Your search keyword '"Wilson WC"' showing total 239 results

101. Comparison of Rift Valley fever virus replication in North American livestock and wildlife cell lines.

Author

Gaudreault NN, Indran SV, Bryant PK, Richt JA, and Wilson WC

Abstract

Rift Valley fever virus (RVFV) causes disease outbreaks across Africa and the Arabian Peninsula, resulting in high morbidity and mortality among young domestic livestock, frequent abortions in pregnant animals, and potentially severe or fatal disease in humans. The possibility of RVFV spreading to the United States or other countries worldwide is of significant concern to animal and public health, livestock production, and trade. The mechanism for persistence of RVFV during inter-epidemic periods may be through mosquito transovarial transmission and/or by means of a wildlife reservoir. Field investigations in endemic areas and previous in vivo studies have demonstrated that RVFV can infect a wide range of animals, including indigenous wild ruminants of Africa. Yet no predominant wildlife reservoir has been identified, and gaps in our knowledge of RVFV permissive hosts still remain. In North America, domestic goats, sheep, and cattle are susceptible hosts for RVFV and several competent vectors exist. Wild ruminants such as deer might serve as a virus reservoir and given their abundance, wide distribution, and overlap with livestock farms and human populated areas could represent an important risk factor. The objective of this study was to assess a variety of cell lines derived from North American livestock and wildlife for susceptibility and permissiveness to RVFV. Results of this study suggest that RVFV could potentially replicate in native deer species such as white-tailed deer, and possibly a wide range of non-ruminant animals. This work serves to guide and support future animal model studies and risk model assessment regarding this high-consequence zoonotic pathogen.

Published

2015

102. Genetic characterization of epizootic hemorrhagic disease virus strains isolated from cattle in Israel.

Author

Wilson WC, Ruder MG, Klement E, Jasperson DC, Yadin H, Stallknecht DE, Mead DG, and Howerth E

Subjects

Animals, Cattle, Cluster Analysis, Genome, Viral, Hemorrhagic Disease Virus, Epizootic isolation & purification, Israel epidemiology, Molecular Epidemiology, Molecular Sequence Data, Phylogeny, RNA, Viral genetics, Reoviridae Infections epidemiology, Reoviridae Infections virology, Sequence Analysis, DNA, Sequence Homology, Cattle Diseases epidemiology, Cattle Diseases virology, Disease Outbreaks, Genetic Variation, Hemorrhagic Disease Virus, Epizootic classification, Hemorrhagic Disease Virus, Epizootic genetics, Reoviridae Infections veterinary

Abstract

Epizootic hemorrhagic disease virus (EHDV), a member of the genus Orbivirus not reported previously in Israel, was isolated from Israeli cattle during a 'bluetongue-like' disease outbreak in 2006. To ascertain the origin of this new virus, three isolates from the outbreak were fully sequenced and compared with available sequences. Whilst the L2 gene segment clustered with the Australian EHDV serotype 7 (EHDV-7) reference strain, most of the other segments were clustered with EHDV isolates of African/Middle East origin, specifically Bahrain, Nigeria and South Africa. The M6 gene had genetic relatedness to the Australian/Asian strains, but with the limited data available the significance of this relationship is unclear. Only one EHDV-7 L2 sequence was available, and as this gene encodes the serotype-specific epitope, the relationship of these EHDV-7 L2 genes to an Australian EHDV-7 reflects the serotype association, not necessarily the origin. The genetic data indicated that the strains affecting Israel in 2006 may have been related to similar outbreaks that occurred in North Africa in the same year. This finding also supports the hypothesis that EHDV entered Israel during 2006 and was not present there before this outbreak., (© 2015 The Authors.)

Published

2015

103. Orbiviruses: A North American Perspective.

Author

McVey DS, Drolet BS, Ruder MG, Wilson WC, Nayduch D, Pfannenstiel R, Cohnstaedt LW, MacLachlan NJ, and Gay CG

Subjects

Animals, Animals, Wild, Bluetongue prevention & control, Bluetongue transmission, Bluetongue virus immunology, Disease Reservoirs, Hemorrhagic Disease Virus, Epizootic immunology, Humans, Livestock, North America epidemiology, Reoviridae Infections epidemiology, Reoviridae Infections prevention & control, Reoviridae Infections transmission, Sheep, Arthropod Vectors virology, Bluetongue epidemiology, Orbivirus immunology, Reoviridae Infections veterinary, Viral Vaccines immunology

Abstract

Orbiviruses are members of the Reoviridae family and include bluetongue virus (BTV) and epizootic hemorrhagic disease virus (EHDV). These viruses are the cause of significant regional disease outbreaks among livestock and wildlife in the United States, some of which have been characterized by significant morbidity and mortality. Competent vectors are clearly present in most regions of the globe; therefore, all segments of production livestock are at risk for serious disease outbreaks. Animals with subclinical infections also serve as reservoirs of infection and often result in significant trade restrictions. The economic and explicit impacts of BTV and EHDV infections are difficult to measure, but infections are a cause of economic loss for producers and loss of natural resources (wildlife). In response to United States Animal Health Association (USAHA) Resolution 16, the US Department of Agriculture (USDA), in collaboration with the Department of the Interior (DOI), organized a gap analysis workshop composed of international experts on Orbiviruses. The workshop participants met at the Arthropod-Borne Animal Diseases Research Unit in Manhattan, KS, May 14-16, 2013, to assess the available scientific information and status of currently available countermeasures to effectively control and mitigate the impact of an outbreak of an emerging Orbivirus with epizootic potential, with special emphasis given to BTV and EHDV. In assessing the threats, workshop participants determined that available countermeasures are somewhat effective, but several weaknesses were identified that affect their ability to prevent and control disease outbreaks effectively.

Published

2015

104. Diagnostic Tools for Bluetongue and Epizootic Hemorrhagic Disease Viruses Applicable to North American Veterinary Diagnosticians.

Author

Wilson WC, Daniels P, Ostlund EN, Johnson DE, Oberst RD, Hairgrove TB, Mediger J, and McIntosh MT

Subjects

Animals, Bluetongue virus genetics, Bluetongue virus immunology, Genotype, Hemorrhagic Disease Virus, Epizootic genetics, Hemorrhagic Disease Virus, Epizootic immunology, High-Throughput Nucleotide Sequencing veterinary, North America, Reoviridae Infections diagnosis, Reverse Transcriptase Polymerase Chain Reaction veterinary, Sequence Analysis, DNA veterinary, Sheep, Bluetongue diagnosis, Bluetongue virus isolation & purification, Genotyping Techniques veterinary, Hemorrhagic Disease Virus, Epizootic isolation & purification, Reoviridae Infections veterinary

Abstract

This review provides an overview of current and potential new diagnostic tests for bluetongue (BT) and epizootic hemorrhagic disease (EHD) viruses compiled from international participants of the Orbivirus Gap Analysis Workshop, Diagnostic Group. The emphasis of this review is on diagnostic tools available to North American veterinary diagnosticians. Standard diagnostic tests are readily available for BT/EHD viruses, and there are described tests that are published in the World Organization for Animal Health (OIE) Terrestrial Manual. There is however considerable variation in the diagnostic approach to these viruses. Serological assays are well established, and many laboratories are experienced in running these assays. Numerous nucleic acid amplification assays are also available for BT virus (BTV) and EHD virus (EHDV). Although there is considerable experience with BTV reverse-transcriptase PCR (RT-PCR), there are no standards or comparisons of the protocols used by various state and federal veterinary diagnostic laboratories. Methods for genotyping BTV and EHDV isolates are available and are valuable tools for monitoring and analyzing circulating viruses. These methods include RT-PCR panels or arrays, RT-PCR and sequencing of specific genome segments, or the use of next-generation sequencing. In addition to enabling virus characterization, use of advanced molecular detection methods, including DNA microarrays and next-generation sequencing, significantly enhance the ability to detect unique virus strains that may arise through genetic drift, recombination, or viral genome segment reassortment, as well as incursions of new virus strains from other geographical areas.

Published

2015

105. Whole Genome Sequence of Multiple Myeloma-Prone C57BL/KaLwRij Mouse Strain Suggests the Origin of Disease Involves Multiple Cell Types.

Author

Amend SR, Wilson WC, Chu L, Lu L, Liu P, Serie D, Su X, Xu Y, Wang D, Gramolini A, Wen XY, O'Neal J, Hurchla M, Vachon CM, Colditz G, Vij R, Weilbaecher KN, and Tomasson MH

Subjects

Adaptor Proteins, Vesicular Transport genetics, Adaptor Proteins, Vesicular Transport metabolism, Animals, Genome-Wide Association Study, Humans, Mice, Neoplasm Proteins genetics, Neoplasm Proteins metabolism, Point Mutation, Receptors, Tumor Necrosis Factor genetics, Receptors, Tumor Necrosis Factor metabolism, Stromal Cells metabolism, Stromal Cells pathology, B-Lymphocytes metabolism, B-Lymphocytes pathology, Bone Marrow Cells metabolism, Bone Marrow Cells pathology, Macrophages metabolism, Macrophages pathology, Multiple Myeloma genetics, Multiple Myeloma metabolism, Multiple Myeloma pathology, Polymorphism, Single Nucleotide

Abstract

Monoclonal gammopathy of undetermined significance (MGUS) is the requisite precursor to multiple myeloma (MM), a malignancy of antibody-producing plasma B-cells. The genetic basis of MGUS and its progression to MM remains poorly understood. C57BL/KaLwRij (KaLwRij) is a spontaneously-derived inbred mouse strain with a high frequency of benign idiopathic paraproteinemia (BIP), a phenotype with similarities to MGUS including progression to MM. Using mouse haplotype analysis, human MM SNP array data, and whole exome and whole genome sequencing of KaLwRij mice, we identified novel KaLwRij gene variants, including deletion of Samsn1 and deleterious point mutations in Tnfrsf22 and Tnfrsf23. These variants significantly affected multiple cell types implicated in MM pathogenesis including B-cells, macrophages, and bone marrow stromal cells. These data demonstrate that multiple cell types contribute to MM development prior to the acquisition of somatic driver mutations in KaLwRij mice, and suggest that MM may an inherently non-cell autonomous malignancy.

Published

2015

106. Perioperative Point-of-Care Ultrasonography: An Emerging Technology to Be Embraced by Anesthesiologists.

Author

Ramsingh D, Fox JC, and Wilson WC

Subjects

Female, Humans, Male, Ultrasonography, Postoperative Complications diagnostic imaging, Urinary Bladder diagnostic imaging, Urinary Retention diagnostic imaging

Published

2015

107. A human mitochondrial poly(A) polymerase mutation reveals the complexities of post-transcriptional mitochondrial gene expression.

Author

Wilson WC, Hornig-Do HT, Bruni F, Chang JH, Jourdain AA, Martinou JC, Falkenberg M, Spåhr H, Larsson NG, Lewis RJ, Hewitt L, Baslé A, Cross HE, Tong L, Lebel RR, Crosby AH, Chrzanowska-Lightowlers ZM, and Lightowlers RN

Subjects

Fibroblasts metabolism, Gene Expression, Humans, Mitochondrial Proteins genetics, Mutation, Neoplasm Proteins metabolism, Oxidative Phosphorylation, Polynucleotide Adenylyltransferase genetics, Primary Cell Culture, RNA Processing, Post-Transcriptional, RNA, Mitochondrial, RNA-Binding Proteins metabolism, Mitochondrial Proteins metabolism, Polynucleotide Adenylyltransferase metabolism, RNA, Messenger metabolism

Abstract

The p.N478D missense mutation in human mitochondrial poly(A) polymerase (mtPAP) has previously been implicated in a form of spastic ataxia with optic atrophy. In this study, we have investigated fibroblast cell lines established from family members. The homozygous mutation resulted in the loss of polyadenylation of all mitochondrial transcripts assessed; however, oligoadenylation was retained. Interestingly, this had differential effects on transcript stability that were dependent on the particular species of transcript. These changes were accompanied by a severe loss of oxidative phosphorylation complexes I and IV, and perturbation of de novo mitochondrial protein synthesis. Decreases in transcript polyadenylation and in respiratory chain complexes were effectively rescued by overexpression of wild-type mtPAP. Both mutated and wild-type mtPAP localized to the mitochondrial RNA-processing granules thereby eliminating mislocalization as a cause of defective polyadenylation. In vitro polyadenylation assays revealed severely compromised activity by the mutated protein, which generated only short oligo(A) extensions on RNA substrates, irrespective of RNA secondary structure. The addition of LRPPRC/SLIRP, a mitochondrial RNA-binding complex, enhanced activity of the wild-type mtPAP resulting in increased overall tail length. The LRPPRC/SLIRP effect although present was less marked with mutated mtPAP, independent of RNA secondary structure. We conclude that (i) the polymerase activity of mtPAP can be modulated by the presence of LRPPRC/SLIRP, (ii) N478D mtPAP mutation decreases polymerase activity and (iii) the alteration in poly(A) length is sufficient to cause dysregulation of post-transcriptional expression and the pathogenic lack of respiratory chain complexes., (© The Author 2014. Published by Oxford University Press.)

Published

2014

108. Evaluation of lamb and calf responses to Rift Valley fever MP-12 vaccination.

Author

Wilson WC, Bawa B, Drolet BS, Lehiy C, Faburay B, Jasperson DC, Reister L, Gaudreault NN, Carlson J, Ma W, Morozov I, McVey DS, and Richt JA

Subjects

Age Factors, Animals, Antibodies, Viral blood, Cattle, Cattle Diseases virology, Host Specificity, Humans, Immunity, Active, Rift Valley Fever prevention & control, Rift Valley Fever virology, Rift Valley fever virus immunology, Sheep, Sheep Diseases virology, Sheep, Domestic, Vaccination veterinary, Vaccines, Attenuated, Viral Load, Viral Vaccines administration & dosage, Cattle Diseases prevention & control, Rift Valley Fever veterinary, Sheep Diseases prevention & control, Viral Vaccines immunology

Abstract

Rift Valley fever (RVF) is an important viral disease of animals and humans in Africa and the Middle East that is transmitted by mosquitoes. The disease is of concern to international agricultural and public health communities. The RVFV MP-12 strain has been the most safety tested attenuated vaccine strain; thus it is being considered as a potential vaccine for the US national veterinary stockpile. This study was designed to establish safety protocols for large animal research with virulent RVF viruses, establish a target host immune response baseline using RVF MP-12 strain, and independently evaluate this strain as a potential US emergency response vaccine. Ten, approximately four month-old lambs and calves were vaccinated with RVF MP-12 strain; two additional animals per species provided negative control specimens. The animals were monitored for clinical and immune response, fever, and viremia. Two animals per species were sacrificed on 2, 3, 4, 10 and 28 days post infection and full necropsies were performed for histopathological examination. No clinical or febrile responses were observed in this study. The onset and titer of the immune response is discussed. There was no significant histopathology in the lambs; however, 6 out of 10 vaccinated calves had multifocal, random areas of hepatocellular degeneration and necrosis. RVF MP12 antigen was detected in these areas of necrosis by immunohistochemistry in one calf. This study provides independent and baseline information on the RVF MP-12 attenuated vaccination in vaccine relevant age target species and indicates the importance of performing safety testing on vaccine relevant aged target animals., (Published by Elsevier B.V.)

Published

2014

109. Whole genome sequencing and phylogenetic analysis of Bluetongue virus serotype 2 strains isolated in the Americas including a novel strain from the western United States.

Author

Gaudreault NN, Mayo CE, Jasperson DC, Crossley BM, Breitmeyer RE, Johnson DJ, Ostlund EN, MacLachlan NJ, and Wilson WC

Subjects

Animals, Bluetongue virus genetics, Bluetongue virus isolation & purification, California, Cattle, Whole Genome Sequencing veterinary, Bluetongue virology, Bluetongue virus classification, Cattle Diseases virology, Genome, Viral

Abstract

Bluetongue is a potentially fatal arboviral disease of domestic and wild ruminants that is characterized by widespread edema and tissue necrosis. Bluetongue virus (BTV) serotypes 10, 11, 13, and 17 occur throughout much of the United States, whereas serotype 2 (BTV-2) was previously only detected in the southeastern United States. Since 1998, 10 other BTV serotypes have also been isolated from ruminants in the southeastern United States. In 2010, BTV-2 was identified in California for the first time, and preliminary sequence analysis indicated that the virus isolate was closely related to BTV strains circulating in the southeastern United States. In the current study, the whole genome sequence of the California strain of BTV-2 was compared with those of other BTV-2 strains in the Americas. The results of the analysis suggest co-circulation of genetically distinct viruses in the southeastern United States, and further suggest that the 2010 western isolate is closely related to southeastern strains of BTV. Although it remains uncertain as to how this novel virus was translocated to California, the findings of the current study underscore the need for ongoing surveillance of this economically important livestock disease.

Published

2014

110. Efficacy of a recombinant Rift Valley fever virus MP-12 with NSm deletion as a vaccine candidate in sheep.

Author

Weingartl HM, Nfon CK, Zhang S, Marszal P, Wilson WC, Morrill JC, Bettinger GE, and Peters CJ

Subjects

Animals, Antibodies, Neutralizing blood, Antibodies, Viral blood, Immunity, Cellular, Interferon-gamma immunology, Neutralization Tests, RNA, Viral blood, Rift Valley Fever prevention & control, Rift Valley fever virus, Sheep, Sheep Diseases virology, Vaccines, Attenuated immunology, Viremia prevention & control, Rift Valley Fever veterinary, Sheep Diseases prevention & control, Viral Vaccines immunology

Abstract

Rift Valley fever virus (RVFV), a mosquito-borne virus in the Bunyaviridae family and Phlebovirus genus, causes RVF, a disease of ruminants and man, endemic in Sub-Saharan African countries. However, outbreaks in Yemen and Saudi Arabia demonstrate the ability for RVFV to spread into virgin territory and thus the need exists to develop safe and efficacious vaccines that can be used outside the endemic zones. Commercial RVFV vaccines are available but have limitations that prevent their use in disease-free countries. Consequently, there are ongoing efforts to develop and/or improve RVFV vaccines with global acceptability. In this study a previously developed MP-12-derived vaccine candidate with a large deletion of the NSm gene in the pre Gn region of the M segment (arMP-12-ΔNSm21/384) developed by T. Ikegami, that was already shown to be safe in pregnant sheep causing neither abortion nor fetal malformation was further evaluated. This vaccine was tested for protection of sheep from viremia and fever following challenge with virulent RVFV ZH501 strain. A single vaccination with arMP-12-ΔNSm21/384 fully protected sheep when challenged four weeks post vaccination, thereby demonstrating that this vaccine is efficacious in protecting these animals from RVFV infection., (Crown Copyright © 2014. Published by Elsevier Ltd. All rights reserved.)

Published

2014

111. Development of a Rift Valley fever virus viremia challenge model in sheep and goats.

Author

Weingartl HM, Miller M, Nfon C, and Wilson WC

Subjects

Aedes, Animals, Antibodies, Neutralizing blood, Antibodies, Viral blood, Chlorocebus aethiops, Goat Diseases virology, RNA, Viral blood, Sheep Diseases virology, Vero Cells, Virus Cultivation, Disease Models, Animal, Goats virology, Rift Valley Fever veterinary, Rift Valley fever virus, Sheep virology, Viremia

Abstract

Rift Valley fever virus (RVFV), a member of the family Bunyaviridae, causes severe to fatal disease in newborn ruminants, as well as abortions in pregnant animals; both preventable by vaccination. Availability of a challenge model is a pre-requisite for vaccine efficacy trials. Several modes of inoculation with RVFV ZH501 were tested on goats and sheep. Differences in development of infectious viremia were observed between animals inoculated with RVFV produced in mosquito C6/36 cells compared to Vero E6 cell-produced inoculum. Only C6/36-RVFV inoculation led to development of viremia in all inoculated sheep and goats. The C6/36 cell-produced RVFV appeared to be more infectious with earlier onset of viremia, especially in sheep, and may also more closely represent a field situation. Goats were somewhat more resistant to the disease development with lower and shorter infectious virus viremia, and with only some animals developing transient increase in rectal temperature in contrast to sheep. In conclusion, a challenge protocol suitable for goat and sheep vaccine efficacy studies was developed using subcutaneous inoculation of 10(7)PFU per animal with RVFV ZH501 produced in C6/36 cells., (Crown Copyright © 2014. Published by Elsevier Ltd. All rights reserved.)

Published

2014

112. Rift Valley fever virus incorporates the 78 kDa glycoprotein into virions matured in mosquito C6/36 cells.

Author

Weingartl HM, Zhang S, Marszal P, McGreevy A, Burton L, and Wilson WC

Subjects

Amino Acid Sequence, Animals, Cell Line, Glycoproteins chemistry, Glycoproteins genetics, Microscopy, Immunoelectron, Molecular Sequence Data, Rift Valley fever virus genetics, Viral Proteins chemistry, Viral Proteins genetics, Culicidae virology, Rift Valley fever virus pathogenicity, Virion physiology

Abstract

Rift Valley fever virus (RVFV), genus Phlebovirus, family Bunyaviridae is a zoonotic arthropod-borne virus able to transition between distant host species, causing potentially severe disease in humans and ruminants. Viral proteins are encoded by three genomic segments, with the medium M segment coding for four proteins: nonstructural NSm protein, two glycoproteins Gn and Gc and large 78 kDa glycoprotein (LGp) of unknown function. Goat anti-RVFV polyclonal antibody and mouse monoclonal antibody, generated against a polypeptide unique to the LGp within the RVFV proteome, detected this protein in gradient purified RVFV ZH501 virions harvested from mosquito C6/36 cells but not in virions harvested from the mammalian Vero E6 cells. The incorporation of LGp into the mosquito cell line - matured virions was confirmed by immune-electron microscopy. The LGp was incorporated into the virions immediately during the first passage in C6/36 cells of Vero E6 derived virus. Our data indicate that LGp is a structural protein in C6/36 mosquito cell generated virions. The protein may aid the transmission from the mosquitoes to the ruminant host, with a possible role in replication of RVFV in the mosquito host. To our knowledge, this is a first report of different protein composition between virions formed in insect C6/36 versus mammalian Vero E6 cells.

Published

2014

113. Development of a Rift Valley fever real-time RT-PCR assay that can detect all three genome segments.

Author

Wilson WC, Romito M, Jasperson DC, Weingartl H, Binepal YS, Maluleke MR, Wallace DB, van Vuren PJ, and Paweska JT

Subjects

Animals, DNA Primers genetics, Genome, Viral genetics, Humans, Real-Time Polymerase Chain Reaction standards, Reference Standards, Reverse Transcriptase Polymerase Chain Reaction standards, Rift Valley Fever virology, Sensitivity and Specificity, Molecular Diagnostic Techniques methods, Real-Time Polymerase Chain Reaction methods, Reverse Transcriptase Polymerase Chain Reaction methods, Rift Valley Fever diagnosis, Rift Valley Fever veterinary, Rift Valley fever virus isolation & purification

Abstract

Outbreaks of Rift Valley fever in Kenya, Madagascar, Mauritania, and South Africa had devastating effects on livestock and human health. In addition, this disease is a food security issue for endemic countries. There is growing concern for the potential introduction of RVF into non-endemic countries. A number of single-gene target amplification assays have been developed for the rapid detection of RVF viral RNA. This paper describes the development of an improved amplification assay that includes two confirmatory target RNA segments (L and M) and a third target gene, NSs, which is deleted in the Clone 13 commercial vaccine and other candidate vaccines. The assay also contains an exogenous RNA control added during the PCR setup for detection of amplification inhibitors. The assay was evaluated initially with samples from experimentally infected animals, after which clinical veterinary and human samples from endemic countries were tested for further evaluation. The assay has a sensitivity range of 66.7-100% and a specificity of 92.0-100% depending on the comparison. The assay has an overall sensitivity of 92.5%, specificity of 95% and a positive predictive value of 98.7%. The single-tube assay provides confirmation of the presence of RVFV RNA for improved confidence in diagnostic results and a "differentiate infected from vaccinated animals" (DIVA)--compatible marker for RVFV NSs--deleted vaccines, which is useful for RVF endemic countries, but especially important in non-endemic countries., (Published by Elsevier B.V.)

Published

2013

114. Experimental infection of white-tailed deer (Odocoileus virginianus) with Northern European bluetongue virus serotype 8.

Author

Drolet BS, Reister LM, Rigg TD, Nol P, Podell BK, Mecham JO, VerCauteren KC, van Rijn PA, Wilson WC, and Bowen RA

Subjects

Animals, Antibodies, Viral immunology, Bluetongue immunology, Bluetongue virus classification, Bluetongue virus genetics, Bluetongue virus immunology, Deer immunology, Europe, North America, Seasons, Sheep immunology, Sheep Diseases immunology, Sheep Diseases virology, Bluetongue virology, Bluetongue virus physiology, Deer virology

Abstract

Bluetongue (BT) is an insect-transmitted, economically important disease of domestic and wild ruminants. Although only five of the 26 reported bluetongue virus (BTV) serotypes are considered endemic to the USA, 10 exotic serotypes have been isolated primarily in the southeastern region of the country since 1999. For an exotic BTV serotype to become endemic there must be susceptible animal species and competent vectors. In the USA, sheep and white-tailed deer (WTD) are the primary sentinel livestock and wildlife species, respectively. In 2006, BTV-8 was introduced into Northern Europe and subsequently overwintered, causing unprecedented livestock disease and mortality during the 2006-2007 vector seasons. To assess the risk of the European strain of BTV-8 to North American WTD, and understand the role they could play after a similar introduction, eight bluetongue-seronegative WTD were inoculated with BTV-8. Body temperatures and clinical signs were recorded daily. Blood samples were analyzed for BTV RNA with quantitative real time reverse transcriptase polymerase chain reaction (qRT-PCR), serum analyzed for BTV antibodies by cELISA, and tissues taken for histopathology and qRT-PCR. All eight deer became infected and developed moderate to severe clinical disease from days 8 to 15. Peak viremia was from day 7 to 10 with detectable titers through the end of the study (28 days) in most deer. Serum antibody was detected by day 6, peaked by day 10 and continued through day 28. We conclude that North American WTD are highly susceptible to BTV-8 and would act as clinical disease sentinels and amplifying hosts during an outbreak., (Published by Elsevier B.V.)

Published

2013

115. Rift Valley fever risk map model and seroprevalence in selected wild ungulates and camels from Kenya.

Author

Britch SC, Binepal YS, Ruder MG, Kariithi HM, Linthicum KJ, Anyamba A, Small JL, Tucker CJ, Ateya LO, Oriko AA, Gacheru S, and Wilson WC

Subjects

Animals, Animals, Wild virology, Antibodies, Viral blood, Artiodactyla virology, Epidemiological Monitoring, Humans, Kenya epidemiology, Prevalence, Rift Valley Fever blood, Rift Valley Fever epidemiology, Risk, Seroepidemiologic Studies, Camelus virology, Disease Outbreaks, Rift Valley Fever veterinary, Rift Valley fever virus immunology

Abstract

Since the first isolation of Rift Valley fever virus (RVFV) in the 1930s, there have been multiple epizootics and epidemics in animals and humans in sub-Saharan Africa. Prospective climate-based models have recently been developed that flag areas at risk of RVFV transmission in endemic regions based on key environmental indicators that precede Rift Valley fever (RVF) epizootics and epidemics. Although the timing and locations of human case data from the 2006-2007 RVF outbreak in Kenya have been compared to risk zones flagged by the model, seroprevalence of RVF antibodies in wildlife has not yet been analyzed in light of temporal and spatial predictions of RVF activity. Primarily wild ungulate serum samples from periods before, during, and after the 2006-2007 RVF epizootic were analyzed for the presence of RVFV IgM and/or IgG antibody. Results show an increase in RVF seropositivity from samples collected in 2007 (31.8%), compared to antibody prevalence observed from 2000-2006 (3.3%). After the epizootic, average RVF seropositivity diminished to 5% in samples collected from 2008-2009. Overlaying maps of modeled RVF risk assessments with sampling locations indicated positive RVF serology in several species of wild ungulate in or near areas flagged as being at risk for RVF. Our results establish the need to continue and expand sero-surveillance of wildlife species Kenya and elsewhere in the Horn of Africa to further calibrate and improve the RVF risk model, and better understand the dynamics of RVFV transmission.

Published

2013

116. Novel serotype of bluetongue virus, western North America.

Author

Maclachlan NJ, Wilson WC, Crossley BM, Mayo CE, Jasperson DC, Breitmeyer RE, and Whiteford AM

Subjects

Animals, Bluetongue virology, Bluetongue virus classification, Bluetongue virus isolation & purification, Cattle, Cattle Diseases virology, Ceratopogonidae virology, DNA, Viral classification, DNA, Viral isolation & purification, Insect Vectors virology, North America epidemiology, Phylogeny, Reverse Transcriptase Polymerase Chain Reaction, Sequence Analysis, DNA, Serotyping, Bluetongue epidemiology, Bluetongue virus genetics, Cattle Diseases epidemiology, DNA, Viral genetics

Published

2013

117. Surface-enhanced Raman scattering (SERS) detection of multiple viral antigens using magnetic capture of SERS-active nanoparticles.

Author

Neng J, Harpster MH, Wilson WC, and Johnson PA

Subjects

Antigens, Viral immunology, Equipment Design, Equipment Failure Analysis, Light, Nanoparticles ultrastructure, Reproducibility of Results, Scattering, Radiation, Sensitivity and Specificity, Surface Properties, Antigens, Viral analysis, Biosensing Techniques instrumentation, Immunomagnetic Separation instrumentation, Nanoparticles chemistry, Spectrum Analysis, Raman instrumentation

Abstract

A highly sensitive immunoassay based on surface-enhanced Raman scattering (SERS) spectroscopy has been developed for multiplex detection of surface envelope and capsid antigens of the viral zoonotic pathogens West Nile virus (WNV) and Rift Valley fever virus (RVFV). Detection was mediated by antibody recognition using Raman reporter-coated Au nanoparticles (GNPs) and paramagnetic nanoparticles (PMPs) conjugated with polyclonal antibodies specific for each antigen target, followed by 785nm laser excitation of magnetically concentrated GNP/antigen/PMP complexes. The discrimination of WNV and RVFV antigen detection in mixed Raman spectra was achieved by SERS enhancement of Raman spectra specific for the Raman reporter dyes Infrared 792 (IR-792) and Nile Blue (NB), respectively. Assay reactions containing dilutions of both target antigens yielded a reduction in the intensification of IR-792 and NB signature spectrum peaks and provided a conservative limit of detection of ∼5fg/ml for assays conducted in phosphate buffered saline buffer (PBS) and ∼25pg/ml for assays containing PBS spiked with fetal bovine serum. Based on the inherent simplicity of the assay, magnetic capture-based SERS assays afford promise as a biosensor platform that provides high-level multiplex detection sensitivity and can be adapted for portable diagnostic applications in limited resource settings., (Copyright © 2012 Elsevier B.V. All rights reserved.)

Published

2013

118. Diagnostic approaches for Rift Valley fever.

Author

Wilson WC, Weingartl HM, Drolet BS, Davé K, Harpster MH, Johnson PA, Faburay B, Ruder MG, Richt JA, and McVey DS

Subjects

Africa South of the Sahara, Animals, Biosensing Techniques veterinary, Disease Outbreaks prevention & control, Disease Outbreaks veterinary, Genome, Viral, Genomics, Global Health, Nucleic Acid Amplification Techniques, Rift Valley Fever diagnosis, Rift Valley Fever veterinary, Ruminants, Serologic Tests veterinary

Abstract

Disease outbreaks caused by arthropod-borne animal viruses (arboviruses) resulting in significant livestock and economic losses world-wide appear to be increasing. Rift Valley fever (RVF) virus is an important arbovirus that causes lethal disease in cattle, camels, sheep and goats in Sub-Saharan Africa. There is concern that this virus could spread because of global warming, increased animal trade or through bioterrorism. This paper discusses the current and developing approaches to diagnosis of RVF. Diagnostic assays are available for RVF, but availability can be limited and there is a need for global harmonization. Continued improvement of standard serological and viral genome amplification approaches, including new embedded/syndromic testing, biosensor, emerging virus detection and characterization technologies is needed.

Published

2013

119. Race/ethnicity and mental health in the first decade of the 21st century.

Author

Rosenthal BS and Wilson WC

Subjects

Adolescent, Affective Symptoms epidemiology, Anxiety Disorders epidemiology, Cross-Sectional Studies, Depressive Disorder epidemiology, Educational Status, Emotions, Female, Health Surveys, Humans, Male, New York City, Socioeconomic Factors, Surveys and Questionnaires, Urban Population, Young Adult, Affective Symptoms ethnology, Anxiety Disorders ethnology, Depressive Disorder ethnology, Ethnicity psychology, Mental Health ethnology

Abstract

Recent empirical studies on mental health generally report racial/ ethnic differences in depression rates but typically do not control for potential confounding by sample contextual variations in historical epoch, geographical location, and social demography. An empirical study of race/ethnicity differences in psychological distress is reported as an attempt to control these contexts by using a sample that is homogeneous in age, historical epoch, geography, and social demography (954 youth ages 18-19 living in a single, large urban community). No mean differences in psychological distress were observed among four racial/ethnic groups: Asians, African Americans, Latinos, and non-Hispanic Whites. A second analysis compared 17 different racial/ethnic groups defined in terms of family national origin. No differences in psychological distress were found among these groups. The findings are consistent with the view that race/ethnicity itself is not related to disparities in mental health.

Published

2012

120. Surface-enhanced Raman scattering detection of DNAs derived from virus genomes using Au-coated paramagnetic nanoparticles.

Author

Zhang H, Harpster MH, Wilson WC, and Johnson PA

Subjects

DNA chemistry, Genome, Viral genetics, Gold chemistry, Metal Nanoparticles chemistry, Nanotechnology methods, Spectrum Analysis, Raman methods

Abstract

A magnetic capture-based, surface-enhanced Raman scattering (SERS) assay for DNA detection has been developed which utilizes Au-coated paramagnetic nanoparticles (Au@PMPs) as both a SERS substrate and effective bioseparation reagent for the selective removal of target DNAs from solution. Hybridization reactions contained two target DNAs, sequence complementary reporter probes conjugated with spectrally distinct Raman dyes distinct for each target, and Au@PMPs conjugated with sequence complementary capture probes. In this case, target DNAs were derived from the RNA genomes of the Rift Valley Fever virus (RVFV) or West Nile virus (WNV). The hybridization reactions were incubated for a short period and then concentrated within the focus beam of an interrogating laser by magnetic pull-down. The attendant SERS response of each individually captured DNA provided a limit of detection sensitivity in the range 20-100 nM. X-ray diffraction and UV-vis analysis validated both the desired surface plasmon resonance properties and bimetallic composition of synthesized Au@PMPs, and UV-vis spectroscopy confirmed conjugation of the Raman dye compounds malachite green (MG) and erythrosin B (EB) with the RVFV and WNV reporter probes, respectively. Finally, hybridization reactions assembled for multiplexed detection of both targets yielded mixed MG/EB spectra and clearly differentiated peaks which facilitate the quantitative detection of each DNA target. On the basis of the simple design of a single-particle DNA detection assay, the opportunity is provided to develop magnetic capture-based SERS assays that are easily assembled and adapted for high-level multiplex detection using low-cost Raman instrumentation., (© 2012 American Chemical Society)

Published

2012

121. Development and evaluation of one-step rRT-PCR and immunohistochemical methods for detection of Rift Valley fever virus in biosafety level 2 diagnostic laboratories.

Author

Drolet BS, Weingartl HM, Jiang J, Neufeld J, Marszal P, Lindsay R, Miller MM, Czub M, and Wilson WC

Subjects

Animals, Cattle, Rabbits, Rift Valley Fever diagnosis, Rift Valley Fever virology, Sheep, Specimen Handling methods, Viremia diagnosis, Viremia veterinary, Viremia virology, Virology methods, Virus Inactivation, Disinfection methods, Immunohistochemistry methods, Molecular Diagnostic Techniques methods, Real-Time Polymerase Chain Reaction methods, Reverse Transcriptase Polymerase Chain Reaction methods, Rift Valley Fever veterinary, Rift Valley fever virus isolation & purification

Abstract

Rift Valley fever virus (RVFV) is a zoonotic insect transmitted virus endemic to Africa and the Arabian Peninsula. Infection causes abortions and high mortality in newborn ruminants. The overall human infection rate is <1%; however, fatality rates in those with severe clinical disease have been reported as high as 29%. The potential of RVFV as a bioterrorism agent and/or being accidentally introduced into North America is widely recognized. Currently, regional veterinary biosafety level 2 (BSL-2) diagnostic laboratories lack safe, modern, validated diagnostic tests to detect RVFV. An existing one-step real-time RT-PCR (rRT-PCR) assay was modified for quick virus inactivation for use in BSL-2 laboratories, evaluated on serum and tissue samples from experimentally infected lambs and calves, and compared to virus isolation. Viremia was detected in all inoculated sheep with titers reaching 10(6.5) plaque forming units/ml, or up to 10(10) viral RNA copies/ml. Viremia in calves was lower and not detected in all inoculated animals; however, all animals became transiently febrile and were infected as determined by rRT-PCR of tissues. Virus was isolated from rRT-PCR-positive liver and/or spleen in 33% of lamb and 41% of calf samples between 2 and 7 days post inoculation. For RVFV antigen detection, reagents are typically produced at BSL-3Ag or BSL-4 conditions and require inactivation and safety testing for use outside of containment. In this study, antiserum against recombinant RVFV-nucleocapsid (N) was produced to develop an immunohistochemical (IHC) assay which was subsequently evaluated on formalin fixed lamb and calf tissues at BSL-2 laboratory conditions. Antigen was detected by IHC in 79% of rRT-PCR-positive sheep and 70% of rRT-PCR-positive calf tissues tested. Once validated and approved by national regulatory agencies, these assays can be safely produced and distributed to regional diagnostic laboratories, providing capacity for early detection of RVFV in suspected ruminant samples., (Copyright © 2011 Elsevier B.V. All rights reserved.)

Published

2012

122. Surface-enhanced Raman scattering detection of DNA derived from the west nile virus genome using magnetic capture of Raman-active gold nanoparticles.

Author

Zhang H, Harpster MH, Park HJ, Johnson PA, and Wilson WC

Subjects

Base Sequence, DNA, Viral chemistry, DNA, Viral genetics, Lasers, Light, Limit of Detection, Nucleic Acid Hybridization, Oligonucleotide Probes chemistry, Oligonucleotide Probes genetics, Photoelectron Spectroscopy, Scattering, Radiation, Surface Properties, DNA, Viral analysis, Genome, Viral genetics, Gold chemistry, Magnetics, Metal Nanoparticles chemistry, Spectrum Analysis, Raman methods, West Nile virus genetics

Abstract

A model paramagnetic nanoparticle (MNP) assay is demonstrated for surface-enhanced Raman scattering (SERS) detection of DNA oligonucleotides derived from the West Nile virus (WNV) genome. Detection is based on the capture of WNV target sequences by hybridization with complementary oligonucleotide probes covalently linked to fabricated MNPs and Raman reporter tag-conjugated gold nanoparticles (GNPs) and the subsequent removal of GNP-WNV target sequence-MNP hybridization complexes from solution by an externally applied magnetic source. Laser excitation of the pelleted material provided a signature SERS spectrum which is diagnostic for the reporter, 5,5'-dithiobis(succinimidy-2-nitrobenzoate) (DSNB), and restricted to hybridization reactions containing WNV target sequences. Hybridizations containing dilutions of the target oligonucleotide were characterized by a reduction in the intensification of the spectral peaks accorded to the SERS signaling of DSNB, and the limit of detection for target sequence in buffer was 10 pM. Due to the short hybridization times required to conduct the assay and ease with which reproducible Raman spectra can be acquired, the assay is amenable to adaptation within a portable, user-friendly Raman detection platform for nucleic acids.

Published

2011

123. A versatile SERS-based immunoassay for immunoglobulin detection using antigen-coated gold nanoparticles and malachite green-conjugated protein A/G.

Author

Neng J, Harpster MH, Zhang H, Mecham JO, Wilson WC, and Johnson PA

Subjects

Animals, Antibodies, Viral analysis, Antigens, Viral, Bacterial Proteins, Enzyme-Linked Immunosorbent Assay, Gold Colloid, Metal Nanoparticles, Quartz Crystal Microbalance Techniques, Rabbits, Rosaniline Dyes, Spectrum Analysis, Raman, West Nile virus immunology, Biosensing Techniques methods, Immunoassay methods, Immunoglobulins analysis

Abstract

A surface enhanced Raman scattering (SERS) immunoassay for antibody detection in serum is described in the present work. The developed assay is conducted in solution and utilizes Au nanoparticles coated with the envelope (E) protein of West Nile Virus (WNV) as the SERS-active substrate and malachite green (MG)-conjugated protein A/G (MG-pA/G) as a bi-functional Raman tag/antibody binding reporter. Upon incubation of these reagents with serum collected from rabbits inoculated with E antigen, laser interrogation of the sandwiched immunocomplex revealed a SERS signaling response diagnostic for MG. The intensification of signature spectral peaks is shown to be proportionate to the concentration of added serum and the limit of antibody detection is 2 ng/ml of serum. To assess assay performance relative to more a traditional immunoassay, indirect enzyme-linked immunosorbent assays conducted using the same concentrations of reagents were found to be >400-fold less sensitive. Quartz crystal microbalance with dissipation (QCM-D) monitoring of immunocomplex film deposition on solid Au surfaces also confirmed the formation of antigen-antibody-protein A/G trilayers and provided quantitative measurements of film thickness which likely position MG within the sensing distance of laser-elicited, enhanced electromagnetic fields. The sensitivity and inherent versatility of the assay, which is provided by the binding of pA/G to a broad spectrum of immunoglobulins in different mammalian species, suggest that it could be developed as an alternative immunoassay format to the ELISA., (Copyright © 2010 Elsevier B.V. All rights reserved.)

Published

2010

124. Time to play harmoniously with other specialties.

Author

Wilson WC and Manecke G

Subjects

Clinical Competence, Humans, Internet, Cooperative Behavior, Interprofessional Relations, Medicine

Published

2010

125. Potential for North American mosquitoes (Diptera: Culicidae) to transmit rift valley fever virus.

Author

Turell MJ, Wilson WC, and Bennett KE

Subjects

Animals, Cricetinae, Culicidae physiology, Female, Mesocricetus, Rift Valley Fever virology, Viremia, Culicidae virology, Insect Vectors virology, Rift Valley Fever transmission, Rift Valley fever virus physiology

Abstract

To determine which arthropods should be targeted for control should Rift Valley fever virus (RVFV) be detected in North America, we evaluated Culex erraticus (Dyar and Knab), Culex erythrothorax Dyar, Culex nigripalpus Theobald, Culex pipiens L., Culex quinquefasciatus Say, Culex tarsalis Coquillett, Aedes dorsalis (Wiedemann), Aedes vexans (Meigen), Anopheles quadrimaculatus Say, and Culicoides sonorensis Wirth and Jones from the western, midwestern, and southern United States for their ability to transmit RVFV. Female mosquitoes were allowed to feed on adult hamsters inoculated with RVFV, after which engorged mosquitoes were incubated for 7-21 d at 260C, then allowed to refeed on susceptible hamsters, and tested to determine infection, dissemination, and transmission rates. Other specimens were inoculated intrathoracically, held for 7 d, and then allowed to feed on a susceptible hamster to check for a salivary gland barrier. When exposed to hamsters with viremias > or =10(8.8) plaque-forming units/ml blood, Cx. tarsalis transmitted RVFV efficiently (infection rate = 93%, dissemination rate = 56%, and estimated transmission rate = 52%). In contrast, when exposed to the same virus dose, none of the other species tested transmitted RVFV efficiently. Estimated transmission rates for Cx. erythrothorax, Cx. pipiens, Cx. erraticus, and Ae. dorsalis were 10, 8, 4, and 2%, respectively, and for the remaining species were < or = 1%. With the exception of Cx. tarsalis and Cx. pipiens, all species tested had moderate to major salivary gland barriers. None of the C. sonorensis became infected and none of the An. quadrimaculatus tested transmitted RVFV by bite, even after intrathoracic inoculation, indicating that these species would not be competent vectors of RVFV. Although Ae. vexans from Florida and Louisiana were relatively efficient vectors of RVFV, specimens of this species captured in Colorado or California were virtually incompetent, illustrating the need to evaluate local population for their ability to transmit a pathogen. In addition to laboratory vector competence, factors such as seasonal density, host feeding preference, longevity, and foraging behavior should be considered when determining the potential role that these species could play in RVFV transmission.

Published

2010

126. An improved real-time polymerase chain reaction for the simultaneous detection of all serotypes of Epizootic hemorrhagic disease virus.

Author

Clavijo A, Sun F, Lester T, Jasperson DC, and Wilson WC

Subjects

Animals, Base Sequence, Cell Line, Cricetinae, Gene Expression Regulation, Viral, Molecular Sequence Data, RNA, Viral genetics, Serotyping, Hemorrhagic Disease Virus, Epizootic classification, Hemorrhagic Disease Virus, Epizootic isolation & purification, Polymerase Chain Reaction methods

Abstract

Epizootic hemorrhagic disease virus (EHDV) is a significant pathogen of wild and sometimes domestic ungulates worldwide. Rapid and reliable methods for virus detection and identification play an essential part in the control of epizootic hemorrhagic disease (EHD). In the present study, a 1-step real-time polymerase chain reaction (PCR) group-specific assay was developed. The assay detects genome segment 5 (NS1) from all of the 8 serotypes of EHDV. Assay sensitivity was evaluated relative to a conventional gel-based nested PCR using cell culture-derived virus and diagnostic samples from clinically affected white-tailed deer (Odocoileus virginianus). The assay reliably amplified the NS1 gene from any of the EHDV strains tested, including isolates from each of the 8 EHDV serotypes. No cross-reactions were detected when all 24 serotypes of Bluetongue virus, a closely related member of the genus Orbivirus, were tested. A panel of 76 known EHDV-positive clinical samples was used to compare the performance of the assay relative to a previously reported real-time PCR assay. Results indicated that there was no statistically significant difference between the threshold cycle values obtained with both assays. A collection of 178 diagnostic samples submitted for EHD diagnosis was also used for test evaluation. The assay could be applied for rapid detection of EHDV in clinical samples from susceptible ruminants during an outbreak of the disease. In addition, this PCR assay has the benefits of being reliable and simple and could provide a valuable tool for studying the epidemiology of EHDV infection in susceptible ruminants by facilitating the detection of EHDV, regardless of the serotype.

Published

2010

127. Detection of a novel reassortant epizootic hemorrhagic disease virus (EHDV) in the USA containing RNA segments derived from both exotic (EHDV-6) and endemic (EHDV-2) serotypes.

Author

Allison AB, Goekjian VH, Potgieter AC, Wilson WC, Johnson DJ, Mertens PP, and Stallknecht DE

Subjects

Amino Acid Sequence, Animals, Hemorrhagic Disease Virus, Epizootic classification, Hemorrhagic Disease Virus, Epizootic genetics, Molecular Sequence Data, Phylogeny, Reassortant Viruses classification, Reassortant Viruses genetics, Reoviridae Infections virology, Sequence Alignment, United States, Viral Proteins genetics, Deer virology, Hemorrhagic Disease Virus, Epizootic isolation & purification, RNA, Viral genetics, Reassortant Viruses isolation & purification, Recombination, Genetic, Reoviridae Infections veterinary

Abstract

Epizootic hemorrhagic disease virus (EHDV) is a Culicoides-transmitted orbivirus that infects domestic and wild ruminants and is provisionally thought to be distributed throughout Africa, North America, Australia, East Asia and the Middle East. Historically, of the seven proposed serotypes of EHDV, only EHDV-1 and EHDV-2 have been reported from North America. In 2006, EHDV isolates were recovered from moribund or dead white-tailed deer (Odocoileus virginianus) in Indiana and Illinois that could not be identified as either EHDV-1 or EHDV-2 by virus neutralization tests or by serotype-specific RT-PCR. Additional serological and genetic testing identified the isolates as EHDV-6, a serotype that, although originally described from Australia, has recently been recognized as an emerging pathogen of cattle in Morocco, Algeria and Turkey. In 2007 and 2008, EHDV-6 was isolated again from white-tailed deer, this time in Missouri, Kansas and Texas, suggesting that the virus is capable of overwintering and that it may become, or already is, endemic in a geographically widespread region of the USA. Genetic characterization of the virus indicates that it is a reassortant, such that the outer capsid proteins determining serotype specificity (VP2 and VP5) are derived from exotic EHDV-6, whilst the remaining structural and non-structural proteins are apparently obtained from indigenous EHDV-2 (Alberta).

Published

2010

128. SERS detection of indirect viral DNA capture using colloidal gold and methylene blue as a Raman label.

Author

Harpster MH, Zhang H, Sankara-Warrier AK, Ray BH, Ward TR, Kollmar JP, Carron KT, Mecham JO, Corcoran RC, Wilson WC, and Johnson PA

Subjects

Staining and Labeling methods, Biosensing Techniques methods, DNA, Viral analysis, Gold Colloid chemistry, Methylene Blue, Spectrum Analysis, Raman methods

Abstract

An indirect capture model assay using colloidal Au nanoparticles is demonstrated for surface enhanced Raman scattering (SERS) spectroscopy detection of DNA. The sequence targeted for capture was derived from the West Nile Virus (WNV) RNA genome and selected on the basis of exhibiting minimal secondary structure formation. Upon incubation with colloidal Au, hybridization complexes containing the WNV target sequence, a complementary capture oligonucleotide conjugated to a strong tethering group and a complementary reporter oligonucleotide conjugated to methylene blue (MB), a Raman label, anchors the resultant ternary complex to Au nanoparticles and positions MB within the required sensing distance for SERS enhancement. The subsequent elicitation of surface enhanced plasmon resonance by laser excitation provides a spectral peak signature profile that is capture-specific and characteristic of the Raman spectrum for MB. Detection sensitivity is in the submicromolar range and was shown to be highest for thiol, and less so for amino, modifications at the 5' terminus of the capture oligonucleotide. Finally, using Quartz Crystal Microbalance-Dissipation as a tool for modeling ternary complex binding to Au surfaces, quantitative measurements of surface mass coverage on Au plated sensor crystals established a positive correlation between levels of ternary complex adsorption and their correspondent levels of SERS signal intensification. Adapted to a compact Raman spectrometer, which is designed for analyte detection in capillary tubes, this assay provides a rapid, mobile and cost effective alternative to expensive spectroscopic instrumentation, which is often restricted to analytical laboratories.

Published

2009

129. A multiplex real-time reverse transcription polymerase chain reaction assay for detection and differentiation of Bluetongue virus and Epizootic hemorrhagic disease virus serogroups.

Author

Wilson WC, Hindson BJ, O'Hearn ES, Hall S, Tellgren-Roth C, Torres C, Naraghi-Arani P, Mecham JO, and Lenhoff RJ

Subjects

Animals, Base Sequence, Bluetongue epidemiology, Bluetongue virus classification, Cattle, Cattle Diseases epidemiology, Cattle Diseases virology, Cloning, Molecular, DNA Primers, Gene Amplification, Hemorrhagic Disease Virus, Epizootic classification, Phylogeny, Reoviridae Infections epidemiology, Serotyping, Species Specificity, Bluetongue virus genetics, Hemorrhagic Disease Virus, Epizootic genetics, Reverse Transcriptase Polymerase Chain Reaction methods

Abstract

Bluetongue virus (BTV) causes disease in domestic and wild ruminants and results in significant economic loss. The closely related Epizootic hemorrhagic disease virus (EHDV) has been associated with bluetongue-like disease in cattle. Although U.S. EHDV strains have not been experimentally proven to cause disease in cattle, there is serologic evidence of infection in cattle. Therefore, rapid diagnosis and differentiation of BTV and EHDV is required. The genetic sequence information and bioinformatic analysis necessary to design a real-time reverse transcription polymerase chain reaction (RT-PCR) assay for the early detection of indigenous and exotic BTV and EHDV is described. This sequence data foundation focused on 2 conserved target genes: one that is highly expressed in infected mammalian cells, and the other is highly expressed in infected insect cells. The analysis of all BTV and EHDV prototype strains indicated that a complex primer design was necessary for both a virus group-comprehensive and virus group-specific gene amplification diagnostic test. This information has been used as the basis for the development of a rapid multiplex BTV-EHDV real-time RT-PCR that detects all known serotypes of both viruses and distinguishes between BTV and EHDV serogroups. The sensitivity of this rapid, single-tube, real-time RT-PCR assay is sufficient for diagnostic application, without the contamination problems associated with standard gel-based RT-PCR, especially nested RT-PCR tests.

Published

2009

130. Microelectrical sensors as emerging platforms for protein biomarker detection in point-of-care diagnostics.

Author

Arruda DL, Wilson WC, Nguyen C, Yao QW, Caiazzo RJ, Talpasanu I, Dow DE, and Liu BC

Subjects

Electricity, Humans, Nanoparticles, Biomarkers analysis, Biosensing Techniques, Point-of-Care Systems, Proteins analysis

Abstract

Current methods used to measure protein expression on microarrays, such as labeled fluorescent imaging, are not well suited for real-time, diagnostic measurements at the point of care. Studies have shown that microelectrical sensors utilizing silica nanowire, impedimetric, surface acoustic wave, magnetic nanoparticle and microantenna technologies have the potential to impact disease diagnosis by offering sensing characteristics that rival conventional sensing techniques. Their ability to transduce protein binding events into electrical signals may prove essential for the development of next-generation point-of-care devices for molecular diagnostics, where they could be easily integrated with microarray, microfluidic and telemetry technologies. However, common limitations associated with the microelectrical sensors, including problems with sensor fabrication and sensitivity, must first be resolved. This review describes governing technical concepts and provides examples demonstrating the use of various microelectrical sensors in the diagnosis of disease via protein biomarkers.

Published

2009

131. Field evaluation of a multiplex real-time reverse transcription polymerase chain reaction assay for detection of Vesicular stomatitis virus.

Author

Wilson WC, Letchworth GJ, Jiménez C, Herrero MV, Navarro R, Paz P, Cornish TE, Smoliga G, Pauszek SJ, Dornak C, George M, and Rodriguez LL

Subjects

Animals, Central America, Immunohistochemistry veterinary, Mexico, RNA, Viral chemistry, RNA, Viral genetics, Sensitivity and Specificity, Sequence Analysis, DNA, Vesicular Stomatitis diagnosis, Vesicular stomatitis Indiana virus genetics, Vesicular stomatitis New Jersey virus genetics, Animals, Domestic virology, Reverse Transcriptase Polymerase Chain Reaction veterinary, Vesicular Stomatitis virology, Vesicular stomatitis Indiana virus isolation & purification, Vesicular stomatitis New Jersey virus isolation & purification

Abstract

Sporadic outbreaks of vesicular stomatitis (VS) in the United States result in significant economic losses for the U.S. livestock industries because VS is a reportable disease that clinically mimics foot-and-mouth disease. Rapid and accurate differentiation of these 2 diseases is critical because their consequences and control strategies differ radically. The objective of the current study was to field validate a 1-tube multiplexed real-time reverse transcription polymerase chain reaction (real-time RT-PCR) assay for the rapid detection of Vesicular stomatitis New Jersey virus and Vesicular stomatitis Indiana virus strains occurring in Mexico and North and Central America. A comprehensive collection of 622 vesicular lesion samples obtained from cattle, horses, and swine from throughout Mexico and Central America was tested by the real-time RT-PCR assay and virus isolation. Overall, clinical sensitivity and specificity of the real-time RT-PCR were 83% and 99%, respectively. Interestingly, VS virus isolates originating from a specific region of Costa Rica were not detected by real-time RT-PCR. Sequence comparisons of these viruses with the real-time RT-PCR probe and primers showed mismatches in the probe and forward and reverse primer regions. Additional lineage-specific primers and a probe corrected the lack of detection of the missing genetic lineage. Thus, this assay reliably identified existing Mexican and Central American VS viruses and proved readily adaptable as new VS viruses were encountered. An important secondary result of this research was the collection of hundreds of new VS virus isolates that provide a foundation from which many additional studies can arise.

Published

2009

132. Detection of all eight serotypes of Epizootic hemorrhagic disease virus by real-time reverse transcription polymerase chain reaction.

Author

Wilson WC, O'Hearn ES, Tellgren-Roth C, Stallknecht DE, Mead DG, and Mecham JO

Subjects

Animals, Cattle, Hemorrhagic Disease Virus, Epizootic genetics, RNA, Viral chemistry, RNA, Viral genetics, Reoviridae Infections virology, Reverse Transcriptase Polymerase Chain Reaction veterinary, Viral Nonstructural Proteins chemistry, Viral Nonstructural Proteins genetics, Cattle Diseases virology, Hemorrhagic Disease Virus, Epizootic isolation & purification, Reoviridae Infections veterinary

Abstract

Epizootic hemorrhagic disease virus (EHDV) has been associated with bluetongue-like disease in cattle. Although U.S. EHDV strains have not been experimentally proven to cause disease in cattle, there is serologic evidence of infection. Differentiation of Bluetongue virus (BTV) and EHDV is necessary because diagnosis of infection caused by these viruses is often confused. The previously developed nested reverse transcription polymerase chain reaction (nRT-PCR) test for indigenous EHDV disease is sensitive and specific, but it is prone to contamination problems. Additionally, the EHDV nRT-PCR only detects 7 of the 8 serotypes. To develop an improved diagnostic test, sequence analysis was performed on 2 conserved target genes; one is highly expressed in infected mammalian cells, whereas the other is highly expressed in infected insect cells. This information was used to develop a rapid EHDV real-time PCR that detects all 8 EHDV serotypes. The EHDV assay did not cross-react with BTV strains and performed similarly to the nRT-PCR tests with archived clinical samples. In addition, it is superior to the nRT-PCR, not only because it is a closed system with fewer cross-contamination problems, but also because it detects all 8 serotypes and is less labor and time intensive.

Published

2009

133. Bluetongue virus serotype 17 sequence variation associated with neutralization.

Author

Wilson WC, Bernard KA, Israel BA, and Mecham JO

Subjects

Amino Acid Sequence, Animals, Bluetongue virology, Bluetongue virus classification, Capsid Proteins chemistry, Capsid Proteins genetics, Molecular Sequence Data, Mutation, Neutralization Tests, RNA, Viral analysis, Sequence Alignment, Serotyping, Sheep Diseases virology, Antibodies, Viral immunology, Bluetongue virus genetics, Bluetongue virus immunology, Genetic Variation

Abstract

Bluetongue virus (BTV) is an insect-transmitted orbivirus of importance to the cattle and sheep industry. The VP2 protein, encoded by L2, contains neutralizing epitopes. Previously, a panel of neutralizing monoclonal antibodies (MAbs) to the BTV serotype 17 (BTV-17) prototype strain was generated and it was determined that the neutralization domain consists of three overlapping epitopes. Over 30 amino acid changes were found between a neutralized BTV-17 prototype strain and a non-neutralized BTV-17 198 strain. In this study, the L2 genes from eight additional strains, representing both the neutralized and non-neutralized groups of BTV-17, were sequenced to determine the degree of conservation of the previously characterized differences. Comparison of the deduced amino acid sequences showed that 91% (30/33) of the previously noted changes were conserved within each group. The sequence of the M5 gene that encodes VP5 was also examined, since this surface protein has also been shown to affect neutralization. No consistent changes were noted between the neutralized and non-neutralized groups of BTV-17 by analysis of the VP5 protein. Finally, the L2 sequences of five MAb neutralization escape mutants were determined to identify specific amino acids involved in neutralization and perhaps virulence. All five mutants contained 1-3 amino acid changes that were in close proximity to a previously described variable region. These amino acid changes likely define critical sites in the overlapping neutralization domains previously described. This is the first description of two BT virus populations that have distinct neutralization characteristics co-circulating in a defined geographical region.

Published

2008

134. The NS3 proteins of global strains of bluetongue virus evolve into regional topotypes through negative (purifying) selection.

Author

Balasuriya UB, Nadler SA, Wilson WC, Pritchard LI, Smythe AB, Savini G, Monaco F, De Santis P, Zhang N, Tabachnick WJ, and Maclachlan NJ

Subjects

Amino Acid Sequence, Evolution, Molecular, Molecular Sequence Data, Phylogeny, Viral Nonstructural Proteins chemistry, Viral Nonstructural Proteins classification, Bluetongue virus genetics, Selection, Genetic, Viral Nonstructural Proteins genetics

Abstract

Comparison of the deduced amino acid sequences of the genes (S10) encoding the NS3 protein of 137 strains of bluetongue virus (BTV) from Africa, the Americas, Asia, Australia and the Mediterranean Basin showed limited variation. Common to all NS3 sequences were potential glycosylation sites at amino acid residues 63 and 150 and a cysteine at residue 137, whereas a cysteine at residue 181 was not conserved. The PPXY and PS/TAP late-domain motifs were conserved in all but three of the viruses. Phylogenetic analyses of these same sequences yielded two principal clades that grouped the viruses irrespective of their serotype or year of isolation (1900-2003). All viruses from Asia and Australia were grouped in one clade, whereas those from the other regions were present in both clades. Each clade segregated into distinct subclades that included viruses from single or multiple regions, and the S10 genes of some field viruses were identical to those of live-attenuated BTV vaccines. There was no evidence of positive selection on the S10 gene as assessed by reconstruction of ancestral codon states on the phylogeny, rather the functional constraints of the NS3 protein are expressed through substantial negative (purifying) selection.

Published

2008

135. A Rift Valley fever risk surveillance system for Africa using remotely sensed data: potential for use on other continents.

Author

Linthicum KJ, Anyamba A, Britch SC, Chretien JP, Erickson RL, Small J, Tucker CJ, Bennett KE, Mayer RT, Schmidtmann ET, Andreadis TG, Anderson JF, Wilson WC, Freier JE, James AM, Miller RS, Drolet BS, Miller SN, Tedrow CA, Bailey CL, Strickman DA, Barnard DR, Clark GG, and Zou L

Abstract

The authors developed a monitoring and risk mapping system using normalized difference vegetation index (NDVI) times series data derived from the advanced very high resolution radiometer (AVHRR) instrument on polar orbiting national oceanographic and atmospheric administration (NOAA) satellites to map areas with a potential for a Rift Valley fever (RVF) outbreaks in sub-Saharan Africa. This system is potentially an important tool for local, national and international organisations involved in the prevention and control of animal and human disease, permitting focused and timely implementation of disease control strategies several months before an outbreak. We are currently developing a geographic information system (GIS)-based remotely sensed early warning system for potential RVF vectors in the United States. Forecasts of the potential emergence of mosquito vectors will be disseminated throughout the United States, providing several months' warning in advance of potentially elevated mosquito populations. This would allow timely, targeted implementation of mosquito control, animal quarantine and vaccine strategies to reduce or prevent animal and human disease.

Published

2007

136. Chronic thromboembolic pulmonary hypertension and pulmonary thromboendarterectomy.

Author

Manecke GR Jr, Wilson WC, Auger WR, and Jamieson SW

Subjects

Anesthesia, Chronic Disease, Humans, Operating Rooms organization & administration, Postoperative Care, Pulmonary Embolism complications, Pulmonary Embolism diagnosis, Thromboembolism diagnosis, Thromboembolism etiology, Treatment Outcome, Endarterectomy, Pulmonary Embolism surgery, Thromboembolism surgery

Abstract

Chronic thromboembolic pulmonary hypertension results from incomplete resolution of a pulmonary embolus or from recurrent pulmonary emboli. Its incidence is underappreciated, and it is currently an undertreated phenomenon. Pulmonary thromboendarterectomy is currently the safest and most effective treatment for this condition. The surgery involves midline sternotomy, profound hypothermic circulatory arrest, and complete endarterectomy of the pulmonary vascular tree. Success depends on effective coordination of multiple medical teams, including pulmonary medicine, anesthesiology, and surgery. This review, based on the past 30 years of experience at University of California San Diego Medical Center, includes information about the clinical history, diagnostic workup, anesthesia, surgical approach, and postoperative care. Outcome data are discussed, as are avenues for future research.

Published

2005

137. Vector competence of Culicoides sonorensis (Diptera: Ceratopogonidae) for vesicular stomatitis virus.

Author

Drolet BS, Campbell CL, Stuart MA, and Wilson WC

Subjects

Animals, Cells, Cultured, Ceratopogonidae anatomy & histology, Intestines virology, Microscopy, Electron, Time Factors, Vesicular stomatitis Indiana virus isolation & purification, Virus Replication, Ceratopogonidae virology, Insect Vectors virology, Vesicular stomatitis Indiana virus growth & development

Abstract

To determine the vector competence of Culicoides sonorensis Wirth & Jones midges for vesicular stomatitis virus (VSV)-New Jersey, insects were experimentally infected per os and sampled over time. Viral replication, as determined by in situ hybridization, was seen in epithelial, neural, and hemolymph cell types throughout the insect. Spatial and temporal distribution of virus was determined by immunohistochemical examination of sequentially sampled insects. Tissues of the alimentary canal were infected in a temporal pattern that paralleled the route of digestion/absorption: foregut and midgut by day 1, surrounding hemolymph and Malpighian tubules by day 3, and finally the midgut/ hindgut junction, hindgut, and rectal region by day 5. The circulation of virus in the hemolymph by day 3 coincided with infection of the dermis and fat bodies, the salivary glands, eyes, cerebral and subthoracic ganglia, and the ovaries. Oviduct epithelium and ovarial sheaths were infected by day 3, followed by infection of the developing oocytes by day 5. Interestingly, neural infections were seen in the subabdominal ganglia innervating the midgut in 33% of insects by 1 d postfeeding in the absence of positive staining in the hemolymph or surrounding tissues. A retrograde axonal transport infection route for these ganglia is discussed. The disseminated, productive, noncytolytic infection in Culicoides is consistent with that of an efficient biological vector for VSV. Virus readily replicated throughout the insect, passing both midgut and salivary gland infection barriers and reaching transmission-related organs in 3 d. Establishing the competence of this insect vector for VSV provides the foundation for animal transmission studies in the future. The possibility of horizontal, transovarial, and mechanical transmission is discussed.

Published

2005

138. Midgut and salivary gland transcriptomes of the arbovirus vector Culicoides sonorensis (Diptera: Ceratopogonidae).

Author

Campbell CL, Vandyke KA, Letchworth GJ, Drolet BS, Hanekamp T, and Wilson WC

Subjects

Amino Acid Sequence, Animals, Arboviruses, Base Sequence, Ceratopogonidae metabolism, Ceratopogonidae virology, DNA Primers, DNA, Complementary genetics, Expressed Sequence Tags, Female, Gene Expression, In Situ Hybridization, Insect Proteins genetics, Insect Vectors metabolism, Insect Vectors virology, Male, Molecular Sequence Data, Polymerase Chain Reaction methods, RNA, Messenger genetics, Sequence Alignment, Sequence Analysis, DNA, Sex Factors, Allergens genetics, Ceratopogonidae genetics, Gastrointestinal Tract metabolism, Insect Vectors genetics, Nerve Tissue Proteins genetics, RNA, Messenger metabolism, Salivary Glands metabolism

Abstract

Numerous Culicoides spp. are important vectors of livestock or human disease pathogens. Transcriptome information from midguts and salivary glands of adult female Culicoides sonorensis provides new insight into vector biology. Of 1719 expressed sequence tags (ESTs) from adult serum-fed female midguts harvested within 5 h of feeding, twenty-eight clusters of serine proteases were derived. Four clusters encode putative iron binding proteins (FER1, FERL, PXDL1, PXDL2), and two clusters encode metalloendopeptidases (MDP6C, MDP6D) that probably function in bloodmeal catabolism. In addition, a diverse variety of housekeeping cDNAs were identified. Selected midgut protease transcripts were analysed by quantitative real-time PCR (q-PCR): TRY1&#95;115 and MDP6C mRNAs were induced in adult female midguts upon feeding, whereas TRY1&#95;156 and CHYM1 were abundant in midguts both before and immediately after feeding. Of 708 salivary gland ESTs analysed, clusters representing two new classes of protein families were identified: a new class of D7 proteins and a new class of Kunitz-type protease inhibitors. Additional cDNAs representing putative immunomodulatory proteins were also identified: 5' nucleotidases, antigen 5-related proteins, a hyaluronidase, a platelet-activating factor acetylhydrolase, mucins and several immune response cDNAs. Analysis by q-PCR showed that all D7 and Kunitz domain transcripts tested were highly enriched in female heads compared with other tissues and were generally absent from males. The mRNAs of two additional protease inhibitors, TFPI1 and TFPI2, were detected in salivary glands of paraffin-embedded females by in situ hybridization.

Published

2005

139. Exposure to community violence and upper respiratory illness in older adolescents.

Author

Wilson WC, Rosenthal BS, and Austin S

Subjects

Adolescent, Adult, Cross-Sectional Studies, Female, Health Surveys, Humans, Incidence, Male, Minority Groups, Residence Characteristics, Respiratory Tract Infections epidemiology, Respiratory Tract Infections psychology, Stress, Psychological, Urban Population, Environmental Exposure, Respiratory Tract Infections etiology, Violence

Abstract

Purpose: To examine the relationship between exposure to chronic community violence and upper respiratory illness (URI) symptoms among urban adolescents of color; and to test the generality of a model of the relationship between social stress and URI., Method: The research used a cross-sectional correlational design. The sample was 769 first-semester first-year students in an urban nonresidential 4-year college from the academic years 1999-2002. Data were collected by a group-administered questionnaire in academic classes. The research used three multi-item additive scales (each with high reliability and validity): exposure to community violence, psychological distress, and URI symptoms. Multiple regression procedures were used to analyze the data., Results: Positive correlations were obtained between: exposure to community violence and reporting of URI (r = .19), exposure and psychological distress (r = .22), and psychological distress and URI (r = .51). The relationship between exposure to community violence and URI is greatly reduced when level of psychological distress is statistically controlled., Conclusions: Exposure to community violence is related to experiencing URI symptoms among older urban adolescents of color; the effect size of the relationship is small-medium. Psychological distress mediates the impact of exposure to community violence on URI. The findings expand the range of social stressors that are empirically related to URI, and populations in which a relationship between social stressors and URI may be found.

Published

2005

140. Studies on overwintering of bluetongue viruses in insects.

Author

White DM, Wilson WC, Blair CD, and Beaty BJ

Subjects

Animals, Bluetongue virus genetics, Cells, Cultured, Colorado, Genome, Viral, Larva virology, Phylogeny, RNA, Viral analysis, Reverse Transcriptase Polymerase Chain Reaction, Bluetongue virus isolation & purification, Ceratopogonidae virology, Ecosystem, Insect Vectors virology, Seasons

Abstract

Bluetongue viruses (BTVs) are economically important arboviruses that affect sheep and cattle. The overwintering mechanism of BTVs in temperate climates has eluded researchers for many years. Many arboviruses overwinter in their invertebrate vectors. To test the hypothesis that BTVs overwinter in their vertically infected insect vectors, Culicoides sonorensis larvae were collected from long-term study sites in northern Colorado, USA, and assayed for the presence of BTV RNA by nested RT-PCR. Sequences from BTV RNA segment 7 were detected in 30 % (17/56) of pools composed of larvae and pupae collected in 1998 and in 10 % (31/319) of pools composed of adults reared from larvae collected in 1996. BTV was not isolated from the insects. Additionally, Culicoides cell-culture lines derived from material collected at one of the sites, or derived from insect samples collected during a BTV outbreak, contained BTV RNA segment 7. In contrast, segment 2 RNA was detected at half the rate of segment 7 RNA in the field-collected larvae and was only detected in the Culicoides cell lines with one of two primer sets. These data suggest that BTVs could overwinter in the insect vector and that there is reduced expression of the outer capsid genes during persistent infection.

Published

2005

141. Field-deployable real-time polymerase chain reaction detection of bluetongue and epizootic haemorrhagic disease viral ribonucleic acid.

Author

Wilson WC, Stallknecht DE, and Mecham JO

Abstract

Nucleic acid sequence information from molecular evolution studies of bluetongue virus (BTV) and related epizootic haemorrhagic disease virus (EHDV) strains has resulted in a large database of genomic information. Published sequence data and sequence data from our laboratory were used to design real-time field-deployable reverse transcriptase-polymerase chain reaction assays for the detection of BTV or EHDV viral RNA. The assays used standard RNA extraction and TaqMan chemistries and the entire process was completed in

Published

2004

142. Preventing a fatal outcome Addison's disease.

Author

Wilson WC

Subjects

Addison Disease physiopathology, Fatal Outcome, Humans, Male, Middle Aged, Addison Disease diagnosis, Addison Disease therapy

Abstract

Low serum sodium levels combined with decreased extracellular volume are your key to recognizing this potentially lethal but very treatable disease.

Published

2004

143. Molecular investigations of orbivirus/vector interactions.

Author

Campbell CL, McNulty MJ, Letchworth GJ, and Wilson WC

Abstract

Defining predictors for insect-transmitted virus (arbovirus) disease cycles requires an understanding of the molecular interactions between the virus and vector insect. Studies of orbiviruses from numerous geographic regions have indicated that virus genes are affected by insect population differences. Therefore, the authors have initiated genetic studies of Culicoides sonorensis, isolating cDNAs for characterisation of differential insect gene expression, as well as a gene discovery project. Previous work identified insect transcripts elevated in orbivirus-infected female midguts at one day post infection (pI). Here, we report cDNAs that were more abundant in midguts two days following an epizootic haemorrhagic disease virus feeding, as well in head/salivary glands at three days pI. Of the cDNAs identified in midguts at two days pI, three encode translational machinery components, and three encode components that affect cellular structural features. Of the differentially expressed salivary gland cDNAs, only one was homologous to a previously identified gene, a putative odorant binding protein.

Published

2004

144. Culture-independent analysis of midgut microbiota in the arbovirus vector Culicoides sonorensis (Diptera: Ceratopogonidae).

Author

Campbell CL, Mummey DL, Schmidtmann ET, and Wilson WC

Subjects

Animals, Arbovirus Infections transmission, Base Sequence, Cloning, Molecular, Culicidae classification, Culicidae genetics, Culicidae virology, DNA genetics, DNA Primers, DNA, Ribosomal genetics, Digestive System virology, Female, Insect Vectors, RNA, Ribosomal, 16S genetics, Restriction Mapping, Culicidae microbiology, Digestive System microbiology

Abstract

Differences in midgut microbial communities inhabiting Culicoides spp., insect vectors of virus pathogens, may affect the variation observed in the ability of these biting midges to propagate arthropod-borne viruses. As a first step toward addressing this hypothesis, midgut bacterial communities were compared between Culicoides species expected to be efficient and inefficient vectors of virus pathogens. We used 16S rDNA sequence and restriction fragment information to provisionally identify 36 bacterial genera from guts of wild adult female biting midges, Culicoides sonorensis Wirth and Jones and Culicoides variipennis (Coquillet), from two geographical locations. Bacterial identification was made by sequence analysis of 16S rDNA fragments and by terminal restriction fragment length polymorphism analysis of polymerase chain reaction-amplified 16S rDNA fragments from adult guts. Of 36 bacterial genera identified, 12 had been previously identified in other insects: Comomonas, Enterobacter, Klebsiella, Acinetobacter, Pseudomonas, Stenotrophomonas, Staphylococcus, Chryseobacterium, Moraxella, Acholeplasma, Flavobacterium, and Rickettsia, Significant differences in bacterial community composition were found between all three groups of wild adult females analyzed: live-trapped C. sonorensis, laboratory-emerged C. sonorensis, and laboratory-emerged C. variipennis.

Published

2004

145. Deep hypothermic circulatory arrest and the femoral-to-radial arterial pressure gradient.

Author

Manecke GR Jr, Parimucha M, Stratmann G, Wilson WC, Roth DM, Auger WR, Kerr KM, Jamieson SW, Kapelanski DP, and Mitchell MM

Subjects

Age Factors, Cardiopulmonary Bypass, Endarterectomy methods, Female, Humans, Hypertension, Pulmonary surgery, Male, Middle Aged, Monitoring, Intraoperative methods, Postoperative Period, Retrospective Studies, Time Factors, Blood Pressure physiology, Femoral Artery physiopathology, Heart Arrest, Induced methods, Hypothermia, Induced methods, Radial Artery physiopathology

Abstract

Objectives: To determine the femoral-to-radial arterial pressure gradient, as well as the factors associated with them, in patients receiving cardiopulmonary bypass (CPB) with profound hypothermia and circulatory arrest., Design: Retrospective automated hemodynamic record review., Setting: University hospital., Participants: Patients undergoing pulmonary thromboendarterectomy with deep hypothermic circulatory arrest., Measurements and Main Results: The automated hemodynamic records of 54 consecutive patients undergoing pulmonary thromboendarterectomy with deep hypothermic circulatory arrest were reviewed, comparing the femoral and radial arterial pressures throughout the intraoperative period. In 20 of the patients, the hemodynamic data from the first 16 postoperative hours were also studied. Forty-one of 54 (76%) of the patients exhibited a mean arterial gradient of at least 10 mmHg either during or after CPB, femoral being higher. Clinically significant gradients were noted throughout the CPB period and the post-CPB period in these patients. In the 54 patients studied, the systolic blood pressure (SBP) gradient was 32 +/- 19 mmHg after CPB (95% confidence limits 28.2 mmHg, 39.0 mmHg), and the mean arterial pressure (MAP) gradient was 6.3 +/- 4.9 mmHg (95% confidence limits 5.5 mmHg, 8.6 mmHg). The duration of clinically significant SBP (>10 mmHg) and MAP (>5 mmHg) gradients in the postoperative period were 5.2 +/- 5.7 hours and 5.8 +/- 7.2 hours, respectively. Advanced age correlated with high post-CPB pressure gradients in this population and was associated with prolonged postoperative resolution of the gradients., Conclusions: The femoral-to-radial arterial pressure gradients, particularly systolic, after CPB, were greater and of longer duration in these patients undergoing deep hypothermic circulatory arrest than gradients previously reported for routine CPB. Central arterial pressure monitoring is recommended for patients undergoing deep hypothermic circulatory arrest, being valuable both for intraoperative and postoperative care.

Published

2004

146. Psychological effects of attack on the World Trade Center: analysis before and after.

Author

Wilson WC and Rosenthal BS

Subjects

Adolescent, Adult, Cross-Sectional Studies, Female, Humans, Male, Mental Disorders diagnosis, Mental Disorders psychology, New York City, Prospective Studies, Psychiatric Status Rating Scales, Research Design, Retrospective Studies, Stress Disorders, Post-Traumatic psychology, Stress, Psychological psychology, Students psychology, Surveys and Questionnaires, Disasters statistics & numerical data, Life Change Events, Stress Disorders, Post-Traumatic diagnosis, Stress, Psychological diagnosis, Terrorism psychology

Abstract

Four different studies using a total sample of 711 from the same New York City student population tested a model that has emerged from previous research on disasters. The model suggests that postdisaster psychological distress is a function of exposure to the disaster, predisaster psychological distress, acute distress following the disaster, time elapsed between disaster and observation of distress, and additional traumatic experiences since the disaster. Although findings replicate those of previous cross-sectional studies regarding association of exposure and distress after the disaster, before and after studies did not detect an effect on postdisaster psychological distress of the World Trade Center attack. Great caution must be used in attributing elevated psychological distress observed postdisaster to the effects of the disaster.

Published

2004

147. Antigen capture competitive enzyme-linked immunosorbent assays using baculovirus-expressed antigens for diagnosis of bluetongue virus and epizootic hemorrhagic disease virus.

Author

Mecham JO and Wilson WC

Subjects

Animals, Antibodies, Viral blood, Antigens, Viral analysis, Blotting, Western, Bluetongue virus isolation & purification, Cattle, Cloning, Molecular, Deer, Enzyme-Linked Immunosorbent Assay methods, Recombinant Proteins analysis, Sheep, Spodoptera, Time Factors, Antigens, Viral genetics, Bluetongue diagnosis, Hemorrhagic Disease Virus, Epizootic isolation & purification, Reoviridae Infections diagnosis

Abstract

Bluetongue virus (BTV) and epizootic hemorrhagic disease virus (EHDV) are orbiviruses that infect both livestock and wild ruminants. Antigenic cross-reactivity between BTV and EHDV often results in serologic misdiagnosis. Competitive enzyme-linked immunosorbent assays (c-ELISAs) show increased sensitivity and specificity for the identification of these viral diseases; however, the preparation of cell culture-derived viral antigen for these tests is laborious and variable from batch to batch, and the resulting antigen may be infectious. To overcome these problems, the genes coding for a structural protein, VP7, of BTV and EHDV were cloned into baculovirus and the recombinant proteins were expressed in Sf9 cultured insect cells. Recombinant viral proteins released into the baculovirus-infected Sf9 cell culture supernatant were used in antigen capture c-ELISAs (Ag Cap c-ELISA) tests that specifically detected antibody in the serum of cattle experimentally infected with BTV and EHDV. The diagnostic utility of the Ag Cap c-ELISA was demonstrated by comparison with a commercial c-ELISA. The Ag Cap c-ELISA offers the advantages of using an easily produced, easily standardized, noninfectious antigen that does not require further purification or concentration.

Published

2004

148. Grasshoppers (Orthoptera: Acrididae) could serve as reservoirs and vectors of vesicular stomatitis virus.

Author

Nunamaker RA, Lockwood JA, Stith CE, Campbell CL, Schell SP, Drolet BS, Wilson WC, White DM, and Letchworth GJ

Subjects

Animals, Cattle, Grasshoppers growth & development, Humans, Life Cycle Stages, Disease Reservoirs, Grasshoppers virology, Insect Vectors virology, Rhabdoviridae Infections transmission, Stomatitis virology, Vesicular stomatitis Indiana virus growth & development, Vesicular stomatitis Indiana virus isolation & purification

Abstract

Vesicular stomatitis (VS) is an economically devastating disease of livestock in the Americas. Despite strong circumstantial evidence for the role of arthropods in epizootics, no hematophagous vector explains the field evidence. Based on the spatiotemporal association of grasshopper outbreaks and VS epizootics, we investigated the potential role of these insects as vectors and reservoirs of the disease. The critical steps in the grasshopper-bovine transmission cycle were demonstrated, including 1) 62% of grasshoppers [Melanoplus sanguinipes (F.)] fed vesicular stomatitis virus (VSV) from cell culture became infected, with titers reaching 40,000 times the inoculative dose; 2) 40% of grasshoppers that cannibalized VSV-infected grasshopper cadavers became infected, amplifying virus up to 1,000-fold; 3) one of three cattle consuming VSV-infected grasshopper cadavers contracted typical VS and shed virus in saliva; and 4) 15% of grasshoppers became infected when fed saliva from this infected cow. The ecological conditions and biological processes necessary for these transmissions to occur are present throughout much of the Americas. Field studies will be required to show these findings are relevant to the natural epidemiology of VSV.

Published

2003

149. The S7 gene and VP7 protein are highly conserved among temporally and geographically distinct American isolates of epizootic hemorrhagic disease virus.

Author

Mecham JO, Stallknecht D, and Wilson WC

Subjects

Capsid Proteins genetics, Conserved Sequence, Hemorrhagic Disease Virus, Epizootic classification, Sequence Homology, Amino Acid, Sequence Homology, Nucleic Acid, United States, Viral Proteins chemistry, Capsid Proteins chemistry, Genes, Viral, Hemorrhagic Disease Virus, Epizootic genetics, Hemorrhagic Disease Virus, Epizootic isolation & purification, Phylogeny, Viral Structural Proteins genetics

Abstract

Complete sequences of genome segment 7 (S7) from six isolates of epizootic hemorrhagic disease virus serotype 1 (EHDV-1) and 37 isolates of serotype 2 (EHDV-2) were determined. These isolates were made between 1978 and 2001 from the southeast, mid-Atlantic, Midwest and intermountain United States. Analysis of the S7 sequence similarities showed 98.1% identity among the EHDV-1 isolates and 91.0% identity among the EHDV-2 isolates. Comparison of the deduced amino acid similarities showed an even greater degree of similarity among the isolates (100% among the EHDV-1 isolates and 98.9% identity among the EHDV-2 isolates). There was only 75.8% identity between the EHDV-1 and EHDV-2 isolates at the nucleic acid level; however, there was 93.7% identity between the two groups at the amino acid level. The ratio of non-synonymous to synonymous nucleotide indicates a strong selection for silent substitutions. There was no evidence for reassortment between EHDV-1 and EHDV-2 isolates. The high degree of conservation of S7 gene codons and the VP7 protein, suggests that little variation is allowed in preserving the function of this protein. The high degree of conservation also validates the use of diagnostic tests for EHDV based on S7 and VP7.

Published

2003

150. Replication of bluetongue virus and epizootic hemorrhagic disease virus in pulmonary artery endothelial cells obtained from cattle, sheep, and deer.

Author

McLaughlin BE, DeMaula CD, Wilson WC, Boyce WM, and MacLachlan NJ

Subjects

Animals, Endothelium, Vascular cytology, Pulmonary Artery cytology, Species Specificity, Bluetongue virus physiology, Cattle virology, Deer virology, Endothelium, Vascular virology, Hemorrhagic Disease Virus, Epizootic physiology, Sheep, Domestic virology, Virus Replication

Abstract

Objective: To compare replication of bluetongue virus (BTV) and epizootic hemorrhagic disease virus (EHDV) in pulmonary artery endothelial cells (ECs) obtained from juvenile cattle, sheep, white-tailed deer (WTD; Odocoileus virginianus), and black-tailed deer (BTD; O hemionus columbianus)., Sample Population: Cultures of pulmonary artery ECs obtained from 3 cattle, 3 sheep, 3 WTD, and 1 BTD., Procedure: Purified cultures of pulmonary artery ECs were established. Replication, incidence of infection, and cytopathic effects of prototype strains of BTV serotype 17 (BTV-17) and 2 serotypes of EHDV (EHDV-1), and (EHDV-2) were compared in replicate cultures of ECs from each of the 4 ruminant species by use of virus titration and flow cytometric analysis., Results: All 3 viruses replicated in ECs from the 4 ruminant species; however, BTV-17 replicated more rapidly than did either serotype of EHDV. Each virus replicated to a high titer in all ECs, although titers of EHDV-1 were significantly lower in sheep ECs than in ECs of other species. Furthermore, all viruses caused extensive cytopathic effects and a high incidence of cellular infection; however, incidence of cellular infection and cytopathic effects were significantly lower in EHDV-1-infected sheep ECs and EHDV-2-infected BTD ECs., Conclusions and Clinical Relevance: There were only minor differences in replication, incidence of infection, and cytopathic effects for BTV-17, EHDV-1, or EHDV-2 in ECs of cattle, sheep, BTD, and WTD. It is not likely that differences in expression of disease in BTV- and EHDV-infected ruminants are attributable only to species-specific differences in the susceptibility of ECs to infection with the 2 orbiviruses.

Published

2003