Genetics of familial combined hyperlipidemia and risk of coronary heart disease

doi:10.1093/hmg/ddh069

Human Molecular Genetics Advance Access originally published online on February 5, 2004

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Human Molecular Genetics, 2004, Vol. 13, Review Issue 1 R149-R160
DOI: 10.1093/hmg/ddh069

Genetics of familial combined hyperlipidemia and risk of coronary heart disease

C.C. Shoulders^*, E.L. Jones and R.P. Naoumova

MRC Clinical Sciences Centre, Imperial College London, Hammersmith Hospital, Du Cane Road, London W12 0NN, UK

Coronary heart disease is the leading cause of death in developedcountries. This alarming statistic is partly attributable tolifestyle, and partly due to the genetic factors that make humanshighly susceptible to atherosclerotic vascular disease. Theprincipal metabolic causes of atherosclerosis include hyperlipidemia,hypertension, obesity, insulin resistance and diabetes mellitus.Here we discuss the aetiology of familial combined hyperlipidemia(FCHL), a highly atherogenic disorder affecting 1–2% ofthe Western world. Genome-wide linkage studies indicate thatmore than three genes contribute to the pernicious lipid profileof FCHL, and that these genes reside within the 1q21–23,11p14.1–q12.1 and 16q22–24.1 chromosomal regions.Other loci include 1p31, 6q16.1–16.3 and 8p23.3–22,but the linkage data for these are not yet persuasive. Combinedlinkage and association analyses provide compelling evidencefor the involvement of two distinct alleles at the APOA1/C3/A4/A5gene cluster in the transmission of FCHL. An important lessonarising from the study of a complex genetic disorder, such asFCHL, that lacks a consensus on diagnostic criteria, is thatan understanding of complex genetic disorders can derive fromcomparative analyses of genome-wide linkage data generated fromconditions that share phenotypic overlap. The identificationof potential genetic overlap between FCHL and the MetabolicSyndrome, which is estimated to affect 47 million Americans,promises to deliver new targets for reducing the risk of importantconditions such as cardiovascular disease and stroke.

^* To whom correspondence should be addressed. Tel: +44 2083838308; Fax: +44 2083832028; Email: carol.shoulders{at}csc.mrc.ac.uk

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