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三维解构信号传导

Deconstructing signaling in three dimensions.

作者信息

Rubashkin Matthew G, Ou Guanqing, Weaver Valerie M

机构信息

Joint Bioengineering Program, UC-Berkeley/UCSF, Center for Bioengineering and Tissue Regeneration, Department of Surgery, University of California, San Francisco , San Francisco, California 94143, United States.

出版信息

Biochemistry. 2014 Apr 8;53(13):2078-90. doi: 10.1021/bi401710d. Epub 2014 Mar 28.

Abstract

Cells in vivo exist within the context of a multicellular tissue, where their behavior is governed by homo- and heterotypic cell-cell interactions, the material properties of the extracellular matrix, and the distribution of various soluble and physical factors. Most methods currently used to study and manipulate cellular behavior in vitro, however, sacrifice physiological relevance for experimental expediency. The fallacy of such approaches has been highlighted by the recent development and application of three-dimensional culture models to cell biology, which has revealed striking phenotypic differences in cell survival, migration, and differentiation in genetically identical cells simply by varying culture conditions. These perplexing findings beg the question of what constitutes a three-dimensional culture and why cells behave so differently in two- and three-dimensional culture formats. In the following review, we dissect the fundamental differences between two- and three-dimensional culture conditions. We begin by establishing a basic definition of what "three dimensions" means at different biological scales and discuss how dimensionality influences cell signaling across different length scales. We identify which three-dimensional features most potently influence intracellular signaling and distinguish between conserved biological principles that are maintained across culture conditions and cellular behaviors that are sensitive to microenvironmental context. Finally, we highlight state-of-the-art molecular tools amenable to the study of signaling in three dimensions under conditions that facilitate deconstruction of signaling in a more physiologically relevant manner.

摘要

体内的细胞存在于多细胞组织的环境中,其行为受同型和异型细胞间相互作用、细胞外基质的材料特性以及各种可溶性和物理因子的分布所支配。然而,目前大多数用于体外研究和操纵细胞行为的方法,都为了实验的便利性而牺牲了生理相关性。三维培养模型在细胞生物学中的最新发展和应用凸显了此类方法的谬误,这表明仅仅通过改变培养条件,基因相同的细胞在细胞存活、迁移和分化方面就会表现出惊人的表型差异。这些令人困惑的发现引发了这样一个问题:什么构成了三维培养,以及为什么细胞在二维和三维培养形式中的行为会如此不同。在以下综述中,我们剖析二维和三维培养条件之间的根本差异。我们首先确立 “三维” 在不同生物学尺度上的基本定义,并讨论维度如何影响不同长度尺度上的细胞信号传导。我们确定哪些三维特征对细胞内信号传导影响最为显著,并区分在不同培养条件下保持不变的保守生物学原理和对微环境背景敏感的细胞行为。最后,我们重点介绍了一些先进的分子工具,这些工具适用于在便于以更符合生理相关性的方式解构信号传导的条件下研究三维信号传导。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f93b/3985742/aecbd3b92c80/bi-2013-01710d_0002.jpg

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