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DMAb inoculation of synthetic cross reactive antibodies protects against lethal influenza A and B infections.

npj Vaccines. 2017-05; 
Sarah T. C. Elliott,Nicole L. Kallewaard,Ebony Benjamin, Leslie Wachter-Rosati,Josephine M. McAuliffe,Ami Patel,Trevor R. F. Smith.Katherine Schultheis,Daniel H. Park,Seleeke Flingai,Megan C. Wise,Janess Mendoza,Stephanie Ramos,Kate E. Broderick,Jian Yan,Laurent M. Humeau, Niranjan Y. Sardesai,Kar Muthumani,Qing Zhu,David B. Weiner.
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Gene Synthesis ...Antibody amino acid sequences were DNA codon-optimized and RNA-optimized for expression in human/ mouse, and resulting DNA transgenes were synthesized de novo (Genscript, Piscataway, NJ, USA). … Get A Quote

摘要

Influenza virus remains a significant public health threat despite innovative vaccines and antiviral drugs. A major limitation to current vaccinations and therapies against influenza virus is pathogenic diversity generated by shift and drift. A simple, cost-effective passive immunization strategy via in vivo production of cross-protective antibody molecules may augment existing vaccines and antiviral drugs in seasonal and pandemic outbreaks. We engineered synthetic plasmid DNA to encode two novel and broadly cross-protective monoclonal antibodies targeting influenza A and B. We utilized enhanced in vivo delivery of these plasmid DNA-encoded monoclonal antibody (DMAb) constructs and show that this strategy induc... More

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