Multiple Approaches to Repurposing Drugs for Neuroblastoma

Overview

Journal Bioorg Med Chem

Specialties Biochemistry
Chemistry

Date 2022 Oct 8

PMID 36208544

Authors

Laura Rank

Ana C Puhl

Tammy M Havener

Edward Anderson

Daniel H Foil

Kimberley M Zorn

Natalia Monakhova

Olga Riabova

Anthony J Hickey

Vadim Makarov

Sean Ekins

Affiliations

Soon will be listed here.

Abstract

Neuroblastoma (NB) is the second leading extracranial solid tumor of early childhood with about two-thirds of cases presenting before the age of 5, and accounts for roughly 15 percent of all pediatric cancer fatalities in the United States. Treatments against NB are lacking, resulting in a low survival rate in high-risk patients. A repurposing approach using already approved or clinical stage compounds can be used for diseases for which the patient population is small, and the commercial market limited. We have used Bayesian machine learning, in vitro cell assays, and combination analysis to identify molecules with potential use for NB. We demonstrated that pyronaridine (SH-SY5Y IC 1.70 µM, SK-N-AS IC 3.45 µM), BAY 11-7082 (SH-SY5Y IC 0.85 µM, SK-N-AS IC 1.23 µM), niclosamide (SH-SY5Y IC 0.87 µM, SK-N-AS IC 2.33 µM) and fingolimod (SH-SY5Y IC 4.71 µM, SK-N-AS IC 6.11 µM) showed cytotoxicity against NB. As several of the molecules are approved drugs in the US or elsewhere, they may be repurposed more readily for NB treatment. Pyronaridine was also tested in combinations in SH-SY5Y cells and demonstrated an antagonistic effect with either etoposide or crizotinib. Whereas when crizotinib and etoposide were combined with each other they had a synergistic effect in these cells. We have also described several analogs of pyronaridine to explore the structure-activity relationship against cell lines. We describe multiple molecules demonstrating cytotoxicity against NB and the further evaluation of these molecules and combinations using other NB cells lines and in vivo models will be important in the future to assess translational potential.

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