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念珠菌病的动物模型。

Animal models of candidiasis.

作者信息

Clancy Cornelius J, Cheng Shaoji, Nguyen Minh Hong

机构信息

University of Florida College of Medicine and North Florida/South Georgia Veterans Health System, Gainsville, FL, USA.

出版信息

Methods Mol Biol. 2009;499:65-76. doi: 10.1007/978-1-60327-151-6_8.

Abstract

Animal models are powerful tools to study the pathogenesis of diverse types of candidiasis. Murine models are particularly attractive because of cost, ease of handling, technical feasibility, and experience with their use. In this chapter, we describe methods for two of the most popular murine models of disease caused by Candida albicans. In an intravenously disseminated candidiasis (DC) model, immunocompetent mice are infected by lateral tail vein injections of a C. albicans suspension. Endpoints include mortality, tissue burdens of infection (most importantly in the kidneys, although spleens and livers are sometimes also assessed), and histopathology of infected organs. In a model of oral/esophageal candidiasis, mice are immunosuppressed with cortisone acetate and inoculated in the oral cavities using swabs saturated with a C. albicans suspension. Since mice do not die from oral candidiasis in this model, endpoints are tissue burden of infection and histopathology. The DC and oral/esophageal models are most commonly used for studies of C. albicans virulence, in which the disease-causing ability of a mutant strain is compared with an isogenic parent strain. Nevertheless, the basic techniques we describe are also applicable to models adapted to investigate other aspects of pathogenesis, such as spatiotemporal patterns of gene expression, specific aspects of host immune response and assessment of antifungal agents, immunomodulatory strategies, and vaccines.

摘要

动物模型是研究多种念珠菌病发病机制的有力工具。由于成本、易于操作、技术可行性以及使用经验等因素,小鼠模型特别具有吸引力。在本章中,我们描述了两种由白色念珠菌引起的最常用小鼠疾病模型的方法。在静脉播散性念珠菌病(DC)模型中,通过向侧尾静脉注射白色念珠菌悬液来感染免疫功能正常的小鼠。观察指标包括死亡率、感染的组织负荷(最重要的是在肾脏,尽管有时也评估脾脏和肝脏)以及感染器官的组织病理学。在口腔/食管念珠菌病模型中,用醋酸可的松对小鼠进行免疫抑制,并用饱和了白色念珠菌悬液的拭子在口腔中接种。由于在该模型中小鼠不会死于口腔念珠菌病,观察指标为感染的组织负荷和组织病理学。DC模型和口腔/食管模型最常用于白色念珠菌毒力研究,即将突变株的致病能力与同基因亲本菌株进行比较。然而,我们描述的基本技术也适用于为研究发病机制其他方面而改编的模型,例如基因表达的时空模式、宿主免疫反应的特定方面以及抗真菌药物、免疫调节策略和疫苗的评估。

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