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Vascular calcification in animal models of CKD: A review.

机译:CKD动物模型中的血管钙化:综述。

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Vascular calcification is a significant contributor to the cardiovascular mortality observed in chronic kidney disease (CKD). This review discusses the animal models (5/6 nephrectomy, mouse electrocautery model and dietary adenine) that have been employed in the study of vascular calcification outcomes in CKD. Rodent models of CKD generate a range of severity in the vascular calcification phenotype. Major limitations of the 5/6th nephrectomy model include the requirement for surgery and the need to use either excessive dietary phosphorus or vitamin D. Major limitations of the mouse electrocautery model include the requirement for surgery, the mortality rate when very advanced CKD develops, and resistance to vascular calcification without the use of transgenic animals. This is balanced against the major advantage of the ability to study transgenic animals to further understand the mechanisms associated with either the acceleration or inhibition of calcification. Dietary adenine generates severe CKD and does not require surgery. The major disadvantage is the weight loss that ensues when rats receive a diet containing 0.75% adenine. In summary, animal models are useful to study CKD-associated vascular calcification and the results obtained in these pre-clinical animal studies appear to translate to the evidence, however limited, which exists in humans with CKD.
机译:血管钙化是慢性肾脏病(CKD)中观察到的心血管死亡率的重要因素。这篇综述讨论了已用于研究CKD血管钙化结局的动物模型(5/6肾切除术,小鼠电灼模型和饮食腺嘌呤)。 CKD的啮齿动物模型会在血管钙化表型中产生一系列严重性。第5/6号肾切除术模型的主要限制包括手术需求和使用过量的饮食中磷或维生素D的需求。小鼠电灼模型的主要限制包括手术需求,非常严重的CKD发生时的死亡率以及无需使用转基因动物即可抵抗血管钙化。这与研究转基因动物以进一步了解与加速或抑制钙化有关的机制的主要优势相平衡。膳食腺嘌呤会产生严重的CKD,不需要手术。主要的缺点是,当大鼠接受含有0.75%腺嘌呤的饮食时,体重会随之减轻。总而言之,动物模型可用于研究与CKD相关的血管钙化,并且在这些临床前动物研究中获得的结果似乎可以转化为证据,但仅限于患有CKD的人。

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