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用于肿瘤转移和治疗靶点评估的个性化血管化肿瘤类器官芯片

Personalized Vascularized Tumor Organoid-on-a-Chip for Tumor Metastasis and Therapeutic Targeting Assessment.

作者信息

Du Yang, Wang Yi-Ran, Bao Qi-Yuan, Xu Xin-Xin, Xu Congling, Wang Shaoxuan, Liu Qi, Liu Fan, Zeng Yu-Lian, Wang Ya-Jun, Liu Wei, Liu Yixin, Yu Sai-Xi, Chen Yu-Chen, Wang Chen, Zhang Weibin, Gao Hai, Luo Hao, Liu Baohong, Jing Guangyin, Guo Ming, Chen Fei Xavier, Liu Yan-Jun

机构信息

Shanghai Xuhui Central Hospital, Zhongshan-Xuhui Hospital, Shanghai Key Laboratory of Medical Epigenetics, Institutes of Biomedical Sciences, Department of Chemistry, Fudan University, Shanghai, 200032, China.

Department of Orthopaedics, Ruijin Hospital, Shanghai Jiao Tong University School of Medicine, Shanghai, 200025, China.

出版信息

Adv Mater. 2025 Feb;37(6):e2412815. doi: 10.1002/adma.202412815. Epub 2024 Dec 26.

Abstract

While tumor organoids have revolutionized cancer research by recapitulating the cellular architecture and behaviors of real tumors in vitro, their lack of functional vasculature hinders their attainment of full physiological capabilities. Current efforts to vascularize organoids are struggling to achieve well-defined vascular networks, mimicking the intricate hierarchy observed in vivo, which restricts the physiological relevance particularly for studying tumor progression and response to therapies targeting the tumor vasculature. An innovative vascularized patient-derived tumor organoids (PDTOs)-on-a-chip with hierarchical, tumor-specific microvasculature is presented, providing a versatile platform to explore tumor-vascular dynamics and antivascular drug efficacy. It is found that highly metastatic tumor cells induced vessel angiogenesis and simultaneously migrated toward blood vessels via the Notch pathway. The evident association between the angiogenic and migratory capacities of PDTOs and their clinical metastatic outcomes underscores the potential of the innovative platform for evaluating tumor metastasis, thus offering valuable insights for clinical decision-making. Ultimately, the system represents a promising avenue for advancing the understanding of tumor metastasis and developing personalized treatment strategies based on patient-specific tumor characteristics.

摘要

虽然肿瘤类器官通过在体外重现真实肿瘤的细胞结构和行为,给癌症研究带来了变革,但其缺乏功能性脉管系统阻碍了其获得完整的生理功能。目前使类器官血管化的努力难以实现明确的血管网络,难以模拟体内观察到的复杂层级结构,这限制了其生理相关性,特别是在研究肿瘤进展以及对针对肿瘤脉管系统的疗法的反应方面。本文展示了一种具有层级化、肿瘤特异性微血管的创新型血管化患者来源肿瘤类器官芯片,为探索肿瘤-血管动态和抗血管药物疗效提供了一个通用平台。研究发现,高转移性肿瘤细胞诱导血管生成,并同时通过Notch通路向血管迁移。肿瘤类器官的血管生成和迁移能力与其临床转移结果之间的明显关联,凸显了这个创新平台在评估肿瘤转移方面的潜力,从而为临床决策提供有价值的见解。最终,该系统为深化对肿瘤转移的理解以及基于患者特异性肿瘤特征制定个性化治疗策略提供了一条有前景的途径。

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