Assessment of U.S. Agriculture Sector and Human Vulnerability to a Rift Valley Fever Outbreak

Hughes, Randi Catherine

2011 May 1900

Foreign animal disease outbreaks can cause substantial economic losses. Policy makers need information on both the vulnerability of the food supply to disease epidemics and the impacts of alternative protection actions. This research focused on the assessment of the U.S. agricultural sector and human vulnerability to a Rift Valley Fever (RVF) outbreak and the value of a select set of alternative disease control strategies. RVF is a vector-borne, zoonotic disease that affects both livestock and humans; thus both animal and human consequences of an outbreak were examined. This research was conducted in two parts. Livestock impact assessment used an integrated epidemic/economic model to examine the extent of RVF spread in the animal population and its consequences plus the outcome of implementing two different control strategies: emergency vaccination and larvicide vector control. The number of infected, aborted, and dead animals is best controlled by coupling vaccination along with larvicide, but results in the second highest median national welfare loss. Therefore, careful decisions must be made as to what actions should be taken. Total national producer welfare is reduced with each scenario, and is more severe than the total national welfare loss (producer, consumer, and processor together). Consumer welfare is increased with each scenario due to a drop in prices of some commodities, and in some instances, an increase in supply as well. The majority of the national welfare loss can be attributed to the producers' and processors' loss in welfare. The highest damages are seen in the regions of the outbreak such as the South Central (SC). Other regions such as the Corn Belt, Lake States, and South East regions also see high damages due to price changes. The outbreak did not have substantial price effect on dairy products, but did have noticeable price changes for live cattle such as heifer calves, stocked yearling, and dairy calves. Prices for substitutes such as pork, chicken, and turkey experienced a price reduction, which can also be a factor resulting in consumer welfare gains. Human impact assessment utilized an inferential procedure for estimating the human consequences which comprise of a cost of illness calculation to assess the dollar cost of human illnesses and deaths, as well as a Disability Adjusted Life Year calculation to give an estimate of the burden of disease on public health as a whole. With potential costs above $2 billion for human illness, and with this number not accounting for loss or damages to other sectors of the economy, it can be highly probable that investing in a human vaccination campaign can be cost-effective and possibly cost-reducing. This cost along with the economic loss of the agriculture sector suggests substantial potential losses to the U.S. if this hypothetical situation were to become reality. Combining total loss estimates from the cost of illness and ASM models, potential damage of a RVF outbreak could range from 121 million to 2.3 billion US 2010$. The results of this study show the economic damages of an outbreak in the livestock population being much greater relative to the outbreak in the human population (roughly 16 times greater). It should be pointed out that both cost estimates are most likely under estimated. The animal outbreak is not incorporating all susceptible livestock (e.g. hogs and goats), and the human illness is not incorporating other damages to society (e.g. damages due to loss of tourism). By providing estimates on the potential economic outcomes, policy makers can better choose where, when, and how to invest their resources.

RVF

Rift Valley Fever

OIE

World Organization for Animal Health

FAO

Food and Agriculture Organization

WNV

West Nile Virus

A comparison study of gravid and under house CO2 mosquito traps in Harris County, Texas

White, Stephanie Lyn

10 October 2008

Harris County Mosquito Control Division (HCMCD) is responsible for surveillance of mosquito species that are vectors of St. Louis Encephalitis (SLE) virus and West Nile Virus (WNV) within Harris County, Texas, including the Houston metroplex. The metroplex area has some unique attributes and a vast variety of environmental habitats that are attractive to vectors of arboviruses and for the transmission of arboviruses to the human population. Data describing the efficacy of Gravid (GV) and Underhouse (UH) CO2 traps were analyzed to determine if there is a significant difference between these two trap types with respect to the number of mosquitoes and the variety of mosquito species caught. This study was conducted during the off-peak HCMCD trapping season, to gain information in preparation for a yearround trapping program utilizing Underhouse CO2 traps for WNV and SLE virus surveillance. Adjusting for the week of collection, results suggest that Gravid traps caught significantly (P = 0.009) more mosquitoes (mean = 23.134 per trap) in the study area than Underhouse traps (mean = 3.616 per trap), and that Underhouse Traps caught a larger variety of mosquito species (n = 13) than Gravid Traps (n = 11), out of 15 total different species caught. Gravid and Underhouse traps caught 9 out of 15 of the same mosquito species during the study period. Culex quinquefasciatus mosquito catches in Gravid traps and temperature were strongly correlated (Spearman's Correlation Coefficient = 0.707, P = 0.005). Geographic Information System spatial analysis indicated clustering of Culex quinquefasciatus mosquito catches in both Gravid traps, week 9 and 21 (Moran's I = 0.69, P = 0.040 and 0.74, P = 0.021, respectfully ) and Underhouse traps, week 13 and 19 (Moran's I = 0.92, P = 0.002, and 0.89, P = 0.011, respectfully). It is recommended that Harris County Mosquito Control Division continue to utilize gravid traps as a primary method of surveillance. Gravid traps (16,194) caught 85% more mosquitoes than Underhouse traps (2,531) over the fourteen week study period. Their overall success far outweighs the additional materials or labor required for their use in a successful surveillance program.

Zoonotic Disease

Vector Borne

Mosquito Traps

Mosquito

Harris County

Gravid Traps

Houston

Mosquito Control

Texas

Underhouse Traps

West Nile Virus

Cytotoxic T lymphocyte Responses Against Japanese Encephalitis Virus In Mice: Specificity And Immunotherapeutic Value

Krishna, Kaja Murali

10 1900

Cytotoxic T Lymphocytes (CTL) are known to play an important role in clearing infectious virus from infected hosts in a variety of viral infections. Depending on the type of virus and mode of virus entry both class I and class II restricted CTL can contribute to protection from virus-induced disease. Although CD8 positive CTL are associated with virus elimination and control in many viral infections, elimination of neurotropic viruses from the Central Nervous system (CNS) is more complex due to the lowered expression of MHC antigens on neuronal cells. This failure to constitutively express high levels of MHC antigens by neurons could serve as an advantage to avoid damage to this differentiated and non-renewable tissue. However, abnormal induction of MHC antigens in the CNS mediated by CD4 positive lymphocytes or by astrocytes have also been shown to cause destructive inflammation in the CNS. The present study deals with CTL responses against one such neurotropic virus called Japanese Encephalitis Virus (JEV). JEV is a positive-stranded RNA virus that belongs to the flavivirus group, a group that is among the most important agents causing human encephalitis worldwide. Although passive transfer of monoclonal antibodies against this virus has been shown to confer protection of mice from lethal challenge with virus, neither the presence of CTL against this virus nor its role in conferring protection has been reported so far. Understanding the CTL responses against these viruses acquired importance in light of recent reports that neurovirulence of JEV and yellow fever viruses can be enhanced by the administration of virus specific antibodies. Hence this study was undertaken to examine the possibility of raising CTL specific to JEV. The specificity of the CTL raised, their therapeutic value and the ability of different lymphocyte subsets to mediate protection in vivo are dealt with in this study. Generation of CTL against JEV The generation of CTL against JEV in BALB/c mice, requires MHC defined cell lines that not only support virus infection but are also histocompatible. Several cell lines were initially examined for their ability to support JEV infection as a prc-rcquisitc before their utilization in in vivo and in vitro stimulation protocols aimed at generating JEV-specific CTL. Virus infection was monitored by immunofluorescence using JEV envelope-specific monoclonal antibodies as well as by titration of virus produced from infected cells by plaque assays. These different cell lines that were characterised for their ability to support JEV infection were then utilised to generate and monitor antiviral CTL. Several in vivo immunisation protocols were examined initially find out which of these infected cells prime BALB/c mice efficiently for generation of virus-specific CTL upon secondary stimulation in vitro with infected syngeneic cells. Immunisation of mice with infected cells per se was preferred over free virus since this was thought to facilitate priming against some viral non-structural proteins preferentially found on infected cells in addition to other viral structural proteins. It was observed that not only infected syngeneic and allogeneic cells but also infected xenogeneic cells prime BALB/c mice for the generation of JEV- specific CTL upon secondary restimulation in vitro. An optimal protocol was standardised for the generation of CTL against JEV. This included primary in vivo immunisation of mice followed by secondary in vitro restimulation of splenocytes with infected syngeneic cells. Either immunisation alone or in vitro stimulation of naive splenocytes alone was unsuccessful. The effector cells generated specifically lysed JEV-infccted P388D1 targets but not uninfected P388D1 or YAC-1 targets suggesting that the lysis on infected targets is not mediated by Natural Killer activity. Specificity and MHC restriction of anti JEV Effectors Cell depletion studies using complement mediated lysis were performed to examine the phenotype of the cells mediating virus specific lysis of infected targets. Depletion of Lyt 2.2+ or Thy 1+ but not L3T4+ sub-populations of effector cells inhibited lysis of infected targets showing that the effectors mediating virus-specific lysis were Lyt-2+ T cells. Examination of target specificities and MHC restriction of the antiviral CTL generated showed that although infected xenogeneic cells were used for immunisation, the effector cells recognised only infected syngeneic (P388D1, Sp2/0) and semisyngeneic (Neuro 2a, YAC-1) cells. Virus-specific recognition was found to be class I Kd and class I Dd restricted. These effector cells were also found to recognise cells infected with a closely related flavivirus, West Nile Virus (WNV) suggesting that they were crossreactive to some degree. Based on the consensus motif that has been established for H-2Kd associated peptides, several nonamers were predicted as possible CTL epitopes by scanning the deduced amino acid sequences of three strains of JEV and WNV. Among several predicted nonamers, three peptides were examined for their ability to reconstitute lysis of uninfected targets by polyclonal anti JEV CTL populations. Results demonstrate that peptides derived from NS1 and NS3 but not NS5 protein of JEV were able to partially reconstitute lysis of uninfected targets by effectors when pulsed with the appropriate peptide. Protective ability of the CTL raised against JEV To examine whether anti-JEV effectors raised in vitro could confer protection from intracerebral challenge with JEV, these effectors were adoptively transferred into adult BALB/c mice intracerebrally along with 10 x LDJ0 dose of JEV. More than 55% of these animals were protected from death and survived beyond 100 days after JEV challenge demonstrating that adoptively transferred anti-JEV effectors could indeed confer protection from lethal challenge with JEV. However, adoptive transfer of effectors by either intravenous or intraperitoneal routes did not protect adult mice from the lethal effects of intracerebral challenge with JEV. In contrast to adult mice, newborn mice were not protected from death by the adoptively transferred effector cells. This was also supported by experiments where a correlation was observed with the increasing age of mice and the success of protection conferred by the adoptively transferred effector cells. To establish the identity of cell subsets responsible for protection, Lyt 2, L3T4 or Thy 1 positive cells were specifically depleted from the polyclonal CTL by multiple cycles of complement mediated lysis and the remaining cells were adoptively transferred intracerebrally along with 10 x LD of JEV. These results demonstrate that both Lyt 2 and L3T4 positive T cells present in the effector population were necessary to confer protection of adult mice. Examination of virus-specific neutralising antibodies in the sera of protected and unprotected mice revealed that presence of L3T4 positive cells in the adoptively transferred population increases virus-specific neutralising antibodies. However presence of neutralising antibodies alone was not sufficient to confer protection. The protection required both Lyt-2 and L3T4 positive cells together. These studies could in the long term throw some light on similar observations about age dependant susceptibility to JEV in humans.

Medicine

Immunotherapy - Mice

Japanese Encephalitis Virus (JEV)

Cytotoxic T Lymphocytes (CTL)

Enciphilitis Virus

West Nile Virus (WNV)

Designed to deceive : President Hosni Mubarak's Toshka project

Deputy, Emmarie

26 July 2011

Since the dawn of industrialization, many authoritarian regimes have taken on massive public works projects which seem impressive or farfetched. Few onlookers are surprised when these projects are not completed or are completed at such a high cost that they appear to be an exercise in futility. Usually these failures are written off as dictatorial incompetence and overambition, but the initial motivations for beginning them are rarely addressed. This paper will argue that, rather than being a symptom of precipitant development or front for embezzlement, many of these projects were designed to fail because the regime received the largest benefit by starting them—not by completing them. Empirically this research will focus on the Toshka ‘New River Valley’ project in Egypt, which is Egypt’s largest development project and is designed to create a second Nile River Valley in the South and eventually be home to 20% of the Egypt’s population. In this report I explore the governments’ motivations, their intentions, the resulting symbolism and the repercussions of the Toshka project. / text

Mubārak, Muḥammad Ḥusnī, 1928-

Mubarak, Hosni

Toshka New River Valley project

Megaprojects

Politics and government

Egypt

Nile River

Land development

Genetic approaches to the analysis of body colouration in Nile tilapia (Oreochromis niloticus)

Rajaee, Amy H.

January 2011

Body colouration in tilapia is an important trait affecting consumer preference. In the Nile tilapia (Oreochromis niloticus), there are three colour variants which are normal (wild type), red and blond. In some countries, the red variant is important and reaches higher prices in the market. However, one major problem regarding red tilapia culture is their body colouration which is often associated with blotching (mainly black but also red) which is undesirable for the consumer. The overall aim of this work was to expand knowledge on various aspects of body colouration in Nile tilapia using genetic approaches. The results of this research are presented as four different manuscripts. The manuscripts (here referred as Papers) have either been published (Paper IV) or are to be submitted (Paper I, II and III) in relevant peer reviewed journals. Paper I and II investigated the inheritance of black blotching and other body colour components of the red body colour. Specifically, Paper I consisted of two preliminary trials (Trial 1 and 2), to look at the ontogeny of black blotching and body colour components over a period of six months. Trial 1 investigated the effect of tank background colour (light vs dark) on black blotching and other body colour components and was carried out using a fully inbred (all female) clonal red line. Trial 2 was carried out using mixed sex fish and was aimed to investigate the association of black blotching with the sex of the fish. The results from this study were used to guide the experiment described in Paper II. Sixteen red sires with various levels of black and red blotching were crossed to clonal females and the inheritance of blotching and other body colour components were investigated using parent-offspring regressions. The results showed no significant heritability for black blotching and body redness, but a significant correlation for body redness and black blotching was found in female offspring at one sampling point suggesting that attempts to increase body redness may increase black blotching, as had been hypothesized. Paper III was divided into two parts. The first objective was to map the blond locus onto the tilapia linkage map and the second was to investigate the interaction of the blond and red genes on black blotching using the blond-linked markers to distinguish different blond genotypes in heterozygous red fish (i.e. RrBlbl or Rrblbl). In the blond fish, the formation of melanin is almost blocked via much reduced melanophores and this feature may be able to help reducing the black blotching in red tilapia. Two intraspecific families (O. niloticus) and one interspecific family (O. aureus and O. niloticus) were used as mapping families and the blond locus was located in LG5. Four out of eight markers were successfully used to assess the interaction of blond on red blotched fish. The blond gene did not significantly reduce the area of blotching but did reduce the saturation (paler blotching) and enhanced the redness of body colour in the Rrblbl fish compared to the RrBlbl group. Finally, Paper IV aimed to find out the effect of male colouration on reproductive success in Nile tilapia. A choice of one wild type male and one red male was presented to red or wild type females and these fish were allowed to spawn under semi-natural spawning conditions. Eggs were collected from the female’s mouth after spawning and paternity was assessed using microsatellite genotyping and phenotype scoring. No significant departures from equal mating success were observed between the red and wild type males, however there was a significant difference between the red and wild type females in the frequency of secondary paternal contribution to egg batches. The results suggest that mating success of wild type and red tilapia is approximately equal. The results from this research help to broaden our knowledge and understanding on the aspects of body colouration in Nile tilapia and provide fundamental information for further research.

597

Eine Studie zum Vorkommen des West-Nil-Virus in der Wildvogelpopulation Deutschlands

Prell, Juliane

14 November 2013

In den letzten Jahren erreichten viele neue (emerging) Viren Europa, die zum Teil (z.T.) zoonotisch auf den Menschen übertragbar sind. So musste man sich mit Geflügel- und Schweinegrippe, Blauzungenkrankheit, Infektiöser Anämie der Einhufer oder auch SARS (severe acute respiratory syndrome) auseinandersetzen. Bedingt durch verschiedene Faktoren, wie Klimawandel oder zunehmende Globalisierung und damit einhergehendem Verkehr zwischen den Kontinenten verbesserten sich auch die Bedingungen für die Virusverbreitung, so dass viele für Deutschland untypische Krankheitserreger auch hier auftraten. Das West-Nil-Virus (WNV) ist in Europa bereits endemisch verbreitet und könnte somit eine besondere Gefahr für Deutschland darstellen. Es ist ein bekannter Zoonose-Erreger, und sein Eintrag und die rasche Verbreitung des Virus in Amerika 1999 zeigten wie gefährlich neue Viren in naiven Populationen sein können. Über die Verbreitung des Virus in Deutschland gibt es nur wenige Studien z.B. des Robert-Koch-Instituts (LINKE et al. 2007a) und des Friedrich-Loeffler-Instituts (SEIDOWSKI et al. 2010), wobei in keiner Studie tote Vögel als Untersuchungsmaterial genutzt wurden. Da das WNV in Amerika mit einem auffälligen Vogelsterben einherging, ist es naheliegend, den Virusnachweis zuerst bei toten Vögeln zu erbringen.

West-Nil-Virus

real-time RT-PCR

Epidemiologie

West Nile virus

real time RT-PCR

epidemiology

ddc:636.089

Circulation du virus West-Nile dans les populations équines d'Iran : impact épidémiologique de l'environnement et du climat

Ahmadnejad, Farzaneh

25 January 2012

L'épidémie de West-Nile en Amérique du Nord en 2002, qui a touché plus de quarante états aux Etats-Unis, a conduit les Agences de santé à s'interroger sur le risque d'émergence, à l'extérieur de la zone intertropicale, de zoonoses vectorielles. Cette épidémie associée au changement climatique, a bien mis en évidence le rôle central de l'avifaune migratrice dans la diffusion du virus. La biologie des oiseaux, tout particulièrement le phénomène migratoire, permet un transport des virus sur de longues distances et entre espèces très diversifiées. Le Moyen-Orient, qui est situé au carrefour de différents continents, est extrêmement propice à la propagation des virus émergents dans les pays du Nord. La circulation du virus West Nile a été rapportée dans différents pays de la région, tels que l'Egypte, Israël, Liban, Irak, Emirats Arabes Unis et Iran. Saidi et al. (1970) ont montré la présence d'anticorps anti-virus du Nil occidental au sein de la population de la côte caspienne (Nord de l'Iran), des provinces du Khorassan (Nord-Est) et du Khuzestan (Sud-Ouest). Notre étude, conduite dans le cadre d'un programme associant TIMC-IMAG UMR 5525 UJF CNRS VetAgroSup, le Réseau International des Instituts Pasteurs et le Centre National d'Etudes Spatiales, vise: (i) à caractériser la circulation du virus de West-Nile au sein des populations équines d'Iran ; et (ii) et à modéliser l'impact sanitaire de l'environnement et du climat sur la transmission. Les résultats acquis permettent d'apprécier le risque associé à la dissémination spatio-temporelle du virus par les oiseaux migrateurs. Une attention toute particulière est portée à l'étude des déterminants environnementaux et climatiques susceptibles d'accroitre le potentiel de transmission du virus.

Incidence spatiale

Émergence

Serologie

Arbovirus

Diagnostic

West-Nile

Oiseaux sauvages et virus West Nile : étude éco-épidémiologique en Camargue

Jourdain, Elsa

14 December 2006

Le travail présenté ici s'intéresse au rôle des oiseaux sauvages dans l'épidémiologie du virus West Nile (WN) en Camargue. Des espèces d'oiseaux susceptibles d'intervenir dans les différentes phases de circulation du virus (introduction, amplification, dispersion, émergence) sont identifiées en s'appuyant sur les données bibliographiques relatives à la maladie et sur des critères ornithologiques. Les investigations épidémiologiques effectuées pour quelques unes de ces espèces en 2004 (année épizootique) et en 2005 (année post-épizootique) montrent que le virus WN circule dans la population d'oiseaux de Camargue. Pour les oiseaux migrateurs arrivant d'Afrique au printemps, les dates et lieux de ces contacts restent inconnus. Concernant les oiseaux sédentaires, deux isolats d'une même souche virale ont été obtenus en 2004, réciproquement à partir du cerveau d'une Pie bavarde Pica pica et d'un Moineau domestique Passer domesticus, et totalement séquencés. L'étude phylogénétique de cette souche montre qu'elle appartient au même cluster que celles précédemment isolées en Europe méditerranéenne. Les résultats sérologiques et virologiques chez ces deux espèces d'oiseaux, souvent observées à proximité des écuries, en font des candidates à l'amplification et l'émergence du virus WN chez les chevaux de Camargue. La mise en évidence, en 2005, d'ARN viral dans les fientes d'une Pie bavarde conforte cette hypothèse. Les recherches doivent se poursuivre pour évaluer la part respective des différents oiseaux de Camargue dans la circulation du virus WN en utilisant d'autres approches, comme par exemple l'analyse des repas de sang des moustiques vecteurs, récemment identifiés.

virus West Nile

épidémiologie

écologie

oiseaux sauvages

Camargue

Expression diagnostisch verwendbarer Antigene zum Nachweis West-Nil-Virus-spezifischer Antikörper

Delker, Anna Maria

26 March 2014

Grundlage der vorliegenden Arbeit ist die Überlegung, dass eine Möglichkeit, die Spezifität der bisher angewendeten Verfahren zur West-Nil-Virus-Diagnostik zu verbessern, in der Anwendung rekombinanter WNV-spezifischer Antigene besteht. Die unter anderem auf bioinformatischen Methoden basierende Identifikation von potenziellen B-Zell-Epitopen und Auswahl entsprechender Sequenzabschnitte richtete sich dabei gezielt auf immunogene Bereiche, die innerhalb der Gruppe der Flaviviren einen ausreichenden Sequenzunterschied zu allen weiteren sequenzverwandten Erregern, zusammengefasst im Japanische Enzephalitis-Serokomplex, boten. Drei ausgewählte Bereiche innerhalb der Strukturproteinsequenz, bezeichnet als prM, Cnat und Cme, sollten mit Hilfe des Expressionssystems Pichia pastoris bzw. Escherichia coli rekombinant exprimiert werden. Nach Erarbeitung optimaler Expressionsbedingungen folgte die affinitätschromatografische Reinigung der im weiteren Verlauf zur Immunisierung von Balb/c-Mäusen eingesetzten Polypeptide. Die gewonnenen Seren der nach verschiedenen Immunisierungsprotokollen geimpften Mäuse wurden im Anschluss immunologisch untersucht. Es zeigte sich, dass die rekombinanten Derivate des Capsid-Proteins eine deutliche Serokonversion hervorriefen. Analysen der mit Cnat und MBP-Cme immunisierten Mausseren wiesen vorhandene peptidspezifische sowie virusspezifische Antikörper nach. Der Einsatz dieser gewonnenen Peptidantigene im indirekten ELISA-Testsystem zur Detektion WNV-spezifischer Antikörper unter Verwendung humaner WNV-IgG-positiver Serumproben zeigte positive Resultate. Im Gegensatz hierzu führte die Immunisierung mit prM lediglich zu einer unspezifischen murinen Antikörperbildung. Die Unterscheidung zwischen WNV-positiven und WNV negativen Humanseren war unter Verwendung des rekombinanten Antigens prM nicht möglich. Im Ergebnis zeigten zwei der drei in dieser Arbeit rekombinant erstellten Strukturproteinabschnitte ihr immunologisches Potenzial in der Generierung muriner WNV spezifischer Antikörper. Zudem konnte mit der Expression der WNV-spezifischen C Protein Antigene ein Beitrag zur Etablierung eines indirekten ELISA-Testsystems zur Detektion WNV-bedingter Humaninfektionen geleistet werden.

West-Nil-Virus

humane Flavivirusinfektionen

rekombinante Proteinexpression

Pichia pastoris

E. coli

rekombinante Antigene

West-Nile-Virus

ddc:610

A GIS model for predicting potential "high risk" areas of West Nile virus by identifying ideal mosquito breeding habitats

Wallis, Robert Charles,

January 2005

Thesis (M.S.) -- Mississippi State University. Department of Geosciences. / Title from title screen. Includes bibliographical references.