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血清分子对IgE抗体产生的调节。III. 同种异体淋巴细胞相互作用诱导抑制活性及同种异体效应抑制IgE合成

Regulation of IgE antibody production by serum molecules. III. Induction of suppressive activity by allogeneic lymphoid cell interactions and suppression of IgE synthesis by the allogeneic effect.

作者信息

Katz D H

出版信息

J Exp Med. 1979 Feb 1;149(2):539-44. doi: 10.1084/jem.149.2.539.

DOI:10.1084/jem.149.2.539
PMID:762501
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2184816/
Abstract

Antibody responses of the IgE class are, like other immunoglobulin classes, regulated by a finely-tuned network of complex cellular and molecular interactions (1). Previous studies conducted in our laboratory (2, 3) have provided new insights into the differences in control mechanisms that result in individuals manifesting either the high (allergic) or low (nonallergic) IgE responder phenotype. These experiments have shown that certain manipulations (i.e. low dose X-irradiation) convert normally low responder mice to high IgE responders, apparently by diminishing a suppressor T-cell mechanism which normally dampens, rather selectively, IgE antibody production in such individuals. Similar findings have been made by Watanabe et al. (4). Recently, we have been studying the types of manipulations that could reverse the high IgE responsive state back to a low one. These studies (2, 3, 5, 6) have demonstrated that the high IgE responses induced in low responder mice can be substantially diminished, and even abolished, by passively transfusing serum or ascetic fluid from donor mice previously inoculated with mycobacterial-containing complete Freund's adjuvant (CFA). Because the suppressive activity of CFA-immune serum or ascitic fluid is so highly selective for IgE antibody production, we have recently termed these serum substances suppressive factors of allergy (SFA) (2, 3). The present study was undertaken to determine whether alternative means, particularly those that avoid administration of CFA, could be devised for the induction of SFA. Herein, we report the effectiveness of allogeneic lymphoid cell interactions in inducing SFA, both in vivo and in vitro, as well as the potent suppressive effects of an in vivo allogeneic effect on irradiation enhanced IgE antibody production in low responder mice.

摘要

IgE类抗体反应与其他免疫球蛋白类一样,受复杂细胞和分子相互作用的精细调节网络调控(1)。我们实验室之前进行的研究(2,3)为导致个体表现出高(过敏)或低(非过敏)IgE应答者表型的控制机制差异提供了新见解。这些实验表明,某些操作(即低剂量X射线照射)可使正常的低应答小鼠转变为高IgE应答者,显然是通过减少一种抑制性T细胞机制,该机制通常会选择性地抑制此类个体的IgE抗体产生。渡边等人(4)也有类似发现。最近,我们一直在研究能够将高IgE反应状态逆转回低反应状态的操作类型。这些研究(2,3,5,6)表明,通过被动输注先前接种含分枝杆菌的完全弗氏佐剂(CFA)的供体小鼠的血清或腹水,低应答小鼠中诱导的高IgE反应可大幅减弱甚至消除。由于CFA免疫血清或腹水的抑制活性对IgE抗体产生具有高度选择性,我们最近将这些血清物质称为过敏抑制因子(SFA)(2,3)。本研究旨在确定是否可以设计出替代方法,特别是那些避免使用CFA的方法来诱导SFA。在此,我们报告同种异体淋巴细胞相互作用在体内和体外诱导SFA的有效性,以及体内同种异体效应对低应答小鼠照射增强的IgE抗体产生的强大抑制作用。

相似文献

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Regulation of IgE antibody production by serum molecules. III. Induction of suppressive activity by allogeneic lymphoid cell interactions and suppression of IgE synthesis by the allogeneic effect.血清分子对IgE抗体产生的调节。III. 同种异体淋巴细胞相互作用诱导抑制活性及同种异体效应抑制IgE合成
J Exp Med. 1979 Feb 1;149(2):539-44. doi: 10.1084/jem.149.2.539.
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FcR epsilon+ lymphocytes and regulation of the IgE antibody system. III. Suppressive factor of allergy (SFA) is produced during the in vitro FcR epsilon expression cascade and displays corollary physiologic activity in vivo.FcRε⁺淋巴细胞与IgE抗体系统的调节。III. 过敏抑制因子(SFA)在体外FcRε表达级联反应过程中产生,并在体内表现出相应的生理活性。
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Regulation of IgE antibody production by serum molecules. VI: Preliminary biochemical and immunological characterization of serum molecules active in suppressing IgE antibody production.血清分子对IgE抗体产生的调节。VI:抑制IgE抗体产生的活性血清分子的初步生化及免疫学特性分析
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Regulation of IgE antibody production by serum molecules. I. Serum from complete Freund's adjuvant-immune donors suppresses irradiation-enhanced IgE production in low responder mouse strains.血清分子对IgE抗体产生的调节。I. 来自完全弗氏佐剂免疫供体的血清抑制低反应性小鼠品系中辐射增强的IgE产生。
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Hapten-specific IgE antibody responses in mice. VII. Conversion of IgE "non-responder" strains to IgE "responders" by elimination of suppressor T cell activity.小鼠中半抗原特异性IgE抗体反应。VII. 通过消除抑制性T细胞活性将IgE“无反应”品系转变为IgE“有反应”品系。
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Hapten-specific IgE antibody responses in mice. VI. Selective enhancement of IgE antibody production by low doses of X-irradiation and by cyclophosphamide.小鼠中半抗原特异性IgE抗体反应。VI. 低剂量X射线照射和环磷酰胺对IgE抗体产生的选择性增强作用。
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The IgE antibody system is coordinately regulated by FcR epsilon-positive lymphoid cells and IgE-selective soluble factors.
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Regulation of IgE antibody production by serum molecules. VII. The IgE-selective damping activity of suppressive factor of allergy (SFA) is exerted across both strain and species restriction barriers.血清分子对IgE抗体产生的调节作用。VII. 变应性抑制因子(SFA)的IgE选择性抑制活性跨越品系和物种限制屏障发挥作用。
J Immunol. 1980 Feb;124(2):819-24.

引用本文的文献

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Allergy to bee stings: a review.蜂蜇过敏:综述
J R Soc Med. 1980 Nov;73(11):807-10. doi: 10.1177/014107688007301110.
2
Recent studies on the regulation of IgE antibody synthesis in experimental animals and man.近期关于实验动物和人类中IgE抗体合成调控的研究。
Immunology. 1980 Sep;41(1):1-24.
3
Suppression of IgE antibody production in SJL mice. IV. Interaction of primed and unprimed T cells.SJL小鼠中IgE抗体产生的抑制。IV. 致敏T细胞与未致敏T细胞的相互作用。
J Exp Med. 1979 Sep 19;150(3):507-16. doi: 10.1084/jem.150.3.507.

本文引用的文献

1
Hapten-specific IgE antibody responses in mice. IV. Evidence for distinctive sensitivities of IgE and IgG B lymphocytes to the regulatory influence of T cells.小鼠对半抗原特异性的IgE抗体反应。IV. IgE和IgG B淋巴细胞对T细胞调节影响的独特敏感性的证据。
J Immunol. 1974 Sep;113(3):974-83.
2
Suppression of IgE antibody production in SJL mice. I. Nonspecific suppressor T cells.SJL小鼠中IgE抗体产生的抑制作用。I. 非特异性抑制性T细胞。
J Exp Med. 1976 Apr 1;143(4):833-45. doi: 10.1084/jem.143.4.833.
3
Suppression of IgE antibody production in SJL mice. III. Characterization of a suppressor substance extracted from normal SJL spleen cells.SJL小鼠中IgE抗体产生的抑制作用。III. 从正常SJL脾细胞中提取的一种抑制物质的特性
J Exp Med. 1977 Jun 1;145(6):1501-10. doi: 10.1084/jem.145.6.1501.
4
Regulation of IgE antibody production by serum molecules. II. Strain-specificity of the suppressive activity of serum from complete freund's adjuvant-immune low responder mouse donors.
J Immunol. 1978 Jun;120(6):2060-7.
5
Regulation of IgE antibody production by serum molecules. I. Serum from complete Freund's adjuvant-immune donors suppresses irradiation-enhanced IgE production in low responder mouse strains.血清分子对IgE抗体产生的调节。I. 来自完全弗氏佐剂免疫供体的血清抑制低反应性小鼠品系中辐射增强的IgE产生。
J Immunol. 1978 Jun;120(6):2050-9.
6
The allergic phenotype: manifestation of 'allergic breakthrough' and imbalance in normal 'damping' of IgE antibody production.
Immunol Rev. 1978;41:77-108. doi: 10.1111/j.1600-065x.1978.tb01461.x.
7
Control of IgE antibody production by suppressor substances.抑制物质对IgE抗体产生的控制。
J Allergy Clin Immunol. 1978 Jul;62(1):44-55. doi: 10.1016/0091-6749(78)90072-6.
8
Induction of specific immune unresponsiveness with purified mixed leukocyte culture-activated T lymphoblasts as autoimmunogen. II. An analysis of the effects measured at the cellular and serological levels.以纯化的混合淋巴细胞培养激活的T淋巴母细胞作为自身免疫原诱导特异性免疫无反应性。II. 细胞水平和血清学水平所测效应的分析
J Exp Med. 1978 Jan 1;147(1):50-61. doi: 10.1084/jem.147.1.50.
9
Regulation of antibody response in different immunoglobulin classes. III. In vitro demonstration of "IgE class-specific" suppressor functions of DNP-mycobacterium-primed T cells and the soluble factor released from these cells.不同免疫球蛋白类别的抗体应答调节。III. 二硝基苯-分枝杆菌致敏T细胞的“IgE类别特异性”抑制功能及这些细胞释放的可溶性因子的体外证明。
J Immunol. 1977 Jul;119(1):149-55.