Emily Penny scite author profile

Background: Members of the family Iridoviridae can cause severe diseases resulting in significant economic and environmental losses. Very little is known about how iridoviruses cause disease in their host. In the present study, we describe the re-analysis of the Iridoviridae family of complex DNA viruses using a variety of comparative genomic tools to yield a greater consensus among the annotated sequences of its members.

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Antibody dependent enhancement of frog virus 3 infection

Eaton

Penny

Brunetti

2010

Virol J

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BackgroundViruses included in the family Iridoviridae are large, icosahedral, dsDNA viruses that are subdivided into 5 genera. Frog virus 3 (FV3) is the type species of the genus Ranavirus and the best studied iridovirus at the molecular level. Typically, antibodies directed against a virus act to neutralize the virus and limit infection. Antibody dependent enhancement occurs when viral antibodies enhance infectivity of the virus rather than neutralize it.ResultsHere we show that anti-FV3 serum present at the time of FV3 infection enhances infectivity of the virus in two non-immune teleost cell lines. We found that antibody dependent enhancement of FV3 was dependent on the Fc portion of anti-FV3 antibodies but not related to complement. Furthermore, the presence of anti-FV3 serum during an FV3 infection in a non-immune mammalian cell line resulted in neutralization of the virus. Our results suggest that a cell surface receptor specific to teleost cell lines is responsible for the enhancement.ConclusionsThis report represents the first evidence of antibody dependent enhancement in iridoviruses. The data suggests that anti-FV3 serum can either neutralize or enhance viral infection and that enhancement is related to a novel antibody dependent enhancement pathway found in teleosts that is Fc dependent.

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Localization of Frog Virus 3 Conserved Viral Proteins 88R, 91R, and 94L

Penny

Brunetti

2019

Viruses

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The characterization of the function of conserved viral genes is central to developing a greater understanding of important aspects of viral replication or pathogenesis. A comparative genomic analysis of the iridoviral genomes identified 26 core genes conserved across the family Iridoviridae. Three of those conserved genes have no defined function; these include the homologs of frog virus 3 (FV3) open reading frames (ORFs) 88R, 91R, and 94L. Conserved viral genes that have been previously identified are known to participate in a number of viral activities including: transcriptional regulation, DNA replication/repair/modification/processing, protein modification, and viral structural proteins. To begin to characterize the conserved FV3 ORFs 88R, 91R, and 94L, we cloned the genes and determined their intracellular localization. We demonstrated that 88R localizes to the cytoplasm of the cell while 91R localizes to the nucleus and 94L localizes to the endoplasmic reticulum (ER).

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Screening for Depression and Posttraumatic Stress Disorder in Patients With Burns

Simmons¹,

Waldrop²,

Penny³

2022

The Journal for Nurse Practitioners

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[P1–338]: SMELL IDENTIFICATION IMPAIRMENT IN EARLY ONSET ALZHEIMER's DIASEASE AND MILD COGNITIVE IMPAIRMENT

Velayudhan

Morkeh-Wilson

Penny

et al. 2017

Alzheimer's & Dementia

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Emily Penny

Comparative genomic analysis of the family Iridoviridae: re-annotating and defining the core set of iridovirus genes

Antibody dependent enhancement of frog virus 3 infection

Localization of Frog Virus 3 Conserved Viral Proteins 88R, 91R, and 94L

Screening for Depression and Posttraumatic Stress Disorder in Patients With Burns

[P1–338]: SMELL IDENTIFICATION IMPAIRMENT IN EARLY ONSET ALZHEIMER's DIASEASE AND MILD COGNITIVE IMPAIRMENT

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