Duck hepatitis B virus

Duck hepatitis B virus
Virus classification
(unranked):	Virus
Phylum:	incertae sedis
Class:	incertae sedis
Order:	incertae sedis
Family:	Hepadnaviridae
Genus:	Avihepadnavirus
Species:	Duck hepatitis B virus

Duck hepatitis B virus, abbreviated DHBV, is part of the genus Avihepadnavirus of the Hepadnaviridae, and is the causal agent of duck hepatitis B.

DHBV is a small DNA virus with a diameter of 40–45 nm. The viral envelope is made up from host cell lipid, with viral surface antigens (DHBsAg). The icosahedral nucleocapsid within, is composed of the virus core antigen (DHBcAg) and surrounds the DNA genome and viral polymerase. The viral genome is a circular double stranded DNA molecule about 3000 base pairs long. The genome has three overlapping open reading frames or ORFs:

C-ORF – encoding the core antigen and pre-core protein which are processed and secreted as DHBcAg
S-ORF – codes for the surface antigen DHBsAg
P-ORF – encoding the viral polymerase.

On binding and entry of the virus to the host cell, the genome is transported to the nucleus to be transcribed. Novel viral RNA is then transferred to the cytoplasm for translation and subsequent protein synthesis.

Duck hepatitis B virus has provided a basis for the use of vaccines and prophylactic treatments for individuals at high risk of human Hepatitis B virus (HBV).[1] The virus has also provided as a useful animal model in the absence of one from the HBV,[2] and as scaffold for the development of chimeric virus-like particles.[3]

References

Jilbert AR, Kotlarski I (March–April 2000). "Immune responses to duck hepatitis B virus infection". Developmental and Comparative Immunology. 24 (2–3): 285–302. doi:10.1016/S0145-305X(99)00079-8. PMID 10717294.
Cooper A, Paran N, Shaul Y (2003-07-11). "The earliest steps in hepatitis B virus infection". Biochimica et Biophysica Acta. 1614 (1): 89–96. doi:10.1016/S0005-2736(03)00166-4. PMID 12873769.
Wetzel D, Rolf T, Suckow M, Kranz A, Barbian A, Chan JA, Leitsch J, Weniger M, Jenzelewski J, Kouskousis B, Palmer C, Beeson JG, Schembecker G, Merz J, Piontek P (2018). "Establishment of a yeast-based VLP platform for antigen presentation". Microbial Cell Factories. 17 (1): 17. doi:10.1186/s12934-018-0868-0. PMC 5798182. PMID 29402276.

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[1] Jilbert AR, Kotlarski I (March–April 2000). "Immune responses to duck hepatitis B virus infection". Developmental and Comparative Immunology. 24 (2–3): 285–302. doi:10.1016/S0145-305X(99)00079-8. PMID 10717294.

[2] Cooper A, Paran N, Shaul Y (2003-07-11). "The earliest steps in hepatitis B virus infection". Biochimica et Biophysica Acta. 1614 (1): 89–96. doi:10.1016/S0005-2736(03)00166-4. PMID 12873769.

[Wetzel2018-3] Wetzel D, Rolf T, Suckow M, Kranz A, Barbian A, Chan JA, Leitsch J, Weniger M, Jenzelewski J, Kouskousis B, Palmer C, Beeson JG, Schembecker G, Merz J, Piontek P (2018). "Establishment of a yeast-based VLP platform for antigen presentation". Microbial Cell Factories. 17 (1): 17. doi:10.1186/s12934-018-0868-0. PMC 5798182. PMID 29402276.