Graphene Oxide-A Tool for the Preparation of Chemically Crosslinking Free Alginate-Chitosan-Collagen Scaffolds for Bone Tissue Engineering

Elayaraja Kolanthai; Pugazhendhi Abinaya Sindu; Deepak Kumar Khajuria; Sarath Chandra Veerla; Dhandapani Kuppuswamy; Luiz Henrique Catalani; D Roy Mahapatra

doi:10.1021/acsami.8b00699

Graphene Oxide-A Tool for the Preparation of Chemically Crosslinking Free Alginate-Chitosan-Collagen Scaffolds for Bone Tissue Engineering

ACS Appl Mater Interfaces. 2018 Apr 18;10(15):12441-12452. doi: 10.1021/acsami.8b00699. Epub 2018 Apr 9.

Authors

Elayaraja Kolanthai^{1

2}, Pugazhendhi Abinaya Sindu³, Deepak Kumar Khajuria¹, Sarath Chandra Veerla¹, Dhandapani Kuppuswamy⁴, Luiz Henrique Catalani², D Roy Mahapatra¹

Affiliations

¹ Laboratory for Integrative Multiscale Engineering Materials and Systems, Department of Aerospace Engineering , Indian Institute of Science , Bangalore 560012 , India.
² Departamento de Química Fundamental, Instituto de Química , Universityof São Paulo , Av. Prof. LineuPrestes, 784 , 05508-000 São Paulo , Brazil.
³ Centre for Biotechnology , Anna University , Chennai 600 025 , India.
⁴ Cardiology Division, Department of Medicine, Gazes Cardiac Research Institute , Medical University of South Carolina , Charleston , South Carolina 29425-2221 , United States.

PMID: 29589895
DOI: 10.1021/acsami.8b00699

Abstract

Developing a biodegradable scaffold remains a major challenge in bone tissue engineering. This study was aimed at developing novel alginate-chitosan-collagen (SA-CS-Col)-based composite scaffolds consisting of graphene oxide (GO) to enrich porous structures, elicited by the freeze-drying technique. To characterize porosity, water absorption, and compressive modulus, GO scaffolds (SA-CS-Col-GO) were prepared with and without Ca²⁺-mediated crosslinking (chemical crosslinking) and analyzed using Raman, Fourier transform infrared (FTIR), X-ray diffraction (XRD), and scanning electron microscopy techniques. The incorporation of GO into the SA-CS-Col matrix increased both crosslinking density as indicated by the reduction of crystalline peaks in the XRD patterns and polyelectrolyte ion complex as confirmed by FTIR. GO scaffolds showed increased mechanical properties which were further increased for chemically crosslinked scaffolds. All scaffolds exhibited interconnected pores of 10-250 μm range. By increasing the crosslinking density with Ca²⁺, a decrease in the porosity/swelling ratio was observed. Moreover, the SA-CS-Col-GO scaffold with or without chemical crosslinking was more stable as compared to SA-CS or SA-CS-Col scaffolds when placed in aqueous solution. To perform in vitro biochemical studies, mouse osteoblast cells were grown on various scaffolds and evaluated for cell proliferation by using MTT assay and mineralization and differentiation by alizarin red S staining. These measurements showed a significant increase for cells attached to the SA-CS-Col-GO scaffold compared to SA-CS or SA-CS-Col composites. However, chemical crosslinking of SA-CS-Col-GO showed no effect on the osteogenic ability of osteoblasts. These studies indicate the potential use of GO to prepare free SA-CS-Col scaffolds with preserved porous structure with elongated Col fibrils and that these composites, which are biocompatible and stable in a biological medium, could be used for application in engineering bone tissues.

Keywords: alginate; bone tissue engineering; chitosan; collagen; graphene oxide; hydrogel.

MeSH terms

Alginic Acid
Animals
Biocompatible Materials
Cell Proliferation
Chitosan
Collagen
Graphite / chemistry*
Mice
Porosity
Tissue Engineering
Tissue Scaffolds

Substances

Biocompatible Materials
graphene oxide
Graphite
Alginic Acid
Collagen
Chitosan