| Literature DB >> 7493033 |
N H Robin1, G J Feldman, A L Aronson, H F Mitchell, R Weksberg, C O Leonard, B K Burton, K D Josephson, R Laxová, K A Aleck, J E Allanson, M L Guion-Almeida, R A Martin, L G Leichtman, R A Price, J M Opitz, M Muenke.
Abstract
Opitz syndrome (OS, McKusick 145410) is a well described genetic syndrome affecting multiple organ systems whose cardinal manifestations include widely spaced eyes and hypospadias (Fig. 1). It was first reported as two separate entities, BBB syndrome, and G syndrome. However, subsequent reports of families in which the BBB and G syndrome segregated within a single kindred suggested that they were a single clinical entity. Although the original pedigrees were consistent with X-linked and autosomal dominant inheritance, male-to-male transmission in subsequent reports suggested that OS was inherited as an autosomal dominant trait. Here we report that OS is a heterogeneous disorder, with an X-linked and an autosomal locus. Three families were linked to DXS987 in Xp22, with a lod score of 3.53 at zero recombination. Five families were linked to D22S345 from chromosome 22q11.2, with a lod score of 3.53 at zero recombination. This represents the first classic multiple congenital anomaly syndrome with an X-linked and an autosomal form.Entities:
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Year: 1995 PMID: 7493033 DOI: 10.1038/ng1295-459
Source DB: PubMed Journal: Nat Genet ISSN: 1061-4036 Impact factor: 38.330