Literature DB >> 23288419

Novel mutations in Marburg virus glycoprotein associated with viral evasion from antibody mediated immune pressure.

Masahiro Kajihara1, Eri Nakayama1, Andrea Marzi2, Manabu Igarashi3, Heinz Feldmann2, Ayato Takada4,1.   

Abstract

Marburg virus (MARV) and Ebola virus, members of the family Filoviridae, cause lethal haemorrhagic fever in humans and non-human primates. Although the outbreaks are concentrated mainly in Central Africa, these viruses are potential agents of imported infectious diseases and bioterrorism in non-African countries. Recent studies demonstrated that non-human primates passively immunized with virus-specific antibodies were successfully protected against fatal filovirus infection, highlighting the important role of antibodies in protective immunity for this disease. However, the mechanisms underlying potential evasion from antibody mediated immune pressure are not well understood. To analyse possible mutations involved in immune evasion in the MARV envelope glycoprotein (GP) which is the major target of protective antibodies, we selected escape mutants of recombinant vesicular stomatitis virus (rVSV) expressing MARV GP (rVSVΔG/MARVGP) by using two GP-specific mAbs, AGP127-8 and MGP72-17, which have been previously shown to inhibit MARV budding. Interestingly, several rVSVΔG/MARVGP variants escaping from the mAb pressure-acquired amino acid substitutions in the furin-cleavage site rather than in the mAb-specific epitopes, suggesting that these epitopes are recessed, not exposed on the uncleaved GP molecule, and therefore inaccessible to the mAbs. More surprisingly, some variants escaping mAb MGP72-17 lacked a large proportion of the mucin-like region of GP, indicating that these mutants efficiently escaped the selective pressure by deleting the mucin-like region including the mAb-specific epitope. Our data demonstrate that MARV GP possesses the potential to evade antibody mediated immune pressure due to extraordinary structural flexibility and variability.

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Year:  2013        PMID: 23288419      PMCID: PMC3709686          DOI: 10.1099/vir.0.049114-0

Source DB:  PubMed          Journal:  J Gen Virol        ISSN: 0022-1317            Impact factor:   3.891


  39 in total

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4.  Endoproteolytic processing of the ebola virus envelope glycoprotein: cleavage is not required for function.

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5.  Foreign glycoproteins expressed from recombinant vesicular stomatitis viruses are incorporated efficiently into virus particles.

Authors:  M J Schnell; L Buonocore; E Kretzschmar; E Johnson; J K Rose
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2.  Interaction between TIM-1 and NPC1 Is Important for Cellular Entry of Ebola Virus.

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3.  Therapeutics for postexposure treatment of Ebola virus infection.

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4.  Initiating a watch list for Ebola virus antibody escape mutations.

Authors:  Craig R Miller; Erin L Johnson; Aran Z Burke; Kyle P Martin; Tanya A Miura; Holly A Wichman; Celeste J Brown; F Marty Ytreberg
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5.  Unveiling a Drift Resistant Cryptotope within Marburgvirus Nucleoprotein Recognized by Llama Single-Domain Antibodies.

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6.  A Single Amino Acid Change in the Marburg Virus Glycoprotein Arises during Serial Cell Culture Passages and Attenuates the Virus in a Macaque Model of Disease.

Authors:  Kendra J Alfson; Laura E Avena; Jenny Delgado; Michael W Beadles; Jean L Patterson; Ricardo Carrion; Anthony Griffiths
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Journal:  Lancet Infect Dis       Date:  2020-06-18       Impact factor: 25.071

8.  Two Point Mutations in Old World Hantavirus Glycoproteins Afford the Generation of Highly Infectious Recombinant Vesicular Stomatitis Virus Vectors.

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9.  Generation and Selection of a Panel of Pan-Filovirus Single-Chain Antibodies using Cell-Free Ribosome Display.

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  9 in total

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