Dimethyl sulfoxide blocks herpes simplex virus-1 productive infection in vitro acting at different stages with positive cooperativity. Application of micro-array analysis

doi:10.1186/1471-2334-2-9

BMC Infectious Diseases

Volume 2

Viewing options:

Abstract
Full text
PDF (327KB)
Additional files

Associated material:

Related literature:

Articles citing this article
on Google Scholar
on ISI Web of Science
on PubMed Central
Other articles by authors
on Google Scholar

Aguilar JS
Roy D
Ghazal P
Wagner EK

on PubMed

Aguilar JS
Roy D
Ghazal P
Wagner EK
Related articles/pages
on Google

on Google Scholar

on PubMed

Tools:

Post to:

Research article

Dimethyl sulfoxide blocks herpes simplex virus-1 productive infection in vitro acting at different stages with positive cooperativity. Application of micro-array analysis

JS Aguilar¹ , D Roy² , P Ghazal² and EK Wagner¹

¹Dept. of Mol. Biol. & Biochem, U. Calif. Irvine, 19172 Jamboree Road, Irvine, CA 92697, USA

²Genomic Technology & Informatics Centre, University of Edinburgh, Summerhall EH9 1QH, UK

author email corresponding author email

BMC Infectious Diseases 2002, 2:9doi:10.1186/1471-2334-2-9


Published:	24 May 2002

Abstract

Background

Dimethyl sulfoxide (DMSO) is frequently used at a concentration of up to 95% in the formulation of antiherpetic agents because of its properties as a skin penetration enhancer. Here, we have analyzed the effect of DMSO on several parameters of Herpes Simplex Virus replication.

Methods

Productive infection levels of HSV-1 were determined by plaque assay or by reporter gene activity, and its DNA replication was estimated by PCR. Transcript levels were evaluated with HSV-specific DNA micro-arrays.

Results

DMSO blocks productive infection in vitro in different cell types with a 50% inhibitory concentration (IC₅₀) from 0.7 to 2% depending upon the multiplicity of infection. The concentration dependence exhibits a Hill coefficient greater than 1, indicating that DMSO blocks productive infection by acting at multiple different points (mechanisms of action) with positive cooperativity. Consistently, we identified at least three distinct temporal target mechanisms for inhibition of virus growth by DMSO. At late stages of infection, DMSO reduces virion infectivity, and markedly inhibits viral DNA replication. A third mode of action was revealed using an oligonucleotide-based DNA microarray system for HSV. These experiments showed that DMSO reduced the transcript levels of many HSV-1 genes; including several genes coding for proteins involved in forming and assembling the virion. Also, DMSO markedly inhibited some but not all early transcripts indicating a previously unknown mode for inhibiting the early phase of HSV transcription-replication cycle.

Conclusion

These observations suggest that DMSO itself may have a role in the anti-herpetic activity of formulations utilizing it as a dispersant.