Search for the best indicators for the presence of a VPS13B gene mutation and confirmation of diagnostic criteria in a series of 34 patients genotyped for suspected Cohen syndrome.

[cohen syndrome]

Cohen syndrome is a rare autosomal recessive inherited disorder that results from mutations of the VPS 13 B gene . Clinical features consist of a combination of mental retardation , facial dysmorphism , postnatal microcephaly , truncal obesity , slender extremities , joint hyperextensibility , myopia , progressive chorioretinal dystrophy , and intermittent neutropenia .The aim of the study was to determine which of the above clinical features were the best indicators for the presence of VPS 13 B gene mutations in a series of 34 patients with suspected Cohen syndrome referred for molecular analysis of VPS 13 B .14 VPS 13 B gene mutations were identified in 12 patients , and no mutation was found in 22 patients . The presence of chorioretinal dystrophy (92 % vs 32 %, p =0 .0023 ), intermittent neutropenia (92 % vs 5 %, p <0 .001 ), and postnatal microcephaly (100 % vs 48 %, p =0 .0045 ) was significantly higher in the group of patients with a VPS 13 B gene mutation compared to the group of patients without a mutation . All patients with VPS 13 B mutations had chorioretinal dystrophy and /or intermittent neutropenia . The Kolehmainen diagnostic criteria provided 100 % sensibility and 77 % specificity when applied to this series .From this study and a review of more than 160 genotyped cases from the literature , it is concluded that , given the large size of the gene , VPS 13 B screening is not indicated in the absence of chorioretinal dystrophy or neutropenia in patients aged over 5 years . The follow-up of young patients could be a satisfactory alternative unless there are some reproductive issues .