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基于芯片上肾单位模型研究人类肾脏(病理)生理学的系统评价。

A systematic review of kidney-on-a-chip-based models to study human renal (patho-)physiology.

机构信息

Department of Nephrology and Hypertension, UMC Utrecht, 3584CX Utrecht, The Netherlands.

esqLABS GmbH, 26683 Saterland, Germany.

出版信息

Dis Model Mech. 2023 Jun 1;16(6). doi: 10.1242/dmm.050113. Epub 2023 Jun 19.

Abstract

As kidney diseases affect ∼10% of the world population, understanding the underlying mechanisms and developing therapeutic interventions are of high importance. Although animal models have enhanced knowledge of disease mechanisms, human (patho-)physiology may not be adequately represented in animals. Developments in microfluidics and renal cell biology have enabled the development of dynamic models to study renal (patho-)physiology in vitro. Allowing inclusion of human cells and combining different organ models, such as kidney-on-a-chip (KoC) models, enable the refinement and reduction of animal experiments. We systematically reviewed the methodological quality, applicability and effectiveness of kidney-based (multi-)organ-on-a-chip models, and describe the state-of-the-art, strengths and limitations, and opportunities regarding basic research and implementation of these models. We conclude that KoC models have evolved to complex models capable of mimicking systemic (patho-)physiological processes. Commercial chips and human induced pluripotent stem cells and organoids are important for KoC models to study disease mechanisms and assess drug effects, even in a personalized manner. This contributes to the Reduction, Refinement and Replacement of animal models for kidney research. A lack of reporting of intra- and inter-laboratory reproducibility and translational capacity currently hampers implementation of these models.

摘要

由于肾脏疾病影响了全球约 10%的人口,因此了解其潜在机制并开发治疗干预措施非常重要。尽管动物模型增强了对疾病机制的了解,但动物可能无法充分代表人类(病理)生理学。微流控和肾细胞生物学的发展使动态模型得以开发,从而可以在体外研究肾脏(病理)生理学。这些模型允许纳入人类细胞并结合不同的器官模型,如肾芯片(KoC)模型,从而可以改进和减少动物实验。我们系统地回顾了基于肾脏的(多)器官芯片模型的方法学质量、适用性和有效性,并描述了这些模型在基础研究和实施方面的最新进展、优势和局限性以及机会。我们得出的结论是,KoC 模型已经发展成为能够模拟全身(病理)生理过程的复杂模型。商业芯片和人类诱导多能干细胞和类器官对于 KoC 模型研究疾病机制和评估药物作用非常重要,甚至可以实现个性化研究。这有助于减少、改进和替代肾脏研究的动物模型。目前,这些模型的报告缺乏关于实验室内部和实验室之间的可重复性和转化能力,这限制了它们的实施。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3df7/10309579/d08b7f6b9927/dmm-16-050113-g1.jpg

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