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A co-crystal berberine-ibuprofen improves obesity by inhibiting the protein kinases TBK1 and IKKɛ

Man Wang, Rong Xu, Xiaoli Liu, Ling Zhang, Siyan Qiu, Yuting Lu, Peng Zhang, Ming Yan, Jing Zhu

2022Communications Biology23 citationsDOIOpen Access PDF

Abstract

Berberine (BBR) exerts specific therapeutic effects on various diseases such as diabetes, obesity, and other inflammation-associated diseases. However, the low oral bioavailability (below 1%) of berberine due to its poor solubility and membrane permeability limits its clinical use. In this paper, we have prepared a 1:1 co-crystal berberine-ibuprofen (BJ) using drug salt metathesis and co-crystal technology. Pharmacokinetic studies demonstrate a 3-fold increase in vivo bioavailability of BJ compared to that of BBR, and BJ is more effective in treating obesity and its related metabolism in vitro and in vivo. We also find that BJ promotes mitochondrial biogenesis by inhibiting TBK1 and inducing AMP-activated protein kinase (AMPK) phosphorylation, and BJ increases adipocyte sensitivity to catecholamine by inhibiting IKKε. Together, our findings support that co-crystal BJ is likely to be an effective agent for treating obesity and its related metabolic diseases targeting TBK1 and IKKε.

Topics & Concepts

BerberinePharmacologyChemistryBioavailabilityIn vivoKinaseAMPKIκB kinaseProtein kinase AMedicineBiochemistryBiologySignal transductionNF-κBBiotechnologyBerberine and alkaloids researchGinseng Biological Effects and ApplicationsPhytochemistry and biological activities of Ficus species
A co-crystal berberine-ibuprofen improves obesity by inhibiting the protein kinases TBK1 and IKKɛ | Litcius