Pesquisa | Index Medicus Global

Síndrome de interrupción del tallo pituitario: Relaciones clínicas, bioquímicas y neurorradiológicas / Pituitary stalk interruption syndrome: Clinical, biochemical and neuroradiological relationships

Castro, Laura Cecilia; Martín, Silvia Edith; Bulacio, Sebastián; Dichko, Daniela; Silvano, Liliana; Sobrero, Gabriela; Aguirre, Cecilia; Franchioni de Muñoz, Liliana; Miras, Mirta Beatriz.

Rev. argent. endocrinol. metab ; 54(4): 151-159, dic. 2017. graf, tab

Artigo em Espanhol | LILACS | ID: biblio-957982

RESUMO

El síndrome de interrupción del tallo pituitario (PSIS) se caracteriza por la demostración neurorradiológica de un tallo pituitario ausente, interrumpido o hipoplásico, adenohipófisis aplásica/hipoplásica o neurohipófisis ectópica. Este síndrome se ha relacionado con formas severas de hipopituitarismo congénito (HPC), asociado a múltiples deficiencias de hormonas pituitarias (MPHD). Evaluamos a pacientes con HPC y PSIS, analizando los signos y los síntomas neonatales al diagnóstico, relacionándolos con las deficiencias hormonales pituitarias y signos neurorradiológicos presentes. Estudiamos retrospectivamente a 80 pacientes asistidos en el Hospital de Niños de Córdoba, con diagnóstico de HPC, de los cuales 42 (52%) presentaron PSIS; 22 mujeres y 20 varones, EC: 5 días-9,5 años. El 62% presentó MPHD y el 38% insuficiencia somatotrófica aislada (IGHD). El análisis de las variables perinatales demostró antecedentes de parto natural en el 52% (11/21) de las MPHD vs. 13% (2/15) de las IGHD. Cuatro pacientes, 2 con MPHD y 2 con IGHD presentaban antecedentes obstétricos consistentes en presentación podálica y transversa respectivamente, todos ellos resueltos mediante operación cesárea. Los signos y los síntomas perinatales fueron hipo- glucemia: 61% en MPHD vs. 19% en IGHD, p: 0,0105; ictericia: 38% en MPHD vs. 25% en IGHD; micropene: 77% en MPHD y colestasis: 19% en MPHD. Convulsiones neonatales se presentaron en el 75% de los niños con MPHD e hipoglucemia. EC media de consulta: 2,1 años en MPHD (30% en el período neonatal, 70% antes de 2 años) y 3,6 años en IGHD (44% en menores de 2 años). Los pacientes con MPHD presentaban: tallo no visible 81% (n: 21/26) vs. tallo hipoplásico: 19% (n: 5/26), p: 0,0001; en IGHD 56% (n: 9/16) vs. 44% (n: 7/16), p: 0,5067, respectivamente. El 100% de los neonatos con HPC tenían tallo pituitario ausente. Concluimos que la demostración de PSIS en niños con HPC proporciona información valiosa como predictor de la severidad fenotípica, la presencia de MPHD y de la respuesta al tratamiento. La baja frecuencia de antecedentes obstétricos posicionales potencialmente distócicos, como parte de los mecanismos fisiopatogénicos responsables de PSIS, indicaría la necesidad de analizar la importancia de posibles factores genéticos y epigenéticos involucrados. El diagnóstico precoz de HPC debe sospecharse en presencia de signos y síntomas clínicos, tales como hipoglucemia, colestasis, micropene y defectos asociados en la línea media facial. La resonancia magnética cerebral debe formar parte de los estudios complementarios en pacientes con esta presunción diagnóstica, especialmente a edades tempranas. El reconocimiento tardío de esta entidad puede aumentar la morbilidad y la mortalidad con efectos potenciales deletéreos y permanentes.

Pituitary stalk interruption syndrome (PSIS) is characterised by the combination of an interrupted or thin pituitary stalk, absent or ectopic posterior pituitary, and anterior pituitary hypoplasia. It is manifested as isolated (IGHD) or combined pituitary hormone deficiencies (CPHD) of variable degrees and timing of onset, with a wide spectrum of clinical phenotypes. PSIS may be an isolated morphological abnormality or be part of a syndrome. A retrospective evaluation is presented of clinical signs and symptoms present at early life stages, as well as an analysis of their relationship with hormone laboratory tests and diagnostic imaging in children with congenital hypopituitarism (CHP), and PSIS. This study was performed in a single centre on a sample of 42 children out of a total of 80 CHP patients, with a chronological age range between 5 days and 9.5 years from a database analysed over a period of 26 years. The study included 26/42 (62%) with CPHD and 16/42 (38%) with IGHD. The analysis of perinatal variables showed a natural delivery in 52% (11/21) of CPHD vs 13% (2/15) of IGHD. Four patients, two with CPHD and two IGHD had breech and transverse presentation respectively. All of them were resolved by caesarean section. The perinatal histories showed hypoglycaemia (61% CPHD vs 19% IGHD, P=.0105), jaundice (38% CPHDvs25% IGHD), micropenis (75%CPHD), hypoglycaemic seizures (75% CPHD), and cholestasis (19% CPHD). The mean CA of consulting for CPHD patients was 2.1 years, 30% in neonatal period and 70% before 2 years. The mean chronical age (CA) was 3.6 years in IGHD patients, with 44% of them less than 2 years. MRI showed that 81% of CPHD patients had absence of pituitary stalk vs 19% with thin pituitary stalk (P=.0001); Patients with IGHD presented 56% absence of pituitary stalk vs 44% with thin pituitary stalk (P=.5067). All (100%) of the patients diagnosed in the neonatal stage had absent pituitary stalk. The characterisation of GH deficient patients by presence and type of hypothalamic-pituitary imaging abnormality provides valuable information as a predictor of phenotypic severity, treatment response, and the potential to develop additional hormonal deficiencies. We conclude that demonstrating PSIS in children with HPC provides valuable information as a predictor of phenotypic severity, presence of MPHD, and response to treatment. The low frequency of potentially dysfunctional positional obstetric history, as part of the pathophysiological mechanisms responsible for PSIS, would indicate the need to analyse the importance of possible genetic and epigenetic factors involved. Early diagnosis of HPC should be suspected in the presence of clinical signs and symptoms, such as hypoglycaemia, cholestasis, micropenis, and associated facial midline defects. MRI should be part of complementary studies in patients with this diagnostic suspicion, especially at an early age. Late recognition of this entity may increase morbidity and mortality with potential permanent deleterious effects.

Assuntos

Humanos , Masculino , Feminino , Recém-Nascido , Lactente , Pré-Escolar , Criança , Hipófise/anormalidades , Hipófise/fisiopatologia , Hipopituitarismo/congênito , Hormônio do Crescimento/deficiência , Colestase/etiologia , Hipoglicemia/etiologia , Hipopituitarismo/diagnóstico

Shock neonatal como forma de presentación de panhipopituitarismo. A propósito de un caso clínico / Neonatal shock as the initial presentation of panhypopituitarism. A clinical case

Ospitaleche, Mariangel; Ghione, Andrea; Ramírez, María José; Silvera, Fernando.

Arch. pediatr. Urug ; 88(3): 161-167, jun. 2017. tab, graf

Artigo em Espanhol | LILACS | ID: biblio-887778

RESUMO

Resumen: El panhipopituitarismo congénito es una enfermedad poco frecuente, de presentación clínica variable, dependiendo del déficit hormonal. La interrupción del tallo hipofisario, una de las etiologías, se diagnostica solo en un 23% de los casos en el período neonatal, causando hipogenesia de la hipófisis anterior y agenesia o ectopia de la hipófisis posterior. El diagnóstico temprano y el tratamiento oportuno condicionan la morbimortalidad. Se presenta el caso de un recién nacido de término, sexo femenino, pequeño para la edad gestacional, producto de embarazo y parto sin complicaciones. Sin dismorfias. Ingresó a la unidad neonatal a las 14 h de vida por hipotermia leve e hipoglicemias con elevados requerimientos de glucosa parenteral. En la evolución episodios reiterados de shock de etiología no clara, que responden al tratamiento instituido. Se descartó causa infecciosa, cardiovascular y metabólica. Agregó movimientos anormales, inestabilidad hemodinámica y anisocoria; por lo cual se solicitó resonancia nuclear magnética de cráneo que informo neurohipófisis ectópica asociado a tallo hipofisario y adenohipófisis hipoplásica. La determinación hormonal reveló: cortisol 0,2 (g/dl (normal >3 para recién nacidos de término), adenocorticotrofina (ACTH) 15,8 pg/ml (7,2-63,6), T4 0,78 ng/dl (1-1,6), TSH 3,83 (UI/ml (0,6-6) y hormona de crecimiento (GH) 2,45 ng/ml (0,05-6). Con diagnóstico de insuficiencia suprarrenal e hipotiroidismo secundario se inició tratamiento con hidrocortisona oral 20 mg/m2/día en dos dosis y T4 25 (g/día, con buena evolución posterior. Alta a domicilio a los 45 días de vida. El objetivo de esta presentación es exponer una etiología poco frecuente de un cuadro clínico habitual en la unidad neonatal, como lo es el shock.

Summary: Congenital panhypopituitarism is a rare disease which may have variable clinical presentations, depending on the hormonal deficit. Disruption of the hypophyseal stem, one of the etiologies, is diagnosed in only 23% of the cases in the neonatal period, causing hypogenesis of the anterior pituitary and agenesis or ectopia of the posterior pituitary. Early diagnosis and timely treatment have an impact on morbidity and mortality. We present the case of a term newborn, female, small for gestational age, product of pregnancy and childbirth without complications. No dysmorphism. She was admitted into the neonatal unit at 14 hours of life, due to mild hypothermia and hypoglycemia with high parenteral glucose requirements. In the evolution, repeated episodes of shock of unclear etiology occurred, which responded to the treatment applied. Infectious, cardiovascular and metabolic causes were ruled out. The patient added abnormal movements, hemodynamic instability and anisocoria. Thus, MRI of the skull was requested, and it revealed ectopic neurohypophysis associated with hypophyseal stem and hypoplastic adenohypophysis.

Neonatal cholestasis in congenital pituitary hormone deficiency and isolated hypocortisolism: characterization of liver dysfunction and follow-up / Colestase neonatal na deficiência congênita de hormônio hipofisário e hipocortisolismo isolado: caracterização da disfunção hepática e acompanhamento

Braslavsky, Débora; Keselman, Ana; Galoppo, Marcela; Lezama, Carol; Chiesa, Ana; Galoppo, Cristina; Bergadá, Ignacio.

Arq. bras. endocrinol. metab ; 55(8): 622-627, nov. 2011. graf

Artigo em Inglês | LILACS | ID: lil-610464

RESUMO

INTRODUCTION: Neonatal cholestasis due to endocrine diseases is infrequent and poorly reco-gnized. Referral to the pediatric endocrinologist is delayed. OBJECTIVE: We characterized cholestasis in infants with congenital pituitary hormone deficiencies (CPHD), and its resolution after hormone replacement therapy (HRT). SUBJECTS AND METHODS: Sixteen patients (12 males) were included; eleven with CPHD, and five with isolated central hypocortisolism. RESULTS: Onset of cholestasis occurred at a median age of 18 days of life (range 2-120). Ten and nine patients had elevated transaminases and γGT, respectively. Referral to the endocrinologist occurred at 32 days (range 1 - 72). Remission of cholestasis occurred at a median age of 65 days, whereas liver enzymes occurred at 90 days. In our cohort isolated, hypocortisolism was a transient disorder. CONCLUSION: Cholestasis due to hormonal deficiencies completely resolved upon introduction of HRT. Isolated hypocortisolism may be a transient cause of cholestasis that needs to be re-evaluated after remission of cholestasis.

INTRODUÇÃO: A colestase neonatal causada por doenças endócrinas é pouco frequente e reconhecida. Existe um atraso no encaminhamento dos pacientes a um endocrinologista pediátrico. OBJETIVO: Caracterizamos a colestase em recém-nascidos com deficiências congênitas de hormônio hipofisário (DCHH) e sua resolução após a terapia de reposição hormonal (TRH). SUJEITOS E MÉTODOS: Dezesseis pacientes (12 do sexo masculino) foram incluídos; sete com DCHH, e cinco com hipocortisolismo central isolado. RESULTADOS: O início da colestase ocorreu aos 18 dias de vida (variação 2-120). Dez e nove pacientes apresentaram elevação das transaminases e γGT, respectivamente. A consulta com um endocrinologista aconteceu aos 32 dias (variação 1-72). A remissão da colestase ocorreu em uma idade mediana de 65 dias, enquanto a remissão das enzimas hepáticas aconteceu aos 90 dias. Na coorte isolada, o hipocortisolismo foi uma desordem transitória. CONCLUSÃO: A colestase causada por deficiências hormonais foi completamente resolvida após a introdução da TRH. O hipocortisolismo pode ser uma causa transitória da colestase e precisa ser reavaliado após a remissão da colestase.

Assuntos

Feminino , Humanos , Lactente , Masculino , Insuficiência Adrenal/etiologia , Colestase/etiologia , Hidrocortisona/uso terapêutico , Hipopituitarismo/congênito , Hepatopatias/etiologia , Tiroxina/uso terapêutico , Idade de Início , Insuficiência Adrenal/fisiopatologia , Colestase/fisiopatologia , Seguimentos , Terapia de Reposição Hormonal/métodos , Hidrocortisona/deficiência , Hipopituitarismo/tratamento farmacológico , Hepatopatias/fisiopatologia , Hormônios Adeno-Hipofisários/deficiência , Indução de Remissão , Estudos Retrospectivos , Resultado do Tratamento

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