Current developments in modelling the tumour microenvironment in vitro: Incorporation of biochemical and physical gradients

Monieb A.M. Ahmed, Anika Nagelkerke
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引用次数: 5

Abstract

Tumour cell proliferation, metabolism and treatment response depend on the dynamic interaction of the tumour cells with other cellular components and physicochemical gradients present in the tumour microenvironment. Traditional experimental approaches used to investigate the dynamic tumour tissue face a number of limitations, such as lack of biological relevance for the tumour microenvironment and the difficulty to precisely control fluctuating internal conditions, for example in oxygen and nutrients. The arrival of advanced in vitro models represents an alternative approach for modelling the tumour microenvironment using cutting-edge technologies, such as microfabrication. Advanced model systems provide a promising platform for modelling the physiochemical conditions of the tumour microenvironment in a well-controlled manner. Amongst others, advanced in vitro models aim to recreate gradients of oxygen, nutrients and endogenous chemokines, and cell proliferation. Furthermore, the establishment of mechanical cues within such models, e.g., flow and extracellular matrix properties that influence cellular behaviour, are active research areas. These model systems aim to maintain tumour cells in an environment that resembles in vivo conditions. A prominent example of such a system is the microfluidic tumour-on-chip model, which aims to precisely control the local chemical and physical environment that surrounds the tumour cells. In addition, these models also have the potential to recapitulate environmental conditions in isolation or in combination. This enables the analysis of the dynamic interactions between different conditions and their potentially synergistic effects on tumour cells. In this review, we will discuss the various gradients present within the tumour microenvironment and the effects they exert on tumour cells. We will further highlight the challenges and limitations of traditional experimental models in modelling these gradients. We will outline recent achievements in advanced in vitro models with a particular focus on tumour-on-chip systems. We will also discuss the future of these models in cancer research and their contribution to developing more biologically relevant models for cancer research.

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体外肿瘤微环境建模的最新进展:生化和物理梯度的结合
肿瘤细胞的增殖、代谢和治疗反应取决于肿瘤细胞与肿瘤微环境中其他细胞成分和物理化学梯度的动态相互作用。用于研究动态肿瘤组织的传统实验方法面临许多限制,例如缺乏与肿瘤微环境的生物学相关性以及难以精确控制波动的内部条件,例如氧气和营养物质。先进的体外模型的到来代表了使用尖端技术(如微加工)模拟肿瘤微环境的另一种方法。先进的模型系统为以良好控制的方式模拟肿瘤微环境的物理化学条件提供了一个有前途的平台。其中,先进的体外模型旨在重建氧气、营养物质和内源性趋化因子的梯度,以及细胞增殖。此外,在这些模型中建立机械线索,例如影响细胞行为的流动和细胞外基质特性,是活跃的研究领域。这些模型系统旨在将肿瘤细胞维持在类似于体内条件的环境中。这种系统的一个突出例子是微流控肿瘤芯片模型,其目的是精确控制肿瘤细胞周围的局部化学和物理环境。此外,这些模型还具有单独或组合地概括环境条件的潜力。这使得分析不同条件之间的动态相互作用及其对肿瘤细胞的潜在协同作用成为可能。在这篇综述中,我们将讨论肿瘤微环境中存在的各种梯度及其对肿瘤细胞的影响。我们将进一步强调传统实验模型在模拟这些梯度方面的挑战和局限性。我们将概述最近在先进的体外模型中取得的成就,特别关注肿瘤芯片系统。我们还将讨论这些模型在癌症研究中的未来,以及它们对开发更多与癌症研究相关的生物学模型的贡献。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Organs-on-a-chip
Organs-on-a-chip Analytical Chemistry, Biochemistry, Genetics and Molecular Biology (General), Cell Biology, Pharmacology, Toxicology and Pharmaceutics (General)
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审稿时长
125 days
期刊最新文献
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