is a rare disorder characterized by mental and physical retardation, typical facies, and short and broad thumbs and halluces (1)
a reported incidence of 1 in 125 000 people
also cardiac, neurologic, ocular, and skeletal abnormalities may occur
aetiology of RTS has recently been clarified
previously this disorder was previously believed to be inherited as X-linked with heterozygous females being more mildly affected (2,3)
an autosomal dominant mutation is now believed to be the most probable cause of RTS
in studies, many RTS patients have been shown to have molecular mutations or microdeletions of chromosome 16p13.3. This region contains the gene for the human cAMP response element binding (CREB) protein (CBP)
CBP is an important regulatory protein within the cell and interacts with a myriad of other such proteins
however this mutation or microdeletion is only found in a minority of RTS cases (4-25%) (1)
except for rare cases, no phenotype-genotype correlation between RTS patients with or without deletion was detected and therefore normal fluorescent in situ hybridization (FISH) results, do not exclude the diagnosis of RTS (1)
in a study by Wallerstein et al (4), growth retardation, nevus flammeus, coloboma, and hypotonia were found to have positive predictive value for the presence of deletion
Wallerstein R, Anderson CE, Hay B, et al. Submicroscopic deletions at 16p13.3 in Rubinstein-Taybi syndrome: frequency and clinical manifestations in a North American population. J Med Genet 1997;34: 203-206.
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