Clinical, genetic and molecular study of Rokitansky-Mayer-Küster-Hauser syndrome and related conditions / Estudo genético-clínico e molecular da síndrome de Rokitansky-Mayer-Küster-Hauser e condições afins

AUTOR(ES)

Carola Cheroki

DATA DE PUBLICAÇÃO

2008

RESUMO

Background: Mayer-Rokitansky-Küster-Hauser (MRKH) syndrome, comprising utero-vaginal atresia in otherwise phenotypically normal women with a normal karyotype (46,XX), has an incidence of about 1/5,000 among newborn girls. Anomalies of the genital tract range from upper vaginal atresia to total Müllerian agenesis (congenital absence of the Fallopian tubes, uterus, and upper vagina). Patients with müllerian aplasia (MA) often exhibit additional clinical features such as renal, vertebral and cardiac defects. A number of different syndromes have been associated with MA, and in most cases its aetiology remains poorly understood. We studied 43 women with the MRKH defect and 21 relatives presenting associated anomalies. The study included clinical and ultrasonographic examination of the urogenital system, radiographs of the vertebral column and sequencing of three candidate genes named RAR gama, RXR alpha and WNT-4. Fifteen of our patients, with more complex phenotypes (genital, renal, cardiac, and skeletal defects), were screened for DNA copy number changes by 1 Mb whole genome bacterial artificial chromosome (BAC) array based comparative genomic hybridization (CGH). The detected alterations were validated by an independent method and further mapped by high resolution oligo-arrays. Results: All patients had a normal 46,XX karyotype and were also normal to the RAR gama, RXR alpha and WNT-4 genes. Submicroscopic genomic imbalances affecting the 1q21.1, 17q12, 22q11.21, and Xq21.31 chromosome regions were detected in five probands. Presence of the alterations in the normal mother of one patient suggests incomplete penetrance and/or variable expressivity. Conclusion: 5 of the 15 patients were found to have cryptic genomic alterations. The imbalances on 22q11.21 support recent findings by us and others that alterations in this chromosome region may result in impairment of müllerian duct development. The remaining imbalances indicate involvement of previously unknown chromosome regions in MA, and point specifically to LHX1 and KLHL4 as candidate genes.

ASSUNTO(S)

genomic imbalances expressividade variável short vagina aplasia útero vaginal array-cgh absent or rudimentary uterus copy number variation (cnvs) anomalias cromossômicas submicroscópicas

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