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B细胞是外周淋巴结中起始抗原呈递细胞。

The B cell is the initiating antigen-presenting cell in peripheral lymph nodes.

作者信息

Janeway C A, Ron J, Katz M E

出版信息

J Immunol. 1987 Feb 15;138(4):1051-5.

PMID:3100626
Abstract

We have examined the role of B cells in antigen presentation in lymph nodes in several ways. We found that mice depleted of B lymphocytes via chronic injection of anti-mu-chain antibody do not mount peripheral lymph node T cell proliferative responses to normally immunogenic doses of antigen. Depletion of B cells by passage of immune lymph node cells over anti-immunoglobulin columns early after immunization depletes antigen-presenting function from draining lymph nodes, and this function can be restored by using B cells or splenic adherent cells to allow the remaining T cells to proliferate. Lymph node B cells present antigen very effectively to lines of antigen-specific T cells. However, unfractionated lymph node cells from anti-mu-treated mice present very poorly, if at all, whereas unfractionated spleen cells from the same mice do present antigen. This is in keeping with our previous finding that helper T cell function in the spleen is normal in B cell-deprived mice. Finally, when mice homozygous for the lymphoproliferative gene lpr are treated chronically with anti-mu-chain antibody, lymphadenopathy is greatly retarded, suggesting a role for B cells in the massive proliferation of T cells in this syndrome. From this analysis, it would appear that the initiating antigen-presenting cell in the lymph node is a B lymphocyte, and that B lymphocytes in lymph nodes may be distinct from those in the spleen. It is of interest that these results also suggest that the lymph node lacks an antigen-presenting cell that is found in the spleen, perhaps the dendritic cell.

摘要

我们通过多种方式研究了B细胞在淋巴结抗原呈递中的作用。我们发现,通过长期注射抗μ链抗体使B淋巴细胞耗竭的小鼠,对正常免疫原剂量的抗原不会产生外周淋巴结T细胞增殖反应。免疫后早期,将免疫淋巴结细胞通过抗免疫球蛋白柱,可使B细胞耗竭,从而使引流淋巴结的抗原呈递功能丧失,而使用B细胞或脾黏附细胞可恢复该功能,使剩余的T细胞增殖。淋巴结B细胞能非常有效地将抗原呈递给抗原特异性T细胞系。然而,来自抗μ处理小鼠的未分级淋巴结细胞即使能呈递抗原,效率也非常低,而来自相同小鼠的未分级脾细胞则能呈递抗原。这与我们之前的发现一致,即在B细胞缺失的小鼠中,脾脏中的辅助性T细胞功能正常。最后,当长期用抗μ链抗体处理淋巴增殖基因lpr纯合的小鼠时,淋巴结病的发展会大大延迟,这表明B细胞在该综合征中T细胞的大量增殖中起作用。从这个分析来看,淋巴结中起始的抗原呈递细胞似乎是B淋巴细胞,而且淋巴结中的B淋巴细胞可能与脾脏中的不同。有趣的是,这些结果还表明淋巴结缺乏一种在脾脏中发现的抗原呈递细胞,可能是树突状细胞。

相似文献

1
The B cell is the initiating antigen-presenting cell in peripheral lymph nodes.B细胞是外周淋巴结中起始抗原呈递细胞。
J Immunol. 1987 Feb 15;138(4):1051-5.
2
T cell priming in vivo: a major role for B cells in presenting antigen to T cells in lymph nodes.体内T细胞致敏:B细胞在淋巴结中将抗原呈递给T细胞的主要作用。
J Immunol. 1987 May 1;138(9):2848-56.
3
Differential responses of B cells from the spleen and lymph node to TNP-Ficoll.脾脏和淋巴结来源的B细胞对三硝基苯-聚蔗糖的不同反应。
J Immunol. 1988 May 1;140(9):2925-30.
4
Role of B cells in the stimulation of syngeneic mixed lymphocyte responses.B细胞在同基因混合淋巴细胞反应刺激中的作用。
Behring Inst Mitt. 1983 May(72):107-16.
5
Comparison of antigen presentation by lymph node cells from protein and peptide-primed mice.蛋白质致敏小鼠和肽致敏小鼠的淋巴结细胞抗原呈递比较。
Immunology. 1993 Jan;78(1):58-64.
6
Enhancement of antigenic potency in vitro and immunogenicity in vivo by coupling the antigen to anti-immunoglobulin.通过将抗原与抗免疫球蛋白偶联来增强体外抗原效力和体内免疫原性。
J Immunol. 1986 Jan;136(1):58-65.
7
Antibody conjugates mimic specific B cell presentation of antigen: relationship between T and B cell specificity.抗体偶联物模拟抗原的特异性B细胞呈递:T细胞与B细胞特异性之间的关系。
J Immunol. 1987 Jun 15;138(12):4133-42.
8
Unresponsiveness of MRL/MP-lpr/lpr mice to antigen given subcutaneously in adjuvant: partial restoration of response after local injection of B cells.MRL/MP-lpr/lpr小鼠对皮下注射于佐剂中的抗原无反应:局部注射B细胞后反应部分恢复。
J Immunol. 1987 Jul 15;139(2):400-5.
9
Defective induction of antigen-reactive proliferating T cells in B cell-deprived mice. II. Anti-mu treatment affects the initiation and recruitment of T cells.B细胞缺失小鼠中抗原反应性增殖T细胞的诱导缺陷。II. 抗μ治疗影响T细胞的起始和募集。
Eur J Immunol. 1983 Feb;13(2):167-71. doi: 10.1002/eji.1830130214.
10
T cell development in B cell deficient mice. III. Restriction specificity of suppressor T cell factor(s) produced in mice treated chronically with rabbit anti-mouse mu chain antibody.B细胞缺陷小鼠中的T细胞发育。III. 用兔抗小鼠μ链抗体长期处理的小鼠所产生的抑制性T细胞因子的限制特异性。
J Mol Cell Immunol. 1985;2(2):107-17.

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