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线虫分泌物介导的细胞增殖的深度抑制

Profound suppression of cellular proliferation mediated by the secretions of nematodes.

作者信息

Allen J E, MacDonald A S

机构信息

Institute of Cell, Animal and Population Biology, University of Edinburgh, UK.

出版信息

Parasite Immunol. 1998 May;20(5):241-7. doi: 10.1046/j.1365-3024.1998.00151.x.

DOI:10.1046/j.1365-3024.1998.00151.x
PMID:9651925
Abstract

Loss of T lymphocyte proliferation and the emergence of a host response that is dominated by a Th2-type profile are well-established features of human filarial infection. Down-regulation and modulation of host T cell responses during lymphatic filariasis has been investigated by implantation of parasite stages into inbred mice. Adherent peritoneal exudate cells (PEC) from mice transplanted with adult or larval Brugia malayi parasites are profoundly anti-proliferative but do not prevent antigen-specific cytokine production by T cells. We demonstrate here that the excretory/secretory (E/S) products of the adult parasite are sufficient to induce PEC that block proliferation if injected daily into mice. We have previously shown that in vivo production of host IL-4 is required for the generation of suppressive cells. Because the induction of host IL-4 is characteristic of infection with nematodes, we asked whether E/S from two other nematode parasites, Nippostrongylus braziliensis and Toxocara canis were also capable of generating a suppressor cell population. Injection of E/S from these two parasites also led to a reduction in T cell proliferation suggesting that this mechanism of down-regulating host responses is a feature common to nematode parasites.

摘要

T淋巴细胞增殖丧失以及以Th2型为主导的宿主反应的出现是人类丝虫感染的既定特征。通过将寄生虫阶段植入近交小鼠来研究淋巴丝虫病期间宿主T细胞反应的下调和调节。移植了成年或幼虫马来布鲁线虫寄生虫的小鼠的贴壁腹膜渗出细胞(PEC)具有很强的抗增殖能力,但并不阻止T细胞产生抗原特异性细胞因子。我们在此证明,如果每天给小鼠注射成年寄生虫的排泄/分泌(E/S)产物,足以诱导出能阻断增殖的PEC。我们之前已经表明,宿主IL-4的体内产生是产生抑制性细胞所必需的。由于宿主IL-4的诱导是线虫感染的特征,我们询问来自另外两种线虫寄生虫——巴西日圆线虫和犬弓首蛔虫的E/S是否也能够产生抑制性细胞群体。注射来自这两种寄生虫的E/S也导致T细胞增殖减少,这表明这种下调宿主反应的机制是线虫寄生虫共有的特征。

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