The lectins griffithsin, cyanovirin-N and scytovirin inhibit HIV-1 binding to the DC-SIGN receptor and transfer to CD4+ cells

Alexandre, Kabamba B.; Gray, Elin S.; Mufhandu, Hazel Tumelo; McMahon, James B.; Chakauya, Ereck; O’Keefe, Barry R.; Chikwamba, Rachel; Morris, Lynn

doi:10.1016/j.virol.2011.12.001

Cited by 52 publications

(52 citation statements)

References 65 publications

(109 reference statements)

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“…Indeed, 2 h is enough for HIV endocytosis to reach saturation in permissive cell lines, 12 while 24 h is time enough for replication. 13 And in our study the 5-fold increase of HIV RNA associated with cells from 2 h to 24 h might seem a sign of replication. But virus in the infected cells presumably have not replicated because (1) the B-THP-1/DC-SIGN cell line is almost identical to the Raji/DC-SIGN 14 and (2) endocytosis of HIV in Raji/DC-SIGN cells is not observed and they are not permissive to HIV infection.…”

supporting

confidence: 49%

“…12 Inhibitors of HIV infection and transinfection via the DC-SIGN lectin receptor have been tested only in preclinical studies. [13][14][15] Development or application of known drugs for the inhibition of HIV/DC-SIGN interaction may help in decreasing transinfection of T cells and in preventing the infection of DCs that serve as a long-term reservoir of HIV.…”

mentioning

confidence: 99%

“…DC-SIGN inhibitors are of special interest as a means of preventing DC infection and CD4 + T cell transinfection by HIV. Many potential DC-SIGN inhibitors are in various stages of research, [13][14][15] and approaches for the high-throughput screening of potential inhibitors are being developed. 37 Our earlier studies on human macrophages 38 demonstrate that dextrans are also inhibitors of the interaction of HIV with another C-type lectin MR (CD206).…”

mentioning

confidence: 99%

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Short Communication: Inhibition of DC-SIGN-Mediated HIV-1 Infection by Complementary Actions of Dendritic Cell Receptor Antagonists and Env-Targeting Virus Inactivators

Pustylnikov

Dave

Khan

et al. 2016

AIDS Research and Human Retroviruses

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The DC-SIGN receptor on human dendritic cells interacts with HIV gp120 to promote both infection of antigenpresenting cells and transinfection of T cells. We hypothesized that in DC-SIGN-expressing cells, both DC-SIGN ligands such as dextrans and gp120 antagonists such as peptide triazoles would inhibit HIV infection with potential complementary antagonist effects. To test this hypothesis, we evaluated the effects of dextran (D66), isomaltooligosaccharides (D06), and several peptide triazoles (HNG156, K13, and UM15) on HIV infection of B-THP-1/DC-SIGN cells. In surface plasmon resonance competition assays, D66 (IC 50 = 35.4 lM) and D06 (IC 50 = 3.4 mM) prevented binding of soluble DC-SIGN to immobilized mannosylated bovine serum albumin (BSA). An efficacious dose-dependent inhibition of DC-SIGN-mediated HIV infection in both pretreatment and posttreatment settings was observed, as indicated by inhibitory potentials (EC 50 ) [D66 (8 lM), D06 (48 mM), HNG156 (40 lM), UM15 (100 nM), and K13 (25 nM)]. Importantly, both dextrans and peptide triazoles significantly decreased HIV gag RNA levels [D66 (7-fold), D06 (13-fold), HNG156 (7-fold), K-13 (3-fold), and UM15 (6-fold)]. Interestingly, D06 at the highest effective concentration showed a 14-fold decrease of infection, while its combination with 50 lM HNG156 showed a 26-fold decrease. Hence, these compounds can combine to inactivate the viruses and suppress DC-SIGN-mediated virus-cell interaction that as shown earlier leads to dendritic cell HIV infection and transinfection dependent on the DC-SIGN receptor.

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confidence: 49%

mentioning

confidence: 99%

mentioning

confidence: 99%

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Short Communication: Inhibition of DC-SIGN-Mediated HIV-1 Infection by Complementary Actions of Dendritic Cell Receptor Antagonists and Env-Targeting Virus Inactivators

Pustylnikov

Dave

Khan

et al. 2016

AIDS Research and Human Retroviruses

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“…Although DENV has high mannose-type glycans on the E-protein, there was no antiviral activity of AH against DENV infection. Other CBAs such as microvirin, griffithsin and Banlec have been shown to exhibit potent activity against HIV replication [93][94][95], but these CBAs did not show antiviral activity against DENV. Previously, it has been shown that the CBAs HHA, GNA and UDA also target the N-glycans of other viruses, such as HIV, HCV [79] and HCMV [80].…”

Section: Broad Antiviral Activity Of Cbas Against Denvmentioning

confidence: 99%

Broad Antiviral Activity of Carbohydrate-Binding Agents Against Dengue Virus Infection

Alen¹,

Schols²

2012

Carbohydrates - Comprehensive Studies on Glycobiology and Glycotechnology

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“…and spleens (C) weights were measured relatively to body weight at sacrifice. [29,31,37,142,189,190].…”

Section: Discussionmentioning

confidence: 99%

Evaluation of the safety and pharmacokinetic profile of the broad spectrum antiviral lectin Griffithsin.

Barton¹,

Lynn²

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The lectins griffithsin, cyanovirin-N and scytovirin inhibit HIV-1 binding to the DC-SIGN receptor and transfer to CD4+ cells

Cited by 52 publications

References 65 publications

Short Communication: Inhibition of DC-SIGN-Mediated HIV-1 Infection by Complementary Actions of Dendritic Cell Receptor Antagonists and Env-Targeting Virus Inactivators

Short Communication: Inhibition of DC-SIGN-Mediated HIV-1 Infection by Complementary Actions of Dendritic Cell Receptor Antagonists and Env-Targeting Virus Inactivators

Broad Antiviral Activity of Carbohydrate-Binding Agents Against Dengue Virus Infection

Evaluation of the safety and pharmacokinetic profile of the broad spectrum antiviral lectin Griffithsin.

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