Mechanism of Human Antibody-Mediated Neutralization of Marburg Virus

Flyak, Andrew I.; Ilinykh, Philipp A.; Murin, Charles D.; Garrón, Tania; Shen, Xiaoli; Fusco, Marnie L.; Hanabusa, Takao; Bornholdt, Zachary A.; Slaughter, James C.; Sapparapu, Gopal; Klages, Curtis; Ksiazek, Thomas G.; Ward, Andrew B.; Saphire, Erica Ollmann; Bukreyev, Alexander

doi:10.1016/j.cell.2015.01.031

Cited by 138 publications

(228 citation statements)

References 45 publications

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“…Human hybridomas were generated as described previously (39). In brief, cryopreserved PBMC samples from subjects 110 and 117 were transformed with EBV, CpG, and additional supplements.…”

Section: Methodsmentioning

confidence: 99%

“…Cells from wells with supernatants reacting with HCV antigens were fused with HMMA2.5 myeloma cells using an electrofusion technique (40). After fusion, hybridoma cell lines were cloned by limited dilutions and single-cell fluorescence-activated cell sorting and expanded in post-fusion medium as previously described (39). HiTrap Protein G or HiTrap MabSelectSure columns were used to purify HCV-specific antibodies from filtered cell culture supernatants.…”

Section: Methodsmentioning

confidence: 99%

“…Total cellular RNA was extracted from clonal hybridomas that produced HCV antibodies, and RT-PCR reaction was performed using mixtures of primers designed to amplify all heavy chain or light chain antibody variable regions. Antibody variable gene sequence analysis was performed as previously described (39). Heavy and light chain antibody variable region sequences were analyzed using the IMGT/V-Quest program (51,52).…”

Section: Methodsmentioning

confidence: 99%

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Broadly neutralizing antibodies with few somatic mutations and hepatitis C virus clearance

et al. 2017

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“…Human hybridomas were generated as described previously (39). In brief, cryopreserved PBMC samples from subjects 110 and 117 were transformed with EBV, CpG, and additional supplements.…”

Section: Methodsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

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Broadly neutralizing antibodies with few somatic mutations and hepatitis C virus clearance

et al. 2017

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“…Standard mouse models, using C57BL/6 or BALB/c, could only be utilized with a mouse-adapted Ravn 17,20 or mouse-adapted Ci67 18 , as previously done by others. These antibodies bind to Ci67 with some cross reactivity to Angola or Musoke, but are not cross reactive to Ravn.…”

Section: In Vivo Mouse Protection Studymentioning

confidence: 99%

“…administration of a 100 mg of antibody, with multi-dose regimen beginning 24-hr pre-exposure followed by 24 hr post-exposure against 1000 PFU mouse-adapted Ci67 strain. 18 The mAbs described in our studies were assessed in both male and female groups of mice with no efficacy differences observed between sexes. In addition to the baseline protection study, we re-challenged our mice thirty-five days after the initial exposure.…”

Section: In Vivo Mouse Protection Studymentioning

confidence: 99%

Generation and characterization of protective antibodies to Marburg virus

Froude

Pelat²,

Miethe

et al. 2017

mAbs

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Marburg virus (MARV) and Ebola virus (EBOV) have been a source of epidemics and outbreaks for several decades. We present here the generation and characterization of the first protective antibodies specific for wild-type MARV. Non-human primates (NHP), cynomolgus macaques, were immunized with viral-replicon particles expressing the glycoproteins (GP) of MARV (Ci67 isolate). An antibody fragment (single-chain variable fragment, scFv) phage display library was built after four immunogen injections, and screened against the GP 1-649 of MARV. Sequencing of 192 selected clones identified 18 clones with distinct V H and V L sequences. Four of these recombinant antibodies (R4A1, R4B11, R4G2, and R3F6) were produced in the scFv-Fc format for in vivo studies. Mice that were challenged with wild-type Marburg virus (Ci67 isolate) receiving 100 mg of scFv-Fc on days ¡1, 1 and 3 demonstrated protective efficacies ranging from 75-100%. The amino-acid sequences of the scFv-Fcs are similar to those of their human germline counterparts, sharing an identity ranging between 68 and 100% to human germline immunoglobulin. These results demonstrate for the first time that recombinant antibodies offer protection against wild-type MARV, and suggest they may be promising candidates for further therapeutic development especially due to their human homology.

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Structure of glycosylated NPC1 luminal domain C reveals insights into NPC2 and Ebola virus interactions

et al. 2016

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Niemann‐pick type C1 (NPC1) is an endo/lysosomal membrane protein involved in intracellular cholesterol trafficking, and its luminal domain C is an essential endosomal receptor for Ebola and Marburg viruses. We have determined the crystal structure of glycosylated NPC1 luminal domain C and find all seven possible sites are glycosylated. Mapping the disease mutations onto the glycosylated structure reveals a potential binding face for NPC2. Knowledge‐based docking of NPC1 onto Ebola viral glycoprotein and sequence analysis of filovirus susceptible and refractory species reveals four critical residues, H418, Q421, F502 and F504, some or all of which are likely responsible for the species‐specific susceptibility to the virus infection.

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Mechanism of Human Antibody-Mediated Neutralization of Marburg Virus

Cited by 138 publications

References 45 publications

Broadly neutralizing antibodies with few somatic mutations and hepatitis C virus clearance

Broadly neutralizing antibodies with few somatic mutations and hepatitis C virus clearance

Generation and characterization of protective antibodies to Marburg virus

Structure of glycosylated NPC1 luminal domain C reveals insights into NPC2 and Ebola virus interactions

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