4.7 Article

Deciphering the Mechanics of Cancer Spheroid Growth in 3D Environments through Microfluidics Driven Mechanical Actuation

期刊

ADVANCED HEALTHCARE MATERIALS
卷 12, 期 14, 页码 -

出版社

WILEY
DOI: 10.1002/adhm.202201842

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3D growth; cancer-on-chip; matrix remodeling; tumor progression

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This study develops a microfluidic platform to investigate the mechanical properties of tumor spheroids and their surrounding matrix simultaneously, revealing the mechanical interdependency between the two entities. For spheroids embedded within soft hydrogels, the Young's modulus of the matrix decreases, while spheroids within stiff hydrogels do not significantly affect the Young's modulus of the surrounding matrix.
Uncontrolled growth of tumor cells is a key contributor to cancer-associated mortalities. Tumor growth is a biomechanical process whereby the cancer cells displace the surrounding matrix that provides mechanical resistance to the growing cells. The process of tumor growth and remodeling is regulated by material properties of both the cancer cells and their surrounding matrix, yet the mechanical interdependency between the two entities is not well understood. Herein, this work develops a microfluidic platform that precisely positions tumor spheroids within a hydrogel and mechanically probes the growing spheroids and surrounding matrix simultaneously. By using hydrostatic pressure to deform the spheroid-laden hydrogel along with confocal imaging and finite element (FE) analysis, this work deduces the material properties of the spheroid and the matrix in situ. For spheroids embedded within soft hydrogels, decreases in the Young's modulus of the matrix are detected at discrete locations accompanied by localized tumor growth. Contrastingly, spheroids within stiff hydrogels do not significantly decrease the Young's modulus of the surrounding matrix, despite exhibiting growth. Spheroids in stiff matrices leverage their high bulk modulus to grow and display a uniform volumetric expansion. Collectively, a quantitative platform is established and new insights into tumor growth within a stiff 3D environment are provided.

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