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通过鼻腔免疫抑制免疫反应。

Suppression of the immune response by nasal immunization.

作者信息

Waldo F B, van den Wall Bake A W, Mestecky J, Husby S

机构信息

Department of Pediatrics, University of Alabama at Birmingham.

出版信息

Clin Immunol Immunopathol. 1994 Jul;72(1):30-4. doi: 10.1006/clin.1994.1103.

Abstract

Intranasal immunization results in both a mucosal and a systemic immune response in humans. Intranasal tetanus toxoid immunization in humans causes an increased serum IgA1 antibody response to tetanus toxoid following a subsequent intramuscular immunization. We hypothesized that intranasal priming with a novel protein antigen, keyhole limpet hemocyanin (KLH), would similarly result in an up-regulated systemic IgA response after a subsequent systemic immunization. To test this hypothesis, five healthy adults received a primary series of intranasal KLH immunizations followed 3 months later by a subcutaneous KLH immunizations Eight healthy adults received only a subcutaneous KLH immunization and served as controls. The nasal immunization resulted in a brisk and sustained serum IgM, IgA, and IgG antibody response and a mucosal IgA response. The subcutaneous immunization alone resulted in a serum antibody response and the development of delayed type hypersensitivity by skin testing. When the nasally primed subjects received a subsequent subcutaneous immunization there was a decline in the serum concentration of IgA and IgG antibodies to KLH. In addition, the nasally primed subjects failed to develop delayed type hypersensitivity to KLH following subcutaneous immunization. These data suggest that the nasal mucosa can induce a mucosal and systemic response; however, it may also suppress a subsequent immune response to systemic immunization.

摘要

鼻内免疫在人体中可引发黏膜免疫反应和全身免疫反应。人体鼻内接种破伤风类毒素后,在随后进行肌肉注射免疫时,会使血清中针对破伤风类毒素的IgA1抗体反应增强。我们推测,用新型蛋白质抗原钥孔戚血蓝蛋白(KLH)进行鼻内初免,在随后进行全身免疫后,同样会导致全身IgA反应上调。为验证这一假设,5名健康成年人接受了一系列鼻内KLH免疫初免,3个月后再进行皮下KLH免疫;8名健康成年人仅接受皮下KLH免疫作为对照。鼻内免疫引发了快速且持续的血清IgM、IgA和IgG抗体反应以及黏膜IgA反应。单独的皮下免疫引发了血清抗体反应,并通过皮肤试验出现了迟发型超敏反应。当经鼻初免的受试者随后接受皮下免疫时,针对KLH的IgA和IgG抗体血清浓度下降。此外,经鼻初免的受试者在皮下免疫后未出现针对KLH的迟发型超敏反应。这些数据表明,鼻黏膜可诱导黏膜和全身反应;然而,它也可能抑制随后对全身免疫的免疫反应。

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