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  • The Global ETD Search service is a free service for researchers to find electronic theses and dissertations. This service is provided by the Networked Digital Library of Theses and Dissertations.
    Our metadata is collected from universities around the world. If you manage a university/consortium/country archive and want to be added, details can be found on the NDLTD website.

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1

Tailored influenza virus vaccines for both the young and old: Vaccine Efficacy of Whole Inactivated Vaccines bearing Immunomodulatory Adjuvants or Multimeric peptides

Khan, Tila 25 July 2012 (has links)
Influenza epidemics and pandemics remain a significant burden to world health and economy. Low efficacy of current inactivated influenza vaccines in the elderly and immunocompromized and the inability to protect against antigenically drifted or shifted strains of influenza virus are the two major problems in influenza vaccine research. To overcome these hurdles, we have utilized an in vitro cell culture vaccine platform, which results in whole inactivated influenza vaccine (WIV) bearing bioactive membrane-anchored immunomodulatory proteins such as cytokines on the virion surface, collectively known as CYT-IVACs (Cytokine bearing-Inactivated Vaccine). In addition, we tested whether a multimeric M2e peptide presented on WIV can serve to enhance immunogenicity and augment protective efficacy of whole virus vaccines. Our panel of cytokines includes IL-2, IL-4, IL-12, IL-23, and Flt3L as well as the multimeric M2e peptide, all fused to the membrane anchoring regions of influenza virus hemagglutinin protein and constitutively expressed in virus permissive MDCK cell line. Subsequent infection with influenza virus results in incorporation of fusion constructs directly into budding progeny virions that are harvested, purified and inactivated to generate distinct CYT-IVAC formulations. Following validation of immunomodulator incorporation, vaccines were tested for in vivo efficacy in either "young adult" or "aged" female Balb/c mice. Our results demonstrate that our CYT-IVAC~IL-12/HA and CYT-IVAC~IL-23/HA serve as potent mucosal adjuvants in young adult mice elicited significantly high levels of mucosal IgA antibodies and afford superior protection against lethal virus challenge. Our Flt3L/HA formulation was the most effective stimulator of systemic anti-viral antibody levels. In "aged" mice a single dose formulation of IL-12 bearing CYTIVAC was superior at affording protection against lethal homotypic virus challenge. Finally, administration of multimeric M2e molecule co-presented on WIV elicited prolonged antibody responses in "young adult mice" and provided cross-protection from challenge with the heterologous influenza A pandemic strain 2009 H1N1. In conclusion, the CYT-IVAC approach represents a novel tailored advancement to current WIV approaches that has the potential to elicit both potent mucosal and systemic immune responses in young and old. / Ph. D.
vaccine
M2e
cytokine
virus
influenza
whole inactivated vaccine
2

Ability of ELISAs to detect antibodies against porcine respiratory and reproductive syndrome virus in serum of pigs after inactivated vaccination and subsequent challenge

Sattler, Tatjana, Pikalo, Jutta, Wodak, Eveline, Schmoll, Friedrich 14 December 2016 (has links) (PDF)
Background: In this study, six enzyme-linked immunosorbent assays (ELISA), intended for routine porcine reproductive and respiratory syndrome virus (PRRSV) herd monitoring, are tested for their ability to detect PRRSV specific antibodies in the serum of pigs after vaccination with an inactivated PRRSV type 1 vaccine and subsequent infection with a highly pathogenic (HP) PRRSV field strain. For this reason, ten piglets (group V) from a PRRSV negative herd were vaccinated twice at the age of 2 and 4 weeks with an inactivated PRRSV vaccine. Ten additional piglets (group N) from the sameherd remained unvaccinated. Three weeks after second vaccination, each of the piglets received an intradermal application of an HP PRRSV field strain. Serum samples were taken before first vaccination as well as before and 3, 7, 10 and 14 days after HP PRRSV application. All serum samples were tested for PRRSV RNA by reverse transcriptase quantitative polymerase chain reaction (RT-qPCR) as well as for PRRSV antibodies with all six study ELISAs. Results: At the beginning of the study (before vaccination), all of the piglets were PRRSV antibody negative with all study ELISAs. They also tested negative for PRRSV RNA measured by RT-qPCR. From day 3 after HP PRRSV application until the end of the study, a viremia was detected by RT-qPCR in all of the piglets. On day 0 (day of HP PRRSV application), nine out of ten piglets of the pre-vaccinated group tested PRRSV antibody positive with one of the tested ELISAs, although with lower S/P values than after infection. On day 10 after HP PRRSV application, all study ELISAs except one had significantly higher S/P or OD values, respectively more positive samples, in group V than in group N. Conclusions: Only one of the tested ELISAs was able to detect reliably PRRSV antibodies in pigs vaccinated with an inactivated PRRSV vaccine. With most of the tested ELISAs, higher S/P values respectively more positive samples after PRRSV infection were seen in the pre-vaccinated group than in the non-vaccinated.
Schwein
ELISA
Enzyme-linked Immunosorbent AssayPRRSV
PRRS-Virus
Totimpfstoff
swine
ELISA
PRRSV
inactivated vaccine
ddc:636
3

STUDY TOWARD THE DEVELOPMENT OF ADVANCED INFLUENZA VACCINES

Wang, Leyi 11 September 2009 (has links)
No description available.
Virology
Avian Influenza
NS1 truncation variants
temperature sensitive
mutations
non-coding region
live attenuated vaccine
inactivated vaccine
4

Untersuchung verschiedener in Sachsen angewandter Impfstrategien zur Vorbeugung der Salmonella Enteritidis-Infektion in Legehennenbeständen

Käser, Cornelia 26 September 2012 (has links) (PDF)
In der vorliegenden Arbeit wurde einerseits der Verlauf der Schutzwirkung der zurzeit in Sachsens Legehennenbeständen überwiegend angewandten Impfschemata gegen Salmonella Enteritidis (SE) untersucht. Andererseits wurden die Impfschemata, die ausschließlich modifizierte Lebendimpfstoffe (MLV) umfassen, und Impfschemata, die aus einer Kombination von MLV und Inaktivatimpfstoffen (KV) bestehen, auf Unterschiede in der Wirksamkeit geprüft. Um die Wirksamkeit der Impfschemata im Verlauf der Legeperiode und im Vergleich miteinander untersuchen zu können, wurden zu drei verschiedenen Zeitpunkten der Legeperiode (39., 54. und 69. Lebenswoche (LW)) Infektionsversuche mit einem Nalidixinsäure-resistenten SE-Stamm durchgeführt. Es wurden insgesamt 180 Legehennen verwendet, die in fünf verschiedenen Herkunftsbetrieben etwa gleicher Größe aufgezogen und geimpft worden waren. In jedem der Herkunftsbetriebe wurde eines von fünf Impfschemata (A bis E) angewendet. Die Impfschemata A und C beinhalteten ausschließlich MLV, die Impfschemata B, D und E eine Kombination aus MLV und KV. Zu den genannten Zeitpunkten (39., 54. und 69. LW) wurden jeweils zwölf Tiere aus den Betrieben in den Infektionsstall des Instituts für Tierhygiene und Öffentliches Veterinärwesen verbracht und eingestallt. Nach der Adaptionsphase von einer Woche und der Prüfung der Tiere auf Salmonellenfreiheit wurde jedes Tier mit 1,0 x109 KbE SE oral infiziert. Zwei und sieben Tage post infectionem (p.inf). wurden jeweils sechs Hennen euthanasiert und seziert. Caeca, Leber-, Ovar- und Oviduktproben wurden entnommen und gemäß anerkannter quantitativer und qualitativer Untersuchungsmethoden auf den Infektionsstamm untersucht. Zur Kontrolle der Erregerausscheidung wurden ein, drei und fünf Tage p.inf. Kloakentupferproben von jedem Tier entnommen und entsprechend auf SE untersucht. Die Ergebnisse dieser Untersuchungen variierten in Abhängigkeit von Versuchs- und Sektions- bzw. Kloakentupferentnahmezeitpunkt, untersuchtem Organ sowie quantitativer und qualitativer Untersuchung. Die ausschließlich mit MLV geimpften Gruppen A und C wiesen im Vergleich zu den Gruppen D und E, die mit demselben MLV und zusätzlich mit einem KV geimpft worden waren, in den Kloakentupfer- und Caecumproben in der Regel qualitativ und quantitativ weniger Salmonellen auf. Der Salmonellennachweis in den Leberproben und den vereinzelt besiedelten Reproduktionsorganen variierte nur geringfügig zwischen den Impfgruppen. Da die Tiere der vier Impfgruppen aus jeweils anderen Herkunftsbetrieben stammten, sind haltungsbedingte Unterschiede anzunehmen. Das äußere Erscheinungsbild (Befiederung, Bemuskelung, makroskopische pathologische Veränderungen) und das Sozialverhalten der Tiere variierten, was mit Unterschieden in der Immunität einhergehen kann. Bei den Tieren der Gruppe A bzw. C waren in der 69. LW und in 54. LW, respektive, ein ausgeprägtes kannibalistisches Verhalten und dessen Konsequenzen (reduzierte Wasser- und Futteraufnahme der gepickten Tiere, Hackverletzungen) zu beobachten. Tendenziell waren die Tiere der Gruppen B bis E in der 54. LW stärker mit SE belastet als in der 39. und 69. LW. Ein Einfluss der unter Umständen erhöhten Umgebungstemperaturen in den Betrieben sowie des hohen Leistungsstresses während der mittleren Phase der Legeperiode auf die Immunität der 54 LW alten Tiere, die im August 2010 infiziert wurden, ist nicht auszuschließen. Auch eine sich ausbildende Altersresistenz könnte die bessere Salmonellenabwehr der 69 LW alten Tiere erklären. Tiere der Gruppe A waren jedoch in der 69. LW am stärksten mit SE belastet, was auf ein Nachlassen der durch die Impfung induzierten Immunität und möglicherweise auf den im Vergleich zu den jüngeren Tieren allgemein schwächeren Zustand der Tiere zurückzuführen ist. Die Ergebnisse einer Kontrollgruppe zur Beurteilung der von der Impfung unabhängigen Faktoren fehlen. Da in den sächsischen Legehennenhaltungen aufgrund der hohen Tierzahlen entsprechend der Hühner-Salmonellen Verordnung (Impfpflicht für Betriebe mit mehr als 350 Tieren) gegen SE geimpft wird, hätten zur Bildung einer ungeimpften Kontrollgruppe Tiere aus kleineren Betrieben oder Zuchttierhaltungen mit völlig anderen Haltungsstrukturen verwendet werden müssen. Damit wären die wissenschaftlichen Ansprüche an eine Kontrollgruppe jedoch nicht erfüllt worden. Entsprechend der Ergebnisse und Umstände dieser Studie scheint eine Zusatzimpfung mit einem KV im Vergleich zu einer Impfung mit ausschließlich MLV keinen Vorteil im Schutz vor SE zu bieten. Es konnte gezeigt werden, dass die Immunität der gemäß der Impfschemata B bis E geimpften Legehennen gegen SE am Ende der Legeperiode nicht nachlässt. Die Impfung allein kann den Erreger nicht eliminieren und muss daher stets in ein verantwortungsvolles und vielseitiges Bekämpfungsprogramm integriert werden.
Salmonella Enteritidis
Legehenne
Lebendimpfstoffe
Inaktivatimpfstoffe
experimentelle Infektion
Salmonella Enteritidis
laying hen
live vaccine
inactivated vaccine
experimental infection
ddc:636.089
5

Vacinologia e patogenicidade de amostras recombinantes de herpesvírus bovino tipo 1 (BoHV-1) / Vaccinology and pathogenicity of recombinants strains of the bovine herpesvirus type 1 (BoHV-1)

Silva, Alessandra D'Avila da January 2007 (has links)
O herpesvírus bovino tipo 1 (BoHV-1) é um dos principais agentes causadores de prejuízos econômicos em criações de bovinos. A vacinação tem sido amplamente utilizada para minimizar as perdas causadas por infecções pelo BoHV-1. Dentre as vacinas disponíveis, as vacinas desenvolvidas a partir de amostras virais recombinantes apresentam a vantagem de permitirem a diferenciação entre animais infectados e imunizados. Anteriormente, foi desenvolvida uma vacina recombinante diferencial com uma amostra de BoHV-1 brasileira baseada na deleção do gene que codifica a glicoproteína E (gE). No primeiro capítulo do presente trabalho, a segurança e imunogenicidade desta vacina recombinante inativada foi avaliada. Os experimentos de imunização, desafio e reativação da vacina diferencial em animais experimentalmente inoculados demonstraram que a vacina recombinante foi segura e eficiente ao minimizar ou mesmo prevenir os efeitos da infecção pelo BoHV-1. No segundo capítulo, a segurança da vacina gE- foi avaliada, através da imunização intramuscular (IM) de 22 vacas (14 BoHV-1 soronegativas e 8 soropositivas) prenhes. Foi observada soroconverão, mas não abortos e nem anormalidades fetais nos animais imunizados. Na segunda parte do mesmo estudo foi analizada a capacidade do vírus recombinante difundir-se em um rebanho bovino. Quatro terneiros foram inoculados pela rota intranasal (IN) com a amostra recombinante gE- e, posteriormente, adicionados a outros 16 animais com mesma idade e semelhante condição corporal durante 180 dias. Todos os animais foram monitorados diariamente em busca de sintomatologia clínica. Foi observada soroconversão apenas nos animais imunizados. Estes resultados indicam que, nas condições deste estudo, a amostra recombinante não causou nenhum dano nas vacas prenhes ou em seus terneiros e não foi capaz de difundir-se horizontalmente no rebanho. No terceiro capítulo foi avaliada a patogenicidade de uma amostra recombinante de BoHV-1 com deleção no gene Us9, utilizando coelhos como modelo experimental. Coelhos com quatro semanas de idade foram divididos em quatro grupos (A, B, C, D). Dois grupos (A e B) foram infectados via intranasal (IN) e dois (C e D) infectados via intraocular (IO). Em cada via de infecção, um grupo foi infectado com o vírus recombinante e o outro com o vírus selvagem (wt). Após a infecção IO, todos os animais, de ambos os grupos, desenvolveram intensa conjuntivite entre os dias 3 a 10 pós-inoculação (pi). Vírus infeccioso foi consistentemente isolado a partir dos suabes oculares entre os dias 1 a 10 pi chegando a um título máximo de 103,05 TCID50/mL. Nos grupos infectados pela via IN com BoHV-1 wt, 4/4 coelhos apresentaram sintomatologia característica da doença, tais como: pirexia, apatia, anorexia, tosse, secreção nasal severa (entre os dias 2 e 8 pi). Animais inoculados com o recombinante apresentaram apatia, anorexia e descarga nasal (entre os dias 3 e 7 pi). Vírus infeccioso foi isolado em diversos tecidos tanto nos animais inoculados com o vírus wt como recombinante. Ambos os vírus foram capazes de replicar nas mucosas. Análises histológicas dos tecidos dos animais demonstraram lesões em ambos os grupos. Este estudo apresentou que a proteína Us9 não tem um papel significante na patogenicidade in vivo. / Bovine herpesvirus type 1 (BoHV-1) is an the major cause of losses in cattle. Vaccination has been widely applied to minimize losses induced by BoHV-1 infections. Vacines developed from recombinant strains have the advantage of allow the differentiation between immunized and infected animals. Previously, a recombinant differential BoHV-1 vaccine based on a glycoprotein E deleted (gE) virus was developed. In the first chapter of the present work, the safety and immunogenicity of such recombinant, as a inactivate vaccine, was evaluated. The experiments showed that the DIVA vaccinne was safe and efficient in order to minimize or even prevent the clinical signs of the infection by BoHV- 1. In the second chapter of the present study, the safety of the gE- vaccine during pregnancy was evaluated by the intramuscular inoculation into 22 pregnant dams (14 BoHV-1 seronegative; 8 seropositive). Seroconversion was detected but no abortions, stillbirths or fetal abnormalities were seen after vaccination. In the second part of the same study, the potential of the gE- vaccine virus to spread among beef cattle under field conditions was examined. Four heifers were inoculated intranasally (IN) with the gE- vaccine and mixed with other 16 animals at the same age and body conditions, for 180 days. All animals were daily monitored for clinical signs.. Seroconversion was observed only in vaccinated heifers. These results indicate that, under the conditions of the present study, the gE vaccine virus did not cause any noticeable harmful effect on pregnant dams and on its offspring and did not spread horizontally among cattle. In the third chapter the pathogenicity of a US9 negative recombinant strain BoHV-1 using rabbits as an experimental model was avaluated. Rabbits four weeks old were divided in four groups (A, B, C, D) within four rabbits per group. Two groups were infected IN route and two via intraocular (IO). In each route, one group was infected by recombinant virus and the other infected by wild type (wt) virus. After IO infection, all rabbits developed intense conjunctivitis between days 3 to 10 pos infection (pi). Infective virus was consistently isolated from ocular swabs on days 1 to 10, reaching a maximum of 103.05 TCID50/mL. Animals infected in the IN rote with BoHV-1 wt, 4/4 rabbits showed characteristic signs of disease, which included pyrexia, apathy, anorexia, cough, severe nasal secretion between days 2 to 8. Rabbits inoculated with recombinant virus showed apathy, anorexia, nasal secretion (between days 3 and 7pi). Infectious virus was isolated in differents tissues as much as animals inoculated with wt and recombinant virus. Both virus were capable of replication in the mucosa nasal and ocular of the inoculated rabbits. Histopatological lesions were evident in both groups. In the present study showed which the US9 protein have not significantly in the pathogenicity in vivo.
Herpesvírus bovino
Virologia veterinaria : Vacinas
Vacinas
Bovine herpesvirus type 1
gE protein
US9 protein
Pathogenicity
Inactivated vaccine
Recombinant virus
6

Vacinologia e patogenicidade de amostras recombinantes de herpesvírus bovino tipo 1 (BoHV-1) / Vaccinology and pathogenicity of recombinants strains of the bovine herpesvirus type 1 (BoHV-1)

Silva, Alessandra D'Avila da January 2007 (has links)
O herpesvírus bovino tipo 1 (BoHV-1) é um dos principais agentes causadores de prejuízos econômicos em criações de bovinos. A vacinação tem sido amplamente utilizada para minimizar as perdas causadas por infecções pelo BoHV-1. Dentre as vacinas disponíveis, as vacinas desenvolvidas a partir de amostras virais recombinantes apresentam a vantagem de permitirem a diferenciação entre animais infectados e imunizados. Anteriormente, foi desenvolvida uma vacina recombinante diferencial com uma amostra de BoHV-1 brasileira baseada na deleção do gene que codifica a glicoproteína E (gE). No primeiro capítulo do presente trabalho, a segurança e imunogenicidade desta vacina recombinante inativada foi avaliada. Os experimentos de imunização, desafio e reativação da vacina diferencial em animais experimentalmente inoculados demonstraram que a vacina recombinante foi segura e eficiente ao minimizar ou mesmo prevenir os efeitos da infecção pelo BoHV-1. No segundo capítulo, a segurança da vacina gE- foi avaliada, através da imunização intramuscular (IM) de 22 vacas (14 BoHV-1 soronegativas e 8 soropositivas) prenhes. Foi observada soroconverão, mas não abortos e nem anormalidades fetais nos animais imunizados. Na segunda parte do mesmo estudo foi analizada a capacidade do vírus recombinante difundir-se em um rebanho bovino. Quatro terneiros foram inoculados pela rota intranasal (IN) com a amostra recombinante gE- e, posteriormente, adicionados a outros 16 animais com mesma idade e semelhante condição corporal durante 180 dias. Todos os animais foram monitorados diariamente em busca de sintomatologia clínica. Foi observada soroconversão apenas nos animais imunizados. Estes resultados indicam que, nas condições deste estudo, a amostra recombinante não causou nenhum dano nas vacas prenhes ou em seus terneiros e não foi capaz de difundir-se horizontalmente no rebanho. No terceiro capítulo foi avaliada a patogenicidade de uma amostra recombinante de BoHV-1 com deleção no gene Us9, utilizando coelhos como modelo experimental. Coelhos com quatro semanas de idade foram divididos em quatro grupos (A, B, C, D). Dois grupos (A e B) foram infectados via intranasal (IN) e dois (C e D) infectados via intraocular (IO). Em cada via de infecção, um grupo foi infectado com o vírus recombinante e o outro com o vírus selvagem (wt). Após a infecção IO, todos os animais, de ambos os grupos, desenvolveram intensa conjuntivite entre os dias 3 a 10 pós-inoculação (pi). Vírus infeccioso foi consistentemente isolado a partir dos suabes oculares entre os dias 1 a 10 pi chegando a um título máximo de 103,05 TCID50/mL. Nos grupos infectados pela via IN com BoHV-1 wt, 4/4 coelhos apresentaram sintomatologia característica da doença, tais como: pirexia, apatia, anorexia, tosse, secreção nasal severa (entre os dias 2 e 8 pi). Animais inoculados com o recombinante apresentaram apatia, anorexia e descarga nasal (entre os dias 3 e 7 pi). Vírus infeccioso foi isolado em diversos tecidos tanto nos animais inoculados com o vírus wt como recombinante. Ambos os vírus foram capazes de replicar nas mucosas. Análises histológicas dos tecidos dos animais demonstraram lesões em ambos os grupos. Este estudo apresentou que a proteína Us9 não tem um papel significante na patogenicidade in vivo. / Bovine herpesvirus type 1 (BoHV-1) is an the major cause of losses in cattle. Vaccination has been widely applied to minimize losses induced by BoHV-1 infections. Vacines developed from recombinant strains have the advantage of allow the differentiation between immunized and infected animals. Previously, a recombinant differential BoHV-1 vaccine based on a glycoprotein E deleted (gE) virus was developed. In the first chapter of the present work, the safety and immunogenicity of such recombinant, as a inactivate vaccine, was evaluated. The experiments showed that the DIVA vaccinne was safe and efficient in order to minimize or even prevent the clinical signs of the infection by BoHV- 1. In the second chapter of the present study, the safety of the gE- vaccine during pregnancy was evaluated by the intramuscular inoculation into 22 pregnant dams (14 BoHV-1 seronegative; 8 seropositive). Seroconversion was detected but no abortions, stillbirths or fetal abnormalities were seen after vaccination. In the second part of the same study, the potential of the gE- vaccine virus to spread among beef cattle under field conditions was examined. Four heifers were inoculated intranasally (IN) with the gE- vaccine and mixed with other 16 animals at the same age and body conditions, for 180 days. All animals were daily monitored for clinical signs.. Seroconversion was observed only in vaccinated heifers. These results indicate that, under the conditions of the present study, the gE vaccine virus did not cause any noticeable harmful effect on pregnant dams and on its offspring and did not spread horizontally among cattle. In the third chapter the pathogenicity of a US9 negative recombinant strain BoHV-1 using rabbits as an experimental model was avaluated. Rabbits four weeks old were divided in four groups (A, B, C, D) within four rabbits per group. Two groups were infected IN route and two via intraocular (IO). In each route, one group was infected by recombinant virus and the other infected by wild type (wt) virus. After IO infection, all rabbits developed intense conjunctivitis between days 3 to 10 pos infection (pi). Infective virus was consistently isolated from ocular swabs on days 1 to 10, reaching a maximum of 103.05 TCID50/mL. Animals infected in the IN rote with BoHV-1 wt, 4/4 rabbits showed characteristic signs of disease, which included pyrexia, apathy, anorexia, cough, severe nasal secretion between days 2 to 8. Rabbits inoculated with recombinant virus showed apathy, anorexia, nasal secretion (between days 3 and 7pi). Infectious virus was isolated in differents tissues as much as animals inoculated with wt and recombinant virus. Both virus were capable of replication in the mucosa nasal and ocular of the inoculated rabbits. Histopatological lesions were evident in both groups. In the present study showed which the US9 protein have not significantly in the pathogenicity in vivo.
Herpesvírus bovino
Virologia veterinaria : Vacinas
Vacinas
Bovine herpesvirus type 1
gE protein
US9 protein
Pathogenicity
Inactivated vaccine
Recombinant virus
7

Vacinologia e patogenicidade de amostras recombinantes de herpesvírus bovino tipo 1 (BoHV-1) / Vaccinology and pathogenicity of recombinants strains of the bovine herpesvirus type 1 (BoHV-1)

Silva, Alessandra D'Avila da January 2007 (has links)
O herpesvírus bovino tipo 1 (BoHV-1) é um dos principais agentes causadores de prejuízos econômicos em criações de bovinos. A vacinação tem sido amplamente utilizada para minimizar as perdas causadas por infecções pelo BoHV-1. Dentre as vacinas disponíveis, as vacinas desenvolvidas a partir de amostras virais recombinantes apresentam a vantagem de permitirem a diferenciação entre animais infectados e imunizados. Anteriormente, foi desenvolvida uma vacina recombinante diferencial com uma amostra de BoHV-1 brasileira baseada na deleção do gene que codifica a glicoproteína E (gE). No primeiro capítulo do presente trabalho, a segurança e imunogenicidade desta vacina recombinante inativada foi avaliada. Os experimentos de imunização, desafio e reativação da vacina diferencial em animais experimentalmente inoculados demonstraram que a vacina recombinante foi segura e eficiente ao minimizar ou mesmo prevenir os efeitos da infecção pelo BoHV-1. No segundo capítulo, a segurança da vacina gE- foi avaliada, através da imunização intramuscular (IM) de 22 vacas (14 BoHV-1 soronegativas e 8 soropositivas) prenhes. Foi observada soroconverão, mas não abortos e nem anormalidades fetais nos animais imunizados. Na segunda parte do mesmo estudo foi analizada a capacidade do vírus recombinante difundir-se em um rebanho bovino. Quatro terneiros foram inoculados pela rota intranasal (IN) com a amostra recombinante gE- e, posteriormente, adicionados a outros 16 animais com mesma idade e semelhante condição corporal durante 180 dias. Todos os animais foram monitorados diariamente em busca de sintomatologia clínica. Foi observada soroconversão apenas nos animais imunizados. Estes resultados indicam que, nas condições deste estudo, a amostra recombinante não causou nenhum dano nas vacas prenhes ou em seus terneiros e não foi capaz de difundir-se horizontalmente no rebanho. No terceiro capítulo foi avaliada a patogenicidade de uma amostra recombinante de BoHV-1 com deleção no gene Us9, utilizando coelhos como modelo experimental. Coelhos com quatro semanas de idade foram divididos em quatro grupos (A, B, C, D). Dois grupos (A e B) foram infectados via intranasal (IN) e dois (C e D) infectados via intraocular (IO). Em cada via de infecção, um grupo foi infectado com o vírus recombinante e o outro com o vírus selvagem (wt). Após a infecção IO, todos os animais, de ambos os grupos, desenvolveram intensa conjuntivite entre os dias 3 a 10 pós-inoculação (pi). Vírus infeccioso foi consistentemente isolado a partir dos suabes oculares entre os dias 1 a 10 pi chegando a um título máximo de 103,05 TCID50/mL. Nos grupos infectados pela via IN com BoHV-1 wt, 4/4 coelhos apresentaram sintomatologia característica da doença, tais como: pirexia, apatia, anorexia, tosse, secreção nasal severa (entre os dias 2 e 8 pi). Animais inoculados com o recombinante apresentaram apatia, anorexia e descarga nasal (entre os dias 3 e 7 pi). Vírus infeccioso foi isolado em diversos tecidos tanto nos animais inoculados com o vírus wt como recombinante. Ambos os vírus foram capazes de replicar nas mucosas. Análises histológicas dos tecidos dos animais demonstraram lesões em ambos os grupos. Este estudo apresentou que a proteína Us9 não tem um papel significante na patogenicidade in vivo. / Bovine herpesvirus type 1 (BoHV-1) is an the major cause of losses in cattle. Vaccination has been widely applied to minimize losses induced by BoHV-1 infections. Vacines developed from recombinant strains have the advantage of allow the differentiation between immunized and infected animals. Previously, a recombinant differential BoHV-1 vaccine based on a glycoprotein E deleted (gE) virus was developed. In the first chapter of the present work, the safety and immunogenicity of such recombinant, as a inactivate vaccine, was evaluated. The experiments showed that the DIVA vaccinne was safe and efficient in order to minimize or even prevent the clinical signs of the infection by BoHV- 1. In the second chapter of the present study, the safety of the gE- vaccine during pregnancy was evaluated by the intramuscular inoculation into 22 pregnant dams (14 BoHV-1 seronegative; 8 seropositive). Seroconversion was detected but no abortions, stillbirths or fetal abnormalities were seen after vaccination. In the second part of the same study, the potential of the gE- vaccine virus to spread among beef cattle under field conditions was examined. Four heifers were inoculated intranasally (IN) with the gE- vaccine and mixed with other 16 animals at the same age and body conditions, for 180 days. All animals were daily monitored for clinical signs.. Seroconversion was observed only in vaccinated heifers. These results indicate that, under the conditions of the present study, the gE vaccine virus did not cause any noticeable harmful effect on pregnant dams and on its offspring and did not spread horizontally among cattle. In the third chapter the pathogenicity of a US9 negative recombinant strain BoHV-1 using rabbits as an experimental model was avaluated. Rabbits four weeks old were divided in four groups (A, B, C, D) within four rabbits per group. Two groups were infected IN route and two via intraocular (IO). In each route, one group was infected by recombinant virus and the other infected by wild type (wt) virus. After IO infection, all rabbits developed intense conjunctivitis between days 3 to 10 pos infection (pi). Infective virus was consistently isolated from ocular swabs on days 1 to 10, reaching a maximum of 103.05 TCID50/mL. Animals infected in the IN rote with BoHV-1 wt, 4/4 rabbits showed characteristic signs of disease, which included pyrexia, apathy, anorexia, cough, severe nasal secretion between days 2 to 8. Rabbits inoculated with recombinant virus showed apathy, anorexia, nasal secretion (between days 3 and 7pi). Infectious virus was isolated in differents tissues as much as animals inoculated with wt and recombinant virus. Both virus were capable of replication in the mucosa nasal and ocular of the inoculated rabbits. Histopatological lesions were evident in both groups. In the present study showed which the US9 protein have not significantly in the pathogenicity in vivo.
Herpesvírus bovino
Virologia veterinaria : Vacinas
Vacinas
Bovine herpesvirus type 1
gE protein
US9 protein
Pathogenicity
Inactivated vaccine
Recombinant virus
8

Resposta de crianças portadoras de síndrome de Down e de hepatopatia crônica a uma vacina inativada (HAVRIX) contra hepatite A

Ferreira, Cristina Helena Targa January 2001 (has links)
Objetivo: A vacina inativada contra HVA (Havrix) é altamente eficaz e segura em crianças saudáveis. Não há muitos dados disponíveis na literatura sobre a resposta de crianças imunocomprometidas à essa vacina. O objetivo deste estudo foi avaliar a resposta de pacientes pediátricos portadores de Síndrome de Down e de Hepatopatia Crônica à uma vacina inativada contra Hepatite A, comparando suas respostas com as de crianças saudáveis. Casuística e Métodos: Foi realizado um estudo prospectivo, aberto e controlado com 138 crianças e adolescentes, de 1 a 16 anos, suscetíveis à infecção pelo virus A (anti-HVA negativo). Os indivíduos foram divididos em 3 grupos: Grupo I: portadores de Síndrome de Down (n = 49), Grupo II: Hepatopatas Crônicos (n = 34) e Grupo III: controle, composto por crianças saudáveis (n = 55). Todos os indivíduos recebiam 2 doses, nos meses 0 e 6, da vacina Havrix 720 UE , aplicada intramuscular, no deltóide. Um mês após cada dose da vacina, as crianças e os adolescentes eram submetidas à coleta de sangue para realização de titulação de anticorpos anti-HVA. Resultados: As taxas de soroconversão, após a primeira dose da vacina, no mês 1, foram de 92%, 76% e 94% nos grupos I, II e III, respectivamente. Um mês após a segunda dose, as porcentagens de soroconversão foram de 100% x 97% x 100%, para os grupos, na mesma ordem. As médias geométricas dos títulos de anticorpos anti-HVA foram, na primeira e segunda coletas, de 164,02 e 1719,86 mUI/ml nas crianças com Síndrome de Down, de 107,77 e 812,40 mUI/ml nos cirróticos e de 160,77 e 2344,90 mUI/ml, no grupo controle. O grupo dos pacientes cirróticos apresentou diferença estatisticamente significativa em relação às taxas de soroconversão no primeiro mês, após 1 dose da vacina, e aos títulos de anticorpos anti-HVA no final do estudo, quando comparado aos controles saudáveis. Apenas 14% dos indivíduos vacinados apresentaram sintomas locais, como dor e vermelhidão. Cinco porcento apresentaram sintomas gerais. Não ocorreu nenhum efeito adverso sério ou reação imediata à vacina. Os efeitos adversos diminuíram por ocasião da segunda dose.Conclusões: A vacina inativada Havrix, contra Hepatite A, provoca altas taxas de soroconversão e é altamente segura em pacientes pediátricos portadores de Síndrome de Down e de Cirrose. As crianças e adolescentes com Cirrose respondem à vacina inativada anti-HVA com títulos de anticorpos mais baixos do que as crianças saudáveis e do que as portadoras de Síndrome de Down. / Objective: The inactivated hepatitis A vaccine (Havrix) is highly immunogenic and safe in healthy children. However, data about the response of immunocompromised children to this vaccine are not very frequent in the literature. The objective of this study was to assess the response of pediatric patients with Down syndrome and chronic liver disease to an inactivated hepatitis A vaccine, and to compare their responses to those of healthy children. Patients and Methods: A prospective, open-label, controlled study was performed with 138 children and adolescents susceptible to hepatitis A virus (anti-HAV negative) with ages between 1 and 16 years. Patients were divided into three groups: Group I, Down syndrome patients (n = 49); Group II, patients with chronic liver disease (n = 34); and Group III, healthy children/controls (n = 55). All patients and controls received two intramuscular doses of Havrix 720 UE in the deltoid muscle at months 0 and 6. One month after each dose, patients underwent blood collection for the assessment of anti-HAV titers. Results: Seroconversion rates after the first dose (month 1) were 92%, 76%, and 94% in Groups I, II, and III, respectively; one month after the second dose, these percentages were 100%, 97%, and 100%. Geometric mean titers were 164.02 and 1719.86 mUI/ml in the first and second collections for Down syndrome children; 107.77 and 812.40 mUI/ml for cirrhotic patients; and 160.77 and 2344.90 mUI/ml for controls. The group of cirrhotic patients presented a statistically significant difference in seroconversion rates at month 1, and in anti-HAV titers in the end of the study when compared to healthy controls. Only 14% of the vaccinated individuals presented local symptoms, such as pain and redness; 5% presented general symptoms. No severe adverse effects or immediate reaction to the vaccine were observed. The occurrence of adverse reactions was lower in the application of the second dose. Conclusions: The inactivated hepatitis A vaccine (Havrix) presents high rates of seroconversion and is highly safe in pediatric patients with Down syndrome and cirrhosis. Cirrhotic children and adolescents have responded to the inactivated hepatitis A vaccine with lower antibody titers when compared to healthy children and Down syndrome.
Hepatite A
Síndrome de Down
Hepatopatias
Vacinas contra hepatite A
Criança
Down syndrome
Chronic liver disease
Cirrhosis
Hepatitis A
Hepatitis A vaccine
Inactivated vaccine
Immunodeficiency
Immunocompromised
Anti-HAV antibody
9

Resposta de crianças portadoras de síndrome de Down e de hepatopatia crônica a uma vacina inativada (HAVRIX) contra hepatite A

Ferreira, Cristina Helena Targa January 2001 (has links)
Objetivo: A vacina inativada contra HVA (Havrix) é altamente eficaz e segura em crianças saudáveis. Não há muitos dados disponíveis na literatura sobre a resposta de crianças imunocomprometidas à essa vacina. O objetivo deste estudo foi avaliar a resposta de pacientes pediátricos portadores de Síndrome de Down e de Hepatopatia Crônica à uma vacina inativada contra Hepatite A, comparando suas respostas com as de crianças saudáveis. Casuística e Métodos: Foi realizado um estudo prospectivo, aberto e controlado com 138 crianças e adolescentes, de 1 a 16 anos, suscetíveis à infecção pelo virus A (anti-HVA negativo). Os indivíduos foram divididos em 3 grupos: Grupo I: portadores de Síndrome de Down (n = 49), Grupo II: Hepatopatas Crônicos (n = 34) e Grupo III: controle, composto por crianças saudáveis (n = 55). Todos os indivíduos recebiam 2 doses, nos meses 0 e 6, da vacina Havrix 720 UE , aplicada intramuscular, no deltóide. Um mês após cada dose da vacina, as crianças e os adolescentes eram submetidas à coleta de sangue para realização de titulação de anticorpos anti-HVA. Resultados: As taxas de soroconversão, após a primeira dose da vacina, no mês 1, foram de 92%, 76% e 94% nos grupos I, II e III, respectivamente. Um mês após a segunda dose, as porcentagens de soroconversão foram de 100% x 97% x 100%, para os grupos, na mesma ordem. As médias geométricas dos títulos de anticorpos anti-HVA foram, na primeira e segunda coletas, de 164,02 e 1719,86 mUI/ml nas crianças com Síndrome de Down, de 107,77 e 812,40 mUI/ml nos cirróticos e de 160,77 e 2344,90 mUI/ml, no grupo controle. O grupo dos pacientes cirróticos apresentou diferença estatisticamente significativa em relação às taxas de soroconversão no primeiro mês, após 1 dose da vacina, e aos títulos de anticorpos anti-HVA no final do estudo, quando comparado aos controles saudáveis. Apenas 14% dos indivíduos vacinados apresentaram sintomas locais, como dor e vermelhidão. Cinco porcento apresentaram sintomas gerais. Não ocorreu nenhum efeito adverso sério ou reação imediata à vacina. Os efeitos adversos diminuíram por ocasião da segunda dose.Conclusões: A vacina inativada Havrix, contra Hepatite A, provoca altas taxas de soroconversão e é altamente segura em pacientes pediátricos portadores de Síndrome de Down e de Cirrose. As crianças e adolescentes com Cirrose respondem à vacina inativada anti-HVA com títulos de anticorpos mais baixos do que as crianças saudáveis e do que as portadoras de Síndrome de Down. / Objective: The inactivated hepatitis A vaccine (Havrix) is highly immunogenic and safe in healthy children. However, data about the response of immunocompromised children to this vaccine are not very frequent in the literature. The objective of this study was to assess the response of pediatric patients with Down syndrome and chronic liver disease to an inactivated hepatitis A vaccine, and to compare their responses to those of healthy children. Patients and Methods: A prospective, open-label, controlled study was performed with 138 children and adolescents susceptible to hepatitis A virus (anti-HAV negative) with ages between 1 and 16 years. Patients were divided into three groups: Group I, Down syndrome patients (n = 49); Group II, patients with chronic liver disease (n = 34); and Group III, healthy children/controls (n = 55). All patients and controls received two intramuscular doses of Havrix 720 UE in the deltoid muscle at months 0 and 6. One month after each dose, patients underwent blood collection for the assessment of anti-HAV titers. Results: Seroconversion rates after the first dose (month 1) were 92%, 76%, and 94% in Groups I, II, and III, respectively; one month after the second dose, these percentages were 100%, 97%, and 100%. Geometric mean titers were 164.02 and 1719.86 mUI/ml in the first and second collections for Down syndrome children; 107.77 and 812.40 mUI/ml for cirrhotic patients; and 160.77 and 2344.90 mUI/ml for controls. The group of cirrhotic patients presented a statistically significant difference in seroconversion rates at month 1, and in anti-HAV titers in the end of the study when compared to healthy controls. Only 14% of the vaccinated individuals presented local symptoms, such as pain and redness; 5% presented general symptoms. No severe adverse effects or immediate reaction to the vaccine were observed. The occurrence of adverse reactions was lower in the application of the second dose. Conclusions: The inactivated hepatitis A vaccine (Havrix) presents high rates of seroconversion and is highly safe in pediatric patients with Down syndrome and cirrhosis. Cirrhotic children and adolescents have responded to the inactivated hepatitis A vaccine with lower antibody titers when compared to healthy children and Down syndrome.
Hepatite A
Síndrome de Down
Hepatopatias
Vacinas contra hepatite A
Criança
Down syndrome
Chronic liver disease
Cirrhosis
Hepatitis A
Hepatitis A vaccine
Inactivated vaccine
Immunodeficiency
Immunocompromised
Anti-HAV antibody
10

Resposta de crianças portadoras de síndrome de Down e de hepatopatia crônica a uma vacina inativada (HAVRIX) contra hepatite A

Ferreira, Cristina Helena Targa January 2001 (has links)
Objetivo: A vacina inativada contra HVA (Havrix) é altamente eficaz e segura em crianças saudáveis. Não há muitos dados disponíveis na literatura sobre a resposta de crianças imunocomprometidas à essa vacina. O objetivo deste estudo foi avaliar a resposta de pacientes pediátricos portadores de Síndrome de Down e de Hepatopatia Crônica à uma vacina inativada contra Hepatite A, comparando suas respostas com as de crianças saudáveis. Casuística e Métodos: Foi realizado um estudo prospectivo, aberto e controlado com 138 crianças e adolescentes, de 1 a 16 anos, suscetíveis à infecção pelo virus A (anti-HVA negativo). Os indivíduos foram divididos em 3 grupos: Grupo I: portadores de Síndrome de Down (n = 49), Grupo II: Hepatopatas Crônicos (n = 34) e Grupo III: controle, composto por crianças saudáveis (n = 55). Todos os indivíduos recebiam 2 doses, nos meses 0 e 6, da vacina Havrix 720 UE , aplicada intramuscular, no deltóide. Um mês após cada dose da vacina, as crianças e os adolescentes eram submetidas à coleta de sangue para realização de titulação de anticorpos anti-HVA. Resultados: As taxas de soroconversão, após a primeira dose da vacina, no mês 1, foram de 92%, 76% e 94% nos grupos I, II e III, respectivamente. Um mês após a segunda dose, as porcentagens de soroconversão foram de 100% x 97% x 100%, para os grupos, na mesma ordem. As médias geométricas dos títulos de anticorpos anti-HVA foram, na primeira e segunda coletas, de 164,02 e 1719,86 mUI/ml nas crianças com Síndrome de Down, de 107,77 e 812,40 mUI/ml nos cirróticos e de 160,77 e 2344,90 mUI/ml, no grupo controle. O grupo dos pacientes cirróticos apresentou diferença estatisticamente significativa em relação às taxas de soroconversão no primeiro mês, após 1 dose da vacina, e aos títulos de anticorpos anti-HVA no final do estudo, quando comparado aos controles saudáveis. Apenas 14% dos indivíduos vacinados apresentaram sintomas locais, como dor e vermelhidão. Cinco porcento apresentaram sintomas gerais. Não ocorreu nenhum efeito adverso sério ou reação imediata à vacina. Os efeitos adversos diminuíram por ocasião da segunda dose.Conclusões: A vacina inativada Havrix, contra Hepatite A, provoca altas taxas de soroconversão e é altamente segura em pacientes pediátricos portadores de Síndrome de Down e de Cirrose. As crianças e adolescentes com Cirrose respondem à vacina inativada anti-HVA com títulos de anticorpos mais baixos do que as crianças saudáveis e do que as portadoras de Síndrome de Down. / Objective: The inactivated hepatitis A vaccine (Havrix) is highly immunogenic and safe in healthy children. However, data about the response of immunocompromised children to this vaccine are not very frequent in the literature. The objective of this study was to assess the response of pediatric patients with Down syndrome and chronic liver disease to an inactivated hepatitis A vaccine, and to compare their responses to those of healthy children. Patients and Methods: A prospective, open-label, controlled study was performed with 138 children and adolescents susceptible to hepatitis A virus (anti-HAV negative) with ages between 1 and 16 years. Patients were divided into three groups: Group I, Down syndrome patients (n = 49); Group II, patients with chronic liver disease (n = 34); and Group III, healthy children/controls (n = 55). All patients and controls received two intramuscular doses of Havrix 720 UE in the deltoid muscle at months 0 and 6. One month after each dose, patients underwent blood collection for the assessment of anti-HAV titers. Results: Seroconversion rates after the first dose (month 1) were 92%, 76%, and 94% in Groups I, II, and III, respectively; one month after the second dose, these percentages were 100%, 97%, and 100%. Geometric mean titers were 164.02 and 1719.86 mUI/ml in the first and second collections for Down syndrome children; 107.77 and 812.40 mUI/ml for cirrhotic patients; and 160.77 and 2344.90 mUI/ml for controls. The group of cirrhotic patients presented a statistically significant difference in seroconversion rates at month 1, and in anti-HAV titers in the end of the study when compared to healthy controls. Only 14% of the vaccinated individuals presented local symptoms, such as pain and redness; 5% presented general symptoms. No severe adverse effects or immediate reaction to the vaccine were observed. The occurrence of adverse reactions was lower in the application of the second dose. Conclusions: The inactivated hepatitis A vaccine (Havrix) presents high rates of seroconversion and is highly safe in pediatric patients with Down syndrome and cirrhosis. Cirrhotic children and adolescents have responded to the inactivated hepatitis A vaccine with lower antibody titers when compared to healthy children and Down syndrome.
Hepatite A
Síndrome de Down
Hepatopatias
Vacinas contra hepatite A
Criança
Down syndrome
Chronic liver disease
Cirrhosis
Hepatitis A
Hepatitis A vaccine
Inactivated vaccine
Immunodeficiency
Immunocompromised
Anti-HAV antibody

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