Preparation and characterization of immediate release 3D printed tablets using hot melt extruded amorphous cyclosporine a filament

被引:0
|
作者
Jeong, Jin-Hyuk [1 ]
Han, Chang-Soo [2 ]
Kang, Ji-Hyun [1 ,3 ,4 ]
Yoo, Kwang-Hwi [1 ]
Jung, Woong-Young [1 ]
Park, Yun-Sang [2 ]
Kim, Dong-Wook [5 ]
Park, Chun-Woong [1 ]
机构
[1] Chungbuk Natl Univ, Coll Pharm, 194-21,Osongsangmyeong 1 Ro, Cheongju 28160, Chungbuk, South Korea
[2] P2K Bio, Res & Dev Ctr, Cheongju, South Korea
[3] Jeonbuk Natl Univ, Inst New Drug Dev, Sch Pharm, Jeonju, South Korea
[4] Jeonbuk Natl Univ, Resp Drug Dev Res Inst, Sch Pharm, Jeonju, South Korea
[5] Wonkwang Univ, Coll Pharm, Iksan, South Korea
基金
新加坡国家研究基金会;
关键词
Hot melt extrusion; cyclosporine A; 3-dimensional printing; biodegradable filament; solubilization; DRUG-RELEASE; EXTRUSION; DESIGN; FORMULATION; POLYMERS; DOSAGE;
D O I
10.1080/10837450.2025.2472893
中图分类号
R9 [药学];
学科分类号
1007 ;
摘要
3D printing technology is gaining attention as a next-generation approach to drug formulation. Among 3D printing techniques, fused deposition modeling is cost-effective but depends heavily on suitable filaments. Hot melt extrusion enables filament production by incorporating poorly water-soluble drugs like cyclosporine A into polymers to form solid dispersions. However, achieving immediate release formulations with 3D printing remains challenging due to issues such as inadequate tablet disintegration or drug entrapment within the polymer matrix. This study aimed to develop and evaluate immediate release 3D-printed cyclosporine A tablets using HME filaments. Three parameters were modified in the 3D printing process: varying fill speeds, infill densities, and channel lengths. Filaments composed of Kollidon (R) VA 64 and HPC-SSL (1:1) were used to print tablets. Solid-state analysis confirmed cyclosporine A 's amorphous state and partial crystallinity in Xylisorb (R) 300. Dissolution studies revealed that lower infill densities (30%) and fewer walls enhanced drug release by increasing internal void space and reducing hardness. Conversely, greater tablet height (channel length) delayed dissolution. These findings emphasize the critical role of geometric design in drug release, showcasing the potential of 3D printing to create personalized dosage forms tailored to patient needs by optimizing structural parameters.
引用
收藏
页码:295 / 305
页数:11
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