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Article Publish Status: FREE
Abstract Title:

Computational and Experimental Assessments of Magnolol as a Neuroprotective Agent and Utilization of UiO-66(Zr) as Its Drug Delivery System.

Abstract Source:

ACS Omega. 2021 Sep 28 ;6(38):24382-24396. Epub 2021 Sep 15. PMID: 34604621

Abstract Author(s):

Joshua Santos, Mark Tristan Quimque, Rhenz Alfred Liman, Jay Carl Agbay, Allan Patrick G Macabeo, Mary Jho-Anne Corpuz, Yun-Ming Wang, Tsai-Te Lu, Chia-Her Lin, Oliver B Villaflores

Article Affiliation:

Joshua Santos

Abstract:

The phenolic natural product magnolol exhibits neuroprotective properties throughβ-amyloid toxicity in PC-12 cells and ameliorative effects against cognitive deficits in a TgCRND8 transgenic mice model. Its bioavailability and blood-brain barrier crossing ability have been significantly improved using the metal-organic framework (MOF) UiO-66(Zr) as a drug delivery system (DDS).To investigate the neuroprotective effects of the Zr-based DDS, magnolol and magnolol-loaded-UiO-66(Zr) (Mag@UiO-66(Zr)) were evaluated for inhibitory activity against β-secretase and AlCl-induced neurotoxicity. Due to the moderate inhibition observed for magnolol,binding studies were explored againstβ-secretase along with 11 enzymes known to affect Alzheimer's disease (AD). Favorable binding energies against CDK2, CKD5, MARK, and phosphodiesterase 3B (PDE3B) and dynamically stable complexes were noted through molecular docking and molecular dynamic simulation experiments, respectively. The magnolol-loaded DDS UiO-66(Zr) also showed enhanced neuroprotective activity against two pathological indices, namely, neutrophil infiltration and apoptotic neurons, in addition to damage reversal compared to magnolol. Thus, MOFs are promising drug delivery platforms for poorly bioavailable drugs.

Study Type : In Vitro Study

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