AI Article Synopsis

  • * The study involved creating three types of PEGylated acacetin to improve its solubility and anti-inflammatory properties, with PEG-Acacetin showing the most promise by significantly boosting plasma levels and demonstrating increased anti-inflammatory effects.
  • * In tests on mice, PEG-Acacetin effectively reduced bone loss caused by both lipopolysaccharide and ovariectomy, outperforming naked acacetin and suggesting it could be a strong candidate for osteoporosis treatment.

Article Abstract

Osteoporosis is a condition of progressive bone loss attributable to excessive osteoclastic activity. Acacetin is a potential candidate for osteoporosis therapy because it specifically suppressing osteoclastic function. However, the application of acacetin was limited by its poor solubility and bad pharmacokinetic behavior. In current work, we examined whether PEGylation of acacetin enhances its anti-osteoporosis activity in ovariectomy-induced osteoporosis and LPS-induced osteolysis. In the current study, three types of PEGylated acacetin (PEG-A, PEG-A, PEG-A) were tested for their effects on the solubility and anti-inflammatory activity of acacetin in vitro. PEG-Acacetin was selected for further investigation as it demonstrated the strongest anti-inflammatory activity comparable to that of naked acacetin and other two PEGylated acacetin. PEGylation in PEG-Acacetin increased maximum plasma concentration of acacetin by 620.77% in mice. Furthermore, PEG-A showed a higher anti-osteoclastogenic capacity in vitro than that of naked acacetin. It was found that PEG-A treatment in vivo mitigated lipopolysaccharide (LPS)- and ovariectomy (OVX)-induced bone loss in mice. More importantly, the in vivo efficiency of PEG-Acacetin was significantly better than that of naked acacetin. In summary, PEGylated acacetin possesses a clean advantage over the naked acacetin and would be a potential candidate for the osteoporosis therapy.

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Source
http://dx.doi.org/10.1016/j.bmc.2024.117910DOI Listing

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