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用于药物输送系统评估的血管化肿瘤模型:范式转变。

Vascularized tumor models for the evaluation of drug delivery systems: a paradigm shift.

机构信息

Laboratoire Physico Chimie Curie, PCC, CNRS UMR168, Institut Curie, Sorbonne University, PSL University, 75005, Paris, France.

Université Paris Cité, Université Sorbonne Paris Nord, LVTS Inserm U1148, 75018, Paris, France.

出版信息

Drug Deliv Transl Res. 2024 Aug;14(8):2216-2241. doi: 10.1007/s13346-024-01580-3. Epub 2024 Apr 15.

Abstract

As the conversion rate of preclinical studies for cancer treatment is low, user-friendly models that mimic the pathological microenvironment and drug intake with high throughput are scarce. Animal models are key, but an alternative to reduce their use would be valuable. Vascularized tumor-on-chip models combine great versatility with scalable throughput and are easy to use. Several strategies to integrate both tumor and vascular compartments have been developed, but few have been used to assess drug delivery. Permeability, intra/extravasation, and free drug circulation are often evaluated, but imperfectly recapitulate the processes at stake. Indeed, tumor targeting and chemoresistance bypass must be investigated to design promising cancer therapeutics. In vitro models that would help the development of drug delivery systems (DDS) are thus needed. They would allow selecting good candidates before animal studies based on rational criteria such as drug accumulation, diffusion in the tumor, and potency, as well as absence of side damage. In this review, we focus on vascularized tumor models. First, we detail their fabrication, and especially the materials, cell types, and coculture used. Then, the different strategies of vascularization are described along with their classical applications in intra/extravasation or free drug assessment. Finally, current trends in DDS for cancer are discussed with an overview of the current efforts in the domain.

摘要

由于癌症治疗的临床前研究转化率较低,因此缺乏能够高通量模拟病理微环境和药物摄入的用户友好型模型。动物模型是关键,但如果能够找到替代方法来减少其使用,将会非常有价值。血管化肿瘤芯片模型结合了多功能性和可扩展性,并且易于使用。已经开发了几种将肿瘤和血管隔室整合在一起的策略,但很少用于评估药物输送。通常会评估通透性、细胞内/细胞外渗和游离药物循环,但这些方法并不能完美地重现相关过程。实际上,为了设计有前途的癌症治疗方法,必须研究肿瘤靶向和化疗耐药性规避。因此,需要开发有助于药物输送系统 (DDS) 发展的体外模型。这些模型可以根据药物积累、在肿瘤中的扩散和效力以及无副作用等合理标准,在动物研究之前筛选出良好的候选药物。在这篇综述中,我们重点介绍了血管化肿瘤模型。首先,我们详细介绍了它们的制造方法,特别是所用的材料、细胞类型和共培养物。然后,描述了不同的血管化策略,以及它们在细胞内/细胞外渗或游离药物评估中的经典应用。最后,讨论了癌症 DDS 的当前趋势,并概述了该领域的当前努力。

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