Synthesis and Preliminary Evaluation of an ASGPr-Targeted Polycationic <i>β</i>-Cyclodextrin Carrier for Nucleosides and Nucleotides

Jang-Ha Ryu; Weizhong Zheng; Xiao-Hong Yang; Hassan Elsaidi; Jim Diakur; Leonard I. Wiebe

doi:10.3390/pharmaceutics16030323

Pharmaceutics (Feb 2024)

Synthesis and Preliminary Evaluation of an ASGPr-Targeted Polycationic <i>β</i>-Cyclodextrin Carrier for Nucleosides and Nucleotides

Jang-Ha Ryu,
Weizhong Zheng,
Xiao-Hong Yang,
Hassan Elsaidi,
Jim Diakur,
Leonard I. Wiebe

Affiliations

Jang-Ha Ryu: Independent Researcher, Hwasung-city 18245, Republic of Korea
Weizhong Zheng: Independent Researcher, Edmonton, AB T6W 1T4, Canada
Xiao-Hong Yang: Independent Researcher, Edmonton, AB T6G 1Z2, Canada
Hassan Elsaidi: Department of Pharmaceutical Chemistry, Faculty of Pharmacy, University of Alexandria, El Sultan Hussein St. Azarita, Alexandria 21521, Egypt
Jim Diakur: Independent Researcher, Winnipeg, MB R3T 0P4, Canada
Leonard I. Wiebe: Faculty of Pharmacy and Pharmaceutical Sciences, 2-35 Medical Sciences Building, University of Alberta, 8613-114 St., Edmonton, AB T6G 2H7, Canada

DOI: https://doi.org/10.3390/pharmaceutics16030323
Journal volume & issue: Vol. 16, no. 3
p. 323

Abstract

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Most antiviral and anticancer nucleosides are prodrugs that require stepwise phosphorylation to their triphosphate nucleotide form for biological activity. Monophosphorylation may be rate-limiting, and the nucleotides may be unstable and poorly internalized by target cells. Effective targeting and delivery systems for nucleoside drugs, including oligonucleotides used in molecular therapeutics, could augment their efficacy. The development of a carrier designed to effect selective transmembrane internalization of nucleotides via the asialoglycoprotein receptor (ASGPr) is now reported. In this work, the polycationic, polygalactosyl drug delivery carrier heptakis[6-amino-6-deoxy-2-O-(3-(1-thio-β-D-galactopyranosyl)-propyl)]-β-cyclodextrin hepta-acetate salt (GCyDAc), potentially a bifunctional carrier of (poly)nucleotides, was modeled by molecular docking in silico as an ASGPr-ligand, then synthesized for testing. The antivirals arabinosyl adenine (araA, vidarabine, an early generation antiviral nucleoside), arabinosyl adenine 5′-monophosphate (araAMP), and 12-mer-araAMP (p-araAMP) were selected for individual formulation with GCyDAc to develop this concept. Experimentally, beta cyclodextrin was decorated with seven protonated amino substituents on the primary face, and seven thiogalactose residues on its secondary face. AraA, araAMP, and p-araAMP were individually complexed with GCyDAc and complex formation for each drug was confirmed by differential scanning calorimetry (DSC). Finally, the free drugs and their GCyDAc complexes were evaluated for antiviral activity using ASGPr-expressing HepAD38 cells in cell culture. In this model, araA, araAMP, and p-araAMP showed relative antiviral potencies of 1.0, 1.1, and 1.2, respectively. In comparison, GCyDAc-complexes of araA, araAMP, and p-araAMP were 2.5, 1.3, and 1.2 times more effective than non-complexed araA in suppressing viral DNA production. The antiviral potencies of these complexes were minimally supportive of the hypothesis that ASGPr-targeted, CyD-based charge-association complexation of nucleosides and nucleotides could effectively enhance antiviral efficacy. GCyDAc was non-toxic to mammalian cells in cell culture, as determined using the MTS proliferation assay.

Published in Pharmaceutics

ISSN: 1999-4923 (Online)
Publisher: MDPI AG
Country of publisher: Switzerland
LCC subjects: Medicine: Pharmacy and materia medica
Website: http://www.mdpi.com/journal/pharmaceutics/

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