Your search keyword '"Oliveira, Carla Raquel Pereira"' showing total 12 results

1. The Impact of Diabetes Education on Continuous Glucose Monitoring in SUS-Dependent Patients in a Northeastern Brazilian City

Author

Borges, Lysandro Pinto, primary, de Jesus, Pamela Chaves, additional, de Souza, Jessiane Bispo, additional, Silva, Deise Maria Rego Rodrigues, additional, Moura, Pedro Henrique Macedo, additional, Santos, Ronaldy Santana, additional, Barreto, Marina dos Santos, additional, Guimarães, Adriana Gibara, additional, da Mota Santana, Lucas Alves, additional, da Fonseca, Dennyson Leandro Mathias, additional, Barreto, Ikaro Daniel de Carvalho, additional, de Mello Silva, Breno, additional, Oliveira, Carla Raquel Pereira, additional, Rezende, Karla Freire, additional, Melo, Naira Horta, additional, Santos, Elenalda Ferreira dos, additional, Queiroz, Carmem Lúcia Matias de, additional, Xavier, Lucia Helena Modesto, additional, Cabral-Marques, Otávio, additional, and Silva, Eloia Emanuelly Dias, additional

Published

2024

2. Lack of Evidence of Premature Atherosclerosis in Untreated Severe Isolated Growth Hormone (GH) Deficiency due to a GH-Releasing Hormone Receptor Mutation

Author

Oliveira, Joselina Luzia Menezes, Marques-Santos, Celi, Barreto-Filho, José Augusto, Filho, Roberto Ximenes, Britto, Allan Valadão de Oliveira, Souza, Anita Hermínia Oliveira, Prado, Clarisse Miranda, Oliveira, Carla Raquel Pereira, Pereira, Rossana Maria C., Vicente, Tábita de Almeida Ribeiro, Farias, Catarine Teles, Aguiar-Oliveira, Manuel Hermínio, and Salvatori, Roberto

Published

2006

3. Brazilian adult individuals with untreated isolated GH deficiency do not have accelerated subclinical atherosclerosis

Author

Burgos, Ursula Maria Moreira Costa, Oliveira, Carla Raquel Pereira, Salvatori, Roberto, Barreto Filho, José Augusto Soares, Campos, Viviane Correia, Oliveira, Francielle Temer de, Rocha, Ivina Elaine dos Santos, Oliveira, Joselina Luzia Menezes, Silva, Wersley Araújo, and Oliveira, Manuel Herminio de Aguiar

Subjects

Aterosclerose coronária, Multi-detector CT, Coronary atherosclerosis, Isolated growth hormone deficiency, Calcium score

Abstract

GH and its principal mediator IGF1 have important effects on metabolic and cardiovascular (CV) status. While acquired GH deficiency (GHD) is often associated with increased CV risk, the consequences of congenital GHD are not known. We have described a large group of patients with isolated GHD (IGHD) due to a homozygous mutation (c.57C1GOA) in the GH releasing hormone receptor gene, and shown that adult GH-naı¨ve individuals have no evidence of clinically evident premature atherosclerosis. To test whether subclinical atherosclerosis is anticipated in untreated IGHD, we performed a cross-sectional study of 25 IGHD and 27 adult controls matched for age and gender. A comprehensive clinical and biochemical panel and coronary artery calcium scores were evaluated by multi-detector tomography. Height, weight, IGF1, homeostasis model assessment of insulin resistance, creatinine and creatininekinase were lower in the IGHD group. Median and interquartile range of calcium scores distribution was similar in the two groups: IGHD 0(0) and control 0(4.9). The vast majority of the calcium scores (20 of 25 IGHD (80%) and 18 of 27 controls (66.6%)) were equal to zero (difference not significant). There was no difference in the calcium scores classification. None of IGHD subjects had minimal calcification, which were present in four controls. Three IGHD and four controls had mild calcification. There were two IGHD individuals with moderate calcification and one control with severe calcification. Our study provides evidence that subjects with congenital isolated lifetime and untreated severe IGHD do not have accelerated subclinical coronary atherosclerosis.

Published

2016

4. Avaliação da eficiência e desfecho da triagem e manejo da PKU no Estado de Sergipe, Brasil

Author

Ramalho, Antônio Roberto de Oliveira, Ramalho, Roberto Jose Rabelo, Oliveira, Carla Raquel Pereira, Magalhães, Marta Maria Galvão de Sousa, Santos, Elenilde Gomes, Matos, Diana O., Oliveira, Mario C. P., Oliveira, André L. P., Oliveira, Manuel Herminio de Aguiar, and Sarmento, Polyana Maria Palmeira

Subjects

Coverage, Cobertura, Screening neonatal, Phenylalanine, Incidence, Incidência, Phenylketonuria, Fenilcetonúria, Fenilalanina, Triagem neonatal

Abstract

Objectives: Phenylketonuria (PKU) was the first inherited metabolic disease known to cause mental retardation for which a newborn screening program (NBS) was developed. The objective of this study was to evaluate the effectiveness of PKU NBS and the management of cases in the northeastern Brazilian state of Sergipe (SE). Materials and methods: We reviewed the phenylalanine concentrations in filter-paper collected from the heel (PKUneo) of 43,449 newborns; blood concentrations obtained by venipuncture in the subjects with abnormal PKUneo; the children’s age at several phases of the program, the incidence of the disease from January 2007 to June 2008; and metabolic control of the patients. Results: The coverage of NBS/SE was 78.93%. The children’s age was 10 ± 7 days at PKUneo collection. Twelve children were recalled based on the PKUneo cutoff value at 28 ± 13 days. From these, the concentrations of phenylalanine collected by venipuncture were normal in five children. The incidence of hyperphenylalaninemia was 1/43,449, and of PKU was 1/8,690 (5 cases). One suspected subject died. Another death occurred in the cohort, in a confirmed PKU case. PKU treatment began within 51 ± 12 days of life. In the four patients under dietary phenylalanine restriction, metabolic control was often difficult. Conclusions: PKU NBS/SE has satisfactory coverage and adequate cutoff for recalling patients and diagnosis, but the onset of treatment is delayed, and follow-up metabolic control is frequently inadequate._________________________________________________________________________________________ RESUMO: Objetivos: A fenilcetonúria (PKU) foi a primeira causa metabólica hereditária de retardamento mental para a qual foi desenvolvido um programa de triagem em recém-nascidos (NBS). O objetivo deste estudo foi avaliar a eficácia do NBS para a PKU e o manejo dos casos em Sergipe (SE), Brasil. Materiais e métodos: Revisamos as concentrações de fenilalanina no filtro de papel coletado do calcanhar (PKUneo) de 43.449 recém-nascidos, suas concentrações de sangue obtidas por punção venosa em indivíduos com PKUneo anormal, a idade das crianças em diversas fases do programa, a incidência da doença no período de janeiro de 2007 a junho de 2008 e o controle metabólico dos pacientes. Resultados: A cobertura da NBS/SE foi de 78,93%. A idade das crianças era de 10 ± 7 dias na coleta de PKUneo. Doze crianças foram reconvocadas com base no ponto de corte de PKUneo aos 28 ± 13 dias de idade. Destas, as concentrações de fenilalanina por venipunctura foram normais em cinco. A incidência da hiperfenilalaninemia foi 1/43.449 e de PKU foi 1/8.690 (5 casos), e um indivíduo suspeito foi a óbito. Outro óbito ocorreu na coorte em um caso de PKU confirmado. O tratamento para a PKU começou com 51 ± 12 dias. Nos quatro pacientes sob restrição de fenilalanina alimentar, o controle metabólico foi frequentemente difícil. Conclusões: PKU NBS/SE apresenta uma cobertura satisfatória e ponto de corte adequado para reconvocação e diagnóstico, mas o início do tratamento é atrasado e o controle no seguimento é frequentemente inadequado.

Published

2014

5. Comparação entre a resposta de crescimento ao tratamento com hormônio de crescimento (GH) em crianças com insensibilidade parcial ao GH ou deficiência de GH leve

Author

Cardoso, Daniela Felix, Martinelli Junior, Carlos Eduardo, Campos, Viviane Correia, Santos, Elenilde Gomes, Rocha, Ivina Elaine dos Santos, Oliveira, Carla Raquel Pereira, Vicente, Tábita de Almeida Ribeiro, Pereira, Rossana Maria Cahino, Pereira, Francisco de Assis, Cartaxo, Carla Kalline Alves, Milani, Soraya Lopes Sader, Oliveira, Mario C. P., Melo, Enaldo Vieira de, Oliveira, André L. P., and Oliveira, Manuel Herminio de Aguiar

Subjects

Idiopathic short stature, Tratamento com hormônio do crescimento, Deficiência de hormônio do crescimento, Growth hormone therapy, Baixa estatura idiopática, Growth hormone deficiency, Partial GH insensitivity, Insensibilidade parcial ao GH

Abstract

Objectives: GH therapy is still controversial, except in severe GH deficiency (SGHD). The objective of this study was to compare the response to growth hormone (GH) therapy in children with partial GH insensitivity (PGHIS) and mild GH deficiency (MGHD) with those with SGHD. Subjects and methods: Fifteen PGHIS, 11 MGHD, and 19 SGHD subjects, followed up for more than one year in the Brazilian public care service, were evaluated regarding anthropometric and laboratory data at the beginning of treatment, after one year (1st year) on treatment, and at the last assessment (up to ten years in SGHD, up to four years in MGHD, and up to eight years in PGHIS). Results: Initial height standard deviation score (SDS) in SGHD was lower than in MGHD and PGHIS. Although the increase in 1st year height SDS in comparison to initial height SDS was not different among the groups, height-SDS after the first year of treatment remained lower in SGHD than in MGHD. There was no difference in height-SDS at the last assessment of the children among the three groups. GH therapy, in the entire period of observation, caused a trend towards lower increase in height SDS in PGHIS than SGHD but similar increases were observed in MGHD and SGHD. Conclusion: GH therapy increases height in PGHIS and produces similar height effects in MGHD and SGHD. _________________________________________________________________________________________ RESUMO: Objetivos: O tratamento com GH é ainda controverso, salvo na deficiência grave de GH (SGHD). O objetivo deste estudo foi comparar a resposta ao tratamento com GH em indivíduos com insensibilidade parcial ao GH (PGHIS) e na deficiência moderada do GH (MGHD) com SGHD. Sujeitos e métodos: Quinze pacientes com PGHIS, 11 com MGHD e 19 com SGHD, seguidos por mais de um ano no Sistema Único de Saúde, foram avaliados antropométrica e laboratorialmente, no início, com um ano de tratamento e na última avaliação (tempo máximo de dez anos na SGHD, quatro anos na MGHD e oito anos na PGHIS). Resultados: O escore de desvio-padrão (EDP) da estatura inicial foi menor nos indivíduos com SGHD do que naqueles com MGHD e PGHIS. Embora o aumento no EDP da estatura no primeiro ano em comparação com o inicial não fosse diferente entre os grupos, o EDP da altura no primeiro ano de tratamento permaneceu menor na SGHD que na MGHD. Não houve diferença no EDP da estatura na última avaliação entre os três grupos. O tratamento com GH, no período completo da observação, provocou uma tendência a menor aumento no EDP da estatura nos pacientes com PGHIS que naqueles com SGHD, entretanto aumentos semelhantes foram encontrados nos grupos MGHD e SGHD. Conclusão: O tratamento com GH aumentou a estatura nos indivíduos com PGHIS e produziu efeitos similares na estatura em MGHD e SGHD.

Published

2014

6. Lifetime congenital isolated GH deficiency does not protect from the development of diabetes

Author

Vicente, Tábita de Almeida Ribeiro, Rocha, Ivina Elaine dos Santos, Salvatori, Roberto, Oliveira, Carla Raquel Pereira, Pereira, Rossana Maria Cahino, Souza, Anita Herminia Oliveira, Campos, Viviane Correia, Santos, Elenilde Gomes, Araujo, Rachel Diniz Correia de, Valença, Eugenia Herminia Oliveira, Pereira, Carlos de Carvalho Epitácio, Oliveira, Mario C. P., Mari, Andrea, and Oliveira, Manuel Herminio de Aguiar

Subjects

GH deficiency, congenital, hereditary, and neonatal diseases and abnormalities, β-cell function, Diabetes, nutritional and metabolic diseases, Sensibilidade à insulina, Insulin sensitivity, Deficiência de GH

Abstract

Objectives: Adult subjects with untreated, lifetime, isolated GH deficiency (IGHD) due to a homozygous GHRH receptor gene mutation (MUT/MUT) residing in Itabaianinha, Brazil, present with lower BMI, higher prevalence of impaired glucose tolerance (IGT), increased insulin sensitivity (IS), and reduced β-cell function (βCF) when compared with non-BMI-matched homozygous normal controls. However, the prevalence of diabetes mellitus (DM) in this cohort is unknown. Comparing their IS and βCF with BMI-matched individuals heterozygous for the same mutation (MUT/N) may be useful to elucidate the role of the GH–IGF1 axis in IS and βCF. The purposes of this work were to verify the prevalence of IGT and DM in adult MUT/MUT subjects from this kindred and to compare IS and βCF in MUT/MUT and MUT/N. Design: Cross-sectional study. Methods: We studied most (51) of the living IGHD adults of this kindred who are GH naive. The oral glucose tolerance test (OGTT) could be performed in 34 subjects, fasting glucose was measured in 15, while two had a previous diagnosis of DM. The OGTT results of 24 MUT/MUT subjects were compared with those of 25 BMI-matched MUT/N subjects. IS was assessed by homeostatic model assessment of insulin resistance (HOMA–IR), quantitative IS check index, and oral glucose IS index for 2 and 3 h. βCF was assayed by HOMA-β, insulinogenic index, and the area under the curve of insulin:glucose ratio. Results The prevalence of DM and IGT in IGHD was 15.68 and 38.23% respectively. IS was increased and βCF was reduced in MUT/MUT in comparison with MUT/N. Conclusions: Lifetime, untreated IGHD increases IS, impairs βCF, and does not provide protection from diabetes.

Published

2013

7. Emerging role of the GH/IGF-I on cardiometabolic control

Author

Oliveira, Carla Raquel Pereira, Moreno, Rafael Alexandre Meneguz, Oliveira, Manuel Herminio de Aguiar, and Barreto Filho, José Augusto Soares

Subjects

Metabolismo, Lipólisis, Lipólise, Lypolisis, Metabolism, Factor de crecimiento insulin-like I, Grelina, Fator de crescimento insulin-like I, Resistência à insulina, Insulin-like growth factor I, Insulin resistance, Resistencia a la insulina, Ghrelin

Abstract

O hormônio de crescimento (GH), principal regulador do crescimento pós-natal, tem importantes ações metabólicas em diferentes tecidos, sinérgicas ou até antagônicas às do fator de crescimento semelhante à insulina tipo I (IGF-I), produzido sobretudo no fígado após ligação do GH ao seu receptor. Experimentos em modelos animais indicam um papel importante do GH na resistência a insulina, enquanto o papel do IGF-I nessa condição ainda não está completamente elucidado. Em humanos, o GH promove aumento da lipólise e da oxidação lipídica, enquanto o IGF-I desencadeia o aumento da oxidação lipídica apenas cronicamente. Enquanto as ações sobre o crescimento são tempo limitado, as ações metabólicas e cardiovasculares do eixo GH/IGF-I perduram durante toda a vida. Os potenciais efeitos anabólicos do GH têm sido utilizados em condições crônicas e hipercatabólicas, embora as investigações sobre os desfechos clínicos ainda sejam escassas. Neste artigo, pretendemos revisar as ações metabólicas do GH oriundas de modelos animais, os estudos em humanos normais e indivíduos com deficiência de GH, diabete melito tipo 1, síndrome metabólica, estados hipercatabólicos e a relação do eixo GH/IGF-I com as adipocinas, disfunção endotelial e aterogênese._________________________________________________________________________________________ ABSTRACT: Growth hormone (GH), the main regulator for post-natal growth, has important metabolic actions on different tissues, similar or opposite to insulin like growth factor I (IGF-I), mainly produced by the liver after the binding of GH to its receptor. Experiments with animal models indicate an important role of GH on insulin resistance although the IGF-I role is not yet completely established. In humans, GH promotes an increase on lypolisis and lipid oxidation, while IGF-I leads to an increase on lipid oxidation only in a chronic way. While growth actions are time-limited, metabolic and cardiovascular actions of the GH/IGF-I axis are throughout life. GH anabolic effects have been used on chronic and hypercatabolic conditions, although investigations on the clinical outcomes are still scarce. In this paper, we intend to review GH metabolic actions experienced by animal models, studies with normal humans and GH deficient individuals, individuals with diabetes mellitus type 1 and metabolic syndrome individuals, hypercatabolic states and the relationship between GH and adipokines, endothelial disfunction and atherogenesis._________________________________________________________________________________________ RESUMEN: La hormona de crecimiento (GH), principal regulador del crecimiento postnatal, tiene importantes acciones metabólicas en diversos tejidos, sinérgicas o incluso antagónicas a las del factor de crecimiento, a semejanza de la insulina tipo I (IGF-I) producido, principalmente, en el hígado y después del vínculo del GH con su receptor. Experimentos en modelos animales indican un papel importante del GH en la resistencia a la insulina, mientras que el papel del IGF-I en esa condición, todavía no está completamente elucidado. En los humanos, el GH genera el aumento de la lipólisis y de la oxidación lipídica, mientras que el IGF-I desencadena el aumento de la oxidación lipídica solamente desde el punto de vista crónico. Mientras las acciones sobre el crecimiento son de tiempo limitado, las acciones metabólicas y cardiovasculares del eje GH/IGF-I duran toda la vida. Los efectos potenciales anabólicos del GH han sido utilizados en condiciones crónicas e hipercatabólicas, aunque las investigaciones sobre los desenlaces clínicos todavía sean escasas. En este artículo, pretendemos revisar las acciones metabólicas del GH provenientes de modelos animales, los estudios en humanos normales y en individuos con deficiencia de GH, diabetes mellitus tipo 1, síndrome metabólico, estados hipercatabólicos y la relación del eje GH/IGF-I con las adipocinas, disfunción endotelial y aterogénesis.

Published

2011

8. ADIPOKINES, URINARY ALBUMIN EXCRETION, INSULIN SENSITIVITY AND BETA CELL FUNCTION IN ISOLATED GROWTH HORMONE DEFICIENCY

Author

Oliveira, Carla Raquel Pereira and Barreto Filho, José Augusto Soares

Subjects

GH deficiency, Adipokines, CIENCIAS DA SAUDE::MEDICINA [CNPQ], Excreção urinária de albumina, Sensibilidade insulínica, Insulin sensitivity, Adipocinas, Deficiência de GH, Urinary albumin excretion

Abstract

The aim of this study was to assess the dissociation between the presence of cardiovascular risk factors, and the lack of premature atherosclerosis and left venticular hipertrophy (LVH) in isolated GH deficiency (IGHD) due to a mutation in the GH releasing hormone receptor gene. A two step protocol was performed. In the first experiment, serum adiponectin and leptin, and urinary albumin excretion (UAE) were studied in 20 IGHD individuals (7 M/ 13 F; 50,8 ± 14,6 years) and 22 control subjects (C) (8 M/ 14 F; 49,9 ± 11.5 years). IGHD subjects in comparison to C presents high adiponectin levels (p= 0,041) whereas leptin and UAE were similar. In the second experiment, oral glucose tolerance test (1,75 g/Kg in IGHD and 75 g in C) with glucose and insulin mesuarements at 0, 30, 60, 90, 120 e 180 minutes was performed in 24 IGHD subjects (12 M/ 12 F; 39,25 ± 11,73 years) and 25 C subjects (14 M/ 11 F; 39,96 ± 12,49 years). Insulin sensitivity (IS) was assessed by HOMAir, lower values, higher IS; QUICKI, OGIS 2 and OGIS, higher values, higher IS (for the three parameters). Beta cell function was assayed by HOMA-beta, insulinogenic index and area under the curve of the relation between insulin and glucose (AUC I/G). ANOVA indicated glucose response was higher (p

Published

2010

9. Long time consequences of the growth hormone deficiency

Author

Oliveira, Carla Raquel Pereira, Pereira, Rossana Maria Cahino, Barreto Filho, José Augusto Soares, and Oliveira, Manuel Herminio de Aguiar

Subjects

Hormônio do crescimento, Deficiência de hormônio de crescimento, Growth hormone deficiency, Growth hormone

Abstract

Este artigo descreve as conseqüências puras, em longo prazo, da deficiência isolada e vitalícia do hormônio de crescimento (GH) porque usa um modelo único de resistência ao hormônio liberador do GH (GHRH), em virtude da mutação homozigótica no gene do receptor do GHRH, em uma centena de indivíduos acometidos. Elas incluem baixa estatura grave com estatura final entre -9,6 a -5,2 desvios-padrão abaixo da média, com redução proporcional das dimensões ósseas, redução do volume da adenohipófise corrigido para o volume craniano e da tireóide, do útero, do baço e da massa ventricular esquerda, todos corrigidos para a superfície corporal, em contraste com o tamanho de pâncreas e fígado, maior que o de controles, quando igualmente corrigidos. As alterações características da composição corporal incluem redução acentuada da quantidade de massa magra (kg) e aumento do percentual de gordura com depósito predominante no abdome. Nos aspectos metabólicos são encontrados aumento de colesterol total e LDL, redução de insulina e do índice de resistência à insulina homeostasis model assessment, acompanhados de aumento da proteína C reativa de alta sensibilidade e da elevação da pressão arterial sistólica nos adultos, embora sem evidências de aterosclerose precoce. Outros achados incluem resistência óssea menor, embora acima do limiar de fraturas, puberdade atrasada, fertilidade normal, paridade diminuída, climatério antecipado e qualidade de vida normal._________________________________________________________________________________________ ABSTRACT: This article describes the long time consequences of the isolated and lifetime growth hormone (GH) deficiency using a single model of GH releasing hormone resistance (GHRH) due to a homozygous mutation in the GHRH receptor gene, in a hundred of subjects. These consequences include severe short stature with final height between -9.6 and -5.2 standard deviations below of the mean, with proportional reductions of the bone dimensions; reduction of the anterior pituitary corrected to cranial volume and the thyroid, the uterus, the spleen and left ventricular mass volume, all corrected to body surface, in contrast of pancreas and liver size, bigger than in controls, when equally corrected. Body composition features included marked reduction in the amount of fat free mass (kg) and increase of fat mass percentage, with predominant abdominal deposit. In the metabolic aspects, we find increase in the total cholesterol and LDL cholesterol; reduction of the insulin and the insulin resistance assessed by Homeostasis model assessment; increase of ultra sensitive C reactive protein and systolic body. pressure in adults, although without evidences of premature atherosclerosis. Other findings include smaller bone resistance, although above of the threshold of fractures, delayed puberty, normal fertility, small parity, anticipated climacteric and normal quality of life.

Published

2008

10. Neonatal screening program for congenital hypothyroidism in northeast of Brazil: criteria, diagnosis and results

Author

Ramalho, Antônio Roberto de Oliveira, Ramalho, Roberto Jose Rabelo, Oliveira, Carla Raquel Pereira, Santos, Elenilde Gomes, Oliveira, Mario C. P., and Oliveira, Manuel Herminio de Aguiar

Subjects

Tiroxina, Congenital hypothyroidism, TSH, Thyroxin, Hipotireoidismo congênito, Neonatal screening, Triagem neonatal

Abstract

Avaliamos as concentrações do TSH em papel-filtro colhido no calcanhar (TSHneo) de 48.039 crianças triadas do programa de triagem neonatal (PTN) para o hipotireoidismo congênito (HC) de Sergipe, as concentrações de TSH, T4 total e T4 livre colhidas em sangue periférico nas crianças convocadas suspeitas de HC, a idade nas diversas fases do programa, a cobertura e a freqüência do PTN de janeiro de 2005 a agosto de 2006, comparando-as com dados da literatura. Utilizamos para análise os seguintes parâmetros: média, mediana, coeficiente de variação e distribuição de freqüência. A idade da criança por ocasião da coleta em papel filtro no calcanhar foi 10 ± 9 dias (média ± desvio-padrão) e a idade na reali-zação do ensaio do TSHneo foi de 31 ± 13 dias. Em 2005, a cobertura do PTN, para o interior e para a capital de Sergipe, foi de 77% e 73%, respectivamente. Verificamos que em 99,484% das crianças triadas as concentrações do TSH coletado em papel-filtro encontravam-se entre 0,01 e 5,20 µU/mL. As concentrações do TSH decrescem com o aumento da idade até estabilizar entre 11 e 15 dias de vida. Foram convocadas 248 crianças a partir do TSH coletado em papel-filtro (1/194). Na convocação, as concentrações do TSH, T4 e T4 livre coletado por punção venosa estavam normais em 119 crianças (1/404). A freqüência de HC suspeito foi de 1/485 (99 casos), de HC foi de 1/6.005 (8 casos) e de hipotiroxinemia foi de 1/16.013 (3 casos). A terapia para o HC foi iniciada com 51 ± 12 dias._________________________________________________________________________________________ ABSTRACT: It was evaluated the concentration of TSH in blood spot (TSHneo) of 48.039 children included in the Neonatal Screening Program (NSP) for Congenital Hypothyroidism (CH) of Sergipe (SE), a state in the northeast of Brazil. It was also evaluated the concentration of serum TSH, total T4 and free T4 in the recalled children suspicious of having CH, their age in several phases of the program, the covering and frequency of the NSP in the cases from January 2005 to August 2006, comparing them with literature data. The following parameters were used or the analysis: mean, standard deviation, median, coefficient of variation and frequency distribution. The children's age at the collection in filter-paper specimen was 10 ± 9 days (Mean±SD) and the TSHneo execution assay was done in the period of 31 ± 13 days. In 2005 the covering by the NSP was about 77% in the countryside and 73% in Aracaju, the capital of Sergipe. It was verified that in 99,484% of the children included in the screening, the TSHneo varied from 0,01 to 5,20µU/ml, decreasing according to the age and stabilizing when they were between 11 and 15 days. 248 children were recalled from the TSHneo (1/194).The concentrations of TSH, T4 and free T4 collected by venous puncture were normal in 119 children (1/404). The frequency of suspected CH was 1/485 (99 cases), of CH was 1/6005 (8 cases) and of hypothyroxinemia was 1/16013 (3 cases). Therapy for CH began within 51 ± 12 days.

Published

2008

11. Evolution of the screening program for congenital hypothyroidism and phenylketonuria in Sergipe State from 1995 to 2003

Author

Ramalho, Roberto Jose Rabelo, Ramalho, Antônio Roberto de Oliveira, Oliveira, Carla Raquel Pereira, and Oliveira, Manuel Herminio de Aguiar

Subjects

Tiroxina, Thyroxine, Hypothyroidism, Phenylketonurias, Phenylalanine, Fenilcetonúria, Fenilalanina, Neonatal screening, Triagem neonatal, Hipotireoidismo

Abstract

Avaliamos o tempo gasto nas diferentes etapas do Programa de Triagem para o Hipotireoidismo Congênito (HC) e Fenilcetonúria (PKU), sua cobertura e a freqüência em Sergipe, de 1998 a 2003, e comparamos com 1995. A idade da criança na coleta foi 12 ± 11 dias (Média ± Desvio Padrão) em 2003, inferior aos 30 ± 19 dias no 2o semestre de 1995. No 2o semestre/2003, o resultado foi analisado pelo médico com 28 ± 15 dias para o HC e 25 ± 15 dias para o PKU, menor que o tempo utilizado pelo médico no 2o semestre de 1995, 80 ± 40 dias. O tempo, no 2o semestre de 2003, entre o recebimento da amostra da coleta no laboratório e a realização do ensaio foi de 6 ± 4 dias para o TSH e de 3 ± 2 dias para a fenilalanina. A cobertura, em 2003, para o Interior foi de 67% e 85% para a Capital contra 5% e 42% no 2o semestre de 1995, respectivamente. A incidência de 1998 a 2003, no Serviço Público de Saúde de Sergipe para o HC, foi de 1/4850 e para o PKU, de 1/23036. De 1998 a 2003, a terapia foi iniciada com 49 ± 17 e 51 ± 12 dias para o HC e PKU, respectivamente. A redução do tempo nas etapas do programa e o aumento da cobertura indicam uma evolução favorável do referido programa._________________________________________________________________________________________ ABSTRACT: An evaluation was made of the timing delays in the various phases of the Screening Program for Congenital Hypothyroidism (HC) and Phenylketonuria (PKU), the coverage and incidence in the State of Sergipe from 1998 to 2003. The results were compared to the data from 1995. The age of the children in the sampling was 12 ± 11 days (mean ± standard deviation) lower than the 30 ± 19 days in the second semester of 1995. In the second half of 2003, the results were analyzed by the physician after 28 ± 15 days for HC and 25 ± 15 days for PKU, lower than 80 ± 40 days for the second semester of 1995. The period between the receipt of the samples at the laboratory and the assay in the second half of 2003 was 6 ± 4 days for TSH and 3 ± 2 days for phenylalanine. The coverage in 2003 for the interior of the State and the Capital was 67% and 85%, compared with 5% and 42% in the second semester of 1995, respectively. The incidence from 1998 to 2003 in the Public Health Service of Sergipe for HC was 1/4928 and 1/23406 for PKU. From 1998 to 2003 the therapy was initiated after 49 ± 17 days and 51 ± 12 days for HC and PKU, respectively. The reduction in the program timing delays and the increase in the coverage indicate development in the referred program.

Published

2004

12. Growth or somatotrophic hormone: new perspectives in isolated GH deficiency after description of the mutation in the GHRH receptor gene in individuals of Itabaianinha county, Brazil

Author

Souza, Anita Herminia Oliveira, Salvatori, Roberto, Martinelli Junior, Carlos Eduardo, Carvalho, Walter Marcelo Oliveira de, Menezes, Carlos Alberto, Santos, Elenilde Gomes, Barreto Filho, José Augusto Soares, Ramalho, Roberto Jose Rabelo, Oliveira, Carla Raquel Pereira, Alcântara, Paula Regina Silva de, Alcântara, Marta Regina Silva de, Oliveira, Hélio Araújo, Lima, Ivana de Barros, Carneiro, Jamille Nascimento, Santos, Marcos Moura, Gill, Matthew S., Clayton, Peter E., and Oliveira, Manuel Herminio de Aguiar

Subjects

Hormônio do crescimento, Deficiência isolada do GH, Hormônio somatotrófico, Receptor do GHRH, Somatotrophic hormone, Growth hormone, Isolated growth hormone deficiency, GHRH receptor

Abstract

Além de influenciar o crescimento corpóreo, o hormônio do crescimento, ou somatotrófico, desempenha importante papel no metabolismo, composição corporal, perfil lipídico, estado cardiovascular e longevidade. Seu controle é multi-regulado por hormônios, metabólitos e peptídeos hipotalâmicos. Dados sobre a Deficiência Isolada de GH (DIGH) obtidos a partir da descrição da mutação IVS1+1G→A no gene do receptor do hormônio liberador do GH (GHRH-R) em indivíduos da cidade de Itabaianinha, SE, são revisados. São abordadas novas perspectivas sobre o modelo de resistência ao GHRH, a importância do GHRH no controle da secreção de GH, a freqüência das mutações do gene do GHRH-R, a relevância diagnóstica do IGF-I e os achados metabólicos, cardiovasculares e de qualidade de vida nestes indivíduos._________________________________________________________________________________________ ABSTRACT: In addition to stimulating body growth, growth or somatotrophic hormone plays an important role in metabolism, body composition, lipid profile, cardiovascular status and longevity. Its control is multiregulated by hormones, metabolites and hypothalamic peptides. Obtained data of the isolated growth hormone deficiency (IGHD) after the description of the IVS1+1G→A GHRH receptor gene mutation in individuals of Itabaianinha County are reviewed. New perspectives about the growth hormone resistance model, the importance of GHRH in the control of GH secretion, the frequency of GHRH-R gene mutations, the diagnostic relevance of IGF-I and the metabolic, cardiovascular and quality of life findings are approached.

Published

2004