Cyclodextrin Derivatives as Promising Solubilizers to Enhance the Biological Activity of Rosmarinic Acid

Anna Stasiłowicz-Krzemień; Natalia Rosiak; Anita Płazińska; Wojciech Płaziński; Andrzej Miklaszewski; Ewa Tykarska; Judyta Cielecka-Piontek

doi:10.3390/pharmaceutics14102098

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Title

Cyclodextrin Derivatives as Promising Solubilizers to Enhance the Biological Activity of Rosmarinic Acid

Authors

Anna Stasiłowicz-Krzemień
Natalia Rosiak
Anita Płazińska
Wojciech Płaziński
Andrzej Miklaszewski (WIMiFT) ^{[ 1 ][ 2.8 ][ P ]}
Ewa Tykarska
Judyta Cielecka-Piontek

^{[ 1 ]} Instytut Inżynierii Materiałowej, Wydział Inżynierii Materiałowej i Fizyki Technicznej, Politechnika Poznańska | ^{[ P ]} employee

Scientific discipline (Law 2.0)

[2.8] Materials engineering

Year of publication

2022

Published in

Pharmaceutics

Journal year: 2022 | Journal volume: vol. 14 | Journal number: iss. 10

Article type

scientific article

Publication language

english

Keywords

EN

rosmarinic acid
cyclodextrins
neurodegeneration
solubility
permeability
blood–brain barrier

Abstract

EN Rosmarinic acid (RA) is a natural antioxidant with neuroprotective properties; however, its preventive and therapeutic use is limited due to its slight solubility and poor permeability. This study aimed to improve RA physicochemical properties by systems formation with cyclodextrins (CDs): hydroxypropyl-α-CD (HP-α-CD), HP-β-CD, and HP-γ-CD, which were prepared by the solvent evaporation (s.e.) method. The interactions between components were determined by X-ray powder diffraction (XRPD), differential scanning calorimetry (DSC) and Fourier Transform infrared spectroscopy (FTIR). The sites of interaction between RA and CDs were suggested as a result of in silico studies focused on assessing the interaction between molecules. The impact of amorphous systems formation on water solubility, dissolution rate, gastrointestinal (GIT) permeability, and biological activity was studied. RA solubility was increased from 5.869 mg/mL to 113.027 mg/mL, 179.840 mg/mL, and 194.354 mg/mL by systems formation with HP-α-CD, HP-β-CD, and HP-γ-CD, respectively. During apparent solubility studies, the systems provided an acceleration of RA dissolution. Poor RA GIT permeability at pH 4.5 and 5.8, determined by parallel artificial membrane permeability assay (PAMPA system), was increased; RA–HP-γ-CD s.e. indicated the greatest improvement (at pH 4.5 from Papp 6.901 × 10−7 cm/s to 1.085 × 10−6 cm/s and at pH 5.8 from 5.019 × 10−7 cm/s to 9.680 × 10−7 cm/s). Antioxidant activity, which was determined by DPPH, ABTS, CUPRAC, and FRAP methods, was ameliorated by systems; the greatest results were obtained for RA–HP-γ-CD s.e. The inhibition of acetylcholinesterase (AChE) and butyrylcholinesterase (BChE) was increased from 36.876% for AChE and 13.68% for BChE to a maximum inhibition of the enzyme (plateau), and enabled reaching IC50 values for both enzymes by all systems. CDs are efficient excipients for improving RA physicochemical and biological properties. HP-γ-CD was the greatest one with potential for future food or dietary supplement applications.

Date of online publication

30.09.2022

Pages (from - to)

2098 - 1 - 2098 - 22

DOI

10.3390/pharmaceutics14102098

URL

https://www.mdpi.com/1999-4923/14/10/2098

Comments

Article number: 2098

License type

CC BY (attribution alone)