Agnoprotein Is an Essential Egress Factor during BK Polyomavirus Infection

Panou, Margarita-Maria; Prescott, Emma L.; Hurdiss, Daniel L.; Swinscoe, Gemma; Hollinshead, Michael; Caller, Laura G; Morgan, Ethan L.; Carlisle, Louisa; Müller, Marietta; Antoni, Michelle; Kealy, David; Ranson, Neil A.; Crump, Colin M.; Macdonald, Andrew

doi:10.3390/ijms19030902

Cited by 28 publications

(15 citation statements)

References 51 publications

(82 reference statements)

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“…JCV Asp38 is substituted for Glu and Gln for BKV and SV40 agnoproteins, respectively, at the same position , viral transcription, functioning as a viroporin (Suzuki et al, 2013(Suzuki et al, , 2010, virion formation (Sariyer et al, 2006;Suzuki et al, 2012). BKV Agno has also been implicated in interfering with exocytosis (Johannessen et al, 2011), inhibition of the viral DNA replication (Gerits et al, 2015) and egress of virions from the infected cells (Panou et al, 2018). In addition, JCV Agno was shown to deregulate cell cycle progression (Darbinyan et al, 2002).…”

Section: Agnoprotein Is Released From Agnoproteinpositive Cellsmentioning

confidence: 99%

Expression of novel proteins by polyomaviruses and recent advances in the structural and functional features of agnoprotein of JC virus, BK virus, and simian virus 40

Sarıbaş

Coric

Bouaziz

et al. 2018

Journal Cellular Physiology

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Polyomavirus family consists of a highly diverse group of small DNA viruses. The founding family member (MPyV) was first discovered in the newborn mouse in the late 1950s, which induces solid tumors in a wide variety of tissue types that are the epithelial and mesenchymal origin. Later, other family members were also isolated from a number of mammalian, avian and fish species. Some of these viruses significantly contributed to our current understanding of the fundamentals of modern biology such as transcription, replication, splicing, RNA editing, and cell transformation. After the discovery of first two human polyomaviruses (JC virus [JCV] and BK virus [BKV]) in the early 1970s, there has been a rapid expansion in the number of human polyomaviruses in recent years due to the availability of the new technologies and brought the present number to 14. Some of the human polyomaviruses cause considerably serious human diseases, including progressive multifocal leukoencephalopathy, polyomavirus‐associated nephropathy, Merkel cell carcinoma, and trichodysplasia spinulosa. Emerging evidence suggests that the expression of the polyomavirus genome is more complex than previously thought. In addition to encoding universally expressed regulatory and structural proteins (LT‐Ag, Sm t‐Ag, VP1, VP2, and VP3), some polyomaviruses express additional virus‐specific regulatory proteins and microRNAs. This review summarizes the recent advances in polyomavirus genome expression with respect to the new viral proteins and microRNAs other than the universally expressed ones. In addition, a special emphasis is devoted to the recent structural and functional discoveries in the field of polyomavirus agnoprotein which is expressed only by JCV, BKV, and simian virus 40 genomes.

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Section: Agnoprotein Is Released From Agnoproteinpositive Cellsmentioning

confidence: 99%

Expression of novel proteins by polyomaviruses and recent advances in the structural and functional features of agnoprotein of JC virus, BK virus, and simian virus 40

Sarıbaş

Coric

Bouaziz

et al. 2018

Journal Cellular Physiology

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“…Interestingly, immediately upstream of the VP1 gene of SV40, BKPyV, and JCPyV polyomaviruses resides a gene referred to as agnogene that encodes for an approximately 70 amino acid (aa) long Agnoprotein [ 41 ]. Even though the precise role of the Agnoprotein remains unclear, it seems to be involved in virus egress [ 42 ], and a viroporin activity was described [ 43 ]. We hypothesized that the Agnoprotein could play a role in EV-associated polyomavirus egress.…”

Section: Release Of Ev-associated Virionsmentioning

confidence: 99%

Intercellular Transmission of Naked Viruses through Extracellular Vesicles: Focus on Polyomaviruses

Helle

Handala

Bentz

et al. 2020

Viruses

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Extracellular vesicles have recently emerged as a novel mode of viral transmission exploited by naked viruses to exit host cells through a nonlytic pathway. Extracellular vesicles can allow multiple viral particles to collectively traffic in and out of cells, thus enhancing the viral fitness and diversifying the transmission routes while evading the immune system. This has been shown for several RNA viruses that belong to the Picornaviridae, Hepeviridae, Reoviridae, and Caliciviridae families; however, recent studies also demonstrated that the BK and JC viruses, two DNA viruses that belong to the Polyomaviridae family, use a similar strategy. In this review, we provide an update on recent advances in understanding the mechanisms used by naked viruses to hijack extracellular vesicles, and we discuss the implications for the biology of polyomaviruses.

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“…The VP2 and VP3 minor capsid proteins are located on the internal surface of the capsid, with one molecule of VP2 or VP3 associated with each VP1 pentamer . Whilst expressed late in infection, the agnoprotein does not form a structural component of the virus capsid, but rather serves to aid in release of infectious progeny virus from the infected cell …”

Section: Genomic Organizationmentioning

confidence: 99%

“…Late gene transcription ensues and progeny virions are formed within the nucleus once capsid proteins assemble around the newly synthesized genomes . These virions are then released from the infected cell by an incompletely understood mechanism, which may require active secretion of virions rather than passive lysis of the infected cell …”

Section: Viral Lifecyclementioning

confidence: 99%

BK virus: Current understanding of pathogenicity and clinical disease in transplantation

Chong

Antoni

Macdonald

et al. 2019

Reviews in Medical Virology

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BK polyomavirus (BKV) is an important cause of graft loss in renal transplant recipients that continues to pose a significant challenge to clinicians due to its frequently unpredictable onset, persistence, and the lack of effective antiviral agents or prevention strategies. This review covers our current understanding of epidemiology, viral transmission and disease progression, and treatment and prevention strategies that have been used to manage this disease.

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Agnoprotein Is an Essential Egress Factor during BK Polyomavirus Infection

Cited by 28 publications

References 51 publications

Expression of novel proteins by polyomaviruses and recent advances in the structural and functional features of agnoprotein of JC virus, BK virus, and simian virus 40

Expression of novel proteins by polyomaviruses and recent advances in the structural and functional features of agnoprotein of JC virus, BK virus, and simian virus 40

Intercellular Transmission of Naked Viruses through Extracellular Vesicles: Focus on Polyomaviruses

BK virus: Current understanding of pathogenicity and clinical disease in transplantation

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