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用于肝纤维化研究的动物模型。

Animal models for the study of hepatic fibrosis.

机构信息

Laboratoire d'Hépato-Gastro-Entérologie, Institut de Recherche Expérimentale et Clinique, Université catholique de Louvain, Brussels, Belgium.

出版信息

Best Pract Res Clin Gastroenterol. 2011 Apr;25(2):319-33. doi: 10.1016/j.bpg.2011.02.004.

Abstract

Animal models are being used for several decades to study fibrogenesis and to evaluate the anti-fibrotic potential of therapies and strategies. Although immensely valuable for our understanding of pathophysiological processes, they remain models and none of them reproduces a human disease. Each model (meaning stimulus, design, strain and species) displays specific characteristics in the nature of the pathogenesis, the topography and the evolution of fibrosis. We review here the most used as well as some newly described but potentially interesting models including models for studying biliary, immune, alcohol-induced, NASH-associated and viral fibrosis and provide insight on underlying disease processes and practical details. We attempted to delineate the benefits, advantages, limitations and drawbacks of those models. We also report the new opportunities provided by genetically engineered mice for tracking and manipulating cells that participate to fibrosis. Finally, we emphasize the importance of adapting study design to the question addressed.

摘要

几十年来,动物模型一直被用于研究纤维化,并评估治疗和策略的抗纤维化潜力。尽管它们对我们理解病理生理过程非常有价值,但它们仍然是模型,没有一个能够复制人类疾病。每个模型(指刺激、设计、品系和物种)在发病机制的性质、纤维化的分布和演变方面都表现出特定的特征。我们在这里回顾了最常用的以及一些新描述但可能有前途的模型,包括用于研究胆汁淤积性、免疫性、酒精诱导性、NASH 相关和病毒性纤维化的模型,并提供了对潜在疾病过程和实际细节的深入了解。我们试图描述这些模型的优势、优点、局限性和缺点。我们还报告了遗传工程小鼠在跟踪和操纵参与纤维化的细胞方面提供的新机会。最后,我们强调了根据所研究的问题调整研究设计的重要性。

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