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使用独立应用程序的自动跟踪技术对人类工程3D心脏组织进行收缩性分析。

Contractility analysis of human engineered 3D heart tissues by an automatic tracking technique using a standalone application.

作者信息

Rivera-Arbeláez José M, Cofiño-Fabres Carla, Schwach Verena, Boonen Tom, Ten Den Simone A, Vermeul Kim, van den Berg Albert, Segerink Loes I, Ribeiro Marcelo C, Passier Robert

机构信息

Applied Stem Cell Technologies, TechMed Centre, University of Twente, Enschede, The Netherlands.

BIOS Lab-on-a-Chip Group, MESA+ Institute for Nanotechnology, Technical Medical Centre, Max Planck Center for Complex Fluid Dynamics, University of Twente, Enschede, The Netherlands.

出版信息

PLoS One. 2022 Apr 14;17(4):e0266834. doi: 10.1371/journal.pone.0266834. eCollection 2022.

Abstract

The use of Engineered Heart Tissues (EHT) as in vitro model for disease modeling and drug screening has increased, as they provide important insight into the genetic mechanisms, cardiac toxicity or drug responses. Consequently, this has highlighted the need for a standardized, unbiased, robust and automatic way to analyze hallmark physiological features of EHTs. In this study we described and validated a standalone application to analyze physiological features of EHTs in an automatic, robust, and unbiased way, using low computational time. The standalone application "EHT Analysis" contains two analysis modes (automatic and manual) to analyzes the contractile properties and the contraction kinetics of EHTs from high speed bright field videos. As output data, the graphs of displacement, contraction force and contraction kinetics per file will be generated together with the raw data. Additionally, it also generates a summary file containing all the data from the analyzed files, which facilitates and speeds up the post analysis. From our study we highlight the importance of analyzing the axial stress which is the force per surface area (μN/mm2). This allows to have a readout overtime of tissue compaction, axial stress and leave the option to calculate at the end point of an experiment the physiological cross-section area (PSCA). We demonstrated the utility of this tool by analyzing contractile properties and compaction over time of EHTs made out of a double reporter human pluripotent stem cell (hPSC) line (NKX2.5EGFP/+-COUP-TFIImCherry/+) and different ratios of human adult cardiac fibroblasts (HCF). Our standalone application "EHT Analysis" can be applied for different studies where the physiological features of EHTs needs to be analyzed under the effect of a drug compound or in a disease model.

摘要

工程心脏组织(EHT)作为疾病建模和药物筛选的体外模型的应用有所增加,因为它们能为遗传机制、心脏毒性或药物反应提供重要见解。因此,这凸显了对一种标准化、无偏倚、稳健且自动的方法来分析EHT标志性生理特征的需求。在本研究中,我们描述并验证了一个独立应用程序,该程序能以自动、稳健且无偏倚的方式,利用较短的计算时间来分析EHT的生理特征。独立应用程序“EHT分析”包含两种分析模式(自动和手动),用于从高速明场视频中分析EHT的收缩特性和收缩动力学。作为输出数据,将生成每个文件的位移、收缩力和收缩动力学的图表以及原始数据。此外,它还会生成一个包含所有分析文件数据的汇总文件,这有助于并加快后期分析。从我们的研究中,我们强调了分析轴向应力的重要性,轴向应力是每表面积的力(μN/mm²)。这使得能够随时间读出组织压实情况、轴向应力,并可选择在实验终点计算生理横截面积(PSCA)。我们通过分析由双报告人类多能干细胞(hPSC)系(NKX2.5EGFP/+-COUP-TFIImCherry/+)和不同比例的人类成年心脏成纤维细胞(HCF)制成的EHT的收缩特性和随时间的压实情况,证明了该工具的实用性。我们的独立应用程序“EHT分析”可应用于不同的研究,在这些研究中,需要在药物化合物的作用下或疾病模型中分析EHT的生理特征。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a990/9009597/51f072d7f7c7/pone.0266834.g001.jpg

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