About: Cell-dependent interference of a series of new 6-aminoquinolone derivatives with viral (HIV/CMV) transactivation

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À propos de : Cell-dependent interference of a series of new 6-aminoquinolone derivatives with viral (HIV/CMV) transactivation Goto Sponge NotDistinct Permalink

Attributs	Valeurs
type	work Article
Is Part Of	http://hub.abes.fr/oup/periodical/jac/2005/volume_56/issue_5/w
Subject	TAR ORIGINAL ARTICLES latency Tat
Title	Cell-dependent interference of a series of new 6-aminoquinolone derivatives with viral (HIV/CMV) transactivation
has manifestation of work	http://hub.abes.fr/oup/periodical/jac/2005/volume_56/issue_5/101093jacdki328/m/print http://hub.abes.fr/oup/periodical/jac/2005/volume_56/issue_5/101093jacdki328/m/web
related by	http://hub.abes.fr/oup/periodical/jac/2005/volume_56/issue_5/101093jacdki328/authorship/5 http://hub.abes.fr/oup/periodical/jac/2005/volume_56/issue_5/101093jacdki328/authorship/6 http://hub.abes.fr/oup/periodical/jac/2005/volume_56/issue_5/101093jacdki328/authorship/2 http://hub.abes.fr/oup/periodical/jac/2005/volume_56/issue_5/101093jacdki328/authorship/3 http://hub.abes.fr/oup/periodical/jac/2005/volume_56/issue_5/101093jacdki328/authorship/9 http://hub.abes.fr/oup/periodical/jac/2005/volume_56/issue_5/101093jacdki328/authorship/1 http://hub.abes.fr/oup/periodical/jac/2005/volume_56/issue_5/101093jacdki328/authorship/4 http://hub.abes.fr/oup/periodical/jac/2005/volume_56/issue_5/101093jacdki328/authorship/7 http://hub.abes.fr/oup/periodical/jac/2005/volume_56/issue_5/101093jacdki328/authorship/8
Author	De Clercq Erik Tabarrini Oriana Snoeck R. Andrei G. Stevens Miguel Fravolini Arnaldo Pannecouque Christophe Balzarini Jan Cecchetti Violetta
Abstract	Objectives: Quinolone derivatives have been shown to inhibit human immunodeficiency virus (HIV) replication at the transcriptional level. Recently, a series of new 6-aminoquinolones that are endowed with more pronounced anti-HIV activities compared with the formerly reported quinolone derivatives have been published. These potent 6-aminoquinolones were further evaluated for their broad-spectrum antiviral properties. Methods: Latently HIV-1-infected cell lines as well as cytomegalovirus (CMV)-infected fibroblasts were used to evaluate the antiviral potency of the 6-aminoquinolone derivatives. Additionally green fluorescent protein (GFP) transactivation experiments using different promoters were conducted. Results: The compounds completely suppressed tumour necrosis factor alpha (TNF-α)- and phorbol 12-myristate 13-acetate (PMA)-induced HIV-1 expression in latently HIV-1-infected OM-10.1 and U1 cell lines at non-toxic concentrations. In addition, HIV-1 mRNA production was dramatically suppressed in both cell lines in a dose-dependent manner. In the same concentration range, the compounds inhibited TNF-α release from PMA-induced OM-10.1 cells but allowed TNF-α production from PMA-induced U1 cells at all concentrations tested. The 6-aminoquinolone derivatives were not only inhibitory to the Tat-mediated transactivation of the HIV-1 LTR promoter, but were also found to interfere in a cell-dependent way with the transactivation process mediated from the human CMV immediate early and the human EF-1α promoter. Additionally, the 6-aminoquinolone derivatives were also found to be inhibitory to CMV replication in fibroblast cells. Conclusions: It thus appears that the antiviral spectrum of this class of compounds is not confined to the specific inhibition of HIV but encompasses CMV as well. This broad-spectrum activity window might provide an interesting platform for future applications for the 6-aminoquinolone derivatives.
article type	research-article
is part of this journal	Journal of Antimicrobial Chemotherapy

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