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对旋毛虫的肠道免疫是由肠道中产生的OX8 - OX22 - T辅助细胞所具有的特性。

Intestinal immunity to Trichinella spiralis is a property of OX8- OX22- T-helper cells that are generated in the intestine.

作者信息

Korenaga M, Wang C H, Bell R G, Zhu D, Ahmad A

机构信息

James A. Baker Institute for Animal Health, New York State College of Veterinary Medicine, Cornell University, Ithaca 14853.

出版信息

Immunology. 1989 Apr;66(4):588-94.

Abstract

The phenotype of T-helper cells conferring protection against Trichinella spiralis (Ts) was studied using adoptive transfer procedures and T-helper cell subsets isolated by monoclonal antibodies. With these techniques OX8- OX22+ and OX8- OX22- T-helper cell populations were isolated from thoracic duct lymph (TDL) of infected rats three-five-fold more concentrated than in unfractionated lymph. The OX8- OX22- cell subset alone transferred enhanced rejection of adult worms from the intestine. The origin of protective OX8- OX22- cells was examined in mesenteric lymphadenectomized (MX) rats. After MX, protective cells were found in the cell population draining directly from the intestine on Days 2-3 after infection. Protective cells first appeared in the mesenteric lymph node (MLN) and efferent lymph at Day 3. MX rats rejected T. spiralis at the same time as intact controls and showed enhanced rejection when immune TDL were transfused. No evidence was found for a direct role of the MLN in the generation or expression of parasite rejection. Depletion of migrating OX8- OX22- blast cells by 48-hr drainage of TDL did not influence the expression of an anamnestic response to challenge infection. This suggests that an intestinally resident cell population has a substantial role in mediating primary worm rejection and anamnestic immunity. Day 2 OX8- OX22- cells from MX rats proliferated in response to the presentation of adult and muscle larvae antigens in vitro. We conclude that protection resides in the OX8- OX22- T-helper cell subset that is produced and functions in the intestine.

摘要

采用过继转移程序和通过单克隆抗体分离的辅助性T细胞亚群,研究了赋予抗旋毛虫(Ts)保护作用的辅助性T细胞表型。利用这些技术,从感染大鼠的胸导管淋巴(TDL)中分离出OX8 - OX22⁺和OX8 - OX22⁻辅助性T细胞群体,其浓度比未分级的淋巴中的浓度高3至5倍。仅OX8 - OX22⁻细胞亚群能增强肠道内成虫的排斥反应。在肠系膜淋巴结切除(MX)的大鼠中检查了保护性OX8 - OX22⁻细胞的来源。MX后,在感染后第2 - 3天直接从肠道引流的细胞群体中发现了保护性细胞。保护性细胞在第3天首次出现在肠系膜淋巴结(MLN)和输出淋巴中。MX大鼠与完整对照同时排斥旋毛虫,当输注免疫TDL时排斥反应增强。没有发现MLN在寄生虫排斥反应的产生或表达中起直接作用的证据。通过TDL的48小时引流耗尽迁移的OX8 - OX22⁻母细胞并不影响对攻击感染的回忆反应的表达。这表明肠道驻留细胞群体在介导原发性蠕虫排斥反应和回忆性免疫中起重要作用。来自MX大鼠的第2天OX8 - OX22⁻细胞在体外对成虫和肌肉幼虫抗原的呈递作出增殖反应。我们得出结论,保护作用存在于在肠道中产生并发挥功能的OX8 - OX22⁻辅助性T细胞亚群中。

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