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在二维还是三维空间中进行组织培养?这就是问题所在。

To do tissue culture in two or three dimensions? That is the question.

作者信息

Hoffman R M

机构信息

AntiCancer, Inc., San Diego, California 92110.

出版信息

Stem Cells. 1993 Mar;11(2):105-11. doi: 10.1002/stem.5530110205.

Abstract

Alexis Carrel introduced the in vitro culture of tissues in the beginning of the century utilizing a culture system that allowed the three-dimensional growth of tissues. Leighton improved upon this system by developing a substrate of sponge matrices. Other methods of three-dimensional culture include collagen gels and what are known as organ culture systems on filters or meshes. In addition, cell suspensions can be converted into multicellular spheroids, another form of three-dimensional culture. Comparison of the three-dimensional culture methods with two-dimensional culture methods has shown critical differences in the behavior of biological systems in culture. For example, in vivo-like drug responses are observed in three-dimensional but frequently not in two-dimensional cultures, indicating that drug response may be a function of tissue architecture. The in vivo mechanism of drug resistance may involve alterations in cell-cell interaction which may occur in three-dimensional culture as opposed to monolayer culture. Practical applications of three-dimensional culture include the development of a drug-response assay that correlates not only with drug resistance but also with drug sensitivity and survival of cancer patients. It has been shown that gene expression may be more in vivo-like in three-dimensional cultures than in two-dimensional monolayer cultures. For example, tumor antigens may be expressed in three-dimensional culture and not in monolayer culture. Thus, future studies utilizing three-dimensional cultures may significantly enhance our understanding of gene expression and resistance to drugs and enhance the efficacy of cancer chemotherapy by correctly predicting active drug regimens for individual patients.

摘要

亚历克西斯·卡雷尔在本世纪初引入了组织的体外培养,他使用的培养系统能够使组织进行三维生长。莱顿对该系统进行了改进,开发出一种海绵基质底物。三维培养的其他方法包括胶原凝胶以及在滤膜或网片上的所谓器官培养系统。此外,细胞悬液可转化为多细胞球体,这是三维培养的另一种形式。将三维培养方法与二维培养方法进行比较后发现,培养中的生物系统行为存在关键差异。例如,在三维培养中可观察到类似体内的药物反应,但在二维培养中通常观察不到,这表明药物反应可能是组织结构的一种功能。体内耐药机制可能涉及细胞间相互作用的改变,这种改变可能发生在三维培养而非单层培养中。三维培养的实际应用包括开发一种药物反应检测方法,该方法不仅与耐药性相关,还与癌症患者的药物敏感性和生存率相关。研究表明,三维培养中的基因表达可能比二维单层培养更接近体内情况。例如,肿瘤抗原可能在三维培养中表达,而在单层培养中不表达。因此,未来利用三维培养进行的研究可能会显著增进我们对基因表达和耐药性的理解,并通过正确预测个体患者的有效药物方案来提高癌症化疗的疗效。

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