Caracterização da resposta inflamatória no paciente com infecção por HIV/aids e sepse / Inflammatory response characters in patients with sepsis and HIV infection/AIDS

João Manoel da Silva Júnior

29 August 2011

Sepse é uma resposta sistêmica do hospedeiro à infecção caracterizada por alterações clínicas e laboratoriais. Em pacientes imunodeprimidos, tais alterações podem não ser nem sensíveis nem específicas para causas infecciosas, assim como agentes etiológicos, focos primários de infecção e evolução clínica podem ser distintos. A identificação de marcador laboratorial de sepse poderia auxiliar no diagnóstico, tratamento e avaliação prognóstica dessa população. O objetivo do presente estudo foi avaliar a evolução clínica, laboratorial e de marcadores inflamatórios em pacientes com infecção pelo HIV/aids e sepse, comparando-os a pacientes sépticos não infectados pelo HIV. Tratou-se de estudo prospectivo observacional de pacientes adultos com sepse grave ou choque séptico associados ou não à infecção pelo HIV/aids e admitidos em unidade de terapia intensiva. Os pacientes foram avaliados à admissão, no terceiro e sétimo dias de internação na unidade de terapia intensiva quanto a parâmetros clínicos, laboratoriais e escores de gravidade, assim como os seguintes marcadores inflamatórios: proteína c-reativa (PCR), procalcitonina (PCT), interleucina-6, interleucina-10 e TNF-. Os pacientes também foram avaliados quanto à sobrevida por ocasião da alta da hospitalar, aos 28 dias e após seis meses de inclusão no estudo. O estudo envolveu 58 pacientes consecutivamente com sepse grave e/ou choque séptico, sendo 36 com infecção pelo HIV/aids e 22 com sorologia negativa para HIV. Todos os pacientes com infecção pelo HIV preencheram critérios para aids (CDC/2008). Os pacientes sépticos com infecção pelo HIV/aids apresentaram maior ocorrência de infecções pulmonares (83,3% versus 40,9% p=0,001) e de etiologia fúngica (44,4% versus 9,1% p=0,001). Apesar dos grupos serem semelhantes em termos de xii gravidade, a mortalidade hospitalar e após 6 meses da admissão foi maior nos pacientes com infecção pelo HIV/aids em comparação aos pacientes não infectados pelo HIV (55,6 versus 27,3% p=0,03, e 58,3 versus 27,3% p=0,02, respectivamente). As concentrações iniciais de PCR e PCT foram mais baixas nos pacientes sépticos com aids que em pacientes soronegativos para HIV (130 versus 168 mg/dL p= 0,005 e 1,19 versus 4,06 ng/mL p= 0,04, respectivamente), com tendência a diminuição progressiva nos pacientes sobreviventes. Não houve diferença significativa entre as concentrações iniciais de IL-6 e TNF- em pacientes com ou sem infecção pelo HIV/aids. As concentrações iniciais de IL-10 foram maiores (4,4 pg/mL versus 1,0 pg/mL; p=0,005) e apresentaram melhor poder em predizer o óbito (área sob a curva ROC =0,74) em pacientes sépticos com infecção pelo HIV/aids. Concluindo, a evolução da sepse foi mais grave em pacientes com aids, sendo mais comuns o foco pulmonar e a etiologia fúngica. Além disso, os marcadores de resposta inflamatória apresentaram concentrações menos elevadas na população séptica soropositiva para HIV, exceto pela IL10, que também mostrou ter importante poder prognóstico nesta população / Sepsis is a systemic host response to infection characterized by clinical and laboratory findings. In immunosuppressed patients, these findings may not be sensitive or specific for infectious insults, and etiologic agents, primary foci of infection and clinical outcome may also be different. The identification of a laboratory marker of sepsis could help in diagnosis, treatment and assessment of prognosis for that population. Therefore, the aim of this study was to evaluate the course of clinical, biochemical and inflammatory markers in HIV-infected and HIV-uninfected patients with sepsis. The study was prospective observational in adult patients with severe sepsis or septic shock associated or not to HIV infection/AIDS, and admitted to intensive care unit. Patients were evaluated on the first, third and seventh day of admission in relation to clinical and laboratory parameters, severity scores, besides the following inflammatory markers: c-reactive protein (CRP), procalcitonin (PCT) interleukin-6, interleukin-10 and TNF-. Patients were evaluated according survival at hospital discharge and after six months of admission on the study. The study involved 58 consecutive patients with severe sepsis or septic shock, 36 with HIV infection/AIDS and 22 non HIV-infected. All patients with HIV infection met criteria for AIDS (CDC/2008). The septic patients with HIV infection/AIDS presented more pulmonary infections (83.3% versus 40.9% p = 0.001) and fungal etiology (44.4% versus 9.1% p = 0.001). Although groups presented similar severity, the mortality rate at hospital discharge, 28 days and 6 months after admission was higher in patients with AIDS compared to patients without HIV infection (55.6 versus 27 3% p=0.03, and 58.3 versus 27.3% p=0.02, respectively). The initial concentrations of CRP and PCT were lower in septic patients with AIDS than in HIV-negative patients (130 versus xiv 168 mg/dL p= 0.005 and 1.19 versus 4.06 ng/mL p=0.04, respectively), with tendency to a progressive decrease in surviving patients. There was no significant difference between the initial concentrations of IL-6 and TNF- in patients with or without HIV infection/AIDS. The initial concentrations of IL-10 were higher (4.4 pg/mL versus 1.0 pg/mL, p = 0.005) and also they were better able to predict death (area under ROC curve = 0.78) in septic patients with HIV infection/AIDS. Concluding, the sepsis course was more severe in patients with AIDS, with more common pulmonary focus and fungal etiology. Furthermore, the markers of inflammatory response showed lower concentrations in septic HIV infected patients, except for IL10, which proved to have a significant prognostic power in this population

Calcitonina/sangue

HIV

Inflamação

Interleucina-10

Letalidade

Marcadores biológicos

Proteína C-reativa

Sepse

Síndrome de imunodeficiência adquirida

Acquired immunodeficiency syndrome

Biological markers

C - reactive protein

Calcitonin/blood

HIV

Inflammation

Interleukin-10.

Mortality

Sepsis

Avaliação nutricional de pacientes etilistas crônicos com ou sem doença pancreática / Nutritional assessment of chronic alcoholic patients with and without pancreatic disease

Maria Beatriz Sobral de Oliveira

25 October 2010

A pancreatite crônica alcoólica (PCA) tem o álcool como seu principal fator etiológico, a relação entre ingestão de álcool e estado nutricional é complexa e as características nutricionais dos portadores de PCA são pouco conhecidas. Neste trabalho, foram avaliados três grupos de pacientes do sexo masculino, o primeiro (A) com 20 pacientes com PCA, o segundo (B) com 12 etlistas crônicos não pancreatopatas e não hepatopatas e o terceiro (C) com 16 indivíduos não etlistas, não pancreatopatas e não hepatopatas. Para analisar os três grupos utilizaram-se a avaliação antropométrica, a quantificação da ingestão alcoólica, quando existente, o inquérito dietético obtido por Recordatório de 24 horas, a composição corpórea, obtida por bioimpedância elétrica, exames séricos relacionados à avaliação hepática e pancreática, dosagem de vitaminas e de sais minerais, além de marcadores inflamatórios, como proteína C reativa, seroamiloide A e leptina, além de exames de imagem, como ultrassonografia abdominal e/ou tomografia computadorizada de abdômen. A PCA (Grupo A) não se associou à queda da ingestão dietética, porém houve redução da massa magra, evidenciando desnutrição protéica; os etilistas sem pancreatite (Grupo B) apresentaram menor massa magra em relação aos pacientes do grupo C e foi possível demonstrar que a composição corpórea e o perfil inflamatório são distintos e relevantes, não apenas na PCA (Grupo A), mas também nos etilistas sem lesão pancreática (Grupo B), que também devem ser melhor estudados e acompanhados ao longo do seu curso clínico. Em síntese, encontraram-se evidências de subnutrição e aberrações metabólicas tanto nos casos de alcoolismo com lesão pancreática quanto nos etilistas aparentemente sem lesão pancreática ou hepática. Achado até o momento não relatado pela literatura / Alcoholic pancreatitis has alcohol as the primary etiologic factor. The relationship between alcohol intake and nutritional status is complex and the nutritional characteristics of patients with this disease are unknown. In this study, we evaluated three groups of male patients, one (A) with 20 patients with alcoholic pancreatitis, another (B) with 12 alcoholics without pancreatic or liver disease and the last (C) with 16 non - alcoholics , free from any systemic disease or organ insufficiency. To analyze the three groups, we used anthropometric assessment, quantification of alcohol intake, dietary recall, body composition estimated by bioimpedance analysis, biochemical tests related to liver and pancreatic function, dosage of vitamins and minerals, inflammatory markers namely C-reactive protein, leptin and serum amyloid A, in addition to imaging studies such as abdominal ultrasonography and computed tomography of the abdomen whenever required. Group A was not associated with decrease in food intake, but there was a reduction in lean body mass, indicating undernutrition. Alcoholics without pancreatitis (group B) also showed lower lean mass compared to patients in group C, demonstring that changes in body composition and inflammatory status are distinct and relevant also in alcoholics without pancreatic injury (Group B). They should be better studied and monitored throughout their clinical course. In synthesis evidence of undernutrition and metabolic aberrations were demonstrated in both alcoholism with pancreatic damage and in nominally healthy alcoholics, a finding not hitherto reported in the literature

Bioimpedância

Comportamento alimentar

Doença crônica

Pancreatite alcoólica

Proteína C-reativa

Vitamina B 12

Vitamina D

Alcoholic pancreatitis

Bioimpedance

C-reactive protein

Chronic disease

Feeding behaviour

Vitamin B12

Vitamin D

Efeitos pleiotrópicos com reduções equivalentes do LDL-colesterol: estudo comparativo entre sinvastatina e associação sinvastatina/azetimiba / Pleiotropic effects with equivalent LDL-cholesterol reduction: comparative study between simvastatin and simvastatin/ezetimibe coadministration

Daniel Branco de Araujo

16 August 2007

Introdução: A associação de uma estatina com ezetimiba é tão eficaz quanto altas doses da mesma estatina na redução do LDL-colesterol. Os efeitos que não dependem dessa redução são chamados de pleiotrópicos, entre os quais podemos citar: melhora da função endotelial, efeitos anti-oxidantes, efeitos anti- inflamatórios, entre outros. Objetivo: comparar a ação de dois esquemas de tratamento que obtêm reduções equivalentes de LDL-colesterol (sinvastatina 80 mg ao dia e associação sinvastatina 10mg/ezetimiba 10 mg ao dia), sobre os efeitos pleiotrópicos: inflamação, função endotelial e oxidação da LDL. Métodos: estudamos 23 pacientes randomizados e na forma de cross-over 2x2. A inflamação foi mensurada através da PCR-us, a função endotelial por meio de ultra-sonografia e a oxidação de LDL pelas dosagens de LDL eletronegativa (LDL-) e do anticorpo anti-LDL-. Resultados: A redução do LDL-colesterol foi similar nos dois grupos (45,27% no grupo sinvastatina/ezetimiba (p<0,001) e 49,05% no grupo sinvastatina (p<0,001), sem diferença entre os tratamentos (p=0,968)). Os dois grupos apresentaram melhora da função endotelial (3,61% no grupo sinvastatina/ezetimiba (p=0,003) e 5,08% no grupo sinvastatina (p<0,001), não houve diferença entre os tratamentos (p=0,291)). Houve melhora nos níveis da PCR-us (redução de -22,8% no grupo sinvastatina/ezetimiba (p=0,004) e de 29,69% no grupo sinvastatina (p=0,01), sem diferenças entre os tratamentos (p=0,380)). Não houve redução significativa da LDL-. Ocorreu aumento na concentração do anticorpo anti-LDL eletronegativa apenas no grupo sinvastatina (p=0,045). Conclusões: as duas formas de tratamento são eficazes na melhora da função endotelial e dos níveis de PCR-us. Somente com o uso da sinvastatina em alta dose houve aumento nos níveis de anticorpos anti-LDL-. / Introduction: The co-administration of a statin with ezetimibe is as effective as high doses of the same statin in the reduction of the LDL-cholesterol. The effects which don´t depend of this reduction are called pleiotropic effects, some among them can be cited: endothelial function improvement, antioxidative and anti-inflammatory effects. Objective: compare the effectiveness of these two different treatments that obtain equivalent reductions of LDLcholesterol (simvastatin 80 mg once a day and co-administration of simvastatin 10 mg once a day and ezetimibe 10 mg once a day), about pleiotropic effects: inflammation, endothelial function and LDL oxidation. Methods: we have studied 23 randomized patients in a 2x2 cross-over study. Inflammation was measured by high-sensitive C reactive protein, endothelial function by echocardiography and LDL oxidation by electronegative LDL and electronegative anti-LDL antibodies levels. Results: the LDL-cholesterol was similar between the two groups (45,27% reduction in the simvastatin/ezetimibe group (p<0,001) and 49,05% reduction in the simvastatin group (p<0,001); no difference between treatments was found (p=0,968). The two groups had improvement in endothelial function (3,61% in the simvastatin/ezetimibe group (p=0,003) and 5,08% in the simvastatin group (p<0,001)), no differences was found between the two groups (p=0,291). High-sensitive C reactive protein had a 22,8% reduction in the simvastatin/ezetimiba group (p=0,004) and 29,69% reduction in the simvastatin group (p=0,01), with no significative difference in any of the two treatments (p=0,380). There was no significative difference in LDL- levels. The anti-LDL- antibodies concentration was increased only in the simvastatin group (p=0,045). Conclusion: the two forms of treatments presented some similar pleiotropic effects - improvement in endothelial function and decreased hs-CRP levels. Only with a high simvastatim dose the anti-LDL- antibodies concentration was increased.

Endotélio/efeitos de drogas

Hipercolesterolemia

Lipoproteínas LDL/efeito de drogas

Oxidação

Proteína C-reativa/efeitos de drogas

C-Reactive protein/drug effects

Endothelium/drug effects

Hypercholesterolemia

Lipoproteins LDL/drug effects

Oxidation

Tomografia computadorizada de placa carotídea: uma comparação com a histologia / Carotid Plaque Tomography: a histologic comparison

Gustavo Wruck Kuster

22 October 2015

As características morfológicas da placa aterosclerótica têm sido sugeridas como componentes auxiliares à estenose, na avaliação de risco de acidente vascular cerebral (AVC), em pacientes com doença aterosclerótica carotídea sintomática. O objetivo desse estudo foi comparar as características da placa aterosclerótica de carótida pelo método de tomografia computadorizada com a análise histológica. Foram incluídos 19 pacientes com doença carotídea sintomática submetidos à TC de placa carotídea antes da realização de endarterectomia carotídea. Uma comparação sistemática entre a TC e a histologia foi realizada para determinar a correspondência entre os componentes da placa seguindo a classificação da \"American Heart Association\". Foi considerada placa vulnerável o tipo VI. A histologia foi realizada 5 (±2) dias após a TC. Os laudos (radiologia e patologia) foram comparados pelo investigador principal. Foi dosada a proteína C-Reativa (PCR) sérica e realizada avaliação do desempenho do PCR para detectar placa vulnerável, considerando como padrão-ouro o resultado da avaliação histológica. Foi avaliada a relação entre PCR e o tempo entre o evento e a cirurgia. Para tipo de placa aterosclerótica, foi encontrada uma acurácia de 84,2% (IC 95%: 82,8% a 85,6%), da tomografia em relação à histologia. A concordância para identificar ruptura de capa fibrosa com acurácia 94,7% (IC 95%: 94,2% a 95,3%), e, para calcificação, com acurácia 89.5% (IC 95%: 88,5% a 90,5%), foi considerada alta, e moderada para identificar hemorragia (68% acurácia). A concordância é moderada entre PCR de alto risco e placa vulnerável, e não há relação entre PCR, placa vulnerável e tempo de cirurgia. A tomografia de placa carotídea é um bom método não invasivo para detecção de vulnerabilidade da placa, identificação de ruptura de capa fibrosa e calcificação. Na nossa amostra, a concordância entre PCR alto risco e vulnerabilidade foi moderada, e não observamos relação entre vulnerabilidade, PCR e tempo entre o evento e a endarterectomia / Plaque morphologic characteristics have been suggested as an auxiliary component to luminal narrowing for assessing the risk of stroke associated with carotid atherosclerotic disease (CAD). The purpose of this study was to evaluate the ability of CT angiography (CTA) to categorize carotid artery atherosclerotic plaques (CAP) features in symptomatic patients submitted to endarterectomy according to the AHA histological classification. Nineteen patients with symptomatic CAD who underwent carotid CTA before endarterectomy were enrolled in a prospective study. A systematic comparison of CTA images with histological sections was performed to determine the CT attenuation associated with each component of the CAP. Histologic examination was performed 5 ± 2 days after the CTA. The neuroradiologist\'s reading of these analyses was compared with the histological slides interpretation performed by the same pathologist according to the CAP features following the AHA classification. The type VI plaque was considered as complicated. The two experts were blinded to each other\"s assessments. We performed C reactive Protein (CRP) and the CRP capacity to detect plaque vulnerability, considering histologic features as gold standard and the relation between CRP and time (event-surgery). There was an overall 84.2% (CI 95%: 82.8% a 85.6%), accuracy agreement in CAP classification between CTA and histological analysis. (Tab.1) The agreement between these two methods for the presence of calcification (Tab.2) in the CAP (accuracy 89.5%), and for categorizing the rupture of fibrous cap (accuracy 94,7), was excellent. (Tab. 3). CTA is not a good method to detect hemorrhage (Tab.4). High-risk CRP had moderate power to predict \"complicated plaque\" (Tab. 4) even as high risk CRP + CTA (Tab.5), There are No relation between CRP, complicated plaque and event to surgery delay. (Tab.6) CTA is a non-invasive tool that may help neurologists to categorize CAP features and potentially predict the risk of ischemic stroke in symptomatic CAD patients, and CRP could not be a good marker to complicated carotid plaque

Acidente vascular cerebral

Endarterectomia

Histologia

Placa aterosclerótica

Proteína C-reativa

Tomografia computadorizada por raios X

Atherosclerotic plaque

C-reactive protein

Carotid CT

Endarterectomy

Histological analysis

Tomography X-Ray computed

Subjective Well-Being and Biomarkers of Health : The Relationship between Subjective Well-Being, The immune system and Hypothalamic-Pituitary Adrenal Axis Activation

Catibusic, Sanda-Wictoria

January 2017

An association between inflammation and mood deterioration has been proposed as a potential explanatory mechanism underlying many pathologies. Previous research attributes this consistently reoccurring connection between inflammation and psychopathology that is often reported within the literature, to a relationship between the HPA axis, the body’s stress response system and the immune system. There is evidence of a bidirectional feedback loop between end-products of the immune system and the HPA-axis such as cytokines and cortisol. This is supported by research reporting that components of subjective well-being such as positive affect, optimism and life satisfaction can produce beneficial health outcomes by potentially targeting this feedback loop. The present longitudinal study tested if higher positive affect independently corresponds to lower levels of inflammatory markers Interleukin-6 (IL-6) and C-reactive protein (CRP) and HPA axis marker cortisol. The study further tested if higher subjective well-being decreases levels of IL-6 and CRP as well as cortisol. The study employed a subsample of participants from the Midlife in Japan (MIDJA) Biomarker project (n=174) that underwent testing at two separate time points across a period of 4 years. The data included subjective well-being, positive affect, IL-6, CRP, cortisol, perceived stress, neuroticism and demographic variables. Positive affect was not associated with any inflammatory marker or cortisol. Subjective well-being had no effect on CRP but reduced IL-6 and cortisol even when controlling for all control and demographic variables. It is concluded that subjective well-being may be linked to lower inflammation and HPA axis activity. / Ett samband mellan inflammation och sjukdomsbeteende har föreslagits som en förklaringsmekanism bakom förekomsten av många patologier. Den konsekventa anknytningen mellan inflammation och psykopatologi som många tidigare studier demonstrerat innebär ett samband mellan immunsystemet och HPA-axeln som är den struktur som utgör kroppens svar på stressorer. Det finns tecken på en återkopplingsslinga mellan slutprodukter av det immunologiska systemet och HPA-axeln såsom cytokiner och kortisol. Detta har stöd i tidigare forskning som rapporterat att komponenter av subjektivt välbefinnande så som positiv affekt, optimism och livstillfredställelse kan medföra positiva hälsoutfall genom att potentiellt influera denna återkopplingsslinga. Förevarande longitudinella studie testar om högre positiv affekt leder till lägre nivåer av de inflammatoriska markörerna interleukin-6 (IL-6) och C-reaktivt protein (CRP) samt HPA-axel markören kortisol. Studien testar vidare även om högre subjektivt välbefinnande leder till lägre nivåer av IL-6, CRP och kortisol. Deltagarna är ett subsampel från Biomarkerprojektet (n = 174) inom Midlife in Japan (MIDJA) som genomgick testning vid två separata tidpunkter över en period av 4 år. Data består av subjektivt välbefinnande, positiv affekt, IL-6, CRP, kortisol, upplevd stress, neuroticism samt demografiska variabler. Positiv affekt hade ingen signifikant effekt på någon av de inflammatoriska markörerna eller kortisol. Subjektivt välbefinnande hade inte någon signifikant effekt på CRP men reducerade signifikant IL-6 och kortisol och dessa effekter förblev signifikanta efter kontroll för samtliga kontroll och demografiska variabler. Följaktligen dras slutsatsen att subjektivt välbefinnande kan leda till lägre inflammation och HPA-axel aktivitet.

Subjective well-being

Positive affect

biomarkers

inflammatory cytokines

HPA axis

Interleukin 6

C-reactive protein

Cortisol

Subjektivt välbefinnande

Positiv affekt

biomarkörer

inflammatoriska cytokiner

HPA- axeln

Interleukin-6

C-reaktivt protein

Kortisol

Psychology

Psykologi

AVALIAÇÃO DOS NÍVEIS DE ALBUMINA MODIFICADA PELA ISQUEMIA, UM NOVO BIOMARCADOR DE ESTRESSE OXIDATIVO, EM PACIENTES COM ARTRITE REUMATOIDE / ASSESSMENT OF ISCHEMIA- MODIFIED ALBUMIN LEVELS, A NOVEL OXIDATIVE STRESS BIOMARKER, IN PATIENTS WITH RHEUMATOID ARTHRITIS

Leitemperguer, Michele Rodrigues

15 January 2013

Rheumatoid arthritis (RA) is a chronic inflammatory, autoimmune disease, characterized by peripheral and symmetrical polyarthritis that leads to joint destruction and deformity due to erosion of cartilage and bone. This is a common disease that affects approximately 1% of the world population and is more common in women than men, however, its peak incidence occurs between the fourth and sixth decades of life. Large amounts of reactive oxygen species (ROS) have been identified in the synovial fluid of RA patients, and such large amounts may lead to oxidative damage of hyaluronic acid, lipid, cartilage matrix and DNA. The accumulation of ROS in the cells, also serves as major intracellular signaling molecules that amplify the inflammatory response synovium proliferative. The objective of this study was to evaluate the levels of ischemia-modified albumin (IMA) and also other markers of oxidative stress and inflammation in 16 patients with RA and 20 healthy controls. IMA levels were significantly higher in RA patients than healthy controls (0.495 ± 0.01 vs 0.433 ± 0.02 ABSU, P=0.038). No significant differences were observed for the other markers studied. Thus it was concluded that besides RA being related to inflammation, elevated levels of IMA in RA patients suggest that this pathology promotes increased oxidative stress. / A artrite reumatoide (AR) é uma doença inflamatória crônica, de caráter autoimune, caracterizada por poliartrite periférica e simétrica, que leva à deformidade e destruição das articulações devido à erosão da cartilagem e do osso. Esta é uma doença comum que afeta aproximadamente 1% da população mundial, sendo mais frequente em mulheres do que nos homens, no entanto, seu pico de incidência ocorre entre a quarta e sexta décadas de vida. Grandes quantidades de espécies reativas de oxigênio (EROs) foram identificadas no fluido sinovial de pacientes com AR, e essa grande quantidade pode levar a dano oxidativo ao ácido hialurônico, lipídios, matriz da cartilagem e ao DNA. O acumulo de EROs nas células, também serve como importantes moléculas sinalizadoras intracelulares que amplificam a resposta inflamatória - proliferativa sinovial. Assim, o objetivo deste estudo foi avaliar os níveis de albumina modificada pela isquemia (IMA) e outros marcadores de estresse oxidativo e inflamação em 16 pacientes com AR e 20 controles saudáveis. Os níveis de IMA foram significativamente maiores no grupo de pacientes com AR do que os controles saudáveis (0.495 ± 0.01 vs 0.433 ± 0.02 ABSU, P=0.038). Não foram observadas diferenças significativas para os outros marcadores estudados. Desta forma, foi possível concluir que além da AR estar relacionada com a inflamação, os níveis elevados de IMA em pacientes com AR, sugerem que esta patologia promova o aumento do estresse oxidativo.

Artrite reumatoide

Espécies reativas de oxigênio

Albumina modificada pela isquêmia

Proteína C-reativa

Rheumatoid arthritis

Reactive oxygen species

Ischemia-modified albumin

C-reactive protein

Advanced oxidation protein products

CNPQ::CIENCIAS BIOLOGICAS::FARMACOLOGIA

Low-grade inflammation in depression, anxiety and sleep disturbances

Liukkonen, T. (Timo)

06 December 2011

Abstract Depression, anxiety and sleep disorders have been reported to be associated with low level of inflammation, i.e., low-grade inflammation, but mainly in males. The evidence has mainly been based on laboratory or clinical studies with small sample sizes or epidemiological studies with elderly subpopulations. In this study the association of low-grade inflammation with depression, anxiety, and sleep disturbances was investigated using the Northern Finland 1966 Birth Cohort (NFBC 1966). In women, the effect of hormonal factors, menopause and the use of oral contraceptives/hormone replacement therapy on the association between low-grade inflammation and depression was also studied by using the Pieksämäki Study data. In 31-year follow-up of NFBC 1966 (N=6007), the depressive and anxiety symptoms were assessed by Hopkins Symptom Checklist-25 (HSCL-25) and sleep disorders by 15-D questionnaires, while the marker of low-grade inflammation, plasma concentration of high sensitivity C-reactive protein (hs-CRP), was measured. In the Pieksämäki study a representative sample of inhabitants in the town of Pieksämäki were invited to clinical examination. Depressive symptoms were obtained by Beck’s Depression Inventory-21, and hs-CRP was measured (512 women). The results of this study revealed that at epidemiological level, elevated hs CRP levels of &#8805;1.0 mg/L increased the probability of current depressive symptoms of single depressive episode in the two highest subgroups (i.e., HSCL-25 mean scores &#8805;1.75 and &#8805;2.01) 1.4- and 1.7- fold in males, respectively. In addition, anxiety symptoms (HSCL-25 anxiety scale mean score &#8805;1.75) increased independently the probability of elevated hs-CRP levels (&#62;3.0 mg/L) in males over 2-fold. Risk ratio of 1.3 was found for males with moderate to severe sleep disturbances and elevated hs-CRP levels (&#8805;1.0 mg/L). Regarding females, a positive correlation between elevated hs-CRP levels and depressive symptoms was found only among peri- and postmenopausal women not using exogenous hormones. The results suggest that low-grade inflammation is associated not only with depression but also with anxiety and sleep disturbances in young adult men. In women, hormonal factors may have an effect on the association between low-grade inflammation and depression. Further investigations are called for to confirm these findings and furthermore, to determine the possible role of low-grade inflammation in the pathophysiology of these disorders. / Tiivistelmä Depressio, ahdistuneisuushäiriöt ja unihäiriöt on yhdistetty elimistön matala-asteiseen tulehdustilaan, joskin pääasiallisesti vain miehillä. Tulosten yleistettävyyttä ovat rajoittaneet tutkimusten pienet otoskoot tai painottuminen iäkkäisiin väestöaineistoihin. Tässä tutkimuksessa selvitettiin matala-asteisen tulehduksen yhteyttä depressioon, ahdistuneisuuteen ja unihäiriöihin Pohjois-Suomen syntymäkohortti 1966 -aineistossa. Lisäksi Pieksämäki-tutkimuksen aineistossa selvitettiin naisilla menopaussin ja ehkäisyvalmisteiden/vaihdevuosihormonikorvaushoidon vaikutusta depression ja matala-asteisen tulehduksen väliseen yhteyteen. Pohjois-Suomen syntymäkohortti 1966 -tutkimuksen 31-vuotisseurannassa kartoitettiin 6007 henkilöltä masennus- ja ahdistuneisuusoireita Hopkins Symptom Checklist-25 -arviointiasteikolla (HSCL-25) ja unihäiriöitä 15-D-kyselyllä. Lisäksi mitattiin matala-asteisen tulehduksen mittarina käytetyn herkän C-reaktiivisen proteiinin (CRP) pitoisuus. Pieksämäki-tutkimuksessa edustava otos Pieksämäen asukkaista kutsuttiin kliiniseen tutkimukseen ja depressiivisiä oireita kartoitettiin Beckin 21-osioisella arviointiasteikolla ja mitattiin herkkä CRP (512 naista). Nuorilla aikuisilla miehillä, joiden herkkä CRP oli kohonnut (&#8805;1.0 mg/l), todettiin 1.7-kertainen masennusoireiden riski, kun katkaisupisteenä käytettiin HSCL-25-kyselyn masennuskeskiarvopistettä &#8805;2.01. Ahdistuneisuusoireet (HSCL-25-kyselyn ahdistuneisuuskeskiarvopisteet &#8805;1.75) lisäsivät kohonneen herkän CRP:n riskiä (&#62;3.0 mg/l) yli kaksinkertaiseksi miehillä. Keskivaikeasta tai vaikeasta unihäiriöstä kärsivillä todettiin 1.3-kertainen kohonneen herkän CRP:n (&#8805;1.0 mg/l) riski. Naisilla positiivinen yhteys masennuksen ja kohonneen herkän CRP:n välillä todettiin vain peri- ja postmenopausaalisilla naisilla, jotka eivät käyttäneet hormonikorvaushoitoa tai suun kautta otettavia ehkäisyvalmisteita. Tutkimustulokset viittaavat matala-asteisen tulehduksen liittyvän depressioon, ahdistukseen ja unihäiriöön nuorilla aikuisilla miehillä. Naisilla hormonaaliset seikat mahdollisesti vaikuttavat depression ja matala-asteisen tulehduksen väliseen yhteyteen. Tulevaisuuden tutkimushaasteena on selvittää matala-asteisen inflammaation mahdollinen merkitys depression, ahdistuneisuuden ja unihäiriöiden patofysiologiassa.

C-reactive protein

anxiety disorders

cohort studies

depressive disorder

hormone replacement therapy

low-grade inflammation

oral contraceptives

sleep disorders

ahdistus

c-reaktiivinen proteiini

depressio

hormonaalinen ehkäisy

hormonikorvaushoito

kohorttitutkimus

matala-asteinentulehdustila

unihäiriö

Impact de la colchicine sur l'inflammation vasculaire

Gingras, Marc-Alexandre

06 1900

Contexte : Des études récentes suggèrent que la colchicine permettrait de diminuer le risque d’événements cardiovasculaires. L’étude COLPET évaluait l’impact de la colchicine sur l’inflammation vasculaire mesurée par TEP/TDM chez des patients souffrant de MCAS stable. Méthodes : Dans cette étude randomisée à double insu de phase II, les patients étaient traités pendant 24 semaines avec 1 comprimé quotidien de colchicine 0.6 mg ou de placebo. L’inflammation vasculaire était évaluée par la captation de 18F-FDG dans l’aorte ascendante et les carotides à la TEP/TDM au début et à la fin de la thérapie. L’issue d’intérêt primaire était la variation de la moyenne du target-to-background ratio maximal des coupes d’images de l’aorte ascendante (Mean MAX TBR). Les issues d’intérêt secondaires incluaient plusieurs paramètres additionnels de TEP/TDM, ainsi que des mesures sériées de biomarqueurs inflammatoires sériques, dont la hs-CRP. Résultats : Cent-onze patients étaient randomisés dans l’étude, dont 56 au groupe placebo et 55 au groupe colchicine. La colchicine n’avait aucun impact significatif sur l’issue d’intérêt primaire (variation de la moyenne: 0.051; IC95% : -0.016 à 0.117; p=0.1346) ou sur les issues d’intérêt secondaires de TEP/TDM. Cependant, les patients traités à la colchicine présentaient une diminution de 28% de leurs niveaux de hs-CRP (p=0.0026). Conclusion : La thérapie à la colchicine pendant 24 semaines n’a eu aucun impact significatif sur la captation de 18F-FDG par l’aorte ascendante et les carotides. Cependant, une réduction de 28 % des niveaux de hs-CRP était observée chez les patients du groupe colchicine. L’étude randomisée multicentrique de phase III Colchicine Cardiovascular Outcomes Trial (COLCOT) est en cours pour évaluer les bénéfices cardiovasculaires à long terme de la colchicine (0.5 mg par jour), lorsque débutée pendant les trente jours suivant un infarctus du myocarde. / Background : Recent studies suggest that colchicine reduces cardiovascular risk. The COLPET Study evaluated the impact of colchicine on vascular inflammation, as measured by PET/CT, in patients with stable CAD. Methods: In this randomized, double-blind, placebo-controlled, phase II clinical trial, patients were treated for 24 weeks with a daily tablet of colchicine 0.6 mg or placebo. Vascular inflammation was assessed by uptake of 18F-FDG in the ascending aorta and carotid arteries on PET/CT at baseline and at the end of study drug therapy. The primary outcome was the change in the mean of maximal target-to-background ratio of the image slices of the ascending aorta (Mean MAX TBR). Secondary outcomes included various PET/CT parameters, as well as serial measures of inflammatory biomarkers, such as hs-CRP. Results: A total of 111 patients were randomized, with 56 in the placebo group and 55 in the colchicine group. Colchicine had no significant impact on the primary outcome (change in mean: 0.051; IC95% : -0.016 à 0.117; p=0.1346) or any of the PET/CT secondary outcomes. In contrast, patients treated with colchicine presented a decrease of 28% in hs-CRP levels (p=0.0026). Conclusion: Colchicine therapy for 24 weeks had no significant impact on vascular uptake of 18F-FDG in the ascending aorta or carotid arteries. However, a reduction of 28% in hs-CRP was observed in the colchicine group. The Colchicine Cardiovascular Outcomes Trial (COLCOT) is a multicenter randomized phase III trial, currently under way, evaluating the long-term cardiovascular benefits of therapy with colchicine (0.5 mg daily) when begun less than thirty days following acute myocardial infarction.

Athérosclérose

Inflammation vasculaire

Maladies cardiovasculaires

Tomographie par émission de positrons

Fluorodéoxyglucose

Colchicine

Protéine C-réactive

Biomarqueurs

Atherosclerosis

Vascular inflammation

Cardiovascular disease

Positron emission tomography

C-reactive protein

Biomarkers

Flow cytometric analysis of leukocyte surface molecule expression in critical illness:comparison between septic and non-septic patients

Jämsä, J. (Joel)

06 June 2017

Abstract Sepsis is a common problem in the intensive care unit (ICU) still having a high mortality and causing high costs to health care system. Currently, there is no marker to distinguish sepsis from other causes of systemic inflammation. Leukocyte surface molecules have been proposed as markers of sepsis. The most promising markers have been neutrophil CD64 and CD11b on monocytes and neutrophils and HLA-DR on monocytes. In this thesis, leukocyte surface molecules were investigated using quantitative flow cytometry in critically ill patients with sepsis, non-septic ICU controls, and healthy volunteers. The surface molecules of interest were neutrophil CD11b and CD64, monocyte CD11b, CD14, CD40, CD64, CD80, HLA-DR, and lymphocyte CD69. First, a special emphasize was indicated in methodological aspects of the quantitative flow cytometry. Then, the surface molecule kinetics was investigated in different types of critically ill patients. Finally, the diagnostic performance of the molecules was determined and compared to that of traditionally used sepsis markers. Furthermore, an example of multiple marker analysis was introduced as a diagnostic tool. The optimal circumstances for leukocyte surface molecule analysis were +4&#176;C temperature throughout the collection and preparation of the samples using tubes containing acid citrate dextrose (ACD) as an anticoagulant, followed by flow cytometry within 6 hours from sampling. Monocyte CD11b and CD40, neutrophil CD11b and CD64, and CD69 on CD4+ T cells and natural killer (NK) cells separated sepsis from non-septic ICU controls and healthy volunteers, neutrophil CD64, having the best area under curve. Procalcitonin (PCT) was second best marker. Monocyte CD40 and NK CD69 may predict positive blood culture detection, whereas CD11b may predict early mortality. In multiple marker analysis, combination of positive neutrophil CD64, C-reactive protein (CRP) and PCT increased post-test probability for sepsis. In conclusion, pre-analytical and analytical factors have effects on results of leukocyte surface molecule analysis. Leukocyte surface molecules may improve sepsis diagnostics in ICU setting. Neutrophil CD64 was the most promising marker. Combination of CD64, CRP and PCT increased the detection of sepsis in ICU. / Tiivistelmä Sepsis on yleinen tehohoidon ongelma, johon liittyy korkea kuolleisuus ja suuret hoidolliset kustannukset. Toistaiseksi ei ole laboratoriomerkkiainetta, joka erottaisi sepsistä sairastavat muista kriittisesti sairaista, joilla on yleistynyt tulehdusvaste. Valkosolujen pintamolekyylien käyttöä sepsiksen laboratoriomerkkiaineena on tutkittu. Lupaavimmat näistä molekyyleistä ovat olleet neutrofiilien CD64, monosyyttien ja neutrofiilien CD11b ja monosyyttien HLA-DR. Tässä väitöskirjassa tutkittiin valkosolujen pintamolekyylejä kriittisesti sairailla sepsistä sairastavilla potilailla, niillä tehohoitopotilailla, joilla ei ollut sepsistä, ja terveillä vapaaehtoisilla virtaussytometriaa käyttäen. Mielenkiinnon kohteina olivat neutrofiilien CD11b ja CD64, monosyyttien CD11b, CD14, CD40, CD64, CD80 ja HLA-DR, sekä lymfosyyttien CD69. Ensimmäiseksi tutkittiin kvantitatiivista virtaussytometriaa menetelmänä. Sen jälkeen pintamolekyylien kinetiikkaa tutkittiin eri potilasryhmillä. Lopuksi määritettiin pintamolekyylien diagnostinen tehokkuus ja sitä verrattiin perinteisempiin sepsiksen diagnostiikassa käytettyihin laboratoriomerkkiaineisiin. Lisäksi selvitettiin usean merkkiaineen mallin diagnostista osuvuutta. Parhaat olosuhteet virtaussytometrialle olivat: +4 &#176;C:n lämpötila näytteenoton ja -käsittelyn aikana, näytteiden ottaminen putkiin, joissa on antikoagulanttina hapan sitraatti-dekstroosi (ACD) ja näytteiden analysointi kuuden tunnin kuluessa näytteenotosta. Monosyyttien CD11b ja CD40, neutrofiilien CD11b ja CD64 sekä CD4+ T-solujen ja NK-solujen CD69 erottivat sepsistä sairastavat tehohoitoverrokeista ja terveistä. Neutrofiilien CD64:llä oli paras erottelukyky. Prokalsitoniini (PCT) oli toiseksi paras merkkiaine. Monosyyttien CD40 ja NK-solujen CD69 voivat parantaa positiivisen veriviljelylöydöksen havaitsemista, kun taas CD11b voi ennustaa varhaista potilaan menehtymistä. Usean merkkiaineen mallissa neutrofiilien CD64 paransi C-reaktiivisen proteiinin (CRP) ja PCT:n tehoa sepsiksen diagnostiikassa. Loppupäätelmänä on, että valkosolujen pintamolekyylien analysointivaiheen eri muuttujilla on vaikutusta virtaussytometriatuloksiin. Valkosolujen pintamolekyylien käyttö voi parantaa sepsiksen diagnostiikkaa teho-osastolla. Neutrofiilien CD64 oli lupaavin merkkiaine. Neutrofiilien CD64:n, CRP:n ja PCT:n yhdistelmä paransi sepsiksen diagnostiikkaa teho-osastolla.

C-reactive protein

CD antigens

flow cytometry

intensive care

laboratory tests

leukocytes

lymphocytes

monocytes

neutrophils

procalcitonin

sepsis

systemic inflammation

C-reaktiivinen proteiini

CD antigeenit

laboratoriomerkkiaineet

lymfosyytit

monosyytit

neutrofiilit

prokalsitoniini

sepsis

tehohoito

valkosolut

virtaussytometria

yleistynyt tulehdusvaste

Proteína C reativa na deficiência isolada monogênica do hormônio de crescimento

Marques-santos, Celi

12 September 2006

The present research has the objective to determinate the seric PCR concentrations in the monogenic isolated deficiency of the growth hormone (DIGH), test the hypothesis that DIGH is associated to the exacerbation of the inflammatory profile, identify the PCR elevation predictors, and evaluate the existence of an association between PCR and premature atherosclerosis. The growth hormone (GH) has as its main function the post-natal longitudinal growth; it interferes in the bone apposition, muscle mass growth, opposes to the action of insulin in the carbohydrates and lipids metabolism, and, in the cardiovascular system, helps the vascular and myocardial remodeling. IGF-I, GH primary mediator, plays a fundamental role in the growth regulation, cellular apoptosis and differentiation. The GH/IGF-I axis acts in the resistance to insulin and phenotypical expression of cardiovascular risk factors, associated to metabolic syndrome. IGF-I avoids the endothelial dysfunction, causes the increase of sensitivity to insulin, and avoids post-prandial dyslipidemia, besides presenting anti-inflammatory and anti-apoptotic activities. The decrease of IGF-I is associated to premature atherosclerosis and high cardiovascular risk. IGF-I role is controversial and its increase is related to the premature atherosclerosis in carotids. The deficiency of GH is associated to the increase of cardiovascular and brain vascular mortality. The inflammation plays an essential role in the atherosclerosis physiopathology from its initial phase up to atherotrombotic events in acute coronary syndromes. C - reactive protein, acute phase reagent of the inflammation, is produced by the liver, due mainly to the interleukin-6 stimulus. As a predictor and a mediator of atherosclerosis, among all circulating inflammatory markers, it is the most stable, the most studied and the one which presented the most constant relationship to future cardiovascular risk in various clinical situations, including asymptomatic individuals. In Itabaininha, Sergipe state we described a population with DIGH, with extremely low levels of IGF-I, high LDL-c and systolic arterial pressure and central obesity, a cluster of risk factors, highly susceptible to atherosclerosis ideal to this research. From this population, eighteen individuals were studied, eight male and ten female, with an average age of 45, compared to a control group composed of twenty individuals of the same region. After the clinical and metabolic characteristics were analyzed, the most relevant results were: PCR showed a meaningful difference between the groups (4,9 mg/l (4,7) vs 1,4 mg/l (2,2)); and IGF-I extremely low (1,0 ng/ml (1,0) vs 164,0 ng/ml (135,0)). The group predicts that PCR is independent from the other metabolic variables (R² = 0, 42), and that IGF-I is the main responsible for the increase of PCR in the DIGH. No association between PCR and the intimatemedia thickness of the carotids could be observed. Conclusion: it was demonstrated that the DIGH present high levels of PCR when compared to the control group; the variable group predicts this variation and IGF-I is the main responsible for the PCR variability. High PCR is not associated to premature atherosclerosis in this high risk differentiated group. / Esta pesquisa demonstra de forma original o grau de inflamação relacionado à deficiência isolada monogênica do hormônio de crescimento (DIGH) através da determinação das concentrações plasmáticas da proteína C reativa (PCR), testa a hipótese de a DIGH estar associada à exacerbação do perfil inflamatório, identifica os preditores da elevação da PCR e avalia a associação de inflamação com aterosclerose precoce. O hormônio de crescimento (GH) tem como função principal, o crescimento longitudinal pós-natal; interfere na aposição óssea, crescimento da massa muscular, opõe-se à ação da insulina no metabolismo dos carboidratos e lipídios e, no aparelho cardiovascular, atua no remodelamento miocárdico e vascular. A sua deficiência está associada ao aumento de mortalidade por doenças cardio e cérebro vasculares. O IGF-I, mediador primário do GH, desempenha papel fundamental na regulação do crescimento, diferenciação e apoptose celular. O eixo GH/IGF-I interfere quanto à resistência à insulina e na expressão fenotípica dos fatores de risco cardiovasculares, associados à síndrome metabólica. O IGF-I evita a disfunção endotelial, promove o aumento da sensibilidade à insulina previne a dislipidemia pós-prandial, além de possuir atividade anti-inflamatória e antiapoptótica. A diminuição do IGF-I está associada à aterosclerose prematura e elevado risco cardiovascular. O papel do IGF-I é controverso e o seu aumento está associado ao aparecimento precoce de aterosclerose em carótidas. A inflamação exerce papel fundamental na fisiopatologia da aterosclerose. A PCR, reagente de fase aguda da inflamação é produzida pelo fígado, em decorrência principalmente do estímulo da interleucina-6. Entre os marcadores inflamatórios circulantes, é a mais estável, a mais estudada e a que apresentou relação mais constante com o risco cardiovascular futuro em diversas situações clínicas, incluindo indivíduos assintomáticos; A PCR é considerada preditora e mediadora da aterosclerose. Em Itabaianinha, Sergipe, foi descrita uma população com DIGH, níveis extremamente baixos de IGF-I, LDL e pressão arterial sistólica elevados, obesidade central, portanto, uma população com múltiplos fatores de risco, altamente susceptível à aterosclerose. Este estudo inseriu 18 indivíduos DIGH, oito do sexo masculino e dez do feminino, idade média de 45 anos, e 20 controles (CO) da mesma região. Analisadas as características clínicas e metabólicas, o grupo DIGH apresentou PCR de (4,9 mg/l (4,7) vs controles (CO) 1,4 mg/l (2,2) com importante diferença significativa (p<0,0001); o IGF-I dos DIGH foi extremamente baixo, 1,0 ng/ml (1,0) vs 164,0 ng/ml (135,0) dos CO, p< 0,0001. O grupo é que prediz ser a PCR independente das outras variáveis metabólicas (R2 = 0,42) e o IGF- I é o principal responsável pelo aumento da PCR nos DIGH. Não houve nenhuma relação de associação entre a PCR e a espessura média-íntima das carótidas do DIGH. Conclusão: ficou demonstrado que os DIGH apresentam níveis muito elevados de PCR que denota um perfil inflamatório exacerbado; o grupo é que prediz esta variação e, o IGF-I é o principal responsável pelo variabilidade da PCR. A PCR elevada na DIGH não está associada à aterosclerose precoce.

Endocrinologia

Cardiologia

Proteína C Reativa

Inflamação

Aterosclerose

IGF-I

Síndrome metabólica

Nanismo hipofisário

C-reactive protein

Inflammation

Atherosclerosis

Growth hormone deficiency

IGF-I

Metabolic Syndrome

CNPQ::CIENCIAS DA SAUDE