3D bioprinted microparticles: Optimizing loading efficiency using advanced DoE technique and machine learning modeling

Jiawei Wang; Niloofar Heshmati Aghda; Junhuang Jiang; Ayishah Mridula Habib; Defang Ouyang; Mohammed Maniruzzaman

doi:10.1016/j.ijpharm.2022.122302

3D bioprinted microparticles: Optimizing loading efficiency using advanced DoE technique and machine learning modeling

Int J Pharm. 2022 Nov 25:628:122302. doi: 10.1016/j.ijpharm.2022.122302. Epub 2022 Oct 17.

Authors

Jiawei Wang¹, Niloofar Heshmati Aghda¹, Junhuang Jiang², Ayishah Mridula Habib¹, Defang Ouyang³, Mohammed Maniruzzaman⁴

Affiliations

¹ Pharmaceutical Engineering and 3D Printing (PharmE3D) Lab, Division of Molecular Pharmaceutics and Drug Delivery, College of Pharmacy, The University of Texas at Austin, Austin, TX 78712, USA.
² Division of Molecular Pharmaceutics and Drug Delivery, College of Pharmacy, The University of Texas at Austin, TX 78712, USA.
³ State Key Laboratory of Quality Research in Chinese Medicine, Institute of Chinese Medical Sciences, University of Macau, Macau 999078, China.
⁴ Pharmaceutical Engineering and 3D Printing (PharmE3D) Lab, Division of Molecular Pharmaceutics and Drug Delivery, College of Pharmacy, The University of Texas at Austin, Austin, TX 78712, USA. Electronic address: M.Maniruzzaman@austin.utexas.edu.

PMID: 36261096
DOI: 10.1016/j.ijpharm.2022.122302

Abstract

Current microparticle (MP) development still strongly relies on the laborious trial-and-error approach. Herein, we developed a systemic method to evaluate the significance of MP formulation factors and predict drug loading efficiency (DLE) using design of experiment (DoE) and machine learning modeling. A first-in-class 3D printing concept was initially employed to fabricate polymeric MPs by a 3D printer. Sprayed Multi Adsorbed-droplet Reposing Technology (SMART) was developed to combine extrusion-based printing with emulsion evaporation technique to fabricate a small molecule drug i.e., 6-thioguanine (6-TG) loaded poly (lactide-co-glycolide) (PLGA) MPs. Compared to conventional emulsion evaporation method, SMART employs the shear force exerted by the printing nozzle rather than the sonication energy to generate smaller emulsion droplets in a single step. Furthermore, the applied shear force in the 3D printing process reported herein is controllable since the emulsion is extruded through the nozzle under preset printing conditions. The formulated MPs exhibited spherical structure with size distribution ∼ 1-3μ m in diameter and reached ∼ 100 % drug release at 10 h. Also, the papain-like protease (PLpro) inhibition efficacy of 6-TG in formulated MPs was maintained even after the printing process under different printing conditions. Furthermore, the formulation factor importance was assessed by DoE statistical analysis and further validated by machine learning modeling. Among the four process parameters (drug amount, printing speed, printing pressure, and nozzle size), drug amount was the most influential formulation factor. Moreover, it is interesting that nearly all the machine learning models, especially decision tree (DT), demonstrated superior performance in predicting DLE compared to DoE regression models. Overall, incorporating DoE and machine learning modeling shows great promises in the prediction and optimization of MP formulations factors by means of a novel SMART technology. Moreover, this systemic approach helps streamline the development of MP with programmable pharmaceutical attributes, representing a new paradigm for digital pharmaceutical science.

Keywords: 3D printing; Design of experiment; Machine learning; Microparticle.

MeSH terms

Emulsions
Machine Learning
Polymers* / chemistry
Printing, Three-Dimensional*

Substances

Emulsions
Polymers

Grants and funding

R01 FD007456/FD/FDA HHS/United States