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A fourth locus for autosomal dominant hypercholesterolemia maps at 16q22.1
Authors:Alice Marques-Pinheiro  Marie Marduel  Jean-Pierre Rabès  Martine Devillers  Ludovic Villéger  Delphine Allard  Jean Weissenbach  Maryse Guerin  Yassine Zair  Danièle Erlich  Claudine Junien  Arnold Munnich  Michel Krempf  Marianne Abifadel  Jean-Philippe Ja?s  The French Research Network on ADH   Catherine Boileau  Mathilde Varret
Affiliation:Alice Marques-Pinheiro, Marie Marduel, Jean-Pierre Rab??s, Martine Devillers, Ludovic Vill??ger, Delphine Allard, Jean Weissenbach, Maryse Guerin, Yassine Zair, Dani??le Erlich, Claudine Junien, Arnold Munnich, Michel Krempf, Marianne Abifadel, Jean-Philippe Ja?s, The French Research Network on ADH8, Catherine Boileau, Mathilde Varret
Abstract:Autosomal dominant hypercholesterolemia (ADH) is characterized by isolated increase in plasmatic low-density lipoprotein (LDL) cholesterol levels associated with high risk of premature cardiovascular disease. Mutations in LDLR, APOB, and PCSK9 genes have been shown to cause ADH. We now report further genetic heterogeneity of ADH through the study of a large French family in which the involvement of these three genes was excluded. A genome-wide scan mapped the disease-causing gene, named HCHOLA4, at 16q22.1 in a 7.89-Mb interval containing 154 genes with a maximum LOD score of 3.9. To reduce the linked region, we genotyped 18 smaller non-LDLR/non-APOB/non-PCSK9-ADH families at the HCHOLA4 locus. Six families did not exclude linkage to the locus, but none allowed reduction of the disease interval. The 154 regional genes were sorted according to the function of the encoded protein and tissue expression profiles, and 57 genes were analyzed through sequencing of their coding region and close flanking intronic parts. No disease-causing mutation was identified in these families, particularly in the LCAT gene. Finally, our results also show the existence of other ADH genes as nine families were neither linked to LDLR, APOB, and PCSK9 genes nor to the new HCHOLA4 locus.
Keywords:hypercholesterolemia   genetics   mapping   lipoprotein metabolism
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