Ebanga™: The most recent FDA-approved drug for treating Ebola

Taki, Elahe; Ghanavati, Roya; Navidifar, Tahereh; Dashtbin, Shirin; Heidary, Mohsen; Moghadamnia, Marjan

doi:10.3389/fphar.2023.1083429

Cited by 9 publications

(15 citation statements)

References 34 publications

(72 reference statements)

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“…Substantial progress has been made in developing vaccines and treatments against EBOV (within species O. zairense), with two vaccines and two monoclonal antibody (mAb)-based treatments licensed for human use (10)(11)(12)(13).…”

Section: Rationalementioning

confidence: 99%

“…Substantial progress has been made in developing vaccines and treatments against EBOV (within species O. zairense ), with two vaccines and two monoclonal antibody (mAb)–based treatments licensed for human use ( 10 – 13 ). However, there are still no medical countermeasures against Marburg virus (MARV) or other ebolaviruses such as Bundibugyo virus (BDBV), Sudan virus (SUDV), or Tai forest virus (TAFV) that are approved for human use.…”

mentioning

confidence: 99%

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Oral administration of obeldesivir protects nonhuman primates against Sudan ebolavirus

Cross,

Woolsey,

Chu

et al. 2024

Science

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Obeldesivir (ODV, GS-5245) is an orally administered prodrug of the parent nucleoside of remdesivir (RDV) and is presently in phase 3 trials for COVID-19 treatment. In this work, we show that ODV and its circulating parent nucleoside metabolite, GS-441524, have similar in vitro antiviral activity against filoviruses, including Marburg virus, Ebola virus, and Sudan virus (SUDV). We also report that once-daily oral ODV treatment of cynomolgus monkeys for 10 days beginning 24 hours after SUDV exposure confers 100% protection against lethal infection. Transcriptomics data show that ODV treatment delayed the onset of inflammation and correlated with antigen presentation and lymphocyte activation. Our results offer promise for the further development of ODV to control outbreaks of filovirus disease more rapidly.

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Section: Rationalementioning

confidence: 99%

mentioning

confidence: 99%

Oral administration of obeldesivir protects nonhuman primates against Sudan ebolavirus

Cross,

Woolsey,

Chu

et al. 2024

Science

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“…Monoclonal antibodies (mAbs) are a promising therapeutic modality for filoviruses and other viral pathogens [5][6][7][8][9][10][11]. MAbs are generally well-tolerated with few off-target effects, have long in vivo half-life, and-especially important for viral diseases-the capacity to recruit immune mediators and clear infected cells via their Fc region.…”

Section: Introductionmentioning

confidence: 99%

“…MAb therapies have been approved for treatment of EBOV, SARS-CoV2, and respiratory syncytial virus (RSV), and are under advanced development for other viral diseases. Inmazeb consists of a cocktail of three EBOV mAbs, and Ebanga is a single-component therapy [7,8]. Other advanced mAb filovirus therapies include the broad-spectrum two-component MBP134 cocktail, which has been demonstrated to protect non-human primates from lethal challenge by EBOV, BDBV, and SUDV, and MBP091, a MARV-and RAVV-specific monotherapy [12][13][14].…”

Section: Introductionmentioning

confidence: 99%

Design and characterization of protective pan-ebolavirus and pan-filovirus bispecific antibodies

Wirchnianski,

Nyakatura,

Herbert

et al. 2024

PLoS Pathog

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Monoclonal antibodies (mAbs) are an important class of antiviral therapeutics. MAbs are highly selective, well tolerated, and have long in vivo half-life as well as the capacity to induce immune-mediated virus clearance. Their activities can be further enhanced by integration of their variable fragments (Fvs) into bispecific antibodies (bsAbs), affording simultaneous targeting of multiple epitopes to improve potency and breadth and/or to mitigate against viral escape by a single mutation. Here, we explore a bsAb strategy for generation of pan-ebolavirus and pan-filovirus immunotherapeutics. Filoviruses, including Ebola virus (EBOV), Sudan virus (SUDV), and Marburg virus (MARV), cause severe hemorrhagic fever. Although there are two FDA-approved mAb therapies for EBOV infection, these do not extend to other filoviruses. Here, we combine Fvs from broad ebolavirus mAbs to generate novel pan-ebolavirus bsAbs that are potently neutralizing, confer protection in mice, and are resistant to viral escape. Moreover, we combine Fvs from pan-ebolavirus mAbs with those of protective MARV mAbs to generate pan-filovirus protective bsAbs. These results provide guidelines for broad antiviral bsAb design and generate new immunotherapeutic candidates.

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“…Since that time, sporadic outbreaks of EBOV have occurred, causing severe disease and often high fatality rates (Sivanandy et al, 2022 ). A vaccine for EBOV as well as monoclonal antibody therapies have been approved by the FDA in the last few years (Ollmann, 2020 ; Taki et al, 2023 ) but there is still a lack of small molecule therapies as well as treatments/vaccines for the five other known types of EBOV. Limited information is available on optimal sites for direct‐acting antivirals against EBOV proteins and mechanistic studies of EBOV protein function may elucidate optimal sites to target and dampen EBOV replication.…”

Section: Introductionmentioning

confidence: 99%

Computational and experimental identification of keystone interactions in Ebola virus matrix protein VP40 dimer formation

Narkhede,

Saxena,

Sharma

et al. 2024

Protein Science

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The Ebola virus (EBOV) is a lipid‐enveloped virus with a negative sense RNA genome that can cause severe and often fatal viral hemorrhagic fever. The assembly and budding of EBOV is regulated by the matrix protein, VP40, which is a peripheral protein that associates with anionic lipids at the inner leaflet of the plasma membrane. VP40 is sufficient to form virus‐like particles (VLPs) from cells, which are nearly indistinguishable from authentic virions. Due to the restrictions of studying EBOV in BSL‐4 facilities, VP40 has served as a surrogate in cellular studies to examine the EBOV assembly and budding process from the host cell plasma membrane. VP40 is a dimer where inhibition of dimer formation halts budding and formation of new VLPs as well as VP40 localization to the plasma membrane inner leaflet. To better understand VP40 dimer stability and critical amino acids to VP40 dimer formation, we integrated computational approaches with experimental validation. Site saturation/alanine scanning calculation, combined with molecular mechanics‐based generalized Born with Poisson‐Boltzmann surface area (MM‐GB/PBSA) method and molecular dynamics simulations were used to predict the energetic contribution of amino acids to VP40 dimer stability and the hydrogen bonding network across the dimer interface. These studies revealed several previously unknown interactions and critical residues predicted to impact VP40 dimer formation. In vitro and cellular studies were then pursued for a subset of VP40 mutations demonstrating reduction in dimer formation (in vitro) or plasma membrane localization (in cells). Together, the computational and experimental approaches revealed critical residues for VP40 dimer stability in an alpha‐helical interface (between residues 106–117) as well as in a loop region (between residues 52–61) below this alpha‐helical region. This study sheds light on the structural origins of VP40 dimer formation and may inform the design of a small molecule that can disrupt VP40 dimer stability.

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Ebanga™: The most recent FDA-approved drug for treating Ebola

Cited by 9 publications

References 34 publications

Oral administration of obeldesivir protects nonhuman primates against Sudan ebolavirus

Oral administration of obeldesivir protects nonhuman primates against Sudan ebolavirus

Design and characterization of protective pan-ebolavirus and pan-filovirus bispecific antibodies

Computational and experimental identification of keystone interactions in Ebola virus matrix protein VP40 dimer formation

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