Multiscale Anisotropic Scaffold Integrating 3D Printing and Electrospinning Techniques as a Heart‐on‐a‐Chip Platform for Evaluating Drug‐Induced Cardiotoxicity

Author:

Liu Sitian1,Wang Zihan12,Chen Xinyi1,Han Mingying3,Xu Jie3,Li Ting1,Yu Liu1,Qin Maoyu1,Long Meng1,Li Mingchuan4,Zhang Hongwu1,Li Yanbing1,Wang Ling3ORCID,Huang Wenhua1,Wu Yaobin1ORCID

Affiliation:

1. Guangdong Engineering Research Center for Translation of Medical 3D Printing Application Guangdong Provincial Key Laboratory of Digital Medicine and Biomechanics Department of Human Anatomy School of Basic Medical Sciences Southern Medical University Guangzhou 510515 China

2. Department of General Surgery Nanfang Hospital Southern Medical University Guangzhou 510515 China

3. Biomaterials Research Center School of Biomedical Engineering Southern Medical University Guangzhou 510515 China

4. Affiliated Cancer Hospital and Institute of Guangzhou Medical University Guangzhou 510095 China

Abstract

AbstractCardiac safety assessments are significant in drug discovery, as drug‐induced cardiotoxicity (DIC) is the primary cause of drug attrition. Despite heart‐on‐a‐chip (HoC) technology becoming an increasingly popular tool for evaluating DIC, its development remains a challenge owing to the anisotropic cardiac structure of the native myocardium. Herein, an anisotropic multiscale cardiac scaffold is presented via a hybrid biofabrication method by combining 3D printing with electrospinning technology, where the 3D‐printed micrometer‐scale scaffold frames enable mimicking the interwoven myocardium anatomical structure and the branched‐aligned electrospun nanofibers network is able to directionally guide cellular arrangements. The in vitro 3D bioengineered cardiac tissues are then fabricated by encapsulating three‐layer multiscale scaffolds within a photocurable methacrylated gelatin hydrogel shell. It is demonstrated that such an anisotropic multiscale structure could contribute to enhancing cardiomyocyte maturation and synchronous beating behavior. More attractively, with the integration of 3D bioengineered cardiac tissues and a self‐designed microfluidic perfusion system, a 3D anisotropic HoC platform is established for evaluating DIC and cardioprotective efficacy. Collectively, these results indicate that the HoC model developed by integrating the 3D bioengineered cardiac tissues could effectively recapitulate the clinical manifestations, thereby highlighting their efficacy as a valuable preclinical platform for testing drug efficacy and cardiotoxicity.

Funder

National Natural Science Foundation of China

Publisher

Wiley

Subject

Pharmaceutical Science,Biomedical Engineering,Biomaterials

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