Literature DB >> 22196970

Reprogramming cardiomyocyte mechanosensing by crosstalk between integrins and hyaluronic acid receptors.

Anant Chopra1, Victor Lin, Amanda McCollough, Sarah Atzet, Glenn D Prestwich, Andrew S Wechsler, Maria E Murray, Shaina A Oake, J Yasha Kresh, Paul A Janmey.   

Abstract

The elastic modulus of bioengineered materials has a strong influence on the phenotype of many cells including cardiomyocytes. On polyacrylamide (PAA) gels that are laminated with ligands for integrins, cardiac myocytes develop well organized sarcomeres only when cultured on substrates with elastic moduli in the range 10 kPa-30 kPa, near those of the healthy tissue. On stiffer substrates (>60 kPa) approximating the damaged heart, myocytes form stress fiber-like filament bundles but lack organized sarcomeres or an elongated shape. On soft (<1 kPa) PAA gels myocytes exhibit disorganized actin networks and sarcomeres. However, when the polyacrylamide matrix is replaced by hyaluronic acid (HA) as the gel network to which integrin ligands are attached, robust development of functional neonatal rat ventricular myocytes occurs on gels with elastic moduli of 200 Pa, a stiffness far below that of the neonatal heart and on which myocytes would be amorphous and dysfunctional when cultured on polyacrylamide-based gels. The HA matrix by itself is not adhesive for myocytes, and the myocyte phenotype depends on the type of integrin ligand that is incorporated within the HA gel, with fibronectin, gelatin, or fibrinogen being more effective than collagen I. These results show that HA alters the integrin-dependent stiffness response of cells in vitro and suggests that expression of HA within the extracellular matrix (ECM) in vivo might similarly alter the response of cells that bind the ECM through integrins. The integration of HA with integrin-specific ECM signaling proteins provides a rationale for engineering a new class of soft hybrid hydrogels that can be used in therapeutic strategies to reverse the remodeling of the injured myocardium. Copyright Â
© 2011 Elsevier Ltd. All rights reserved.

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Year:  2011        PMID: 22196970      PMCID: PMC3386849          DOI: 10.1016/j.jbiomech.2011.11.023

Source DB:  PubMed          Journal:  J Biomech        ISSN: 0021-9290            Impact factor:   2.712


  37 in total

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4.  Stiffness of the substrate influences the phenotype of embryonic chicken cardiac myocytes.

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Review 6.  Micromechanical regulation in cardiac myocytes and fibroblasts: implications for tissue remodeling.

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Authors:  Jeffrey G Jacot; Jody C Martin; Darlene L Hunt
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  30 in total

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2.  Contractility of single cardiomyocytes differentiated from pluripotent stem cells depends on physiological shape and substrate stiffness.

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Review 4.  The (dys)functional extracellular matrix.

Authors:  Benjamin R Freedman; Nathan D Bade; Corinne N Riggin; Sijia Zhang; Philip G Haines; Katy L Ong; Paul A Janmey
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Review 6.  Force measurement tools to explore cadherin mechanotransduction.

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Review 7.  Stiffness Sensing by Cells.

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8.  Soft Substrates Containing Hyaluronan Mimic the Effects of Increased Stiffness on Morphology, Motility, and Proliferation of Glioma Cells.

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Review 9.  Use of flow, electrical, and mechanical stimulation to promote engineering of striated muscles.

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Review 10.  From tissue mechanics to transcription factors.

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