首页> 美国政府科技报告 >Complement Depletion Protects Lupus-prone Mice from Ischemia-reperfusion-initiated Organ Injury.

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Complement Depletion Protects Lupus-prone Mice from Ischemia-reperfusion-initiated Organ Injury.

机译：补体消耗保护易患狼疮的小鼠免受缺血再灌注引起的器官损伤。

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Ischemia-reperfusion (IR) injury causes a vigorous immune response that is amplified by complement activation, leading to local and remote tissue damage. Using MRL/lpr mice, which are known to experience accelerated tissue damage after mesenteric IR injury, we sought to evaluate whether complement inhibition mitigates organ damage. We found that complement depletion with cobra venom factor protected mice from local and remote lung tissue damage. Protection from injury was associated with less complement (C3) and membrane attack complex deposition, less neutrophil infiltration, and lower levels of local proinflammatory cytokine production. In addition, complement depletion was able to decrease the level of oxidative stress as measured by glutathione peroxidase 1 mRNA levels and superoxide dismutase activity. Furthermore, blockage of C5a receptor protected MRL/lpr mice from local tissue damage, but not from remote lung tissue damage. In conclusion, although treatments with cobra venom factor and C5a receptor antagonist were able to protect mice from local tissue damage, treatment with C5a receptor antagonist was not able to protect mice from remote lung tissue damage, implying that more factors contribute to the development of remote tissue damage after IR injury. These data also suggest that complement inhibition at earlier, rather than late, stages can have clinical benefit in conditions that are complicated with IR injury.

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Ioannou, A.; Lieberman, L. A.; Lucca, J. J.; Tsokos, G. C.;
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年度 2012
页码 1-11
总页数 11
原文格式 PDF
正文语种 eng
中图分类工业技术;
关键词
COMPLEMENT(BIOLOGY); ISCHEMIA; LUPUS ERYTHEMATOSUS; ORGANS(ANATOMY); WOUNDS AND INJURIES; ANTIBODIES; MICE; STRESS(PHYSIOLOGY); COMPLEMENT DEPLETION; IR(ISCHEMIA-REPERFUSION); OXIDATIVE STRESS; COBRA VENOM FACTOR; SLE(SYSTEMIC LUPUS ERYTHEMATOSUS);

机译：补体（生物学）;缺血; LUpUs ERYTHEmaTOsUs;器官（解剖）;伤口和伤害;抗体;小鼠;应力（生理学）;补体消耗; IR（缺血 - 再灌注）;氧化应激; COBRa VENOm因子; sLE（系统性红斑狼疮））;

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1. Complement depletion protects lupus-prone mice from ischemia-reperfusion-initiated organ injury [J] . Aetonis Ioannou, Linda A. Lieberman, Jurir J. Dalle Lucca, American Journal of Physiology . 2013,第2Pta1期

机译：补体耗竭保护易患狼疮的小鼠免受缺血再灌注引发的器官损伤
2. IL-2 protects lupus-prone mice from multiple end-organ damage by limiting CD4-CD8-IL-17-producing T cells [J] . MizuiM., KogaT., LiebermanL.A., The Journal of Immunology: Official Journal of the American Association of Immunologists . 2014,第5期

机译：IL-2通过限制产生CD4-CD8-IL-17的T细胞保护易患狼疮的小鼠免受多种末端器官损害
3. IL-2 protects lupus-prone mice from multiple end-organ damage by limiting CD4-CD8-IL-17-producing T cells [J] . MizuiM., KogaT., LiebermanL.A., The Journal of Immunology: Official Journal of the American Association of Immunologists . 2014,第5期

机译：IL-2通过限制产生CD4-CD8-IL-17的T细胞保护易患狼疮的小鼠免受多种末端器官损害
4. Role of Complement Activation Products and Receptors in Lung Inflammatory Injury. [C] . Peter A 第四届上海国际呼吸病研讨会暨第十五届亚太呼吸治疗学会联合会议（ISRD 2007）(4rd Inte . 2007

机译：补体激活产物和受体在肺炎性损伤中的作用。
5. Murine gammaherpesvirus 68 infection protects lupus-prone mice from the development of autoimmunity. [D] . Larson, Jennifer D. 2012

机译：鼠丙种疱疹病毒68感染可保护易患狼疮的小鼠免于自身免疫的发展。
6. Interleukin-2 Protects Lupus-prone Mice from Multiple End-organ Damage by Limiting CD4−CD8− Interleukin-17-producing T-cells [O] . Masayuki Mizui, Tomohiro Koga, Linda A. Lieberman, -1

机译：Interleukin-2通过限制产生CD4-CD8- Interleukin-17的T细胞保护易狼疮小鼠免受多种末端器官损害
7. IL-2 Protects Lupus-Prone Mice from Multiple End-Organ Damage by Limiting CD4−CD8− IL-17–Producing T Cells [O] . Masayuki Mizui, Tomohiro Koga, Linda A. Lieberman, 2014

机译：通过限制产生CD4-CD8-IL-17产生的T细胞，IL-2通过多端器官损伤保护狼疮易一鼠

Complement Depletion Protects Lupus-prone Mice from Ischemia-reperfusion-initiated Organ Injury.

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