CD4 mimetic miniproteins: potent anti-HIV compounds with promising activity as microbicides

doi:10.1093/jac/dkn042

JAC Advance Access originally published online on February 12, 2008
Journal of Antimicrobial Chemotherapy 2008 61(4):818-826; doi:10.1093/jac/dkn042

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© The Author 2008. 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

Original research

CD4 mimetic miniproteins: potent anti-HIV compounds with promising activity as microbicides

Yven Van Herrewege¹, Laurence Morellato², Anne Descours², Laetitia Aerts¹, Jo Michiels¹, Leo Heyndrickx¹, Loïc Martin² and Guido Vanham¹^,3^,*

¹ Virology Unit, Department of Microbiology, Institute of Tropical Medicine, Antwerp, Belgium ² CEA, iBiTecS, Service d’Ingénierie Moléculaire des Protéines, Gif sur Yvette F-91191, France ³ Department of Biomedical Sciences, University of Antwerp, Antwerp, Belgium

Received 19 October 2007; returned 3 December 2007; revised 28 December 2007; accepted 16 January 2008

^* Correspondence address. Virology Unit, Institute of Tropical Medicine, 155 Nationalestraat, B-2000 Antwerp, Belgium. Tel: +32-3-247-62-28; Fax: +32-3-247-63-33; E-mail: gvanham{at}itg.be

Objectives: The antiviral activity of CD4 miniproteins was evaluated aspotential HIV microbicides, using relevant in vitro models.

Methods: Compounds were tested in a single-cycle HIV-1 pseudovirus assayand against replication competent HIV-1 in co-cultures of monocyte-deriveddendritic cells (MO-DC) and CD4+ T cells. Cytotoxic activitywas evaluated in an MTT assay.

Results: Monomeric miniproteins (M47 and M48) showed 50% effective concentration(EC₅₀) values of 79–105 nM against a subtype B, CCR5 co-receptor-usingBa-L pseudovirus. Higher activity was found for the dimericminiproteins M48D30, M48D50 and M48D100 (EC₅₀ between 15 and30 nM), in contrast to the tetrameric miniproteins M48T30, M48T50and M48T100 (EC₅₀ between 107 and 377 nM). The hetero-bivalentminiprotein M48-Hep and miniproteins that targeted the Phe-43cavity on gp120 (M48-U1, M48-U2 and M48-U3) were highly active,with EC₅₀ values as low as 2 nM for M48-U1. All miniproteinsshowed high activity against CCR5 or CXCR4 co-receptor-usingsubtype B and CRF-01_A/E pseudoviruses. Many early M48-basedcompounds were much less active against subtype C pseudoviruses,whereas M48-U compounds that targeted the Phe-43 cavity werevery active against all pseudoviruses, including subtype C.In MO-DC/CD4+ T cell co-cultures with replication-competentHIV-1 Ba-L, EC₅₀ values ranged between 13 and 1719 nM dependingon the miniprotein, with M48-U1, M48-U2 and M48-U3 again beingthe most potent. Importantly, the latter compounds completelyprevented viral replication by treating the cultures from 2h before until 24 h after infection, at non-toxic concentrationsof 66–6564 nM.

Conclusions: These novel CD4 miniproteins might constitute a promising classof HIV microbicides.

Keywords: vaginal microbicides , in vitro activity , sexual transmission

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