Griffithsin Protects Mice from Genital Herpes by Preventing Cell-to-Cell Spread

Nixon, Briana G.; Stefanidou, Martha; Mesquita, Pedro M. M.; Fakioglu, Esra; Segarra, Theodore J.; Rohan, Lisa C.; Halford, William P.; Palmer, Kenneth E.; Herold, Betsy C.

doi:10.1128/jvi.00012-13

Cited by 98 publications

(158 citation statements)

References 54 publications

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“…The increased susceptibility was associated with modest increases in inflammatory mediators in the genital tract and disruption of the epithelial barrier. In contrast, 1% TFV gel, 0.5% PRO 2000, and 0.1% griffithsin gel did not increase the risk of HSV infection in this model (15,17,19). These findings suggest that this relatively inexpensive small-animal model may provide a biomarker of microbicide safety.…”

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confidence: 67%

Vaginally Delivered Tenofovir Disoproxil Fumarate Provides Greater Protection than Tenofovir against Genital Herpes in a Murine Model of Efficacy and Safety

Nixon

Jandl

Teller

et al. 2014

Antimicrob Agents Chemother

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dIncreased susceptibility to genital herpes in medroxyprogesterone-treated mice may provide a surrogate of increased HIV risk and a preclinical biomarker of topical preexposure prophylaxis safety. We evaluated tenofovir disoproxil fumarate (TDF) in this murine model because an intravaginal ring eluting this drug is being advanced into clinical trials. To avoid the complications of surgically inserting a ring, hydroxyethylcellulose (HEC)-stable formulations of TDF were prepared. One week of twice-daily 0.3% TDF gel was well tolerated and did not result in any increase in HSV-2 susceptibility but protected mice from herpes simplex virus 2 (HSV-2) disease compared to mice treated with the HEC placebo gel. No significant increase in inflammatory cytokines or chemokines in vaginal washes or change in cytokine, chemokine, or mitochondrial gene expression in RNA extracted from genital tract tissue was detected. To further evaluate efficacy, mice were treated with gel once daily beginning 12 h prior to high-dose HSV-2 challenge or 2 h before and after viral challenge (BAT24 dosing). The 0.3% TDF gel provided significant protection compared to the HEC gel following either daily (in 9/10 versus 1/10 mice, P < 0.01) or BAT24 (in 14/20 versus 4/20 mice, P < 0.01) dosing. In contrast, 1% tenofovir (TFV) gel protected only 4/10 mice treated with either regimen. Significant protection was also observed with daily 0.03% TDF compared to HEC. Protection was associated with greater murine cellular permeability of radiolabeled TDF than of TFV. Together, these findings suggest that TDF is safe, may provide substantially greater protection against HSV than TFV, and support the further clinical development of a TDF ring.

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confidence: 67%

Vaginally Delivered Tenofovir Disoproxil Fumarate Provides Greater Protection than Tenofovir against Genital Herpes in a Murine Model of Efficacy and Safety

Nixon

Jandl

Teller

et al. 2014

Antimicrob Agents Chemother

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“…We observed that all EFs were nontoxic to cells in all three vaginal cell lines, with the cells showing greater than 93% viability after treatment, indicating their potential for future translation in vivo. We expected favorable cytotoxicity results, as a feature of this platform is that an FDA-approved polymer is used with the promising biologic GRFT, which has demonstrated outstanding safety profiles both in vitro and in vivo (46,56). These results are particularly important for translation in vivo, as cytotoxicity and inflammation have been shown to increase the propensity for infection in clinical trials (2)(3)(4)(5)7).…”

Section: Discussionmentioning

confidence: 99%

“…For the adhesive surface moiety, the biological antiviral lectin GRFT was selected, as it has been demonstrated to bind to and to have antiviral efficacy against a variety of viruses, including HIV-1 and HSV-2 (44)(45)(46)(47)(48)(49)(50)(51). Previous work by our groups has demonstrated that GRFT has an exceptionally potent HIV-1-inhibitory capability as a multivalent front-line HIV entry inhibitor (49)(50)(51)(52)(53)(54), and of the biologically based inhibitors, GRFT has exceptionally potent anti-HIV activity, inactivating HIV-1 immediately upon contact (51,52).…”

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confidence: 99%

“…Previous work by our groups has demonstrated that GRFT has an exceptionally potent HIV-1-inhibitory capability as a multivalent front-line HIV entry inhibitor (49)(50)(51)(52)(53)(54), and of the biologically based inhibitors, GRFT has exceptionally potent anti-HIV activity, inactivating HIV-1 immediately upon contact (51,52). Furthermore, a 0.1% GRFT gel was shown to protect mice against intravaginal HSV-2 challenge, making it a leading protein-based antiviral candidate providing multipurpose protection against both HSV-2 and HIV-1 STIs (46). Moreover, to the benefit of intravaginal administration, GRFT lacks the capacity to induce proinflammatory cytokines in human peripheral blood mononuclear cells, is resistant to a broad array of human proteases, and is stable in the presence of culture medium from vaginal microbes, retaining anti-HIV activity for up to 10 days, even when some of the six carbohydrate binding sites are occupied (55,56).…”

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confidence: 99%

“…Mechanistically, GRFT has been shown to bind the terminal mannose N-linked glycan residues on viral envelope surfaces (51,55,(57)(58)(59). For HIV-1, GRFT is believed to bind to gp120 on the virion and neutralize the virus at entry, whereas for HSV-2, GRFT inhibits infection via the glycoprotein (gP) conformational changes expressed during cell-to-cell spread (46). For both HIV and HSV (among other viruses), these strong interactions between virus gPs and GRFT result in an irreversible biological effect (56) that we hypothesize inactivates the virus, resulting in physicochemical protection.…”

mentioning

confidence: 99%

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Griffithsin-Modified Electrospun Fibers as a Delivery Scaffold To Prevent HIV Infection

Grooms

Vuong

Tyo

et al. 2016

Antimicrob Agents Chemother

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Despite current prophylactic strategies, sexually transmitted infections (STIs) remain significant contributors to global health challenges, spurring the development of new multipurpose delivery technologies to protect individuals from and treat virus infections. However, there are few methods currently available to prevent and no method to date that cures human immunodeficiency virus (HIV) infection or combinations of STIs. While current oral and topical preexposure prophylaxes have protected against HIV infection, they have primarily relied on antiretrovirals (ARVs) to inhibit infection. Yet continued challenges with ARVs include user adherence to daily treatment regimens and the potential toxicity and antiviral resistance associated with chronic use. The integration of new biological agents may avert some of these adverse effects while also providing new mechanisms to prevent infection. Of the biologic-based antivirals, griffithsin (GRFT) has demonstrated potent inhibition of HIV-1 (and a multitude of other viruses) by adhering to and inactivating HIV-1 immediately upon contact. In parallel with the development of GRFT, electrospun fibers (EFs) have emerged as a promising platform for the delivery of agents active against HIV infection. In the study described here, our goal was to extend the mechanistic diversity of active agents and electrospun fibers by incorporating the biologic GRFT on the EF surface rather than within the EFs to inactivate HIV prior to cellular entry. We fabricated and characterized GRFT-modified EFs (GRFT-EFs) with different surface modification densities of GRFT and demonstrated their safety and efficacy against HIV-1 infection in vitro. We believe that EFs are a unique platform that may be enhanced by incorporation of additional antiviral agents to prevent STIs via multiple mechanisms. N ewly acquired sexually transmitted infections (STIs) affect 340 million people per year (1-3) and exert a significant impact on global health. Human immunodeficiency virus type 1 (HIV-1) affects ϳ35 million people globally (2-5), while untreated STIs, such as those caused by herpes simplex virus 2 (HSV-2), can enhance both the acquisition and the transmission of HIV and other agents of STIs by 2-to 4-fold (6, 7). In light of the findings of recent clinical trials, a specific, multipurpose prevention technology that has the ability to prevent multiple STIs using one delivery platform and that also increases user adherence urgently needs to be developed (8-18). In the study described here, we sought to shift current topical preexposure prophylaxis (PrEP) paradigms by integrating a multipurpose biological delivery approach to debilitate and inactivate HIV.Our long-term goal is to develop a multipurpose biologically inspired electrospun fiber (EF) prevention technology that takes cues from the innate microenvironment of the female reproductive tract to more strategically narrow the gaps in microbicide efficacy. In this work, we evaluated the potential of polymeric EF scaffolds surface modified with the po...

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Promising Marine Molecules in Pharmacology

Bourguet‐Kondracki

Kornprobst²

2014

Outstanding Marine Molecules

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Griffithsin Protects Mice from Genital Herpes by Preventing Cell-to-Cell Spread

Cited by 98 publications

References 54 publications

Vaginally Delivered Tenofovir Disoproxil Fumarate Provides Greater Protection than Tenofovir against Genital Herpes in a Murine Model of Efficacy and Safety

Vaginally Delivered Tenofovir Disoproxil Fumarate Provides Greater Protection than Tenofovir against Genital Herpes in a Murine Model of Efficacy and Safety

Griffithsin-Modified Electrospun Fibers as a Delivery Scaffold To Prevent HIV Infection

Promising Marine Molecules in Pharmacology

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