Large-scale moisture flux analysis for the United States

Wang, Sheng-Hung

03 February 2004

No description available.

Physics, Atmospheric Science

RPC1

NCEP/NCAR

MOISTURE

hPa

MOISTURE FLUX

teleconnection

moisture budget

Relations among Involuntary Stress Responses, Social Support, and Cortisol Output during Acute Social Stress among Adolescent Girls

Hanes, Jacob Wobst

07 1900

This investigation utilized data from a previous laboratory-based study to examine the interactive contributions of trait involuntary stress responses (ISRs, e.g., rumination) and perceived familial social support (SS) on the hypothalamic-pituitary-adrenal axis (HPA; as indexed via salivary cortisol) response to acute stress in a sample of 128 adolescent girls ages 12 to 16. Participants completed a modified Trier Social Stress Test (TSST), and physiologic stress response was indexed via six salivary cortisol samples. Dimensions of ISRs and familial social support were entered into regression models to predict total cortisol circulation defined by area under the curve with respect to ground (AUCG; Pruessner et al., 2003) following the TSST. Neither ISRs or SS were associated with cortisol AUCG, nor was there an interactive effect of SS on relationships between ISRs and AUCG. Implications of present results and methodological recommendations for future investigations are discussed. This may be the first investigation to consider the interactive effects of ISRs and social support on adolescent girls' HPA responses. Greater understanding of these factors in this understudied demographic will improve translational science as well as inform risk assessment and intervention development.

HPA Reactivity

Involuntary Stress Responses

Social Support, TSST

Psychology, Experimental

Psychology, Physiological

Psychology, Behavioral

Vliv stresu na expresi 11β-hydroxysteroiddehydrogenasy v mozku laboratorního potkana / Effect of stress on expression of 11β-hydroxysteroid dehydrogenase in rat brain

Kuželová, Andrea

January 2013

This thesis examines the influence of stress on the activity of hippocampal CA1 area. The main task was to determine whether the stress load affects the changes of the local metabolism of glucocorticoids, and whether the levels of corticosteroid receptors in the CA1 hippocampus are modulated in response to stress. In order to answer these questions, the experiments were carried out using three different rat strains - Fisher, Lewis and Wistar which differ in their activities of hypothalamic-pituitary-adrenal axis. Our results demonstrate that stress has no effect on expression of MR mRNA. Conversely, stress reduces the levels of GR mRNA in CA1 area of the dorsal hippocampus. Moreover, we confirmed that the Lewis and Wistar rats didn't change metabolism of glucocorticoids after stress response. By the Fisher rats increased levels of 11β-HSD1 mRNA expression and therefore increased the metabolism of corticosterone.

\"Alterações na imunidade inespecifica subsequentes à indução de estresse agudo em indivíduos com fobia social e pessoas sem patologias psiquiátricas\" / Alterations in inespecific immunity subsequent to the induction of acute stress in individuals with social phobia and persons without psychiatric disorders

Faustino, Alessandra Fernandes

18 April 2005

As interações entre o sistema nervoso central e os sistemas imune e endócrino são o objeto de estudo da psiconeuroimunologia. Protocolos de indução de estresse têm sido amplamente utilizados como métodos confiáveis de investigação da relação entre transtornos psiquiátricos, aspectos psicológicos, traços de personalidade, ansiedade e a resposta imune. O procedimento de simulação de falar em público (SFP) é um protocolo experimental validado que reconhecidamente é capaz de ativar o eixo hipotálamo-hipófise-adrenal (HPA) e produzir respostas de estresse em sujeitos humanos. Esse método foi utilizado para: 1) Comparar a reatividade imunológica de indivíduos com diagnóstico de fobia social com a de indivíduos sem qualquer diagnóstico psiquiátrico; 2) Investigar se ocorrem alterações imunes subseqüentes à exposição a um estressor agudo induzido em laboratório e 3) identificar e correlacionar parâmetros imunológicos com traços de personalidade, humor, níveis de ansiedade e medidas fisiológicas. Os traços de personalidade foram investigados por meio dos seguintes instrumentos: Inventário de Temperamento e Caráter (TCI), Escala de Afeto Positivo e Negativo (PANAS), Inventário de Ansiedade Traço (IDATE-T), Inventário de Depressão de Beck (BDI), Inventário de Estratégias de ?Coping? de Folkman e Lazarus e Adaptação da Escala de Percepção de Estresse (PSS). Os sintomas de ansiedade foram avaliados por meio da Escala Analógica Visual de Humor (VAMS), da Escala de Sintomas Somáticos (ESS) e do IDATE-Estado. As variáveis psicofisiológicas avaliadas foram pressão arterial sistólica (PAS), diastólica (PAD), batimentos cardíacos (BPM), resposta galvânica da pele (GSR) e temperatura. Os níveis plasmáticos de catecolaminas (adrenalina, noradrenalina e dopamina) e hormônios do eixo HPA (cortisol e ACTH) também foram dosados. Realizou-se a contagem de células imunes polimorfonucleares e mononucleares no sangue periférico e mediu-se a atividade citotóxica de células NK e neutrófilos. Dosou-se proteínas de fase aguda e imunoglobulinas (A, D, G, M e E) a produção de citocinas no sangue por ELISA e RT-PCR. Os dados foram submetidos a análises de variância para dados com medidas repetidas testando efeitos de grupo, sexo, momento experimental e interações. As correlações entre as variáveis foram testadas por regressões múltiplas e coeficientes de correlação de Pearson. Os resultados apontam que o SFP foi eficiente para induzir estresse e produzir alterações detectáveis em diversos dos parâmetros investigados. As diferenças entre fóbicos sociais e controles são significativas para traços de personalidade e atuam ao longo do tempo para as medidas psicofisiológicas. Alterações imunes e hormonais estiveram mais frequentemente associadas ao gênero do que ao grupo experimental, e afetaram mais homens. Além disso, as alterações imunes foram de pequena magnitude afetando componentes inespecíficos da resposta imune. Conjuntamente, os resultados apontam uma relativa ativação do eixo HPA em fóbicos mas que não corresponde a alterações imunes de mesma magnitude. Mais estudos com uma amostra maior e a investigação de outros parâmetros são necessários para compreender melhor como a fobia social afeta o sistema imune de homens e mulheres e investigar se as alterações podem aumentar a susceptibilidade a doenças nesse grupo de sujeitos. Uma vez que essa interação seja melhor compreendida poderá subsidiar estratégias mais adequadas para abordar e elaborar estratégias de prevenção e intervenção capazes de promover comportamentos saudáveis. / Interactions among the nervous, immune and endocrine systems are the object of study of Psychoneuroimmunology. Stress protocols have been broadly used as reliable means to investigate the relationship among psychiatric disorders, psychological aspects, personality traits, anxiety and immune response has been studied using these interactions. The Simulated Public Speaking (SPS) is a validated experimental procedure known to activate the Hypothalamus-Pituitary-Adrenal (HPA) axis and produce stress responses in human subjects. This method was used to: 1) compare the immune reactions of individuals with a diagnosis of social phobia to that of individuals without any psychiatric diagnosis; 2) investigate if immune alterations occur subsequent to the exposure to an acute laboratory induced stressor; 3) identify and correlate immune parameters with personality traits, mood, anxiety levels and physiologic measures. Personality traits were investigated with Cloninger?s Temperament and Character?s Inventory (TCI), Positive and Negative Affects Scale (PANAS), State-Trait Anxiety Scale (STAI?T), Beck?s Depression Inventory (BDI), Lazarus?s Coping Strategies Inventory, Perceived Stress Scale (PSS). Anxiety symptoms were investigated along the procedure with the Bodily Symptoms Scale (ESS), STAI-E and the Visual Analogue Mood Scale (VAMS). Psychophysiologic variables assessed were Systolic (PAS) and Diastolic (PAD) Blood Pressure, Heart Rate (BPM), Galvanic Skin Response (GSR) and temperature. Plasmatic circulating levels of cathecolamines (Adrenaline, Noradrenaline and Dopamine) and HPA axis hormones (Cortisol, ACTH) were assessed. Peripheral blood cell population counts were obtained for polymorphonuclear (PMN) and mononuclear cells. Cytotoxic activity of neutrophils and NK cells was assessed, as well as cytokine production by ELISA and RT-PCR. Acute phase proteins and immunoglobulins (A, D, G, M, and E) were dosed on peripheral blood. Data was submitted to variance analysis for data with repeated measures testing effects of group, sex, experimental moment and interactions on variables. Correlations among variables were tested by multiple regressions and Pearson?s correlation deltas. The results show SPS was efficient in inducing stress and produce detectable alterations in several of the parameters investigated. Differences between social phobics and controls are significant for personality traits and, along time for psychophysiologic measures. Hormonal and immune alterations were more often associated to gender rather than to the group subjects belonged to, with men being more susceptible to the procedure. Also, immune changes were of small magnitude, usually affecting inespecific components of the response. Together, the results point to a relatively higher activation of the HPA-axis in social phobics, but one that does not correspond to immune responses of the same magnitude. Further studies with a larger sample and investigation of other parameters are necessary to better understand how social phobia affects the immune system of men and women and to investigate if the alterations can increase susceptibility to diseases in this group of individuals. Once this interaction is better understood it may provide the basis for an improved design to approach and elaborate prevention/intervention strategies and promote healthy behaviours.

ansiedade

anxiety

diferenças de gênero

eixo HPA

estresse

falar em público

fobia social

gender differences

HPA axis

humanos

humans

inespecific immune response

personality traits.

psiconeuroimunologia

Psychoneuroimmunology

public speaking

resposta imune inespecífica

social phobia

stress

traços de personalidade

Biomarcadores genotóxicos no monitoramento de estuários com diferentes níveis de contaminação utilizando peixes coletados in situ / Genotoxic biomarkers for monitoring estuarine with different levels of contamination using fish collected in situ.

Santos, Patricia Estevam dos

31 July 2009

Algumas áreas do canal de Piaçaguera, localizado na Baixada Santista, SP-Brasil, apresenta alto nível contaminação por hidrocarbonetos policíclicos aromáticos (HPA) entre outros contaminantes nos sedimentos. O objetivo do presente estudo foi verificar diferentes biomarcadores de exposição em bile e de efeitos genotóxicos em sangue de peixes, coletados in situ, que poderiam ser utilizados como ferramenta de monitoramento. O canal de Bertioga foi selecionado como região de referência. Embora não seja uma região sem nenhuma interferência de contaminantes, os sedimentos apresentam baixos valores para HPA, metais e atividade mutagênica. A espécie Mugil curema foi selecionada por ser freqüentemente encontrada em ambas as regiões de estudo. Observamos que os peixes coletados no canal de Piaçaguera apresentaram maior porcentagem de micronúcleos e danos ao DNA (ensaio cometa) no sangue quando comparados com a região de referência. Para o teste de micronúcleo, realizamos leituras de 1000 e 4000 células/indivíduo e não foram observadas diferenças estatísticas, sugerindo que o número de 1000 células poderia ser suficiente para gerar dados confiáveis para a espécie Mugil curema. A avaliação de mutagenicidade da bile foi realizada pelo teste Salmonella/microssoma combinado à extração de bile utilizando Blue rayon (BR) com as linhagens TA98, TA100 e YG1041 com e sem S9 (ativação metabólica). As maiores respostas mutagênicas foram observadas para os peixes coletados no canal de Piaçaguera. A mutagenicidade com a linhagem YG1041 na presença de S9 foi mais elevada quando comparado à mutagenicidade observada na ausência de S9 e também em comparação com a sua linhagem parental TA98, indicando a provável presença de compostos da classe das aminas aromáticas na bile como responsáveis pelos efeitos observados. A quantificação de metabólitos equivalentes de HPA foi realizada por HPLC/fluorescência na bile bruta e embora os resultados não se correlacionem com a mutagenicidade, altos níveis também foram encontrados para os peixes coletados no canal de Piaçaguera em comparação com Bertioga. O protocolo de amplificação do gene ras para a espécie Mugil curema foi estabelecido e os genes foram seqüenciados para verificação da presença de mutações. Não foram observadas mutações nos poucos peixes analisados e mais estudos são necessários para verificar a utilização deste biomarcador. O teste de micronúcleo, ensaio cometa e análise de mutagencidade em bile extraída por Blue rayon parecem ser ferramentas biológicas adequadas para monitoramento da qualidade ambiental de estuários contaminados. / Some areas of the Piaçaguera channel at Baixada Santista, SP, Brazil present high levels of polycyclic aromatic hydrocarbons (PAHs) among other contaminants in the sediment. The aim of the present study was to verify if biomarkers of exposure in bile and effect in blood of fishes collected in the field could be used as a monitoring tool. We selected Bertioga channel as a reference area. Although it is not a pristine area, the sediment presents low values of PAHs, metals and mutagenic activity. We selected the fish species Mugil curema, because they are frequently found in both areas during the entire year. We observed that the fish collected at the Piaçaguera channel showed a higher percentage of micronuclei and DNA damage (comet assay) in blood when compared to the Bertioga channel. The micronucleus readings were done in 1000 and 4000 cells/fish and no statistical difference was observed, suggesting that the number of 1000 cells would be sufficient to generate reliable data for the species Mugil curema , in the studied area. The mutagenicity of the bile was performed using the Salmonella/microsome assay combined with Blue rayon (BR) extraction with TA98, TA100 and YG1041 strains with and without rat liver S9. We observed that the mutagenic responses were higher in fish collected in Piaçaguera. The mutagenicity in YG1041 with S9 in fishes collected in the Piaçaguera channel was higher when compared to the mutagenicity observed in the absence of S9 and also higher than the response with the parental strain TA98. The results suggest that mutagenic polycyclic compounds, probably from the class of the aromatic amines are causing the observed effect. PAH metabolites-equivalent were also determined using HPLC/fluorescence in crude bile, and although the results did not correlate with the mutagenicity, higher levels were observed in fish collected in the Piaçaguera channel when compared to Bertioga. A protocol for amplification of the ras gene for the Mugil curema species was established and gene sequenced. No mutations were observed in the liver of the few fishes analyzed, and more studies are required to verify the utility of this biomarker in this fish. The micronuclei, comet assay and mutagenicity in bile extracted with blue rayon seem to be suitable biological tools to monitor the environmental quality of contaminated estuaries.

ras gene.

Bile de peixes

Biomarcadores

Biomarker

Blue rayon

Blue rayon

Comet assay

Ensaio cometa

Fish bile

Gene ras.

HPA

HPA

Metabolitos em bile

Micronucleus test

Mugil curema

Mugil curema

Mutagenicidade

Mutagenicity

PAH metabolites

Salmonella/microsome

Salmonella/microssoma

Teste de micronúcleo

Exposição gestacional ao etanol e avaliação de níveis de cortisol salivar em crianças em idade escolar / Gestational exposure to ethanol and assessment of salivary cortisol levels in school age children

Rodriguez, Isela Iveth González

30 October 2014

INTRODUÇÃO: Consumo de álcool na gestação é um sério problema de saúde pública envolvendo grande risco de embriotoxicidade e teratogenicidade fetal. Exposição fetal ao álcool causa liberação de glicocorticóides (GC) pela suprarrenal como conseqüência da ativação do eixo hipotálamo-hipófise-adrenal (HPA). Cortisol é o principal glicocorticóide endógeno capaz de interferir na atividade orgânica, influenciando a retroinibição do eixo HPA. Álcool consumido na gravidez pode alterar indiretamente o desenvolvimento fetal ao perturbar as interações hormonais normais dos eixos hipotálamo-pituitária-adrenal (HPA), hipotálamo-hipófise-tireoidal (HPT), hipotálamo-hipófise-gonadal (HPG), entre mãe e feto. OBJETIVOS: Comparar dosagens de cortisol salivar em crianças em idade escolar, com e sem histórico prévio de exposição intrauterina ao álcool, e sua relação com risco materno para Fetal Alcohol Spectrum Disorder (FASD) e intensidade do uso de álcool na gestação. METODOLOGIA: Amostra foi constituída de 76 pares de crianças e mães, de doze a treze anos de idade. Para análise do cortisol, foi coletada saliva e feitas análises por radioimunoensaio. RESULTADOS: Em relação à caracterização da amostra em função do risco materno se obteve significância para \"mãe praticante de religião\" (X²: 5,60; p=0,01). Associação significativa foi observada entre T-ACE positivo (Tolerance, Annoyed,Cut Down e Eye-Opener) na produção do Cortisol Awaking Response (CAR) e ritmo circadiano em função do sexo da criança (F: 9,26; p=0,003). Diferença significativa foi observada nas análises de níveis de cortisol em função do risco materno para FASD onde as análises de variância (t-tests) do cortisol ao despertar foram encontradas para \"CID positivo\" (Clasificação Internacional de doenças) (t:-2,659; p=0,01) e para cortisol aos 30 minutos depois de despertar em função de uso de álcool na gestação (t: -2,03 ; p=0,05). Em relação aos níveis de cortisol em função do uso de álcool na gestação, se obteve diferenças significativas para o cortisol aos 30 minutos depois de despertar (t: -2,03; p=0,05). Foram observadas diferenças significativas (p<0,01) para seguintes variáveis: níveis de cortisol em função do risco materno para FASD, álcool na gestação versus escore AUDIT (Alcohol Use Disorder Identification Test); Álcool na gestação versus T-ACE; Níveis de cortisol ao despertar versus Níveis de cortisol aos 30 min depois de despertar; Níveis de cortisol aos 30 min depois do despertar versus níveis de cortisol aos 60 min depois de despertar e Níveis de cortisol aos 60 min depois de despertar versus escore do AUDIT. As variáveis, álcool na gestação versus diagnóstico pelo CID, níveis de cortisol ao despertar versus escore do TACE, apresentaram significância (p=0,01). As análises com níveis de cortisol ao despertar versus níveis de cortisol aos 60 min depois de despertar; níveis de cortisol ao despertar versus escore do AUDIT-total; níveis de cortisol aos 30 min depois do despertar versus escore do T-ACE apresentaram significância estatística (respectivamente, p=0,03, p=0,04 e p=0,05). Em relação à avaliação da qualidade do sono em crianças com exposição pré-natal ao álcool por sexo, obteve-se significância para resistência em ir para a cama, para as meninas (p=0,01) e nas análises de correlação se observou diferenças significativas para ansiedade do sono versus níveis de cortisol salivar às 23 horas (p=0,01) e escore do SRQ total versus perturbação respiratória do sono (p=0,02). DISCUSSÃO: Se obteve uma associação entre uso de álcool na gestação e produção de cortisol salivar nos filhos, porém outras variáveis inerentes às mães podem influenciar no desenvolvimento do HPA e na produção de cortisol na pré-adolescência. CONCLUSÃO: Estes resultados podem contribuir para o melhor entendimento da fisiopatologia subjacente às manifestações clínicas de crianças expostas ao álcool durante a gestação e a fundamentar planos de prevenção para evitar que mulheres grávidas consumam álcool na gestação. / INTRODUCTION: Alcohol consumption during pregnancy is a serious public health problem, as it involves great risk related to fetal embryotoxicity and teratogenicity. Fetal alcohol exposure causes the release of glucocorticoids (GC) by the adrenal as consequence of activation of the hypothalamic-pituitary-adrenal (HPA) axis. Cortisol is the major endogenous glucocorticoid able to interfere with the organic activity, influencing retroinhibition of HPA axis. Furthermore, alcohol consumed during pregnancy can alter fetal development indirectly by disrupting the normal hormonal interactions of the hypothalamic-pituitary-adrenal axis (HPA), hypothalamic-pituitarytireoidal (HPT), and hypothalamic-pituitary-gonadal (HPG) between mother and fetus. OBJECTIVES: The objective of this research was to compare the measurements of salivary cortisol in school age children with and without previous history of intrauterine exposure to alcohol, and their relationship to maternal risk for Fetal Alcohol Spectrum Disorder (FASD) and the intensity of alcohol use during pregnancy. METHODOLOGY: The study sample consisted of 76 pairs of children and their mothers, between twelve and thirteen years old. For analysis of cortisol, saliva was collected and analyzes were made by radioimmunoassay method. RESULTS: Results show that, in relation to the characterization of the sample as a function of maternal risk for FASD, significance was obtained for the variable mother religious practice versus score of TACE (Tolerance, Annoyed,Cut Down e Eye-Opener) (X²: 5.60, p=0.01). Statistically significant association was observed between the covariate T-ACE and production of CAR (Cortisol Awaking Response) and circadian rhythm versus sex of the child (F: 9.26, p=0.003). Significant differences were also observed in the analysis of cortisol levels as a function of maternal risk for FASD for the test analysis of variance (t-tests) of cortisol after awakening versus \"negative CID\" and \"positive CID\" (International Clasification of Diseases) (t:-2.659; p=0.01) and cortisol at 30 minutes after awakening versus alcohol use during pregnancy (t:-2.03, p=0.05). In relation to cortisol levels due to the use of alcohol during pregnancy, significant differences were obtained for cortisol at 30 minutes after awakening versus alcohol use during pregnancy (t:-2.03, p=0.05). Significant differences (p<0.01) were found for variables: - cortisol levels as a function of maternal risk for FASD; - alcohol during pregnancy versus score of AUDIT (Alcohol Use Disorder Identification Test); - alcohol in pregnancy versus T-ACE; - cortisol levels after awakening versus cortisol levels at 30 min after awakening; - cortisol levels at 30 min after awakening versus cortisol levels at 60 min after awakening and cortisol levels at 60 min after awakening versus score of AUDIT. Analyses of alcohol during pregnancy versus mother diagnose CID (harmful use or dependence), and cortisol levels after awakening versus score of T-ACE showed significance (p=0.01). The analyses of cortisol levels at 60 min after awakening; cortisol levels after awakening versus AUDIT-total; cortisol levels at 30 min after awakening versus score of T-ACE were significant (respectively, p=0.03, p=0.04 and p=0.05). Regarding the assessment of sleep quality in children with prenatal exposure to alcohol by sex, significance was obtained for resistance to going to bed for female children (p=0.01) and through the analysis of correlation was observed significant results for anxiety sleep versus salivary cortisol levels at 23 hours (p=0.01) and score of mother SRQ total versus respiratory sleep disorder (p=0.02). DISCUSSION: An association was found between alcohol use during pregnancy and salivary cortisol in children of women who consumed alcohol during pregnancy, however other variables inherent to mothers could act in the development of the HPA and the production of cortisol in preadolescence. CONCLUSION: These results can contribute to a better understanding of the pathophysiology underlying the clinical manifestations of children exposed to alcohol during pregnancy and to establish a prevention plan to ensure that pregnant women do not consume alcohol during pregnancy.

Alcohol

Álcool

Alterações neuroendócrinas

Cortisol salivar

Diagnóstico psiquiátrico

Exposição fetal ao etanol

Fetal ethanol exposure

Gestação

HPA

HPA

Idade escolar

Neuroendocrine changes

Pregnancy

Psychiatric diagnosis

Radioimmunoassay (RAI)

Radioimunoensaio (RAI)

Salivary cortisol

School age

Biomarcadores genotóxicos no monitoramento de estuários com diferentes níveis de contaminação utilizando peixes coletados in situ / Genotoxic biomarkers for monitoring estuarine with different levels of contamination using fish collected in situ.

Patricia Estevam dos Santos

31 July 2009

Algumas áreas do canal de Piaçaguera, localizado na Baixada Santista, SP-Brasil, apresenta alto nível contaminação por hidrocarbonetos policíclicos aromáticos (HPA) entre outros contaminantes nos sedimentos. O objetivo do presente estudo foi verificar diferentes biomarcadores de exposição em bile e de efeitos genotóxicos em sangue de peixes, coletados in situ, que poderiam ser utilizados como ferramenta de monitoramento. O canal de Bertioga foi selecionado como região de referência. Embora não seja uma região sem nenhuma interferência de contaminantes, os sedimentos apresentam baixos valores para HPA, metais e atividade mutagênica. A espécie Mugil curema foi selecionada por ser freqüentemente encontrada em ambas as regiões de estudo. Observamos que os peixes coletados no canal de Piaçaguera apresentaram maior porcentagem de micronúcleos e danos ao DNA (ensaio cometa) no sangue quando comparados com a região de referência. Para o teste de micronúcleo, realizamos leituras de 1000 e 4000 células/indivíduo e não foram observadas diferenças estatísticas, sugerindo que o número de 1000 células poderia ser suficiente para gerar dados confiáveis para a espécie Mugil curema. A avaliação de mutagenicidade da bile foi realizada pelo teste Salmonella/microssoma combinado à extração de bile utilizando Blue rayon (BR) com as linhagens TA98, TA100 e YG1041 com e sem S9 (ativação metabólica). As maiores respostas mutagênicas foram observadas para os peixes coletados no canal de Piaçaguera. A mutagenicidade com a linhagem YG1041 na presença de S9 foi mais elevada quando comparado à mutagenicidade observada na ausência de S9 e também em comparação com a sua linhagem parental TA98, indicando a provável presença de compostos da classe das aminas aromáticas na bile como responsáveis pelos efeitos observados. A quantificação de metabólitos equivalentes de HPA foi realizada por HPLC/fluorescência na bile bruta e embora os resultados não se correlacionem com a mutagenicidade, altos níveis também foram encontrados para os peixes coletados no canal de Piaçaguera em comparação com Bertioga. O protocolo de amplificação do gene ras para a espécie Mugil curema foi estabelecido e os genes foram seqüenciados para verificação da presença de mutações. Não foram observadas mutações nos poucos peixes analisados e mais estudos são necessários para verificar a utilização deste biomarcador. O teste de micronúcleo, ensaio cometa e análise de mutagencidade em bile extraída por Blue rayon parecem ser ferramentas biológicas adequadas para monitoramento da qualidade ambiental de estuários contaminados. / Some areas of the Piaçaguera channel at Baixada Santista, SP, Brazil present high levels of polycyclic aromatic hydrocarbons (PAHs) among other contaminants in the sediment. The aim of the present study was to verify if biomarkers of exposure in bile and effect in blood of fishes collected in the field could be used as a monitoring tool. We selected Bertioga channel as a reference area. Although it is not a pristine area, the sediment presents low values of PAHs, metals and mutagenic activity. We selected the fish species Mugil curema, because they are frequently found in both areas during the entire year. We observed that the fish collected at the Piaçaguera channel showed a higher percentage of micronuclei and DNA damage (comet assay) in blood when compared to the Bertioga channel. The micronucleus readings were done in 1000 and 4000 cells/fish and no statistical difference was observed, suggesting that the number of 1000 cells would be sufficient to generate reliable data for the species Mugil curema , in the studied area. The mutagenicity of the bile was performed using the Salmonella/microsome assay combined with Blue rayon (BR) extraction with TA98, TA100 and YG1041 strains with and without rat liver S9. We observed that the mutagenic responses were higher in fish collected in Piaçaguera. The mutagenicity in YG1041 with S9 in fishes collected in the Piaçaguera channel was higher when compared to the mutagenicity observed in the absence of S9 and also higher than the response with the parental strain TA98. The results suggest that mutagenic polycyclic compounds, probably from the class of the aromatic amines are causing the observed effect. PAH metabolites-equivalent were also determined using HPLC/fluorescence in crude bile, and although the results did not correlate with the mutagenicity, higher levels were observed in fish collected in the Piaçaguera channel when compared to Bertioga. A protocol for amplification of the ras gene for the Mugil curema species was established and gene sequenced. No mutations were observed in the liver of the few fishes analyzed, and more studies are required to verify the utility of this biomarker in this fish. The micronuclei, comet assay and mutagenicity in bile extracted with blue rayon seem to be suitable biological tools to monitor the environmental quality of contaminated estuaries.

Bile de peixes

Biomarcadores

Blue rayon

Ensaio cometa

Gene ras.

HPA

Metabolitos em bile

Mugil curema

Mutagenicidade

Salmonella/microssoma

Teste de micronúcleo

ras gene.

Biomarker

Blue rayon

Comet assay

Fish bile

HPA

Micronucleus test

Mugil curema

Mutagenicity

PAH metabolites

Salmonella/microsome

The impact of serotonergic and dopaminergic genetic variation on endophenotypes of emotional processing

Armbruster, Diana

29 December 2010

Decades of research in quantitative genetics have found substantial heritability for personality traits as well as for mental disorders which formed the basis of the ongoing molecular genetic studies that aim to identify genetic variations that actually contribute to the manifestation of complex traits. With regard to psychological traits, genetic variation impacting neurotransmitter function have been of particular interest. Additionally, the role of environmental factors including gene × environment interactions has been further investigated and the impor-tance of developmental aspects has been stressed. Furthermore, endophenotypes which link complex traits with their respective biological underpinnings and thus bridge the gap between gene and behaviour have begun to be included in research efforts. In accordance with this approach, this thesis aims to further examine the influence of genetic variation impacting serotonergic and dopaminergic functioning on endophenotypes of anxiety-related behaviour. To this end, two well established paradigms – the acoustic startle reflex and the cortisol stress response – were employed. Both show considerable interindividual variation which has been found in quantitative genetic studies to be at least partly based on genetic factors. In addition, the neural circuits underlying these endophenotypes are relatively well understood and thus reveal references for the detection of associated genetic influences. The results of this thesis associate the overall startle magnitude in two independent samples of young adults with a polymorphism in the promoter region of the serotonin transporter (5-HTT) gene (5-HTTLPR): Carriers of the short (S) allele which results in a reduced gene ex-pression showed a stronger startle magnitude which is in line with numerous findings linking the S allele to increased measures of negative emotionality. In addition to 5-HTTLPR, the effects of past stressful life events on the startle response were investigated: Participants who had recently experienced at least one stressful life event exhibited stronger startle responses and reduced habituation of the startle reflex although there was no 5-HTTLPR × environment inter-action effect. A third study revealed independent and joint effects of 5-HTTLPR and a poly-morphism in the dopamine receptor 4 gene (DRD4) in the same sample of young adults with regard to the cortisol stress response with carriers of the DRD4 7R allele which has been associ-ated with higher scores in sensation seeking, showing reduced cortisol responses. In addition, a 5-HTTLPR × DRD4 interaction effect emerged: 5-HTTLPR long (L) allele carriers showed the lowest cortisol response but only when they possessed at least one copy of the DRD4 7R allele. Moreover, in a fourth study a life span approach was taken and the influence of a further important serotonergic polymorphism which impacts the functioning of tryptophan hydroxylase 2 (TPH2), the rate limiting enzyme in the biosynthesis of serotonin, on interindividual differences in the startle response was investigated in three different age samples: children, young adults and older adults. There was a sex × TPH2 genotype interaction effect in a sample of young adults on the overall startle response while there was no effect of TPH2 in children or older adults. The last study of this thesis presents findings regarding the influence of two dopaminergic polymorphisms in genes encoding the enzyme catechol-O-methyltransferase (COMT) and the dopamine transporter (DAT), respectively, which both terminate dopamine signalling and are thus important regulators of dopaminergic neurotransmission, on the startle reflex in older adults. COMT met/met homozygotes showed the strongest and val/val homozygotes displayed the smallest startle magnitude which is in line with findings linking the COMT met allele to increased scores of anxiety related traits and disorders. Regarding DAT, participants homozygous for the 10R allele, which had previously associated with attention-deficit hyperactivity disorder, showed a stronger overall startle response. In sum, this thesis comprises data on interindividual differences in an electrophysiological and a hormonal endophenotype across the life span and their association with serotonergic and dopaminergic function based on genetic variation. One major finding is the clear evidence for the influence of serotonergic polymorphisms on the startle response in young adults while in contrast in older adults genetic variation in the dopaminergic system exerted considerable influence. These differences might be due to developmental processes in the different stages of life although cohort effects and effects of different recruitment strategies can also not be ruled out. Furthermore, there were significant differences regarding the genetic influence on the acoustic startle reflex and cortisol stress response in one and the same sample which might be due to methodological differences of the two paradigms as well as differences in their underlying neuronal circuits. In conclusion, this thesis supports the acoustic startle reflex and the cortisol stress response as valuable endophenotypes and thus indicators for underlying neurobiological circuits although some methodological issues remain. It also highlights the importance of taking developmental factors and changes over the course of life into account. Finally, this thesis emphasizes the necessity to include reliably and validly assessed past experienced events in molecular genetic studies in order to understand the interplay between genetic and environmental factors in shaping (endo)-phenotypes.

Serotonin

Dopamin

Furcht

Angst

Stress

5-HTTLPR

TPH2

COMT

DAT

Startle-Reflex

HPA-Achse

kritische Lebensereignisse

serotonin

dopamine

fear

anxiety

stress

5-HTTLPR

TPH2

COMT

DAT

startle reflex

HPA axis

critical life events

ddc:155

rvk:CZ 1000

Analyzing pathways from childhood maltreatment to internalizing symptoms and disorders in children and adolescents (AMIS)

White, Lars O., Klein, Annette M., Kirschbaum, Clemens, Kurz-Adam, Maria, Uhr, Manfred, Müller-Myhsok, Bertram, Hoffmann, Katrin, Sierau, Susan, Michel, Andrea, Stalder, Tobias, Horlich, Jenny, Keil, Jan, Andreas, Anna, Resch, Leonhard, Binser, Martin J., Costa, Anna, Giourges, Elena, Neudecker, Eva, Wolf, Christiane, Scheuer, Sandra, Ising, Marcus, Klitzing, Kai von

10 June 2015

Background: Effective interventions for maltreated children are impeded by gaps in our knowledge of the etiopathogenic mechanisms leading from maltreatment to mental disorders. Although some studies have already identified individual risk factors, there is a lack of large-scale multilevel research on how psychosocial, neurobiological, and genetic factors act in concert to modulate risk of internalizing psychopathology in childhood following maltreatment. To help close this gap, we aim to delineate gender-specific pathways from maltreatment to psychological disorder/resilience. To this end, we examine the interplay of specific maltreatment characteristics and psychological, endocrine, metabolomic, and (epi-)genomic stress response patterns as well as cognitive-emotional/social processes as determinants of developmental outcome. Specifically, we will explore endocrine, metabolomic, and epigenetic mechanisms leading from maltreatment to a higher risk of depression and anxiety disorders.

Misshandlung

Entwicklungspsychopathologie

Störungen

Entwicklungsabläufe

neuroendokrine Funktion

HPA-Achse

Gen-Umwelt-Interaktionen

kognitiv-emotionale Strategien

maltreatment

developmental psychopathology

internalizing disorders

developmental pathways

neuroendocrine functioning

HPA axis

gene-environment interaction

cognitive-emotional strategies

ddc:150

Aufmerksamkeitsdefizit-/Hyperaktivitätsstörung (ADHS) im Erwachsenenalter: Stressreagibilität und Stressbewältigung unter Laborbedingungen und im Alltag / Attention-deficit/hyperacitvity disorder (ADHD) in adulthood: Stressreagibility and stress-related coping under laboratory conditions and in everyday life

Lackschewitz, Halina

29 October 2008

No description available.

150 Psychologie

Mathematics and Computer Science

Erwachsene

Stressreaktion

Stressbewältigung

Psychophysiologie

HPA-Achse

Trier Social Stress Test

attention-deficit/hyperactivity disorder

adults

stress response

coping

psychophysology

HPA axis

Trier Social Stress Test

77.70 Klinische Psychologie

77.50 Psychophysiologie

FA Psychologie