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肠道T淋巴细胞在支气管黏膜免疫中的作用。

A role for intestinal T lymphocytes in bronchus mucosal immunity.

作者信息

Wallace F J, Cripps A W, Clancy R L, Husband A J, Witt C S

机构信息

Auspharm Institute of Mucosal Immunology, Jesmond, Australia.

出版信息

Immunology. 1991 Sep;74(1):68-73.

Abstract

Rats immunized by intra-Peyer's patch (IPP) injection with non-typable Haemophilus influenzae (NTHI) have been shown to clear this organism from the respiratory tract faster than non-immunized rats. We therefore performed a series of experiments in order to determine the mechanism of action of the enhanced pulmonary clearance. The experiments show that homing of intestinal T cells to the respiratory tract is an important component in the observed immunity, while specific antibody adsorbed to bacteria does not influence pulmonary bacterial clearance rate. Mucosally derived lymphocytes were collected from the thoracic duct of rats primed by IPP inoculation with NTHI, and intravenously transfused to recipient rats. These rats were shown to clear bacteria from bronchial spaces faster than non-transfused rats, or rats transfused with non-immune lymphocytes. Lymphocytes collected from the spleens of immunized rats were also capable of conferring the ability to accelerate pulmonary clearance. When thoracic duct lymphocytes (TDL) purified for T lymphocytes were transferred to recipients, the NTHI clearance rate was accelerated. In experiments to evaluate the activity of specific antibody, it was demonstrated that NTHI opsonized with antibody from bronchial washings of immunized rats was not cleared from the respiratory tract of naive rats faster than non-opsonized controls. These data indicate that immune clearance of NTHI from the respiratory tract following gut immunization is dependent upon antigen-primed lymphocytes, that primed T cells are capable of conferring this protection, and that a primary role for specific antibody in the process cannot be established.

摘要

通过派伊尔结内注射(IPP)用不可分型流感嗜血杆菌(NTHI)免疫的大鼠已被证明比未免疫的大鼠能更快地从呼吸道清除这种微生物。因此,我们进行了一系列实验,以确定增强的肺部清除作用机制。实验表明,肠道T细胞归巢至呼吸道是观察到的免疫中的一个重要组成部分,而吸附在细菌上的特异性抗体并不影响肺部细菌清除率。从经IPP接种NTHI致敏的大鼠胸导管收集黏膜来源的淋巴细胞,并静脉输注给受体大鼠。这些大鼠被证明比未输注的大鼠或输注非免疫淋巴细胞的大鼠能更快地从支气管腔清除细菌。从免疫大鼠脾脏收集的淋巴细胞也能够赋予加速肺部清除的能力。当纯化的T淋巴细胞胸导管淋巴细胞(TDL)转移给受体时,NTHI清除率加快。在评估特异性抗体活性的实验中,结果表明,用免疫大鼠支气管灌洗抗体调理的NTHI从新生大鼠呼吸道清除的速度并不比未调理的对照更快。这些数据表明,肠道免疫后呼吸道对NTHI的免疫清除依赖于抗原致敏的淋巴细胞,致敏的T细胞能够提供这种保护,并且在此过程中特异性抗体的主要作用无法确定。

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