Application of Molecular Genetics for Diagnosing Familial Hypercholesterolemia in Norway: Results from a Family-Based Screening Program

Trond P. Leren; Turid Manshaus; Unn Skovholt; Tove Skodje; Inger Esther Nossen; Christél Teie; Stine Sørensen; Kari Solberg Bakken

doi:10.1055/s-2004-822989

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Semin Vasc Med 2004; 4(1): 75-85
DOI: 10.1055/s-2004-822989

Application of Molecular Genetics for Diagnosing Familial Hypercholesterolemia in Norway: Results from a Family-Based Screening Program

Trond P. Leren¹ , Turid Manshaus¹ , Unn Skovholt¹ , Tove Skodje¹ , Inger Esther Nossen¹ , Christél Teie¹ , Stine Sørensen¹ , Kari Solberg Bakken¹

¹Medical Genetics Laboratory, Department of Medical Genetics, Rikshospitalet, Oslo, Norway

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Publication Date:
22 March 2004 (online)

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A total of 119 different mutations in the low-density lipoprotein-receptor gene have so far been found to cause familial hypercholesterolemia (FH) among Norwegian patients. As of April 2003, 2390 patients from 959 unrelated families were provided with a molecular genetic diagnosis. Of these, 25.3% had xanthomas and 8.4% had xanthelasma. During the last 2-3 years, a systematic family-based program to identify close relatives of FH patients has been established. A total of 851 relatives of 188 index patients have undergone genetic testing. Four hundred seven people (47.9%) were affected, and 444 (52.1%) were unaffected. Only 41.5% of those affected were on lipid-lowering drugs, and only 6.1% had a value for total serum cholesterol below 193 mg/dL (5.0 mmol/L). A follow-up study was conducted in 146 of 407 affected relatives 6 months after genetic testing was performed. Of those already under treatment at the time of genetic testing, nonsignificant reductions of total serum cholesterol and low-density lipoprotein cholesterol of 3.2% and 7.1% were observed. Of those not under treatment who were aged 18 years and older, the corresponding reductions were 21.2% (p < .0001) and 30.0% (p < .0001), respectively. We conclude that molecular genetic methods represent a feasible and highly efficient tool in a family-based strategy to diagnose FH.

KEYWORDS

familial hypercholesterolemia - genetics - low-density lipoprotein-receptor - mutation

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Trond P Leren M.D. Ph.D.

Medical Genetics Laboratory, Department of Medical Genetics

Rikshospitalet, N-0027 Oslo, Norway

Email: trond.leren@rikshospitalet.no

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