An optimized electrofusion-based protocol for generating virus-specific human monoclonal antibodies

Yu, Xiaojun; McGraw, Patricia; House, Frances S.; Crowe, James E.

doi:10.1016/j.jim.2008.04.008

Cited by 130 publications

(127 citation statements)

References 39 publications

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“…Screening was performed against E1E2 variants 1a53 (autologous) and 1a154 (H77) (heterologous) for subject 117 and 1a53 (heterologous) and 1a38 (autologous) variants for subject 110. 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).…”

Section: Methodsmentioning

confidence: 99%

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

et al. 2017

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Section: Methodsmentioning

confidence: 99%

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

et al. 2017

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“…After 1 wk, culture supernatants were screened by ELISA for binding to recombinant, postfusion RSV A2 F protein and FFL_001. Cells from positive wells were fused with HMMA2.5 myeloma cells by electrofusion (26). Fused cells were plated in 384-well plates in growth medium containing 100 μM hypoxanthine, 0.4 μM aminopterin, 16 μM thymidine (HAT Media Supplement, Sigma), and 7 μg/mL ouabain (Sigma).…”

Section: Methodsmentioning

confidence: 99%

Structural basis for nonneutralizing antibody competition at antigenic site II of the respiratory syncytial virus fusion protein

Mousa

Sauer

Sevy

et al. 2016

Proc. Natl. Acad. Sci. U.S.A.

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Palivizumab was the first antiviral monoclonal antibody (mAb) approved for therapeutic use in humans, and remains a prophylactic treatment for infants at risk for severe disease because of respiratory syncytial virus (RSV). Palivizumab is an engineered humanized version of a murine mAb targeting antigenic site II of the RSV fusion (F) protein, a key target in vaccine development. There are limited reported naturally occurring human mAbs to site II; therefore, the structural basis for human antibody recognition of this major antigenic site is poorly understood. Here, we describe a nonneutralizing class of site II-specific mAbs that competed for binding with palivizumab to postfusion RSV F protein. We also describe two classes of site II-specific neutralizing mAbs, one of which escaped competition with nonneutralizing mAbs. An X-ray crystal structure of the neutralizing mAb 14N4 in complex with F protein showed that the binding angle at which human neutralizing mAbs interact with antigenic site II determines whether or not nonneutralizing antibodies compete with their binding. Fine-mapping studies determined that nonneutralizing mAbs that interfere with binding of neutralizing mAbs recognize site II with a pose that facilitates binding to an epitope containing F surface residues on a neighboring protomer. Neutralizing antibodies, like motavizumab and a new mAb designated 3J20 that escape interference by the inhibiting mAbs, avoid such contact by binding at an angle that is shifted away from the nonneutralizing site. Furthermore, binding to rationally and computationally designed site II helixloop-helix epitope-scaffold vaccines distinguished neutralizing from nonneutralizing site II antibodies.F protein | human respiratory syncytial virus | neutralizing antibodies R espiratory syncytial virus (RSV) is a highly contagious human pathogen, infecting the majority of infants before age 2 y, and is the leading cause of viral bronchiolitis and viral pneumonia in infants and children (1, 2). RSV remains a top priority for vaccine development, as thousands of deaths are recorded worldwide each year because of complications from infection (3). To date, there is no licensed RSV vaccine. A major focus of RSV vaccine development has been inclusion of the RSV fusion (F) protein, a class I fusion glycoprotein that is synthesized as a precursor and cleaved into two disulfide-linked fragments upon maturation into a trimer (4). Although the RSV virion contains two additional surface proteins, the highly-glycosylated attachment (G) protein and the small hydrophobic protein, the F protein is highly conserved among strains of RSV strains and is the major target of protective neutralizing antibodies.The F protein is known to adopt at least two major conformations: the metastable prefusion conformation and the postfusion conformation. Following attachment of the virion to a cell by the G protein, the F protein undergoes a dramatic structural rearrangement, resulting in fusion of the viral and cell membranes, and in cultured cells causes...

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“…4,22 Even though electrofusion of biological cells is potentially a useful method, achieving the sufficient efficiency still requires extensive trial-and-error studies. [23][24][25][26] One of the earliest approaches to improve electrofusion efficiency was the use of hypotonic electrofusion buffer that resulted in the considerable fusion efficiency increase. [27][28][29][30][31][32][33][34] To ensure the improvement of fusion efficiency in hypotonic buffer the duration and the osmolarity of the hypotonic treatment has to molarity of solutions was determined with Knauer vapor pressure osmometer K-7000 (Knauer, Wissenschaftliche Gerätebau, Germany).…”

Section: Cellsmentioning

confidence: 99%

Cell size dynamics and viability of cells exposed to hypotonic treatment and electroporation for electrofusion optimization

Ušaj¹,

Trontelj²,

Hudej³

et al. 2009

Radiology and Oncology

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An optimized electrofusion-based protocol for generating virus-specific human monoclonal antibodies

Cited by 130 publications

References 39 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

Structural basis for nonneutralizing antibody competition at antigenic site II of the respiratory syncytial virus fusion protein

Cell size dynamics and viability of cells exposed to hypotonic treatment and electroporation for electrofusion optimization

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