Abstract
Oculofaciocardiodental (OFCD) and Lenz microphthalmia syndromes form part of a spectrum of X-linked microphthalmia disorders characterized by ocular, dental, cardiac and skeletal anomalies and mental retardation. The two syndromes are allelic, caused by mutations in the BCL-6 corepressor gene (BCOR). To extend the series of phenotypes associated with pathogenic mutations in BCOR, we sequenced the BCOR gene in patients with (1) OFCD syndrome, (2) putative X-linked ('Lenz') microphthalmia syndrome, (3) isolated ocular defects and (4) laterality phenotypes. We present a new cohort of females with OFCD syndrome and null mutations in BCOR, supporting the hypothesis that BCOR is the sole molecular cause of this syndrome. We identify for the first time mosaic BCOR mutations in two females with OFCD syndrome and one apparently asymptomatic female. We present a female diagnosed with isolated ocular defects and identify minor features of OFCD syndrome, suggesting that OFCD syndrome may be mild and underdiagnosed. We have sequenced a cohort of males diagnosed with putative X-linked microphthalmia and found a mutation, p.P85L, in a single case, suggesting that BCOR mutations are not a major cause of X-linked microphthalmia in males. The absence of BCOR mutations in a panel of patients with non-specific laterality defects suggests that mutations in BCOR are not a major cause of isolated heart and laterality defects. Phenotypic analysis of OFCD and Lenz microphthalmia syndromes shows that in addition to the standard diagnostic criteria of congenital cataract, microphthalmia and radiculomegaly, patients should be examined for skeletal defects, particularly radioulnar synostosis, and cardiac/laterality defects.
Highlights
The X-linked microphthalmia syndromes, 11 of which are currently defined (Table 1), comprise a clinically and molecularly diverse group of disorders, a number of which overlap with X-linked mental retardation syndromes
We have focused on the precise clinical features of OFCD and Lenz microphthalmia syndromes, allelic disorders caused by mutation of the BCL-6 corepressor gene (BCOR) gene, as examples of X-linked syndromic microphthalmiaassociated conditions
Given the heterogeneity amongst X-linked microphthalmia syndromes, extension of our knowledge of the mechanism by which BCOR mutation is associated with OFCD and Lenz microphthalmia syndromes may be pertinent to other disorders
Summary
The X-linked microphthalmia syndromes, 11 of which are currently defined (Table 1), comprise a clinically and molecularly diverse group of disorders, a number of which overlap with X-linked mental retardation syndromes. There were numerous extraocular anomalies including mental retardation, palatal and dental anomalies, congenital heart defects, skeletal defects (affecting the fingers and clavicles), unilateral renal aplasia and cryptorchidism;[4] this phenotype substantially overlaps with other X-linked microphthalmia syndromes (Table 1). Another X-linked microphthalmia-associated condition, oculofaciocardiodental (OFCD) syndrome, is characterized by ocular defects (congenital cataracts, microphthalmia), facial anomalies (septate nasal tip, high nasal bridge, midface hypoplasia, palatal anomalies), congenital cardiac defects (atrial/ventricular septal defects, other complex heart defects), dental irregularities (canine radiculomegaly, delayed and persistent dentition, hypodontia) and skeletal anomalies (syndactyly, hammer-type flexion deformities).[5,6,7,8,9,10] All affected individuals are female, with several incidences of mother-daughter transmission
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