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仿生心脏组织培养模型(CTCM),用于模拟心脏生理学和病理生理学的体外模型。

Biomimetic cardiac tissue culture model (CTCM) to emulate cardiac physiology and pathophysiology ex vivo.

机构信息

From the Institute of Molecular Cardiology, Department of Medicine, University of Louisville, Louisville, USA.

Department of Bioengineering, University of Louisville, Louisville, USA.

出版信息

Commun Biol. 2022 Sep 9;5(1):934. doi: 10.1038/s42003-022-03919-3.

Abstract

There is need for a reliable in vitro system that can accurately replicate the cardiac physiological environment for drug testing. The limited availability of human heart tissue culture systems has led to inaccurate interpretations of cardiac-related drug effects. Here, we developed a cardiac tissue culture model (CTCM) that can electro-mechanically stimulate heart slices with physiological stretches in systole and diastole during the cardiac cycle. After 12 days in culture, this approach partially improved the viability of heart slices but did not completely maintain their structural integrity. Therefore, following small molecule screening, we found that the incorporation of 100 nM tri-iodothyronine (T3) and 1 μM dexamethasone (Dex) into our culture media preserved the microscopic structure of the slices for 12 days. When combined with T3/Dex treatment, the CTCM system maintained the transcriptional profile, viability, metabolic activity, and structural integrity for 12 days at the same levels as the fresh heart tissue. Furthermore, overstretching the cardiac tissue induced cardiac hypertrophic signaling in culture, which provides a proof of concept for the ability of the CTCM to emulate cardiac stretch-induced hypertrophic conditions. In conclusion, CTCM can emulate cardiac physiology and pathophysiology in culture for an extended time, thereby enabling reliable drug screening.

摘要

需要有一种可靠的体外系统,可以准确复制心脏的生理环境,用于药物测试。由于人类心脏组织培养系统的可用性有限,导致对心脏相关药物作用的解释不准确。在这里,我们开发了一种心脏组织培养模型(CTCM),可以在心脏周期的收缩和舒张期间对心脏切片进行电机械刺激,实现生理拉伸。在培养 12 天后,这种方法部分提高了心脏切片的活力,但并未完全维持其结构完整性。因此,在进行小分子筛选后,我们发现将 100nM 三碘甲状腺原氨酸(T3)和 1μM 地塞米松(Dex)掺入我们的培养基中,可以在 12 天内保持切片的微观结构。当与 T3/Dex 处理结合使用时,CTCM 系统可以在 12 天内保持与新鲜心脏组织相同的转录谱、活力、代谢活性和结构完整性。此外,过度拉伸心脏组织会在培养中诱导心脏肥厚信号,这为 CTCM 模拟心脏拉伸诱导的肥厚条件的能力提供了概念验证。总之,CTCM 可以在培养中长期模拟心脏的生理和病理生理学,从而实现可靠的药物筛选。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4ca6/9463130/425b18bdcf2b/42003_2022_3919_Fig1_HTML.jpg

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