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Animal models of scleroderma: recent progress

机译:硬皮动物模型:最新进展

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Purpose of reviewWe discuss recent advances in evaluating and optimizing animal models of systemic sclerosis (SSc). Such models could be of value for illuminating etiopathogenesis using hypothesis-testing experimental approaches, for developing effective disease-modifying therapies, and for uncovering clinically relevant biomarkers.Recent findingsWe describe recent advances in previously reported and novel animal models of SSc. The limitations of each animal model and their ability to recapitulate the pathophysiology of recognized molecular subsets of SSc are discussed. We highlight attrition of dermal white adipose tissue as a consistent pathological feature of dermal fibrosis in mouse models, and its relevance to SSc-associated cutaneous fibrosis.SummarySeveral animal models potentially useful for studying SSc pathogenesis have been described. Recent studies highlight particular strengths and weaknesses of selected models in recapitulating distinct features of the human disease. When used in the appropriate experimental setting, and in combination, these models singly and together provide a powerful set of in-vivo tools to define underlying mechanisms of disease and to develop and evaluate effective antifibrotic therapies.
机译:审查的目的我们讨论评估和优化系统性硬化症(SSc)动物模型的最新进展。这样的模型对于使用假设检验实验方法阐明病因,开发有效的疾病缓解疗法以及发现临床相关生物标志物可能具有价值。最新发现我们描述了先前报道的和新颖的SSc动物模型的最新进展。讨论了每种动物模型的局限性及其概括SSc公认分子亚群的病理生理的能力。我们重点研究了皮肤白脂肪组织的损耗,这是小鼠模型中皮肤纤维化的一致病理特征,并且与SSc相关的皮肤纤维化具有相关性。概述已描述了一些可能用于研究SSc发病机理的动物模型。最近的研究突出了所选模型在概括人类疾病独特特征方面的特殊优缺点。当在适当的实验环境中结合使用时,这些模型可以单独或共同提供一组强大的体内工具,以定义疾病的潜在机制以及开发和评估有效的抗纤维化疗法。

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