School of Medicine, Ninewells Hospital and Medical School, University of Dundee, Dundee, DD1 9SY, UK.
J Physiol. 2018 Jan 1;596(1):105-127. doi: 10.1113/JP274915. Epub 2017 Nov 23.
Haem oxygenase 1 (Hmox1) is a cytoprotective enzyme with anti-inflammatory and anti-oxidant properties that is induced in response to multiple noxious environmental stimuli and disease states. Tools to enable its expression to be monitored in vivo have been unavailable until now. In a new Hmox1 reporter model we provide high-fidelity, single-cell resolution blueprints for Hmox1 expression throughout the body of mice. We show for the first time that Hmox1 is constitutively expressed at barrier tissues at the interface between the internal and external environments, and that it is highly induced in muscle cells during systemic inflammation. These data suggest novel biological insights into the role of Hmox1 and pave the way for the use of the model to study the role of environmental stress in disease pathology.
Hmox1 protein holds great promise as a biomarker of in vivo stress responses as it is highly induced in stressed or damaged cells. However, Hmox1 expression patterns have thus far only been available in simple model organisms with limited relevance to humans. We now report a new Hmox1 reporter line that makes it possible to obtain this information in mice, a premiere model system for studying human disease and toxicology. Using a state-of-the-art strategy, we expressed multiple complementary reporter molecules from the murine Hmox1 locus, including firefly luciferase, to allow long-term, non-invasive imaging of Hmox1 expression, and β-galactosidase for high-resolution mapping of expression patterns post-mortem. We validated the model by confirming the fidelity of reporter expression, and its responsiveness to oxidative and inflammatory stimuli. In addition to providing blueprints for Hmox1 expression in mice that provide novel biological insights, this work paves the way for the broad application of this model to establish cellular stresses induced by endogenous processes and those resulting from exposure to drugs and environmental agents. It will also enable studies on the role of oxidative stress in the pathogenesis of disease and its prevention.
血红素加氧酶 1(Hmox1)是一种具有抗炎和抗氧化特性的细胞保护酶,它是对多种有害环境刺激和疾病状态的反应而诱导产生的。直到现在,还没有工具可以监测其在体内的表达。在一个新的 Hmox1 报告模型中,我们为小鼠体内的 Hmox1 表达提供了高保真度的单细胞分辨率蓝图。我们首次表明,Hmox1 在内外环境界面的屏障组织中持续表达,并且在全身炎症期间在肌肉细胞中高度诱导。这些数据为 Hmox1 的作用提供了新的生物学见解,并为使用该模型研究环境应激在疾病发病机制中的作用铺平了道路。
Hmox1 蛋白作为一种体内应激反应生物标志物具有很大的应用前景,因为它在应激或受损细胞中高度诱导。然而,Hmox1 的表达模式迄今为止仅在与人类相关性有限的简单模式生物中可用。我们现在报告了一种新的 Hmox1 报告基因系,使得在小鼠中获得这些信息成为可能,小鼠是研究人类疾病和毒理学的首要模型系统。我们使用最先进的策略,从鼠 Hmox1 基因座表达了多个互补的报告分子,包括萤火虫荧光素酶,以实现 Hmox1 表达的长期、非侵入性成像,以及β-半乳糖苷酶,以实现死后表达模式的高分辨率映射。我们通过确认报告基因表达的保真度及其对氧化和炎症刺激的反应性来验证该模型。除了为小鼠提供 Hmox1 表达的蓝图,提供新的生物学见解外,这项工作还为广泛应用该模型建立内源性过程和暴露于药物和环境因素引起的细胞应激铺平了道路。它还将使研究氧化应激在疾病发病机制及其预防中的作用成为可能。
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