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 Effect of Health Literacy in Low Estimated Glomerular Filtration and Diabetes

Johnston, Nicklett Johnston

01 January 2017

Health literacy is widespread, but its potential is not recognized. By not recognizing health literacy, patients have the burden of coping with diabetes with renal complications without full knowledge of their responsibility to their health. The focus of the project was to assess participants with diabetes with low health literacy and low mean glomerular filtration rate (eGFR). The project goal was achieved by the assessment of the participants' health literacy and eGFR before and after education for their diabetes, then assessed to determine if teaching the participants would improve their health literacy, lab values, and overall health. Participants were recruited by being patients of the designated clinic and screened for diabetes and low eGFR, for a total of 30 participants. The Brief Health Literacy Screen was used to measure health literacy. The health of the participants was appraised by the laboratory values of eGFR and fasting glucose. The project methodology was an observational design using correlation and 2-sample t analysis with the variables eGFR, fasting glucose, and health literacy. The variables were compared before and after the participants' education. Results showed health literacy with patient education was associated with greater patient self-efficacy and improved fasting glucose numbers, eGFR flows, and health literacy scores. The current health climate shows value in different types of health providers. Social change was defined by the project launching a nurse practitioner as the leader for advancing the treatment plans of chronic kidney disease. This project impacts social change by showing patients in the process of improved health and empowering the patients to be advocates of their own health.

Chronic kidney disease

Creatinine

Health literacy

Microalbumin urine

Medicine and Health Sciences

Nursing

Stanovení kreatininu pomocí pulsní amperometrie / Determination of creatinine using pulsed amperometry

Giampaglia, Dominika

January 2021

This diploma thesis deals with the determination of creatinine using a combination of flow injection analysis (FIA) or high-performance liquid chromatography (HPLC) with pulse amperometry, an electrochemical technique based on the application of potential pulses on a gold working electrode. The determination was performed in a basic environment of borate buffer with creatinine concentration of 1∙10-4 mol∙l-1 . The lenght of the cleaning and activation pulse was optimized as well as the pH of the running buffer. A cleaning pulse of +1.8 V was first applied to the electrode for 100 ms, then an activation potential of -0.5 V was applied for 150 ms and then a measuring potential of +0.2 V for 300 ms. The optimal pH was selected as pH=9,4. Methanol and acetonitrile were added to the borate buffer to test whether creatinine could be determined in presence of these organic solvents and whether flow injection analysis could be transformed into HPLC. Methanol in the system caused peak deformation, acetonitrile did not cause the peak deformation in the system, at higher contents the baseline was destabilized. Furthermore, the calibration dependence in the range of concentrations from 2.5∙10-4 mol∙l-1 to 5∙10-6 mol ∙ l-1 was measured using PAD in combination with FIA. At higher concentrations, peaks splitted....

THE ROLE OF RNASE L IN THE KIDNEY FUNCTION

Alghamdi, Norah

10 May 2019

No description available.

Chemistry

Immunology

Analytical Chemistry

Anatomy and Physiology

Animal Sciences

Animals

Biochemistry

Biology

Biomedical Research

Cellular Biology

RNase L

kidney

folic acid

acute kidney injury

creatinine

EGF

ADAM10

AKI

Novel electrochemical aptamer-based sensing mechanism inspired by selection strategies

Lyalina, Tatiana

01 1900

Des millions de patients souffrant d’insuffisance cardiaque bénéficieraient d’analyses sanguines hebdomadaires pour surveiller l’évolution de leur état de santé comme c’est le cas avec les personnes atteintes du diabète. Cependant, il n’existe pas de technologies d’analyses sanguines rapides et efficaces pour détecter des marqueurs d’insuffisance cardiaque, telle que la créatinine, la NT-proBNP et la troponine I par exemple. La possibilité pour les patients de surveiller leurs taux de créatinine régulièrement, du confort de chez soi, améliorerait largement leur qualité de vie ainsi que leur taux de survie. En suivant leur taux de créatinine, le patient pourrait prédire des signes d’insuffisance cardiaque, et ainsi faire ajuster leur plan de traitement en conséquence. Pour y arriver, les biocapteurs électrochimiques, dont un exemple est le glucomètre, représentent une classe prometteuse de dispositifs d’analyse sanguine puisqu’ils sont faciles à utiliser, rapides, peu coûteux, sensibles, stables et potentiellement universels. Les biocapteurs électrochimiques à base d’ADN pourraient potentiellement être adaptés en biocapteur de créatinine, par l’entremise d’aptamères. Le but de cette recherche est de développer un nouveau mécanisme de détection universel et efficace pouvant être adapté directement à partir des stratégies de sélection des aptamères. Pour ce faire, nous avons identifié et caractérisé un élément de bioreconnaissance sélectif pour la créatinine. Ensuite, nous avons conçu une nouvelle stratégie de détection et nous avons validé cette nouvelle stratégie par spectroscopie de fluorescence avant de l’adapter pour une détection électrochimique. Par la suite, nous avons optimisé les performances du biocapteur en modulant des paramètres analytiques tels que sa gamme linéaire et son gain de signal, tout en validant ses performances dans une matrice complexe comme le sérum. Les résultats de cette recherche suggèrent que la stratégie de conception du nouveau biocapteur électrochimique à base d’aptamère est prometteuse pour la détection efficace de biomarqueurs sanguins. Ce type de mécanisme pourrait être facilement adapté pour détecter d'autres molécules cliniquement pertinentes en modifiant simplement la stratégie de sélection de l'aptamère. / Millions of patients suffering from heart failure would greatly benefit from weekly blood analysis to help them manage their disease state like patients suffering from diabetes. However, no simple blood monitoring technologies detecting heart failure biomarkers, such as creatinine, NT-proBNP, and troponin I, are available. The ability to determine and regularly monitor the creatinine level in the home setting would greatly improve the patient’s quality of life and survival rate. Knowing the concentration of creatinine help to predict heart failure and to revise the treatment plan if the concentration of creatinine is abnormal. To achieve this, electrochemical sensors, like a glucometer, represent a promising class of blood analysis devices due to their ease of use, fast response, low cost, inherent sensitivity and stability, and potential universality. More specifically, DNA-based electrochemical biosensors could potentially be adapted into a creatinine sensor by using aptamers specific to a biomarker. To achieve this goal, we identified a selective biorecognition element for creatinine detection and characterized it. We also designed a novel sensing aptamer-based strategy and validated this strategy by fluorescent spectroscopy before transposing it into the electrochemical format. We then optimized the performance of the sensor by tuning its signal gain and characterizing the dynamic range while also validating its performance in serum. The results of this work suggest that the electrochemical aptamer-based strategy represents a promising sensing mechanism. We believe this mechanism could be easily adapted to detect other clinically relevant molecules by simply relying on the aptamer’s selection strategy.

Biocapteur

Capteur électrochimique

Aptamère

Créatinine

SELEX

Électrochimie

Sérum

Sang

Biosensor

Electrochemical sensor

Aptamer

Creatinine

Electrochemistry

Serum

Whole blood

Chemistry / Chimie (UMI : 0485)

Influence of Adult Males, Dietary Phytoestrogens, and an Index of In Utero Androgen Exposure on Sexual Development In The Female Mouse (Mus Musculus) / Males, Diet, Prenatal Androgens and Female Sexual Maturity

Khan, Ayesha

07 1900

<p> The age at which a juvenile female reaches sexual maturity can be modulated by a variety of environmental and social factors. Experiments described in this thesis were designed to enhance the current understanding of the relationships among three variables that influence the onset of sexual maturation in female mice (Mus musculus), including: [1] exposure to dietary phytoestrogens during development, [2] variations in prenatal androgens, and [3] the presence or absence of genetically-unrelated males after weaning. For the first time, age at onset of male-induced female puberty was investigated using non-invasive behavioural and fertility measures. Through enzyme immunoassay procedures, daily output of urinary creatinine, 17P-estradiol, and progesterone was profiled in developing females that were either isolated or exposed to adult males. Uterine and ovarian tissue was also measured in such females, and male exposure was observed to increase reproductive tissue mass and was influenced by prior androgen exposure in interaction with diet and male presence. Male-exposed females fed a diet containing phytoestrogens immediately became sexually receptive when housed directly with males, and they conceived earlier than females in other conditions. Females with longer anogenital distance, which reflects higher in utero androgen exposure, displayed more escape attempts and aggressive posturing in the direct presence of males, especially when they had been housed near males and fed the phytoestrogen-containing diet. Urinary 17P-estradiol was substantially reduced in females raised on the phytoestrogenfree diet. Urinary output of progesterone was not strongly influenced by diet. Maleexposed females ' output of progesterone and 17P-estradiol was more dynamic in comparison to that of isolated females. The size of this effect depended on diet, prior androgen exposure, and whether urinary steroid measures were adjusted by urinary creatinine. Urinary creatinine was elevated by the low phytoestrogen diet and reduced by male exposure. These data suggest that dietary phytoestrogens and in utero androgen exposure interact with presence or absence of males in determining the age at onset of sexual maturity in developing females. </p> <p> A final experiment was designed to examine two components of adult male urine, preputial gland emissions and unconjugated estrogens, that have been posited to act on females to advance reproductive maturation. Intact and preputialectomized males were compared in their output of urinary creatinine, 17~-estradiol, and testosterone, and in their influence on reproductive tissue in juvenile females. Lack of preputial glands did not hinder the capacity of males to induce uterine and ovarian growth in females. Male urinary creatinine was reduced by exposure to juvenile females. Creatinine-adjusted 17~estradiol and testosterone were greater in female-exposed males, regardless of whether the preputial glands were present. Based on these findings and those reported elsewhere, it is probable that male excreted urinary steroids are important in regulating reproductive changes in developing females exposed to males. </p> / Thesis / Doctor of Philosophy (PhD)

Modulation du cytochrome P450 dans un modèle murin d'insuffisance rénale chronique

Boisvert, Caroline

04 1900

Introduction : Les modèles murins sont grandement utilisés dans l’étude des maladies rénales et des pathologies associées. La concentration de la créatinine sérique est un bon indicateur de la filtration glomérulaire et en présence d’insuffisance rénale chronique (IRC), les concentrations de créatinine sérique (et la clairance) reflètent la sévérité de l’IRC. De plus, il a été démontré que l’IRC modifie le métabolisme des médicaments en diminuant l’activité et l’expression des enzymes hépatiques du cytochrome P450 (CYP450). Afin d’étudier la modulation du P450 par l’IRC avec un modèle murin et de confirmer nos résultats chez le rat, nous devons 1) développer un modèle d’IRC chez la souris, 2) mettre au point une technique de dosage des marqueurs de l’IRC et, 3) évaluer l’expression protéique du CYP450 en présence IRC. Matériel et Méthode : Trois modèles chirurgicaux d’IRC chez la souris ont été développés. Une méthode du dosage de la créatinine par chromatographie liquide à haute performance (CLHP) a été mise au point chez la souris et l’expression protéique du P450 a été mesurée par immunobuvardage de type Western. Résultats : Plusieurs paramètres de CLHP comme le pH, la concentration et le débit de la phase mobile modifient le pic d’élution et le temps de rétention de la créatinine. Concernant le modèle expérimental, on observe une perte de poids et une augmentation de la concentration plasmatique de la créatinine chez les souris avec une IRC. De plus, l’expression protéique de plusieurs isoformes du cytochrome P450 est modulée par l’IRC. Nous observons une diminution du CYP 2D de 42% (p < 0,01), du CYP 3A11 de 60% et du CYP 1A de 37% (p <0,01) par rapport aux souris témoins. On ne dénote aucun changement significatif au niveau de l’isoforme 2E1. Conclusion : Il est possible d’induire une insuffisance rénale chronique chez la souris suite à une néphrectomie. La technique de dosage de la créatinine par CLHP est précise et exacte et permet de caractériser la sévérité de l’IRC chez la souris. L’expression protéique du CYP450 est régulée à la baisse dans le foie des souris atteintes d’IRC. / Background: Mice models are widely used in renal studies. Seric creatinine concentration is used to evaluate glomerular filtration rate and is a good marker of chronic renal failure (CRF). It has been shown that CRF diminishes drug metabolism in the rat because of a downregulation of hepatic cytochrome P450 (CYP450) isoforms. To study CYP450 regulation in the mouse model, we needed to 1) develop a model of CRF in the mouse, 2) define a method of dosage of CRF markers, and 3) evaluate CYP450 protein expression in the liver of mice with CRF. Methods: Models of CRF were tested and sub-total nephrectomy was selected because of the efficacy and reproducibility to induce CRF. A high pressure liquid chromatography (HPLC) method for the dosage of creatinine in mice sera was developed. Liver protein expression of CYP1A1, CYP3A11, CYP2D and CYP2E1 was assessed by Western Blot analysis. Results: HPLC parameters such as pH, mobile phase concentration and flow rate modified the elution profile. Weight loss and high seric creatinine concentrations are seen in mice with CRF. Furthermore, protein expression of CYP1A, CYP3A11 and CYP2D was decreased in liver microsomes of mice with CRF by 37%, 60% and 42%, respectively (p<0.01) compared to sham-operated mice. We found no significant difference in the expression of CYP2E1. Conclusions: CRF models are reproducible in the mouse. The HPLC method for creatinine determination is precise and accurate, and can assess the severity of CRF. Hepatic protein expression of CYP450 is modulated in presence of CRF as in the rat.

Insuffisance rénale chronique

Métabolisme des médicaments

Cytochrome P450

Souris

Créatinine

Néphrectomie

Chronic renal failure

Drug metabolism

Mice

HPLC

Nephrectomy

Cytochrome P450

Creatinine

Efeitos decorrentes do preparo para radioiodoterapia do câncer de tireoide no ritmo de filtração glomerular renal: estudo randomizado comparando suspensão hormonal tireoidiana  com o uso do hormônio estimulador da tireoide recombinante humano (TSHrh) / Effects due radioiodine therapy for thyroid cancer in renal glomerular filtration rate: randomized study comparing thyroid hormone withdrawal with the use of recombinant human thyroid stimulating hormone (rhTSH)

George Barberio Coura Filho

25 February 2016

Foi estudado o ritmo de filtração glomerular (RFG) de pacientes com câncer bem diferenciado da tireoide submetidos à radioiodoterapia (RIT). O estudo avaliou o RFG durante estímulo do hormônio estimulador da tireoide (TSH) por suspensão da reposição hormonal tireoidiana (RHT) ou no uso do hormônio estimulador da tireoide recombinante humano (TSHrh), correlacionou o RFG com o perfil hormonal tireoidiano, avaliou o RFG durante e na semana após a RIT, avaliou o RFG e a dose efetiva de radiação para corpo inteiro e correlacionou métodos de estimativa de RFG. Vinte e oito pacientes incluídos em estudo clínico randomizado não cego foram divididos em dois grupos de 14 pacientes, sendo o grupo A (GA) submetido à suspensão da RHT e o grupo B (GB) ao uso do TSHrh. Os pacientes tiveram antes e após o estímulo do TSH a determinação do RFG por 51Cr-EDTA e coletas séricas do perfil hormonal tireoidiano e creatinina, albumina e ureia, e, após a RIT, colheram exames séricos de creatinina, albumina e ureia, e tiveram estimadas suas doses efetivas de corpo inteiro. Os exames de creatinina, albumina e ureia foram utilizados para estimar o RFG pelas equações de creatinina sérica, Modified Diet in Renal Disease (MDRD), e Cockcroft-Gault. O GA apresentou, pelo 51Cr-EDTA, variação de -18,5% do RFG de 94,4±18,6 mL/min antes da suspensão da RHT para 76,2±15,7 mL/min (p=0,0002) e o GB apresentou pelo 51Cr-EDTA variação de 4% do RFG de 90,8±18,4 mL/min antes do TSHrh para 92,6±15,2 mL/min (p=0,64). O RFG variou significativamente só no GA, sem apresentar proporcionalidade entre as variações do hormônio tireoidiano e do RFG. Não houve correlação do RFG com elevação do TSH. Por equações baseadas em creatinina, houve, no GA, queda do RFG durante toda a suspensão da RHT e estabilidade após o retorno da RHT, e, no GB, houve estabilidade do RFG durante todo o estudo. A dose efetiva de corpo inteiro não apresentou diferenças significativas entre os grupos (p=0,76). Na comparação entre o 51Cr-EDTA e as equações para estimativa de RFG, a correlação de Pearson foi de 0,78 para creatinina sérica, 0,79 para MDRD e 0,66 para CockcroftGault, e a comparação das variações do RFG observadas no GA entre o 51Cr-EDTA e a equação por creatinina sérica foram estatisticamente diferentes. Concluiu-se que o RFG apresenta redução na suspensão da RHT, relacionado ao hipotireoidismo e não à elevação de TSH, voltando a estabilizar após retorno da RHT, e que não varia no uso do TSHrh, que a dose efetiva de corpo inteiro não varia entre os grupos proporcionalmente ao RFG, e que a melhor correlação foi do 51Cr-EDTA com a equação MDRD / Glomerular filtration rate (GFR) was studied in well differentiated thyroid cancer patients referred for radioiodine therapy (RIT). The study evaluated GFR during thyroid stimulating hormone (TSH) stimulation after thyroid hormone withdrawal (THW) or after recombinant human thyroid stimulating hormone (rhTSH), correlated GFR with thyroid hormone profile, evaluated GFR during and in the week after RIT, evaluated GFR and whole body radiation effective dose, and correlated different methods for GFR determination. 28 patients were included in a non-blinded randomized clinical trial and divided in two groups of 14 patients, being group A (GA) stimulated by THW and group B (GB) stimulated by rhTSH. Patients had GFR determined by 51Cr-EDTA, as well as serum thyroid hormone profile, creatinine, albumin and urea before and after TSH stimulation, and after RIT had determined their serum creatinine, albumin and urea and whole body radiation effective dose. Creatinine, albumin and urea were used to estimate GFR by serum creatinine, Modified Diet in Renal Disease (MDRD), and Cockcroft-Gault equations. GA presented a -18,5% GFR variation by 51CrEDTA varying from 94,4 ± 18,6 mL/min before THW to 76,2±15,7 mL/min after THW (p=0,0002) while GB presented a 4% GFR variation by 51Cr-EDTA varying from 90,8 ± 18,4 mL/min before TSHrh to 92,6 ± 15,2 mL/min after rhTSH (p=0,64). GFR significantly varied only in GA without presenting proportionality with thyroid hormone variation. There was no correlation between rise in TSH levels and GFR. Creatinine equations demonstrated a sustained reduction in GFR during THW and GFR stability after thyroid hormone reposition, while GB presented stable GFR during the whole study. Whole body radiation effective dose didn\'t present significant differences between the two groups (p=0,76). Comparing 51Cr-EDTA and GFR estimative equations presented Pearson correlation score of 0,78 for serum creatinine, 0,79 for MDRD and 0,66 for Cockcroft-Gault, while comparison between variances in GA between 51Cr-EDTA e serum creatinine equation was significantly different. In conclusion GFR presents a reduction during THW related to hypothyroidism and not to TSH rise and stabilizing after thyroid hormone therapy, GFR does not vary during rhTSH, whole body radiation effective dose does not vary between the two groups proportionally to GFR, and that MDRD equation had the best correlation with 51Cr-EDTA

Creatinina

Dosimetria

Hipotireoidismo

Hormônios hipofisários

Hormônios tireóideos

Medicina nuclear

Neoplasias da glândula tireoide

Proteção radiológica

Taxa de filtração glomerular

Tireotropina

Creatinine

Dosimetry

Glomerular filtration rate

Hypothyroidism

Nuclear medicine

Pituitary hormones

Radiological protection

Thyroid hormone

Thyroid neoplasms

Thyrotropin

Muscle Wasting in Non-end Stage Chronic Kidney Disease : Determinants and Outcomes / Faible masse musculaire évaluée par la créatininurie des 24h dans la maladie rénale chronique : déterminants et risques associés

Tynkevich, Elena

10 December 2014

Faible masse musculaire a été peu étudiée chez les patients avant le stade terminal de la maladie rénale chronique (MRC). Nous avons évalué la masse musculaire à partir de la créatininurie des 24h pour étudier ses déterminants, son évolution avec le déclin de la fonction rénale ainsi que ses liens avec les risques de progression vers l’insuffisance rénale terminale traitée (IRTT) et de décès avant IRTT. Dans la cohorte NephroTest incluant 1429 patients avec une MRC stades 1 à 4, le débit de filtration glomérulaire a été mesuré par la clairance du 51Cr-EDTA (DFGm) et estimé par l’équation CKD EPI (DFGe). La créatininurie moyenne à l’inclusion diminuait de 15.3±3.1 à 12.1±3.3 mmol/24 chez les hommes et de 9.6±1.9 à 7.6±2.5 chez les femmes, pour une baisse du DFGm de ≥ 60 à < 15 mL/min/1.73 m2. Être plus âgé, avoir un diabète, un faible IMC ou un niveau faible de protéinurie et d’apports protidiques était associé à un niveau faible de créatininurie. Un déclin annuel du DFGm de 5 mL/min/1.73 m2 était lié à une baisse de créatininurie, indépendamment de ces déterminants. Au cours d’un suivi médian de 3.6 ans, 229 patients ont développé une IRTT, et 113 sont décédés avant IRTT. Après ajustement sur les facteurs de confusion, le hasard ratio (HR) était de 1.6 (0.88-2.9) pour le risque de décès et de 0.60 (0.39-0.91) pour le risque d’IRTT, dans le 1er vs 4ème quartile de créatininurie. La baisse de la créatininurie apparait précocement dans la MRC et est liée au décès avant dialyse. La diminution du risque d’IRTT pourrait s’expliquer par un démarrage plus tardif de la dialyse en raison d’une surestimation du DFGm par le DFGe chez les patients avec une faible créatininurie. / Mainly described in patients on dialysis, muscle wasting has received little attention in early stage chronic kidney disease (CKD). We used 24-hour creatininuria to assess determinants of low muscle mass and its putative associations with CKD outcomes, using data from the NephroTest cohort, including 1429 non-dialysis patients with CKD stages 1 to 5. Kidney function was assessed with both measured (mGFR, by 51Cr-EDTA renal clearance) and estimated glomerular filtration rate (eGFR, by CKD-EPI equation). End-stage renal disease (ESRD) and pre-ESRD death were the main studied outcomes. The mean baseline creatininuria decreased from 15.3±3.1 to 12.1±3.3 mmol/24 h in men and from 9.6±1.9 to 7.6±2.5 in women, when mGFR fell from ≥ 60 to < 15 mL/min/1.73 m2. Other determinants of low creatininuria were an older age, diabetes, a lower body mass index, a lower level of proteinuria or protein intake. A fast annual decline in mGFR of 5 mL/min/1.73 m2 was linked with a 2-fold decrease in creatininuria, independent of changes in protein intake and other determinants of muscle mass. Over a median follow-up of 3.6 years, 229 patients developed ESRD and 113 patients died before ESRD. After adjustment for confounders, patients with low muscle mass showed a significantly higher risk for pre-ESRD death (HR 1.6, 95% CI 0.88-2.9), but a lower risk for ESRD (HR 0.60, 95% CI 0.39-0.91). The latter was reversed (HR 1.5, 95% CI 1.01-2.4) when mGFR was replaced by eGFR. Decrease in 24-hour creatininuria may appear early in CKD patients, is related to pre-ESRD death. The lower risk for ESRD may reflect later dialysis start due to overestimation of true GFR by eGFR in patients with low muscle mass.

Créatininurie

Débit de filtration glomérulaire

Décès

Épidémiologie

Faible masse musculaire

Insuffisance rénale terminale

Maladies rénale chronique

Malnutrition

Chronic kidney disease

Epidemiology and outcomes

Glomerular filtration rate

Muscle wasting

Urinary creatinine excretion

Malnutrition

End-stage chronic kidney disease

Efeitos decorrentes do preparo para radioiodoterapia do câncer de tireoide no ritmo de filtração glomerular renal: estudo randomizado comparando suspensão hormonal tireoidiana  com o uso do hormônio estimulador da tireoide recombinante humano (TSHrh) / Effects due radioiodine therapy for thyroid cancer in renal glomerular filtration rate: randomized study comparing thyroid hormone withdrawal with the use of recombinant human thyroid stimulating hormone (rhTSH)

Coura Filho, George Barberio

25 February 2016

Foi estudado o ritmo de filtração glomerular (RFG) de pacientes com câncer bem diferenciado da tireoide submetidos à radioiodoterapia (RIT). O estudo avaliou o RFG durante estímulo do hormônio estimulador da tireoide (TSH) por suspensão da reposição hormonal tireoidiana (RHT) ou no uso do hormônio estimulador da tireoide recombinante humano (TSHrh), correlacionou o RFG com o perfil hormonal tireoidiano, avaliou o RFG durante e na semana após a RIT, avaliou o RFG e a dose efetiva de radiação para corpo inteiro e correlacionou métodos de estimativa de RFG. Vinte e oito pacientes incluídos em estudo clínico randomizado não cego foram divididos em dois grupos de 14 pacientes, sendo o grupo A (GA) submetido à suspensão da RHT e o grupo B (GB) ao uso do TSHrh. Os pacientes tiveram antes e após o estímulo do TSH a determinação do RFG por 51Cr-EDTA e coletas séricas do perfil hormonal tireoidiano e creatinina, albumina e ureia, e, após a RIT, colheram exames séricos de creatinina, albumina e ureia, e tiveram estimadas suas doses efetivas de corpo inteiro. Os exames de creatinina, albumina e ureia foram utilizados para estimar o RFG pelas equações de creatinina sérica, Modified Diet in Renal Disease (MDRD), e Cockcroft-Gault. O GA apresentou, pelo 51Cr-EDTA, variação de -18,5% do RFG de 94,4±18,6 mL/min antes da suspensão da RHT para 76,2±15,7 mL/min (p=0,0002) e o GB apresentou pelo 51Cr-EDTA variação de 4% do RFG de 90,8±18,4 mL/min antes do TSHrh para 92,6±15,2 mL/min (p=0,64). O RFG variou significativamente só no GA, sem apresentar proporcionalidade entre as variações do hormônio tireoidiano e do RFG. Não houve correlação do RFG com elevação do TSH. Por equações baseadas em creatinina, houve, no GA, queda do RFG durante toda a suspensão da RHT e estabilidade após o retorno da RHT, e, no GB, houve estabilidade do RFG durante todo o estudo. A dose efetiva de corpo inteiro não apresentou diferenças significativas entre os grupos (p=0,76). Na comparação entre o 51Cr-EDTA e as equações para estimativa de RFG, a correlação de Pearson foi de 0,78 para creatinina sérica, 0,79 para MDRD e 0,66 para CockcroftGault, e a comparação das variações do RFG observadas no GA entre o 51Cr-EDTA e a equação por creatinina sérica foram estatisticamente diferentes. Concluiu-se que o RFG apresenta redução na suspensão da RHT, relacionado ao hipotireoidismo e não à elevação de TSH, voltando a estabilizar após retorno da RHT, e que não varia no uso do TSHrh, que a dose efetiva de corpo inteiro não varia entre os grupos proporcionalmente ao RFG, e que a melhor correlação foi do 51Cr-EDTA com a equação MDRD / Glomerular filtration rate (GFR) was studied in well differentiated thyroid cancer patients referred for radioiodine therapy (RIT). The study evaluated GFR during thyroid stimulating hormone (TSH) stimulation after thyroid hormone withdrawal (THW) or after recombinant human thyroid stimulating hormone (rhTSH), correlated GFR with thyroid hormone profile, evaluated GFR during and in the week after RIT, evaluated GFR and whole body radiation effective dose, and correlated different methods for GFR determination. 28 patients were included in a non-blinded randomized clinical trial and divided in two groups of 14 patients, being group A (GA) stimulated by THW and group B (GB) stimulated by rhTSH. Patients had GFR determined by 51Cr-EDTA, as well as serum thyroid hormone profile, creatinine, albumin and urea before and after TSH stimulation, and after RIT had determined their serum creatinine, albumin and urea and whole body radiation effective dose. Creatinine, albumin and urea were used to estimate GFR by serum creatinine, Modified Diet in Renal Disease (MDRD), and Cockcroft-Gault equations. GA presented a -18,5% GFR variation by 51CrEDTA varying from 94,4 ± 18,6 mL/min before THW to 76,2±15,7 mL/min after THW (p=0,0002) while GB presented a 4% GFR variation by 51Cr-EDTA varying from 90,8 ± 18,4 mL/min before TSHrh to 92,6 ± 15,2 mL/min after rhTSH (p=0,64). GFR significantly varied only in GA without presenting proportionality with thyroid hormone variation. There was no correlation between rise in TSH levels and GFR. Creatinine equations demonstrated a sustained reduction in GFR during THW and GFR stability after thyroid hormone reposition, while GB presented stable GFR during the whole study. Whole body radiation effective dose didn\'t present significant differences between the two groups (p=0,76). Comparing 51Cr-EDTA and GFR estimative equations presented Pearson correlation score of 0,78 for serum creatinine, 0,79 for MDRD and 0,66 for Cockcroft-Gault, while comparison between variances in GA between 51Cr-EDTA e serum creatinine equation was significantly different. In conclusion GFR presents a reduction during THW related to hypothyroidism and not to TSH rise and stabilizing after thyroid hormone therapy, GFR does not vary during rhTSH, whole body radiation effective dose does not vary between the two groups proportionally to GFR, and that MDRD equation had the best correlation with 51Cr-EDTA

Creatinina

Creatinine

Dosimetria

Dosimetry

Glomerular filtration rate

Hipotireoidismo

Hormônios hipofisários

Hormônios tireóideos

Hypothyroidism

Medicina nuclear

Neoplasias da glândula tireoide

Nuclear medicine

Pituitary hormones

Proteção radiológica

Radiological protection

Taxa de filtração glomerular

Thyroid hormone

Thyroid neoplasms

Thyrotropin

Tireotropina