Abstract
We previously reported the antiviral capacity of human serum albumin (HSA), which was modified by the introduction of a single (Suc-HSA) or two carboxylic groups (Aco-HSA) per lysine residue, yielding strongly negatively charged polypeptides, Here we report the antiviral effect of these modified HSAs on replication of primary HIV-1 isolates that differed with respect to syncytium-inducing (SI) capacity and cell tropism. Both Suc-HSA and Aco-HSA potently inhibited replication of primary HIV-1 variants, independent of the SI capacity of the HIV-I variant, with IC50 values in the range of 50 to 187 mu g/ml. The inhibition of the formation of syncytia and the absence of proviral DNA products in cells inoculated with HIV-1 in the presence of Suc-HSA or Aco-HSA pointed to interference at an early level in the virus replication cycle. The inhibitory capacity of Suc-HSA and Aco-HSA on primary HIV-1 variants suggests that these agents are potential candidates for use in antiviral therapy in HIV-infected individuals.
Original language | English |
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Pages (from-to) | 179-185 |
Number of pages | 7 |
Journal | Aids Research and Human Retroviruses |
Volume | 13 |
Issue number | 2 |
Publication status | Published - 20-Jan-1997 |
Keywords
- HUMAN-IMMUNODEFICIENCY-VIRUS
- RECOMBINANT SOLUBLE CD4
- AIDS-RELATED COMPLEX
- DEXTRAN SULFATE
- BIOLOGICAL PHENOTYPE
- CELL-CULTURE
- T4 ANTIGEN
- INFECTION
- RECEPTOR
- TROPISM