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利用体内斑马鱼模型来了解嗜中性粒细胞性呼吸道疾病的生化基础。

Using in vivo zebrafish models to understand the biochemical basis of neutrophilic respiratory disease.

作者信息

Martin Jane S, Renshaw Stephen A

机构信息

MRC Centre for Developmental and Biomedical Genetics, University of Sheffield, Western Bank, Sheffield S10 2TN, UK.

出版信息

Biochem Soc Trans. 2009 Aug;37(Pt 4):830-7. doi: 10.1042/BST0370830.

Abstract

Neutrophilic inflammation in the lung protects against infectious disease, and usually resolves spontaneously after removal of the inflammatory stimulus. However, much lung disease is caused by a failure of resolution of neutrophilic inflammation. Our laboratory is seeking an understanding of the biochemical basis of inflammation resolution, using the zebrafish model system. Zebrafish larvae are transparent, allowing visualization of GFP (green fluorescent protein)-labelled leucocytes during inflammation in vivo, and they can be readily manipulated by a range of forward and reverse genetic techniques. This combination of advantages makes zebrafish a powerful tool for the study of in vivo inflammatory processes. Using this model, we have visualized the process of inflammation resolution in vivo, and identified a role for apoptosis in this process. In addition, we have performed a forward genetic screen for mutants with defective resolution of inflammation, and reverse genetic experiments examining the influence of candidate genes on inflammation resolution. We have established a platform for screening for compounds with anti-inflammatory activity, which has yielded a number of interesting leads. Looking forward to succeed in the future, we are working at combining mutants, transgenes and pharmacological agents to dissect the biochemical basis of inflammation resolution, and to identify compounds that might be used to treat patients with respiratory disease.

摘要

肺部的中性粒细胞炎症可抵御传染病,并且在炎症刺激消除后通常会自发消退。然而,许多肺部疾病是由中性粒细胞炎症消退失败所致。我们实验室正在利用斑马鱼模型系统来深入了解炎症消退的生化基础。斑马鱼幼体是透明的,这使得在体内炎症过程中能够可视化绿色荧光蛋白(GFP)标记的白细胞,并且可以通过一系列正向和反向遗传技术对它们进行轻松操作。这些优势的结合使斑马鱼成为研究体内炎症过程的强大工具。利用这个模型,我们已经在体内可视化了炎症消退的过程,并确定了细胞凋亡在这个过程中的作用。此外,我们对炎症消退存在缺陷的突变体进行了正向遗传筛选,并通过反向遗传实验研究了候选基因对炎症消退的影响。我们已经建立了一个筛选具有抗炎活性化合物的平台,该平台已经产生了一些有趣的线索。展望未来取得成功,我们正在致力于将突变体、转基因和药物制剂结合起来,以剖析炎症消退的生化基础,并确定可能用于治疗呼吸系统疾病患者的化合物。

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