Abstract

Heterozygous familial hypercholesterolaemia (FH) is a common inborn error of lipoprotein metabolism, which strongly predisposes for coronary artery disease and premature cardiac death. 1 In 1994, a family based active identification programme for FH was implemented in the Netherlands. It is based on DNA diagnosis of the LDL-receptor gene mutation, which enables us to search selectively for patients in a high risk population. The programme initially targets first and second degree relatives of FH probands (diagnosed at Lipid Research Clinics throughout the country) and extends further into the family only when new patients are identified. The programme aims to identify mutation carriers and to refer them to Lipid Research Clinics for extensive individual risk assessment and, if necessary, treatment. As no carefully collected data are available for cholesterol levels among the general population of LDL-receptor gene mutation carriers, the large majority of whom are asymptomatic, we studied the prevalence of hypercholesterolaemia among screenees with a proved LDLreceptor gene mutation.