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Genetically determined resistance to listeriosis is associated with increased accumulation of inflammatory neutrophils and macrophages which have enhanced listericidal activity.遗传决定的对李斯特菌病的抗性与具有增强的杀李斯特菌活性的炎性中性粒细胞和巨噬细胞的积累增加有关。
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Roles of factor increasing monocytopoiesis (FIM) and macrophage activation in host resistance to Listeria monocytogenes.促进单核细胞生成因子(FIM)和巨噬细胞激活在宿主抗单核细胞增生李斯特菌感染中的作用
Infection. 1988;16 Suppl 2:S137-40. doi: 10.1007/BF01639736.
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Comparison of responsiveness to the monocytosis-producing activity of Listeria monocytogenes in mice genetically susceptible or resistant to listeriosis.对单核细胞增多性李斯特菌产生单核细胞增多活性的反应性在对李斯特菌病遗传易感或抗性小鼠中的比较。
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Analysis of macrophage bactericidal function in genetically resistant and susceptible mice by using the temperature-sensitive mutant of Listeria monocytogenes.利用单核细胞增生李斯特菌的温度敏感突变体分析基因抗性和易感小鼠的巨噬细胞杀菌功能。
Infect Immun. 1986 Nov;54(2):315-21. doi: 10.1128/iai.54.2.315-321.1986.
10
Increased activity of FIM in serum of mice during a Mycobacterium bovis (BCG) infection.在牛分枝杆菌(卡介苗)感染期间,小鼠血清中FIM活性增加。
Immunology. 1990 Jul;70(3):327-31.

本文引用的文献

1
Genetic linkage of resistance to Listeria monocytogenes with macrophage inflammatory responses.对单核细胞增生李斯特菌的抗性与巨噬细胞炎症反应的遗传连锁
J Immunol. 1981 Aug;127(2):402-7.
2
Synthesis and release of factor increasing monocytopoiesis (FIM) by macrophages.巨噬细胞合成并释放单核细胞生成增加因子(FIM)。
Adv Exp Med Biol. 1982;141:225-32. doi: 10.1007/978-1-4684-8088-7_24.
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Are the Lsh and Ity disease resistance genes at one locus on mouse chromosome 1?Lsh和Ity抗病基因位于小鼠1号染色体的一个基因座上吗?
Nature. 1982 Jun 10;297(5866):510-1. doi: 10.1038/297510a0.
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Genetic regulation of resistance to intracellular pathogens.对细胞内病原体抗性的遗传调控。
Nature. 1982 Jun 10;297(5866):506-9. doi: 10.1038/297506a0.
5
Macrophages in resistance to rickettsial infections: genetic analysis of susceptibility to lethal effects of Rickettsia akari infection and development of activated, cytotoxic macrophages in A and B10.a mice.巨噬细胞在抗立克次体感染中的作用:对感染立克次体痘致死效应易感性的遗传分析以及A和B10.a小鼠中活化细胞毒性巨噬细胞的发育
J Immunol. 1982 Oct;129(4):1719-23.
6
Genetically determined differences in antibacterial activity of macrophages are expressed in the environment in which the macrophage precursors mature.巨噬细胞抗菌活性的基因决定差异在巨噬细胞前体成熟的环境中得以体现。
Cell Immunol. 1980 Aug 1;53(2):341-9. doi: 10.1016/0008-8749(80)90334-2.
7
Presence of the factor increasing monocytopoiesis (FIM) in rabbit peripheral blood during an acute inflammation.急性炎症期间兔外周血中单核细胞生成增加因子(FIM)的存在。
J Reticuloendothel Soc. 1983 Sep;34(3):235-52.
8
Quantitative study on the production and kinetics of mononuclear phagocytes during an acute inflammatory reaction.急性炎症反应期间单核吞噬细胞生成及动力学的定量研究。
J Exp Med. 1973 Dec 1;138(6):1314-30. doi: 10.1084/jem.138.6.1314.
9
Peritoneal macrophage response in neonatal mice.新生小鼠的腹膜巨噬细胞反应
J Reticuloendothel Soc. 1973 Aug;14(2):181-91.
10
A serum facted by newborn calf serum.一种由新生牛血清促成的血清。
Cell Tissue Kinet. 1976 Jan;9(1):51-63.

近交系小鼠品系对增加单核细胞生成因子的反应差异。

Differences in the response of inbred mouse strains to the factor increasing monocytopoiesis.

作者信息

Sluiter W, Elzenga-Claasen I, van der Voort van der Kley-van Andel A, van Furth R

出版信息

J Exp Med. 1984 Feb 1;159(2):524-36. doi: 10.1084/jem.159.2.524.

DOI:10.1084/jem.159.2.524
PMID:6693834
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2187230/
Abstract

Previous studies have shown that monocyte production during an inflammatory response is controlled by the factor increasing monocytopoiesis (FIM), secreted by macrophages at the site of inflammation. The inflammatory reaction to latex particles and a saline-soluble extract of Listeria monocytogenes (SEL), expressed as the number of monocytes in the circulation and of macrophages at the site of inflammation, was about twice as strong in C57BL/10 mice compared with CBA mice. This raised the question as to the mechanism underlying these differences. One possibility might be that these mouse strains differ with respect to the production of FIM, but this cannot be the case because the maximum levels of FIM activity in the serum of both C57BL/10 and CBA mice given latex or SEL intraperitoneally were almost the same; however, the courses of FIM activity in the two strains after intraperitoneal latex were not exactly synchronous. Another possibility is that the sensitivity of monocyte precursor cells for FIM differs. Evidence for the latter was provided by the finding that the intravenous injection of sera with FIM activity obtained from C57BL/10 and from CBA mice into the C57BL/10 mice evoked monocytosis, whereas CBA mice did not respond to these sera. Earlier studies showed that an increase of monocytes after the injection of serum containing FIM reflects increased monocyte production. Taken together, the results of the present study demonstrate that one of the mechanisms underlying the genetic control of the inflammatory response is, rather than enhanced FIM synthesis, the ability of monocyte precursors in the bone marrow to respond to FIM by increased monocyte production.

摘要

先前的研究表明,炎症反应期间单核细胞的产生受炎症部位巨噬细胞分泌的促单核细胞生成因子(FIM)控制。对乳胶颗粒和单核细胞增生李斯特菌的水溶性提取物(SEL)的炎症反应,以循环中的单核细胞数量和炎症部位的巨噬细胞数量表示,C57BL/10小鼠的反应强度约为CBA小鼠的两倍。这就引发了关于这些差异背后机制的问题。一种可能性可能是这些小鼠品系在FIM的产生方面存在差异,但情况并非如此,因为腹腔注射乳胶或SEL后,C57BL/10和CBA小鼠血清中FIM活性的最高水平几乎相同;然而,腹腔注射乳胶后,这两个品系中FIM活性的变化过程并非完全同步。另一种可能性是单核细胞前体细胞对FIM的敏感性不同。后者的证据来自以下发现:将从C57BL/10和CBA小鼠获得的具有FIM活性的血清静脉注射到C57BL/10小鼠中会引起单核细胞增多,而CBA小鼠对这些血清没有反应。早期研究表明,注射含FIM的血清后单核细胞增加反映了单核细胞产生的增加。综上所述,本研究结果表明,炎症反应遗传控制的潜在机制之一不是FIM合成增强,而是骨髓中的单核细胞前体通过增加单核细胞产生来响应FIM的能力。