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相似文献

1
Role of macrophages in immunological maturation.巨噬细胞在免疫成熟中的作用。
J Exp Med. 1968 Sep 1;128(3):459-67. doi: 10.1084/jem.128.3.459.
2
Requirement for continuous antigenic stimulation in the development and differentiation of antibody-forming cells. The effect of passive antibody on the primary and secondary response.抗体形成细胞发育和分化过程中对持续抗原刺激的需求。被动抗体对初次和二次反应的影响。
J Exp Med. 1969 May 1;129(5):953-71. doi: 10.1084/jem.129.5.953.
3
Transplantation of adult peritoneal cells into newborn mice.将成年腹膜细胞移植到新生小鼠体内。
Transplantation. 1969 Sep;8(3):241-8. doi: 10.1097/00007890-196909000-00005.
4
Functional maturation of neonatal spleen cells.新生脾脏细胞的功能成熟
Immunology. 1979 Mar;36(3):527-32.
5
Gallium arsenide exposure impairs processing of particulate antigen by macrophages: modification of the antigen reverses the functional defect.砷化镓暴露会损害巨噬细胞对颗粒性抗原的处理:抗原的修饰可逆转功能缺陷。
Life Sci. 2004 Jun 11;75(4):485-98. doi: 10.1016/j.lfs.2004.01.011.
6
Ontogeny of 'macrophage' function. III. Manifestation of high accessory cell activity for primary antibody response by Ia+ functional cells in newborn mouse spleen in collaboration with Ia- macrophages.“巨噬细胞”功能的个体发生。III. 新生小鼠脾脏中Ia⁺功能细胞与Ia⁻巨噬细胞协作对初次抗体应答表现出高辅助细胞活性。
Immunology. 1982 Nov;47(3):449-57.
7
Mechanism by which adult mouse peritoneal macrophages affect neonatal suppressor cell activity.成年小鼠腹腔巨噬细胞影响新生抑制细胞活性的机制。
Transplantation. 1983 Sep;36(3):328-33. doi: 10.1097/00007890-198309000-00019.
8
Immune responses in vitro. II. Suppression of the immune response in vitro by specific antibody.体外免疫反应。II. 特异性抗体对体外免疫反应的抑制
J Exp Med. 1969 Aug 1;130(2):365-79. doi: 10.1084/jem.130.2.365.
9
Effect of adult peritoneal cells on the antibody response of newborn mice to sheep red blood cells.成年腹膜细胞对新生小鼠针对绵羊红细胞的抗体反应的影响。
J Immunol. 1971 Jun;106(6):1681-3.
10
Comparison of the immune response potential of newborn mice to T-dependent and T-independent synthetic polypeptides.新生小鼠对T依赖型和T非依赖型合成多肽免疫反应潜力的比较。
Immunology. 1976 Feb;30(2):261-6.

引用本文的文献

1
Immunology and Virus Diseases.免疫学与病毒疾病
J R Coll Physicians Lond. 1970 Oct;5(1):31-45.
2
Growth of Mycobacterium lepraemurium in Cell-Impermeable Diffusion Chambers.细胞不可渗透扩散室中麻风分枝杆菌的生长。
Infect Immun. 1971 Jan;3(1):127-32. doi: 10.1128/iai.3.1.127-132.1971.
3
Ontogeny of murine macrophages: functions related to antigen presentation.小鼠巨噬细胞的个体发育:与抗原呈递相关的功能
Infect Immun. 1982 Apr;36(1):169-75. doi: 10.1128/iai.36.1.169-175.1982.
4
Enhancement of resistance to infections by endotoxin-induced serum factor from Mycobacterium bovis BCG-infected mice.卡介苗感染小鼠的内毒素诱导血清因子增强对感染的抵抗力
Infect Immun. 1980 Jun;28(3):654-9. doi: 10.1128/iai.28.3.654-659.1980.
5
Lung alveolar histiocytes engaged in antibody production.参与抗体产生的肺肺泡组织细胞。
Immunology. 1969 Aug;17(2):207-26.
6
Immune responses in vitro. I. Cellular requirements for the immune response by nonprimed and primed spleen cells in vitro.体外免疫反应。I. 体外非致敏和致敏脾细胞免疫反应的细胞需求。
J Exp Med. 1969 Aug 1;130(2):345-64. doi: 10.1084/jem.130.2.345.
7
Maturation of hemolysin-producing cell clones. II. The appearance and localization of precursor units in lymphoid tissues of neonatal mice.产溶血素细胞克隆的成熟。II. 新生小鼠淋巴组织中前体单位的出现及定位。
J Exp Med. 1970 Jun 1;131(6):1261-70. doi: 10.1084/jem.131.6.1261.
8
Cellular recognition by mouse lymphocytes in vitro. I. Definition of a new technique and results of stimulation by phytohemagglutinin and specific antigens.小鼠淋巴细胞在体外的细胞识别。I. 一种新技术的定义以及植物血凝素和特异性抗原刺激的结果。
J Exp Med. 1970 Jun 1;131(6):1049-78. doi: 10.1084/jem.131.6.1049.
9
Cells involved in the immune response. 8. The relationship between the loss and reappearance of antigen-reactive cells and immune responsiveness after irradiation of normal adult rabbits.参与免疫反应的细胞。8. 正常成年兔经照射后抗原反应性细胞的丧失与再现及免疫反应性之间的关系。
J Exp Med. 1969 Oct 1;130(4):867-76. doi: 10.1084/jem.130.4.867.
10
Studies on the effect of macrophages in an in vitro graft reaction system.巨噬细胞在体外移植反应系统中的作用研究。
Immunology. 1971 Nov;21(5):861-7.

本文引用的文献

1
INTRACELLULAR DISTRIBUTION AND DEGRADATION OF BACTERIOPHAGE IN MAMMALIAN TISSUES.噬菌体在哺乳动物组织中的细胞内分布与降解
J Immunol. 1965 Apr;94:544-50.
2
Role of macrophages in antibody production. Immune response to sheep red blood cells.巨噬细胞在抗体产生中的作用。对绵羊红细胞的免疫反应。
J Immunol. 1967 Oct;99(4):744-50.
3
The role of macrophages in the induction of antibody in x-irradiated animals.巨噬细胞在受X射线照射动物体内抗体诱导中的作用。
Immunology. 1967 Feb;12(2):197-206.
4
Mechanism of induction of immunological tolerance. II. Simultaneous development of priming and tolerance.免疫耐受的诱导机制。II. 致敏与耐受的同时发生。
Aust J Exp Biol Med Sci. 1966 Aug;44(4):327-40. doi: 10.1038/icb.1966.32.
5
Studies of the mechanism of antigen stimulation of DNA synthesis in rabbit spleen cultures.兔脾细胞培养中抗原刺激DNA合成机制的研究。
Immunology. 1965 Dec;9(6):529-41.
6
Mouse peritoneal cells: their ability to elicit or produce antibody after exposure to antigen.小鼠腹腔细胞:暴露于抗原后引发或产生抗体的能力。
Immunology. 1968 Mar;14(3):379-92.

巨噬细胞在免疫成熟中的作用。

Role of macrophages in immunological maturation.

作者信息

Argyris B F

出版信息

J Exp Med. 1968 Sep 1;128(3):459-67. doi: 10.1084/jem.128.3.459.

DOI:10.1084/jem.128.3.459
PMID:5666960
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2138526/
Abstract
  1. Transplantation of peritoneal macrophages from thioglycollate-stimulated adult C3H donor mice, into 3-day-old C3H mice results in an enhanced antibody response to simultaneously injected SRBC. The increase in immuno-competence is even more pronounced when 1-day-old C3H mice are pretreated with adult macrophages and sensitized 3 days later with SRBC. Nonviable macrophages or nonviable spleen cells are ineffective. 2. There is a critical period in the development of the neonatal mouse during which the spleen cells benefit from the addition of adult macrophages. Treatment before or beyond this stage is ineffective. 3. Very high doses (20 million) of macrophages are less effective in stimulating antibody synthesis to SRBC than doses of 5 or 10 million, suggesting that a critical ratio of macrophages to immunocompetent cells may be required for enhancing antibody synthesis in young mice. 4. The results are discussed in the light of the hypothesis that newborn mice are immunologically deficient not because they lack immunocompetent cells but because they lack an antigen recognition or antigen-processing system in the form of functional macrophages.
摘要
  1. 将经巯基乙酸刺激的成年C3H供体小鼠的腹腔巨噬细胞移植到3日龄的C3H小鼠体内,会增强对同时注射的绵羊红细胞(SRBC)的抗体反应。当1日龄的C3H小鼠先用成年巨噬细胞预处理,3天后再用SRBC致敏时,免疫能力的增强更为明显。无活力的巨噬细胞或无活力的脾细胞无效。2. 新生小鼠发育过程中有一个关键时期,在此期间脾细胞会从添加成年巨噬细胞中受益。在此阶段之前或之后进行处理均无效。3. 非常高剂量(2000万)的巨噬细胞在刺激对SRBC的抗体合成方面不如500万或1000万剂量有效,这表明增强幼鼠抗体合成可能需要巨噬细胞与免疫活性细胞的关键比例。4. 根据新生小鼠免疫缺陷不是因为缺乏免疫活性细胞,而是因为缺乏功能性巨噬细胞形式的抗原识别或抗原处理系统这一假说对结果进行了讨论。