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Experimental tuberculosis: the role of comparative pathology in the discovery of improved tuberculosis treatment strategies.

机译:实验性结核病:比较病理学在发现改进的结核病治疗策略中的作用。

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The use of laboratory animals is critical to the discovery and in vivo pre-clinical testing of new drugs and drug combinations for use in humans. M. tuberculosis infection of mice, rats, guinea pigs, rabbits and non-human primates are the most commonly used animal models of human tuberculosis. While granulomatous inflammation characterizes the most fundamental host response to M. tuberculosis aerosol infection in humans and animals, there are important species differences in pulmonary and extra-pulmonary lesion morphology which may influence responses to drug therapy. Lesions that progress to necrosis or cavitation are common, unfavorable host responses in naturally occurring tuberculosis of humans, but are not seen consistently in experimental infections in most animal model species. The importance of these unique lesion morphologies is that they represent irreversible tissue damage that can harbor persistent bacilli which are difficult to treat with standard therapies. Understanding the differences in host response to experimental tuberculosis infections may aid in selecting the most appropriate animal models to test drugs that have been rationally designed to have specific mechanisms of action in vivo. A better understanding of lesion pathogenesis across species may also aid in the identification of novel therapeutic targets or strategies that can be used alone or in combination with more conventional tuberculosis treatments in humans.
机译:实验动物的使用对于发现用于人类的新药物和药物组合以及进行体内临床前测试至关重要。小鼠,大鼠,豚鼠,兔子和非人类灵长类动物的结核分枝杆菌感染是人类结核病最常用的动物模型。虽然肉芽肿性炎症是人类和动物对结核分枝杆菌气溶胶感染最基本的宿主反应特征,但肺部和肺外病变形态存在重要的物种差异,这可能会影响对药物治疗的反应。在人类自然发生的结核病中,进展为坏死或空化的病变是常见的,不利的宿主反应,但在大多数动物模型物种的实验性感染中均未见到。这些独特的病变形态的重要性在于,它们代表了不可逆的组织损伤,可以保留持续的细菌,而这些细菌很难用标准疗法治疗。了解宿主对实验性结核感染的反应差异可能有助于选择最合适的动物模型来测试经过合理设计以具有体内特定作用机制的药物。更好地了解跨物种的病变发病机理,也可能有助于确定可以单独使用或与人类更常规的结核病治疗结合使用的新型治疗靶标或策略。

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