淋巴结(LN)基质细胞可以通过支持特定部位的环境来影响 T 细胞功能并影响 IgA 反应。为了阐明 LN 基质细胞对诱导耐受的重要性,将 mLN 或外周 LN 移植到小鼠中(mLNtx 或 pLNtx),并通过卵清蛋白诱导口服耐受。与 mLNtx 小鼠相比,pLNtx 中的迟发型超敏反应(DTH)反应降低。在 pLNtx 中鉴定到 IL-10 表达降低、Treg 百分比降低和 B 细胞比例增加。B 细胞的增加导致可检测到 mLNtx 中的特异性免疫球蛋白产生。此外,耐受的外周 LN 的转移 IgG(+)细胞诱导 DTH 反应强烈降低,而 CD4(+)细胞的效率较低。因此,基质细胞对创造独特的环境具有重要影响。此外,pLNtx 的环境通过 B 细胞积累和抗体产生诱导耐受表型。

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