2013
DOI: 10.1517/14728222.2013.827663
|View full text |Cite
|
Sign up to set email alerts
|

The DNA helicase–primase complex as a target for herpes viral infection

Abstract: Introduction The Herpesviridae are responsible for debilitating acute and chronic infections, and some members of this family are associated with human cancers. Conventional anti-herpesviral therapy targets the viral DNA polymerase and has been extremely successful; however, the emergence of drug-resistant virus strains, especially in neonates and immunocompromised patients, underscores the need for continued development of anti-herpes drugs. In this article, we explore an alternative target for antiviral ther… Show more

Help me understand this report

Search citation statements

Order By: Relevance

Paper Sections

Select...
1
1
1
1

Citation Types

0
36
0
1

Year Published

2013
2013
2021
2021

Publication Types

Select...
6
2
1

Relationship

0
9

Authors

Journals

citations
Cited by 39 publications
(37 citation statements)
references
References 119 publications
(151 reference statements)
0
36
0
1
Order By: Relevance
“…Not unexpectedly given its novel host-targeted mechanisms of action, peg-ArgI was effective at inhibiting drug resistant HSV-1. Similar to newly identified helicase-primase anti-herpetic drugs (Betz et al, 2002; Kleymann et al, 2002; Weller and Kuchta, 2013), peg-ArgI was superior to acyclovir in its ability to inhibit infectious viral yield, virus-induced cytopathic effect, and viral spread. However, unlike HSVprotein targeting helicase-primase inhibitors, peg-ArgI modulation of host arginine-associated metabolic pathways minimizes the likelihood that viruses could evolve resistance.…”
Section: Discussionmentioning
confidence: 80%
“…Not unexpectedly given its novel host-targeted mechanisms of action, peg-ArgI was effective at inhibiting drug resistant HSV-1. Similar to newly identified helicase-primase anti-herpetic drugs (Betz et al, 2002; Kleymann et al, 2002; Weller and Kuchta, 2013), peg-ArgI was superior to acyclovir in its ability to inhibit infectious viral yield, virus-induced cytopathic effect, and viral spread. However, unlike HSVprotein targeting helicase-primase inhibitors, peg-ArgI modulation of host arginine-associated metabolic pathways minimizes the likelihood that viruses could evolve resistance.…”
Section: Discussionmentioning
confidence: 80%
“…However, at the molar ratio of 1:1, which was supposed to be functional in vivo by structural information [27e29], DnaI showed no inhibition effect on ATPase activity of DnaB (data not shown). This may be explained by an assumption of competition between DnaI and ATP, since ATP hydrolysis was supposed to promote release of DnaC (homologous to DnaI Bst ) from DnaB in E. coli [30,31], conversely, the binding of ATP to DnaB may be inhibited by high concentration of DnaI. However, this assumption requires more work to be done.…”
Section: Investigations On the Effect Of Dnag Bst Dnai Bsu And Ssdnmentioning
confidence: 99%
“…For anyone new to the field of herpes virus DNA replication may I point you to the perfect introduction to this subject by the doyenne of herpes virus helicase-primase, Sandra K Weller and her co-author, Robert D Kuchta [1]. This is not only an 'expert' opinion in every sense but is also a lucid and readable account that brings a potentially rather dry subject to life.…”
Section: An Insight Into How Herpes Dna Replication Proteins Interactmentioning
confidence: 99%