4.8 Article

Micropatterned gellan gum-based hydrogels tailored with laminin-derived peptides for skeletal muscle tissue engineering

Journal

BIOMATERIALS
Volume 279, Issue -, Pages -

Publisher

ELSEVIER SCI LTD
DOI: 10.1016/j.biomaterials.2021.121217

Keywords

Gellan gum; Micropattern; Peptide; Skeletal muscle; Tissue engineering

Funding

  1. Portuguese Foundation for Science and Technology (FCT) [FCT PD/BD/128090/2016, PD/59/2013, CEECIND/00352/2017]
  2. FCT Fundacao para a Ciencia e a Tecnologia, I.P.
  3. COMPETE 2020 FEDER funds, under the Scientific Employment Stimulus - Individual Call (CEEC Individual) [2020.01541.CEECIND/CP1600/CT0024]
  4. Programa Operacional Regional do Norte - FEDER [028070]
  5. EU Framework Programme for Research and Innovation H2020 on FoReCaST [668983]
  6. BREAST-IT FCT-Portugal project [PTDC/BTM-ORG/28168/2017]
  7. Fundação para a Ciência e a Tecnologia [2020.01541.CEECIND/CP1600/CT0024] Funding Source: FCT

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Current therapies for skeletal muscle disorders/injuries are limited, necessitating the development of new treatments. Skeletal muscle tissue engineered platforms could provide valuable insights into the pathophysiology of skeletal muscle disorders/injuries and the efficacy of new therapies.
The efficacy of current therapies for skeletal muscle disorders/injuries are limited urging the need for new treatments. Skeletal muscle tissue engineered platforms represent a promising tool to shed light on the pathophysiology of skeletal muscle disorders/injuries and to investigate the efficacy of new therapies. Herein, we developed a skeletal muscle platform composed of aligned and differentiated myoblasts on micropatterned gellan gum (GG)-based hydrogels tailored with a laminin-derived peptide. To this aim, the binding of murine skeletal muscle cells (C2C12) to different laminin-derived peptides (CIKVAVS (V), KNRLTIELEVRTC (T), and RKRLQVQLSIRTC (Q)) and the binding of laminin-derived peptides to chemically functionalized GG was studied. C2C12-binding to peptide V, T and Q was 10%, 48% and 25%, whereas the peptide tethering to GG was 60%, 40% and 31%, respectively. Peptide-biofunctionalized hydrogels prepared with different polymer content showed different mechanics and peptide exposure at hydrogel surface. Cellular adhesion was detected in all hydrogel formulations, but spreading and differentiation was only promoted in peptide Q-biofunctionalized hydrogels and preferably in stiffer hydrogels. Myoblast alignment was promoted in micropatterned hydrogel surfaces. Overall, the engineered skeletal muscle herein proposed can be further explored as a platform to better understand skeletal muscle disorders/injuries and to screen new therapies.

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