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      3D Spatiotemporal Mechanical Microenvironment: A Hydrogel-Based Platform for Guiding Stem Cell Fate

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          Mechanical forces direct stem cell behaviour in development and regeneration

          Stem cells and their local microenvironment, or niche, communicate through mechanical cues to regulate cell fate and cell behaviour and to guide developmental processes. During embryonic development, mechanical forces are involved in patterning and organogenesis. The physical environment of pluripotent stem cells regulates their self-renewal and differentiation. Mechanical and physical cues are also important in adult tissues, where adult stem cells require physical interactions with the extracellular matrix to maintain their potency. In vitro, synthetic models of the stem cell niche can be used to precisely control and manipulate the biophysical and biochemical properties of the stem cell microenvironment and to examine how the mode and magnitude of mechanical cues, such as matrix stiffness or applied forces, direct stem cell differentiation and function. Fundamental insights into the mechanobiology of stem cells also inform the design of artificial niches to support stem cells for regenerative therapies.
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            Designing cell-compatible hydrogels for biomedical applications.

            Hydrogels are polymeric materials distinguished by high water content and diverse physical properties. They can be engineered to resemble the extracellular environment of the body's tissues in ways that enable their use in medical implants, biosensors, and drug-delivery devices. Cell-compatible hydrogels are designed by using a strategy of coordinated control over physical properties and bioactivity to influence specific interactions with cellular systems, including spatial and temporal patterns of biochemical and biomechanical cues known to modulate cell behavior. Important new discoveries in stem cell research, cancer biology, and cellular morphogenesis have been realized with model hydrogel systems premised on these designs. Basic and clinical applications for hydrogels in cell therapy, tissue engineering, and biomedical research continue to drive design improvements using performance-based materials engineering paradigms.
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              Human breast cancer invasion and aggression correlates with ECM stiffening and immune cell infiltration.

              Tumors are stiff and data suggest that the extracellular matrix stiffening that correlates with experimental mammary malignancy drives tumor invasion and metastasis. Nevertheless, the relationship between tissue and extracellular matrix stiffness and human breast cancer progression and aggression remains unclear. We undertook a biophysical and biochemical assessment of stromal-epithelial interactions in noninvasive, invasive and normal adjacent human breast tissue and in breast cancers of increasingly aggressive subtype. Our analysis revealed that human breast cancer transformation is accompanied by an incremental increase in collagen deposition and a progressive linearization and thickening of interstitial collagen. The linearization of collagen was visualized as an overall increase in tissue birefringence and was most striking at the invasive front of the tumor where the stiffness of the stroma and cellular mechanosignaling were the highest. Amongst breast cancer subtypes we found that the stroma at the invasive region of the more aggressive Basal-like and Her2 tumor subtypes was the most heterogeneous and the stiffest when compared to the less aggressive luminal A and B subtypes. Intriguingly, we quantified the greatest number of infiltrating macrophages and the highest level of TGF beta signaling within the cells at the invasive front. We also established that stroma stiffness and the level of cellular TGF beta signaling positively correlated with each other and with the number of infiltrating tumor-activated macrophages, which was highest in the more aggressive tumor subtypes. These findings indicate that human breast cancer progression and aggression, collagen linearization and stromal stiffening are linked and implicate tissue inflammation and TGF beta.
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                Author and article information

                Journal
                Advanced Materials
                Adv. Mater.
                Wiley
                09359648
                December 2018
                December 2018
                July 31 2018
                : 30
                : 49
                : 1705911
                Affiliations
                [1 ]The Key Laboratory of Biomedical Information Engineering of Ministry of Education; School of Life Science and Technology; Xi'an Jiaotong University; Xi'an 710049 P. R. China
                [2 ]Bioinspired Engineering and Biomechanics Center (BEBC); Xi'an Jiaotong University; Xi'an 710049 P. R. China
                [3 ]State Key Laboratory for Diagnosis and Treatment of Infectious Diseases; First Affiliated Hospital; College of Medicine; Zhejiang University; Hangzhou Zhejiang Province 310003 P. R. China
                [4 ]Collaborative Innovation Center for Diagnosis and Treatment of Infectious Diseases; Hangzhou Zhejiang Province 310003 P. R. China
                [5 ]Institute for Translational Medicine; Zhejiang University; Hangzhou Zhejiang Province 310029 P. R. China
                [6 ]Department of Gynaecology and Obstetrics; First Hospital of Xi'an Jiaotong University; Xi'an 710061 P. R. China
                [7 ]MOE Key Laboratory for Multifunctional Materials and Structures; Xi'an Jiaotong University; Xi'an 710049 P. R. China
                Article
                10.1002/adma.201705911
                30063260
                8ab272a1-b471-4f1e-87bd-94ee120bfa9d
                © 2018

                http://doi.wiley.com/10.1002/tdm_license_1.1

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