Congenital adrenal hyperplasia, ovarian failure and Ehlers-Danlos syndrome due to a 6p deletion.

[congenital adrenal hyperplasia]

Cryptic deletions in balanced de novo translocations represent a frequent cause of abnormal phenotypes , including Mendelian diseases . In this study , we describe a patient with multiple congenital abnormalities , such as late-onset congenital adrenal hyperplasia (CAH ), primary ovarian failure and Ehlers-Danlos syndrome (EDS ), who carries a de novo t (6 ;14 )(p 21 ;q 32 ) translocation . Genomic array analysis identified a cryptic 1 .1 -Mb heterozygous deletion , adjacent to the breakpoint on chromosome 6 , extending from 6 p 21 .33 to 6 p 21 .32 and affecting 85 genes , including CYP 21 A 2 ,TNXB and MSH 5 . Multiplex ligation-dependent probe amplification analysis of the 6 p 21 .3 region was performed in the patient and her family and revealed a 30 -kb deletion in the patient 's normal chromosome 6 , inherited from her mother , resulting in homozygous loss of genes CYP 21 A 1 P and C 4 B . CYP 21 A 2 sequencing showed that its promoter region was not affected by the 30 -kb deletion , suggesting that the deletion of other regulatory sequences in the normal chromosome 6 caused a loss of function of the CYP 21 A 2 gene . EDS and primary ovarian failure phenotypes could be explained by the loss of genes TNXB and MSH 5 , a finding that may contribute to the characterization of disease-causing genes . The detection of this de novo microdeletion drastically reduced the estimated recurrence risk for CAH in the family .