Identification of individual structural fragments of N,N'-(bis-5-nitropyrimidyl)dispirotripiperazine derivatives for cytotoxicity and antiherpetic activity allows the prediction of new highly active compounds

doi:10.1093/jac/dkm172

JAC Advance Access originally published online on June 5, 2007
Journal of Antimicrobial Chemotherapy 2007 60(1):68-77; doi:10.1093/jac/dkm172

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© The Author 2007. Published by Oxford University Press on behalf of the British Society for Antimicrobial Chemotherapy. All rights reserved. For Permissions, please e-mail: journals.permissions@oxfordjournals.org

Identification of individual structural fragments of N,N'-(bis-5-nitropyrimidyl)dispirotripiperazine derivatives for cytotoxicity and antiherpetic activity allows the prediction of new highly active compounds

A. G. Artemenko¹, E. N. Muratov¹, V. E. Kuz'min¹, N. A. Kovdienko¹, A. I. Hromov¹, V. A. Makarov², O. B. Riabova², P. Wutzler³ and M. Schmidtke³^,*

¹ A.V. Bogatsky Physical-Chemical Institute, Lustdorfskaya doroga 86, Odessa, Ukraine ² Research Center for Antibiotics, Nagatinskaya Str. 3a, Moscow, Russia ³ Institute of Virology and Antiviral Therapy, Friedrich Schiller University, Hans-Knoell-Str. 2, Jena, Germany

Received 30 January 2007; returned 6 April 2007; revised 20 April 2007; accepted 23 April 2007

^* Corresponding author. Tel: +49-3641-657222; Fax: +49-3641-657301; E-mail: michaela.schmidtke{at}med.uni-jena.de

Objectives: The objectives of this study were (i) to apply computer-basedtechnologies to evaluate the structure of 48 N,N'-(bis-5-nitropyrimidyl)dispirotripiperazineswhich belong to a new class of highly active antiviral compoundsbinding to cell surface heparan sulphates, (ii) to understandthe chemical– biological interactions governing theiractivities, and (iii) to design new compounds with strong antiviralactivity.

Methods: The logarithm of 50% cytotoxic concentration (CC₅₀) in GMK cells,of 50% inhibitory concentration (IC₅₀) against herpes simplexvirus type 1, and of selectivity index (SI = CC₅₀/IC₅₀) wasused to develop quantitative structure–activity relationships(QSARs) based on simplex representation of molecular structure.The QSAR model was applied to design new compounds. Two of thesecompounds were synthesized, physico-chemically characterizedand tested for cytotoxicity and antiviral activity.

Results: Statistic characteristics for partial least squares models allowthe prediction of CC₅₀, IC₅₀ and SI values. The QSAR resultsdemonstrate a high impact of individual structural fragmentsfor antiviral activity. Molecular fragments that promote andinterfere with antiviral activity were defined on the basisof the obtained models. Electrostatic factors (38%) and hydrophobicity(34%) were the most important determinants of antiherpetic activity.Using the established method, new potential dispirotripiperazinederivatives were computationally designed. Two of these computationallydesigned compounds were synthesized. The biological test resultsconfirm the computationally predicted values of these compounds.

Conclusions: The established QSAR model is suitable for the design of newantiherpetic compounds and prediction of their activity.

Keywords: QSAR , SiRMS , herpes virus , heparan sulfate , antiviral , drug design

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