Structural requirements for and consequences of an antiviral porphyrin binding to the V3 loop of the human immunodeficiency virus (HIV‐1) envelope glycoprotein gp120

Neurath, A. R.; Strick, N.; Debnath, Asim K.

doi:10.1002/jmr.300080604

Cited by 32 publications

(17 citation statements)

References 75 publications

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“…These results showed that an important target of these compounds is the viral Env protein. Neurath et al (26,27) have correlated the anti-HIV activity by using an assay for cytotoxicity on a T-cell line that measures the inhibition of the interaction between gp120 and antibodies specific for the V3 hypervariable loop of this protein. In this series of approximately 20 porphyrins from both the natural and synthetic classes, there was no clear correlation overall between inhibition of antibody binding to gp120 and overall activity in an antiviral assay.…”

Section: Discussionmentioning

confidence: 99%

“…Protoporphyrin (3), hemin (22,25), and other related natural porphyrins and metalloporphyrins (11-13, 16, 25-29) have been shown to have activity against HIV in the micromolar range in such antiviral assays. Sulfonated derivatives of tetraphenylporphyrin have also been shown to be active (16,28,38) as have other selected tetra-arylporphyrins (11,15,16,(26)(27)(28). The mechanisms of action and the stage in the viral life cycle at which the porphyrins exert their inhibitory effects on HIV-1 are not well understood.…”

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confidence: 99%

“…A third mechanism by which porphyrins may inhibit HIV is via interaction with the envelope (Env) protein. Binding to a sequence in the V3 loop of the HIV-1 Env protein has been reported as a possible mechanism by which such compounds could inactivate viral infectivity (12,(25)(26)(27)38). The V3 loop is a principal antigenic determinant of the external domain of the viral Env protein and is thought to play an important role in viral attachment and penetration (6,36,44,47,50).…”

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confidence: 99%

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Inactivation of Human Immunodeficiency Virus Type 1 by Porphyrins

Vzorov¹,

Dixon

Trommel

et al. 2002

Antimicrob Agents Chemother

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We have evaluated the anti-human immunodeficiency virus (HIV) activity of a series of natural and synthetic porphyrins to identify compounds that could potentially be used as microbicides to provide a defense against infection by sexually transmitted virus. For assays we used an epithelial HeLa-CD4 cell line with an integrated long terminal repeat-␤-galactosidase gene. For structure-activity analysis, we divided the porphyrins tested into three classes: (i) natural porphyrins, (ii) metallo-tetraphenylporphyrin tetrasulfonate (metallo-TPPS4) derivatives, and (iii) sulfonated tetra-arylporphyrin derivatives. None of the natural porphyrins studied reduced infection by more than 80% at a concentration of 5 g/ml in these assays. Some metal chelates of TPPS4 were more active, and a number of sulfonated tetra-aryl derivatives showed significantly higher activity. Some of the most active compounds were the sulfonated tetranaphthyl porphyrin (TNapPS), sulfonated tetra-anthracenyl porphyrin (TAnthPS), and sulfonated 2,6-difluoro-meso-tetraphenylporphine [TPP(2,6-F2)S] and its copper chelate [TPP(2,6-F2)S,Cu], which reduced infection by 99, 96, 94, and 96%, respectively. Our observations indicate that at least some of these compounds are virucidal, i.e., that they render the virus noninfectious. The active compounds were found to inhibit binding of the HIV type 1 gp120 to CD4 and also to completely inhibit the ability of Env proteins expressed from recombinant vectors to induce cell fusion with receptor-bearing target cells. These results support the conclusion that modified porphyrins exhibit substantial activity against HIV and that their target is the HIV Env protein.

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Section: Discussionmentioning

confidence: 99%

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Inactivation of Human Immunodeficiency Virus Type 1 by Porphyrins

Vzorov¹,

Dixon

Trommel

et al. 2002

Antimicrob Agents Chemother

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“…For experiments described in Fig. 6, a full length V3loop peptide (1 mg in 0.5 mL PBS) from HIV-1 rrm gp120 (Neurath et al, 1995b) was reduced with 10 mM 2-mercaptoethanol (2-ME) for 1 h at 25°C. The reduced peptide was separated from excess 2-ME by molecular exclusion chromatography on Sephadex G-10 (Pharmacia).…”

Section: Biotinylation Of 3hp-f3-mentioning

confidence: 99%

3-Hydroxyphthaloyl-β-Lactoglobulin. I. Optimization of Production and Comparison with other Compounds Considered for Chemoprophylaxis of Mucosally Transmitted Human Immunodeficiency Virus Type 1

Neurath

Debnath

Strick

et al. 1997

Antivir Chem Chemother

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Modification of the major bovine whey protein, β-lactoglobulin (β-LG) by 3-hydroxyphthalic anhydride (3HP) leads to the generation of a potent inhibitor of infection by human immunodeficiency virus (HIV) types 1 and 2, designated 3HP-β-LG. 3HP-β-LG also has antiviral activity against herpesviruses, albeit at concentrations exceeding those required for inhibition of HIV-1 infection. The topical application of 3HP-β-LG to decrease the rate of sexual transmission of HIV and other sexually transmitted viruses worldwide is being considered. Results presented here: (i) define the conditions for chemical modification of β-LG by 3HP, resulting in 3HP-β-LG with optimum anti-HIV-1 activity; (ii) show that β-LG, prior to chemical modification, or 3HP-β-LG can be exposed to the elevated temperatures used to pasteurize milk without adversely affecting anti-HIV-1 activity; (iii) provide evidence that 3HP-β-LG is a more potent anti-HIV-1 compound than sulphated polysaccharides, other candidate compounds considered as prophylactic agents to prevent sexual transmission of HIV-1; and (iv) confirm that the primary target for 3HP-β-LG is CD4, although binding to the HIV-1 envelope protein gp120 was also observed and contributed to the antiviral activity of 3HP-β-LG.

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“…Attempts to gain better understanding of the structure of the third variable domain, designated as V3 loop, of the human immunodeficiency virus (HIV-1) gp120 envelope glycoprotein, a target for anti-HIV drug discovery [12][13][14], was the principal reason for us to model disulfide bonded loops in proteins. This loop, bonded by a pair of invariant cysteines, has been shown to play an important role in virus entry into CD4+ cells and in the tropism and infectivity of HIV-1 [15].…”

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A ′Fragment Fitting Approach′ to Model Disulfide Loops by Utilizing Homologous Peptide Fragments from Unrelated Proteins of Known Structures: Application to the V3 Loop of the HIV-1 Envelope Glycoprotein gp120

Debnath

1996

J Mol Med

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Structural requirements for and consequences of an antiviral porphyrin binding to the V3 loop of the human immunodeficiency virus (HIV‐1) envelope glycoprotein gp120

Cited by 32 publications

References 75 publications

Inactivation of Human Immunodeficiency Virus Type 1 by Porphyrins

Inactivation of Human Immunodeficiency Virus Type 1 by Porphyrins

3-Hydroxyphthaloyl-β-Lactoglobulin. I. Optimization of Production and Comparison with other Compounds Considered for Chemoprophylaxis of Mucosally Transmitted Human Immunodeficiency Virus Type 1

A ′Fragment Fitting Approach′ to Model Disulfide Loops by Utilizing Homologous Peptide Fragments from Unrelated Proteins of Known Structures: Application to the V3 Loop of the HIV-1 Envelope Glycoprotein gp120

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