Walleye dermal sarcoma virus

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Walleye dermal sarcoma virus
Virus classification Red Pencil Icon.png
(unranked): Virus
Realm: Riboviria
Kingdom: Pararnavirae
Phylum: Artverviricota
Class: Revtraviricetes
Order: Ortervirales
Family: Retroviridae
Genus: Epsilonretrovirus
Species:
Walleye dermal sarcoma virus

The Walleye dermal sarcoma virus (WDSV) is a retrovirus that infects walleye (Sander vitreus) often causing oncogenesis. [1] WDSV is an exogenous retrovirus belonging to the subfamily Orthoretrovirinae. This virus is related to the walleye epidermal hyperplasia viruses type 1 and type 2 (WEHV-1& WEHV-2), all belonging to the epsilonretrovirus genus based on similarities of the gene coding for the reverse transcriptase conserved in retroviruses.

Contents

Infections

The virus infects soft tissues of the walleye, causing sarcoma neoplasia to form along the body, protruding from between the scales of the boney fish. Skin lesions from WDSV and WEHV were both identified in walleye from Oneida Lake, New York in 1969. [2] The tumors associated with these viruses appear to have a seasonal cycle appearing in the fall then regressing in the springtime, an individual walleye appears to form the neoplasia once in the lifetime in the fish. In a season about 30% of walleye from Oneida Lake form tumors associated with WDSV. [3] Transmission of the virus is suspected to be fish to fish contact during spawning. The regression correlates with the increase temperature in spring along with an increase in the walleye's immune activity. [3]

Genome

With a genome of WDSV is 12.71 kb reading for 7 genes, WDSV is the largest known retrovirus genome. [4] Of the 7 genes in three are common among retroviruses, group-specific antigen (gag), polymerase (pol), and envelope (env), the remaining four genes are por, orf-A, orf-B, and orf-C the orf genes' functions have been undetermined. [5] The genetics in the virus is a single strand RNA.[ citation needed ]

Related Research Articles

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A retrovirus is a type of virus that inserts a DNA copy of its RNA genome into the DNA of a host cell that it invades, thus changing the genome of that cell. Once inside the host cell's cytoplasm, the virus uses its own reverse transcriptase enzyme to produce DNA from its RNA genome, the reverse of the usual pattern, thus retro (backwards). The new DNA is then incorporated into the host cell genome by an integrase enzyme, at which point the retroviral DNA is referred to as a provirus. The host cell then treats the viral DNA as part of its own genome, transcribing and translating the viral genes along with the cell's own genes, producing the proteins required to assemble new copies of the virus. Many retroviruses cause serious diseases in humans, other mammals, and birds.

Mouse mammary tumor virus (MMTV) is a milk-transmitted retrovirus like the HTL viruses, HI viruses, and BLV. It belongs to the genus Betaretrovirus. MMTV was formerly known as Bittner virus, and previously the "milk factor", referring to the extra-chromosomal vertical transmission of murine breast cancer by adoptive nursing, demonstrated in 1936, by John Joseph Bittner while working at the Jackson Laboratory in Bar Harbor, Maine. Bittner established the theory that a cancerous agent, or "milk factor", could be transmitted by cancerous mothers to young mice from a virus in their mother's milk. The majority of mammary tumors in mice are caused by mouse mammary tumor virus.

<span class="mw-page-title-main">Kaposi's sarcoma-associated herpesvirus</span> Species of virus

Kaposi's sarcoma-associated herpesvirus (KSHV) is the ninth known human herpesvirus; its formal name according to the International Committee on Taxonomy of Viruses (ICTV) is Human gammaherpesvirus 8, or HHV-8 in short. Like other herpesviruses, its informal names are used interchangeably with its formal ICTV name. This virus causes Kaposi's sarcoma, a cancer commonly occurring in AIDS patients, as well as primary effusion lymphoma, HHV-8-associated multicentric Castleman's disease and KSHV inflammatory cytokine syndrome. It is one of seven currently known human cancer viruses, or oncoviruses. Even after so many years of discovery of KSHV/HHV8, there is no known cure for KSHV associated tumorigenesis.

<span class="mw-page-title-main">Oncovirus</span> Viruses that can cause cancer

An oncovirus or oncogenic virus is a virus that can cause cancer. This term originated from studies of acutely transforming retroviruses in the 1950–60s, when the term "oncornaviruses" was used to denote their RNA virus origin. With the letters "RNA" removed, it now refers to any virus with a DNA or RNA genome causing cancer and is synonymous with "tumor virus" or "cancer virus". The vast majority of human and animal viruses do not cause cancer, probably because of longstanding co-evolution between the virus and its host. Oncoviruses have been important not only in epidemiology, but also in investigations of cell cycle control mechanisms such as the retinoblastoma protein.

<i>Gammaretrovirus</i> Genus of viruses

Gammaretrovirus is a genus in the Retroviridae family. Example species are the murine leukemia virus and the feline leukemia virus. They cause various sarcomas, leukemias and immune deficiencies in mammals, reptiles and birds.

<span class="mw-page-title-main">Endogenous retrovirus</span> Inherited retrovirus encoded in an organisms genome

Endogenous retroviruses (ERVs) are endogenous viral elements in the genome that closely resemble and can be derived from retroviruses. They are abundant in the genomes of jawed vertebrates, and they comprise up to 5–8% of the human genome.

<i>Jaagsiekte sheep retrovirus</i> Species of virus

Jaagsiekte sheep retrovirus (JSRV) is a betaretrovirus which is the causative agent of a contagious lung cancer in sheep, called ovine pulmonary adenocarcinoma.

Rous sarcoma virus (RSV) is a retrovirus and is the first oncovirus to have been described. It causes sarcoma in chickens.

The gag-onc fusion protein is a general term for a fusion protein formed from a group-specific antigen ('gag') gene and that of an oncogene ('onc'), a gene that plays a role in the development of a cancer. The name is also written as Gag-v-Onc, with "v" indicating that the Onc sequence resides in a viral genome. Onc is a generic placeholder for a given specific oncogene, such as C-jun..

Avian sarcoma leukosis virus (ASLV) is an endogenous retrovirus that infects and can lead to cancer in chickens; experimentally it can infect other species of birds and mammals. ASLV replicates in chicken embryo fibroblasts, the cells that contribute to the formation of connective tissues. Different forms of the disease exist, including lymphoblastic, erythroblastic, and osteopetrotic.

Koala retrovirus (KoRV) is a retrovirus that is present in many populations of koalas. It has been implicated as the agent of koala immune deficiency syndrome (KIDS), an AIDS-like immunodeficiency that leaves infected koalas more susceptible to infectious disease and cancers. The virus is thought to be a recently introduced exogenous virus that is also integrating into the koala genome. Thus the virus can transmit both horizontally and vertically. The horizontal modes of transmission are not well defined but are thought to require close contact.

The walleye epidermal hyperplasia viruses are two species of retroviruses classified under Epsilonretrovirus, a genus in the family of Retroviridae. There are three genome sequenced and identified exogenous retroviruses of this genus which include two known types associated with walleye epidermal hyperplasia disease. Both viral types are confirmed to be the causative agents of the neoplastic condition in the freshwater fish species, the North American walleye (Sander vitreus). The specific association of retroviral infection with proliferative lesions in fish is based on the presence of retrovirus-like particles and reverse transcriptase activity from neoplastic tissue. Although both virus types have been observed in lesions of diseased fish, each cell of the infected tissue is host to a specific virus. Transmission studies have also shown that WEHV-2 has been the more proliferative agent of the condition as compared to WEHV-1.

Lymphocystivirus is a genus of viruses, in the family Iridoviridae. Fish serve as natural hosts. There are four species in this genus. Diseases associated with this genus include: tumor-like growths on the skin.

Retroviral matrix proteins are components of envelope-associated capsids of retroviruses. These proteins line the inner surface of viral envelopes and are associated with viral membranes.

Peter K. Vogt is an American molecular biologist, virologist and geneticist. His research focuses on retroviruses and viral and cellular oncogenes.

Esocid lymphosarcoma, also known as Esox lymphosarcoma is a transmissible tumor which affects two species of fish, northern pike and Muskellunge, in North America and Europe. The tumors initially are found in the skin, but later in the course of the disease are also found in the internal organs. The tumors appear as colorless skin protrusions which are several centimeters in diameter. A retrovirus has been detected in affected cells by electron microscopy. The disease is spread by physical contact between fish, probably during the spring spawning season. The disease has the lowest prevalence in the summer.

Sandra L. Quackenbush is an American virologist working as an associate professor of retrovirology at the Colorado State University College of Veterinary Medicine and Biomedical Sciences. Quackenbush also serves as the associate head of graduate education for the Microbiology, Immunology & Pathology Department within the college. Her research interests include viral pathogenesis, with emphasis in viral-induced oncogenesis.

Human endogenous retrovirus K (HERV-K) or Human teratocarcinoma-derived virus (HDTV) is a family of human endogenous retroviruses associated with malignant tumors of the testes. Phylogenetically, the HERV-K group belongs to the ERV2 or Class II or Betaretrovirus-like supergroup. Over the past several years, it has been found that this group of ERVs play an important role in embryogenesis, but their expression is silenced in most cell types in healthy adults. The HERV-K family, and particularly its subgroup HML-2, is the youngest and most transcriptionally active group and hence, it is the best studied among other ERVs. Reactivation of it or anomalous expression of HML-2 in adult tissues has been associated with various types of cancer and with neurodegenerative diseases such as amytrophic lateral sclerosis (ALS). Endogenous retrovirus K (HERV-K) is related to mammary tumor virus in mice. It exists in the human and cercopithecoid genomes. Human genome contains hundreds of copies of HERV-K and many of them possess complete open reading frames (ORFs) that are transcribed and translated, especially in early embryogenesis and in malignancies. HERV-K is also found in apes and Old World monkeys. It is uncertain how long ago in primate evolution the full-length HERV-K proviruses which are in the human genome today were created.

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<span class="mw-page-title-main">Enzootic nasal tumor virus</span> Species of virus

The enzootic nasal tumor virus of the betaretrovirus genus is a carcinogenic retrovirus that causes enzootic nasal adenocarcinoma in sheep and goats. Strain ENTV-1 is found in sheep and strain ENTV-2 is found in goats. The virus causes tumor growth in the upper nasal cavity and is closely related to JSRV which also causes respiratory tumors in ovine. The disease, enzootic nasal adenocarcinoma is common in North America and is found in sheep and goats on every continent except New Zealand and Australia. There are more than 27 betaretroviruses similar to ENVT and JSRV in the ovine genome. In the future, research on ENTV may become important in studying viruses that cause human lung cancer.

References

  1. Poulet FM, Bowser PR, Casey JW (January 1996). "PCR and RT-PCR analysis of infection and transcriptional activity of walleye dermal sarcoma virus (WDSV) in organs of adult walleyes (Stizostedion vitreum)". Veterinary Pathology. 33 (1): 66–73. doi:10.1177/030098589603300107. PMID   8826007. S2CID   43016124.
  2. Rovnak J, Quackenbush SL (September 2010). "Walleye dermal sarcoma virus: molecular biology and oncogenesis". Viruses. 2 (9): 1984–1999. doi: 10.3390/v2091984 . PMC   3185748 . PMID   21994717.
  3. 1 2 MacLachlan NJ, Dubovi EJ, eds. (2017-01-01). "Chapter 14 - Retroviridae". Fenner's Veterinary Virology (Fifth ed.). Boston: Academic Press. pp. 269–297. doi:10.1016/b978-0-12-800946-8.00014-3. ISBN   978-0-12-800946-8.
  4. Holzschu DL, Martineau D, Fodor SK, Vogt VM, Bowser PR, Casey JW (September 1995). "Nucleotide sequence and protein analysis of a complex piscine retrovirus, walleye dermal sarcoma virus". Journal of Virology. 69 (9): 5320–5331. doi:10.1128/jvi.69.9.5320-5331.1995. PMC   189371 . PMID   7636975.
  5. Zhang Z, Du Tremblay D, Lang BF, Martineau D (November 1996). "Phylogenetic and epidemiologic analysis of the walleye dermal sarcoma virus". Virology. 225 (2): 406–412. doi: 10.1006/viro.1996.0616 . PMID   8918928.
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