4.8 Article

In vitro myogenesis induced by human recombinant elastin-like proteins

Journal

BIOMATERIALS
Volume 67, Issue -, Pages 240-253

Publisher

ELSEVIER SCI LTD
DOI: 10.1016/j.biomaterials.2015.07.041

Keywords

Elastin-like polypeptides; Biomimetic materials; Cell adhesion; Skeletal muscle regeneration; Excitation-contraction coupling; Intracellular calcium

Funding

  1. European Regional Development Fund [CB 101]
  2. Universita degli Studi di Trieste (Finanziamento di Ateneo per progetti di ricerca scientifica - FRA)
  3. Beneficentia Stiftung, Vaduz, Lichtenstein [BEN 2014/125]

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Mammalian adult skeletal muscle has a limited ability to regenerate after injury, usage or trauma. A promising strategy for successful regenerative technology is the engineering of bio interfaces that mimic the characteristics of the extracellular matrix. Human elastin-like polypeptides (HELPs) have been synthesized as biomimetic materials that maintain some peculiar properties of the native protein. We developed a novel Human Elastin Like Polypeptide obtained by fusing the elastin-like backbone to a domain present in the alpha 2 chain of type IV collagen, containing two RGD motives. We employed this peptide as adhesion substrate for C2C12 myoblasts and compared its effects to those induced by two other polypeptides of the HELP series. Myoblast adhered to all HELPs coatings, where they assumed morphology and cytoarchitecture that depended on the polypeptide structure. Adhesion to HELPs stimulated at a different extent cell proliferation and differentiation, the expression of Myosin Heavy Chain and the fusion of aligned fibers into multinucleated myotubes. Adhesion substrates significantly altered myotubes stiffness, measured by Atomic Force Microscopy, and differently affected the cells Ca2+ handling capacity and the maturation of excitation-contraction coupling machinery, evaluated by Ca2+ imaging. Overall, our findings indicate that the properties of HELP biopolymers can be exploited for dissecting the molecular connections underlying myogenic differentiation and for designing novel substrates for skeletal muscle regeneration. (C) 2015 Elsevier Ltd. All rights reserved.

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