ABSTRACT
Joubert syndrome (JS) is an autosomal recessive inherited disorder characterized by hypotonia, cerebellar vermis hypoplasia, ocular abnormalities (e.g, pigmentary retinopathy, oculomotor apraxia and nystagmus), renal cysts and hepatic fibrosis. Respiratory abnormalities, as apnea and hyperpnea, may be present, as well as mental retardation. At least seven JS loci have been determined and five genes identified. Herein, we report five children, belonging to independent families, with JS: they shared the same typical MRI abnormality, known as molar tooth sign, but had an otherwise quite variable phenotype, regarding mostly their cognitive performance, visual abilities and extra-neurological compromise.
A síndrome de Joubert (SJ) é uma doença hereditária, autossômica recessiva, caracterizada por hipotonia, hipoplasia do vermis cerebelar, anormalidades oculares (p.ex., retinite pigmentar, apraxia oculomotora e nistagmo), cistos renais e fibrose hepática. Anormalidades respiratórias tais como apnéia e hiperpnéia podem estar presentes, assim como deficiência mental. Pelo menos sete loci e cinco genes diferentes associados à SJ já foram identificados. Este artigo relata cinco crianças com SJ, pertencentes a diferentes famílias. Todos os pacientes compartilham a mesma anormalidade típica da RM, conhecida como sinal do dente molar, e apresentam ampla variabilidade clínica em relação ao desempenho cognitivo, comprometimento visual e alterações extra-neurológicas.
Subject(s)
Adolescent , Child , Child, Preschool , Female , Humans , Male , Cerebellum/abnormalities , Intellectual Disability , Kidney Diseases/pathology , Ocular Motility Disorders/pathology , Cerebellum/pathology , Kidney Diseases/congenital , Kidney Diseases/genetics , Magnetic Resonance Imaging , Ocular Motility Disorders/congenital , Ocular Motility Disorders/genetics , SyndromeABSTRACT
We present a two-generation family with Brown syndrome. The proband was a six and a half-year-old female who presented with a history of failure of dextro-elevation of her left eye. A full ophthalmic evaluation was consistent with a left Brown syndrome. Family history revealed that her mother was operated on as a child for left Brown syndrome and examination of her four and a half-year-old sibling showed similar affection in the left eye. Autosomal dominant inheritance has been postulated in this condition. To our knowledge this is the first report of three members of a two-generation family with left-sided Brown syndrome. Genetic counseling of Brown syndrome cases is advised; nevertheless, identification of the responsible gene should shed more light on its genetics.
Subject(s)
Adult , Child , Eye Movements/physiology , Female , Follow-Up Studies , Genetic Predisposition to Disease , Humans , Infant , Male , Nuclear Family , Ocular Motility Disorders/genetics , Pedigree , Phenotype , Vision, BinocularABSTRACT
Objetivo: Correlacionar tipo clínico de fibrosis muscular congénita (CFEOM tipo 1) y falla genética en los miembros afectados en tres generaciones de una familia chilena. Metodología: enrolamiento de portadores de fibrosis muscular congénita tipo clínico 1 (CFEOM 1) según protocolo. Fotografía y video, pedigrí familiar, obtención de muestra de sangre, extracción del DNA linfositario de casos/control, Linkage análisis de DNA. Resultados: Identificación de mutación AD en cromosoma 11, gen KIF21A en todos los afectados en una familia con tres generaciones con CFEOM tipo 1. Codifica proteína motora kinesina, que participa en el desarrollo del III par craneal. Conclusiones: En este tipo de estrabismo la alteración primaria es inervacional y no muscular. Relación entre forma clínica y cromosoma afectado permite caracterizar genéticamente las distintas formas clínicas de la enfermedad. Se propone una clasificación clínica nueva de los estrabismos restrictivos congénitos.
Aim: To correlate a clinical type of congenital muscular fibrosis (CFEOM type 1) with a genetic flaw in the affected members of three generations of a single Chilean family. Methods: Clinical type 1 congenital muscular fibrosis carriers were enrolled according to protocol. For each patient, the following information was collected: Video and pictures, family pedigree, blood samples, case/ control lymphocytes DNA, and DNA linkage analysis. Results: An AD mutation in chromosome 11 was identified. KIF21A gene was found in all affected members of the family over the three generations. It codified The motor protein kinesin, which is involved in the development of the third cranial nerve. Conclusions: In this form of strabismus, the primary dysfunction is innervational rather than muscular. The relationship between the clinical form and the affected chromosome permits identification of the various clinical forms of the disease. We propose a new clinical classification of the congenital restrictive strabismus.