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First-in-class small molecule potentiators of cancer virotherapy

Authors :
Andrew Chen
Penny J. Le
Nader El Sayes
Jeffrey C. Smith
Kerkeslin Keillor
John C. Bell
Colin Davis
Christopher N. Boddy
Ramya Krishnan
Hwan Hee Son
Fabrice Le Boeuf
Jean-Simon Diallo
Andrew Macklin
Carlos R. Canez
Paula Ou
Christina Moi
Mark H. Dornan
Mohammed Selman
Christophe Pardin
Source :
Scientific Reports
Publication Year :
2016
Publisher :
Nature Publishing Group, 2016.

Abstract

The use of engineered viral strains such as gene therapy vectors and oncolytic viruses (OV) to selectively destroy cancer cells is poised to make a major impact in the clinic and revolutionize cancer therapy. In particular, several studies have shown that OV therapy is safe and well tolerated in humans and can infect a broad range of cancers. Yet in clinical studies OV therapy has highly variable response rates. The heterogeneous nature of tumors is widely accepted to be a major obstacle for OV therapeutics and highlights a need for strategies to improve viral replication efficacy. Here, we describe the development of a new class of small molecules for selectively enhancing OV replication in cancer tissue. Medicinal chemistry studies led to the identification of compounds that enhance multiple OVs and gene therapy vectors. Lead compounds increase OV growth up to 2000-fold in vitro and demonstrate remarkable selectivity for cancer cells over normal tissue ex vivo and in vivo. These small molecules also demonstrate enhanced stability with reduced electrophilicity and are highly tolerated in animals. This pharmacoviral approach expands the scope of OVs to include resistant tumors, further potentiating this transformative therapy. It is easily foreseeable that this approach can be applied to therapeutically enhance other attenuated viral vectors.

Details

Language :
English
ISSN :
20452322
Volume :
6
Database :
OpenAIRE
Journal :
Scientific Reports
Accession number :
edsair.doi.dedup.....285f1f068095fa7414e7041396071366