Viruses (Aug 2012)

A Limited Structural Modification Results in a Significantly More Efficacious Diazachrysene-Based Filovirus Inhibitor

  • Rekha G. Panchal,
  • Bogdan A. Šolaja,
  • James C. Burnett,
  • Cary Retterer,
  • Sina Bavari,
  • Brett Eaton,
  • Života Selaković,
  • Dejan Opsenica

DOI
https://doi.org/10.3390/v4081279
Journal volume & issue
Vol. 4, no. 8
pp. 1279 – 1288

Abstract

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Ebola (EBOV) and Marburg (MARV) filoviruses are highly infectious pathogens causing deadly hemorrhagic fever in humans and non-human primates. Promising vaccine candidates providing immunity against filoviruses have been reported. However, the sporadic nature and swift progression of filovirus disease underlines the need for the development of small molecule therapeutics providing immediate antiviral effects. Herein we describe a brief structural exploration of two previously reported diazachrysene (DAAC)-based EBOV inhibitors. Specifically, three analogs were prepared to examine how slight substituent modifications would affect inhibitory efficacy and inhibitor-mediated toxicity during not only EBOV, but also MARV cellular infection. Of the three analogs, one was highly efficacious, providing IC<sub>50</sub> values of 0.696 µM ± 0.13 µM and 2.76 µM ± 0.21 µM against EBOV and MARV infection, respectively, with little or no associated cellular toxicity. Overall, the structure-activity and structure-toxicity results from this study provide a framework for the future development of DAAC-based filovirus inhibitors that will be both active and non-toxic <em>in vivo</em>.

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