Cardiac Troponins in Patients with Suspected or Confirmed Acute Coronary Syndrome : New Applications for Biomarkers in Coronary Artery Disease

Eggers, Kai

January 2007

The cardiac troponins are the biochemical markers of choice for the diagnosis of acute myocardial infarction (AMI) and risk prediction in patients with acute coronary syndrome (ACS). In this thesis, the role of early serial cardiac troponin I (cTnI) testing was assessed in fairly unselected patient populations admitted because of chest pain and participating in the FAST II-study (n=197) and the FASTER I-study (n=380). Additionally, the importance of cTnI testing in stable post-ACS patients from the FRISC II-study (n=1092) was studied. The analyses in chest pain patients demonstrate that cTnI is very useful for early diagnostic and prognostic assessment. cTnI allowed already 2 hours after admission the reliable exclusion of AMI and the identification of low-risk patients when ECG findings and a renal marker such as cystatin C were added as conjuncts. Other biomarkers such as CK-MB, myoglobin, NT-pro BNP or CRP did not provide superior clinical information. However, myoglobin may be valuable in combination with cTnI results for the early prediction of an impending major AMI when used as input variable for an artificial neural network. Such an approach applying cTnI results only may also furthermore improve the early diagnosis of AMI. Persistent cTnI elevation > 0.01 μg/L was detectable using a high-sensitive assay in 26% of the stable post-ACS patients from the FRISC II-study. NT-pro BNP levels at 6 months were the most important variable independently associated to persistent cTnI elevation besides male gender, indicating a relationship between adverse left ventricular remodeling processes and cTnI leakage. Patients with persistent cTnI elevation had a considerable risk for both mortality and AMI during 5 year follow-up. These analyses thus, confirm the value of cTnI for early assessment of chest pain patients and provide new and unique evidence regarding the role of cTnI for risk prediction in post-ACS populations.

Internal medicine

Ischemic heart disease

Acute myocardial infarction

Troponin

Natriuretic peptide

CRP

Cystatin C

Artificial neural network

Point of care measurements

Risk prediction

Invärtesmedicin

The kidney in different stages of the cardiovascular continuum

Nerpin, Elisabet

January 2013

Patients with chronic kidney disease are at higher risk of developing cardiovascular disease. The complex, interaction between the kidney and the cardiovascular system is incompletely understood, particularly at the early stages of the cardiovascular continuum. The overall aim of this thesis was to clarify novel aspects of the interplay between the kidney and the cardiovascular system at different stages of the cardiovascular continuum; from risk factors such as insulin resistance, inflammation and oxidative stress, via sub-clinical cardiovascular damage such as endothelial dysfunction and left ventricular dysfunction, to overt cardiovascular death. This thesis is based on two community-based cohorts of elderly, Uppsala Longitudinal Study of Adult Men (ULSAM) and Prospective Investigation of the Vasculature in Uppsala Seniors (PIVUS). The first study, show that higher insulin sensitivity, measured with euglycemic-hyperinsulinemic clamp technique was associated to improve estimated glomerular filtration rate (eGFR) in participants with normal fasting plasma glucose, normal glucose tolerance and normal eGFR. In longitudinal analyses, higher insulin sensitivity at baseline was associated with lower risk of impaired renal function during follow-up. In the second study, eGFR was inversely associated with different inflammatory markers (C-reactive protein, interleukin-6, serum amyloid A) and positively associated with a marker of oxidative stress (urinary F2-isoprostanes). In line with this, the urinary albumin/creatinine ratio was positively associated with these inflammatory markers, and negatively associated with oxidative stress. In study three, higher eGFR was associated with better endothelial function as assessed by the invasive forearm model. Further, in study four, higher eGFR was significantly associated with higher left ventricular systolic function (ejection fraction). The 5th study of the thesis shows that higher urinary albumin excretion rate (UAER) and lower eGFR was independently associated with an increased risk for cardiovascular mortality. Analyses of global model fit, discrimination, calibration, and reclassification suggest that UAER and eGFR add relevant prognostic information beyond established cardiovascular risk factors in participants without prevalent cardiovascular disease. Conclusion: this thesis show that the interaction between the kidney and the cardiovascular system plays an important role in the development of cardiovascular disease and that this interplay begins at an early asymptomatic stage of the disease process.

epidemiology

chronic kidney disease

cystatin C

glomerular filtration rate

albuminuria

euglycemic hyperinsulinemic clamp

insulin sensitivity

inflammation

oxidative stress

Pharmacometric Models for Antibacterial Agents to Improve Dosing Strategies

Nielsen, Elisabet I

January 2011

Antibiotics are among the most commonly prescribed drugs. Although the majority of these drugs were developed several decades ago, optimal dosage (dose, dosing interval and treatment duration) have still not been well defined. This thesis focuses on the development and evaluation of pharmacometric models that can be used as tools in the establishment of improved dosing strategies for novel and already clinically available antibacterial drugs. Infectious diseases are common causes of death in preterm and term newborn infants. A population pharmacokinetic (PK) model for gentamicin was developed based on data from a prospective study. Body-weight and age (gestational and post-natal age) were found to be major factors contributing to variability in gentamicin clearance and therefore important patient characteristics to consider for improved dosing regimens. A semi-mechanistic pharmacokinetic-pharmacodynamic (PKPD) model was also developed, to characterize in vitro bacterial growth and killing kinetics following exposure to six antibacterial drugs, representing a broad selection of mechanisms of action and PK as well as PD characteristics. The model performed well in describing a wide range of static and dynamic drug exposures and was easily applied to other bacterial strains and antibiotics. It is, therefore, likely to find application in early drug development programs. Dosing of antibiotics is usually based on summary endpoints such as the PK/PD indices. Predictions based on the PKPD model showed that the commonly used PK/PD indices were well identified for all investigated drugs, supporting that models based on in vitro data can be predictive of antibacterial effects observed in vivo. However, the PK/PD indices were sensitive to the study conditions and were not always consistent between patient populations. The PK/PD indices may therefore extrapolate poorly across sub-populations. A semi-mechanistic modeling approach, utilizing the type of models described here, may thus have higher predictive value in a dose optimization tailored to specific patient populations.

Pharmacometrics

pharmacokinetics

pharmacodynamics

modeling

NONMEM

antibiotics

in vitro

time-kill curve

PK/PD indices

gentamicin

aminoglycosides

newborn infants

premature infants

cystatin C

Biopharmacy

Biofarmaci

Cistatina C plasmática como biomarcador de lesão renal aguda em idosos após correção de fratura de fêmur / Plasma Cystatin C in acute renal injury in the elderly after subarachnoid block for correction of femur fracture

Andrade Neto, José de Souza

16 October 2017

Submitted by jose de souza andrade neto andrade (neto.jsa@hotmail.com) on 2018-01-09T15:51:07Z No. of bitstreams: 1 José Andrade Neto - Doutorado em Anestesiologia.pdf: 670032 bytes, checksum: b5c727b9c523ebb565c09234ac9ba901 (MD5) / Approved for entry into archive by Luciana Pizzani null (luciana@btu.unesp.br) on 2018-01-10T12:53:05Z (GMT) No. of bitstreams: 1 andrade neto_js_doc_int.pdf: 670032 bytes, checksum: b5c727b9c523ebb565c09234ac9ba901 (MD5) / Made available in DSpace on 2018-01-10T12:53:05Z (GMT). No. of bitstreams: 1 andrade neto_js_doc_int.pdf: 670032 bytes, checksum: b5c727b9c523ebb565c09234ac9ba901 (MD5) Previous issue date: 2017-10-16 / Introdução: a lesão renal aguda (LRA) é prevalente em pacientes hospitalizados e responsável por alta morbimortalidade. No entanto, ainda não há um marcador precoce e acurado para seu diagnóstico. Pacientes idosos estão em risco de desenvolver LRA no pós-operatório de grandes cirurgias. Objetivos: avaliar o biomarcador cistatina C plasmática como preditor precoce de LRA no período pós-operatório de cirurgia para correção de fratura de fêmur em idosos. Método: cinquenta e nove pacientes idosos submetidos à cirurgia de correção de fratura de fêmur foram estudados prospectivamente por 48 horas do pós-operatório. Amostras de sangue foram coletadas para análise de cistatina C plasmática nos seguintes tempos: logo ao término da cirurgia, no período de 4 e 24 horas depois. Amostras da creatinina foram coletadas na admissão hospitalar, ao término da cirurgia, 4, 24 e 48 horas no pós-operatório. Para a determinação do diagnóstico e estadiamento de LRA foi utilizado o critério KDIGO (Kidney Disease Improve Global Outcomes Acute Kidney Injury Workgroup). Foi analisada a precocidade e acurácia, esta última por meio da área sob a curva receiver operating characteristic (AUC ROC), da molécula de cistatina C plasmática para diagnóstico de LRA (KDIGO ≥1). Resultados: vinte e um pacientes (35,5%) apresentaram LRA. A cistatina C plasmática foi um marcador precoce de LRA elevando-se 4 horas após o fim da cirurgia (p < 0,003). Obteve uma AUC ROC em 4 horas de 0,750 (IC 95% de 0,610 a 0,860) e de 0,778 (IC 95% de 0,640 a 0,870) em 24 horas do pós-operatório. Conclusão: a molécula de cistatina C plasmática é um marcador precoce e com boa acurácia (apresentou AUC ROC > 0,70) para LRA, além de possuir elevado valor preditivo negativo para o ponto de corte de 0,92mg/L após 4 horas do término da cirurgia.

cistatina C

idosos

lesão renal aguda

biomarcador renal

creatinina

fratura de fêmur

cystatin C

elderly

acute renal injury

renal biomarker

creatinine

femur fracture

Avaliação de marcadores de lesão do túbulo proximal renal e incidência de redução da filtração glomerular em pacientes portadores de Hepatite B em uso de tenofovir / Evaluation of markers of renal proximal tubule injury and incidence of reduced glomerular filtration in patients with hepatitis B using tenofovir

Álan Fernandes Laurindo

27 January 2015

Tenofovir (TDF), um antirretroviral análogo nucleotídeo inibidor da transcriptase reversa, indicado para o tratamento da infecção pelo vírus da Hepatite B em indivíduos HBeAg reagentes, não cirróticos, tem sido implicado na ocorrência de Injúria renal aguda (IRA) e lesão do túbulo proximal renal (TPR), com características semelhantes à Síndrome de Fanconi, caracterizada por glicosúria, bicarbonatúria, fosfatúria, uricosúria e proteinúria de baixo peso molecular. Outros trabalhos sugerem que os pacientes em uso de TDF sofram toxicidade aos glomérulos, com uma pequena, porém significante redução da taxa de filtração glomerular. O tempo de uso da droga para que ocorra lesão renal é desconhecido. Entretanto, a maioria dos estudos de investigação de nefrotoxicidade do TDF foi realizada em pacientes portadores de infecção pelo HIV. Especula-se que a nefrotoxicidade desta droga possa ser exacerbada ou reduzida pelo uso de outras medicações, frequentemente usadas por pacientes com HIV, que competem com o transporte tubular ou com sua metabolização, aumentando o seu nível sérico. O objetivo geral deste trabalho é avaliar prospectivamente a incidência de lesão renal pelo uso de TDF em pacientes portadores de hepatite B. Os objetivos específicos deste trabalho são: (1) avaliar incidência de lesão do TPR através da avaliação da excreção urinária de ácido úrico, fósforo e da proteína de baixo peso molecular neutrophil gelatinase associated lipocalin (NGAL); (2) avaliar a incidência de redução aguda da taxa de filtração glomerular (LRA) ou redução crônica da mesma. Métodos: Foram incluídos 24 pacientes portadores de Hepatite B que tiveram indicação de iniciar o uso de TDF com idade superior a 18 anos ou inferior a 75 anos. Neste estudo prospectivo, foi realizado a coleta de dados clínicos (idade, gênero, etnia, tempo de doença, antecedentes pessoais, medicações concomitantes, fator de risco para contaminação do VHB, história familiar de infecção VHB) e a avaliação laboratorial foi feita através da coleta de sangue e urina feitas antes do início do uso do TDF e, posteriormente à sua introdução, semestralmente durante 2 anos. Ao final do seguimento foi avaliada a incidência de lesão renal pelo uso de TDF, através das seguintes dosagens: glicemia, fosfatemia, gasometria, creatinina e Cistatina C séricas, microalbuminúria, proteinúria, proteinúria de baixo peso molecular (NGAL), clearance de creatinina, fosfatúria, uricosúria e urina rotina. Foi feita análise estatística comparativa entre os pacientes que usaram o TDF pré tratamento e pós tratamento para detectar lesão do TPR ou redução da taxa de filtração glomerular ao longo do tempo. Resultados: Não foi identificado aumento significativo da creatinina no decorrer do estudo (p = 0,09; R = 2,4%), entretanto, foi observada uma queda significativa nos valores do clearance de creatinina em 24 horas (p < 0,01; R = 15,8%). Não foi observada tendência de queda da filtração glomerular através das fórmulas MDRD simplificada (p = 0,11), CKD-EPI (p=0,14), CKD-EPI cystatin C (p = 0,23). Em relação à cistatina C sérica também não foi observada sua elevação no decorrer do tempo (p=0,15; R = 2,4%). Não foi observado, utilizando-se modelo de regressão linear, aumento na excreção urinária de albumina no decorrer do estudo (p = 0,97; R = 0,00%), mas houve aumento significativo na proteinúria de 24h (p < 0,01). Foi observada também, redução da uricosúria com o passar do tempo (p = 0,01; R = 6,7%) e houve correlação positiva entre o clearance de creatinina dosado em urina de 24 horas e a excreção de ácido úrico em urina de 24 horas (p=0,01; r = + 0,60). A fração de excreção de fósforo (urina de 24h): não foi observada alteração no decorrer do tempo (p = 0,83; R = 0,5%), porém houve correlação negativa com entre o clearance de creatinina dosado em urina de 24 horas e a fração de excreção de fósforo (FePO4) dosada em urina de 24 horas (p = 0,05; r = - 0,25). A detecção de NGAL na urina foi feita pelo índice UNGAL/Ucreat e não foi observado aumento significativo de sua excreção no decorrer do tempo (p = 0,40, r = 0,8%). Conclusão: em conclusão no presente estudo observou-se desenvolvimento de lesão renal aguda em 10% dos pacientes em uso de tenofovir e redução significativa da filtração glomerular. A fosfatúria e proteinúria observados sugerem que a lesão tenha sido decorrente de tubulopatia proximal e os marcadores mais específicos de lesão renal, cistatina C e NGAL, não foram superiores aos biomarcadores disponíveis na prática clínica na detecção destas alterações. / Tenofovir (TDF) a nucleotide analog reverse transcriptase inhibitor antiretroviral indicated for the treatment of infection with the hepatitis B virus in reagents HBeAg individuals, non-cirrhotic patients, has been implicated in the occurrence of acute kidney Injury (AKI) and the proximal tubule injury kidney (TPR), with similar to Fanconi syndrome characterized by glucosuria, bicarbonatúria, phosphaturia, proteinuria, uricosuria and low molecular weight characteristics. Other studies suggest that patients using TDF toxicity suffer the glomeruli, with a small but significant reduction in glomerular filtration rate. The time of drug use for kidney damage that occurs is unknown. However, most of the research studies of nephrotoxicity TDF was performed in patients with HIV infection. It is speculated that the nephrotoxicity of this drug may be exacerbated or reduced by the use of other medications, often used by patients with HIV, which compete with the tubular transport or metabolism, increasing its serum level. The overall objective of this study is to prospectively evaluate the incidence of renal injury by the use of TDF in patients with hepatitis B. The specific objectives of this work are: (1) assess the incidence of injury TPR by assessment of urinary excretion of uric acid, phosphorus and protein of low molecular weight neutrophil gelatinase associated lipocalin (NGAL); (2) assess the incidence of acute reduction in glomerular filtration rate (IRA) or chronic reduction. Methods: 24 patients with hepatitis B who were advised to initiate the use of TDF over the age of 18 years or below 75 years were included. In this prospective study, the collection of clinical data (age, gender, ethnicity, duration of disease, personal history, concomitant medications, risk factor for HBV infection, family history of HBV infection) and laboratory evaluation was done by collect blood and urine samples taken before initiation of the use of TDF and after its introduction, semiannually for 2 years. At final follow-up the incidence of renal injury by the use of TDF was assessed through the following dosages: glucose, phosphatemia, gases, creatinine and serum cystatin C, microalbuminuria, proteinuria, low molecular weight proteinuria (NGAL), clearance creatinine, phosphaturia, uricosuria and urine routine. The comparative statistical analysis of patients using TDF pre-treatment and post treatment to detect the TPR injury or reduced glomerular filtration rate over time. Results: There was not significant increase in creatinine identified during the study (p = 0.09; R = 2.4%), however, a significant decrease was observed in the values of creatinine clearance at 24 hours (p <0.01; R = 15.8%). No downward trend was observed in glomerular filtration through the simplified MDRD formulas (p = 0.11), CKD-EPI (p = 0.14), CKD-EPI cystatin C (p = 0.23). Regarding the serum cystatin C its elevation was not observed over time (p = 0.15, R = 2.4%). Increased urinary albumin excretion during the study was not observed using a linear regression model (p = 0.97, R = 0.00%), but there was significant increase in 24-hour proteinuria (p <0, 01). And there was a positive correlation between creatinine clearance at 24 hour urine and the excretion of uric acid in 24 hour urine (p = 0.01, R = + 0.60), uricosuria reduction over time was also observed (p = 0.01, R = 6.7%). No change was observed over time in the fractional excretion of phosphorus (24 h urine), (p = 0.83; R = 0.5%), but there was a negative correlation between creatinine clearance urine dosed at 24 hours and fractional excretion of phosphorus (FePO4) measured in 24 hour urine (p = 0.05, r = - 0.25). The detection of NGAL in the urine was taken by UNGAL / Ucreat index and was not observed significant increase in excretion over time (p = 0.40, r = 0.8%). Conclusion: In conclusion at the present study we observed the development of acute kidney injury in 10% of patients using tenofovir and a significant reduction in glomerular filtration. The phosphaturia and proteinuria observed suggest that the injury has been caused by proximal tubulopathy and more specific markers of renal injury as cystatin C and NGAL were not greater than the available biomarkers in clinical practice for their detection.

Cistatina C

Hepatite

Lesão renal

NGAL

Tenofovir

Tubulopatia proximal renal

Cystatin C

Hepatitis B

Kidney injury

NGAL

Proximal tubulopathy kidney

Tenofovir

Cistatina C plasmática como biomarcador de lesão renal aguda em idosos após correção de fratura de fêmur

Andrade Neto, José de Souza.

January 2017

Orientador: Norma Sueli Pinheiro Módolo / Resumo: Introdução: a lesão renal aguda (LRA) é prevalente em pacientes hospitalizados e responsável por alta morbimortalidade. No entanto, ainda não há um marcador precoce e acurado para seu diagnóstico. Pacientes idosos estão em risco de desenvolver LRA no pós-operatório de grandes cirurgias. Objetivos: avaliar o biomarcador cistatina C plasmática como preditor precoce de LRA no período pós-operatório de cirurgia para correção de fratura de fêmur em idosos. Método: cinquenta e nove pacientes idosos submetidos à cirurgia de correção de fratura de fêmur foram estudados prospectivamente por 48 horas do pós-operatório. Amostras de sangue foram coletadas para análise de cistatina C plasmática nos seguintes tempos: logo ao término da cirurgia, no período de 4 e 24 horas depois. Amostras da creatinina foram coletadas na admissão hospitalar, ao término da cirurgia, 4, 24 e 48 horas no pós-operatório. Para a determinação do diagnóstico e estadiamento de LRA foi utilizado o critério KDIGO (Kidney Disease Improve Global Outcomes Acute Kidney Injury Workgroup). Foi analisada a precocidade e acurácia, esta última por meio da área sob a curva receiver operating characteristic (AUC ROC), da molécula de cistatina C plasmática para diagnóstico de LRA (KDIGO ≥1). Resultados: vinte e um pacientes (35,5%) apresentaram LRA. A cistatina C plasmática foi um marcador precoce de LRA elevando-se 4 horas após o fim da cirurgia (p < 0,003). Obteve uma AUC ROC em 4 horas de 0,750 (IC 95% de 0,610 a 0,860) e de... (Resumo completo, clicar acesso eletrônico abaixo) / Doutor

cistatina C

Idosos.

Lesão renal aguda.

biomarcador renal

Creatinina.

fratura de fêmur

cystatin C

Idosos.

Lesão renal aguda.

renal biomarker

creatinine

femur fracture

The effects of long-term homocysteine-lowering treatment with folic acid, vitamin B6 and Vitamin B12 on vascular structure and function in stroke

Potter, Kathleen

January 2009

[Truncated abstract] An elevated total plasma homocysteine concentration (tHcy) is associated with an increased risk of myocardial infarction and ischemic stroke. Folic acid, vitamin B6 and B12 supplements significantly reduce tHcy even in people who are not overtly vitamin deficient. If homocysteine is a causal risk factor for atherothrombotic events, treatment with B-vitamins might prove a simple and cost-effective means to reduce cardiovascular risk. However, it remains unclear whether elevated tHcy causes atherosclerosis or is simply a risk marker. To prove that homocysteine is a modifiable risk factor for cardiovascular disease it is necessary to show that lowering tHcy reduces vascular risk. The aim of this study was to determine whether long-term homocysteine-lowering with B-vitamins would improve vascular structure and function in people with a history of stroke. This study was a cross-sectional sub-study of the Vitamins TO Prevent Stroke trial (VITATOPS), a multi-centre, randomised, double-blind, placebo-controlled clinical trial designed to test the efficacy and safety of B-vitamins (folic acid 2mg, vitamin B6 25mg and vitamin B12 0.5mg) in the prevention of vascular events in patients with a recent history of stroke or transient ischemic attack. 173 VITATOPS participants were recruited for the current study. Age, sex, stroke type, medications, cardiovascular risk factors and smoking history were recorded and blood pressure, height, weight, waist and hip girth were measured in all subjects at least two years after randomisation. ... After a mean treatment period of 3.9 ± 0.9 years, the subjects randomised to vitamin treatment had significantly lower tHcy than the subjects randomised to placebo (7.9mol/L, 95%CI 7.5, 8.4 versus 11.8mol/L, 95%CI 10.9, 12.8; p<0.001). There were no significant differences between groups in CIMT (0.84 ± 0.17mm vitamins versus 0.83 ± 0.18mm placebo; p=0.74) or FMD (median of 4.0%, IQR 0.9, 7.2, vitamins versus 3.0%, IQR 0.6, 6.6 placebo; p=0.48). Pooled estimates from the meta-analyses showed that B-vitamin treatment reduces CIMT by 0.10mm (95%CI –0.20, -0.01mm) and increases FMD by 1.4%, (95%CI 0.7, 2.2), although these estimates may have been influenced by positive publication bias. The improvement in FMD was significant in studies of less than eight weeks duration but not in studies with longer treatment periods. The association between tHcy and CIMT and FMD was eliminated by adjustment for renal function and long-term B-vitamin treatment did not alter the strong linear relationship between tHcy and cystatin C. Lowering tHcy did not alter arterial wall inflammation assessed by 18FDG-PET, although small subject numbers meant we were unable to exclude a minor treatment effect. Long-term homocysteine-lowering with B-vitamin treatment did not improve CIMT or FMD or reduce arterial wall inflammation in people with a history of stroke. The relationship between tHcy and these markers of vascular risk was eliminated by adjustment for renal function. Our data are consistent with the hypothesis that elevated tHcy is a risk marker for cardiovascular disease rather than a modifiable causal risk factor.

Cerebrovascular disease -- Prevention

Homocysteine -- Pathophysiology

Vitamin B6 -- Therapeutic use -- Testing

Folic acid -- Therapeutic use -- Testing

Vitamin B complex

Folic acid

B-vitamins

Carotid intima medial thickness

Cystatin C

Effets de deux xénohormones, la génistéine et la vinclozoline, sur le développement et les fonctions exocrines et endocrines des glandes salivaires submandibulaires de rats Wistar Han : influence de la période d'exposition en fonction de l'âge et du sexe / Effect of two xeno-hormones, genistein and vinclozolin on development and exocrines and endocrines functions of submandibular salivary glands of Wistar Han rats : influence of exposure period

Kouidhi-Lamloum, Wided

19 December 2012

Les glandes salivaires sont des glandes mixtes : la salive (produit exocrine) estimpliquée dans le maintien de l’homéostasie buccale alors que les secrétions endocrines (ex :facteurs de croissance) ont un rôle physiologique (gamétogénèse, ostéogenèse,hypertension…) Chez les mammifères, elles affichent un dimorphisme sexuel qui laisseentrevoir une sensibilité éventuelle à des xeno-hormones.Ce mémoire présente l’action de la génistéine (phyto-oestrogène) et/ou de la vinclozoline(anti-androgène) sur la glande submandibulaire (SM) de rat lors d’une exposition précoce viala mère (gestation-lactation) et lors d’une exposition pendant la période de croissance (dusevrage à l’âge adulte). Les glandes SM, prélevées au stade immature et jeune adulte, ont faitl’objet d’une analyse histologique et d’une étude de marqueurs moléculaire des fonctionsendocrines et exocrines associées aux processus gustatifs. L’exposition précoce ralenti ledéveloppement de la glande SM et augmente sélectivement la préférence au sucré des malesimmatures mais pas des adultes ; l’analyse moléculaire révèle une action sélective sur lesfonctions exocrines corrélée à celle sur les préférences, ainsi qu’une action sur les fonctionsendocrines (facteurs de croissances) qui s’inverse avec l’âge. L’exposition à partir du sevrageperturbe seulement les mâles qui présentent des altérations des structures sécrétrices coupléesà des modifications d’expression des récepteurs hormonaux et facteurs de croissance, maisaussi au taux sérique de l’EGF.Cette étude identifie la glande submandibulaire comme cible de perturbateurs endocriniens etpose la question des conséquences physiologiques à terme / The salivary glands are mixed glands: saliva (exocrine product) is involved inmaintaining oral homeostasis whereas endocrine secretions (eg growth factors) have aphysiological role (gametogenesis, osteogenesis, hypertension ..). In mammals, they displaysexual dimorphism suggesting a possible susceptibility to xeno-hormones.This manuscript presents the action of genistein (phytoestrogen) and/or vinclozolin (antiandrogenic)on the submandibular gland (SM) rats when performing an early exposure via themother (pregnancy, lactation) or an exposure during the growth period (from weaning toadulthood). The SM glands, collected at immature and young adult ages, have been analyzedaccording histological aspect and expression of molecular markers of endocrine and exocrinefunctions associated with gustatory process. The early exposure disrupted the development ofthe SM gland and selectively increases the sweet preference in immature males but not inadults; molecular analysis reveals a selective action on exocrine functions related to the sweetpreferences and also an action on endocrine functions (growth factors) which reverses withage. Exposure from weaning disrupts only the male salivary glands with alterations insecretory structures coupled with changes in expression of both, sex-hormone receptors andgrowth factors, but also in serum EGF.This study identifies the submandibular gland as a target for endocrine disruptors and raisesthe question of the further physiological consequences

Préférence au sucré

Gustine

Cystatine C

Mucine 10

EGF

NGF

TGF

Récepteur Androgène

Récepteur Progestérone

Granular Convoluted Tubule

Sweet Preference

Gustine

Cystatin C

Mucin 10

EGF

NGF

TGF

Androgen receptor

Progesterone Receptor

Granular Convoluted Tubule

571.8

612.4

612.8

Impact du bicarbonate de sodium sur la prévention de la néphropathie induite par le produit de contraste en chirurgie endovasculaire pour anévrysme de l’aorte

Brulotte, Véronique

12 1900

Introduction: L’approche endovasculaire pour la réparation d’anévrysmes aortiques s’associe à une utilisation importante de produit de contraste, qui peut causer une néphropathie induite par le produit de contraste (NIC) en postopératoire. L’hydratation intraveineuse peut réduire l’incidence de NIC, mais quel produit utiliser reste incertain. Nous avons évalué le bicarbonate de sodium, comparé au NaCl 0,9%, pour réduire l’incidence de NIC. Méthode: Nous avons mené une étude prospective, randomisée et contrôlée à double insu chez 34 patients subissant une chirurgie endovasculaire pour anévrysme aortique. Les patients des deux groupes (17 patients par groupe) ont reçu du bicarbonate de sodium ou du NaCl 0,9% à raison de 3 mL/kg/h pour une heure avant l’intervention puis 1 mL/kg/h jusqu’à 6 h après la fin de la chirurgie. Tous les patients ont reçu du N-acétylcystéine. L’objectif principal était l’incidence de NIC, définie comme une élévation de plus de 25% de la créatinine sérique 48 h suivant l’exposition au produit de contraste. Des biomarqueurs précoces de lésion rénale ont été mesurés. Résultats: Une NIC s’est développée chez 1 patient (5,88%) appartenant au groupe bicarbonate, comparé à aucun patient (0%) dans le groupe NaCl 0,9% (P = 0,31). Les biomarqueurs de lésion rénale étaient significativement augmentés dans les deux groupes après l’exposition au produit de contraste. Conclusions: Nous avons démontré un faible taux d’insuffisance rénale suivant une chirurgie endovasculaire aortique, que l’hydratation soit effectuée avec du bicarbonate ou du NaCl 0,9%, malgré une élévation des biomarqueurs de lésion rénale. / Background: The endovascular approach for the repair of aortic aneurysm involves the administration of large quantities of contrast media, which can cause contrast-induced nephropathy (CIN) in the post operative period. The only proven strategy to prevent CIN is intravenous hydration, but what type of infusion to use is not clear. We evaluated the efficacy of sodium bicarbonate, compared with NaCl 0.9%, to reduce the incidence of postoperative renal failure. Methods: We conducted a prospective, controlled, double-blind, randomized study in patients presenting for endovascular aortic aneurysm surgery. Patients in group A (n = 17) received sodium bicarbonate 3 mL/kg/h for 1 h before the procedure and then 1 mL/kg/h until 6 h after surgery, whereas patients in group B (n= 17) received the same amount of NaCl 0.9%. All patients received N-acetylcysteine. The primary end point was CIN, defined by serum creatinine greater than 25 % above baseline 48 h post operatively. Biomarkers of renal injury were measured. Results: CIN developed in one patient in the bicarbonate group (5,88%), compared with no patient in the NaCl 0,9% group (0%) (difference 5.88%;95% CI -5.3% to 17.06%, P = 0.31). Interleukin-18, N-acetyl-β-D-glucosaminidase and Kidney Injury Molecule-1 increased significantly in both groups after exposure to contrast media. Conclusions: We demonstrated a low rate of renal failure following endovascular aortic surgery using contrast media, regardless of whether bicarbonate or NaCl 0.9% was used for hydration, despite significant elevation in biomarkers of renal injury.

Anévrysme de l’aorte

créatinine

cystatine c

interleukine 18

KidneyInjury Molecule-1

N-acétyl-β-D-glucosaminidase

N-acétylcystéine

Neutrophilgelatinase-associatedlipocalin

Aortic aneurysm

creatinine

cystatin c

interleukin-18

Kidney Injury Molecule-1

N-acetyl-β-D-glucosaminidase

Impact du bicarbonate de sodium sur la prévention de la néphropathie induite par le produit de contraste en chirurgie endovasculaire pour anévrysme de l’aorte

Brulotte, Véronique

12 1900

Introduction: L’approche endovasculaire pour la réparation d’anévrysmes aortiques s’associe à une utilisation importante de produit de contraste, qui peut causer une néphropathie induite par le produit de contraste (NIC) en postopératoire. L’hydratation intraveineuse peut réduire l’incidence de NIC, mais quel produit utiliser reste incertain. Nous avons évalué le bicarbonate de sodium, comparé au NaCl 0,9%, pour réduire l’incidence de NIC. Méthode: Nous avons mené une étude prospective, randomisée et contrôlée à double insu chez 34 patients subissant une chirurgie endovasculaire pour anévrysme aortique. Les patients des deux groupes (17 patients par groupe) ont reçu du bicarbonate de sodium ou du NaCl 0,9% à raison de 3 mL/kg/h pour une heure avant l’intervention puis 1 mL/kg/h jusqu’à 6 h après la fin de la chirurgie. Tous les patients ont reçu du N-acétylcystéine. L’objectif principal était l’incidence de NIC, définie comme une élévation de plus de 25% de la créatinine sérique 48 h suivant l’exposition au produit de contraste. Des biomarqueurs précoces de lésion rénale ont été mesurés. Résultats: Une NIC s’est développée chez 1 patient (5,88%) appartenant au groupe bicarbonate, comparé à aucun patient (0%) dans le groupe NaCl 0,9% (P = 0,31). Les biomarqueurs de lésion rénale étaient significativement augmentés dans les deux groupes après l’exposition au produit de contraste. Conclusions: Nous avons démontré un faible taux d’insuffisance rénale suivant une chirurgie endovasculaire aortique, que l’hydratation soit effectuée avec du bicarbonate ou du NaCl 0,9%, malgré une élévation des biomarqueurs de lésion rénale. / Background: The endovascular approach for the repair of aortic aneurysm involves the administration of large quantities of contrast media, which can cause contrast-induced nephropathy (CIN) in the post operative period. The only proven strategy to prevent CIN is intravenous hydration, but what type of infusion to use is not clear. We evaluated the efficacy of sodium bicarbonate, compared with NaCl 0.9%, to reduce the incidence of postoperative renal failure. Methods: We conducted a prospective, controlled, double-blind, randomized study in patients presenting for endovascular aortic aneurysm surgery. Patients in group A (n = 17) received sodium bicarbonate 3 mL/kg/h for 1 h before the procedure and then 1 mL/kg/h until 6 h after surgery, whereas patients in group B (n= 17) received the same amount of NaCl 0.9%. All patients received N-acetylcysteine. The primary end point was CIN, defined by serum creatinine greater than 25 % above baseline 48 h post operatively. Biomarkers of renal injury were measured. Results: CIN developed in one patient in the bicarbonate group (5,88%), compared with no patient in the NaCl 0,9% group (0%) (difference 5.88%;95% CI -5.3% to 17.06%, P = 0.31). Interleukin-18, N-acetyl-β-D-glucosaminidase and Kidney Injury Molecule-1 increased significantly in both groups after exposure to contrast media. Conclusions: We demonstrated a low rate of renal failure following endovascular aortic surgery using contrast media, regardless of whether bicarbonate or NaCl 0.9% was used for hydration, despite significant elevation in biomarkers of renal injury.

Anévrysme de l’aorte

créatinine

cystatine c

interleukine 18

KidneyInjury Molecule-1

N-acétyl-β-D-glucosaminidase

N-acétylcystéine

Neutrophilgelatinase-associatedlipocalin

Aortic aneurysm

creatinine

cystatin c

interleukin-18

Kidney Injury Molecule-1

N-acetyl-β-D-glucosaminidase