• congenital heart defects
• Noonan syndrome
• LEOPARD syndrome
• PTPN11

• CFCS, cardio-facio-cutaneous syndrome
• LEOPARD, multiple lentigines, ECG conduction abnormalities, ocular hypertelorism, pulmonary stenosis, abnormal genitalia, retardation of growth and sensorineural deafness
• ML/LS, multiple lentigines/LEOPARD syndrome
• SSCP, single strand conformation polymorphism

Noonan syndrome (MIM 163950), an autosomal dominant disorder with an estimated prevalence of 1/1000–2500 at birth, is characterised by short stature, facial anomalies, pterygium colli, and congenital heart disease.^1,2 Although pulmonary valve stenosis with dysplastic leaflets, hypertrophic cardiomyopathy, and atrial septal defects (ASD) are the most common congenital heart defects in Noonan syndrome,³ a broad spectrum of cardiac phenotypes has been recognised.^2–6 About half the affected individuals have PTPN11 gene mutations.^7–9 This gene, which maps to chromosome 12q22-qter,¹⁰ encodes for the human SH2 domain containing protein tyrosine phosphatase (SHP2).¹¹PTPN11 gene mutations have also been detected in multiple lentigines/LEOPARD syndrome (multiple lentigines, ECG conduction abnormalities, ocular hypertelorism, pulmonary stenosis, abnormal genitalia, retardation of growth and sensorineural deafness; ML/LS, MIM 151100),^12,13 in Noonan-like/multiple giant cell lesion syndrome (MIM 163955),⁸ in two families presumably affected by cardio-facio-cutaneous syndrome (CFCS, MIM 115150),¹⁴ but not in sporadic CFCS.¹⁵ The clinical and genetic heterogeneity of these disorders suggests a possible relation between different PTPN11 gene mutations and distinct clinical features. A genotype–phenotype correlation study in Noonan syndrome found an association between pulmonary stenosis and PTPN11 mutations.⁸ Our aim in this study was to screen a large cohort of patients with Noonan syndrome and ML/LS in order to expand the genotype–phenotype correlation analysis, with particular emphasis on cardiac diseases.