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小鼠肺和肺门淋巴结对非胸腺依赖性抗原的初次抗体反应。

Primary antibody responses to thymus-independent antigens in the lungs and hilar lymph nodes of mice.

作者信息

Goud S N, Kaplan A M, Subbarao B

机构信息

Sanders-Brown Center on Aging, University of Kentucky, Lexington 40536-0230.

出版信息

Infect Immun. 1990 Jul;58(7):2035-41. doi: 10.1128/iai.58.7.2035-2041.1990.

Abstract

B lymphocytes from the pulmonary lymphoid tissues were stimulated with a variety of thymus-independent (TI) antigens by intratracheal (i.t.) immunization. Immune responses in the lungs and hilar lymph nodes (HLN), which are part of the localized lymphoid tissue, as well as in the spleen, the systemic lymphoid organ, were studied. Thus, primary i.t. immunization of mice with the TI-1 antigen trinitrophenyl-lipopolysaccharide (TNP-LPS) elicited both antigen-specific and polyclonal plaque-forming cell responses from HLN, lung, and splenic B lymphocytes. These responses appeared as early as 3 days after immunization and declined by day 7. Similar immunization with another TI-1 antigen, TNP-Brucella abortus, resulted in anti-TNP responses in both pulmonary and systemic lymphoid tissues, although the kinetics of the antibody response were different than those to TNP-LPS. Interestingly an i.t. immunization with a TI-2 antigen, TNP-Ficoll, failed to induce an anti-TNP PFC response from HLN and lung B cells, although there was good antibody formation from splenic B cells. Antibody response to TNP-Ficoll was restored in pulmonary tissues when mice were immunized with TNP-Ficoll mixed with unconjugated B. abortus. In conclusion, our results indicate that TI-1 and TI-2 antigens differ in their ability to induce antibody responses in the pulmonary lymphoid tissues. The inability of TNP-Ficoll to elicit an antibody response in pulmonary lymphoid tissues has significance in the development of vaccines containing bacterial polysaccharides.

摘要

通过气管内(i.t.)免疫,用多种非胸腺依赖性(TI)抗原刺激来自肺淋巴组织的B淋巴细胞。研究了作为局部淋巴组织一部分的肺和肺门淋巴结(HLN)以及作为全身淋巴器官的脾脏中的免疫反应。因此,用TI-1抗原三硝基苯基脂多糖(TNP-LPS)对小鼠进行初次气管内免疫,可引发HLN、肺和脾脏B淋巴细胞的抗原特异性和多克隆空斑形成细胞反应。这些反应在免疫后3天最早出现,并在第7天下降。用另一种TI-1抗原TNP-流产布鲁氏菌进行类似免疫,在肺和全身淋巴组织中均产生了抗TNP反应,尽管抗体反应的动力学与对TNP-LPS的反应不同。有趣的是,用TI-2抗原TNP-菲可进行气管内免疫,未能诱导HLN和肺B细胞产生抗TNP PFC反应,尽管脾脏B细胞有良好的抗体形成。当用与未结合的流产布鲁氏菌混合的TNP-菲可免疫小鼠时,肺组织中对TNP-菲可的抗体反应得以恢复。总之,我们的结果表明,TI-1和TI-2抗原在诱导肺淋巴组织中抗体反应的能力上存在差异。TNP-菲可在肺淋巴组织中无法引发抗体反应,这对含细菌多糖疫苗的开发具有重要意义。

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