The Amorphous Solid Dispersion of Chrysin in Plasdone® S630 Demonstrates Improved Oral Bioavailability and Antihyperlipidemic Performance in Rats

Chenhui Wang; Xiaowei Liu; Ruihan Zhao; Meiqing Yang; Wenqian Liu; Qiuyang Dai; Xiaofeng Bao; Yong Chen; Jun Ma

doi:10.3390/pharmaceutics15102378

The Amorphous Solid Dispersion of Chrysin in Plasdone^® S630 Demonstrates Improved Oral Bioavailability and Antihyperlipidemic Performance in Rats

Pharmaceutics. 2023 Sep 24;15(10):2378. doi: 10.3390/pharmaceutics15102378.

Authors

Chenhui Wang¹, Xiaowei Liu¹, Ruihan Zhao², Meiqing Yang¹, Wenqian Liu¹, Qiuyang Dai¹, Xiaofeng Bao¹, Yong Chen¹, Jun Ma³

Affiliations

¹ School of Pharmacy, Nantong University, 19 Qixiu Road, Nantong 226001, China.
² School of Pharmacy, China Pharmaceutical University, 639 Longmian Avenue, Nanjing 211198, China.
³ Shenzhen Wanhe Pharmaceutical Company & Guangdong Provincial Key Laboratory of Microecological Preparations, 7 Huitong Road, Shenzhen 518107, China.

Abstract

Chrysin is a flavonoid with various biological activities. However, its low water solubility and strong metabolism render its oral bioavailability rather poor. This study aimed to develop a stable solid dispersion formulation of chrysin to improve the dissolution of chrysin, so as to increase its oral bioavailability and improve its antihyperlipidemic activities. A solid dispersion of chrysin was prepared using a solvent evaporation method, with Plasdone^® S630 as the hydrophilic carrier. The formulations were characterized via X-ray diffraction, in vitro dissolution studies, and stability studies. An in-situ perfusion model was used to evaluate the absorption rates. Plasma pharmacokinetics and antihyperlipidemic performance after the oral administration of the chrysin formulations were investigated in rats. It was found that the solid dispersion of chrysin prepared using the drug-polymer mass ratio of 1:6 can form the optimized formulation. X-ray diffraction results showed that the chrysin was in an amorphous state in this optimized formulation. The cumulative release percentage of the optimized solid dispersion of chrysin at pH 1.2 and pH 6.8 was elevated to above 90% within 24 h, indicating that the formulation could enhance the dissolution rates of chrysin. Stability studies showed that the optimized formulation presented acceptable long-term storage stability, but it was susceptible to high temperature and humidity. The solid dispersion of chrysin showed higher absorption rates in the in-situ perfusion model. Pharmacokinetic studies revealed that C_max and AUC after the intragastric administration of solid dispersion of chrysin were appreciably higher than those resulting from chrysin suspension. The oral bioavailability of the solid dispersion of chrysin was 41 times higher than that of chrysin suspension. Pharmacological studies suggested that the solid dispersion of chrysin was more powerful than chrysin raw material in improving biochemical indicators in the hyperlipidemic model in rats. This study reveals the potential use of a novel oral formulation of chrysin to reduce the currently required high dose.

Keywords: XRD; antihyperlipidemic performance; chrysin; dissolution; in-situ perfusion; oral bioavailability; solid dispersion; stability.

Abstract

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