Abstract
Arteannuin B (AB) has been found to demonstrate obvious anti-tumor activity. However, AB is not available for clinical use due to its very low solubility and very short half-life. This study aimed to develop AB long sustained-release microspheres (ABMs) to improve the feasibility of clinical applications. Firstly, AB-polylactic-co-glycolic acid (PLGA) microspheres were prepared by a single emulsification method. In vitro characterization studies showed that ABMs had a low burst release and stable in vitro release for up to one week. The particle size of microspheres was 69.10 μm (D50). The drug loading is 37.8%, and the encapsulation rate is 85%. Moreover, molecular dynamics modeling was firstly used to simulate the preparation process of microspheres, which clearly indicated the molecular image of microspheres and provided in-depth insights for understanding several key preparation parameters. Next, in vivo pharmacokinetics (PK) study was carried out to evaluate its sustained release effect in Sprague-Dawley (SD) rats. Subsequently, the methyl thiazolyl tetrazolium (MTT) method with human lung cancer cells (A549) was used to evaluate the in vitro efficacy of ABMs, which showed the IC50 of ABMs (3.82 μM) to be lower than that of AB (16.03 μM) at day four. Finally, in vivo anti-tumor activity and basic toxicity studies were performed on BALB/c nude mice by subcutaneous injection once a week, four times in total. The relative tumor proliferation rate T/C of AMBs was lower than 40% and lasted for 21 days after administration. The organ index, organ staining, and tumor cell staining indicated the excellent safety of ABMs than Cis-platinum. In summary, the ABMs were successfully developed and evaluated with a low burst release and a stable release within a week. Molecular dynamics modeling was firstly applied to investigate the molecular mechanism of the microsphere preparation. Moreover, the ABMs possess excellent in vitro and in vivo anti-tumor activity and low toxicity, showing great potential for clinical applications.
Highlights
In order to further improve the therapeutic potential of Arteannuin B (AB) in clinical applications, this study aimed to develop AB-polylactic-co-glycolic acid (PLGA) sustained-release microspheres using the emulsionsolvent evaporation method
Given the aqueous solubility9 of issue of AB, the single-emulsion method was used for the preparation of AB long sustained-release microspheres (ABMs)
Mechanism of ABMs was revealed from a microscopic point of view
Summary
Arteannuin B (AB) was first isolated in 1973 from Artemisia annua L. and was a precursor of arteannuin, a sesquiterpene lactone compound with antimalarial effect [1,2]. Compared with traditional arteannuin derivatives, it has no peroxy bridge structure, as 4.0/). Pharmaceutics 2021, 13, x FOR PEER REVIEW. Compared with traditional arteannuin derivatives, it has no peroxy bridge structure, as shown Figure. Modern pharmacological researches have shown that has antishown inin. ABAB has nono antimalarial activity [3], but it exhibits strong anti-inflammatory and immunological activities malarial activity [3], but it exhibits strong anti-inflammatory and immunological activities preliminary screening. With the deepening of research, people gradually discovinin preliminary screening [4].[4]
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