Because of the importance of monocytes/macrophages (M/M) as an in vivo reservoir of human immunodeficiency virus (HIV), a study was done to investigate whether viral replication in chronically infected macrophages (HIV M/M) could be inhibited by various drugs, including U-75875, an inhibitor of HIV protease. HIV replication in M/M and in chronically infected T cells was dramatically decreased by U-75875, while other drugs, including zidovudine, interferon-α, and an antisense oligodeoxynucleotide against the rev gene, were effective antiviral agents only in de novo-infected cells. Virus titer in HIV M/M was reduced ∼105-fold by nontoxic concentrations of U-75875, while no effect on HIV DNA or virus antigen expression on cell membrane was achieved in M/M infected either chronically or de novo. Thus, U-75875 essentially worked against late stages of viral replication. These data support the use of protease inhibitors, alone or in combination, in the therapy of HIV-infected patients. © 1993 by The University of Chicago.

Perno, C.-., Bergamini, A., Pesce, C.d., Milanese, G., Capozzi, M., Aquaro, S., et al. (1993). Inhibition of the Protease of Human Immunodeficiency Virus Blocks Replication and Infectivity of the Virus in Chronically Infected Macrophages. THE JOURNAL OF INFECTIOUS DISEASES, 168(5), 1148-1156 [10.1093/infdis/168.5.1148].

Inhibition of the Protease of Human Immunodeficiency Virus Blocks Replication and Infectivity of the Virus in Chronically Infected Macrophages

Bergamini, A.;Pesce, C. D.;Capozzi, M.;Aquaro, S.;Rocchi, G.;Garaci, E.;
1993-01-01

Abstract

Because of the importance of monocytes/macrophages (M/M) as an in vivo reservoir of human immunodeficiency virus (HIV), a study was done to investigate whether viral replication in chronically infected macrophages (HIV M/M) could be inhibited by various drugs, including U-75875, an inhibitor of HIV protease. HIV replication in M/M and in chronically infected T cells was dramatically decreased by U-75875, while other drugs, including zidovudine, interferon-α, and an antisense oligodeoxynucleotide against the rev gene, were effective antiviral agents only in de novo-infected cells. Virus titer in HIV M/M was reduced ∼105-fold by nontoxic concentrations of U-75875, while no effect on HIV DNA or virus antigen expression on cell membrane was achieved in M/M infected either chronically or de novo. Thus, U-75875 essentially worked against late stages of viral replication. These data support the use of protease inhibitors, alone or in combination, in the therapy of HIV-infected patients. © 1993 by The University of Chicago.
1993
Pubblicato
Rilevanza internazionale
Articolo
Esperti anonimi
Settore MED/07
Settore MEDS-03/A - Microbiologia e microbiologia clinica
English
Perno, C.-., Bergamini, A., Pesce, C.d., Milanese, G., Capozzi, M., Aquaro, S., et al. (1993). Inhibition of the Protease of Human Immunodeficiency Virus Blocks Replication and Infectivity of the Virus in Chronically Infected Macrophages. THE JOURNAL OF INFECTIOUS DISEASES, 168(5), 1148-1156 [10.1093/infdis/168.5.1148].
Perno, C-; Bergamini, A; Pesce, Cd; Milanese, G; Capozzi, M; Aquaro, S; Thaisrivongs, S; Tarpley, Wg; Zon, G; D?agostini, C; Rocchi, G; Garaci, E; Cal...espandi
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/2108/413285
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