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Improvement of antithrombotic activity of red ginseng extract by nanoencapsulation using chitosan and antithrombotic cross-linkers: polyglutamic acid and fucodianopen access

Authors
Kim, Eun SuhLee, Ji-SooLee, Hyeon Gyu
Issue Date
Mar-2021
Publisher
KOREAN SOC GINSENG
Keywords
Antithrombotic activity; Chitosan nanoparticle; Ionic gelation; Platelet aggregation; Red ginseng; Response surface methodology
Citation
JOURNAL OF GINSENG RESEARCH, v.45, no.2, pp.236 - 245
Indexed
SCIE
SCOPUS
KCI
Journal Title
JOURNAL OF GINSENG RESEARCH
Volume
45
Number
2
Start Page
236
End Page
245
URI
https://scholarworks.bwise.kr/hanyang/handle/2021.sw.hanyang/142231
DOI
10.1016/j.jgr.2020.04.001
ISSN
1226-8453
Abstract
Background: Red ginseng (RG) extract, especially ginsenoside Rg1 and Rb1 fractions has been reported to have antithrombotic activities. However, gastric instability and low intestinal permeability are considered to be obstacles to its oral administration. We hypothesized that stability, permeability, and activities of RG might be improved by encapsulation within nanoparticles (NPs) prepared with antithrombotic coating materials. Methods: RG-loaded chitosan (CS) NPs (PF-NPs) were prepared by complex ionic gelation with the antithrombotic wall materials, polyglutamic acid (PGA), and fucoidan (Fu). The concentrations of PGA (mg/mL, X-1) and Fu (mg/mL, X-2) were optimized for the smallest particle size by response surface methodology. Antithrombotic activities of RG and PF-NPs were analyzed using ex vivo and in vivo antiplatelet activities, in vivo carrageenan-induced mouse tail, and arteriovenous shunt rat thrombosis models. Results: In accordance with a quadratic regression model, the smallest PF-NPs (286 + 36.6 nm) were fabricated at 0.628 mg/mL PGA and 0.081 mg/mL Fu. The inhibitory activities of RG on ex vivo and in vivo platelet aggregation and thrombosis in in vivo arteriovenous shunt significantly (p < 0.05) increased to approximately 66.82%, 35.42%, and 38.95%, respectively, by encapsulation within PF-NPs. For an in vivo carrageenan-induced mouse tail thrombosis model, though RG had a weaker inhibitory effect, PF-NPs reduced thrombus significantly due to the presence of PGA and Fu. Conclusion: PF-NPs contributed to improve the activities of RG not only by nanoencapsulation but also by antithrombotic coating materials. Therefore, PG-NPs can be suggested as an efficient delivery system for oral administration of RG.
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COLLEGE OF HUMAN ECOLOGY (DEPARTMENT OF FOOD & NUTRITION)
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