Three-dimensional printed isoniazid liposome photothermal composite scaffolds and their performance evaluation

doi:10.12307/2026.844

Abstract

Abstract: BACKGROUND: Drug-loaded bone scaffolds for tuberculosis treatment suffer from problems such as drug burst release in the early stages of treatment and insufficient drug release in the later stages, which leads to low drug concentration at the lesion, therefore, it is imperative to build a drug controlled-release system on the tissue-engineered bone scaffolds.
OBJECTIVE: To prepare photothermal composite scaffolds with different isoniazid liposome doping ratios and characterize their mechanical and biological properties.
METHODS: Isoniazid liposomes were prepared using the thin-film hydration method. The microstructure, encapsulation efficiency, drug loading capacity, particle size, and Zeta potential of liposomes were characterized. 15 mg of isoniazid was selected as the total drug amount for a single drug-loaded scaffold. Isoniazid drug powder, isoniazid liposome powder at 2%, 5%, and 8% of the total drug amount, respectively, were mixed uniformly with the scaffold base material (hydroxyapatite and β-tricalcium phosphate in a mass ratio of 6:4) and 3% of the photothermal agent polypyrrole nanoparticles (by mass fraction of the scaffold base material) to prepare extrusion printing powders. 13% polyvinyl alcohol gel was added to the extrusion printing powder in a 1:1 mass ratio. Pure isoniazid scaffolds and three kinds of isoniazid liposome photothermal scaffolds were fabricated using extrusion-based 3D bioprinting. The microstructure, porosity, mechanical properties, and drug release performance of the photothermal scaffolds were characterized. Mouse embryonic osteoblasts (MC3T3 cells) were cultured with extracts from the four kinds of scaffolds. The cytotoxicity of the scaffolds was detected using the MTT assay.
RESULTS AND CONCLUSION: (1) Under transmission electron microscopy, isoniazid liposomes appeared as spherical vesicles with a relatively regular shape. The encapsulation efficiency of isoniazid liposomes was (28.67±0.62)%, the drug loading capacity was (3.54±0.19)%, the average particle size was (363.63±10.42) nm, and the average Zeta potential was (-4.68±0.72) mV. (2) Scanning electron microscopy showed that compared with the pure isoniazid scaffold, the isoniazid liposome photothermal scaffold had more pores internally. With the increase of isoniazid liposome content, the porosity of the photothermal scaffold showed an increasing trend, while the compressive strength and elastic modulus showed a decreasing trend, but still met the minimum compressive strength required for tissue implantation experiments in animals. The incorporation of isoniazid liposomes effectively solved the problem of drug burst release in the early stage of drug release from the scaffold, and the cumulative drug release rate in the early stage was inversely proportional to the amount of isoniazid liposomes incorporated. After irradiation with an 808 nm near-infrared laser, the cumulative drug release rate of the isoniazid liposome photothermal scaffold increased compared with that without near-infrared laser irradiation. With the increase of isoniazid liposome content, the photothermal controlled release performance of the scaffold became more significant in the later stage of drug release. MTT assay showed that the relative proliferation rate of MC3T3 cells cultured with the extracts of the four kinds of scaffolds for 24, 72, and 120 hours was all greater than 70%, indicating no significant cytotoxicity. The results show that the isoniazid liposome photothermal scaffold has good mechanical properties, drug-controlled release performance, and cytocompatibility.

Key words: bone tuberculosis, 3D printing, drug-loaded scaffolds, liposome, polypyrrole, controlled drug release, biomaterials

CLC Number:

Yang Guang, Yin Zhitao, Xu Yan. Three-dimensional printed isoniazid liposome photothermal composite scaffolds and their performance evaluation[J]. Chinese Journal of Tissue Engineering Research, 2026, 30(26): 6701-6709.

Figures/Tables 13

2.7 支架的释药性能分析结果 2.7.1 异烟肼脂质体光热支架药物缓释性能分析结合图11和表2可以分析得出，纯异烟肼支架前期72 h累积释药率达到76.259%，相比异烟肼脂质体光热支架出现显著药物突释现象，这可能是由于实验药物异烟肼的水溶性较好且分子质量较小，通过直接包埋方式搭载到支架中时，支架内部孔隙中异烟肼药物浓度较高，与外部PBS形成浓度差而加速向外部扩散[32]。异烟肼脂质体的掺入可显著缓解支架的前期药物突释现象，异烟肼脂质体光热支架前72 h的累积释药率分别为59.711%，43.104%，36.819%，较纯异烟肼支架前72 h的累积释药率显著下降，并且随着异烟肼脂质体掺杂量的增多，光热支架药物缓释性能增强，造成这种现象的原因可能是：由于异烟肼脂质体的磷脂双分子层对药物具有包覆作用，亲水性药物异烟肼被包封在脂质体的内水相中，支架中异烟肼释放时需穿过脂质体磷脂双分子层这一物理屏障再二次扩散到模拟体液中，故随着异烟肼脂质体的掺杂量的增加，支架的这一缓释现象更为明显。 2.7.2 支架药物控释性能分析结合图11和表2可以分析得出，相较于未经近红外光照射的同种支架，2%，5%，8%异烟肼脂质体光热支架经近红外光照射后在72-120 h的累积释药率分别增加4.519%，4.697%，9.832%，336-504 h的累积释药率分别增加1.567%，2.368%，3.144%，表现出较强的近红外光控释性能，这是由于掺杂的聚吡咯纳米颗粒具有较强的近红外吸收性能，当其吸收光能时内部的电子会被激发跃迁到更高能级，而处于激发态的电子返回基态时会以热能的形式释放能量，此过程将光能转化为热能[33]，使支架温度升高，进而使脂质体磷脂双分子层通透性增强，导致脂膜孔隙增大，加快包封的异烟肼向模拟体液中扩散，同时，支架周围环境温度升高使分子热运动更为剧烈，有利于支架的降解和药物分子的释放。随着异烟肼脂质体掺杂量的增多，光热支架释药后期(336-504 h)的近红外光控释性能增强，结合药物缓解性能分析实验结果，这是由于异烟肼脂质体掺杂量较大时光热支架释药前期药物缓释较好，使得释药后期支架中留存的药量增多，能够更容易满足骨结核治疗后期对药物浓度的需求。 "

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