RESUMO
Introducción: La córnea plana congénita es una rara anomalía de herencia autosómica dominante o recesiva. Los defectos del ciclo de la urea son errores innatos del metabolismo que puede producir encefalopatía progresiva. Objetivo: Describir las características clínicas de un paciente con diagnósticos de córnea plana congénita y error innato del metabolismo. Presentación del caso: Paciente masculino de 7 años de edad, miembro de la cuarta generación de una familia con diagnóstico de córnea plana congénita. Al examen oftalmológico se observó en ambos ojos esclerización superior del limbo, aplanamiento corneal generalizado y cámaras anteriores estrechas. La topografía corneal mostró patrones esféricos y aplanamiento corneal más prominente en la media y extrema periferia. A la edad de 5 años comenzó a presentar ataxia recurrente, crisis epilépticas de inicio focal motoras clónicas en el hemicuerpo derecho y vómitos. Ingresó en estado de coma en la unidad de cuidados intensivos pediátricos del Hospital Pediátrico Universitario "William Soler". Se planteó encefalopatía progresiva por trastorno en el ciclo de la urea luego de constatarse hiperamonemia (error congénito del metabolismo), sin acidosis metabólica. Conclusiones: La córnea plana congénita es una enfermedad caracterizada por aplanamiento corneal generalizado con repercusión en la calidad visual. Los errores innatos del metabolismo debidos a trastornos en el ciclo de la urea se caracterizan por manifestaciones neurológicas graves con peligro potencial para la vida. Resulta novedosa la presentación de estas dos enfermedades infrecuentes en un mismo paciente, asociación que no aparece publicada con anterioridad.
Introduction: Congenital flat cornea is a rare anomaly of dominant or recessive autosomal inheritance. Urea cycle defects are inborn errors of metabolism that can lead to progressive encephalopathy. Objective: To describe the clinical characteristics of a patient with diagnoses of congenital flat cornea and inborn error of metabolism. Case Presentation: A 7-year-old male patient, member of the fourth generation of a family diagnosed with congenital flat cornea. Ophthalmological examination showed upper limbal sclerization, generalized corneal flattening and narrow anterior chambers in both eyes. Corneal topography showed more prominent spherical patterns and corneal flattening in the middle and extreme periphery. At the age of 5 years, he began to present recurrent ataxia, focal onset epileptic seizures of clonic motor in the right hemibody and vomiting. He was admitted in a coma in the pediatric intensive care unit of "William Soler" University Pediatric Hospital. Progressive encephalopathy was stated due to disorder in the urea cycle after hyperammonemia (congenital error of metabolism) was observed, without metabolic acidosis. Conclusions: Congenital flat cornea is a disease characterized by generalized corneal flattening with an impact on visual quality. Inborn errors of metabolism due to disorders in the urea cycle are characterized by severe neurological manifestations with potential danger to life. The presentation of these two rare diseases in the same patient is novel; an association that has not been published previously.
RESUMO
MIDAS syndrome (microphthalmia-dermal aplasia-sclerocornea) is an X-linked dominant genetic disease. In most patients, the unbalanced translocation or deletion of the X chromosome short-arm 22.3 band is observed. This disease characteristically presents as linear atrophy of the skin limited to the face and neck, accompanied by congenital eye disease. A 9-month-old female who had linear skin atrophy on the right side of her chin visited our clinic. She also presented with microphthalmia and sclerocornea on her right eye. Results of a chromosomal study revealed a deletion of the X-chromosome short-arm 22.31 band. Here, we report on this MIDAS syndrome patient with linear skin atrophy on the face.
Assuntos
Feminino , Humanos , Lactente , Atrofia , Queixo , Oftalmopatias , Microftalmia , Pescoço , Pele , Cromossomo XRESUMO
The developmental birth eye disorder of iris is known as aniridia. Heterozygous PAX6 gene, which causes human aniridia and small eye in mice, is located on chromosome 11p13. The variability had been documented between the affected individuals within the families, is due to genotypic variation. Haploinsufficiency renders PAX6 allele non-functional or amorphic, however it presents hypomorphic or neomorphic alleles. India is not a well-studied ethnic group, hence the focus on congenital aniridia gene analysis supports the literature and the phenotypic association were analysed both in sporadic as well as familial. The consistent association of truncating PAX6 mutations with the phenotype is owing to non-sensemediated decay (NMD). It is presumed that the genetic impact of increased homozygosity and heterozygocity in Indian counter part arises as the consequence of consanguineous marriages. The real fact involved in congenital aniridia with other related phenotypes with PAX6 mutations are still controversial.