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Two parallel routes of the complement-mediated antibody-dependent enhancement of HIV-1 infection

Authors :
Tünde Hidvégi
Gérard J. Arlaud
Hartmut Hampl
Anna Erdei
Peter Späth
József Nemes
Eszter Ujhelyi
Ferenc Tóth
Jolán Kiss
Berhane Ghebrehiwet
Judit Szabó
Nicole M. Thielens
Zoltán Prohászka
Krisztina Kerekes
Manfred P. Dierich
George Füst
Source :
AIDS. 11:949-958
Publication Year :
1997
Publisher :
Ovid Technologies (Wolters Kluwer Health), 1997.

Abstract

Objective To study the mechanism of the complement-mediated antibody-dependent enhancement (C'-ADE) of HIV infection which may play a significant role in the progression of HIV-disease. Methods In vitro complement activating and complement-mediated HIV-infection enhancing abilities of three human anti-gp41 monoclonal antibodies (MAb) were tested. C'-ADE was estimated using HIV-1IIIB and CR2 (CD21)-carrying MT-4 target cells. Normal human serum (NHS), purified C1q, C1q-deficient (C1qD) and C2-deficient (C2D) human sera were applied as complement sources. Results All MAb mediated increased C1q binding to solid-phase gp41. All MAb had a marked dose-dependent and strictly complement-mediated HIV-infection enhancing effect. Mixtures of the MAb with purified C1q also significantly increased HIV-1 infection. C1qD serum had a markedly lower enhancing effect than NHS, which could be raised to normal level by addition of purified C1q. Pretreatment of the target cells with anti-CR2 antibodies only partially inhibited the enhancing effect of the MAb plus normal human serum. Conclusion These novel findings indicate that besides the well-known facilitation of entry of HIV-1 by the interaction between virus-bound C3 fragments and CR2 present on the target cells, fixation of C1q to intact virions also results in an enhanced productive HIV-1 infection in the MT-4 cell cultures.

Details

ISSN :
02699370
Volume :
11
Database :
OpenAIRE
Journal :
AIDS
Accession number :
edsair.doi.dedup.....027a94ad8ba9a1e3e305a1dc7c4a6ffd
Full Text :
https://doi.org/10.1097/00002030-199708000-00002