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用于疾病建模和监测癌症化疗引起的心脏毒性的心脏-乳腺癌芯片平台。

A Heart-Breast Cancer-on-a-Chip Platform for Disease Modeling and Monitoring of Cardiotoxicity Induced by Cancer Chemotherapy.

机构信息

Division of Engineering in Medicine, Brigham and Women's Hospital, Department of Medicine, Harvard Medical School, Cambridge, MA, 02139, USA.

Harvard-MIT Division of Health Sciences and Technology Massachusetts Institute of Technology, Cambridge, MA, 02139, USA.

出版信息

Small. 2021 Apr;17(15):e2004258. doi: 10.1002/smll.202004258. Epub 2020 Oct 23.

Abstract

Cardiotoxicity is one of the most serious side effects of cancer chemotherapy. Current approaches to monitoring of chemotherapy-induced cardiotoxicity (CIC) as well as model systems that develop in vivo or in vitro CIC platforms fail to notice early signs of CIC. Moreover, breast cancer (BC) patients with preexisting cardiac dysfunctions may lead to different incident levels of CIC. Here, a model is presented for investigating CIC where not only induced pluripotent stem cell (iPSC)-derived cardiac tissues are interacted with BC tissues on a dual-organ platform, but electrochemical immuno-aptasensors can also monitor cell-secreted multiple biomarkers. Fibrotic stages of iPSC-derived cardiac tissues are promoted with a supplement of transforming growth factor-β 1 to assess the differential functionality in healthy and fibrotic cardiac tissues after treatment with doxorubicin (DOX). The production trend of biomarkers evaluated by using the immuno-aptasensors well-matches the outcomes from conventional enzyme-linked immunosorbent assay, demonstrating the accuracy of the authors' sensing platform with much higher sensitivity and lower detection limits for early monitoring of CIC and BC progression. Furthermore, the versatility of this platform is demonstrated by applying a nanoparticle-based DOX-delivery system. The proposed platform would potentially help allow early detection and prediction of CIC in individual patients in the future.

摘要

心脏毒性是癌症化疗最严重的副作用之一。目前用于监测化疗诱导的心脏毒性(CIC)的方法以及体内或体外开发的模型系统都无法注意到 CIC 的早期迹象。此外,患有先前存在的心脏功能障碍的乳腺癌(BC)患者可能导致不同水平的 CIC 事件。在这里,提出了一种用于研究 CIC 的模型,其中不仅将诱导多能干细胞(iPSC)衍生的心脏组织与 BC 组织在双器官平台上相互作用,而且电化学免疫适体传感器还可以监测细胞分泌的多种生物标志物。用转化生长因子-β 1补充物促进 iPSC 衍生的心脏组织的纤维化阶段,以评估在用多柔比星(DOX)治疗后健康和纤维化心脏组织的差异功能。使用免疫适体传感器评估的生物标志物的产生趋势与传统酶联免疫吸附测定的结果非常吻合,证明了作者的传感平台的准确性,其具有更高的灵敏度和更低的检测限,可用于早期监测 CIC 和 BC 的进展。此外,通过应用基于纳米颗粒的 DOX 递药系统证明了该平台的多功能性。该平台有可能有助于将来在个体患者中进行 CIC 的早期检测和预测。

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