Assuntos
COVID-19 , Úlcera , Humanos , Úlcera/diagnóstico , Úlcera/etiologia , COVID-19/complicações , SARS-CoV-2RESUMO
Introducción: El retraso global del desarrollo (RGD) y la discapacidad intelectual (DI) son un motivo de consulta frecuente en la consulta de Neuropediatría. Actualmente, la hibridación genómica comparada constituye una de las principales técnicas aplicadas al diagnóstico de esta patología. Resulta útil determinar qué características fenotípicas se asocian a obtener un resultado etiológico en el test genético. Métodos: Se llevó a cabo un estudio ciego pormenorizado de las características clínicas, antropométricas y morfológicas de 80 individuos afectos de DI no explicada y se analizó cuales estaban asociadas a obtener un resultado etiológico en el array-CGH. Resultados: El resultado del array fue patológico en un 27,5% de los casos. Los factores que se asociaron estadísticamente a tener una prueba de array-CGH patológica fueron los antecedentes familiares de DI/RGD (OR: 12,1), la presencia de malformaciones congénitas (OR: 5,33), más de 3 rasgos dismórficos faciales (OR: 20,9) y la hipotonía periférica (OR: 3,25). Conclusiones: Nuestros hallazgos coinciden con otras series publicadas. Por lo tanto, asumimos que la probabilidad de encontrar variación en el número de copias de significado patológico mediante array-CGH aumenta si alguna de las características anteriores está presentes en individuos afectos de DI/RGD (AU)
Introduction: Global developmental delay (GDD) and intellectual disability (ID) are frequent reasons for consultation in paediatric neurology departments. Nowadays, array comparative genomic hybridisation (array-CGH) is one of the most widely used techniques for diagnosing these disorders. Our purpose was to determine the phenotypic features associated with pathological results in this genetic test. Methods: We conducted a blind study of the epidemiological, clinical, anthropometric, and morphological features of 80 patients with unexplained ID to determine which features were associated with pathological results in array-CGH. Results: Pathological results were found in 27.5% of the patients. Factors associated with pathological results in array-CGH were a family history of GDD/ID (OR = 12.1), congenital malformations (OR = 5.33), having more than 3 facial dysmorphic features (OR = 20.9), and hypotonia (OR = 3.25). Conclusions: Our findings are consistent with those reported by other published series. We therefore conclude that the probability of having pathological results in array-CGH increases with the presence of any of the features mentioned above in patients with ID/GDD (AU)
Assuntos
Humanos , Masculino , Feminino , Lactente , Pré-Escolar , Criança , Adolescente , Deficiência Intelectual/genética , Transtornos Globais do Desenvolvimento Infantil/genética , Hibridização Genômica Comparativa/métodos , Fenótipo , Marcadores Genéticos/genética , FaciesRESUMO
Objetivo: Estudio descriptivo de epilepsias sintomáticas, según edad de inicio, controladas en una Unidad de Neuropediatría de referencia regional durante 3 años. Pacientes y métodos: Niños con diagnóstico de epilepsia sintomática, controlados del 1 de enero del 2008 hasta el 31 de diciembre del 2010. Resultados: De 4595 niños en el periodo de estudio, recibieron el diagnóstico de epilepsia 605 (13,17%), siendo 277 (45,79%) epilepsias sintomáticas. Entre los pacientes que iniciaron la epilepsia por debajo del año de vida predominan las de etiología sintomática (67,72%). Entre los que la iniciaron entre 1-3 años, fueron sintomáticas el 61,39%. En cuanto a su etiología, ha sido: encefalopatías prenatales (24,46% del total de epilepsias), encefalopatías perinatales (9,26%), encefalopatías posnatales (3,14%), encefalopatías metabólicas y degenerativas (1,98%), esclerosis mesial temporal (1,32%), síndromes neurocutáneos (2,64%), malformaciones vasculares (0,17%), cavernomas (0,17%) y tumores intracraneales (2,48%). Algunas etiologías inician sus manifestaciones epilépticas por debajo del año de vida, como el síndrome de Down, la lisencefalia genética, la infección congénita por citomegalovirus, la encefalopatía hipóxico-isquémica, las encefalopatías metabólicas o la esclerosis tuberosa. Conclusiones: La ausencia de una clasificación universalmente aceptada de los síndromes epilépticos dificulta comparaciones entre series. Sugerimos que todas las epilepsias son sintomáticas puesto que tienen causa, genética o adquirida. La edad de inicio orienta a determinadas etiologías. Una clasificación útil es la etiológica, con 2 grupos: un gran grupo con las etiologías establecidas o síndromes genéticos muy probables y otro de casos sin causa establecida, que con los avances en neuroimagen y genética cada vez será menor (AU)
Objective: We conducted a descriptive study of symptomatic epilepsy by age at onset in a cohort of patients who were followed up at a neuropaediatric department of a reference hospital over a 3-year period. Patients and methods: We included all children with epilepsy who were followed up from January 1, 2008 to December 31, 2010. Results: Of the 4595 children seen during the study period, 605 (13.17%) were diagnosed with epilepsy; 277 (45.79%) of these had symptomatic epilepsy. Symptomatic epilepsy accounted for 67.72% and 61.39% of all epilepsies starting before one year of age, or between the ages of one and 3, respectively. The aetiologies of symptomatic epilepsy in our sample were: prenatal encephalopathies (24.46% of all epileptic patients), perinatal encephalopathies (9.26%), post-natal encephalopathies (3.14%), metabolic and degenerative encephalopathies (1.98%), mesial temporal sclerosis (1.32%), neurocutaneous syndromes (2.64%), vascular malformations (0.17%), cavernomas (0.17%), and intracranial tumours (2.48%). In some aetiologies, seizures begin before the age of one; these include Down syndrome, genetic lissencephaly, congenital cytomegalovirus infection, hypoxic-ischaemic encephalopathy, metabolic encephalopathies, and tuberous sclerosis. Conclusions: The lack of a universally accepted classification of epileptic syndromes makes it difficult to compare series from different studies. We suggest that all epilepsies are symptomatic because they have a cause, whether genetic or acquired. The age of onset may point to specific aetiologies. Classifying epilepsy by aetiology might be a useful approach. We could establish 2 groups: a large group including epileptic syndromes with known aetiologies or associated with genetic syndromes which are very likely to cause epilepsy, and another group including epileptic syndromes with no known cause. Thanks to the advances in neuroimaging and genetics, the latter group is expected to become increasingly smaller (AU)
Assuntos
Humanos , Lactente , Epilepsia/etiologia , Encefalopatias/complicações , Idade de Início , Epidemiologia Descritiva , Predisposição Genética para Doença , Lesão Encefálica Crônica/epidemiologia , Encefalopatias Metabólicas/epidemiologia , Meningite/epidemiologiaRESUMO
OBJECTIVE: We conducted a descriptive study of symptomatic epilepsy by age at onset in a cohort of patients who were followed up at a neuropaediatric department of a reference hospital over a 3-year period PATIENTS AND METHODS: We included all children with epilepsy who were followed up from January 1, 2008 to December 31, 2010 RESULTS: Of the 4595 children seen during the study period, 605 (13.17%) were diagnosed with epilepsy; 277 (45.79%) of these had symptomatic epilepsy. Symptomatic epilepsy accounted for 67.72% and 61.39% of all epilepsies starting before one year of age, or between the ages of one and 3, respectively. The aetiologies of symptomatic epilepsy in our sample were: prenatal encephalopathies (24.46% of all epileptic patients), perinatal encephalopathies (9.26%), post-natal encephalopathies (3.14%), metabolic and degenerative encephalopathies (1.98%), mesial temporal sclerosis (1.32%), neurocutaneous syndromes (2.64%), vascular malformations (0.17%), cavernomas (0.17%), and intracranial tumours (2.48%). In some aetiologies, seizures begin before the age of one; these include Down syndrome, genetic lissencephaly, congenital cytomegalovirus infection, hypoxic-ischaemic encephalopathy, metabolic encephalopathies, and tuberous sclerosis. CONCLUSIONS: The lack of a universally accepted classification of epileptic syndromes makes it difficult to compare series from different studies. We suggest that all epilepsies are symptomatic because they have a cause, whether genetic or acquired. The age of onset may point to specific aetiologies. Classifying epilepsy by aetiology might be a useful approach. We could establish 2 groups: a large group including epileptic syndromes with known aetiologies or associated with genetic syndromes which are very likely to cause epilepsy, and another group including epileptic syndromes with no known cause. Thanks to the advances in neuroimaging and genetics, the latter group is expected to become increasingly smaller.
Assuntos
Idade de Início , Epilepsia/classificação , Epilepsia/etiologia , Neurologia , Pediatria , Encefalopatias/classificação , Criança , Pré-Escolar , Epilepsia/genética , Feminino , Seguimentos , Humanos , Lactente , Masculino , Estudos RetrospectivosRESUMO
INTRODUCTION: Global developmental delay (GDD) and intellectual disability (ID) are frequent reasons for consultation in paediatric neurology departments. Nowadays, array comparative genomic hybridisation (array-CGH) is one of the most widely used techniques for diagnosing these disorders. Our purpose was to determine the phenotypic features associated with pathological results in this genetic test. METHODS: We conducted a blind study of the epidemiological, clinical, anthropometric, and morphological features of 80 patients with unexplained ID to determine which features were associated with pathological results in array-CGH. RESULTS: Pathological results were found in 27.5% of the patients. Factors associated with pathological results in array-CGH were a family history of GDD/ID (OR = 12.1), congenital malformations (OR = 5.33), having more than 3 facial dysmorphic features (OR = 20.9), and hypotonia (OR = 3.25). CONCLUSIONS: Our findings are consistent with those reported by other published series. We therefore conclude that the probability of having pathological results in array-CGH increases with the presence of any of the features mentioned above in patients with ID/GDD.
Assuntos
Hibridização Genômica Comparativa/métodos , Deficiências do Desenvolvimento/genética , Deficiência Intelectual/genética , Deficiência Intelectual/patologia , Fenótipo , Criança , Feminino , Humanos , MasculinoRESUMO
AIM: A descriptive study of non-symptomatic epilepsy (idiopathic and cryptogenic), according to age at onset, monitored at a Neuropediatric Section of regional reference over a period of three years. PATIENTS AND METHODS: A review of neuropediatric database medical records of children with non-symptomatic epilepsy supervised from Jan 1, 2008 till December 31, 2010. RESULTS: Of the 4595 children attended during the period, 605 were diagnosed with epilepsy (13.17%): 156 (25.79%) idiopathic epilepsies and 172 (28.43%) cryptogenic epilepsies. The average age at onset of the total was 4.78 years: 6.31 years in idiopathic epilepsies and 5.43 years in cryptogenic epilepsies. 26.12% of all the epilepsies began in the first year of life. Idiopathic epilepsy predominates in the startup group of 6-10 years and cryptogenic epilepsy in 3-6 years. Absence epilepsy and benign childhood epilepsy with centro-temporal spikes are the idiopathic epileptic syndromes most prevalent. CONCLUSIONS: Many differences exist among published epidemiological data on childhood epilepsy due to the difficulty of a syndromic diagnosis in children, caused by clinical and electroencephalographic variability. The absence of a universally accepted classification of epileptic syndromes makes it difficult to compare publications. All epilepsies are symptomatic as they have a cause, whether it be genetic or acquired. A useful classification would be etiological, with two groups: one large with established etiology or very likely genetic syndromes and another with no established cause. The age at onset indicates specific etiologies.
TITLE: Estudio descriptivo de las epilepsias no sintomaticas segun la edad de inicio en una unidad de neuropediatria de referencia regional.Objetivo. Estudio descriptivo de las epilepsias no sintomaticas (idiopaticas y criptogenicas), segun la edad de inicio, controladas en una unidad de neuropediatria de referencia regional durante tres años. Pacientes y metodos. Revision de historias de niños con epilepsia no sintomatica de la base de datos de neuropediatria controlados del 1 de enero de 2008 al 31 de diciembre de 2010. Resultados. De 4.595 niños atendidos en el periodo, se diagnosticaron de epilepsia 605 (13,17%), de las cuales 156 (25,79%) fueron idiopaticas, y 172 (28,43%), criptogenicas. La edad media de inicio del total fue de 4,78 años; 6,31 años en las idiopaticas y 5,43 años en las criptogenicas. El 26,12% del total de epilepsias se inicio en el primer año. Las epilepsias idiopaticas predominan en el grupo de inicio de 6-10 años, y las criptogenicas, en el de 3-6 años. La epilepsia de ausencias y la epilepsia benigna de la infancia con paroxismos centrotemporales son los sindromes epilepticos idiopaticos mas prevalentes. Conclusiones. Existen muchas diferencias de datos epidemiologicos publicados sobre epilepsia infantil por la dificultad que entraña un diagnostico sindromico en la edad pediatrica, debido a la variabilidad clinica y electroencefalografica. La ausencia de una clasificacion universalmente aceptada de los sindromes epilepticos dificulta comparaciones entre series. Todas las epilepsias son sintomaticas, puesto que tienen causa, sea genetica o adquirida. Una clasificacion util es la etiologica, con dos grupos: un gran grupo con las etiologias establecidas o sindromes geneticos muy probables y otro de casos sin causa establecida. La edad de inicio orienta a determinadas etiologias.
Assuntos
Idade de Início , Epilepsia Tipo Ausência/epidemiologia , Epilepsia Rolândica/epidemiologia , Epilepsia/epidemiologia , Criança , Pré-Escolar , Eletroencefalografia , Humanos , SíndromeRESUMO
El presente documento expone un resumen de la actual sistemática de trabajo de las Unidades dc Neuropediatría y Metabolismo del Hospital Universitario Miguel Servet de Zaragoza. Se dispone de herramientas de trabajo de enorme utilidad: bases de datos de neuropediatría y metabolismo, protocolos, hojas de información y consentimientos informados. A partir de dichas herramientas, se expone la actividad de las Unidades asistenciales, docentes y de investigación, incluida la actividad generada por el cribado neonatal ampliado (AU)
This document represents a summary of how the Neutopediatric and Metabolic Units work at the University Hospital Miguel Servet in Zaragoza. The extremely useful tools available today are Neuropediatric and Metabolic Data Bases, clinical protocols, parents and professionals information sheets and informed consent forms. Health-care, educational and research activity, including amplified neonatal screening, are drawn from these tools (AU)
Assuntos
Humanos , Masculino , Feminino , Criança , Pediatria/educação , Pediatria/métodos , Metabolismo/genética , Cuidado do Lactente/organização & administração , Ensino/classificação , Ensino/organização & administração , Protocolos Clínicos/classificação , Consentimento dos Pais/ética , Atenção Primária à Saúde , Pediatria/classificação , Pediatria , Metabolismo/fisiologia , Cuidado do Lactente/história , Ensino/história , Ensino , Bases de Dados Estatísticos , Protocolos Clínicos/normas , Consentimento dos Pais/história , Atenção Primária à Saúde/métodosRESUMO
Introducción: España es el primer país de Europa en número de adopciones internacionales. Los niños adoptados podrían tener mayor riesgo de presentar una patología neurológica. Objetivo: Describir la serie de pacientes adoptados atendidos en la consulta de neuropediatría durante un periodo de 22 años, determinar las patologías neurológicas más prevalentes y analizar los posibles factores de riesgo. Pacientes y métodos: Niños adoptados atendidos desde mayo de 1990 hasta mayo de 2012 (n= 226), divididos en dos grupos: adoptados nacionales (AN= 59) y adoptados internacionales (AI= 167). El grupo AI fue subdividido en cuatro áreas de procedencia: Europa del Este (AI-E), Latinoamérica (AI-L), países orientales (AI-O) e India (AI-I). Resultados: Se desconoce la mayoría de antecedentes previos a la adopción, entre los cuales los más frecuentes son el consumo materno de alcohol durante la gestación (9,3%), los malos tratos (3,5%) y el abandono (3,5%). La edad media de adopción en AI (2,71 años) fue significativamente mayor que en AN, sin diferencias en la edad media de la primera visita. Fueron remitidos desde atención primaria el 51,3% de los casos. Los motivos de consulta principales fueron el retraso psicomotor (20,8%) y los problemas escolares (12,4%). Las patologías neurológicas más prevalentes fueron los problemas de atención (30,5%, significativamente más frecuentes en los grupos AI y AI-E), la discapacidad intelectual (18,6%) y el retraso psicomotor (7,5%). El síndrome alcohólico fetal (18,1%) es prácticamente exclusivo del subgrupo AI-E. Discusión: El país de origen puede influir en el tipo de patología neurológica de los niños adoptados. Ciertos factores, como la edad de adopción, los antecedentes familiares o la estancia en orfanatos, marcan las posibilidades de desarrollo del niño (AU)
Introduction: Spain is the first country in Europe by number of international adoptions. Adopted children may be at increased risk for neurological disease. Objective: Describe the number of patients seen in consultation adopted neuropediatric for a period of 22 years, to determine the most prevalent neurological pathologies and analyze potential risk factors. Patients and methods: Children with a history of adoption attended May-1990 to May-2012 (n= 226) divided into two groups: national adopted (AN= 59) and international (AI= 167). The AI group was subdivided into four areas of origin: Eastern Europe (AI-E), Latin America (AI-L), Eastern Countries (AI-O) and India (AI-I). Results: Most pre-adoption history is unknown, the most frequent alcohol consumption during pregnancy (9.3%), abuse (3.5%) and neglect (3.5%). The average age of adoption AI (2.71 years) was significantly higher than in AN, finding no differences in mean age at first visit. Were referred from primary care 51.3%. The main reasons for visiting were psychomotor retardation (20.8%) and school problems (12.4%). The most prevalent neurological disorders were attention problems (30.5%, significantly more frequent in AI and AI-E), intellectual disability (18.6%) and psychomotor retardation (7.5%). The fetal alcohol syndrome (18.1%) is almost unique subgroup AI-E. Discussion: The country of origin may influence the type of neurological pathology of adopted children. Factors such as age of adoption, family history or stay in orphanages mark the childs developmental possibilities (AU)
Assuntos
Criança , Humanos , Adoção , Doenças do Sistema Nervoso Central/epidemiologia , Deficiências do Desenvolvimento/epidemiologia , Hospitais Pediátricos/estatística & dados numéricos , Fatores de Risco , Transtornos Psicomotores/epidemiologiaRESUMO
INTRODUCTION: Gorlin syndrome (GS) is a disorder transmitted by dominant autosomal inheritance associated to mutations in PTCH1, the main characteristic of which is the appearance of basal cell carcinomas, together with skeletal abnormalities, odontogenic keratocysts and intracranial tumours. CASE REPORT: A girl aged 3 years and 10 months, who was admitted due to acute ataxia. Some of the more striking features in the patient's personal history include psychomotor retardation and a family history of suspected GS in the mother as a result of a maxillary cyst. An examination revealed macrocephaly with a prominent forehead and hypertelorism, as well as nevus. A genetic study for GS was requested, in which mutation c.930delC was detected in exon 6 of the PTCH1 gene in heterozygosis. CONCLUSIONS: In GS there is an increase in the likelihood of developing basal cell carcinomas and strict dermatological monitoring is necessary. A clinical neurological follow-up and also magnetic resonance imaging scans are needed for an early diagnosis of intracranial tumours, especially in the case of medulloblastomas. Odontogenic keratocysts, other skin disorders, and cardiac and ovarian fibromas are characteristic, as are skeletal abnormalities, which require regular clinical and neuroimaging controls and treatment if needed, but radiation must be avoided. GS is a rare disorder, but it must be suspected in the presence of characteristic alterations. It requires a multidisciplinary follow-up, and it is also necessary to establish a protocol on how to act so as to allow early diagnosis and treatment of the potentially severe complications deriving from this disease.
TITLE: Sindrome de Gorlin en la edad pediatrica.Introduccion. El sindrome de Gorlin (SG) es un trastorno de herencia autosomica dominante asociado a mutaciones en el gen PTCH1, cuya principal caracteristica es la aparicion de carcinomas basocelulares, unido a anomalias esqueleticas, queratoquistes odontogenicos y tumores intracraneales. Caso clinico. Niña de 3 años y 10 meses, ingresada por ataxia aguda. Destacan como antecedentes personales retraso psicomotor y como antecedentes familiares la sospecha de SG en la madre por quiste maxilar. En la exploracion, se aprecia macrocefalia con frente prominente e hipertelorismo, asi como nevo. Se solicita estudio genetico de SG, en el que se detecta la mutacion c.930delC en el exon 6 del gen PTCH1 en heterocigosis. Conclusiones. En el SG hay un aumento de la susceptibilidad al desarrollo de carcinomas basocelulares y es preciso un estrecho control dermatologico. Es necesario un seguimiento neurologico clinico y de imagen, mediante resonancia magnetica, para el diagnostico precoz de tumores intracraneales, fundamentalmente el meduloblastoma. Tambien son caracteristicos los queratoquistes odontogenicos, otras alteraciones cutaneas, fibromas cardiacos y ovaricos, asi como anomalias esqueleticas, que precisan controles clinicos y de imagen periodicos, y tratamiento en caso de ser necesarios, pero debe evitarse la radiacion. El SG es un trastorno poco frecuente, que se debe sospechar ante la presencia de alteraciones caracteristicas. Es necesario un seguimiento multidisciplinar, asi como establecer un protocolo de actuacion, para un temprano diagnostico y tratamiento de las complicaciones potencialmente graves derivadas de esta enfermedad.
Assuntos
Síndrome do Nevo Basocelular/diagnóstico , Receptores de Superfície Celular/genética , Adulto , Síndrome do Nevo Basocelular/genética , Pré-Escolar , Deficiências do Desenvolvimento/genética , Éxons/genética , Feminino , Heterozigoto , Humanos , Hipertelorismo/genética , Deficiência Intelectual/genética , Neoplasias Maxilares/genética , Megalencefalia/genética , Receptores Patched , Receptor Patched-1 , Receptores de Superfície Celular/deficiência , Deleção de SequênciaRESUMO
Se presenta el caso de un chico de 14 años que acude a un Servicio de Urgencias hospitalario por presentar dolor mesotorácico y dificultad para respirar. En la radiografía de tórax se aprecia una condensación en el lóbulo superior derecho y serología IgM positiva para Mycoplasma pneumoniae. Inicialmente se diagnosticó de neumonía atípica y se trató con amoxicilina más claritromicina. Cuarenta y ocho horas después acude al centro de Atención Primaria (AP). En la historia clínica de AP figura el antecedente paterno de haber padecido una tuberculosis pleuropulmonar cinco años antes. El niño presentó en ese momento un Mantoux positivo con radiografía de tórax normal y fue tratado de forma profiláctica con isoniacida. Estos antecedentes llevan a plantear el diagnóstico de tuberculosis, repitiéndose el Mantoux y poniendo en marcha la petición de baciloscopias y cultivo para Mycobacterium tuberculosis, siendo ambos positivos. El tratamiento inicial fue sustituido por un tratamiento con cuatro fármacos antituberculosos. La valoración de la renovación de recetas por parte de la enfermera de AP cuestionó el correcto cumplimiento del tratamiento. Todo ello llevó a una mueva intervención del equipo de AP para informar, reforzar y responsabilizar a la familia acerca del correcto cumplimiento del tratamiento (AU)
The authors present the case of a 14 years old boy attended in a hospital emergency room for thoracic pain and difficult breathing. The Rx shows a condensation in LSD and IgM serology positive for mycoplasma pneumoniae. Initially it was diagnosed with atypical pneumonia and was treated with amoxicillin and clarythromicin. Forty-eight hours later he attends the Health Primary Care Center. Primary care medical history contains the paternal antecedent of having suffered a pleuropulmonar tuberculosis five years earlier. The child presented a positive Mantoux with normal Rx at that time and he was treated with prophylactic isoniazid. These records raise the question of the potential diagnosis of tuberculosis, performing the mantoux test again and a smear and culture for mycobacterium tuberculosis, resulting both positive. The initial treatment was replaced by a treatment with four antituberculous drugs. The evaluation of the renewal of prescriptions by the primary care nurse questioned the correct treatment compliance. This led to an intervention of the primary care team to inform, strengthen and force the responsibility of the family about the correct treatment compliance (AU)
Assuntos
Humanos , Masculino , Adolescente , Pneumonia por Mycoplasma/diagnóstico , Pneumonia por Mycoplasma/terapia , Infecções por Mycoplasma/complicações , Infecções por Mycoplasma/diagnóstico , Mycoplasma pneumoniae/isolamento & purificação , Mycoplasma pneumoniae/patogenicidade , Mycobacterium tuberculosis/isolamento & purificação , Claritromicina/uso terapêutico , Isoniazida/uso terapêutico , Etambutol/uso terapêutico , Pneumonia por Mycoplasma/fisiopatologia , Pneumonia por Mycoplasma , Tuberculose Pulmonar/complicações , Pneumonia por Mycoplasma/complicações , Tuberculose Pulmonar/diagnóstico , Atenção Primária à Saúde/métodos , Radiografia Torácica , Rifampina/uso terapêuticoRESUMO
Streptococcus bovis es un microorganismo del grupo D no enterococo, que produce habitualmente infecciones en adultos inmunodeprimidos y, de forma excepcional, casos de infecciones invasivas en neonatos, generalmente causadas por la variante 2 del biotipo II. Es importante la correcta identificación microbiológica, ya que su tratamiento y pronóstico son muy diferentes respecto al resto de estreptococos. Presentamos el caso de un neonato de 9 días de vida, con un cuadro clínico de sepsis y meningitis con convulsiones y hemorragia intracraneal, aislamiento en sangre y en el líquido cefalorraquídeo de S. bovis biotipo I, y buena respuesta clínica al tratamiento con ampicilina y cefotaxima. Este caso es el primero registrado en nuestra unidad, y posiblemente también el primero documentado en la literatura según la revisión de la bibliografía realizada. Se comentan aspectos de interés de la afección (AU)
Streptococcus bovis is a nonenterococcal, group D streptococcus, which frequently causes infections in immunocompromised adults and exceptionally cases of invasive infections in neonates, often caused by the variant 2 of the biotype II. It is important the correct microbiological identification because the treatment and prognostic are very different from other streptococcus. We report a case of a 9-day-old neonate with sepsis and meningitis with seizures and intracranial bleeding, with CSF and blood isolation of S. bovis biotype I, with good response to ampicillin and cefotaxime treatment. This is the first case in our service and probably the first documented in the literature according to the bibliography review. We comment the most interesting aspects of the affection (AU)
