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1
Induction of contact sensitivity by cell-associated immunocomplexes requires activation of the early complement components.细胞相关免疫复合物诱导接触敏感性需要早期补体成分的激活。
Int J Exp Pathol. 1992 Dec;73(6):741-50.
2
Role of the fourth complement component (C4) in the regulation of contact sensitivity. III. In vivo effect of purified C4.第四补体成分(C4)在接触敏感性调节中的作用。III. 纯化C4的体内效应。
Cell Immunol. 1989 Oct 1;123(1):236-43. doi: 10.1016/0008-8749(89)90283-9.
3
Complement activation by cell-associated immune complexes in contact sensitivity.接触性超敏反应中细胞相关免疫复合物介导的补体激活
Cell Immunol. 1984 Dec;89(2):376-84. doi: 10.1016/0008-8749(84)90339-3.
4
Role of the fourth complement component (C4) in the regulation of contact sensitivity. II. Qualitative differences between C4 molecules from high- and low-C4 mouse strains.第四补体成分(C4)在接触敏感性调节中的作用。II. 高C4和低C4小鼠品系C4分子的质性差异。
Cell Immunol. 1989 Apr 1;119(2):243-51. doi: 10.1016/0008-8749(89)90241-4.
5
Role of the fourth complement component (C4) in the regulation of contact sensitivity. I. Analysis in mice with high and low C4 levels.第四补体成分(C4)在接触敏感性调节中的作用。I. 对C4水平高和低的小鼠的分析。
Cell Immunol. 1987 Apr 1;105(2):386-96. doi: 10.1016/0008-8749(87)90086-4.
6
Molecular basis of complement resistance of human melanoma cells expressing the C3-cleaving membrane protease p65.表达裂解C3的膜蛋白酶p65的人黑色素瘤细胞补体抗性的分子基础
Cancer Res. 1993 Feb 1;53(3):592-9.
7
The failure to show a necessary role for C3 in the in vitro antibody response.未能证明补体3(C3)在体外抗体反应中发挥必要作用。
Eur J Immunol. 1975 Mar;5(3):185-93. doi: 10.1002/eji.1830050307.
8
Immunoregulatory role of Ig isotypes. I. Induction of contrasuppressor T cells for contact sensitivity responses by antibodies of the IgM, IgG1, and IgG3 isotypes.免疫球蛋白同种型的免疫调节作用。I. IgM、IgG1和IgG3同种型抗体诱导接触敏感性反应的抗抑制性T细胞。
J Immunol. 1988 Aug 1;141(3):756-64.
9
Induction of contact sensitivity. Selective induction of delayed hypersensitivity by the injection of cells from draining lymph nodes into the footpads of normal recipients.接触敏感性的诱导。通过将引流淋巴结中的细胞注射到正常受体的足垫中,选择性诱导迟发型超敏反应。
Immunology. 1978 Apr;34(4):725-31.
10
Analysis of the induction phase of contact sensitivity by footpad transfer of regional lymph node cells. Macrophages and radioresistant T-lymphocytes induce immunity.通过局部淋巴结细胞的足垫转移分析接触敏感性的诱导期。巨噬细胞和抗辐射T淋巴细胞诱导免疫。
Immunology. 1977 Jan;32(1):81-8.

引用本文的文献

1
Activated complement component 3 (C3) is required for ultraviolet induction of immunosuppression and antigenic tolerance.紫外线诱导免疫抑制和抗原耐受性需要激活补体成分3(C3)。
J Exp Med. 1998 Apr 6;187(7):1133-8. doi: 10.1084/jem.187.7.1133.

本文引用的文献

1
Immunogenic cells in the regional lymph nodes after painting with the contact sensitizers picryl chloride and oxazolone: evidence for the presence of IgM antibody on their surface.在用接触性致敏剂氯化苦基和恶唑酮涂抹后区域淋巴结中的免疫原性细胞:其表面存在IgM抗体的证据。
Immunology. 1983 Mar;48(3):561-9.
2
Delayed hypersensitivity reactions to Listeria monocytogenes in rats decomplemented with cobra factor and in C5-deficient mice.用眼镜蛇因子去补体的大鼠及C5缺陷小鼠对单核细胞增生李斯特菌的迟发型超敏反应
Immunology. 1981 Jun;43(2):271-9.
3
Complement activation by cell-associated immune complexes in contact sensitivity.接触性超敏反应中细胞相关免疫复合物介导的补体激活
Cell Immunol. 1984 Dec;89(2):376-84. doi: 10.1016/0008-8749(84)90339-3.
4
A comparison of the properties of two classes, C4A and C4B, of the human complement component C4.人类补体成分C4的两个类别C4A和C4B的特性比较。
EMBO J. 1984 Aug;3(8):1819-23. doi: 10.1002/j.1460-2075.1984.tb02052.x.
5
Role of the fourth complement component (C4) in the regulation of contact sensitivity. I. Analysis in mice with high and low C4 levels.第四补体成分(C4)在接触敏感性调节中的作用。I. 对C4水平高和低的小鼠的分析。
Cell Immunol. 1987 Apr 1;105(2):386-96. doi: 10.1016/0008-8749(87)90086-4.
6
C4-mediated inhibition of immune precipitation and differences in inhibitory action of genetic variants, C4A3 and C4B1.C4介导的免疫沉淀抑制作用以及基因变体C4A3和C4B1抑制作用的差异
Complement. 1988;5(3):110-9. doi: 10.1159/000463045.
7
Antigen-bound C3b and C4b enhance antigen-presenting cell function in activation of human T-cell clones.抗原结合的C3b和C4b在人T细胞克隆激活中增强抗原呈递细胞功能。
Immunology. 1988 Oct;65(2):229-35.
8
The molecular basis of the low hemolytic activity of C4 molecules from low-C4 mice with IgM-coated erythrocytes.来自低C4小鼠且红细胞被IgM包被的C4分子溶血活性低的分子基础。
Eur J Immunol. 1989 Sep;19(9):1613-8. doi: 10.1002/eji.1830190914.
9
Role of the fourth complement component (C4) in the regulation of contact sensitivity. III. In vivo effect of purified C4.第四补体成分(C4)在接触敏感性调节中的作用。III. 纯化C4的体内效应。
Cell Immunol. 1989 Oct 1;123(1):236-43. doi: 10.1016/0008-8749(89)90283-9.
10
Role of the fourth complement component (C4) in the regulation of contact sensitivity. II. Qualitative differences between C4 molecules from high- and low-C4 mouse strains.第四补体成分(C4)在接触敏感性调节中的作用。II. 高C4和低C4小鼠品系C4分子的质性差异。
Cell Immunol. 1989 Apr 1;119(2):243-51. doi: 10.1016/0008-8749(89)90241-4.

细胞相关免疫复合物诱导接触敏感性需要早期补体成分的激活。

Induction of contact sensitivity by cell-associated immunocomplexes requires activation of the early complement components.

作者信息

Lio D, Sireci G, Gervasi F, Dieli F, Salerno A

机构信息

Institute of General Pathology, University of Palermo, Italy.

出版信息

Int J Exp Pathol. 1992 Dec;73(6):741-50.

PMID:1493103
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2002425/
Abstract

Lymph node cells collected from CBA/J mice 4 days after painting the skin with picryl chloride behave like antigen presenting cells and induce contact sensitivity when injected into naive recipient mice. The immunizing capacity of these '4-day' cells is due to T cells which carry on their membrane hapten-IgM immunocomplexes. Incubation of the cells with complement from mouse strains that express high C4 serum levels (C4H), abolishes their immunizing capacity. This effect is related to the activation of the early components of the classical complement pathway, as supported by experiments using C3 and C4-depleted or C5 and C6-genetically deficient mouse sera. The detection of different amounts of C3b and C4b on the surface of 4-day T cells after incubation with C4L and C4H sera supports the possibility that membrane bound activated complement components could modify the immunizing capacity of these cells. Results herein reported suggest that membrane-bound C3b and C4b are not per se inhibitory but interfere with the residual complement activating capacity of 4-day T cells. The role of complement activation by 4-day T cells is pivotal as complement depletion of recipient mice by cobra venom factor (CVF) inhibits the immunizing capacity of untreated 4-day T cells, while 4-day T cells treated with complement in vitro and injected together with C4a anaphylatoxin are able to immunize recipient mice.

摘要

在用苦味酸氯涂抹皮肤4天后从CBA/J小鼠收集的淋巴结细胞表现得像抗原呈递细胞,当注入未致敏的受体小鼠时可诱导接触性敏感。这些“4天”细胞的免疫能力归因于其细胞膜上携带半抗原-IgM免疫复合物的T细胞。将这些细胞与表达高C4血清水平(C4H)的小鼠品系的补体一起孵育,会消除它们的免疫能力。如使用C3和C4缺失或C5和C6基因缺陷小鼠血清的实验所支持的,这种效应与经典补体途径早期成分的激活有关。在用C4L和C4H血清孵育后,在4天T细胞表面检测到不同量的C3b和C4b,这支持了膜结合的活化补体成分可能改变这些细胞免疫能力的可能性。本文报道的结果表明,膜结合的C3b和C4b本身并无抑制作用,但会干扰4天T细胞剩余的补体激活能力。4天T细胞激活补体的作用至关重要,因为用眼镜蛇毒因子(CVF)使受体小鼠补体耗竭会抑制未处理的4天T细胞的免疫能力,而体外经补体处理并与C4a过敏毒素一起注射的4天T细胞能够使受体小鼠产生免疫。