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  • About
  • 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.
291

Genetische Marker bei hausärztlichen Patienten mit oraler Antikoagulation / Genetic markers in patients taking phenprocoumon

Hess, Stephan 02 June 2004 (has links)
No description available.
292

Relação entre os polimorfismos da paraoxonase 1 e do citocromo P450 em pacientes com imunodeficiência comum variável em uso de medicamentos ou exposição a poluentes ambientais / Relation between paraoxonase 1 and cytochrome P450 gene polymorphisms and patients with common variable immunodeficiency and in use of medication or exposed to enviromental pollutants

Bruno Carnevale Sini 05 December 2017 (has links)
INTRODUÇÃO. A Imunodeficiencia comum variável (ICV) é uma doença heterogênea caracterizada pela redução dos niveis de IgG, IgA e/ou IgM e da função de anticorpo. As manifestações clínicas incluem a presença de infecções recorrentes ou crônicas, doenças inflamatórias/autoimunes e incidência aumentada de malignidades como linfomas e carcinomas, caracterizando-se, consequentemente, por um estado de ativação imune persistente e alterações do metabolismo oxidativo. Tanto a paraoxonase 1(PON1) quanto o polimorfismo do citocromo p450 (CYP) 2E1 têm importante participação nos processos oxidativos, controlando a extensão dos danos causados por alterações na concentração de oxidantes. Acredita-se que, tal qual ocorre na população normal, tanto a PON1 quanto a CYP2E1 tenham importante papel na gravidade e na sobrevida dos pacientes com ICV. OBJETIVO: estudar os polimorfismos de PON1 e CYP2E1, bem como a atividade arilesterase da PON1, e sua relação com o perfil lipídico, características clínicas, morbidade e mortalidade em pacientes com ICV. MÉTODOS/RESULTADOS: Foram avaliadas as frequências alélicas dos polimorfismos de PON1 e CYP2E1, o perfil lipídico e a atividade arilesterase da PON1 em 101 pacientes com ICV e 16 pacientes com hipogamaglobulinemia secundária (HS) e 130 controles saudáveis. Nos dois grupos de pacientes foi analisada a presença de parâmetros clínicos e laboratoriais, morbidade e gravidade da doença. Houve diferença na frequência dos genótipos de PON1-L55M entre pacientes primários e secundários, sendo o alelo 55L e o genótipo 55LM mais frequente no grupo HS. A atividade arilesterase de PON1 mostrou-se menor nos pacientes com ICV em relação ao grupo controle, com pacientes do genótipo 55MM apresentando os menores valores de atividade. Pacientes com o genótipo 55MM apresentaram doença mais grave quando comparados aos demais grupos genotípicos, sendo essa diferença causada não por uma característica deletéria deste genótipo, mas pelo papel protetor desempenhado pelo alelo 55L; pacientes portadores desse alelo apresentaram menor prevalência de manifestações graves como neoplasias, hepatomegalia, sepse e óbitos, bem como maior sobrevida daqueles que apresentavam ao menos uma cópia deste alelo. CONCLUSÃO: Este constitui o primeiro relato demonstrando maior frequência do genótipo 55LM e do alelo 55L em pacientes com hipogamaglobulinemia secundária e de menor atividade arilesterase em pacientes com ICV portadores do genótipo 55MM. Nossos resultados são sugestivos de que a presença do alelo 55L possa desempenhar papel protetor na ICV. Além disso, foi constatado que a presença de linfonodomegalia, hepatomegalia, esplenomegalia, sepse e hipertensão portal possam ser fatores preditivos tanto de um quadro de doença mais grave quanto de maior mortalidade / Introduction: Common Variable Immunodeficiency (CVID) is a heterogeneous disease characterized by reduced levels of IgG, IgA and / or IgM and antibody function. Clinical manifestations include the presence of recurrent or chronic infections, inflammatory/autoimmune diseases, and increased incidence of malignancies such as lymphomas and carcinomas, which is characterized by a state of persistent immune activation and alterations in oxidative metabolism. Both paraoxonase 1 (PON1) and cytochrome p450 (CYP) 2E1 polymorphism have an important role in oxidative processes, controlling the extent of damage caused by changes in oxidant concentration. It is believed that, as in the normal population, both PON1 and CYP2E1 play an important role in the severity and survival of patients with CVID. Objectives: to study the polymorphisms of PON1 and CYP2E1, as well as the arilesterase activity of PON1, and its relation with the lipid profile, clinical characteristics, morbidity and mortality in patients with CVID. Methods/Results: The allelic frequencies of the PON1 and CYP2E1 polymorphisms, the lipid profile and the arilesterase activity of PON1 in 101 patients with CVID and 16 patients with secondary hypogammaglobulinemia (HS) and 130 healthy controls were evaluated. The presence of clinical and laboratory parameters, morbidity and severity of the disease were analyzed in both groups of patients. There was a difference in the frequency of PON1-L55M genotypes between primary and secondary patients, being the 55L allele and the 55LM genotype more frequent in the HS group. The arilesterase activity of PON1 was lower in patients with CVID than in the control group, with patients of the 55MM genotype showing the lowest values. Patients with the 55MM genotype presented a more severe disease when compared to the other genotype groups, this difference is being caused not by a deleterious characteristic of this genotype, but by the protective role played by the 55L allele; patients with this allele had a lower prevalence of severe manifestations such as malignancies, hepatomegaly, sepsis and deaths, as well as a longer survival of those who had at least one copy of this allele. CONCLUSION: This is the first report showing a higher frequency of the 55LM genotype and the 55L allele in patients with secondary hypogammaglobulinemia and of lower arilesterase activity in patients with CVID with 55MM genotype. Our results suggest that the presence of the 55L allele may play a protective role in CVID. In addition, it was found that the presence of lymph node enlargement, hepatomegaly, splenomegaly, sepsis and portal hypertension may be predictive factors of both a more severe disease and a higher mortality rate
293

Mechanisms and quantitative prediction of Efavirenz metabolism, pharmacogenetics and drug interactions

Xu, Cong 08 1900 (has links)
Indiana University-Purdue University Indianapolis (IUPUI) / The antiretroviral drug efavirenz remains a cornerstone for treatment-naïve HIV patients. Subsequent to the demonstration that efavirenz is a substrate of cytochrome P450 (CYP) 2B6, a number of clinical studies found that the CYP2B6*6 allele is significantly associated with higher efavirenz exposure and/or adverse reactions. However, the mechanism of reduced efavirenz metabolism by this genetic variant is not fully understood and whether this variant exhibits differential susceptibility to metabolic inhibition is also unknown. Ths use of efavirenz is further complicated by the drug interactions associated with it. Therefore, I hypothezised that 1) the CYP2B6*6 allele reduces efavirenz metabolism by altering catalytic properties of CYP2B6; 2) efavirenz alters the pharmacokinetics of co-administered drugs by inhibiting drug metabolizing enzymes. A series of studies was carried out in hepatic microsomal preparations to determine the functional consequences of the CYP2B6*6 allele and to assess inhibition potency of efavirenz on 8 CYPs. The major findings for these studies include: 1) the CYP2B6*6 allele reduces efavirenz metabolism by decreasing substrate binding and catalytic efficiency; 2) functional consequences of the CYP2B6*6 allele appear to be substrate- and cytochrome b5-dependent; 3) the CYP2B6*6 allele confers increased susceptibility to metabolic inhibition; and 4) efavirenz inhibits the activities of CYP2B6, 2C8, 2C9 and 2C19 at therapeutically relevant concentrations. In addition, I explored the hypothesis that the incorporation of in vitro mechanism by which the CYP2B6*6 allele reduced efavirenz metabolism predicts the genetic effect of this allele on efavirenz clearance after a single oral dose by modeling approach. A pharmacogenetics-based in vitro-in vivo extrapolation (IVIVE) model was developed to predict human efavirenz clearance. Taken together, results from this dissertation provide new mechanistic information on how the CYP2B6*6 allale alters substrate metabolism and drug interactions; demonstrate new mechanisms of efavirenz-mediated inhibition interactions; and demonstrate the utility of a pharmacogenetics-based predictive model that can serve as a basis for future studies with efavirenz and other CYP2B6 substrates. Overall these data provide improved understanding of genetic and non-genetic determinant of efavirenz disposition and drug interactions associated with it.
294

Molekularbiologische Untersuchungen zum Einfluß genetischer Wirtsfaktoren auf das Erkrankungsrisiko und den Krankheitsverlauf von Patienten mit Plattenephithelkarzinomen im Kopf-Hals-Bereich

Matthias, Christoph 11 January 2000 (has links)
Neben Zigarettenrauchen und chronischem Alkoholkonsum scheinen genetische Faktoren bei der Entstehung und im Verlauf der Kopf-Hals-Karzinom Erkrankung bedeutsam zu sein. Genvariationen in den Enzymen, die zigarettenrauch-assoziierte Karzinogene (Glutathion-S-Transferase, GST, Cytochrom P450, CYP) metabolisieren, sowie Genvariationen in immunregulierenden Zytokinen (Tumor-Nekrose-Faktor) könnten Grund dieser Beeinflussung sein. Ziel dieser Studie war es, genetische Wirtsfaktoren zu identifizieren, die das Erkrankungsrisiko und das Tumorverhalten bzw. den Krankheitsverlauf von Plattenepithelkarzinomen im oberen Aerodigestivtrakt beeinflussen. Wir beschreiben den Zusammenhang zwischen Genotypen an GSTM1, M3, T1, P1, CYP2D6, 1A1, 2E1 und TNF Mikrosatelliten-Genorten und der Krankheitsentstehung sowie Tumorcharakteristika wie der initialen Tumorgröße, der Halslymphknotenmetastasierung, dem histologischen Differenzierungsgrad des Tumorgewebes und dem rezidivfreien Überleben bei 465 Patienten. Die Genotypen wurden aus der Leukozyten-DNA mittels PCR in Kombination mit Restriktionsenzymverdauungen und Elektrophoresetechniken identifiziert. Sowohl bei den Genvariationen in den entgiftenden Enzymen als auch bei den TNF Mikrosatelliten-Polymorphismen konnten Risikogenotypen festgestellt werden. Die Beeinflussung des Krankheitsverlaufs war teilweise deutlicher ausgeprägt, als die Beeinflussung der Krankheitsentstehung. Patienten mit Mehrfachkarzinomen wiesen die stärkste Anhäufung von Risikogenotypen auf. In dieser Studie konnte erstmals gezeigt werden, daß individuelle Genotypkonstellationen die Entstehung und das Verhalten von Plattenepithelkarzinomen im oberen Aerodigestivtrakt beeinflussen. / Cigarette smoking and alcohol consumption are the main risk factors for the development of head and neck cancer. Additionally, genetic factors seem to be influential. Gene variations in detoxifying enzymes such as glutathione S-transferase (GST) and cytochrome P450 (CYP) and variations in immune regulating proteins like tumor necrosis factor (TNF) are candidate genes. Accordingly, we have examined, in 465 patients with squamous cell carcinoma (SCC) of the head and neck, associations between GSTM1, GSTT1, GSTM3, GSTP1, CYP2D6, CYP1A1, CYP2E1 genotypes and TNF microsatellite polymorphisms and cancer susceptibility, outcome parameters like tumor extension, histological grade, and presence of lymph nodes, and tumor recurrence. Genotypes were determined by PCR; logistic regression and a step-wise model were used to investigate the influence of the individual genes. Individual genotypes in the detoxifying enzymes and TNF were associated with altered cancer risk. The influence on tumor behavior was partially stronger. Patients suffering multiple head and neck cancer showed the highest cumulation of risk mediating genotypes. The data demonstrate site-dependent associations between GST, CYP and TNF genotypes and tumor susceptibility, tumor extension, differentiation, and lymph node involvement, and tumor recurrence in SCC of the head and neck.
295

Avaliação farmacogenética em pacientes tratados com fármacos antitabagismo / Pharmacogenetic evaluation in patients treated with drugs for smoking cessation

Santos, Juliana da Rocha dos 07 April 2015 (has links)
Introdução: A grande variabilidade individual em resposta a fármacos antitabagismo sugere que tratamentos específicos podem ser mais efetivos em determinados subgrupos de fumantes. No contexto de medicina personalizada, o principal objetivo do presente estudo foi avaliar se polimorfismos nos genes CHRNA4, CHRNB2, CYP2B6 e ANKK1 estão associados com a resposta às terapias de cessação tabágica em pacientes provenientes de um programa de assistência ao fumante. Métodos: Estudo de coorte com 483 pacientes fumantes que receberam tratamento farmacológico (vareniclina, vareniclina e bupropiona, bupropiona em monoterapia ou coadministrada com terapia de reposição nicotínica). O sucesso na cessação tabágica foi considerado para os pacientes que completaram 6 meses de abstinência contínua. O teste de Fagerström para a dependência à nicotina (FTND) e o escore de consumo situacional Issa foram utilizados para avaliar a dependência à nicotina. Os polimorfismos CHRNA4 (rs1044396 e rs2236196), CHRNB2 (rs2072660 e rs2072661) e ANKK1 (rs1800497) foram genotipados pela análise da curva de melting e os polimorfismos CYP2B6 *9 (rs3745274), *4 (rs2279343), *5 (rs3211371) foram genotipados por restrição enzimática. Resultados: Os pacientes com o genótipo CC para o polimorfismo CHRNA4 (rs10443196) obtiveram menor taxa de sucesso no tratamento com vareniclina (29,5%) em comparação com os portadores dos genótipos CT ou TT (50,9%) (P=0,007; n=167). Os genótipos CT ou TT foram associados com maior odds ratio para o sucesso (OR=1,67; IC 95%=1,10-2,53; P=0,02), em um modelo multivariado. Os pacientes com o genótipo AA para o polimorfismo CYP2B6 (rs2279343) obtiveram maior taxa de sucesso no tratamento com bupropiona (48,0%) em comparação com portadores dos genótipos AG ou GG (35,5%) (P=0,05; n=237). O genótipo AA foi associado com maior odds ratio para o sucesso no tratamento (OR=1,92; IC 95%=1,08-3,42; P=0,03), em um modelo multivariado. Não foram observadas diferenças significativas nos escores FTND e Issa com relação aos polimorfismos estudados. Conclusão: Os polimorfismos CHRNA4 (rs1044396) e CYP2B6 (rs2279343) estão associados com a cessação tabágica em indivíduos tratados com vareniclina e bupropiona, respectivamente. Sugere-se que estes polimorfismos influenciam a resposta farmacológica e podem ser importantes para o desenho de uma farmacoterapia individualizada / Background: The large individual variability in response to drugs for smoking cessation suggests that specific treatments can be more effective in particular subgroups of smokers. In the context of personalized medicine, the main aim of the present study was to evaluate whether the CHRNA4, CHRNB2, CYP2B6 and ANKK1 polymorphisms are associated with response to smoking cessation therapies in patients from a smoker assistance program. Methods: This cohort study enrolled 483 smoking patients patients who received pharmacological treatment (varenicline, varenicline plus bupropion, bupropion in monoterapy or plus nicotine replacement therapy). Smoking cessation success was considered for patients who completed 6 months of continuous abstinence. Fagerström test for nicotine dependence (FTND) and Issa situational smoking scores were analyzed for nicotine dependence. The CHRNA4 (rs1044396 and rs2236196), CHRNB2 (rs2072660 and rs2072661) and ANKK1 rs1800497 polymorphisms were genotyped by high resolution melting analysis and the CYP2B6 *9 (rs3745274), *4 (rs2279343) and *5 (rs3211371) were genotyped by restriction fragment lenght polymorphisms. Results: Patients with CHRNA4 rs1044396 CC genotype had lower success rate in treatment with varenicline (29.5%) compared with carriers of CT or TT genotypes (50.9%) (P=0.007, n=167). The CT or TT genotypes were associated with higher odds ratio for success (OR=1.67, 95%CI=1.10-2.53, P=0.02), in a multivariate model. Patients with CYP2B6 rs2279343 AA genotype had higher success rate in treatment with bupropion (48.0%) compared with carriers of AG or GG genotypes (35.5%) (P=0.05, n=237). The AA genotype was associated with higher odds ratio for success (OR=1.92, 95%CI=1.08-3.42, P=0.03), in a multivariate model. We did not observe significant differences in the FTND and Issa scores according to the studied polymorphisms. Conclusion: The CHRNA4 rs1044396 and CYP2B6 rs2279343 are associated with smoking cessation in individuals on varenicline and bupropion terapies, respectively. We suggest that these polymorphisms influence the pharmacological response of these drugs and it might be important in the design of individualized pharmacotherapy
296

Efeitos da participação de esteroides-like provenientes da poluição atmosférica no epitélio das vias aéreas em camundongos machos e fêmeas / Effects of the participation of steroid-like compounds from air pollution in the airway epithelium of male and female mice

Yoshizaki, Kelly 28 April 2014 (has links)
O epitélio nasal é a primeira porção do sistema respiratório a entrar em contato com o ambiente externo. Partículas da poluição do ar, principalmente os compostos orgânicos absorvidos, podem atuar como liberadores endócrinos. O receptor aril hidrocarboneto (AhR) é um importante competidor dos receptores de estrógeno-beta (ERbeta) que regulam a transcrição do gene para enzimas de metabolização xenobióticas (enzimas do citocromo P450). O objetivo deste estudo é identificar e quantificar ERbeta, AhR, CYP1A1, CYP1A2, CYP1B1 e o perfil de muco no epitélio nasal de camundongos machos e fêmeas em diferentes fases do ciclo estral. Camundongos BALB/c machos (n=32) e fêmeas (n=84) foram expostos ao ar ambiente e ao MP2,5 concentrado a 600 ug.m-³ em um concentrador de partículas ambientais (CPAs). As fêmeas foram divididas de acordo com as fases do ciclo estral: proestro, estro e diestro. O epitélio nasal foi avaliado por RT-PCR e imuno-histoquímica para análise de expressão de ERbeta (proteína), Erbeta-1 e Erbeta-2 (gene), AhR (proteína e gene) e Cyp1a1, Cyp1a2 and Cyp1b1 (gene). A quantificação de muco neutro - Periodic Acid Schiff\'s (PAS+) e ácido - Alcian Blue (AB+) foi avaliada por morfometria. As exposições foram realizadas durante 5 dias/semana, por 45 ± 55 dias. A expressão de Erbeta-2 RNAm apresentou diferenças em resposta à exposição ao CPAs (p=0,016), bem como uma diminuição em fêmeas, quando comparadas aos camundongos machos (p=0,036). A expressão de Cyp1b1 RNAm foi significantemente menor no grupo exposto ao CPAs, em relação ao grupo exposto ao ar ambiente nas fêmeas em diestro (p=0,036). A expressão de Erbeta foi aumentada no epitélio nasal de fêmeas em estro expostas ao CPAs (p=0,005) e a expressão de AhR foi menor em fêmeas em proestro expostas ao CPAs (p=0,048). A exposição ao CPAs levou ao aumento do conteúdo de muco ácido em camundongos machos (p=0,048), o qual diminuiu em fêmeas (p=0,040), quando comparados ao grupo ar ambiente. Este estudo mostrou que houve diferentes respostas à exposição à poluição do ar no epitélio nasal entre machos e fêmeas, e que essas diferenças podem estar relacionadas com a predisposição de fêmeas apresentarem maior suscetibilidade a doenças respiratórias das vias aéreas / The nasal epithelium is the first portion of the respiratory system to reach contact with the external environment. Air pollution particles, mainly the organic compounds absorbed into them, may act as endocrine releasers. The aryl hydrocarbon (AhR) receptor is an important competitor of estrogenic receptors-beta (ERbeta) that regulate transcription of gene coding for xenobiotic-metabolizing enzymes (cytochrome P450 enzymes). The aim of this study is to identify and quantify in the nasal epithelium of male and female mice in different estrous cycle phases related with ERbeta, AhR, CYP1A1, 1A2, 1B1 and the mucus profile. Male (n=32) and female (n=84) BALB/c mice were exposed to ambient air and PM2.5 concentrated at 600 ug.m-³ in an ambient particle concentrator with a particulate matter diameter of 2.5 um (PM2.5). Females were subdivided in three estrous cycles: proestrus, estrus and diestrus. Nasal epithelium was evaluated through RT-PCR and immunohistochemistry for the expression of ERbeta (protein), Erbeta-1 and Erbeta-2 (gene expression), AhR (protein and gene expression) and Cyp1a1, Cyp1a2 and Cyp1b1 (gene expression). Morphometry was applied for evaluation of mucus profile: acid - Alcian Blue (AB+) and neutral - Periodic Acid Schiff\'s (PAS+). Exposure happened for 5 days/week, for 45 ± 55 days. There were differences in Erbeta-2 mRNA in response to exposition to CPAs (p=0.016), and a significant decrease in female compared male mice (p=0.036). Cyp1b1 mRNA was significantly smaller in the CPAs-exposed group compared with the ambient air group in diestrus female mice (p=0.036). The ERbeta expression increased in the nasal epithelium of CPAs-exposed females in the estrus cycle (p=0.005), and the AhR expression decreased in the proestrus cycle of CPAs-exposed females (p=0.048). The exposure to the CPAs led to an increase in the acidic content of mucus in male mice (p=0.048), and decreased in female mice (p=0.040), compared to the ambient air group. This study showed there were different responses in the nasal epithelia of male and female mice exposed to air pollution, which could be related to the predisposition of the females to present more susceptibility to airway respiratory diseases
297

Avaliação do impacto da inclusão de polimorfismos nos genes ABCB1 e CYP4F2 em algoritmo farmacogenético para dosagem personalizada do anticoagulante varfarina / Impact evaluation of incorporating ABCB1 and CYP4F2 polymorphisms in a genetic-guided warfarin dosing algorithm

Tavares, Letícia Camargo 23 April 2019 (has links)
O anticoagulante oral cumarínico varfarina é vastamente utilizado para o tratamento e prevenção de eventos tromboembólicos, que configuram uma das principais causas de mortalidade mundial. Contudo, de acordo com fatores genéticos e ambientais, os cumarínicos apresentam grande variação em sua farmacocinética e farmacodinâmica, implicando em respostas variáveis entre os indivíduos. Para auxílio na tomada de decisão pelo corpo clínico na terapia com a varfarina, algoritmos farmacogenéticos estimadores de dose têm sido extensivamente estudados e desenvolvidos, com o intuito de estabelecer terapias personalizadas. Neste sentido, o presente estudo teve como objetivos investigar a associação de polimorfismos nos genes ABCB1 e CYP4F2 com a variabilidade do requerimento de dose de varfarina, e, primariamente, avaliar o impacto da inclusão desses polimorfismos como covariáveis do algoritmo farmacogenético estimador de dosagem de varfarina previamente desenvolvido para a população brasileira por Santos et al. (2015). Neste estudo retrospectivo, foram utilizadas amostras de 965 pacientes registrados no Instituto do Coração (InCor) do Hospital das Clínicas da Faculdade de Medicina da Universidade de São Paulo (HC/FMUSP). As genotipagens dos polimorfismos ABCB1 c.3435C>T e CYP4F2 c.1297G>A foram realizadas por meio da amplificação do DNA genômico através da reação em cadeia da polimerase seguida por análise de curva de dissociação (PCR-HRM) ou ensaio TaqMan®, respectivamente para cada variante. Para as análises estatísticas, utilizamos a abordagem de regressão linear múltipla, considerando a dose estável de varfarina como variável resposta e como covariáveis os polimorfismos de interesse nos genes ABCB1 e CYP4F2, bem como outros fatores genéticos, clínicos e demográficos. Nossos resultados sugerem que carreadores da variante ABCB1 c.3435C>T requerem doses médias de manutenção de varfarina inferiores quando comparados aos indivíduos com genótipo selvagem (redução de 2,5 e 4,3 mg/semana, respectivamente para carreadores dos genótipos CT e TT). Ainda, observamos uma grande variabilidade de dose de varfarina no subgrupo de pacientes autodeclarados não-brancos, de acordo com os genótipos ABCB1 (redução de 5,5 e 10,2 mg/semana, respectivamente para carreadores dos genótipos CT e TT). Além disso, verificamos que ambos os polimorfismos ABCB1 c.3435C>T e CYP4F2 c.1297G>A contribuíram para a predição de dose de varfarina, quando associados a outros fatores genotípicos, demográficos e clínicos relevantes, sendo estatisticamente significativos, aumentando o coeficiente de determinação do algoritmo em 2,6% e explicando um adicional de 3,6% da variabilidade interindividual de dosagem. Em conclusão, demonstramos que as genotipagens das variantes ABCB1 c.3435C>T e CYP4F2 c.1297G>A podem ser relevantes para acurar a terapêutica com varfarina na população brasileira / The coumarin oral anticoagulant warfarin has been widely used for treating and preventing thromboembolic events, which are one of the main causes of mortality worldwide. However, according to genetic and environmental factors, coumarins show high variance in pharmacokinetics and pharmacodynamics, resulting in variable interindividual responses. For supporting warfarin clinical decisions, genetic-guided algorithms have been extensively studied and developed, in order to set personalized therapeutics. In this context, the aims of this master\'s research project were to investigate the association of ABCB1 and CYP4F2 polymorphisms with individual\'s warfarin dose requirements and to assess the impact of the inclusion of these polymorphisms as covariates in the genetic-guided dosing algorithm developed by Santos PC et al. (2015) for the Brazilian population. For this retrospective study, 965 patients enrolled in the Heart Institute (InCor), University of São Paulo Medical School (FMUSP) were involved. Genotyping of ABCB1 c.3435C>T and CYP4F2 c.1297G>A were performed by genomic DNA amplification by polymerase chain reaction (PCR), followed by melting curve analysis (HRM-PCR) and TaqMan® assay, respectively. For statistical analysis, we utilized multiple linear regression approach considering warfarin stable dose as the dependent variable and the ABCB1 and CYP4F2 variants, as well as other genetic, clinical and demographic factors as covariates. Our data suggests that carriers of ABCB1 c.3435C>T genotypes require lower mean warfarin maintenance doses when compared to wild-type individuals (reduction of 2.5 and 4.3 mg/week, respectively for CT and TT genotype carriers). Furthermore, we observed large warfarin dose variability for the subgroup of patients who self-declared themselves as non-white according to ABCB1 genotypes (lowering of 5.5 and 10.2 mg/week, respectively for CT and TT genotype carriers). Finally, we verified that both ABCB1 c.3435C>T and CYP4F2 c.1297G>A polymorphisms were able to contribute to warfarin dose prediction, when associated to other relevant genetic, clinical and demographic data, being statistically significant, improving the algorithm\'s coefficient of determination by 2.6% and explaining an additional of 3.6% of the interindividual warfarin dosage variability. In conclusion, in this study we have demonstrated that the genotyping of ABCB1 c.3435C>T and CYP4F2 c.1297G>A may be relevant for improving the management of warfarin therapeutics in Brazilian patients
298

Avaliação farmacogenética em pacientes tratados com fármacos antitabagismo / Pharmacogenetic evaluation in patients treated with drugs for smoking cessation

Juliana da Rocha dos Santos 07 April 2015 (has links)
Introdução: A grande variabilidade individual em resposta a fármacos antitabagismo sugere que tratamentos específicos podem ser mais efetivos em determinados subgrupos de fumantes. No contexto de medicina personalizada, o principal objetivo do presente estudo foi avaliar se polimorfismos nos genes CHRNA4, CHRNB2, CYP2B6 e ANKK1 estão associados com a resposta às terapias de cessação tabágica em pacientes provenientes de um programa de assistência ao fumante. Métodos: Estudo de coorte com 483 pacientes fumantes que receberam tratamento farmacológico (vareniclina, vareniclina e bupropiona, bupropiona em monoterapia ou coadministrada com terapia de reposição nicotínica). O sucesso na cessação tabágica foi considerado para os pacientes que completaram 6 meses de abstinência contínua. O teste de Fagerström para a dependência à nicotina (FTND) e o escore de consumo situacional Issa foram utilizados para avaliar a dependência à nicotina. Os polimorfismos CHRNA4 (rs1044396 e rs2236196), CHRNB2 (rs2072660 e rs2072661) e ANKK1 (rs1800497) foram genotipados pela análise da curva de melting e os polimorfismos CYP2B6 *9 (rs3745274), *4 (rs2279343), *5 (rs3211371) foram genotipados por restrição enzimática. Resultados: Os pacientes com o genótipo CC para o polimorfismo CHRNA4 (rs10443196) obtiveram menor taxa de sucesso no tratamento com vareniclina (29,5%) em comparação com os portadores dos genótipos CT ou TT (50,9%) (P=0,007; n=167). Os genótipos CT ou TT foram associados com maior odds ratio para o sucesso (OR=1,67; IC 95%=1,10-2,53; P=0,02), em um modelo multivariado. Os pacientes com o genótipo AA para o polimorfismo CYP2B6 (rs2279343) obtiveram maior taxa de sucesso no tratamento com bupropiona (48,0%) em comparação com portadores dos genótipos AG ou GG (35,5%) (P=0,05; n=237). O genótipo AA foi associado com maior odds ratio para o sucesso no tratamento (OR=1,92; IC 95%=1,08-3,42; P=0,03), em um modelo multivariado. Não foram observadas diferenças significativas nos escores FTND e Issa com relação aos polimorfismos estudados. Conclusão: Os polimorfismos CHRNA4 (rs1044396) e CYP2B6 (rs2279343) estão associados com a cessação tabágica em indivíduos tratados com vareniclina e bupropiona, respectivamente. Sugere-se que estes polimorfismos influenciam a resposta farmacológica e podem ser importantes para o desenho de uma farmacoterapia individualizada / Background: The large individual variability in response to drugs for smoking cessation suggests that specific treatments can be more effective in particular subgroups of smokers. In the context of personalized medicine, the main aim of the present study was to evaluate whether the CHRNA4, CHRNB2, CYP2B6 and ANKK1 polymorphisms are associated with response to smoking cessation therapies in patients from a smoker assistance program. Methods: This cohort study enrolled 483 smoking patients patients who received pharmacological treatment (varenicline, varenicline plus bupropion, bupropion in monoterapy or plus nicotine replacement therapy). Smoking cessation success was considered for patients who completed 6 months of continuous abstinence. Fagerström test for nicotine dependence (FTND) and Issa situational smoking scores were analyzed for nicotine dependence. The CHRNA4 (rs1044396 and rs2236196), CHRNB2 (rs2072660 and rs2072661) and ANKK1 rs1800497 polymorphisms were genotyped by high resolution melting analysis and the CYP2B6 *9 (rs3745274), *4 (rs2279343) and *5 (rs3211371) were genotyped by restriction fragment lenght polymorphisms. Results: Patients with CHRNA4 rs1044396 CC genotype had lower success rate in treatment with varenicline (29.5%) compared with carriers of CT or TT genotypes (50.9%) (P=0.007, n=167). The CT or TT genotypes were associated with higher odds ratio for success (OR=1.67, 95%CI=1.10-2.53, P=0.02), in a multivariate model. Patients with CYP2B6 rs2279343 AA genotype had higher success rate in treatment with bupropion (48.0%) compared with carriers of AG or GG genotypes (35.5%) (P=0.05, n=237). The AA genotype was associated with higher odds ratio for success (OR=1.92, 95%CI=1.08-3.42, P=0.03), in a multivariate model. We did not observe significant differences in the FTND and Issa scores according to the studied polymorphisms. Conclusion: The CHRNA4 rs1044396 and CYP2B6 rs2279343 are associated with smoking cessation in individuals on varenicline and bupropion terapies, respectively. We suggest that these polymorphisms influence the pharmacological response of these drugs and it might be important in the design of individualized pharmacotherapy
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Efeitos da participação de esteroides-like provenientes da poluição atmosférica no epitélio das vias aéreas em camundongos machos e fêmeas / Effects of the participation of steroid-like compounds from air pollution in the airway epithelium of male and female mice

Kelly Yoshizaki 28 April 2014 (has links)
O epitélio nasal é a primeira porção do sistema respiratório a entrar em contato com o ambiente externo. Partículas da poluição do ar, principalmente os compostos orgânicos absorvidos, podem atuar como liberadores endócrinos. O receptor aril hidrocarboneto (AhR) é um importante competidor dos receptores de estrógeno-beta (ERbeta) que regulam a transcrição do gene para enzimas de metabolização xenobióticas (enzimas do citocromo P450). O objetivo deste estudo é identificar e quantificar ERbeta, AhR, CYP1A1, CYP1A2, CYP1B1 e o perfil de muco no epitélio nasal de camundongos machos e fêmeas em diferentes fases do ciclo estral. Camundongos BALB/c machos (n=32) e fêmeas (n=84) foram expostos ao ar ambiente e ao MP2,5 concentrado a 600 ug.m-³ em um concentrador de partículas ambientais (CPAs). As fêmeas foram divididas de acordo com as fases do ciclo estral: proestro, estro e diestro. O epitélio nasal foi avaliado por RT-PCR e imuno-histoquímica para análise de expressão de ERbeta (proteína), Erbeta-1 e Erbeta-2 (gene), AhR (proteína e gene) e Cyp1a1, Cyp1a2 and Cyp1b1 (gene). A quantificação de muco neutro - Periodic Acid Schiff\'s (PAS+) e ácido - Alcian Blue (AB+) foi avaliada por morfometria. As exposições foram realizadas durante 5 dias/semana, por 45 ± 55 dias. A expressão de Erbeta-2 RNAm apresentou diferenças em resposta à exposição ao CPAs (p=0,016), bem como uma diminuição em fêmeas, quando comparadas aos camundongos machos (p=0,036). A expressão de Cyp1b1 RNAm foi significantemente menor no grupo exposto ao CPAs, em relação ao grupo exposto ao ar ambiente nas fêmeas em diestro (p=0,036). A expressão de Erbeta foi aumentada no epitélio nasal de fêmeas em estro expostas ao CPAs (p=0,005) e a expressão de AhR foi menor em fêmeas em proestro expostas ao CPAs (p=0,048). A exposição ao CPAs levou ao aumento do conteúdo de muco ácido em camundongos machos (p=0,048), o qual diminuiu em fêmeas (p=0,040), quando comparados ao grupo ar ambiente. Este estudo mostrou que houve diferentes respostas à exposição à poluição do ar no epitélio nasal entre machos e fêmeas, e que essas diferenças podem estar relacionadas com a predisposição de fêmeas apresentarem maior suscetibilidade a doenças respiratórias das vias aéreas / The nasal epithelium is the first portion of the respiratory system to reach contact with the external environment. Air pollution particles, mainly the organic compounds absorbed into them, may act as endocrine releasers. The aryl hydrocarbon (AhR) receptor is an important competitor of estrogenic receptors-beta (ERbeta) that regulate transcription of gene coding for xenobiotic-metabolizing enzymes (cytochrome P450 enzymes). The aim of this study is to identify and quantify in the nasal epithelium of male and female mice in different estrous cycle phases related with ERbeta, AhR, CYP1A1, 1A2, 1B1 and the mucus profile. Male (n=32) and female (n=84) BALB/c mice were exposed to ambient air and PM2.5 concentrated at 600 ug.m-³ in an ambient particle concentrator with a particulate matter diameter of 2.5 um (PM2.5). Females were subdivided in three estrous cycles: proestrus, estrus and diestrus. Nasal epithelium was evaluated through RT-PCR and immunohistochemistry for the expression of ERbeta (protein), Erbeta-1 and Erbeta-2 (gene expression), AhR (protein and gene expression) and Cyp1a1, Cyp1a2 and Cyp1b1 (gene expression). Morphometry was applied for evaluation of mucus profile: acid - Alcian Blue (AB+) and neutral - Periodic Acid Schiff\'s (PAS+). Exposure happened for 5 days/week, for 45 ± 55 days. There were differences in Erbeta-2 mRNA in response to exposition to CPAs (p=0.016), and a significant decrease in female compared male mice (p=0.036). Cyp1b1 mRNA was significantly smaller in the CPAs-exposed group compared with the ambient air group in diestrus female mice (p=0.036). The ERbeta expression increased in the nasal epithelium of CPAs-exposed females in the estrus cycle (p=0.005), and the AhR expression decreased in the proestrus cycle of CPAs-exposed females (p=0.048). The exposure to the CPAs led to an increase in the acidic content of mucus in male mice (p=0.048), and decreased in female mice (p=0.040), compared to the ambient air group. This study showed there were different responses in the nasal epithelia of male and female mice exposed to air pollution, which could be related to the predisposition of the females to present more susceptibility to airway respiratory diseases
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Identification and mechanistic investigation of clinically important myopathic drug-drug interactions

Han, Xu January 2014 (has links)
Indiana University-Purdue University Indianapolis (IUPUI) / Drug-drug interactions (DDIs) refer to situations where one drug affects the pharmacokinetics or pharmacodynamics of another. DDIs represent a major cause of morbidity and mortality. A common adverse drug reaction (ADR) that can result from, or be exacerbated by DDIs is drug-induced myopathy. Identifying DDIs and understanding their underlying mechanisms is key to the prevention of undesirable effects of DDIs and to efforts to optimize therapeutic outcomes. This dissertation is dedicated to identification of clinically important myopathic DDIs and to elucidation of their underlying mechanisms. Using data mined from the published cytochrome P450 (CYP) drug interaction literature, 13,197 drug pairs were predicted to potentially interact by pairing a substrate and an inhibitor of a major CYP isoform in humans. Prescribing data for these drug pairs and their associations with myopathy were then examined in a large electronic medical record database. The analyses identified fifteen drug pairs as DDIs significantly associated with an increased risk of myopathy. These significant myopathic DDIs involved clinically important drugs including alprazolam, chloroquine, duloxetine, hydroxychloroquine, loratadine, omeprazole, promethazine, quetiapine, risperidone, ropinirole, trazodone and simvastatin. Data from in vitro experiments indicated that the interaction between quetiapine and chloroquine (risk ratio, RR, 2.17, p-value 5.29E-05) may result from the inhibitory effects of quetiapine on chloroquine metabolism by cytochrome P450s (CYPs). The in vitro data also suggested that the interaction between simvastatin and loratadine (RR 1.6, p-value 4.75E-07) may result from synergistic toxicity of simvastatin and desloratadine, the major metabolite of loratadine, to muscle cells, and from the inhibitory effect of simvastatin acid, the active metabolite of simvastatin, on the hepatic uptake of desloratadine via OATP1B1/1B3. Our data not only identified unknown myopathic DDIs of clinical consequence, but also shed light on their underlying pharmacokinetic and pharmacodynamic mechanisms. More importantly, our approach exemplified a new strategy for identification and investigation of DDIs, one that combined literature mining using bioinformatic algorithms, ADR detection using a pharmacoepidemiologic design, and mechanistic studies employing in vitro experimental models.

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