Aldo Mari

22q11 deletions in isolated and syndromic patients with tetralogy of Fallot

Tetralogy of Fallot (TF) is a congenital conotruncal heart defect commonly found in DiGeorge (DGS) and velo-cardio-facial (VCFS) syndromes. The deletion of chromosome 22q11 (de122q11) is a well established cause of DGS and VCFS, and it has been demonstrated also in sporadic or familial cases of TF. In order to investigate the prevalence of de122q11 in patients with TF, we analyzed the DNA of 137 consecutive patients with syndromic and isolated TF, using the HD7k probe, which detects hemizygosity for the D22S134 locus. De122q11 has been detected in 11/26 (42%) syndromic patients. Evidence for hemizygosity was obtained in all patients with DGS and in 8/15 patients with VCFS. None of the 107 patients with isolated TF had de122q11. Our experience suggests that children with TF and de122q11 always present major or minor extracardiac anomalies. These features, including subtle facial dysmorphisms, should be checked routinely in patients with TF and other conotruncal heart defects.

Detection of an atypical 7q11.23 deletion in Williams syndrome patients which does not include the STX1A and FZD3 genes

We present two patients with the full Williams syndrome (WS) phenotype carrying a smaller deletion than typically observed. The deleted region spans from the elastin gene to marker D7S1870. This observation narrows the minimal region of deletion in WS and suggests that the syntaxin 1A and frizzled genes are not responsible for the major features of this developmental disorder and provides important insight into understanding the genotype-phenotype correlation in WS.

Analysis of the elastin gene in 60 patients with clinical diagnosis of Williams syndrome

Williams syndrome (WS) is caused by deletion of the elastin (ELN) gene. We have analyzed an intragenic restriction fragment length polymorphism (RFLP) and the gene dosage of ELN using a new probe (FP4) in a series of 60 sporadic patients with a clinical diagnosis of WS. Deletion of the ELN gene was shown in 54 cases, while clinical revaluation of the 6 patients without the deletion did not confirm the diagnosis of WS. These results support the genetic homogeneity of WS, and the high accuracy of ELN molecular analysis, which can be confidenty used for providing genetic counselling to WS families.

A highly polymorphic CA/GT repeat (LIMK1GT) within the Williams syndrome critical region

Candidate gene: Williams syndrome (WS; MIM* 194050) is a developmental disorder characterized by mental and statural deficiency, elfin face, supravalvular aortic stenosis (SVAS) and peripheral pulmonary arterial stenosis, and infantile hypercalcemia (1, 2). Inherited and de nouo deletions of genes mapping in the 7q11.23 region, are responsible for the pathogenesis of this disorder (36). Hemizygosity of the elastin (ELN) and LIM-kinasel (LIMKl) genes, which map in the commonly deleted region, account for vascular, connective and visuospatial constructive cognition abnormalities observed in WS (3, 4). The availability of microsatellite DNA markers at these loci, is thkefore of great importance for diagnosis, genetic counselling and genotype-phenotype studies.