RESUMO
Background and aims We aimed to evaluate the differences in some cardiovascular risk (CVR) factors between adult patients without and with phenylketonuria (PKU) and to explore the correlation between waist circumference (WC) and body mass index (BMI) with the previous variables. Methods This was an observational casecontrol study that included patients older than 18 years with a diagnosis of classic PKU. The controls were age- and sex-matched individuals. We collected demographic, epidemiological, clinical, and laboratory variables, including WC, BMI, and lipid profile parameters. Results A total of 72 patients (25 controls and 47 cases) were included with a mean age of 36 years, of which 45 (62%) were women. Adult PKU patients showed lower high-density lipoprotein cholesterol (HDL-c) and higher triglyceride (TG) levels than the control group. We found an association between WC and uric acid (B=0.024, P=0.013, 95%CI: 0.0050.043), TG (B=0.768, P=0.024, 95%CI: 0.1071.428), and HDL-c (B=−0.254, P=0.026, 95%CI: −0.477 to (−0.032)) levels in PKU patients. However, we did not find any trend between WC and uric acid, TG and HDL-c levels that reached statistical significance (P<0.05) in patients without PKU. Conclusions Waist circumference rather than BMI may better represent the CVR in patients with PKU (AU)
Introducción y objetivos Nuestro objetivo fue evaluar las diferencias en algunos factores de riesgo cardiovascular entre pacientes adultos sin y con fenilcetonuria (FCU) y explorar la correlación del perímetro cintura (PC) e índice de masa corporal (IMC) con las variables previas. Métodos Fue un estudio de casos y controles que incluyó pacientes mayores de 18 años con diagnóstico de FCU clásica. Los controles fueron individuos emparejados por edad y sexo. Se recogieron variables demográficas, epidemiológicas, clínicas y de laboratorio, destacando PC, IMC y parámetros del perfil lipídico. Resultados Se reclutaron 72 pacientes (25 controles y 47 casos) con una edad media de 36 años (62% mujeres). Respecto al grupo control, los pacientes adultos con FCU mostraron niveles más bajos de colesterol de lipoproteínas de alta densidad (HDL-c) y más altos de triglicéridos. En los pacientes con FCU, PC se asoció con los niveles de ácido úrico (B=0,024, P=0,013, 95% CI: 0,005-0,043), triglicéridos (B=0,768, P=0,024, 95% CI: 0,107-1.428) y HDL-c (B=−0,254, P=0,026, 95% CI: −0,477[−0,032]). Sin embargo, no encontramos ninguna tendencia entre WC y dichas variables que alcanzara significación estadística en los pacientes sin FCU. Aunque observamos una buena correlación entre el IMC y PC en pacientes sin y con FCU, el aumento de PC por unidad de aumento de IMC podría ser mayor en estos últimos. Conclusiones Perímetro de cintura podría representar mejor que IMC el riesgo cardiovascular en pacientes con FCU (AU)
Assuntos
Humanos , Masculino , Feminino , Adulto , Pessoa de Meia-Idade , Razão Cintura-Estatura , Fenilcetonúrias/complicações , Índice de Massa Corporal , Estudos de Casos e ControlesRESUMO
BACKGROUND AND AIMS: We aimed to evaluate the differences in some cardiovascular risk (CVR) factors between adult patients without and with phenylketonuria (PKU) and to explore the correlation between waist circumference (WC) and body mass index (BMI) with the previous variables. METHODS: This was an observational case-control study that included patients older than 18 years with a diagnosis of classic PKU. The controls were age- and sex-matched individuals. We collected demographic, epidemiological, clinical, and laboratory variables, including WC, BMI, and lipid profile parameters. RESULTS: A total of 72 patients (25 controls and 47 cases) were included with a mean age of 36 years, of which 45 (62%) were women. Adult PKU patients showed lower high-density lipoprotein cholesterol (HDL-c) and higher triglyceride (TG) levels than the control group. We found an association between WC and uric acid (B=0.024, P=0.013, 95%CI: 0.005-0.043), TG (B=0.768, P=0.024, 95%CI: 0.107-1.428), and HDL-c (B=-0.254, P=0.026, 95%CI: -0.477 to (-0.032)) levels in PKU patients. However, we did not find any trend between WC and uric acid, TG and HDL-c levels that reached statistical significance (P<0.05) in patients without PKU. CONCLUSIONS: Waist circumference rather than BMI may better represent the CVR in patients with PKU.
Assuntos
Doenças Cardiovasculares , Fenilcetonúrias , Humanos , Adulto , Feminino , Masculino , Circunferência da Cintura , Obesidade , Fatores de Risco , Doenças Cardiovasculares/diagnóstico , Doenças Cardiovasculares/epidemiologia , Doenças Cardiovasculares/etiologia , Estudos de Casos e Controles , Ácido Úrico , Triglicerídeos , Índice de Massa Corporal , HDL-Colesterol , Fatores de Risco de Doenças Cardíacas , Fenilcetonúrias/complicações , Fenilcetonúrias/diagnósticoRESUMO
Introducción: La fenilcetonuria es el trastorno hereditario más frecuente del metabolismo de los aminoácidos y su abordaje suele centrarse en die-tas restringidas en fenilalanina, un aminoácido presente en el edulcorante aspartamo habitualmente usado como excipiente en tecnología farmacéutica. Objetivo: El objetivo principal es la revisión de los medicamentos sin receta comercializados en España hasta marzo de 2023 y que contienen aspartamo en su composición. Método: Se realizó una revisión en la base de datos BOT plus de todos los medicamentos comercializados en España que contienen aspartamo. Se seleccionaron solo los MSR. Se consultaron las fichas técnicas en el Centro de información online de medicamentos de la AEMPS (CIMA), y los datos obtenidos se registraron en una tabla. Resultados: Se obtuvieron 570 medicamentos; 58 eran MSR. Cuando exista petición de MSR con aspartamo en pacientes con fenilcetonuria, en el SIF, tras su evaluación, en el 100% de los casos, el farmacéutico aplicando el Servicio de Indicación Farmacéutica podría indicar un MSR alternativo, con el mismo principio activo pero sin aspartamo como excipiente. Conclusiones: La actuación del farmacéutico comunitario para aplicar el SIF es muy importante en pacientes con fenilcetonuria. Existen medicamentos que no requieren prescripción y se pueden indicar en estos pacientes. El farmacéutico debe tener a su disposición las herramientas necesarias que le faciliten el SIF con este tipo de enfermos. (AU)
Introduction: Phenylketonuria is the most common inherited disorder of amino acid metabolism and its management usually focuses on diets restricted in phenylalanine, an amino acid present in the sweet-ener aspartame commonly used as an excipient in pharmaceutical technology. Objective: The main objective is the review of non-prescription medicines marketed in Spain until March 2023 and that contain aspartame in their composition.Methods: A review of all medicines marketed in Spain containing aspartame was carried out in the BOT plus database. Only MSRs were selected. The data sheets were consulted at the AEMPS online medicines information centre (CIMA), and the data obtained were recorded in a table.Results: 570 medicines were obtained; 58 were MSRs. When there is a request for MSRs with aspartame in patients with phenylketonuria, in the SIF, after evaluation, in 100% of the cases, the pharmacist applying the Pharmaceutical Indication Service could indicate an alternative MSR, with the same active ingredient but without aspartame as an excipient.Conclusions: The action of the community phar-macist to apply the SIF is very important in patients with phenylketonuria. There are medicines that do not require a prescription and can be prescribed for these patients. Pharmacists should have the necessary tools at their disposal to facilitate the SIF with this type of patient. (AU)
Assuntos
Humanos , Aprovação de Drogas , Bases de Dados de Produtos Farmacêuticos/classificação , Medicamentos sem Prescrição/análise , Medicamentos sem Prescrição/farmacologia , Fenilcetonúrias/tratamento farmacológico , Aspartame/farmacologia , Excipientes Farmacêuticos/análise , Excipientes Farmacêuticos/farmacologia , Segurança do Paciente , EspanhaRESUMO
INTRODUCTION: Intermediate Inborn Errors of Metabolism (IEM) are a group of inherited diseases that include phenylketonuria (PKU), tyrosinemia II (TSII), organic acidaemias and ornithine transcarbamylase deficiency (OTCD), among others. They are increasingly more common in adults due to improved management. This has allowed more affected women to consider having children with good prospects. However, pregnancy may worsen metabolic control and/or increase maternal-fetal complications. The objective is to analyse the characteristics and outcomes of pregnancies of our patients with IEM. METHODS: Retrospective descriptive study. Pregnancies of women with IEM attended to at the adult IEM referral unit of the Hospital Universitario Virgen del Rocío were included. The qualitative variables were described as n(%) and the quantitative as P50 (P25-P75). RESULTS: 24 pregnancies were recorded: 12 newborns were healthy, 1 inherited their mother's disease, 2 had maternal phenylketonuria syndrome, 1 was stillborn (gestational week 31â¯+â¯5), 5 were spontaneous abortions and 3 were voluntarily terminated. The gestations were divided into metabolically controlled and uncontrolled. CONCLUSIONS: Pregnancy planning and multidisciplinary management through to postpartum is essential to ensure maternal and fetal health. The basis of treatment in PKU and TSII is a strict protein-limited diet. Events that increase protein catabolism in organic acidaemias and DOTC should be avoided. Further investigation of pregnancy outcomes in women with IEM is needed.
Assuntos
Aborto Espontâneo , Erros Inatos do Metabolismo dos Aminoácidos , Erros Inatos do Metabolismo , Criança , Gravidez , Adulto , Humanos , Recém-Nascido , Feminino , Estudos Retrospectivos , Erros Inatos do Metabolismo/terapia , Resultado da GravidezRESUMO
Introducción: la fenilcetonuria (PKU) es el error congénito del metabolismo de las proteínas más frecuente. El tratamiento dietético consiste en un plan de alimentación con una ingesta de proteínas naturales restringida, un sustituto proteico libre o de bajo contenido en fenilalanina (Phe) y el aporte de alimentos muy bajos en proteínas. El objetivo principal de este trabajo fue investigar si es posible aumentar la ingesta de proteína natural (PN) que se indica a los pacientes con PKU manteniendo los dosajes de Phe en sangre en rangos de seguridad. Materiales y método: se buscaron en 6 bases de datos electrónicas artículos publicados. Se identificaron un total de 154 artículos de Pub Med por intervalo de años desde 1999 a 2020. Se eligieron 15 artículos que se adaptaron a los criterios de inclusión y exclusión y respondían al objeto de estudio de esta revisión bibliográfica. Resultados: hay varios factores que pueden influenciar la estimación de la tolerancia de Phe como la severidad del fenotipo del paciente, la edad, el rango de seguridad de Phe en sangre, la prescripción de Phe y la adherencia al sustituto proteico. Si los niveles de Phe en sangre se mantienen en forma constante dentro del rango adecuado y por un período determinado, se debería considerar un incremento de la ingesta de Phe. El aumento de la ingesta de PN deberá ser realizado de manera controlada, individual y evaluando en forma constante el impacto en los dosajes de Phe en sangre. Conclusión: optimizar la ingesta de PN ofrece una mejora en la calidad de vida de pacientes con PKU, facilita la capacidad del paciente para socializar y contribuye a una mejor adherencia a la dieta(AU).
Introduction: phenylketonuria (PKU) is the most frequent inborn error of protein metabolism. The dietary treatment consists of a diet with a restricted natural protein intake, a free or low phenylalanine (Phe) protein substitute, and the intake of low protein food. The main objective of this work is to analyze if it is possible to increase the natural protein (NP) intake prescribed to PKU patients while maintaining blood Phe dosages within safe range. Materials and method: studies published were searched in 6 electronic data- basis. A total of 154 Pub Med articles were identified by range of years from 1999 to 2020. Fifteen articles which met the inclusion and exclusion criteria and responded to the objective of this bibliographic review were chosen. Results: several factors may influence Phe tolerance, such as severity of the patient´s phenotype, age, blood Phe safe range, Phe prescription and adherence to protein substitute. If Phe blood levels remain constantly within safe range and for a certain period, an increase of Phe intake should be considered. Increase of NP intake must be carried out in a controlled manner, individually and constantly evaluating blood Phe levels. Conclusion: optimizing NP intake offers the PKU patient an improvement in quality of life, facilitates the patient´s ability to socialize and contributes to a better adherence to the diet(AU).
Assuntos
Fenilcetonúrias , Fenilcetonúrias/dietoterapia , Proteínas , Ingestão de Alimentos , MetabolismoRESUMO
La fenilcetonuria y otras hiperfenilalaninemias son enfermedades genéticas cuya detección actualmente es obligatoria en México, tanto en el sector público como en el privado. La detección y el tratamiento oportunos han demostrado prevenir las manifestaciones neurológicas y la discapacidad que caracterizan esta enfermedad. Por ello, es de suma importancia que el pediatra y el personal de salud involucrados en la atención de estos pacientes conozcan, comprendan e implementen el manejo nutricional de manera correcta. Aunque existen varios tratamientos, el más utilizado es la restricción dietética de fenilalanina. El tratamiento nutricio incluye el uso de la llamada «fórmula médica¼ o «fórmula metabólica sin fenilalanina¼, la cual fue concebida desde el primer tercio del siglo XX. Posteriormente, se han realizado múltiples estudios y modificaciones con el fin de mejorar el pronóstico de los pacientes. El presente trabajo describe las principales características y diferencias entre las fórmulas libres de fenilalanina de seguimiento disponibles en México, para que el personal de salud cuente con elementos para su correcta prescripción.
Assuntos
Fenilcetonúrias , Humanos , México , Fenilcetonúrias/metabolismoRESUMO
ABSTRACT Objective: To identify phenylalanine hydroxylase (PAH) mutations in patients with phenylketonuria (PKU) from the Newborn Screening Service in Mato Grosso, Midwest Brazil. Methods: This is a cross-sectional descriptive study. The sample consisted of 19 PKU patients diagnosed by newborn screening. Molecular analysis: DNA extraction using the "salting-out" method. Detection of IVS10nt-11G>A, V388M, R261Q, R261X, R252W, and R408W mutations by the restriction fragment length polymorphism (RFLP) technique. Results: Two mutant alleles were identified in four patients (21.1%), one allele in five patients (26.2%), and none in the remaining ten patients (52.6%). A total of 13/38 alleles were detected, corresponding to 34.2% of the PAH alleles present. The most prevalent variant was V388M (13.2% of the alleles), followed by R261Q (10.1%) and IVS10nt-11G>A (7.9%). Three variants (R261X, R252W, and R408W) were not found. The most frequent mutation types were: missense mutation in eight alleles (18.4%) and splicing in four alleles (10.5%). The model proposed by Guldberg to determine a genotype/phenotype correlation was applied to four classical PKU patients with two identified mutations. In three of them, the predicted moderate/moderate or moderate PKU phenotype did not coincide with the actual diagnosis. The prediction coincided with the diagnosis of one classic PKU patient. The estimated incidence of PKU for Mato Grosso, Brazil, was 1:33,342 live births from 2003 to 2015. Conclusion: The only mutations found in the analyzed samples were the IVS10nt-11G>A, V388M, and R261Q. The genotype/phenotype correlation only occurred in four (5.3%) patients.
RESUMO Objetivo: Identificar mutações da fenilalanina hidroxilase (PAH) em pacientes com PKU (fenilcetonúria) do Serviço de Triagem Neonatal em Mato Grosso. Métodos: Estudo de corte transversal. Amostra composta de 19 pacientes com PKU através do exame de triagem neonatal biológica. Análise molecular: a) extração de DNA pela metodologia "salting out". B) detecção de mutações IVS10nt-11G>A, V388M, R261Q, R261X, R252W e R408W pela técnica de polimorfismo de comprimento de fragmento de restrição (RFLP). Resultados: Dois alelos foram identificados em quatro pacientes (21,1%), um alelo em cinco pacientes (26,2%) e nenhum nos dez pacientes restantes (52,6%). Um total de 13/38 alelos foram identificados, correspondendo a 34,2% dos alelos PAH presentes. A variante mais prevalente foi a V388M (13,2% dos alelos), seguida de R261Q (10,1%) e IVS10nt-11G>A (7,9%). Três variantes (R261X, R252W e R408W) não foram encontradas. Os tipos de mutações mais frequentes foram: troca de sentido em oito alelos (18,4%) e emenda em quatro alelos (10,5%). O modelo proposto por Guldberg para determinar uma correlação genótipo/fenótipo foi aplicado para quatro pacientes clássicos de PKU, com duas mutações identificadas. Em três, o fenótipo previsto de PKU moderada/moderada ou moderada não coincidiu com o diagnóstico real. A predição coincidiu com o diagnóstico de um paciente PKU clássico. A incidência de PKU estimada para Mato Grosso, Brasil foi de 1:33.342 nascidos vivos para o período de 2003 a 2015. Conclusões: Foram encontradas apenas as mutações IVS10nt-11G>A, V388M, R261Q nas amostras analisadas. A correlação genótipo/fenótipo ocorreu em quatro (5,3%) pacientes.
Assuntos
Humanos , Masculino , Feminino , Recém-Nascido , Lactente , Pré-Escolar , Criança , Fenilalanina Hidroxilase/genética , Fenilcetonúrias/genética , Processamento Alternativo , Mutação de Sentido Incorreto , Fenótipo , Polimorfismo de Fragmento de Restrição , Brasil , Análise Mutacional de DNA/métodos , Estudos Transversais , Triagem Neonatal , Alelos , GenótipoRESUMO
La fenilcetonuria, también conocida como PKU, es el error congénito más frecuente del metabolismo de los aminoácidos. La forma grave o PKU clásica no tratada, causa una discapacidad intelectual, aunque los programas de detección en el período neonatal, el diagnóstico y el tratamiento evitan la aparición de los síntomas. A pesar de un diagnóstico y tratamiento temprano hemos observado cierta neurotoxicidad en los pacientes con PKU tratados. Analizamos los demás factores implicados, aparte de la toxicidad por las elevadas concentraciones cerebrales de fenilalanina (Phe), se revisan los defectos de síntesis de neurotransmisores, las alteración de la mielinización cerebral, el efecto de la elevación de Phe en los procesos de transporte y distribución de los aminoácidos neutros con una síntesis anómala de proteínas cerebrales, la deficiencia plasmática y cerebral de tirosina, la neurotoxicidad de los metabolitos de Phe, el defecto de la biosíntesis del colesterol o el aumento del estrés oxidativo. Las alteraciones de la sustancia blanca en los pacientes con PKU tienen un papel importante en las manifestaciones neurológicas. El tratamiento de la PKU es para toda la vida y se basa en la reducción del aporte de alimentos que contienen Phe combinado con la administración de una fórmula especial, o en el tratamiento con tetrahidrobiopterina (BH4). Se analizan nuevas opciones terapéuticas.
Phenylketonuria, also known as PKU, is the most frequent congenital inborn error of metabolism. The severe form or classic PKU untreated causes intellectual disability, although with the early detection programs in the neonatal period, diagnosis and treatment prevent the appearance of the symptoms. Despite early diagnosis and treatment we have observed some neurotoxicity in treated PKU patients. We analyzed the factors involved apart from the toxicity due to the high cerebral concentrations of phenylalanine (Phe), the defects of synthesis of neurotransmitters, the alteration of cerebral myelination, the effect of the elevation of Phe in the processes of transport and distribution of neutral amino acids with an abnormal synthesis of brain proteins, plasma and cerebral tyrosine deficiency, the neurotoxicity of Phe metabolites, the defect of cholesterol biosynthesis or the increase of oxidative stress. White matter alterations in early treated PKU patients have an important role in neurological manifestations. The treatment of PKU is for life and is based on the reduction of foods containing Phe combined with the administration of a special formula or tetrahydrobiopterin (BH4) treatment. New therapeutic options will be analyzed.
Assuntos
Humanos , Fenilalanina/efeitos adversos , Fenilcetonúrias/diagnóstico , Fenilcetonúrias/terapia , Tirosina/metabolismo , Neurônios/patologia , Fenilcetonúrias/fisiopatologia , Biopterina/análogos & derivados , Diagnóstico Precoce , DietoterapiaRESUMO
INTRODUCTION: Introduction: casein-derived peptides can be liberated both in vivo via normal digestion of casein, as well as in vitro via enzymatic hydrolysis. These peptides were suggested to have biological activity. Objectives: the aim of this study was to describe the production and characterization of casein peptides and to explore the potential of these peptides as an option for low-phenylalanine diets. Methods: peptides were produced by tryptic hydrolysis of sodium caseinate and acid precipitation with HCl, followed by precipitation with ethanol or aggregation of CaCl2 or ZnSO4. Results: the amino acid analysis revealed a significant reduction in the amount of phenylalanine from the original protein. Conclusion: casein-derived peptides could be a future alternative of short chain peptides to low-phenylalanine formulations.
INTRODUCCIÓN: Introducción: los péptidos derivados de la caseína se pueden liberar tanto in vivo, a través de la digestión normal de la caseína, como in vitro a través de la hidrólisis enzimática. Se sugirió que estos péptidos tenían actividad biológica. Objetivos: el objetivo de este estudio fue describir la producción y caracterización de péptidos de caseína y explorar el potencial de estos péptidos como una opción para las dietas con bajo contenido de fenilalanina. Métodos: los péptidos se produjeron por hidrólisis tríptica de caseinato de sodio y precipitación ácida con HCl, seguido de precipitación con etanol o agregación de CaCl2 o ZnSO4. Resultados: el análisis de aminoácidos reveló una reducción significativa en la cantidad de fenilalanina de la proteína original. Conclusión: los péptidos derivados de la caseína podrían ser una alternativa futura de los péptidos de cadena corta a las formulaciones con bajo contenido de fenilalanina.
Assuntos
Caseínas/análise , Fenilalanina , Fenilcetonúrias/dietoterapia , Aminoácidos/análise , Aminoácidos/metabolismo , Caseínas/metabolismo , Dieta , Humanos , Peptídeos/análise , Peptídeos/metabolismoRESUMO
La fenilcetonuria (PKU) es causada por una actividad deficiente de la enzima fenilalanina hidroxilasa. En los pacientes con esta deficiencia la fenilalanina (Phe) no puede ser convertida en tirosina, aumentando sus niveles en sangre y de otros metabolitos neurotóxicos, provocando un retraso mental irreversible. El tratamiento fundamentalmente se basa en una dieta controlada de Phe. Sin embargo, los alimentos libres o bajos en Phe son escasos. El objetivo de esta investigación es obtener hidrolizados proteicos con bajo contenido de Phe a partir del suero dulce de leche en polvo y harina de E. edulis Triana. El aislado proteico (96,01% proteína cruda) se obtuvo por solubilización y precipitación de las proteínas de la harina, mientras que las proteínas del suero (15,69% proteína cruda) fueron tratadas en su matriz original. Las proteínas del suero y el asilado fueron hidrolizadas enzimáticamente con pepsina y proteasa de Streptomyces griseus. La concentración de Phe se determinó por fluorometría y por HPLC, de lo cual la Phe de las proteínas del suero es liberada una hora antes que las del chachafruto, debido a que las proteínas del suero en parte fueron hidrolizadas en la elaboración del queso. Además, los resultados de la utilización del carbón activados como captor de Phe indican la reducción total del contenido de este aminoácido en los hidrolizados y la reducción de la concentración de otros aminoácidos(AU)
henylketonuria (PKU) is caused by a low activity of the enzyme phenylalanine hydroxylase. In patients with this deficiency, phenylalanine (Phe) cannot be converted to tyrosine, increasing blood levels and other neurotoxic metabolites, causing irreversible mental retardation. The treatment is fundamentally based on a controlled diet of Phe. However, free or low-Phe foods are scarce. The objective of this research is to obtain protein hydrolysates with low Phe content from sweet milk powder and E. edulis Triana flour. The protein isolate (96.01% crude protein) was obtained by solubilization and precipitation of the flour proteins, while the whey proteins (15.69% crude protein) were treated in their original matrix. Serum and asylated proteins were enzymatically hydrolyzed with pepsin and Streptomyces griseus protease. The concentration of Phe was determined by fluorometry and by HPLC, from which the Phe of whey proteins is released one hour earlier than those of chachafruto, due to the fact that the whey proteins were partially hydrolyzed in the elaboration of the cheese. In addition, the results of the use of charcoal activated as Phe captor indicate the total reduction of the content of this amino acid in the hydrolysates and the reduction of the concentration of other amino acids(AU)
Assuntos
Humanos , Masculino , Feminino , Fenilcetonúrias/patologia , Hidrolisados de Proteína/análise , Proteínas do Soro do Leite/administração & dosagem , Proteínas do Soro do Leite/biossíntese , Doenças Nutricionais e Metabólicas , Distúrbios NutricionaisRESUMO
Introdução: Redução da densidade mineral óssea (DMO) está associada à Fenilcetonúria (PKU), mas a causa desta associação não é completamente entendida. O objetivo desse estudo foi avaliar a ingestão de nutrientes relacionados ao metabolismo ósseo (cálcio, fósforo, magnésio, potássio), e sua associação com a DMO em pacientes com PKU. Métodos: Estudo transversal, observacional. Foram incluídos 15 pacientes (PKU Clássica=8; Leve=7; mediana de idade=16 anos, IQ=15-20), todos em tratamento com dieta restrita em fenilalanina (Phe) e 13 em uso de fórmula metabólica. Foi realizado recordatório alimentar de 24 horas de um dia e demais dados (histórico de fraturas, parâmetros antropométricos, DMO e níveis plasmáticos de Phe, Tyr, cálcio) foram obtidos por revisão de prontuário. Resultados: Nenhum paciente apresentou histórico de fraturas e seis realizavam suplementação de cálcio (alteração prévia da DMO=5; baixa ingestão=1). A mediana dos níveis de Phe foi 11,6 mg/dL (IQ=9,3-13,3). Em relação ao recordatório alimentar, dez indivíduos apresentaram inadequado consumo de carboidratos; 14, de lipídeos; 9, de cálcio; 11, de magnésio; 13, de fósforo; e todos de potássio. A mediana da DMO foi de 0,989 g/cm2 (IQ=0,903-1,069), sendo duas classificadas como reduzidas para idade, ambas de pacientes com PKU Leve que recebiam suplementação de cálcio. Não foi observada correlação entre níveis de Phe, DMO e demais variáveis analisadas. Conclusão: Redução da DMO não foi frequente na amostra, embora ingestão inadequada de cálcio assim o seja. Estudos adicionais são necessários para esclarecer o efeito da Phe e da ingestão dietética sobre o metabolismo ósseo na PKU. (AU)
Introduction: Reduced bone mineral density (BMD) is associated with phenylketonuria (PKU), but this association is not completely understood. This research aimed to evaluate intake of nutrients related to bone metabolism (calcium, phosphorus, magnesium, potassium) and its association with BMD in patients with PKU. Methods: In this cross-sectional, observational study, 15 patients with PKU (Classical=8, Mild=7; median age=16 years, IQ=15-20 years) were included, all of them on phenylalanine (Phe) restricted diet and 13 being supplemented with a metabolic formula. A 24-hour dietary recall was performed and remaining data (history of fractures, anthropometric parameters, BMD and plasma Phe, tyrosine and calcium levels) were obtained through medical chart review. Results: No patient had any fractures and six received calcium supplements, five due to previous change in BMD and one due to inadequate nutritional intake. Median Phe level was 11.6 mg/dL (IQ=9.3-13.3). In relation to dietary recall, all individuals had inadequate intake of some nutrient (carbohydrate=10; lipids=14; calcium=9; magnesium=11; phosphorus=13; potassium=15). The median BMD was 0.989 g/cm2 (IQ=0.903-1.069). Two cases were classified as low BMD for age, both in patients with mild PKU receiving calcium supplements. Conclusion: Reduced BMD was not common in this sample, although inadequate calcium intake was frequently reported. Additional studies are needed to clarify the effect of Phe and dietary intake on bone metabolism in patients with PKU.(AU)
Assuntos
Humanos , Masculino , Feminino , Adolescente , Adulto , Fenilcetonúrias/complicações , Fenilcetonúrias/dietoterapia , Densidade Óssea , DensitometriaRESUMO
Abstract Objectives To show the general prevalence and to characterize tetrahydrobiopterin (BH4) deficiencies with hyperphenylalaninemia, identified by the Neonatal Screening Program of the State of Minas Gerais. Methods Descriptive study of patients with BH4 deficiency identified by the Neonatal Screening Program of the State of Minas Gerais. Results The prevalence found was 2.1 for 1,000,000 live births, with a frequency of 1.71% among hyperphenylalaninemias. There were four cases (40%) with 6-pyruvoyl-tetrahydropterin synthase deficiency, three with GTP cyclohydrolase I - autosomal recessive form deficiency, and three with dihydropteridine reductase deficiency (30% each). Six patients were diagnosed due to clinical suspicion and four cases due to systematic screening in neonatal screening. After the start of the treatment, patients identified by neonatal screening had rapid improvement and improved neuropsychomotor development compared to those diagnosed by the medical history. Conclusions The prevalence of BH4 deficiencies in Minas Gerais was slightly higher than that found in the literature, but the frequency among hyperphenylalaninemias was similar. Although rare, they are severe diseases and, if left untreated, lead to developmental delays, abnormal movements, seizures, and premature death. Early treatment onset (starting before 5 months of age) showed good results in preventing intellectual disability, justifying the screening of these deficiencies in newborns with hyperphenylalaninemia identified at the neonatal screening programs for phenylketonuria.
Resumo Objetivos Apresentar a prevalência geral e caracterizar as deficiências de tetrahidrobiopterina - BH4 - com hiperfenilalaninemia, identificadas pelo Programa de Triagem Neonatal do Estadode Minas Gerais. Métodos Estudo descritivo de pacientes com deficiência de BH4 do Programa de Triagem Neonatal do Estado de Minas Gerais. Resultados A prevalência encontrada foi de 2,1 para 1.000.000 recém-nascidos vivos e a frequência de 1,71%, dentre as hiperfenilalaninemias. Quatro casos (40%) com deficiência de 6-piruvoil-tetrahidropterina sintase, três com deficiência de GTP ciclohidrolase I e três com deficiência de dihidropteridina redutase (30% cada um). Seis pacientes foram diagnosticadospor suspeita clínica e quatro pela pesquisa sistemática na triagem neonatal. Após o início do tratamento, os pacientes identificados pela triagem neonatal tiveram melhora rápida e melhor desenvolvimento neuropsicomotor em comparação com aqueles diagnosticados pela história clínica. Conclusões A prevalência das deficiências de BH4 em Minas Gerais foi um pouco maior que a encontrada na literatura, mas a frequência, entre as hiperfenilalaninemias, foi semelhante. Embora raras, são graves e, se não tratadas, levam a atraso de desenvolvimento, movimentos anormais, convulsões e morte precoce. O tratamento precoce (início antes dos 5 meses) mostrou bons resultados na prevenção de deficiência intelectual, justificando a pesquisa dessas deficiências nos recém-nascidos com hiperfenilalaninemia pelos programas de triagem neonatalpara fenilcetonúria.
Assuntos
Humanos , Masculino , Feminino , Recém-Nascido , Fenilcetonúrias/diagnóstico , Fósforo-Oxigênio Liases/deficiência , Fenilcetonúrias/complicações , Fenilcetonúrias/epidemiologia , Brasil/epidemiologia , Prevalência , Estudos Transversais , Estudos Retrospectivos , Triagem NeonatalRESUMO
Introducción. La fenilcetonuria (FCU) es un error innato del metabolismo debido a deficiencia hereditaria de la enzima fenilalanina hidroxilasa causando acúmulo de fenilalanina (Phe) en varios tejidos del cuerpo humano, ocasionando retraso global del desarrollo. Existen grandes variaciones en la incidencia de FCU por grupo étnico, observándose que es más frecuente en caucásicos y en nativos amerindios, mientras que una menor incidencia se observa en afroamericanos, mestizos y asiáticos. En general, la incidencia de la FCU en caucásicos es de 1 en 10.000; mientras que en afroamericanos es de 1 en 200.000. Se ha observado que se presenta con mayor frecuencia en personas cuyos antepasados provienen del norte de Europa, en comparación con personas de origen afroamericano, judío o japonés. Caso clínico. Masculino prematuro muy prematuro de 29 semanas de edad gestacional, nace con apgar 7 8 que posteriormente presenta dificultad respiratoria que se incrementa por lo que fue necesario colocar en ventilación mecánica invasiva con parámetros altos que evolucionan a VAFO; posteriormente se intenta colocar SOG la cual no se logra colocar con facilidad. Paciente con mala evolución respiratoria, acidosis metabólica persistente, no tolera la alimentación a la leche materna, presenta distensión abdominal que lleva a suspender la vía oral por varias ocasiones. A la exploración física paciente presenta hipo actividad marcada posteriormente episodios convulsivos, pupilas normales, piel blanca, dermatitis del pañal; resto normal. Se toma nuevo tamiz haciéndose diagnóstico de FCU clásica, tratándose con formula libre de Phe. Paciente incrementa peso con la alimentación libre Phe, sin embargo, las múltiples complicaciones respiratorias sobre todo llevan a un deceso por proceso séptico asociado. Conclusión. La FCU puede ser diagnosticada tempranamente por tamiz neonatal, realizado de rutina en Ecuador sin embargo los resultados aun siendo tomados como tamizaje tienen un periodo de entrega e 30 días tiempo que puede obscurecer el diagnóstico y ayuda oportuna en ciertos casos. Cabe recalcar que en varias provincias de nuestro país aún no se realiza el tamizaje neonatal, por lo que es muy importante conocer la enfermedad para diagnosticarla previo a que existan complicaciones múltiples.
Introduction. Phenylketonuria (PKU) is an inborn error of metabolism due to hereditary deficiency of the enzyme phenylalanine hydroxylase causing accumulation of phenylalanine (Phe) in various tissues of the human body, causing global developmental delay. There are large variations in the incidence of FCU by ethnic group, being observed that it is more frequent in Caucasians and Native Amerindians, while a lower incidence is observed in African-Americans, mestizos and Asians. In general, the incidence of FCU in Caucasians is 1 in 10,000; while in African-Americans it is 1 in 200,000. It has been observed that it occurs more frequently in people whose ancestors come from northern Europe, compared to people of African-American, Jewish or Japanese origin. Clinical case. Very premature male of 29 weeks of gestational age, born with apgar 7 - 8 that later presents respiratory difficulty that increases so it was necessary to place in invasive mechanical ventilation with high parameters that evolve to HFOV; subsequently, an attempt is made to place SOG, which can not be easily placed. Patient with bad respiratory evolution, persistent metabolic acidosis, does not tolerate feeding to breast milk, presents abdominal distension that leads to suspend the oral route several times. On physical examination, the patient presented hypo activity, which was subsequently marked by convulsive episodes, normal pupils, white skin, diaper rash; rest normal. A new sieve is taken making a diagnosis of classic FCU, treating with Phe-free formula. Patient increases weight with free feeding Phe nevertheless the multiple respiratory complications mainly lead to a death by associated septic process. Conclusion. The FCU can be diagnosed early by neonatal screening, performed routinely in Ecuador, however, the results even being taken as a screening have a delivery period of 30 days that may obscure the diagnosis and timely help in certain cases. It should be noted that even in several provinces of our country, neonatal screening is still not done, so it is very important to know the disease to diagnose it before there are multiple complications.
Assuntos
Humanos , Recém-Nascido , Fenilcetonúrias , Anormalidades Congênitas , Doenças do PrematuroRESUMO
RESUMEN Las mutaciones del gen PAH generan deficiencia de la enzima fenilalanina hidroxilasa. Su actividad final varía desde una actividad casi nula o indetectable en la fenilcetonuria clásica hasta una actividad residual del 10 al 35% de la normal. Esta alteración corresponde al error innato del metabolismo de los aminoácidos más frecuente, afectando a 1 de cada 10.000 personas. Las diferentes cantidades de fenilalanina en sangre se traducen en un espectro amplio de manifestaciones clínicas que incluyen retraso global del desarrollo, discapacidad intelectual, convulsiones, rasgos autistas y comportamiento agresivo en los casos más graves. El diagnóstico temprano a través de los programas de tamizaje neonatal se considera prioritario pues las intervenciones oportunas evitan el daño del sistema nervioso central. Conclusiones: El diagnóstico en Colombia es tardío, las intervenciones realizadas a partir de ese momento son fútiles pues el deterioro cognitivo es irreparable, por lo tanto es imperativa la realización de pruebas diagnósticas tempranas cuando aún las intervenciones médicas pueden impactar la mejoría clínica del paciente con disminución importante de la morbilidad propia de esta patología, convirtiéndose en una necesidad la ampliación del programa de tamizaje neonatal, el cual estaría amparado bajo la ley colombiana de enfermedades huérfanas.
ABSTRACT Mutations in the PAH gene generate phenylalanine hydroxylase enzyme deficiency. Its final activity varies from almost null or undetectable in classical phenylketonuria to a residual activity of 10 to 35% of normal activity. This alteration corresponds to the innate more frequent error of the metabolism of the amino acids, affecting 1 of every 10,000 people. Different amounts of phenylalanine in blood translate into a broad spectrum of clinical manifestations including global developmental delay, intellectual disability, seizures, autistic traits, and aggressive behavior in the most severe cases. Early diagnosis through neonatal screening programs is considered a priority because timely interventions avoid damage to the central nervous system. Conclusions: The diagnosis in Colombia is belated, the interventions made from that moment are futile because the cognitive deterioration is irreparable. Therefore, it is imperative to carry out early diagnostic tests when medical interventions can still impact the clinical improvement of the patient with an important decrease of the morbidity characteristic of this pathology, making it necessary to expand the neonatal screening program which would be protected under the Colombian law of orphan diseases.
RESUMO
OBJECTIVES: To show the general prevalence and to characterize tetrahydrobiopterin (BH4) deficiencies with hyperphenylalaninemia, identified by the Neonatal Screening Program of the State of Minas Gerais. METHODS: Descriptive study of patients with BH4 deficiency identified by the Neonatal Screening Program of the State of Minas Gerais. RESULTS: The prevalence found was 2.1 for 1,000,000 live births, with a frequency of 1.71% among hyperphenylalaninemias. There were four cases (40%) with 6-pyruvoyl-tetrahydropterin synthase deficiency, three with GTP cyclohydrolase I - autosomal recessive form deficiency, and three with dihydropteridine reductase deficiency (30% each). Six patients were diagnosed due to clinical suspicion and four cases due to systematic screening in neonatal screening. After the start of the treatment, patients identified by neonatal screening had rapid improvement and improved neuropsychomotor development compared to those diagnosed by the medical history. CONCLUSIONS: The prevalence of BH4 deficiencies in Minas Gerais was slightly higher than that found in the literature, but the frequency among hyperphenylalaninemias was similar. Although rare, they are severe diseases and, if left untreated, lead to developmental delays, abnormal movements, seizures, and premature death. Early treatment onset (starting before 5 months of age) showed good results in preventing intellectual disability, justifying the screening of these deficiencies in newborns with hyperphenylalaninemia identified at the neonatal screening programs for phenylketonuria.
Assuntos
Fenilcetonúrias/diagnóstico , Fósforo-Oxigênio Liases/deficiência , Brasil/epidemiologia , Estudos Transversais , Feminino , Humanos , Recém-Nascido , Masculino , Triagem Neonatal , Fenilcetonúrias/complicações , Fenilcetonúrias/epidemiologia , Prevalência , Estudos RetrospectivosRESUMO
La fenilcetonuria es un error innato del metabolismo, producido por mutaciones en el gen de la fenilalanina hidroxilasa. Se describe el caso de un adolescente de 15 años con diagnóstico tardío de fenilcetonuria, quien presenta retardo mental severo, convulsiones e hipopigmentación. En este estudio se realizó el diagnóstico molecular de fenilcetonuria y se detectó la mutación p.R252W en homocigosis en el gen que codifica para la fenilalanina hidroxilasa. La presencia de esta variante nos permitió inferir la falta de respuesta a la terapia con sapropterina, medicamento que actúa como cofactor de la enzima, por la ausencia de actividad enzimática residual reportada para esta variante. Debido al retraso psicomotor del paciente, se decidió aplicar terapia lúdica y fortalecimiento muscular a través de la intervención fisioterapéutica; sin embargo, no se observó una mejoría permanente al aplicar este tratamiento, motivado por la falta de continuidad.
Phenylketonuria is an inborn error of metabolism due to mutations on the phenylalanine hydroxylase gene. We described the case of a 15 years old-adolescent with late diagnosis of phenylketonuria, who presents severe mental retardation, convulsions and hypopigmentation. In this study, the molecular diagnosis of phenylketonuria was performed, detecting p.R252W mutation in homozygous state on the phenylalanine hydroxylase gene. The presence of this variant allowed us to infer the lack of response to drug therapy with sapropterina which works as an enzyme cofactor, due to the absence of residual enzymatic activity reported for the p.R252W variant. Physical therapy was applied through playful therapy and muscular strengthening, because of the psychomotor retardation present in the patient. The failing in continuing with the physical therapy program stopped the patient´s improvement.
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Introducción: La fenilcetonuria es el error congénito del metabolismo más frecuente y es la primera enfermedad del metabolismo con un tratamiento exitoso que evita la discapacidad intelectual. Tanto en el mundo como en la Argentina la fenilcetonuria inauguró la lista de enfermedades del tamizaje neonatal. La prueba de pesquisa neonatal tiene una relación entre el costo y la eficacia altamente favorable cuando la prueba de pesquisa da un resultado correcto; en caso contrario, esta prueba dejaría de ser eficaz. La fenilcetonuria clásica está causada por la deficiencia de la enzima fenilalanina hidroxilasa, responsable de la conversión de fenilalanina a tirosina. Objetivo: El objetivo del presente trabajo fue identificar pacientes con fenilcetonuria que no han sido diagnosticados por medio de la pesquisa neonatal; también, describir la presentación clínica de la enfermedad y analizar las causas de la falta de diagnóstico y de las potenciales repercusiones para los programas de pesquisa en la Argentina. Antecedentes históricos y de normativas: Se describen brevemente los antecedentes históricos de la fenilcetonuria y de la prueba de tamizaje neonatal. A partir de 1986, por medio de la Ley 23413, se establece la obligatoriedad de realizar la pesquisa neonatal de fenilcetonuria en la República Argentina. Materiales y métodos: Analizamos los pacientes con diagnóstico de fenilcetonuria que se encuentran en seguimiento en el Hospital de Pediatría S.A.M.I.C. Prof. Dr. Juan P. Garrahan desde 2000 hasta 2015. Hallamos una serie de casos con diagnóstico de fenilcetonuria que no han sido diagnosticados por la prueba de pesquisa neonatal, y los comparamos. Estudiamos las políticas de Salud Pública que reglamentan las pruebas de pesquisa en la Argentina. Resultado y conclusiones: Se identificaron tres pacientes con fenilcetonuria clásica de diagnóstico tardío con discapacidad intelectual. Los tres casos son sujetos oriundos de Neuquén, Argentina, con la prueba de pesquisa informada como "negativa"; en los tres, la muestra fue tomada tempranamente. Para que los programas de pesquisa sean efectivos, en primer lugar deben existir políticas sanitarias unificadas para todas las provincias argentinas, con un sistema de coordinación, formación, educación, evaluación y estadística eficiente. Es fundamental conocer el impacto que causa no detectar a estos pacientes ya que esta revisión demuestra que, ante el fracaso de la prueba de pesquisa neonatal, es posible evitar el resultado de tres personas con discapacidad intelectual, dos de ellas totalmente dependientes de sus familias y del sistema sanitario.
Introduction: Phenylketonuria (PKU) is the most prevalent disorder caused by an inborn error in aminoacid metabolism and it is the first disease that has a successful treatment that prevents intellectual disabilities. It is the first disorder included in neonatal screening programmes in the world, as it also happens in our country. Furthermore, newborn screening is a highly favorable cost-effective test when the screening test is well done, otherwise the cost effectiveness would be unfavorable. Classical PKU is caused by phenylalanine hydroxylase that catalyses the conversion of the essential amino acid L-phenylalanine to L-tyrosine. Objective: To identify patients with PKU who have not been diagnosed by means of newborn screening tests. Description of the clinical presentation of the disease. Analysis of the causes and potential implications for newborn screening programs. Historical antecedents and regulations: The historical background of PKU and of the disease neonatal screening tests are briefly described Since 1986 the National Law #23413 establishes the obligation of performing the Neonatal Screening of phenylketonuria in Argentina. Materials and methods: We analized patients with PKU admitted and followed up in the Hospital de Pediatría S.A.M.I.C. Prof. Dr. Juan P. Garrahan from 2000 to 2015 We found a case series of patients with phenylketonuria that have not been diagnosed by means of the newborn screening test and we compared them. Analysis of Public Health Care policies and the laws that regulate the screening tests in Argentina. Results and conclusion: Three patients were identified and diagnosed with classic PKU of late diagnosis and presented mental disability. The three cases were from Neuquén province, Argentina. The neonatal screening tests had reported as "negative" and the three samples had been taken early. If the screening programs are to be effective what is needed, in the first place, it is to have uniform health care policies with national coverage with an efficient system of coordination, training, education, evaluation and statistics. It is essential to know the impact that implies not to identify these patients. In this review, we have noticed that the failure of the newborn screening tests resulted in three patients with intellectual disabilities, two of them totally dependent on their families and the health care system.
Assuntos
Humanos , Recém-Nascido , Lactente , Pré-Escolar , Fenilalanina Hidroxilase , Fenilcetonúrias , Saúde Pública , Deficiência Intelectual , Doenças Metabólicas , Doenças e Anormalidades Congênitas, Hereditárias e NeonataisRESUMO
Aunque, con tratamiento precoz, los pacientes con fenilcetonuria pueden presentar niveles de inteligencia normales, es importante optimizar el control dietético para mantener niveles de fenilalanina adecuados y poder desarrollar su potencial intelectual sin alteraciones en sus tareas diarias por déficits en las funciones ejecutivas. Se presenta una serie de 26 pacientes, diagnosticados y tratados precozmente, a quienes se realizó una evaluación psicométrica junto con determinaciones de fenilalanina a lo largo de su vida y en el momento de realización de los tests. Se observa una tendencia a la relación inversa entre el cociente intelectual y la fenilalanina concurrente, la mediana de fenilalanina y el cociente fenilalanina/tirosina, así como una tendencia a la relación negativa entre las funciones ejecutivas y los valores de fenilalanina concurrentes y durante la vida.
Although with early treatment phenylketonuria patients may have average intelligence levels, it is important to optimize the nutritional management to maintain adequate phenylalanine levels, so that patients can develop their intellectual potential free of abnormalities in their daily activities due to deficits of cognitive executive functions. This study presents a series of 26 patients, diagnosed and treated early, who underwent a psychometric evaluation together with phenylalanine determinations along their lives, and at the time of doing the tests. A trend is observed towards a reverse relationship between IQ and concurrent phenylalanine concentration, phenylalanine median and phenylalanine/tyrosine ratio. Likewise, a trend towards a negative relationship is observed between executive functions and concurrent phenylalanine values along patients' lives.
Assuntos
Humanos , Animais , Masculino , Criança , Adolescente , Fenilalanina/sangue , Fenilcetonúrias/sangue , Fenilcetonúrias/terapia , Testes Neuropsicológicos , Fenilcetonúrias/psicologia , Testes de InteligênciaRESUMO
OBJETIVO: Verificar o perfil sociodemográfico e a frequência de abandono de tratamento dos portadores de fenilcetonúria atendidos em um serviço de referência. MÉTODOS: Estudo retrospectivo, transverso, descritivo, com abordagem quantitativa, envolvendo todos os prontuários de pacientes fenilcetonúricos, atendidos no Serviço de Referência de Triagem Neonatal do Centro de Saúde-Escola Marco da Universidade do Estado do Pará, até novembro de 2013, com protocolo de autoria própria. RESULTADOS: No total, 36 pacientes compuseram a amostra; 52,77% eram do sexo feminino e 47,23% do sexo masculino. Três quartos não residiam em Belém (75%). Apenas um caso de abandono do tratamento (2,77%) foi confirmado, ou seja, um número ínfimo. Quanto ao diagnóstico da doença, 80,55% foram precoces. CONCLUSÃO: O perfil sociodemográfico traçado no atendimento do Centro de Saúde-Escola da Universidade do Estado do Pará foi: uma criança entre zero a 4 anos, do sexo feminino, diagnosticada precocemente, não residente em Belém, com tratamento efetivo, sem intercorrências que a fizessem abandonar o tratamento.
OBJECTIVE: To check the sociodemographic profile and the frequency of treatment abandon of phenylketonuria patients treated at a reference service. METHODS: Retrospective, cross-sectional, descriptive, quantitative approach study, involving all records of phenylketonuria patients treated at the neonatal screening reference center of the Marco School Health Center of State University of Pará until November 2013, with own protocol. RESULTS: It was counted 36 pacients, 52.77 % were female and 47.23% male. 3/4 doesn't live in Belém (75%). Only one confirmed case of noncompliance (2.77%), small number, however should be eradicated. Regarding the diagnosis of this disease, 80.55% were early. RESULTS: The sample was composed of 36 patients; 52.77 % were female and 47,23% male. Three of each four patients did not live in Belém (75%). We observed only one confirmed case of noncompliance (2.77%), that is a small number. Regarding the diagnosis of this disease, 80.55% were early. CONCLUSION: The sociodemographic profile in stroke care Centro de Saúde-Escola Marco was a child between zero to 4 years old female diagnosed early, non-resident of Belém, with sporadic and effective treatment without complications that made them to abandon treatment.
Assuntos
Humanos , Masculino , Feminino , Recém-Nascido , Lactente , Pré-Escolar , Criança , Perfil de Saúde , Triagem Neonatal , Pacientes Desistentes do Tratamento/estatística & dados numéricos , FenilcetonúriasRESUMO
A fenilcetonúria, doença metabólica hereditária, autossômica recessiva, é a mais frequente das aminoacidopatias. Quando não diagnosticada e tratada precocemente, causa retardo mental grave. Os programas de triagem neonatal transformaram a histó- ria natural dessa doença, possibilitando o diagnóstico neonatal e a instituição imediata do tratamento dietético. Atualmente, os pacientes com controle adequado têm vida normal. Nas últimas décadas, alterações nutricionais têm sido relacionadas ao tratamento dietético e aos seus desvios, especialmente após a primeira década de vida. Neste artigo apresenta-se o caso de um adolescente que desenvolveu anemia megaloblástica por deficiente ingestão de vitamina B12 e uma revisão da literatura sobre o tema.(AU)
Phenylketonuria, inherited metabolic disease, autosomal recessive, is the most common of aminoacidopathies. If not diagnosed and treated early, causes severe mental retardation. The newborn screening programs have transformed the natural history of this disease, allowing the neonatal diagnosis and the immediate institution of dietary treatment. Currently, patients with adequate control have normal life. In recent decades, nutritional changes have been related to dietary treatment and its deviations, especially after the first decade of life. In this article we present the case of a teenager who developed megaloblastic anemia due to poor intake of vitamin B12 and a literature review on the topic(AU)
