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新生小鼠巨噬细胞Ia表达的调控——脾抑制细胞的作用

Control of macrophage Ia expression in neonatal mice--role of a splenic suppressor cell.

作者信息

Snyder D S, Lu C Y, Unanue E R

出版信息

J Immunol. 1982 Mar;128(3):1458-65.

PMID:6460061
Abstract

The control of macrophage expression of I region-associated antigens (Ia) in neonatal mice was studied by comparing responses of neonatal and adult mice to immune vs nonimmune stimuli. Adults generated peritoneal exudates rich in Ia-bearing macrophages in response to i.p. injection of live Listeria monocytogenes, Listeria-immune T cells, and heat-killed Listeria, or a soluble mediator termed macrophage Ia-recruiting factor (MIRF). Neonates failed to respond to these stimuli. In contrast, both neonates and adults generated Ia-negative peritoneal exudates when stimulated with thioglycollate. A neonatal spleen cell that blocked the response of adults both to immune T cells and heat-killed Listeria and to MIRF was identified and characterized. Some of the suppressor cells appeared to be early precursors of the phagocytic lineage that develop into mature monocyte-macrophages. Suppression was apparently mediated by metabolites of arachidonic acid since indomethacin and aspirin in vivo blocked the effect. Similar suppressor activity was found in adult bone marrow and in adult resident peritoneal exudate cells. Thus, the phagocytic line autoregulates its surface expression of Ia in both neonatal and adult mice. This mechanism becomes particularly pointed during early development and could contribute to the lack of immunity during ontogeny.

摘要

通过比较新生小鼠和成年小鼠对免疫刺激与非免疫刺激的反应,研究了新生小鼠巨噬细胞I区相关抗原(Ia)表达的调控。成年小鼠腹腔注射活的单核细胞增生李斯特菌、李斯特菌免疫T细胞、热灭活的李斯特菌或一种称为巨噬细胞Ia招募因子(MIRF)的可溶性介质后,会产生富含Ia阳性巨噬细胞的腹腔渗出液。新生小鼠对这些刺激无反应。相反,用巯基乙酸刺激时,新生小鼠和成年小鼠都会产生Ia阴性腹腔渗出液。鉴定并表征了一种能阻断成年小鼠对免疫T细胞、热灭活李斯特菌和MIRF反应的新生脾细胞。一些抑制细胞似乎是吞噬细胞系的早期前体,可发育为成熟的单核细胞-巨噬细胞。抑制作用显然是由花生四烯酸的代谢产物介导的,因为体内的吲哚美辛和阿司匹林可阻断这种作用。在成年骨髓和成年常驻腹腔渗出细胞中也发现了类似的抑制活性。因此,吞噬细胞系在新生小鼠和成年小鼠中均能自动调节其Ia的表面表达。这种机制在早期发育过程中尤为突出,可能导致个体发育过程中免疫力的缺乏。

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