Avaliação de respostas nociceptiva e neuroquímica induzidas por estimulação transcraniana por corrente contínua (ETCC) em ratos submetidos a um modelo de dor neuropática

Cioato, Stefania Giotti

January 2014

A dor neuropática (DN) é causada por uma lesão primária ou por uma disfunção no sistema nervoso periférico (SNP) ou central (SNC), sendo que os principais sintomas são a alodinia mecânica e a hiperalgesia a estímulos térmicos e mecânicos. A DN apresenta resposta analgésica insuficiente com terapeuticas farmacológicas clássicas, sendo um desafio para o tratamento clínico. Técnicas de neuromodulação central, como a estimulação transcraniana por corrente contínua (ETCC), representam um recurso promissor no manejo da dor, uma vez que promovem neuroplasticidade em vias envolvidas com o processo doloroso, sendo um método não-invasivo que pode ser combinado com outras terapias. Sendo assim, o objetivo deste estudo foi investigar os efeitos do tratamento repetido com ETCC na resposta hiperalgésica térmica e mecânica em modelo experimental de DN. Adicionalmente, foram avaliados os níveis de IL-1β, IL-10, TNF-α e NGF em estruturas do SNC destes animais. Todos os procedimentos foram aprovado pela Comissão de Ética no Uso de Animais (CEUA/HCPA:120512). Oitenta e quatro ratos machos Wistar foram divididos em 7 grupos: controle, dor neuropática, dor neuropática+ETCC, dor neuropática+sham ETCC, sham dor neuropática, sham dor neuropática+ETCC e sham dor neuropática+sham ETCC. O modelo de DN foi induzido por meio de ligura parcial do nervo isquiático na pata esquerda. O sham do modelo de DN seguiu o mesmo protocolo, com simulação da ligadura parcial do nervo isquiático e o grupo controle não sofreu nenhuma manipulação. O tratamento com ETCC consistiu em 20minutos/dia/8 dias, com intensidade de 0,5mA. Para o sham do tratamento, os eletrodos foram apenas fixados à cabeça do animal durante 20 minutos/dia/8 dias, sem nenhuma estimulação. A hiperalgesia térmica e mecânica foi avaliada por meio dos testes da Placa Quente e de Von Frey, respectivamente, no tempo basal, 7 e 14 dias após a cirurgia e imediatamente, 24 horas e 7 dias após o final do tratamento. Os níveis de IL-1β, IL-10, TNF-α e NGF no cortex cerebral, medula espinhal e tronco cerebral foram determinados por ELISA 48 horas e 7 dias após o final do tratamento. A análise estatística para os testes nociceptivos foi realizada através da Generalized Estimation Equation (GEE)/Bonferroni e para as análises bioquímicas por ANOVA de uma via (IL-1β, IL-10, TNF-α ) e ANOVA de três vias (NGF). Os dados estão expressos como media+erro padrão da média, sendo considerado significativo p<0.05. Nossos resultados demonstraram que a DN altera os níveis de IL-1β, IL-10, TNF-α e NGF no SNC em curto e longo prazo. Além disso, a ETCC reduz a resposta nociceptiva a curto e longo prazo e na modulação dos níveis de citocinas no sistema nervoso central neste modelo. Evidencia-se a importância do papel do sistema imune central nos processos de continuidade da dor neuropática, que pode estar envolvido com as alterações neuroplásticas maladaptativas características dessa patologia. / Neuropathic pain (NP) is caused by a primary insult or dysfunction in the central or peripheral nervous system and its prevalence depends on the type of trauma and related dysfunction. The main symptoms are mechanical allodynia and hyperalgesia to both mechanical and thermal stimuli. NP often shows insufficient response to classic analgesics and remains a challenge to medical treatment and scientific research; and the search for new therapies for this pathology is of fundamental important. Central neuromodulation techniques, such as transcranial direct current stimulation (tDCS), represent a promising resource to pain management since they promote neuroplasticity in the central system of pain. Moreover, tDCS has the advantages of being a noninvasive technique and can be combined with other interventions. The aim of this study was investigated the effects of tDCS in the thermal and mechanical hyperalgesia induced by chronic constriction injury (CCI) of sciatic nerve and measured its effect on the neurochemical markers (IL-1β, IL-10, TNF-α, and NGF levels) on central nervous system structures. All experiments and procedures were approved by the Institutional Animal Care and Use Committee (GPPG-HCPA No.120512) and performed in accordance with the Guide for the Care and Use of Laboratory Animals 8th ed. The CCI of sciatic nerve was used for the induction of NP. For sham surgery, the sciatic nerve was exposed similarly, but it was not ligated. The control group did not undergo surgical procedure. After the establishment of NP, the rats of treated groups were subjected to a 20 minutes session of anodal tDCS, every afternoon for eight days, under a direct constant current of 0.5 mA intensity. The thermal and mechanical hyperalgesia was assessed by Hot plate and Von Frey test, respectively, and evaluated on baseline, 7 and 14 days after surgery; immediately, 24 hours and 7 days after treatment. The IL-1β, IL-10, TNF-α and NGF levels on cortex, spinal cord and brainstem were determined by sandwich-ELISA at 48 hours and 7 days after the end of treatment. Data were expressed as the mean±standard error of the mean (S.E.M). Generalized Estimating Equation (GEE) followed by Bonferroni was performed to compare all groups in different times of nociceptive tests and to biochemical data the one-way ANOVA was used to compare the IL-1β, IL-10, TNF-α and three-way ANOVA was used to compare the NGF levels. P-values less than 0.05 were considered significant. SPSS 19.0 for Windows was used for statistical analysis. In summary, we showed that anodal tDCS is effective to relieve NP and modulate cytokine in CCI rat model, and its effect is observed at long-term. In addition, the CCI model induced increased NGF levels in cerebral cortex and spinal cord at long-lasting time, evidencing the important feature of this neurotrophin in neuropathic pain condition. Additionally, we observed an important role of the central immune system in the neuropathic process, which can be involved with the maladaptative neuroplastic changes.

Dor

Estimulação magnética transcraniana

Fator de crescimento neural

Citocinas

Neuropathic pain

Transcranial direct current stimulation

IL-1β

IL-10

TNF-α

NFG

Rats

Efeito da Quimiocina CXCL10 na infecÃÃo por Leishmania infantum/chagasi em camundongos BALB/C / Effect of chemokine CXCL10 in Leishmania infantum chagasi infection in BALB/c mice.

Webertty Mayk EufrÃsio de Figueiredo

17 February 2012

A leishmaniose visceral causada por Leishmania infantum chagasi à caracterizada pela perda da habilidade do hospedeiro gerar uma resposta imunolÃgica eficaz. Neste estudo, foi investigado o papel da quimiocina CXCL10 no controle da infecÃÃo por L. infantum chagasi in vivo. Grupos de camundongos BALB/c foram tratados ou nÃo com CXCL10 (5 &#956;g/kg) com 1, 3 e 7 dias de infecÃÃo e apÃs 1, 7 e 23 dias do tratamento, alguns parÃmetros foram avaliados: a carga parasitÃria, os nÃveis de IFN-&#61543;, IL-4, TGF-&#946; e IL-10, e as alteraÃÃes histopatolÃgicas no fÃgado. ApÃs 23 dias de tratamento, CXCL10 induziu, no baÃo, uma reduÃÃo expressiva no nÃmero de parasitos, quando comparado ao grupo controle. No fÃgado, a carga parasitÃria mostrou uma queda no grupo tratado, entre o 7 e 23 dia apÃs o tratamento. Entretanto, o efeito leishmanicida de CXCL10, neste trabalho, nÃo parece ser mediado por NO, uma vez que nÃo houve diferenÃa na produÃÃo de NO entre os grupos. IFN-&#947; foi induzida de maneira mais significativa no grupo tratado do que nos controles, e atingiu sua produÃÃo mÃxima (100 pg/mL) no 23 dia apÃs o tratamento, correlacionando-se com a queda da carga parasitÃria nos ÃrgÃos-alvo. IL-4 foi produzida em baixas concentraÃÃes, em ambos os grupos, embora os animais tratados com CXCL10 tenham mostrado nÃveis mais elevados do que os controles. Em relaÃÃo Ãs citocinas antiinflamatÃrias, apÃs 23 dias do tratamento, os nÃveis de IL-10 nos animais tratados foram menores do que os do controle. A produÃÃo de TGF-&#946; apÃs 7 dias do tratamento foi 2 vezes menor no grupo tratado quando comparado ao controle, e apÃs 23 dias do tratamento, essa citocina continuou com nÃveis mais baixos do que aqueles observados no controle. Na anÃlise histopatolÃgica do fÃgado apÃs o 1 dia do tratamento, foram encontrados, em ambos os grupos, mais granulomas imaturos (GI), do que infiltrados nÃo granulomatosos (NG) e alguns poucos granulomas maduros (GM) apenas no grupo tratado. ApÃs 7 dias do tratamento, a quantidade de infiltrados NG estava menor e os GI ainda foram os mais encontrados, em ambos os grupos, alÃm disso, foi observado um pequeno aumento de GM no grupo tratado. Em resumo, diante dos resultados encontrados, à possÃvel sugerir um importante papel leishmanicida de CXCL10 em camundongos BALB/c infectados por L. infantum chagasi, que parece ser mediado por uma expressiva produÃÃo de IFN-g e supressÃo das citocinas imunorreguladoras, IL-10 e TGF-&#946;, abrindo a hipÃtese se isto nÃo estaria associado a uma diminuiÃÃo na frequÃncia de cÃlulas T regulatÃrias, induzida por CXCL10, nesses animais. / Visceral leishmaniasis caused by Leishmania infantum chagasi is characterized by the loss of the ability of host to generate an effective immune response. In this study it was investigated the role of CXCL10 chemokine in controlling L. infantum chagasi infection in vivo. Groups of BALB/c mice were treated or not with recombinant CXCL10 chemokine (5 &#956;g/kg) with 1, 3 and 7 days of infection and after 1, 7 and 23 days of treatment, some parameters were evaluated: parasite load, levels of IFN-g, IL-4, TGF-&#946; and IL-10, and the histopathological alterations in the liver. After 23 days of treatment, CXCL10 induced in the spleen a significant reduction on the number of parasites as compared to control group. In the liver, parasite load decreased in treated group between the 7th and 23th day post treatment. However, the antileishmanial effect of CXCL10, in this work, does not seem to be mediated by NO, since there was no difference in the NO production among the groups. IFN-&#947; was induced most significantly in treated group than in controls, and reached its maximum production (100 pg/mL) on day 23 after treatment, correlating with the reduction in parasite burden in target organs. IL-4 was produced in low doses, in both groups, although treated animals had shown higher levels than control group. Regarding to anti-inflammatory cytokines, after the 23th day of treatment, IL-10 levels in treated animals were smaller than in control group. Production of TGF-&#946; after 7 days of treatment was 2 times lower in treated group when compared to control, and after the 23th day of treatment, this cytokine remained with lower levels than those observed in control. In the histopathological analysis of the liver after the 1st day of treatment, were found in both groups more immature granulomas (GI) than non-granulomatous infiltrate (NG), and some few mature granulomas (GM) were only observed in treated group. After 7 days of treatment, the amount of NG infiltrates was lower, and GI were still the most frequent in both groups, besides a slight increase of GM was observed in treated group. In summary, at the light of the found results, it is possible to suggest an important leishmanicidal role to CXCL10 in BALB/c mice infected by L. infantum chagasi, which seems to be mediated by a significant IFN-g production, and suppression of immunoregulatory cytokines, IL-10 and TGF-&#946;, opening the hypothesis that this would be associated to a decrease in the frequency of regulatory T cells induced by CXCL10 in these animals.

L. infantum chagasi

IFN-&#61543;

L. infantum chagasi

CXCL10

IFN-&#61543

IL-4

IL-10

TGF-&#946

granuloma

DOENCAS INFECCIOSAS E PARASITARIAS

Associação entre polimorfismos de genes do sistema imunológico (IL-10, TNF-a) e a infecção por HPV nos diferentes graus de lesões cervicais

Igansi, Cristine Nascente

January 2009

Estudos epidemiológicos e moleculares têm sugerido que o HPV é o principal fator de risco para o desenvolvimento de lesões malignas na cérvice uterina. E, sendo o número de infecções extremamente maior do que o número de casos de câncer cervical, este fato nos leva à investigação de outros fatores associados, como por exemplo, a predisposição imunológica do hospedeiro. Este estudo tem como objetivo avaliar a associação dos polimorfismos (-1082A/G) e (-308 A/G), localizados nos genes da IL-10 e TNF-α, respectivamente, com a infecção genital pelo Papilomavírus Humano (HPV), incluindo os tipos oncogênicos HPV-16, 18 e 31, visto que, estas citocinas são moléculas importantes na resposta imune contra infecções virais. Trata-se de um estudo de casos e controles. O grupo controle foi composto por 211 mulheres, que apresentavam resultado negativo para infecção genital por HPV, identificada através da técnica de Reação em Cadeia da Polimerase (PCR) e exame citopatológico sem alterações. Já os casos, corresponderam a 84 mulheres com infecção genital por HPV e resultado anatomopatológico alterado. A técnica de amplificação refratária de mutações (ARMS-PCR) foi utilizada para a identificação dos polimorfismos. Regressão logística múltipla foi utilizada para verificar a associação das variáveis estudadas com o desfecho (infecção genital pelo HPV).O cálculo de Equilíbrio de Hardy-Weinberg foi utilizado para verificar se as freqüências alélicas e gentotípicas observadas estão de acordo com as esperadas na população em estudo. Para os resultados de IL-10, a freqüência genotípica observada nos casos foi de 11,9% (AA), 28,6% (AG) e 59,5% (GG); a freqüência alélica foi de 26,0% para A e 74,0% para G. No grupo controle, a freqüência genotípica encontrada foi 22,8% (AA), 48,8% (AG) e 28,4% (GG); a freqüência alélica foi de 47,0% para A e 53,0% para G. Houve diferença significativa entre os grupos estudados, tanto para a freqüência alélica quanto para a genotípica (p<0,0001). Entre as mulheres com infecção, encontramos associação das lesões intraepiteliais escamosas de baixo grau (LGSIL) com o genótipo GG (p=0,02). As variáveis idade (RC=4,70; IC95%: 2,61-8,40), co-infecção por HIV (RC=11,21; IC95%:1,002-125,33) e o genótipo GG (RC=4,22; IC95%: 1,84-9,61) permaneceram independentemente associados ao desfecho (infecção genital pelo HPV). Para TNF-α, a homozigosidade do alelo G (genótipo GG) foi encontrada em maior freqüência nos casos (36,9%), seguido por 35,7% do genótipo AA e 27,4% do genótipo AG. Houve diferença significativa entre os grupos estudados, tanto para a freqüência alélica (p<0,0002) quanto para a genotípica: AA (p=0,03), AG e GG (p<0,0001). Analisando a associação com lesões cervicais e tipos oncogênicos, encontramos associação entre o genótipo GG e LGSIL (p<0,01). O genótipo GG está associado ao tipo oncogênico HPV-16 (p<0,05), e à co-infecção pelo vírus HIV (p<0,001). As variáveis idade (RC=3,46; IC95%: 1,89-6,33), os genótipos AG (RC=9,21; IC95%: 4,29-19,75) e AA (RC=2,73; IC95%: 1,25-6,00) permaneceram independentemente associados ao desfecho (infecção genital pelo HPV). Com estes resultados, é possível sugerir que a predisposição determinada geneticamente para a produção de altos níveis de IL-10 e TNF-α parece estar associada à infecção genital pelo HPV, mostrando a importância da resposta imunológica do hospedeiro no processo de infecção e na progressão das lesões cervicais geradas pelo Papilomavírus Humano. / Molecular and epidemiological studies have suggested that HPV is the most important risk factor for the development of malignant lesions in the uterine cervix. The fact that the number of HPV infections is extremely greater than the number of cervical cancer cases leads us to the investigation of other risk factors, such as the predisposition of the host immune. The present study aimed to evaluate the influence of genetic polymorphisms (-1082A/G) and (-308A/G), located in the genes of IL-10 and TNF-α, respectively, with the genital HPV infection, including oncogenic HPV-16, 18 and 31, since these cytokines are important molecules in the immune response against viral infections. This is a case-control study. The control group was composed by 211 women, who have tested negative for HPV genital infection by the Polymerase Chain Reaction (PCR) technique, and who had normal cytologic results. Cases were 84 women with HPV genital infection and abnormal anatomopathological results. The technique of amplification refractory mutation system (ARMS-PCR) was used to identify the polymorphisms. Multiple logistic regression was used to verify the association between the study factors and the outcome (genital infection by HPV). The Hardy-Weinberg equilibrium was used to verify whether the observed allelic and genotypic frequencies were according with the expected in the studied population. For the results of IL-10, the genotypic frequencies observed in the group of women with infection was 11.9% (AA), 28,6% (AG) and 59.5% (GG), the allelic frequency was 26.0% for 74.0% for A and G. In the control group, the frequency was found genotypical 22.8% (AA), 48.8% (AG) and 28.4% (GG), the allelic frequency was 47.0% to 53.0% for A and G. There were significant differences between groups, both for the allelic frequency as for the genotypic (p<0.0001). Among women with infection, we found association of injuries LGSIL with the GG genotype (p=0021). The variables age (OR=4.70; 95%IC: 2.61-8.40), HIV co-infection (OR=11.21; 95%IC: 1.002-125,33), and genotype GG (OR=4.22; 95%IC: 1.84-9.61) remained independently associated to the outcome (genital HPV infection). For TNF-α analysis, the genotypic frequencies observed in the group of patients was 22.0% (AA), 69.0% (AG) and 8.0% (GG), the allelic frequency was 57.0% and 43.0% for A to G. In the control group, the frequency genotype was found 35.0% (AA), 27.0% (AG) and 36.0% (GG), the allelic frequency was 49.0% for A and 51.0% for G. There were significant differences between groups, both for the allelic frequency (p<0.0002) and to the genotypic: AA (p=0.03), AG e GG (p<0.0001). Analysing the association with cervical lesions and with high-risk type, there was found a significant association, between the genotype GG and LGSIL (p<0.01). The genotype GG is associated with the HPV-16 infection (p<0.05) and with the HIV virus co-infection (p<0001). The variables age (OR=3.46; 95%IC: 1.89-6.33), genotypes AG (OR=9.21; 95%IC: 4.29-19.75) and AA (OR=2.73; 95%IC: 1.25- 6.00) remained independently associated to the outcome (genital HPV infection). The results suggest that the genetically determined predisposition to produce high levels of IL- 10 and TNF-α may be related to the genital HPV infection showing the importance of the host immune response in the progression of cervical lesions caused by the Human Papillomavirus.

Papillomavirus humano

Polimorfismo genético

Neoplasias do colo do útero

Infecções por papillomavirus

Lesões

Fator de necrose tumoral alfa

Interleucina-10

HPV

Polymorphism

IL-10

TNF-α

Cervical cancer

Avaliação de respostas nociceptiva e neuroquímica induzidas por estimulação transcraniana por corrente contínua (ETCC) em ratos submetidos a um modelo de dor neuropática

Cioato, Stefania Giotti

January 2014

A dor neuropática (DN) é causada por uma lesão primária ou por uma disfunção no sistema nervoso periférico (SNP) ou central (SNC), sendo que os principais sintomas são a alodinia mecânica e a hiperalgesia a estímulos térmicos e mecânicos. A DN apresenta resposta analgésica insuficiente com terapeuticas farmacológicas clássicas, sendo um desafio para o tratamento clínico. Técnicas de neuromodulação central, como a estimulação transcraniana por corrente contínua (ETCC), representam um recurso promissor no manejo da dor, uma vez que promovem neuroplasticidade em vias envolvidas com o processo doloroso, sendo um método não-invasivo que pode ser combinado com outras terapias. Sendo assim, o objetivo deste estudo foi investigar os efeitos do tratamento repetido com ETCC na resposta hiperalgésica térmica e mecânica em modelo experimental de DN. Adicionalmente, foram avaliados os níveis de IL-1β, IL-10, TNF-α e NGF em estruturas do SNC destes animais. Todos os procedimentos foram aprovado pela Comissão de Ética no Uso de Animais (CEUA/HCPA:120512). Oitenta e quatro ratos machos Wistar foram divididos em 7 grupos: controle, dor neuropática, dor neuropática+ETCC, dor neuropática+sham ETCC, sham dor neuropática, sham dor neuropática+ETCC e sham dor neuropática+sham ETCC. O modelo de DN foi induzido por meio de ligura parcial do nervo isquiático na pata esquerda. O sham do modelo de DN seguiu o mesmo protocolo, com simulação da ligadura parcial do nervo isquiático e o grupo controle não sofreu nenhuma manipulação. O tratamento com ETCC consistiu em 20minutos/dia/8 dias, com intensidade de 0,5mA. Para o sham do tratamento, os eletrodos foram apenas fixados à cabeça do animal durante 20 minutos/dia/8 dias, sem nenhuma estimulação. A hiperalgesia térmica e mecânica foi avaliada por meio dos testes da Placa Quente e de Von Frey, respectivamente, no tempo basal, 7 e 14 dias após a cirurgia e imediatamente, 24 horas e 7 dias após o final do tratamento. Os níveis de IL-1β, IL-10, TNF-α e NGF no cortex cerebral, medula espinhal e tronco cerebral foram determinados por ELISA 48 horas e 7 dias após o final do tratamento. A análise estatística para os testes nociceptivos foi realizada através da Generalized Estimation Equation (GEE)/Bonferroni e para as análises bioquímicas por ANOVA de uma via (IL-1β, IL-10, TNF-α ) e ANOVA de três vias (NGF). Os dados estão expressos como media+erro padrão da média, sendo considerado significativo p<0.05. Nossos resultados demonstraram que a DN altera os níveis de IL-1β, IL-10, TNF-α e NGF no SNC em curto e longo prazo. Além disso, a ETCC reduz a resposta nociceptiva a curto e longo prazo e na modulação dos níveis de citocinas no sistema nervoso central neste modelo. Evidencia-se a importância do papel do sistema imune central nos processos de continuidade da dor neuropática, que pode estar envolvido com as alterações neuroplásticas maladaptativas características dessa patologia. / Neuropathic pain (NP) is caused by a primary insult or dysfunction in the central or peripheral nervous system and its prevalence depends on the type of trauma and related dysfunction. The main symptoms are mechanical allodynia and hyperalgesia to both mechanical and thermal stimuli. NP often shows insufficient response to classic analgesics and remains a challenge to medical treatment and scientific research; and the search for new therapies for this pathology is of fundamental important. Central neuromodulation techniques, such as transcranial direct current stimulation (tDCS), represent a promising resource to pain management since they promote neuroplasticity in the central system of pain. Moreover, tDCS has the advantages of being a noninvasive technique and can be combined with other interventions. The aim of this study was investigated the effects of tDCS in the thermal and mechanical hyperalgesia induced by chronic constriction injury (CCI) of sciatic nerve and measured its effect on the neurochemical markers (IL-1β, IL-10, TNF-α, and NGF levels) on central nervous system structures. All experiments and procedures were approved by the Institutional Animal Care and Use Committee (GPPG-HCPA No.120512) and performed in accordance with the Guide for the Care and Use of Laboratory Animals 8th ed. The CCI of sciatic nerve was used for the induction of NP. For sham surgery, the sciatic nerve was exposed similarly, but it was not ligated. The control group did not undergo surgical procedure. After the establishment of NP, the rats of treated groups were subjected to a 20 minutes session of anodal tDCS, every afternoon for eight days, under a direct constant current of 0.5 mA intensity. The thermal and mechanical hyperalgesia was assessed by Hot plate and Von Frey test, respectively, and evaluated on baseline, 7 and 14 days after surgery; immediately, 24 hours and 7 days after treatment. The IL-1β, IL-10, TNF-α and NGF levels on cortex, spinal cord and brainstem were determined by sandwich-ELISA at 48 hours and 7 days after the end of treatment. Data were expressed as the mean±standard error of the mean (S.E.M). Generalized Estimating Equation (GEE) followed by Bonferroni was performed to compare all groups in different times of nociceptive tests and to biochemical data the one-way ANOVA was used to compare the IL-1β, IL-10, TNF-α and three-way ANOVA was used to compare the NGF levels. P-values less than 0.05 were considered significant. SPSS 19.0 for Windows was used for statistical analysis. In summary, we showed that anodal tDCS is effective to relieve NP and modulate cytokine in CCI rat model, and its effect is observed at long-term. In addition, the CCI model induced increased NGF levels in cerebral cortex and spinal cord at long-lasting time, evidencing the important feature of this neurotrophin in neuropathic pain condition. Additionally, we observed an important role of the central immune system in the neuropathic process, which can be involved with the maladaptative neuroplastic changes.

Dor

Estimulação magnética transcraniana

Fator de crescimento neural

Citocinas

Neuropathic pain

Transcranial direct current stimulation

IL-1β

IL-10

TNF-α

NFG

Rats

Rozdílná schopnost in vitro vypěstovaných dendritických buněk dětí zdravých a alergických matek stimulovat imunitní odpověď / Different capacity of in vitro generated monocyte-derived dendritic cells of newborns of healthy and allergic mothers to prime immune responses

Súkeníková, Lenka

January 2017

(EN) Reduced microbial stimulation of an immature neonatal immune system can lead to a poor balance adjustment of immune responses, thus contributing to the development of allergic diseases, whose incidence continues to rise. One of the promising precautionary measures seems to be an early preventive administration of probiotic bacteria to pregnant or nursing mothers, or to newborns. Previous works have described a beneficial effect of Escherichia coli O83:K24:H31 (E. coli O83) in the prevention of allergic diseases. In order to contribute to the clarification of E. coli O83 effects on the neonatal immune system, its immune- modulating properties were tested in vitro on umbilical cord blood cells. The ability of E. coli O83 to support the maturation of in vitro-derived dendritic cells from cord blood precursors (moDCs) of the children of healthy (children with a relatively low risk of allergy) and allergic (children at a relatively high risk of developing allergies) mothers was tracked by flow cytometry, qPCR and ELISA. Probiotic bacteria-stimulated moDCs were subsequently cultured with autologous naive CD4+ T lymphocytes and immune response polarization was also characterised by flow cytometry, qPCR, and ELISA. It was evident from the results that E. coli O83 promoted moDCs maturation. The presence of...

The immune-modulating activity of Artemisia afra

Kriel, Yusra

January 2010

Magister Scientiae - MSc / This study shows that herbs can be effectively screened for potiential bio-activity using in vitro methods. Further studies will be needed to better explore Artemisia afra&rsquo;s effect on immunoregulation, particularly long term effects of the herb on the immune system and its effect on other disease states. / South Africa

Artemisia afra

Cell-mediated immunity

Cytotoxicity

ELISA

IFN- γ

IL-6

IL-10

Inflammatory activity

Humoral immunity

Human whole blood cultures

LDH assay

Study of transcription factors involved in the upregulation of IL-10 expression in human CD4 T cells costimulated by T cell receptor and type I interferon / Etude chez l'homme des facteurs de transcriptions impliqués dans l'expression de l'IL-10 par les cellules T CD4 co-stimulées par le TCR et l'interferon de type I

Govender, Umeshree

22 March 2016

L'objectif de cette thèse a été d'étudier le mécanisme de la coopération entre les voies de signalisation du TCR et de l'interféron de type I qui est responsable de l'augmentation d'expression de la cytokine anti-inflammatoire IL-10 dans les lymphocytes T CD45RA+CD4+ humains. En utilisant une approche transcriptomique et d'interférence d'ARNm, j'ai observé que les voies IFN et TCR contrôlent différemment l'expression des STATs et que les BATFs sont induits par l'IFN et augmentés par la costimulation TCR/IFN. STAT3 a été identifié comme régulateur majeur de l'IL-10 et il est recruté à proximité d'un site de liaison pour BATF au locus IL-10. Sur la base d'essais de co-silencing des trois BATFs, nous avons proposé que les BATFs contrôlent l'amplitude de la réponse IFN en agissant comme facteurs de transcription " pionniers ". D'autres résultats obtenus par une étude transcriptomique d'environ 200 gènes, montrent des contributions uniques et combinées des voies TCR et de l'IFN dans le programme d'expression de gènes des lymphocytes CD45RA+CD4+ activés et indiquent que d'autres facteurs de transcription pourraient réguler l'IL-10. Cette étude est susceptible d'apporter une connaissance plus large de mécanismes impliqués dans la régulation croisée entre les voies TCR et IFN. / In CD4 T cells several transcription factors (TFs) regulate expression of the anti-inflammatory cytokine IL-10. I investigated how type I interferon (IFN) cytokines and T cell receptor (TCR) pathways cooperate toward early upregulation of IL-10 in human CD45RA+ CD4+ T cells. I interrogated the role of the STAT and BATF family by transciptomics and RNAi-mediated gene-silencing. IFN and TCR induced STAT2 and STAT3 expression, respectively, while the BATFs were induced early by IFN and further enhanced by TCR/IFN together. STAT3 was the major regulator of TCR- and TCR/IFN-mediated IL-10 while STAT2 contributed to the latter. STAT3 was recruited adjacent to a BATF-binding site at the IL-10 locus early in response to TCR/IFN. Co-silencing of the three BATFs led to a marked decrease in TCR- and TCR/IFN-mediated IL-10. We propose that the BATFs control the magnitude of the IFN response as pioneer factors. Additional results of transcriptional profiling of ± 200 genes, including TFs downstream of TCR and IFN and TFs involved in IL-10 regulation, revealed that TCR and IFN provide unique and combined contributions to the early CD45RA+CD4+ T cell gene activation program and identified other potential TFs involved in TCR/IFN-mediated IL-10 transcription. This study may provide broad mechanistic bases for crosstalk between the TCR- and IFN-pathways.

Interféron de type I

Il-10

Lymphocyte T CD4

Facteurs de transcription

Régulation de gène

Cytokines

Interleukin 10

Type I interferons

Transcription factors

571.96

An in vitro study on the immunotoxicity of sewage effluents discharged into the Eerste River-Kuils river water catchment system

Magcwebeba, Tandeka

January 2008

Magister Scientiae - MSc / "The aim of the study was to use in vitro human whole blood cultures to screen the water samples collected from the Eerste/Plankenbrug river system for cytotoxicity and inflammatory activity and for the first time investigate the impact on the cell- mediated and humoral immune pathways. Water samples were collected fronm the sites during the dry summer season and rainy winter season. Blood was collected from the healthy male volunteers and diluted with RPMI 1640. For cytotoxicity and inflammatory activity 2.5ul of blood for 18-20 hrs at 37 C... This study shows that waster from the Plankenbrug River is heavily polluted by contaminants from both the agricultural area and informal settlement of Kayamandi. These contaminants can be potentially immunotoxic during the summer season and they can result in inflammatory diarrheal disease and immunosuppression in exposed individuals..."

Cell-mediated immunity

Cytotoxicity

ELISA

IL-6

IFN-γ

IL-10

Inflammatory activity

Humoral immunity

Human whole blood cultures

LDH assay

Molecular characterization of E.histolytica strains and the impact of host genetics on amoebic infection in Limpopo and Gauteng Province, South Africa

Ngobeni, Renay

16 February 2016

MSc (Microbiology) / Department of Microbiology

Entamoeba histolytica

SREHP

Chitinase and IL-10

Genetic polymorphisms

571.980968257

Amebiasis -- South Africa -- Limpopo

Die Rolle der Interleukin-10 Gabe auf die posttraumatische systemische Inflammation und Organdysfunktion am Mausmodell

Schreiber, Helen

24 April 2012

Bei IL-10 handelt es sich um ein antiinflammatorisches Zytokin, dessen immunmodulatorische Effekte bereits in zahlreichen Studien aufgezeigt werden konnten. Ziel dieser Studie war, die Unterschiede in der systemischen Inflammation und Organdysfunktion an Mäusen zu untersuchen, die nach Induktion eines hämorrhagischen Schocks, entweder inhalativ oder systemisch, mit IL-10 behandelt wurden. Männliche C57/BL6 Mäuse (6 Tiere pro Gruppe) wurden für 1.5 Stunden blutdruckkontrolliert in einen hämorrhagischen Schock versetzt. Nach anschließender Volumensubstitution wurde ihnen inhalativ oder intraarteriell rekombiniertes Maus - IL-10 verabreicht. Nach einer Gesamtversuchsdauer von 6 - bzw. 24 Stunden erfolgte die Tötung der Tiere. Die Ergebnisse der Studie zeigen, dass die lokale und systemische Verabreichung von IL-10 das Zytokinprofil der systemischen Inflammationsantwort unterschiedlich beeinflusst. Die Lunge kann durch inhalative Gabe von IL-10 geschützt werden, ohne die systemische Inflammationsantwort zu beeinflussen.

info:eu-repo/classification/ddc/636.089

ddc:636.089