Genotype-phenotype analysis of the branchio-oculo-facial syndrome.

نویسندگان

Jeff M Milunsky

Tom M Maher

Geping Zhao

Zhenyuan Wang

John B Mulliken

David Chitayat

Michele Clemens

Heather J Stalker

Mislen Bauer

Michele Burch

Sébastien Chénier

Michael L Cunningham

Arlene V Drack

Sandra Janssens

Audrey Karlea

Regan Klatt

Usha Kini

Ophir Klein

Augusta M Lachmeijer

Andre Megarbane

Nancy J Mendelsohn

Wendy S Meschino

Geert R Mortier

Sandhya Parkash

C Renai Ray

Angharad Roberts

Amy Roberts

Willie Reardon

Rhonda E Schnur

Rosemarie Smith

Miranda Splitt

Kamer Tezcan

Margo L Whiteford

Derek A Wong

Roberto Zori

Angela E Lin

چکیده

Branchio-oculo-facial syndrome (BOFS; OMIM#113620) is a rare autosomal dominant craniofacial disorder with variable expression. Major features include cutaneous and ocular abnormalities, characteristic facies, renal, ectodermal, and temporal bone anomalies. Having determined that mutations involving TFAP2A result in BOFS, we studied a total of 30 families (41 affected individuals); 26/30 (87%) fulfilled our cardinal diagnostic criteria. The original family with the 3.2 Mb deletion including the TFAP2A gene remains the only BOFS family without the typical CL/P and the only family with a deletion. We have identified a hotspot region in the highly conserved exons 4 and 5 of TFAP2A that harbors missense mutations in 27/30 (90%) families. Several of these mutations are recurrent. Mosaicism was detected in one family. To date, genetic heterogeneity has not been observed. Although the cardinal criteria for BOFS have been based on the presence of each of the core defects, an affected family member or thymic remnant, we documented TFAP2A mutations in three (10%) probands in our series without a classic cervical cutaneous defect or ectopic thymus. Temporal bone anomalies were identified in 3/5 patients investigated. The occurrence of CL/P, premature graying, coloboma, heterochromia irides, and ectopic thymus, are evidence for BOFS as a neurocristopathy. Intrafamilial clinical variability can be marked. Although there does not appear to be mutation-specific genotype-phenotype correlations at this time, more patients need to be studied. Clinical testing for TFAP2A mutations is now available and will assist geneticists in confirming the typical cases or excluding the diagnosis in atypical cases.

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منابع مشابه

A Case of Branchio-oculo-facial Syndrome.

Branchio-oculo-facial syndrome (BOFS) is a rare, autosomal dominant disorder. It is characterized by distinct craniofacial abnormalities including abnormal location of the ears, aplastic cervical skin lesions, malformed auricles, conductive hearing loss, ocular abnormalities, and cleft lip and palate. Herein, we describe a case of BOFS with persistent aplasia cutis of the neck in a 5-year-old g...

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Analysis of TFAP2A mutations in Branchio-Oculo-Facial Syndrome indicates functional complexity within the AP-2α DNA-binding domain.

Multiple lines of evidence indicate that the AP-2 transcription factor family has an important regulatory function in human craniofacial development. Notably, mutations in TFAP2A, the gene encoding AP-2α, have been identified in patients with Branchio-Oculo-Facial Syndrome (BOFS). BOFS is an autosomal-dominant trait that commonly presents with facial clefting, eye defects and branchial skin ano...

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عنوان ژورنال:

American journal of medical genetics. Part A

دوره 155A 1 شماره

صفحات -

تاریخ انتشار 2011