Familial hypercholesterolemia (FH) has a prevalence of 1 in 500 in Western society
and predisposes for premature cardiovascular disease. Lipid-lowering treatment of
affected individuals is widely advocated. Maximum health benefit can be obtained in
FH if treatment is started as early as possible, as the World Health Organization
has recently recommended. In 1994 we initiated an active case-finding program for
individuals with FH, based on family investigation and DNA-testing. In an initial
pilot study we established that active family screening supported by DNA diagnostics
resulted in the identification of substantial numbers of FH heterozygotes and determined
that diagnosis by DNA analysis was superior to conventional cholesterol measurement.
Since its initiation, the program has led to the identification of more than 6000
individuals with FH, of whom the greatest part was not adequately treated at the time
of identification. Our findings indicate not only that this case-finding approach
is effective in identifying FH patients who otherwise would not have been identified
but also that the vast majority of these patients seek treatment and are successfully
started on cholesterol-lowering therapy to reduce their risk of premature cardiovascular
disease. Here we describe an effective model to identify and bring under treatment
large numbers of individuals affected by FH.
KEYWORDS
Familial hypercholesterolemia - cardiovascular disease - prevention - case-finding
- genetic testing
REFERENCES
- 1 Familial Hypercholesterolaemia: report of a WHO consultation. World Health Organization,
Human Genetics Programme, Division of Noncommunicable Diseases. WHO/HGN/FH/CONS/98.7.
Paris, October 1997
- 2
Scandinavian Simvastatin Survival Study Group .
Randomised trial of cholesterol lowering in 4444 patients with coronary heart disease:
the Scandinavian Simvastatin Survival Study (4S).
Lancet.
1994;
344
1383-1389
- 3
Shepherd J, Cobbe S, Ford I et al..
Prevention of coronary heart disease with pravastatin in men with hypercholesterolemia
(WOSCOPS).
N Engl J Med.
1995;
333
1301-1307
- 4
Sacks F M, Pfeffer M A, Moye L A et al..
The effect of pravastatin on coronary events in patients with average cholesterol
levels (CARE).
N Engl J Med.
1996;
335
1001-1009
- 5
Downs J R, Clearfield M, Weis S et al..
Primary prevention of acute coronary events with lovastatin in men and women with
average cholesterol levels (AFCAPS/TexCAPS).
JAMA.
1998;
279
1615-1622
- 6
The Long-Term Intervention with Pravastatin in Ischemic Disease (LIPID) Study Group
.
Prevention of cardiovascular events and death with pravastatin in patients with coronary
heart disease and a broad range of initial cholesterol levels.
N Eng J Med.
1998;
339
1349-1357
- 7
Vogt T M.
Risk assessment and health hazard appraisal.
Annu Rev Public Health.
1981;
2
31-47
- 8 Goldstein J L, Hobbs H H, Brown M S. Familial hypercholesterolemia. In: Scriver
CR, Beaudet AL, Sly WS, Valle D The Metabolic Basis of Inherited Disease. New York;
McGraw-Hill 2001: 2863-2913
- 9
Hill J S, Hayden M R, Frohlich J et al..
Genetic and environmental factors affecting the incidence of coronary artery disease
in heterozygous familial hypercholesterolemia.
Arterioscler Thromb.
1991;
11
290-297
- 10
Scientific Steering Committee on behalf of the Simon Broome Register Group .
Mortality in treated heterozygous familial hypercholesterolemia: implications for
clinical management.
Atherosclerosis.
1999;
142
105-115
- 11 Defesche J C. Familial hypercholesterolaemia. In: Betteridge DJ Lipids and Vascular
Disease. London; Martin Dunitz Ltd 2000: 65-76
- 12
Smilde T H, Van Wissen S, Wollersheim H, Trip M D, Kastelein J JP, Stalenhoef A FH.
Effect of aggressive versus conventional lipid lowering on atherosclerosis progression
in familial hypercholesterolemia (ASAP): a prospective, randomised, double-blind trial.
Lancet.
2001;
357
577-581
- 13
Lansberg P J, Tuzgöl S, Van de Ree M A, Defesche J C, Kastelein J J.
The prevalence of familial hypercholesterolemia among adults in general practice is
higher than expected [in Dutch].
Ned Tijdschr Geneeskd.
2000;
144
1437-1440
- 14
Fouchier S W, Defesche J C, Umans-Eckenhausen M AW, Kastelein J JP.
The molecular basis of familial hypercholesterolemia in the Netherlands.
Hum Genet.
2001;
109
602-615
- 15
Umans-Eckenhausen M AW, Defesche J C, Sijbrands E JG, Scheerder R LJM, Kastelein J JP.
Review of the first 5 years of screening for familial hypercholesteroleamia in the
Netherlands.
Lancet.
2001;
357
165-168
- 16
Nijbroek G, Sood S, McIntosh I et al..
Fifteen novel FBN1 mutations causing Marfan syndrome detected by heteroduplex analysis
of genome amplicons.
Am J Hum Genet.
1995;
57
8-21
- 17
Bridges A B, Fead M, Boxer M, Gray J R, Bundy C, Murray A.
Marfan syndrome in a large family: response of family members to a screening program.
J Med Genet.
1992;
29
81-85
- 18
Wonderling D, Umans-Eckenhausen M AW, Marks D, Defesche J C, Kastelein J JP, Thorogood M.
A cost-effectiveness analysis of the genetic screening programme for familial hypercholesterolemia
in The Netherlands.
Semin Vasc Med.
2004;
4
97-104
- 19
Tonstad S, Nøvik T C, Vandvik I H.
Psychosocial function during treatment for familial hypercholesterolemia.
Pediatrics.
1996;
98
249-255
- 20
Umans-Eckenhausen M A, Oort F J, Ferenschild K C, Defesche J C, Kastelein J J, de
Haes J C.
Parental attitude towards genetic testing for familial hypercholesterolemia in children.
J Med Genet.
2002;
39
e49
- 21
De Jongh S, Kerckhoffs M C, Grootenhuis M A et al..
The influence of statin therapy on quality of life, anxiety and concerns in children
with familial hypercholesterolemia and their parents.
Acta Paediatr.
2003;
92
1096-1101
Dr.
J.C. Defesche
Dept. Vascular Medicine, Academic Medical Center
Rm. G1-112B, P.O. Box 22 660
NL-1100 DD Amsterdam, The Netherlands
Email: j.defesche@amc.uva.nl
