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通过向新生小鼠注射非胸腺依赖性(2型)抗原来诱导B细胞致敏。

Induction of B cell priming by neonatal injection of mice with thymic-independent (type 2) antigens.

作者信息

Mosier D E

出版信息

J Immunol. 1978 Oct;121(4):1453-9.

PMID:359707
Abstract

Mice injected at birth with the thymus-independent type 2 antigen TNP-AECM-Ficoll have augmented anti-TNP antibody responses when their spleen cells subsequently are challenged in vitro with TNP-coupled thymic independent or thymic dependent antigens. This neonatal priming effect was shown to occur in neonatal nu/nu mice and thus does not appear to require T lymphocytes. The primary explanation for the priming effect seems to be an increase of approximately 10-fold in the numbers of TNP-specific precursors of antibody-forming cells. The neonatal injection of TNP-AECM-Ficoll induces little or no antibody formation directly. It appears, therefore, that some thymic independent antigens can deliver a signal to immature B cells, which causes clonal expansion, but is unable to induce differentiation into antibody-forming cells.

摘要

出生时注射非胸腺依赖性2型抗原TNP-AECM-菲可的小鼠,当随后用TNP偶联的非胸腺依赖性或胸腺依赖性抗原在体外刺激其脾细胞时,抗TNP抗体反应增强。这种新生期致敏效应在新生期裸鼠中也会出现,因此似乎不需要T淋巴细胞。致敏效应的主要解释似乎是抗体形成细胞的TNP特异性前体细胞数量增加了约10倍。新生期注射TNP-AECM-菲可直接诱导的抗体形成很少或没有。因此,似乎一些非胸腺依赖性抗原可以向未成熟B细胞传递信号,导致克隆扩增,但无法诱导其分化为抗体形成细胞。

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