Design and 3D Printing of Personalized Hybrid and Gradient Structures for Critical Size Bone Defects

Mine Altunbek; Seyedeh Ferdows Afghah; Ali Fallah; Anil Ahmet Acar; Bahattin Koc

doi:10.1021/acsabm.3c00107

Design and 3D Printing of Personalized Hybrid and Gradient Structures for Critical Size Bone Defects

ACS Appl Bio Mater. 2023 May 15;6(5):1873-1885. doi: 10.1021/acsabm.3c00107. Epub 2023 Apr 18.

Authors

Mine Altunbek^{1

2}, Seyedeh Ferdows Afghah^{1

3}, Ali Fallah^{1

3

4}, Anil Ahmet Acar^{1

3}, Bahattin Koc^{1

3

4}

Affiliations

¹ Nanotechnology Research and Application Center, Sabanci University, Istanbul 34956, Turkey.
² University of Massachusetts Lowell, Lowell, Massachusetts 01854, United States.
³ Faculty of Engineering and Natural Sciences, Sabanci University, Istanbul 34956, Turkey.
⁴ Integrated Manufacturing Technologies Research and Application Center, Sabanci University, Istanbul 34906, Turkey.

Abstract

Treating critical-size bone defects with autografts, allografts, or standardized implants is challenging since the healing of the defect area necessitates patient-specific grafts with mechanically and physiologically relevant structures. Three-dimensional (3D) printing using computer-aided design (CAD) is a promising approach for bone tissue engineering applications by producing constructs with customized designs and biomechanical compositions. In this study, we propose 3D printing of personalized and implantable hybrid active scaffolds with a unique architecture and biomaterial composition for critical-size bone defects. The proposed 3D hybrid construct was designed to have a gradient cell-laden poly(ethylene glycol) (PEG) hydrogel, which was surrounded by a porous polycaprolactone (PCL) cage structure to recapitulate the anatomical structure of the defective area. The optimized PCL cage design not only provides improved mechanical properties but also allows the diffusion of nutrients and medium through the scaffold. Three different designs including zigzag, zigzag/spiral, and zigzag/spiral with shifting the zigzag layers were evaluated to find an optimal architecture from a mechanical point of view and permeability that can provide the necessary mechanical strength and oxygen/nutrient diffusion, respectively. Mechanical properties were investigated experimentally and analytically using finite element analysis (FEA), and computational fluid dynamics (CFD) simulation was used to determine the permeability of the structures. A hybrid scaffold was fabricated via 3D printing of the PCL cage structure and a PEG-based bioink comprising a varying number of human bone marrow mesenchymal stem cells (hBMSCs). The gradient bioink was deposited inside the PCL cage through a microcapillary extrusion to generate a mineralized gradient structure. The zigzag/spiral design for the PCL cage was found to be mechanically strong with sufficient and optimum nutrient/gas axial and radial diffusion while the PEG-based hydrogel provided a biocompatible environment for hBMSC viability, differentiation, and mineralization. This study promises the production of personalized constructs for critical-size bone defects by printing different biomaterials and gradient cells with a hybrid design depending on the need for a donor site for implantation.

Keywords: 3D printing; gradient structures; hybrid printing; large bone defects; personalized scaffolds.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Biocompatible Materials* / chemistry
Humans
Hydrogels / chemistry
Printing, Three-Dimensional
Tissue Engineering / methods
Tissue Scaffolds* / chemistry

Substances

Biocompatible Materials
Hydrogels