Abstract
Diverse essential cellular behaviors are determined by extracellular physical cues that are detected by highly orchestrated subcellular interactions with the extracellular microenvironment. To maintain the reciprocity of cellular responses and mechanical properties of the extracellular matrix, cells utilize a variety of signaling pathways that transduce biophysical stimuli to biochemical reactions. Recent advances in the micromanipulation of individual cells have shown that cellular responses to distinct physical and chemical features of the material are fundamental determinants of cellular mechanosensation and mechanotransduction. In the process of outside-in signal transduction, transmembrane protein integrins facilitate the formation of focal adhesion protein clusters that are connected to the cytoskeletal architecture and anchor the cell to the substrate. The linkers of nucleoskeleton and cytoskeleton molecular complexes, collectively termed LINC, are critical signal transducers that relay biophysical signals between the extranuclear cytoplasmic region and intranuclear nucleoplasmic region. Mechanical signals that involve cytoskeletal remodeling ultimately propagate into the nuclear envelope comprising the nuclear lamina in assistance with various nuclear membrane proteins, where nuclear mechanics play a key role in the subsequent alteration of gene expression and epigenetic modification. These intracellular mechanical signaling cues adjust cellular behaviors directly associated with mechanohomeostasis. Diverse strategies to modulate cell-material interfaces, including alteration of surface rigidity, confinement of cell adhesive region, and changes in surface topology, have been proposed to identify cellular signal transduction at the cellular and subcellular levels. In this review, we will discuss how a diversity of alterations in the physical properties of materials induce distinct cellular responses such as adhesion, migration, proliferation, differentiation, and chromosomal organization. Furthermore, the pathological relevance of misregulated cellular mechanosensation and mechanotransduction in the progression of devastating human diseases, including cardiovascular diseases, cancer, and aging, will be extensively reviewed. Understanding cellular responses to various extracellular forces is expected to provide new insights into how cellular mechanoadaptation is modulated by manipulating the mechanics of extracellular matrix and the application of these materials in clinical aspects.
Highlights
Cells are surrounded by a complex microenvironment, and their essential functions are controlled by multiple interactions between cell-cell and cell-extracellular matrix (ECM) (Leiphart et al, 2019)
Disruption of actomyosin contractility of these cells inhibited the expression of lineage markers; alternative stem cell differentiation on varying substrate rigidity depends on nonmuscle myosin II (NMM II)-based cytoskeletal tension (Engler et al, 2006), which is determined by nuclear mechanosensation of substrate stiffness (Swift et al, 2013)
Modulating tissue geometry, stiffness, and biophysical properties results in the perception of different loads of mechanical signals from the microenvironment
Summary
Cells are surrounded by a complex microenvironment, and their essential functions are controlled by multiple interactions between cell-cell and cell-extracellular matrix (ECM) (Leiphart et al, 2019). In addition to chemical stimuli, various mechanical properties of the extracellular matrix (ECM) are involved in changes in cell behavior, including cell adhesion, migration, and differentiation through epigenetic modification (Jansen et al, 2015).
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