Parvovirus B19 Codon Optimized Structural Proteins for Vaccine and Diagnostic Applications

Description:
Parvovirus B19 (B19V) is the only known pathogenic human parvovirus. Infection by this viral pathogen can cause transient aplastic crisis in individuals with high red cell turnover, pure red cell aplasia in immunosuppressed patients, and hydrops fetalis during pregnancy. In children, B19V most commonly causes erythema infectiosum, or fifth's disease. Infection can also cause arthropathy and arthralgia. The virus is very erythrotropic, targeting human erythroid (red blood) progenitors found in the blood, bone marrow, and fetal liver. Currently, there are no approved vaccines or antiviral drugs for the treatment or prevention of B19V infection.

The subject technology is a series of plasmid constructs with codon optimized B19 viral capsid genes (VP1 and VP2) that can be expressed in mammalian cells. Transfection of vectors encoding these optimized VP1 and VP2 genes into different mammalian cell lines, including 293, Cos7, and Hela cells produce virus-like particles (VLPs). The vectors include bicistronic plasmids expressing the VP1 and VP2 proteins at different ratios to produce B19V VLPs with optimal antigenicity for vaccine applications. This technology can also be used for diagnostic applications and development of a viral packaging system for producing infectious B19V virus.
Patent Information:
For Information, Contact:
Vidita Choudhry
Technology Development Specialist
NIH Technology Transfer
301-594-4095
vidita.choudhry@nih.gov
Inventors:
Neal Young
Sachiko Kajigaya
Ning Zhi
Keywords:
Against
AgainstB19V
APPLICATION
B19V
BBXXXX
CAPSID
Cells
CODON
DA4BXX
DA4XXX
DAXXXX
DC5BXX
DC5XXX
DCXXXX
DEVELOPING
DNA-based
DXXXXX
Erythema infectiosum
Fifth Disease
GENES
Human parvovirus B19 infection
Hydrops fetalis
Infection
Non-pennissive
OPTIMIZED
PARTICLE
Parvovirus antenatal infection
Patent Category - Biotechnology
Pure red cell aplasia
USAGE
vaccines
VIRUS-LIKE
VLP-and
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