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一种选择同种型特异性抗体应答的新机制:肠道T细胞在抗抑制回路调节IgA合成中的作用。

A novel mechanism for the selection of isotype-specific antibody responses: the role of intestinal T cells in the regulation of IgA synthesis by the anti-suppressor circuit.

作者信息

Ernst P B, Maeba J, Lee S I, Paraskevas F

机构信息

Intestinal Disease Research Unit, McMaster University, Hamilton, Ontario, Canada.

出版信息

Immunology. 1988 Sep;65(1):59-66.

PMID:2972602
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1385020/
Abstract

Within 6 hr of immunization the serum of mice contains a unique form of processed antigen, which consists of a complex of immunoglobulin (Ig) and antigen formed in the presence of a factor derived from the anti-suppressor inducer T cell. This complex binds to and activates the anti-suppressor effector T cell, which eventually leads to the inhibition of suppressor cell function. Both of these cells are present in the spleen (SPL) and play a role in the regulation of antibody responses. The purpose of these studies was to identify the anti-suppressor T cells in gut-associated lymphoid tissue and compare their function to their splenic counterparts. Inducer cells were detected in the Peyer's patches (PP), mesenteric lymph nodes but not in the intra-epithelial lymphocytes. The effector cells, which take up the complexes, were detected in PP and lamina propria lymphocytes but not in the intraepithelial or mesenteric lymph node lymphocytes. Furthermore, the uptake of the complexes correlated with the presence of T cells bearing Ia antigens. The PP and SPL anti-suppressor cells were compared for their ability to enhance the production of IgA and IgG. The data clearly showed that the product of the inducer cell, and the effector cell it activates, not only enhanced the antigen-specific responses but also selected for isotype-specific antibody responses. Cells from SPL enhanced IgG greater than IgA, whereas cells from PP selected for IgA. Thus, the presence in PP of cells in the anti-suppressor circuit and their ability to selectively promote IgA synthesis suggest that this regulatory mechanism plays a significant role in intestinal immune responses.

摘要

免疫接种后6小时内,小鼠血清中含有一种独特形式的加工抗原,它由免疫球蛋白(Ig)和抗原的复合物组成,该复合物在源自抗抑制诱导T细胞的因子存在下形成。这种复合物结合并激活抗抑制效应T细胞,最终导致抑制细胞功能受到抑制。这两种细胞都存在于脾脏(SPL)中,并在抗体反应的调节中发挥作用。这些研究的目的是鉴定肠道相关淋巴组织中的抗抑制T细胞,并将它们的功能与其脾脏中的对应细胞进行比较。在派尔集合淋巴结(PP)、肠系膜淋巴结中检测到诱导细胞,但在上皮内淋巴细胞中未检测到。摄取复合物的效应细胞在PP和固有层淋巴细胞中检测到,但在上皮内或肠系膜淋巴结淋巴细胞中未检测到。此外,复合物的摄取与携带Ia抗原的T细胞的存在相关。比较了PP和SPL抗抑制细胞增强IgA和IgG产生的能力。数据清楚地表明,诱导细胞及其激活的效应细胞的产物不仅增强了抗原特异性反应,还选择了同型特异性抗体反应。来自SPL的细胞增强IgG的能力大于IgA,而来自PP的细胞则选择IgA。因此,抗抑制回路中的细胞在PP中的存在及其选择性促进IgA合成的能力表明,这种调节机制在肠道免疫反应中起重要作用。

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A novel mechanism for the selection of isotype-specific antibody responses: the role of intestinal T cells in the regulation of IgA synthesis by the anti-suppressor circuit.一种选择同种型特异性抗体应答的新机制:肠道T细胞在抗抑制回路调节IgA合成中的作用。
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Infect Immun. 1992 Feb;60(2):503-9. doi: 10.1128/iai.60.2.503-509.1992.

本文引用的文献

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Systemic tolerance and secretory immunity after oral immunization.口服免疫后的全身耐受性和分泌性免疫
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Characteristics of natural killer cells in the murine intestinal epithelium and lamina propria.小鼠肠道上皮和固有层中自然杀伤细胞的特征
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Contrasuppression. A novel immunoregulatory activity.反向抑制。一种新型免疫调节活性。
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Isotype-specificity of helper T cell clones: Fc alpha receptors regulate T and B cell collaboration for IgA responses.辅助性T细胞克隆的同种型特异性:Fcα受体调节T细胞与B细胞协作以产生IgA应答。
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