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Cytomegalovirus and Vascular Function During PregnancyGombos, Randi B Unknown Date
No description available.
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Proposição de um modelo matemático para o estudo da alteração mecânica do músculo liso da traquéia de ratos Wistar exposto à solução de formaldeído e submetido a doses crescentes de um agente contrátil / Proposition of a mathematical model to study the mechanical change of the smooth muscle of the trachea of Wistar rats exposed to formaldehyde solution and subjected to increasing doses of a contractile agentMac Gayver da Silva Castro 23 July 2012 (has links)
A viscoelasticidade do pulmão do mamífero é determinada principalmente pelas propriedades mecânicas, estrutura e regulação do músculo liso das vias aéreas. A exposição ao ar poluído pode deteriorar essas propriedades com consequências danosas à saúde individual. O formaldeído é um importante poluente presente em ambientes internos que adentra o músculo liso formando ligações covalentes entre proteínas da matriz extracelular e da estrutura intracelular deteriorando algumas funções do músculo liso das vias aéreas, alterando propriedades mecânicas e induzindo a hiperresponsividade. O primeiro objetivo desse trabalho foi desenvolver um modelo de rede viscoelástica bidimensional baseada na tesselação de Voronoi para reproduzir algumas propriedades mecânicas do músculo liso de via aérea a nível de tecido. O segundo objetivo foi comparar os resultados obtidos com o nosso modelo com aqueles previamente observados em experimentos com tiras de tecido após a exposição ao formaldeído. Nosso modelo simula as propriedades mecânicas do músculo liso de via aérea usando um conjunto de molas e amortecedores. Esse conjunto de molas e amortecedores não somente mimetiza as propriedades viscoeláticas do músculo liso mas também o aparato contrátil das células. Nós hipotetizamos que a formação de ligações covalentes, devido à ação do formaldeído, pode ser representada no modelo por uma alteração simples na constante elástica das molas, enquanto que a ação da metacolina reduz o tamanho da mola. Nosso modelo é hábil para reproduzir uma medida de força isométrica onde o músculo liso é sujeito a um agente contrátil, com e sem exposição in vitro ao formaldeído. Assim, a nossa nova abordagem mecanicista incorpora diversas propriedades bem conhecidas do sistema contrátil das células em um tecido a nível de modelo. O modelo pode também ser usado em diferentes escalas biológicas / The viscoelastic properties of the mammalian lung is mainly determined by the mechanical properties, structure and regulation of the airways smooth muscle. The exposure to polluted air may deteriorate these properties with harmful consequences to individual health. Formaldehyde is an important indoor pollutant that permeate through the smooth muscle tissue forming covalent bonds between proteins in the extracellular matrix and intracellular protein structure deteriorating some of the airways smooth muscle functions, changing mechanical properties, and inducing hyperresponsiveness. The first objectives of this work was to develop a two-dimensional viscoelastic network model based on Voronoi tessellation to reproduce some of the mechanical properties of airway smooth muscle at the tissue level. The second objective was to compare the results obtained with our model with those previously observed in tissue strip experiments after the tissue exposure to formaldehyde. Our model simulates the mechanical properties of airway smooth muscle using a set of springs and dashpot. This set of springs and dashpot not only mimic the viscoelastic properties of the smooth muscle but also the cells contractile apparatus. We hypothesize that the formation of covalent bonds, due to the action formaldehyde, can be represented in the model by a simple change in the elastic constant of the springs, while the action of methacholine reduce the size of the spring. Our model is able to reproduce an isometric force measurement, where the smooth muscle is subjected to a titration of a contractile agent, with and without an in vitro exposure to formaldehyde. Thus, our new mechanistic approaches incorporates several well know features of the contractile system of the cells in a tissue level model. The model can also be used in different biological scales
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Efeito do condicionamento físico aeróbico de moderada intensidade na inflamação pulmonar alérgica crônica e na hiperresponsividade brônquica à metacolina em cobaias sensibilizadas / Effects of aerobic physical training with moderate intensity on chronic airway inflammation and bronchial hyperresponsivity to a methacoline in sensitized guinea pigOlivo, Clarice Rosa 17 August 2009 (has links)
O treinamento físico (TF) melhora a resposta imune de indivíduos saudáveis e traz benefícios para o paciente asmático, mas seu papel na resposta alérgica é desconhecido. Objetivo: Avaliar o papel do TF de moderada intensidade na inflamação pulmonar alérgica crônica. Métodos: 54 cobaias, divididas em 4 grupos: grupo controle (C) (não sensibilizados e não treinados), grupo OVA (sensibilizados à ovalbumina (OVA) e não treinados), grupo treinamento físico (TF) (não sensibilizados e submetidos a um TF), e grupo OVA+TF (sensibilizados à OVA e submetidos a um TF). A sensibilização à OVA teve duração de 8 semanas e o programa de TF de 6 semanas iniciando 15 dias após o início da sensibilização. Cada grupo foi dividido em 2 subgrupos. No primeiro foi avaliada a inflamação pulmonar e os níveis de óxido nítrico exalado (NOex) e no segundo, a hiperresponsividade brônquica à metacolina (Mch). Resultados: A sensibilização à OVA induziu a um aumento da densidade de eosinófilos e linfócitos, expressão de IL(interleucina)-4 e IL-13 e na espessura do músculo liso na via aerea assim como espessura do epitélio comparado aos animais não-sensibilizados (p<0,05). Os animais do grupo OVA+TF apresentaram uma redução da densidade de eosinófilos, linfócitos, IL-4 e IL-13 comparado com o grupo OVA (p<0,05). Nem a sensibilização crônica a OVA ou TF influenciaram a expressão das citocinas Th1 (IL-2 e IFN-) ou a expressão das citocinas regulatórias (IL-10 e IL-1-ra) e nos níveis de NOex. Os grupos que realizaram TF tiveram aumento na espessura do epitélio quando comparados com grupos não-treinados embora não há diferença entre os grupos na avaliação da hiperresponsividade brônquica. Conclusão: Nossos resultados sugerem que o TF reduz a inflamação alérgica sem modificar a hiperresponsividade brônquica e o remodelamento das vias aéreas / Background: Aerobic training (TF) has a positive effects on health subjects and bring benefits on the immune system of asthmatic patients. However, its role on allergic immune response remains poorly understood. Objective: To evaluate the effects of TF in chronic allergic inflammation. Methods: Fiftyfour animals, divided in 4 groups: non-trained and non-sensitized (C), nonsensitized and aerobic exercise (TF), ovalbumin sensitized and non-trained (OVA), and sensitized and aerobic exercise (OVA+TF). OVA or saline sensitization was performed during 8 weeks. TF was performed in a treadmill during 6 weeks beginning in the 3rd week of sensitization. Each group were divided in two groups. In the first one, it was evaluated airway inflammation and levels of exhaleted oxide nitric (NOex), on the second, airway hyperresponsiveness to a methacholine (Mch). Results: OVA sensitization induced an increase in the eosinophils and lymphocytes counting, expression of IL-4 and IL-13 and the amount of airway smooth muscle and epithelium thickness compared to non-sensitized animals (p<0.05). Sensitized animals submitted to TF presented a reduction in the eosinophil and lymphocyte counting, expression of IL-4 and IL-13 compared with OVA group (p<0.05) but not OVA-induced changes in airway remodeling (p>0.05). Neither OVA nor TF induced any difference in the expression of Th1 (IL-2 and IFN-) and regulatory cytokine (IL-10 and IL1-ra) and the levels of NOex. Trained groups presented an increase in epithelium thickness as compared to the nontrained groups however we did not find difference between groups on hyperresponsiveness avaliation. Conclusion: Our results suggest that TF reduces allergic airway inflammation without changes in bronchial hyperresponsiveness and airway remodeling
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Efeito do condicionamento físico aeróbico de moderada intensidade na inflamação pulmonar alérgica crônica e na hiperresponsividade brônquica à metacolina em cobaias sensibilizadas / Effects of aerobic physical training with moderate intensity on chronic airway inflammation and bronchial hyperresponsivity to a methacoline in sensitized guinea pigClarice Rosa Olivo 17 August 2009 (has links)
O treinamento físico (TF) melhora a resposta imune de indivíduos saudáveis e traz benefícios para o paciente asmático, mas seu papel na resposta alérgica é desconhecido. Objetivo: Avaliar o papel do TF de moderada intensidade na inflamação pulmonar alérgica crônica. Métodos: 54 cobaias, divididas em 4 grupos: grupo controle (C) (não sensibilizados e não treinados), grupo OVA (sensibilizados à ovalbumina (OVA) e não treinados), grupo treinamento físico (TF) (não sensibilizados e submetidos a um TF), e grupo OVA+TF (sensibilizados à OVA e submetidos a um TF). A sensibilização à OVA teve duração de 8 semanas e o programa de TF de 6 semanas iniciando 15 dias após o início da sensibilização. Cada grupo foi dividido em 2 subgrupos. No primeiro foi avaliada a inflamação pulmonar e os níveis de óxido nítrico exalado (NOex) e no segundo, a hiperresponsividade brônquica à metacolina (Mch). Resultados: A sensibilização à OVA induziu a um aumento da densidade de eosinófilos e linfócitos, expressão de IL(interleucina)-4 e IL-13 e na espessura do músculo liso na via aerea assim como espessura do epitélio comparado aos animais não-sensibilizados (p<0,05). Os animais do grupo OVA+TF apresentaram uma redução da densidade de eosinófilos, linfócitos, IL-4 e IL-13 comparado com o grupo OVA (p<0,05). Nem a sensibilização crônica a OVA ou TF influenciaram a expressão das citocinas Th1 (IL-2 e IFN-) ou a expressão das citocinas regulatórias (IL-10 e IL-1-ra) e nos níveis de NOex. Os grupos que realizaram TF tiveram aumento na espessura do epitélio quando comparados com grupos não-treinados embora não há diferença entre os grupos na avaliação da hiperresponsividade brônquica. Conclusão: Nossos resultados sugerem que o TF reduz a inflamação alérgica sem modificar a hiperresponsividade brônquica e o remodelamento das vias aéreas / Background: Aerobic training (TF) has a positive effects on health subjects and bring benefits on the immune system of asthmatic patients. However, its role on allergic immune response remains poorly understood. Objective: To evaluate the effects of TF in chronic allergic inflammation. Methods: Fiftyfour animals, divided in 4 groups: non-trained and non-sensitized (C), nonsensitized and aerobic exercise (TF), ovalbumin sensitized and non-trained (OVA), and sensitized and aerobic exercise (OVA+TF). OVA or saline sensitization was performed during 8 weeks. TF was performed in a treadmill during 6 weeks beginning in the 3rd week of sensitization. Each group were divided in two groups. In the first one, it was evaluated airway inflammation and levels of exhaleted oxide nitric (NOex), on the second, airway hyperresponsiveness to a methacholine (Mch). Results: OVA sensitization induced an increase in the eosinophils and lymphocytes counting, expression of IL-4 and IL-13 and the amount of airway smooth muscle and epithelium thickness compared to non-sensitized animals (p<0.05). Sensitized animals submitted to TF presented a reduction in the eosinophil and lymphocyte counting, expression of IL-4 and IL-13 compared with OVA group (p<0.05) but not OVA-induced changes in airway remodeling (p>0.05). Neither OVA nor TF induced any difference in the expression of Th1 (IL-2 and IFN-) and regulatory cytokine (IL-10 and IL1-ra) and the levels of NOex. Trained groups presented an increase in epithelium thickness as compared to the nontrained groups however we did not find difference between groups on hyperresponsiveness avaliation. Conclusion: Our results suggest that TF reduces allergic airway inflammation without changes in bronchial hyperresponsiveness and airway remodeling
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Efeito do inibidor de proteinase de origem vegetal EcTI, sobre a inflamação pulmonar alérgica crônica em camundongos Balb/c / Effect of proteinase inhibitor of plant origin EcTI in an experimental model of chronic allergic pulmonary inflammation in Balb/c miceRodrigues, Adriana Palmeira Dias 21 March 2016 (has links)
INTRODUÇÃO: A prevalência de asma tem crescido e a maioria dos pacientes com asma grave não obtém o controle total dos sintomas com as terapias disponíveis, fazendo-se necessária a busca por novas alternativas terapêuticas. Inibidores de proteinases têm sido estudados como tratamento de processos inflamatórios, dentre eles o Enterolobium contortisiliquum Tripsin Inhibitor (EcTI) OBJETIVO: Avaliar se o inibidor de proteinase EcTI modula a hiperresponsividade brônquica à metacolina, inflamação, remodelamento e estresse oxidativo nas vias aéreas e septos alveolares em um modelo experimental de inflamação pulmonar alérgica crônica. MÉTODOS: Vinte e quatro camundongos Balb/c machos, entre seis e sete semanas de vida, pesando em media 25 g foram divididos em quatro grupos: C (controle), OVA (sensibilizados com ovalbumina, 50 ug intraperironeal (i.p) nos dias 0 e 14 e desafiados nos dias 22, 24, 26, 28); C+EC (controle tratados com EcTI (2 mg/kg/i.p) nos dias 22 a 28); OVA+EC (sensibilizados e desafiados com ovalbumina e também tratados com EcTI (2 mg/kg -i.p) nos dias 22 a 28). No dia 29, foram realizadas realizadas: (i) hiperresponsividade à metacolina e obtidas as respostas máximas de resistência e elastância do sistema respiratório; (ii) análise histopatológica do pulmão para quantificação de eosinófilos, fibras colágenas e elásticas nas vias aéreas (VA) e nos septos alveolares (SA); e (iii) imunohistoquímica para quantificação de células positivas para IFN-y, IL-4, IL-5, IL-13, MMP-9, TIMP-1, TGF-beta, iNOS, NF-kB e fração de volume de isoprostano nas VA e nos SA. Uma semana após o dia 29 foi realizada a técnica de anafilaxia cutanea passiva(PCA) para quantificar IgE e IgG1. A significância foi considerada quando p < 0,05. RESULTADOS: Houve aumento de todos os parâmetros avaliados no grupo OVA em relação ao grupo controle (p < 0,05). Houve atenuação da resposta máxima de Rrs e Ers no grupo OVA+EC comparado as grupo OVA (p < 0,05). O tratamento com EcTI nos animais sensibilizados atenuou o número de eosinófilos, células positivas para IL-4, IL-5, IL-13,IFN-y, iNOS, MMP-9, TIMP-1, NF-kB e TGF-beta e fração de volume de isoprostano, fibras colágenas e elásticas nas vias aéreas e nos séptos alveolares quando comparado ao grupo OVA (p < 0,05).Houve reaçao de PCA nos animais sensibilizados com ovalbumina. CONCLUSÃO: EcTI atenuou a hiperresponsividade brônquica, a inflamação, o remodelamento e o estresse oxidativo nesse modelo experimental de inflamação pulmonar alérgica crônica. Embora sejam necessários mais estudos, esse inibidor pode ser considerado uma futura ferramenta farmacológica para o tratamento de asma / BACKGROUND: The number of cases of asthma has grown in recent decades. People who have severe asthma are likely to have more attacks and are at greater risk of a fatal attack, which propose to keep up global attention and keep approaching for advances in asthma care. Proteinase inhibitors of vegetable origin have been studied as a modulator of inflammatory responses and diseases. Among these inhibitors is Enterolobium contortisiliquum Trypsin Inhibitor (EcTI). AIMS: To evaluate the effects of EcTI in pulmonary mechanical, eosinophilic recruitment, inflammatory cytokines, remodeling of extracellular matrix and oxidative stressin an experimental model of chronic allergic pulmonary inflammation. METHODS: Twenty-four young adult male pathogen-free mice BALB/c (6-7 weeks old, 25-30g) were divided into 4 groups: C (control), OVA (sensitized with ovalbumin, 50 ug intraperitoneal (i.p), on days 0 and 14 and challenged with ova 1%, on days 22, 24, 26, 28); C+EC (control treated with EcTI- 2 mg/kg/i.p. from days 22 to 28); OVA+EC (sensitized and challenged with ovalbumin and treated with EcTI (2 mg/kg/i.p) from days 22 to 28). At day 29, we performed: (i) Bronchial hyperresponsiveness to methacholine and obtained the maximum response of resistance (Rrs) and elastance (Ers) of the respiratory system; (ii) lung histopathological analysis by morphometry to quantify eosinophils, collagen and elastic fibers volume fraction in airways; and (iii) immunohistochemistry to quantify IFN-y, IL-4, IL-5, IL-13, MMP-9, TIMP-1, TGF-, iNOS, NF-kB positive cells and isoprostane volume fraction in airways. One week after the day 29 we performed PCA technique to quantify IgE and IgG1 antibodies. Significance was considered at p < 0.05. RESULTS: The EcTI treatment in the ovalbumin-sensitized animals attenuated the maximal response of resistance and elastance of respiratory system after methacholine, the number of eosinophils, IL-4, IL-5, IL-13, IFN-y, NF-kB and iNOS-positive cells, isoprostane, elastic, collagen volume fraction, MMP-9, TIMP-1 and TGF-beta-positive cells compared to OVA group (p < 0.05). PCA was positive in sensitized animals. CONCLUSION: EcTI attenuates bronchial hyperresponsiveness, inflammation, remodeling and oxidative stress activation in this experimental asthma mice model. Although more studies are needed this inhibitor may be considered a future pharmacological tool for the treatment of asthma
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Efeito do inibidor de proteinase de origem vegetal EcTI, sobre a inflamação pulmonar alérgica crônica em camundongos Balb/c / Effect of proteinase inhibitor of plant origin EcTI in an experimental model of chronic allergic pulmonary inflammation in Balb/c miceAdriana Palmeira Dias Rodrigues 21 March 2016 (has links)
INTRODUÇÃO: A prevalência de asma tem crescido e a maioria dos pacientes com asma grave não obtém o controle total dos sintomas com as terapias disponíveis, fazendo-se necessária a busca por novas alternativas terapêuticas. Inibidores de proteinases têm sido estudados como tratamento de processos inflamatórios, dentre eles o Enterolobium contortisiliquum Tripsin Inhibitor (EcTI) OBJETIVO: Avaliar se o inibidor de proteinase EcTI modula a hiperresponsividade brônquica à metacolina, inflamação, remodelamento e estresse oxidativo nas vias aéreas e septos alveolares em um modelo experimental de inflamação pulmonar alérgica crônica. MÉTODOS: Vinte e quatro camundongos Balb/c machos, entre seis e sete semanas de vida, pesando em media 25 g foram divididos em quatro grupos: C (controle), OVA (sensibilizados com ovalbumina, 50 ug intraperironeal (i.p) nos dias 0 e 14 e desafiados nos dias 22, 24, 26, 28); C+EC (controle tratados com EcTI (2 mg/kg/i.p) nos dias 22 a 28); OVA+EC (sensibilizados e desafiados com ovalbumina e também tratados com EcTI (2 mg/kg -i.p) nos dias 22 a 28). No dia 29, foram realizadas realizadas: (i) hiperresponsividade à metacolina e obtidas as respostas máximas de resistência e elastância do sistema respiratório; (ii) análise histopatológica do pulmão para quantificação de eosinófilos, fibras colágenas e elásticas nas vias aéreas (VA) e nos septos alveolares (SA); e (iii) imunohistoquímica para quantificação de células positivas para IFN-y, IL-4, IL-5, IL-13, MMP-9, TIMP-1, TGF-beta, iNOS, NF-kB e fração de volume de isoprostano nas VA e nos SA. Uma semana após o dia 29 foi realizada a técnica de anafilaxia cutanea passiva(PCA) para quantificar IgE e IgG1. A significância foi considerada quando p < 0,05. RESULTADOS: Houve aumento de todos os parâmetros avaliados no grupo OVA em relação ao grupo controle (p < 0,05). Houve atenuação da resposta máxima de Rrs e Ers no grupo OVA+EC comparado as grupo OVA (p < 0,05). O tratamento com EcTI nos animais sensibilizados atenuou o número de eosinófilos, células positivas para IL-4, IL-5, IL-13,IFN-y, iNOS, MMP-9, TIMP-1, NF-kB e TGF-beta e fração de volume de isoprostano, fibras colágenas e elásticas nas vias aéreas e nos séptos alveolares quando comparado ao grupo OVA (p < 0,05).Houve reaçao de PCA nos animais sensibilizados com ovalbumina. CONCLUSÃO: EcTI atenuou a hiperresponsividade brônquica, a inflamação, o remodelamento e o estresse oxidativo nesse modelo experimental de inflamação pulmonar alérgica crônica. Embora sejam necessários mais estudos, esse inibidor pode ser considerado uma futura ferramenta farmacológica para o tratamento de asma / BACKGROUND: The number of cases of asthma has grown in recent decades. People who have severe asthma are likely to have more attacks and are at greater risk of a fatal attack, which propose to keep up global attention and keep approaching for advances in asthma care. Proteinase inhibitors of vegetable origin have been studied as a modulator of inflammatory responses and diseases. Among these inhibitors is Enterolobium contortisiliquum Trypsin Inhibitor (EcTI). AIMS: To evaluate the effects of EcTI in pulmonary mechanical, eosinophilic recruitment, inflammatory cytokines, remodeling of extracellular matrix and oxidative stressin an experimental model of chronic allergic pulmonary inflammation. METHODS: Twenty-four young adult male pathogen-free mice BALB/c (6-7 weeks old, 25-30g) were divided into 4 groups: C (control), OVA (sensitized with ovalbumin, 50 ug intraperitoneal (i.p), on days 0 and 14 and challenged with ova 1%, on days 22, 24, 26, 28); C+EC (control treated with EcTI- 2 mg/kg/i.p. from days 22 to 28); OVA+EC (sensitized and challenged with ovalbumin and treated with EcTI (2 mg/kg/i.p) from days 22 to 28). At day 29, we performed: (i) Bronchial hyperresponsiveness to methacholine and obtained the maximum response of resistance (Rrs) and elastance (Ers) of the respiratory system; (ii) lung histopathological analysis by morphometry to quantify eosinophils, collagen and elastic fibers volume fraction in airways; and (iii) immunohistochemistry to quantify IFN-y, IL-4, IL-5, IL-13, MMP-9, TIMP-1, TGF-, iNOS, NF-kB positive cells and isoprostane volume fraction in airways. One week after the day 29 we performed PCA technique to quantify IgE and IgG1 antibodies. Significance was considered at p < 0.05. RESULTS: The EcTI treatment in the ovalbumin-sensitized animals attenuated the maximal response of resistance and elastance of respiratory system after methacholine, the number of eosinophils, IL-4, IL-5, IL-13, IFN-y, NF-kB and iNOS-positive cells, isoprostane, elastic, collagen volume fraction, MMP-9, TIMP-1 and TGF-beta-positive cells compared to OVA group (p < 0.05). PCA was positive in sensitized animals. CONCLUSION: EcTI attenuates bronchial hyperresponsiveness, inflammation, remodeling and oxidative stress activation in this experimental asthma mice model. Although more studies are needed this inhibitor may be considered a future pharmacological tool for the treatment of asthma
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Investigations on the respiratory effects of ozone in the rodent / Cornelius Jacon LotrietLotriet, Cornelius Jacob January 2010 (has links)
Ozone, being an unstable molecule, is believed to be one of the strongest oxidant
agents known to man. Rapid growth in the application of ozone — both as
disinfectant and as form of alternative medicine — led to questions about the effects
of uncontrolled ozone exposure and inhalation, whether intentional or unintentional,
on the human body.
This study specifically focussed on examining, identifying and substantiating the
respiratory effect of acute exposure (10 min or less) to considerably higher ozone
concentrations than reported on before (19.5 ± 0.5 ppm). Respiratory tissue of
rodents (Duncan–Hartley guinea pigs of both sexes and Male Wistar rats) was
subjected to ozone by utilising three distinctly diverse models of ozone introduction:
(a) in vitro exposure, (b) in vivo exposure, and (c) ex vivo by employing an isolated
lung perfusion model which allows for real–time, breath–by–breath data acquisition of
ozone’s effect on respiratory mechanics. The effect of ozone on the isolated trachea
in the presence of various drugs with well–known effects, including methacholine,
isoproterenol and ascorbic acid was also examined.
The results found in this study identified two direct effects on the isolated trachea due
to ozone exposure: (1) a definite contraction of the isolated trachea immediately after
exposure to ozone, and (2) a clearly visible and significant hyper responsiveness of
the isolated trachea to irritants, e.g. methacholine. Although ozone has a negative
effect on the trachea, it was concluded that ozone has no adverse effect on
muscarinic acetylcholine receptors. An apparent EC50 value of ozone on the trachea
was established by two different methods as (2.77 ± 0.02) x 10–3 M and (2.10 ± 0.03)
x 10–3 M, respectively. Ozone furthermore displayed an attenuation of the beneficial pharmacological
response of –sympathomimetic drugs (i.e. isoproterenol), while isoproterenol itself
has a relaxing effect on the ozone–induced contraction of the isolated trachea.
Indomethacin pre–treatment of isolated tracheal tissue significantly (77%) reduced
the ozone–induced contraction of tracheal smooth muscle, suggesting that COXproducts
of arachidonic acid play a prominent role in the development of pulmonary
function decrements consequent to acute high–dose ozone exposure. Ascorbic acid
exhibited a meaningful prophylactic effect on ozone–induced contraction of both
isolated tracheal tissue and in the isolated lung perfusion model, emphasising the
major role antioxidants play in both the epithelium lining fluid (ELF) of the respiratory
system and in plasma throughout the body in protecting against the destructive
effects of ozone.
Surprisingly, pre–treatment with ascorbic acid did not prevent hyper responsiveness
of isolated tracheal preparations to methacholine after a 10 min ozone (19.5 ± 0.5
ppm) exposure. In the lung perfusion model, the presence of ascorbic acid in the
perfusion medium did, however, significantly reduce the magnitude and rate of
decline in lung compliance after ozone exposure (46% decline with ascorbic acid
versus 96% in the control study without ascorbic acid).
Examination of a lung perfusion model exposed to ozone (19.5 ± 0.5 ppm O3; 5
seconds) presented a significant decline in lung compliance (95.6% within 2 min),
tidal volume (70%) and maximum inspiratory flow (71.2%), with an ensuing reduction
in lung elasticity and severely hampered breathing pattern.
Microscopic examination after acute high–dose inhalation studies did not display any
significant cellular damage, oedema or inflammation after acute high–dose ozone
exposure. This suggests that significant cellular injury and inflammation is possibly
not the causative factor of early breathing difficulty experienced after acute high–dose
ozone inhalation, as these symptoms and particularly the result of inflammatory
precursors, is believed to probably only set in at a later stage.
Although the potential advantages of ozone in certain fields of medicine are not
disputed, ozone, depending on its concentration and cumulative dose, can be either therapeutic or toxic. Observations in this study emphasised that even short bursts of
high–dose ozone inhalation have deleterious effects on respiratory health and care
should be taken not to jump to conclusions regarding ozone’s medical application
without relevant scientific evidence. It must be stressed that high–dose inhalation of
ozone should be avoided at all cost – especially by those with existing airway
diseases. / Thesis (Ph.D. (Pharmacology))--North-West University, Potchefstroom Campus, 2011.
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Investigations on the respiratory effects of ozone in the rodent / Cornelius Jacon LotrietLotriet, Cornelius Jacob January 2010 (has links)
Ozone, being an unstable molecule, is believed to be one of the strongest oxidant
agents known to man. Rapid growth in the application of ozone — both as
disinfectant and as form of alternative medicine — led to questions about the effects
of uncontrolled ozone exposure and inhalation, whether intentional or unintentional,
on the human body.
This study specifically focussed on examining, identifying and substantiating the
respiratory effect of acute exposure (10 min or less) to considerably higher ozone
concentrations than reported on before (19.5 ± 0.5 ppm). Respiratory tissue of
rodents (Duncan–Hartley guinea pigs of both sexes and Male Wistar rats) was
subjected to ozone by utilising three distinctly diverse models of ozone introduction:
(a) in vitro exposure, (b) in vivo exposure, and (c) ex vivo by employing an isolated
lung perfusion model which allows for real–time, breath–by–breath data acquisition of
ozone’s effect on respiratory mechanics. The effect of ozone on the isolated trachea
in the presence of various drugs with well–known effects, including methacholine,
isoproterenol and ascorbic acid was also examined.
The results found in this study identified two direct effects on the isolated trachea due
to ozone exposure: (1) a definite contraction of the isolated trachea immediately after
exposure to ozone, and (2) a clearly visible and significant hyper responsiveness of
the isolated trachea to irritants, e.g. methacholine. Although ozone has a negative
effect on the trachea, it was concluded that ozone has no adverse effect on
muscarinic acetylcholine receptors. An apparent EC50 value of ozone on the trachea
was established by two different methods as (2.77 ± 0.02) x 10–3 M and (2.10 ± 0.03)
x 10–3 M, respectively. Ozone furthermore displayed an attenuation of the beneficial pharmacological
response of –sympathomimetic drugs (i.e. isoproterenol), while isoproterenol itself
has a relaxing effect on the ozone–induced contraction of the isolated trachea.
Indomethacin pre–treatment of isolated tracheal tissue significantly (77%) reduced
the ozone–induced contraction of tracheal smooth muscle, suggesting that COXproducts
of arachidonic acid play a prominent role in the development of pulmonary
function decrements consequent to acute high–dose ozone exposure. Ascorbic acid
exhibited a meaningful prophylactic effect on ozone–induced contraction of both
isolated tracheal tissue and in the isolated lung perfusion model, emphasising the
major role antioxidants play in both the epithelium lining fluid (ELF) of the respiratory
system and in plasma throughout the body in protecting against the destructive
effects of ozone.
Surprisingly, pre–treatment with ascorbic acid did not prevent hyper responsiveness
of isolated tracheal preparations to methacholine after a 10 min ozone (19.5 ± 0.5
ppm) exposure. In the lung perfusion model, the presence of ascorbic acid in the
perfusion medium did, however, significantly reduce the magnitude and rate of
decline in lung compliance after ozone exposure (46% decline with ascorbic acid
versus 96% in the control study without ascorbic acid).
Examination of a lung perfusion model exposed to ozone (19.5 ± 0.5 ppm O3; 5
seconds) presented a significant decline in lung compliance (95.6% within 2 min),
tidal volume (70%) and maximum inspiratory flow (71.2%), with an ensuing reduction
in lung elasticity and severely hampered breathing pattern.
Microscopic examination after acute high–dose inhalation studies did not display any
significant cellular damage, oedema or inflammation after acute high–dose ozone
exposure. This suggests that significant cellular injury and inflammation is possibly
not the causative factor of early breathing difficulty experienced after acute high–dose
ozone inhalation, as these symptoms and particularly the result of inflammatory
precursors, is believed to probably only set in at a later stage.
Although the potential advantages of ozone in certain fields of medicine are not
disputed, ozone, depending on its concentration and cumulative dose, can be either therapeutic or toxic. Observations in this study emphasised that even short bursts of
high–dose ozone inhalation have deleterious effects on respiratory health and care
should be taken not to jump to conclusions regarding ozone’s medical application
without relevant scientific evidence. It must be stressed that high–dose inhalation of
ozone should be avoided at all cost – especially by those with existing airway
diseases. / Thesis (Ph.D. (Pharmacology))--North-West University, Potchefstroom Campus, 2011.
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