Novel frameshift mutation in LIS1 gene is a probable cause of lissencephaly: a case report.

BACKGROUND: Lissencephaly (LIS) is a cortical malformation, characterized by smooth or nearly smooth cerebral surface and a shortage of gyral and sulcal development, which is caused by deficient neuronal migration during embryogenesis. Neuronal migration involves many gene products, among which is the product of the PAFAH1B1 gene, associated with this disease. LIS is a rare disease, characterized by low population frequency, and with non-specific clinical symptoms such as early epilepsy, developmental delay or cerebral palsy-like motor problems. Given that high-throughput sequencing techniques have been improving diagnosis, we have chosen this technique for addressing this patient. CASE PRESENTATION: We present the case of a seven years old male patient with an undiagnosed rare disease, with non-specific clinical symptoms possibly compatible with lissencephaly. The patient was enrolled in a study that included the sequencing of his whole genome. Sequence data was analyzed following a bioinformatic pipeline. The variants obtained were annotated and then subjected to different filters for prioritization. Also mitochondrial genome was analyzed. A novel candidate frameshift insertion in known PAFAH1B1 gene was found, explaining the index case phenotype. The assessment through in silico tools reported that it causes nonsense mediated mechanisms and that it is damaging with high confidence scores. The insertion causes a change in the reading frame, and produces a premature stop codon, severely affecting the protein function and probably the silencing of one allele. The healthy mother did not carry the mutation, and the unaffected father was not available for analysis. CONCLUSIONS: Through this work we found a novel de novo mutation in LIS1/PAFAH1B1 gene, as a likely cause of a rare disease in a young boy with non-specific clinical symptoms. The mutation found correlates with the phenotype studied since the loss of function in the gene product has already been described in this condition. Since there are no other variants in the PAFAH1B1 gene with low population frequency and due to family history, a de novo disease mechanism is proposed.

Lissencephaly in Shih Tzu dogs.

BACKGROUND: Lissencephaly is a brain malformation characterized by smooth and thickened cerebral surface, which may result in structural epilepsy. Lissencephaly is not common in veterinary medicine. Here, we characterize the first cases of lissencephaly in four Shih Tzu dogs, including clinical presentations and findings of magnetic resonance imaging of lissencephaly and several concomitant brain malformations. CASE PRESENTATION: Early-onset acute signs of forebrain abnormalities were observed in all dogs, which were mainly cluster seizures and behavioral alterations. Based on neurological examination, the findings were consistent with symmetrical and bilateral forebrain lesions. Metabolic disorders and inflammatory diseases were excluded. Magnetic resonance imaging for three dogs showed diffuse neocortical agyria and thickened gray matter while one dog had mixed agyria and pachygyria. Other features, such as internal hydrocephalus, supracollicular fluid accumulation, and corpus callosum hypoplasia, were detected concomitantly. Antiepileptic drugs effectively controlled cluster seizures, however, sporadic isolated seizures and signs of forebrain abnormalities, such as behavioral alterations, central blindness, and strabismus persisted. CONCLUSIONS: Lissencephaly should be considered an important differential diagnosis in Shih Tzu dogs presenting with early-onset signs of forebrain abnormalities, including cluster seizures and behavioral alterations. Magnetic resonance imaging was appropriate for ante-mortem diagnosis of lissencephaly and associated cerebral anomalies.

[Congenital Zika syndrome in Argentina: case series study]. / Síndrome de Zika congénito en la Argentina: presentación de dos casos clínicos.

In 2015, there was an increase in the incidence of congenital microcephaly in newborns in Brazil. Months later, the causal relationship between Zika virus and these findings was discovered. In Argentina, during the first outbreak there were 5 cases of congenital Zika syndrome reported. In 2017, there was a new outbreak which involved Salta province. We describe 2 patients with autochthonous congenital Zika syndrome: one of the babies with severe congenital microcephaly with lissencephaly, calcifications and ventriculomegaly; and another baby with postnatal microcephaly with asymmetric polymicrogyria, calcifications and delayed myelination. The real impact of this disease is still uncertain, so it is necessary an adequate multidisciplinary monitoring of patients exposed to Zika virus to better understand the infection and its natural history.

En 2015, se observó un incremento en la incidencia de microcefalia congénita en recién nacidos en Brasil. Meses más tarde, se descubrió la relación causal entre el virus del Zika y estos hallazgos. Durante el primer brote en la Argentina, se reportaron 5 casos de síndrome de Zika congénito. En 2017, hubo un nuevo brote que involucró la provincia de Salta. En este trabajo, se presentan 2 casos clínicos con síndrome de Zika congénito autóctonos: una paciente con microcefalia congénita grave con lisencefalia, calcificaciones corticosubcorticales y ventriculomegalia y otra paciente con microcefalia posnatal con polimicrogiria asimétrica y calcificaciones subcorticales y retraso en la mielinización. El real impacto de esta enfermedad aún es incierto; es necesario un adecuado seguimiento multidisciplinario de los pacientes expuestos al virus del Zika para comprender mejor la infección y su historia natural.

Congenital Zika Virus Infection: Beyond Neonatal Microcephaly.

IMPORTANCE: Recent studies have reported an increase in the number of fetuses and neonates with microcephaly whose mothers were infected with the Zika virus (ZIKV) during pregnancy. To our knowledge, most reports to date have focused on select aspects of the maternal or fetal infection and fetal effects. OBJECTIVE: To describe the prenatal evolution and perinatal outcomes of 11 neonates who had developmental abnormalities and neurological damage associated with ZIKV infection in Brazil. DESIGN, SETTING, AND PARTICIPANTS: We observed 11 infants with congenital ZIKV infection from gestation to 6 months in the state of Paraíba, Brazil. Ten of 11 women included in this study presented with symptoms of ZIKV infection during the first half of pregnancy, and all 11 had laboratory evidence of the infection in several tissues by serology or polymerase chain reaction. Brain damage was confirmed through intrauterine ultrasonography and was complemented by magnetic resonance imaging. Histopathological analysis was performed on the placenta and brain tissue from infants who died. The ZIKV genome was investigated in several tissues and sequenced for further phylogenetic analysis. MAIN OUTCOMES AND MEASURES: Description of the major lesions caused by ZIKV congenital infection. RESULTS: Of the 11 infants, 7 (63.6%) were female, and the median (SD) maternal age at delivery was 25 (6) years. Three of 11 neonates died, giving a perinatal mortality rate of 27.3%. The median (SD) cephalic perimeter at birth was 31 (3) cm, a value lower than the limit to consider a microcephaly case. In all patients, neurological impairments were identified, including microcephaly, a reduction in cerebral volume, ventriculomegaly, cerebellar hypoplasia, lissencephaly with hydrocephalus, and fetal akinesia deformation sequence (ie, arthrogryposis). Results of limited testing for other causes of microcephaly, such as genetic disorders and viral and bacterial infections, were negative, and the ZIKV genome was found in both maternal and neonatal tissues (eg, amniotic fluid, cord blood, placenta, and brain). Phylogenetic analyses showed an intrahost virus variation with some polymorphisms in envelope genes associated with different tissues. CONCLUSIONS AND RELEVANCE: Combined findings from clinical, laboratory, imaging, and pathological examinations provided a more complete picture of the severe damage and developmental abnormalities caused by ZIKV infection than has been previously reported. The term congenital Zika syndrome is preferable to refer to these cases, as microcephaly is just one of the clinical signs of this congenital malformation disorder.

Lissencephaly-pachygyria and cerebellar hypoplasia in a calf / Lisencefalia-paquigiria e hipoplasia cerebelar em um bovino

A case of lissencephaly-pachygyria and cerebellar hypoplasia diagnosed in a Charolais x Tabapuã calf is described. The calf presented since birth, clinical signs characterized by apathy, prolonged recumbency, tremors of the head and neck, ataxia, hypermetria, difficulty walking, blindness and swelling of the joints of the four limbs. Due to the unfavorable prognosis, the animal was euthanized and necropsied at 34 days of age. At necropsy, a rudimentary development of the brain folds (gyri) and grooves (sulci) was observed, and the cerebellum was hypoplastic. The cut surface of the brain exhibited thickening of the gray matter (pachygyria) in the frontal, parietal, temporal and occipital cortices and narrowing of the white matter. In the organs of the thoracic and abdominal cavities, no significant lesions were observed. Histologically, cerebral cortex was thick and exhibited neuronal disorganization of the gray matter. The cerebellum had a thin molecular layer, and neuronal disorganization with ectopia of the Purkinje neurons in the region of the granular and molecular layers. There were no bacterial growths in cultures of joint swabs. This was the only case on the property, which suggests that this malformation, which has not previously been described in cattle, was a sporadic case, and it was not possible to determine its cause. Neurological lesions and clinical sings presented here should be considered in the differential diagnosis of congenital diseases of the central nervous systems of cattle.

Descreve-se um caso de lisencefalia-paquigiria e hipoplasia cerebelar diagnosticado em um bovino, macho, cruza Charolês x Tabapuã que apresentava, desde o nascimento, sinais clínicos caracterizados por apatia, decúbito prolongado, tremores da cabeça e do pescoço, ataxia, hipermetria, dificuldade na marcha, cegueira e aumento de volume nas articulações dos quatro membros. Devido ao prognóstico desfavorável, o bovino foi eutanasiado e necropsiado aos 34 dias de idade. Na abertura da caixa craniana, observou-se formação rudimentar dos giros do telencéfalo e cerebelo hipoplásico. Ao corte o encéfalo, apresentava espessamento da substância cinzenta (paquigiria) do córtex frontal, parietal, temporal e occipital e estreitamento da substância branca. Nos órgãos das cavidades torácica e abdominal, não foram observadas lesões significativas. Histologicamente, no córtex cerebral havia desorganização neuronal da substância cinzenta que estava espessa. No cerebelo, havia diminuição da camada molecular e desorganização neuronal com ectopia dos neurônios de Purkinje na região das camadas granular e molecular. Não houve crescimento bacteriano das culturas de suabes das articulações. O fato de ser o único caso na propriedade sugere que a malformação, sem descrição anterior em bovinos, trata-se de caso esporádico, não sendo determinada sua causa. As alterações neurológicas aqui observadas devem ser levadas em consideração no diagnóstico diferencial de enfermidades congênitas do sistema nervoso central de bovinos.

Lissencephaly-pachygyria and cerebellar hypoplasia in a calf / Lisencefalia-paquigiria e hipoplasia cerebelar em um bovino

A case of lissencephaly-pachygyria and cerebellar hypoplasia diagnosed in a Charolais x Tabapuã calf is described. The calf presented since birth, clinical signs characterized by apathy, prolonged recumbency, tremors of the head and neck, ataxia, hypermetria, difficulty walking, blindness and swelling of the joints of the four limbs. Due to the unfavorable prognosis, the animal was euthanized and necropsied at 34 days of age. At necropsy, a rudimentary development of the brain folds (gyri) and grooves (sulci) was observed, and the cerebellum was hypoplastic. The cut surface of the brain exhibited thickening of the gray matter (pachygyria) in the frontal, parietal, temporal and occipital cortices and narrowing of the white matter. In the organs of the thoracic and abdominal cavities, no significant lesions were observed. Histologically, cerebral cortex was thick and exhibited neuronal disorganization of the gray matter. The cerebellum had a thin molecular layer, and neuronal disorganization with ectopia of the Purkinje neurons in the region of the granular and molecular layers. There were no bacterial growths in cultures of joint swabs. This was the only case on the property, which suggests that this malformation, which has not previously been described in cattle, was a sporadic case, and it was not possible to determine its cause. Neurological lesions and clinical sings presented here should be considered in the differential diagnosis of congenital diseases of the central nervous systems of cattle.(AU)

Descreve-se um caso de lisencefalia-paquigiria e hipoplasia cerebelar diagnosticado em um bovino, macho, cruza Charolês x Tabapuã que apresentava, desde o nascimento, sinais clínicos caracterizados por apatia, decúbito prolongado, tremores da cabeça e do pescoço, ataxia, hipermetria, dificuldade na marcha, cegueira e aumento de volume nas articulações dos quatro membros. Devido ao prognóstico desfavorável, o bovino foi eutanasiado e necropsiado aos 34 dias de idade. Na abertura da caixa craniana, observou-se formação rudimentar dos giros do telencéfalo e cerebelo hipoplásico. Ao corte o encéfalo, apresentava espessamento da substância cinzenta (paquigiria) do córtex frontal, parietal, temporal e occipital e estreitamento da substância branca. Nos órgãos das cavidades torácica e abdominal, não foram observadas lesões significativas. Histologicamente, no córtex cerebral havia desorganização neuronal da substância cinzenta que estava espessa. No cerebelo, havia diminuição da camada molecular e desorganização neuronal com ectopia dos neurônios de Purkinje na região das camadas granular e molecular. Não houve crescimento bacteriano das culturas de suabes das articulações. O fato de ser o único caso na propriedade sugere que a malformação, sem descrição anterior em bovinos, trata-se de caso esporádico, não sendo determinada sua causa. As alterações neurológicas aqui observadas devem ser levadas em consideração no diagnóstico diferencial de enfermidades congênitas do sistema nervoso central de bovinos.(AU)

Response to Comments on "Cortical folding scales universally with surface area and thickness, not number of neurons".

De Lussanet claims that our model that accounts for the degree of folding of the cerebral cortex based on the product of cortical surface area and the square root of cortical thickness is better reduced to the product of gray-matter proportion and folding index. Lewitus et al., in turn, claim that the assumptions of our model are in conflict with experimental data; that the model does not accurately fit the data; and that the ancestral mammalian brain was gyrencephalic. Here, we show that both claims are inappropriate.

BRAIN STRUCTURE. Cortical folding scales universally with surface area and thickness, not number of neurons.

Larger brains tend to have more folded cortices, but what makes the cortex fold has remained unknown. We show that the degree of cortical folding scales uniformly across lissencephalic and gyrencephalic species, across individuals, and within individual cortices as a function of the product of cortical surface area and the square root of cortical thickness. This relation is derived from the minimization of the effective free energy associated with cortical shape according to a simple physical model, based on known mechanisms of axonal elongation. This model also explains the scaling of the folding index of crumpled paper balls. We discuss the implications of this finding for the evolutionary and developmental origin of folding, including the newfound continuum between lissencephaly and gyrencephaly, and for pathologies such as human lissencephaly.

Trastornos de la migración neuronal: un caso de lisencefalia / Neuronal migration disorders: a lissencephaly case

Las malformaciones del desarrollo cortical originan un grupo de patologías, que cursan con diversas manifestaciones las cuales marcan un grado de minusvalía significativo en quienes las padecen. La Lisencefalia es una de las alteraciones de la migración neuronal caracterizada por una corteza cerebral de superficie lisa o con pocas circunvoluciones. Este trastorno está frecuentemente asociado a epilepsias de difícil manejo. Se presenta el caso de un paciente masculino de 18 meses de edad con diagnóstico de Lisencefalia quien cursa con convulsiones tónicas generalizadas desde los 8 meses de edad. Se le realizó TAC de cráneo simple y resonancia magnética de cerebro para confirmar el diagnóstico y se dio manejo farmacológico a las convulsiones.

Malformations of cortical development originate a group of pathologies that involve diverse manifestations that mark a significant degree of disability in those who suffer from. The Lissencephaly is one of alterations in neuronal migration characterized by a smooth surface or with few convolutions in the cerebral cortex. This disorder is often associated with difficult management Epilepsies. We report the case of a male patient from 18 months of age with a diagnosis of Lissencephaly, who presents generalized tonic seizures from 8 months of age. Was performed a simple skull CT and brain magnetic resonance to confirm the diagnosis and the pharmacological management was given to seizures.

Lisencefalia y anomalías asociadas / Lissencephaly and associated anomalies

La lisencefalia (cerebro liso) es una malformación del desarrollo cortical, caracterizada por una deficiente giración, con aspecto macroscópico liso del cerebro. Es causada por una migración neuronal anormal entre las semanas 9 y 13 de la gestación, consecutivas a infecciones virales intrauterinas, ingestión de tóxicos durante el embarazo, radiaciones, escaso fluido de sangre al cerebro o trastornos genéticos asociados a los cromosomas X y 17, con expresión fenotípica variable; se describen tres tipos y se asocia a una veintena de síndromes con esta dolencia, entre ellos: el síndrome de Miller-Dieker, el síndrome de Fukuyama, la enfermedad músculo-ojo-cerebro y el síndrome de Walker-Warburg.2,3 Las lisencefalias clásicas tienen una frecuencia de 11,7 por millón de recién nacidos (1/ 85 470), pero la prevalencia de las formas leves se desconoce(AU)

Avaliação de linguagem em um caso de associação entre surdez e paquigiria / Language evaluation in a case of association between deafness and pachygyria

Para que ocorra a aquisição e o desenvolvimento da linguagem é necessária a associação de uma série de fatores, cujo funcionamento harmonioso determina o sucesso desse processo. O comprometimento auditivo pode ser um obstáculo, mas, mesmo assim, a criança surda será capaz de adquirir linguagem por meio de uma língua de sinais. Porém, quando a criança apresenta alterações neurológicas, o acompanhamento fonoaudiológico se faz necessário. Esta pesquisa é um estudo de caso sobre uma criança surda, com idade de 5 anos e 10 meses, em processo de aquisição da língua de sinais, com comprometimento neurológico. Tem como objetivo avaliar, analisar e aprofundar conhecimentos sobre uma doença rara (paquigiria), associada com surdez, mostrando os impactos que isso pode acarretar à criança, em relação à comunicação. A coleta de dados foi efetuada por meio de avaliações formais e observacionais sobre habilidade e modalidade de comunicação utilizada, desenvolvimento linguístico, fonologia e conhecimento lexical na Língua Brasileira de Sinais (LIBRAS), além da aplicação de um questionário. Os resultados apontaram atraso no processo de aquisição de linguagem, mesmo considerando-se a defasagem entre o nascimento da criança e o início da aquisição da LIBRAS, aspectos que podem estar relacionados com o diagnóstico de paquigiria. É importante que o fonoaudiólogo conheça a LIBRAS e saiba avaliar a linguagem da criança utente dessa língua, pois casos como estes revelam a complexidade da associação entre surdez e quadros neurológicos variados.

In order for the acquisition and development of language to occur, it is necessary to associate a number of factors, whose harmonious functioning determines the success of this process. The hearing loss may be an obstacle, but even so, the deaf child will be able to acquire language through a sign language. However, when the child shows neurological changes, the speech monitoring becomes necessary. This research is a case study of a deaf child, aged 5 years and 10 months, in the acquisition of sign language, who presents neurological impairment. It aims to assess, analyze, and deepen the knowledge on a rare disease (pachygyria) associated with deafness, showing the impact that this can pose to the child regarding communication. Data collection was done through formal evaluations and observational regarding the ability and modality used for communication, language development, phonological and lexical knowledge in Brazilian Sign Language (LIBRAS); in addition to a questionnaire. The results showed delay in language acquisition, even considering the gap between the child’s birth and the early acquisition of LIBRAS, aspects that may be related to the diagnosis of pachygyria. It is important that the audiologist know LIBRAS and know to assess the language of the child who uses this language, because cases like these reveal the complexity of the association between deafness and various neurological disorders.

Development of fetal brain sulci and gyri: assessment through two and three-dimensional ultrasound and magnetic resonance imaging.

BACKGROUND: Cerebral malformations may lead to permanent postnatal sequels. The antenatal detection of anomalous or absent fetal sulci and gyri may indicate abnormal brain development and future neurological and psychomotor problems in that infant. The prenatal diagnosis of these conditions allows genetic counseling, psychological support of the parents and optimization of obstetric management. Diagnosis is usually based on two-dimensional obstetric ultrasound (2DUS) and eventually fetal magnetic resonance imaging (MRI), to confirm findings. Fetal three-dimensional ultrasound (3DUS) using the rendering mode has been recently introduced but has not yet been extensively tested in clinical practice. CONTEXT: This study reviewed and compared three imaging modalities, 2DUS, 3DUS, and MRI, in the analysis of the development of the main sulci and gyri of central nervous system of normal fetuses between 20 and 32 weeks' gestation.

Lissencephaly, abnormal genitalia and refractory epilepsy: case report of XLAG syndrome / Lisencefalia, genitália ambígua e epilepsia refratária: relato de caso da síndrome XLAG

INTRODUCTION: X-linked lissencephaly with ambiguous genitalia (XLAG) is a recently described genetic disorder caused by mutation in the aristaless-related homeobox (ARX) gene (Xp22.13). Patients present with lissencephaly, agenesis of the corpus callosum, refractory epilepsy of neonatal onset, acquired microcephaly and male genotype with ambiguous genitalia. CASE REPORT: Second child born to healthy nonconsanguineous parents, presented with seizures within the first hour of life that remained refractory to phenobarbital, phenytoin and midazolam. Examination identified microcephaly, axial hypotonia, pyramidal signs and ambiguous genitalia. EEG showed disorganized background activity and seizures starting at the right midtemporal, central and occipital regions. MRI showed diffuse pachygyria, moderate thickening of the cortex, enlarged ventricles, agenesis of the corpus callosum and septum pellucidum. Karyotype showed a 46,XY genotype. Additional findings were hypercalciuria, vesicoureteral reflux, patent ductus arteriosus and chronic diarrhea.

INTRODUÇÃO: Lisencefalia com genitália ambígua ligada ao X (XLAG) é doença genética recentemente descrita, causada por mutação no gene aristaless-related homeobox (ARX) (Xp22.13). Os pacientes apresentam lisencefalia, agenesia de corpo caloso, epilepsia refratária com início no período neonatal, microcefalia adquirida e genótipo masculino com genitália ambígua. RELATO DE CASO: Segundo filho de pais não-consangüíneos, apresentou crises na primeira hora de vida que permaneceram refratárias a fenobarbital, fenitoína e midazolam. Apresentava microcefalia, hipotonia axial, sinais de liberação piramidal e genitália ambígua. EEG demonstrou atividade de base desorganizada, crises convulsivas com início nas regiões temporal-média, central e occipital direitas. RNM demonstrou paquigiria difusa, moderado espessamento do córtex, ventrículos aumentados, agenesia de corpo caloso e septo pelúcido. Cariótipo evidenciou genótipo 46,XY. Achados adicionais foram: hipercalciúria, refluxo vésico-ureteral, ducto arterioso persistente e diarréia crônica.

Epilepsia e desordens de malformação do desenvolvimento cortical / Epilepsy and malformations of cortical development disorders

OBJETIVOS: As desordens do desenvolvimento cortical (DDC) constituem a segunda causa de epilepsia refratária. Diversas patologias estão incluídas nas DDC. Seu diagnóstico foi facilitado com o desenvolvimento na neuroimagem. MÉTODOS: No presente artigo, apresentamos sete casos divididos em três grupos, de acordo com o mecanismo de produção das DDC: 1) anormalidades da proliferação e diferenciação de neurônios da glia; 2) anormalidades de migração neuronal; 3) anormalidades na organização neuronal. A investigação consistiu em história mais exame neurológico, avaliação neuropsicológica, ressonância magnética e eletrencefalograma. RESULTADOS E CONCLUSÕES: Três pacientes apresentaram displasia cortical focal, dois apresentaram heterotopia em banda, um paciente apresentava lisencefalia e uma apresentava esquizencefalia. Todos os pacientes apresentavam epilepsia de difícil controle. Malformações corticais constituem um grupo heterogêneo de causas de epilepsia de difícil controle. É importante para o manejo médico que as diversas formas de malformações corticais sejam conhecidas e diagnosticadas, o que foi facilitado pelo advento da ressonância magnética.

OBJECTIVES: Cortical development disorders (CDD) are the second cause of refratary epilepsy. Various patologies are included in the CDD. The diagnosis was easy with the continuous development of the neuroimaging. METHODS: In the present paper we show seven cases divided in three groups, accourding with the mecanism of production of the CDD: 1) proliferation and diferentiation abnormalities of the glial cells; 2) abnormalities of the neuronal migration; 3) abnormalities of the neuronal organization. The investigation consisted in story and neurological examination, neuropsicological avaliation, magnetic ressonance imaging and eletroencephalogram. RESULTS AND CONCLUSION: Three patients had focal cortical dysplasia; two had heterotopic band, one patient had lissecephaly and another had schizencephaly. All the patients had refractory epilepsy. Cortical malformations are a heterogeneous group of refractory epilepsy. Knowing and diagnosing these different types of cortical malformations are important steps for their treatment, and were facilitated by de advent of magnetic resonance imaging.

Trastorno de migración neuronal: a propósito de un caso / Neuronal migration disorder: a clinic case

El Trastorno de Migración Neuronal (TMN) se caracteriza por una serie de malformaciones del Sistema Nervioso Central (SNC) que ocurre entre el segundo y quinto mes de gestación; de etiologías variadas. Producen grados diversos de retardo psicomotriz, convulsiones y otras manifestaciones dependiendo de las áreas afectadas. Presentamos el caso de una paciente de 3 meses de edad, sexo femenino, que presentó convulsiones caracterizadas por espasmos en flexión desde el nacimiento, frecuentes y de corta duración, resistentes a tratamiento anticonvulsivante, sin antecedentes infecciosos, obtenida por cesárea sin complicaciones. Se realizó una TAC, un EEG y una RMN, revelando lisencefalia, hemimegalencefalia y esquizoencefalia del hemisferio cerebral derecho e hipoplasia del cuerpo calloso.

The Neuronal Migration Disorder is characterized by a series of malformations of central nervous system that occur between the second and fifth month of gestation; of different etiologies. Have many grades of psychomotor retarded, seizures and others manifestations depending of affect areas. Present a clinic case of a patient of 3 month old, feminine sex, who presents seizures by spasm in flexion since born, frequent and short durations, resistant a anticonvulsant treatment, without infection record, obtained by caesarean without complications. Performed a TAC, a EEG and a RMN, showed a lisencephaly, hemimegalencephaly and schizoencephaly of right cerebral hemisphere and callus body hipoplasia.

Lissencephaly, abnormal genitalia and refractory epilepsy: case report of XLAG syndrome.

INTRODUCTION: X-linked lissencephaly with ambiguous genitalia (XLAG) is a recently described genetic disorder caused by mutation in the aristaless-related homeobox (ARX) gene (Xp22.13). Patients present with lissencephaly, agenesis of the corpus callosum, refractory epilepsy of neonatal onset, acquired microcephaly and male genotype with ambiguous genitalia. CASE REPORT: Second child born to healthy nonconsanguineous parents, presented with seizures within the first hour of life that remained refractory to phenobarbital, phenytoin and midazolam. Examination identified microcephaly, axial hypotonia, pyramidal signs and ambiguous genitalia. EEG showed disorganized background activity and seizures starting at the right midtemporal, central and occipital regions. MRI showed diffuse pachygyria, moderate thickening of the cortex, enlarged ventricles, agenesis of the corpus callosum and septum pellucidum. Karyotype showed a 46,XY genotype. Additional findings were hypercalciuria, vesicoureteral reflux, patent ductus arteriosus and chronic diarrhea.