Dynamic optimisation for graded tissue scaffolds using machine learning techniques

Authors

Chi Wu, Faculty of Engineering
Boyang Wan, Faculty of Engineering
Yanan Xu, Faculty of Engineering
D. S.Abdullah Al Maruf, Integrated Prosthetics and Reconstruction
Kai Cheng, Royal Prince Alfred Hospital
William T. Lewin, Chris O'Brien Lifehouse
Jianguang Fang, University of Technology Sydney
Hai Xin, Integrated Prosthetics and Reconstruction
Jeremy M. Crook, Chris O'Brien Lifehouse
Jonathan R. Clark, Integrated Prosthetics and Reconstruction
Grant P. Steven, Faculty of Engineering
Qing Li, Faculty of Engineering

Publication Name

Computer Methods in Applied Mechanics and Engineering

Abstract

Tissue scaffolds have emerged as a promising solution for treatment of critical size bone defects, offering significant advantages over conventional strategies. One of the key functionalities of bone scaffolds is their ability to promote long-term bone ingrowth effectively. To enhance this functionality, we develop a novel dynamic optimisation framework to customise bone scaffolds for achieving maximum bone ingrowth outcomes over a certain period in this study. To improve the design efficiency, we extensively leverage machine learning (ML) techniques within our proposed dynamic optimisation framework. Specifically, two neural networks are integrated into a dynamic bone growth model, and another neural network is coupled with a genetic algorithm for dynamic optimisation process. To demonstrate the effectiveness and efficiency of the approach, we employ a sheep mandible reconstruction for treating a critical size bone defect as an illustraive example. To validate the finite element (FE) model established, we first conduct a mechanical test on the sheep mandible assembled with a tailored 3D printed scaffold made of Polyetherketone (PEK) material. Then, we compare three different optimisation schemes, namely uniform design, lateral gradient design, and vertical gradient design, with an empirical design under the same biomechanical conditions. A 18.5 % enhancement is found in the long-term bone ingrowth when the optimised scaffold is adopted in comparison with the empirical design, which is attributed to the fine-tuning of strut sizes within lattice scaffold structures for facilitating bone regeneration in the gradient regions. This study proposes a novel design framework by combining ML and time-dependent topology optimisation, which provides a new methodology for developing innovative tissue scaffolds with better clinical outcomes.

Open Access Status

This publication may be available as open access

Volume

425

Article Number

116911

Funding Number

2024602

Funding Sponsor

National Health and Medical Research Council