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迟发型超敏反应中的淋巴细胞募集。干扰素-γ的作用。

Lymphocyte recruitment in delayed-type hypersensitivity. The role of IFN-gamma.

作者信息

Issekutz T B, Stoltz J M, vd Meide P

机构信息

Department of Pediatrics, Dalhousie University, Halifax, Nova Scotia, Canada.

出版信息

J Immunol. 1988 May 1;140(9):2989-93.

PMID:3129506
Abstract

Lymphocytes are recruited out of the blood into delayed-type hypersensitivity (DTH) reactions, but the factors controlling their migration are poorly understood. Our previous studies have shown that IFN-alpha/beta, its inducers, and T cell lymphokines can induce lymphocyte migration into the skin after intradermal injection. The present studies were designed to determine the effect of rIFN-gamma, IL-1, and anti-IFN-gamma on lymphocyte recruitment into DTH. Small peritoneal exudate lymphocytes, which preferentially migrate to inflammatory sites, were labelled with 111In and injected i.v. into rats. The intradermal injection of IFN-gamma stimulated the migration of these lymphocytes into the skin. IL-1 induced very little migration by itself, but enhanced the effect of IFN-gamma. Kinetic analysis demonstrated that the migration of lymphocytes to IFN-gamma was rapid, with a peak at 6 h, whereas migration into a DTH reaction was minimal for the first 8 h and reached a peak 24 h after intradermal injection. Polyclonal rabbit anti-IFN-gamma anti-serum, and a Mab to IFN-gamma, DB-2, could almost completely block lymphocyte migration induced by IFN-gamma. Furthermore, DB-2 inhibited lymphocyte recruitment into DTH reactions by 50 to 90%. This Mab did not affect migration in response to IFN-alpha/beta, although it partially inhibited the response to polyI:C. The effect of IFN-gamma on lymphocyte recruitment was not specific for small peritoneal exudate lymphocytes, because both spleen T cells and lymph node cells migrated in response to IFN-gamma and DB-2 inhibited the recruitment of splenic T cells to DTH. Thus, IFN-gamma is a potent stimulator of lymphocyte migration into the skin and a major mediator of lymphocyte recruitment into DTH.

摘要

淋巴细胞从血液中被募集到迟发型超敏反应(DTH)部位,但控制其迁移的因素仍知之甚少。我们之前的研究表明,干扰素α/β、其诱导剂以及T细胞淋巴因子在皮内注射后可诱导淋巴细胞迁移至皮肤。本研究旨在确定重组干扰素γ、白细胞介素-1和抗干扰素γ对淋巴细胞募集到DTH反应中的影响。将优先迁移至炎症部位的小腹腔渗出淋巴细胞用铟-111标记后静脉注射到大鼠体内。皮内注射干扰素γ可刺激这些淋巴细胞迁移至皮肤。白细胞介素-1本身诱导的迁移很少,但可增强干扰素γ的作用。动力学分析表明,淋巴细胞对干扰素γ的迁移迅速,在6小时达到峰值,而在皮内注射后的前8小时,迁移至DTH反应部位的情况极少,在24小时达到峰值。多克隆兔抗干扰素γ抗血清以及抗干扰素γ单克隆抗体DB-2几乎可完全阻断干扰素γ诱导的淋巴细胞迁移。此外,DB-2可将淋巴细胞募集到DTH反应中的情况抑制50%至90%。该单克隆抗体不影响对干扰素α/β的迁移反应,尽管它可部分抑制对聚肌胞苷酸的反应。干扰素γ对淋巴细胞募集的作用并非小腹腔渗出淋巴细胞所特有,因为脾T细胞和淋巴结细胞均可对干扰素γ产生迁移反应,且DB-2可抑制脾T细胞募集到DTH反应中。因此,干扰素γ是淋巴细胞迁移至皮肤的有效刺激因子,也是淋巴细胞募集到DTH反应中的主要介质。

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