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抗原呈递B细胞在体内T细胞致敏中的作用。B细胞缺陷小鼠的研究。

The role of antigen-presenting B cells in T cell priming in vivo. Studies of B cell-deficient mice.

作者信息

Kurt-Jones E A, Liano D, HayGlass K A, Benacerraf B, Sy M S, Abbas A K

机构信息

Department of Pathology, Brigham and Women's Hospital, Boston, MA 02115.

出版信息

J Immunol. 1988 Jun 1;140(11):3773-8.

PMID:2453554
Abstract

Mice rendered B cell deficient by treatment with rabbit anti-mouse IgM (anti-mu) antibodies from birth fail to respond when primed with soluble protein antigens in CFA, as measured by T cell proliferation when challenged with antigen in vitro. The role of B cells in T cell priming in vivo was examined by adoptively transferring hapten-specific B cells into anti-mu mice, followed by immunization with haptenated Ag in CFA. The T cell proliferative response to OVA of anti-mu BALB/c mice was partially restored by the administration of TNP or FITC-specific B cells and immunization with TNP-OVA or FITC-OVA, respectively. This reconstitution was Ag-specific, inasmuch as hapten-binding B cells restored the T cell responses to OVA in mice immunized with the same hapten coupled to OVA. The mechanism of B cell reconstitution of T cell priming in anti-mu mice was addressed using parental to F1 B cell transfers. The Ia restriction pattern of the activated T cells from these mice indicated that both direct presentation of Ag by transferred B cells and antibody-mediated enhancement of Ag presentation by non-B, host Ag-presenting cells occurred. Thus, Ag-specific B lymphocytes play a critical role in priming of T cells in vivo.

摘要

从出生起就用兔抗小鼠IgM(抗μ)抗体处理而导致B细胞缺陷的小鼠,当在弗氏完全佐剂(CFA)中用可溶性蛋白抗原进行初次免疫时,体外再次用抗原刺激后通过T细胞增殖检测发现其无反应。通过将半抗原特异性B细胞过继转移到抗μ小鼠体内,然后用CFA中的半抗原化抗原进行免疫,研究了B细胞在体内T细胞初次免疫中的作用。分别给予TNP或FITC特异性B细胞并分别用TNP-OVA或FITC-OVA免疫后,抗μ BALB/c小鼠对OVA的T细胞增殖反应部分恢复。这种重建是抗原特异性的,因为半抗原结合B细胞恢复了用与OVA偶联的相同半抗原免疫的小鼠中T细胞对OVA的反应。使用亲代到F1 B细胞转移研究了抗μ小鼠中B细胞重建T细胞初次免疫的机制。这些小鼠中活化T细胞的Ia限制模式表明,既发生了转移的B细胞直接呈递抗原,也发生了抗体介导的非B宿主抗原呈递细胞增强抗原呈递。因此,抗原特异性B淋巴细胞在体内T细胞的初次免疫中起关键作用。

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