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Immunologia e infezioni

在小鼠体内的巨噬细胞的枯竭和重建

Published: August 01, 2012
doi:
10.3791/4105
, ,
1Department of Graduate Studies,University of British Columbia , 2Department of Molecular Biology,Vrije Universiteit Amsterdam, 3Department of Pediatrics,University of British Columbia

Summary

巨噬细胞发挥核心作用的动态平衡,并在许多组织的病理。这里介绍的协议描述消耗巨噬细胞的方法<em>在体内</em>,来自偏光巨噬细胞,骨髓穿刺,继转移到小鼠巨噬细胞。这些技术允许极化的巨噬细胞在健康和疾病中发挥的作用的决心。

Abstract

巨噬细胞是重要的球员,在传染病的挑战或损伤的先天免疫反应,发起的先天免疫反应和指挥后天免疫反应。巨噬细胞功能障碍可能导致无法安装适当的免疫反应,因此,已在许多疾病的进程,包括炎症性肠病牵连。巨噬细胞显示极化表型大致分为两类。经典活化的巨噬细胞,与干扰素γ或LPS刺激激活,发挥了至关重要的作用,在细菌的挑战,而另外激活的巨噬细胞,IL-4和IL-13激活,参与清除杂物和组织重塑和已在该决议牵连阶段的炎症。在体内的炎症反应,巨噬细胞的免疫细胞浸润的复杂混合物中发现,并可能加剧或resolvin参加Ğ炎症。巨噬细胞的作用,在整个动物模型的定义在原地 ,这是必要的检查消耗从复杂的环境中的巨噬细胞的影响。极化的巨噬细胞表型定义问原位巨噬细胞表型的作用的问题,可以导出体外 ,从骨髓穿刺,并加回或没有事先枯竭的巨噬细胞,小鼠。在这里提出的协议中含有氯膦酸二钠,脂质体,与PBS注射控件,用来消耗结肠巨噬细胞在葡聚糖硫​​酸钠(DSS)诱导小鼠结肠炎。此外,巨噬细胞的极化,推导出体外,并转移到小鼠静脉注射。这种方法的一个需要注意的是,氯膦酸二钠含脂质体耗尽所有专业的吞噬细胞,包括树突状细胞和巨噬细胞,所以,以确保枯竭所观察到的效果是巨噬细胞特异性,重组ØF的巨噬细胞过继转移表型是必要的。全身巨噬细胞耗竭小鼠也可以通过回交小鼠实现到细胞CD11b-DTR背景,这是一个很好的补充办法。含有氯膦酸二钠脂质体介导的枯竭的优势是,它不参与回交小鼠需要的时间和费用,它可以在小鼠小鼠(C57BL / 6小鼠,BALB / c小鼠,或混合背景的背景下,无论使用)。

Protocol

1。使用含有氯磷酸二钠,脂质体的消耗巨噬细胞脂质体储存在4°C注射前两个小时,从冰箱中取出氯膦酸二钠含脂质体,PBS含脂质体,或无菌PBS(喷射控制),使他们能够适应新环境室温(18℃)。 反转管含脂质体的8-10倍,以确保均匀分布,然后装入1 ml注射器200μL。将26号针头注射器顶端。 用你的左手,浮渣鼠标,略低于持有足够的皮肤以固定其头部和四肢的耳朵。 …

Discussion

巨噬细胞的吞噬细胞在免疫系统中发挥重要作用。他们是负责发起的先天免疫反应和指挥后天免疫反应。通常情况下,经典激活巨噬细胞被激活IFNγ的或LPS,并有责任为消除病原体和安装的炎症反应1。相反,IL-4和IL-13激活或者激活巨噬细胞和炎症的决议过程中发挥在碎片中的作用,清除和组织重塑。专门的巨噬细胞在肠道保留其杀菌活性,但不装入一个亲炎症反应2。这种有益菌?…

Divulgazioni

The authors have nothing to disclose.

Acknowledgements

这项工作得到了1“的研究资助津贴”的克隆氏病的和结肠炎加拿大基金会的LMS,谁是1​​消化科/加拿大协会健康研究/克罗恩的小号和结肠炎加拿大新研究者奖基金会加拿大协会的支持。

Materials

Name of the reagent Company Catalogue number
Clodronate-containing liposomes Clodronateliposomes.org  
PBS-containing liposomes Clodronateliposomes.org  
Sterile PBS pH7.4 Invitrogen 14190
IMDM Invitrogen 12440
Fetal Calf Serum (FCS) Invitrogen 12483
acetic acid BDH Aristar BDH3092-500MLP
Monothioglycerol (MTG) Sigma 96-275
Recombinant murine MCSF Stemcell Technologies 02951
Recombinant murine GM-CSF Stemcell Technologies 02935
Recombinant murine IL-3 Stemcell Technologies 02903
Recombinant murine IFNγ Stemcell Technologies 02746
Recombinant murine IL-4 Stemcell Technologies 02714
Cell Dissociation Buffer Invitrogen 13150-016
Rat anti-F4/80 Antibody AbD Serotec MCA497GA
Mouse anti-ArgI Antibody BD Transduction Laboratories 610708

Table 1. Specific reagents used in this protocol.

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Riferimenti

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Tags

DepletionReconstitutionMacrophagesMiceInnate Immune ResponseAcquired Immune ResponseMacrophage DysfunctionDisease ProcessesInflammatory Bowel DiseasesPolarized PhenotypesClassically Activated MacrophagesAlternatively Activated MacrophagesIFN-gammaLPSIL-4IL-13InflammationInflammatory ResponseWhole Animal ModelDepleting MacrophagesComplex EnvironmentPhenotypically Defined Polarized MacrophagesBone Marrow Aspirates
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Weisser, S. B., van Rooijen, N., Sly, L. M. Depletion and Reconstitution of Macrophages in Mice. J. Vis. Exp. (66), e4105, doi:10.3791/4105 (2012).
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