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A third major locus for autosomal dominant hypercholesterolemia maps to 1p34.1-p32

被引:137
作者
Varret, M
Rabès, JP
Saint-Jore, B
Cenarro, A
Marinoni, JC
Civeira, F
Devillers, M
Krempf, M
Coulon, M
Thiart, R
Kotze, MJ
Schmidt, H
Buzzi, JC
Kostner, GM
Bertolini, S
Pocovi, M
Rosa, A
Farnier, M
Martinez, M
Junien, C
Boileau, C
机构
[1] Univ Paris 05, Hop Necker Enfants Malad, Clin Maurice Lamy, INSERM,U383, F-75743 Paris 15, France
[2] Hop St Louis, INSERM, U358, Paris, France
[3] Ctr Hosp Univ Ambroise Pare, Lab Cent Biochim Hormonol & Genet Mol, Boulogne, France
[4] Ctr Hosp Univ Hotel Dieu, Serv Endocrinol, Nantes, France
[5] Point Med, Dijon, France
[6] Univ Zaragoza, Fac Ciencias, Dept Bioquim & Biol Mol & Celular, E-50009 Zaragoza, Spain
[7] Univ Stellenbosch, Fac Med, Div Human Genet, Med Res Council,Cape Heart Grp, ZA-7505 Tygerberg, South Africa
[8] Graz Univ, Inst Med Biochem, A-8010 Graz, Austria
[9] Univ Genoa, Dept Internal Med, Atherosclerosis Prevent Ctr, I-16126 Genoa, Italy
[10] Univ Nacl Cordoba, Fac Ciencias Quim, Consejo Nacl Invest Cient & Tecn, Ctr Invest Quim Biol Cordoba,Dept Quim Biol, RA-5000 Cordoba, Argentina
来源
AMERICAN JOURNAL OF HUMAN GENETICS | 1999年 / 64卷 / 05期
基金
英国医学研究理事会;
关键词
D O I
10.1086/302370
中图分类号
Q3 [遗传学];
学科分类号
071007 ; 090102 ;
摘要
Autosomal dominant hypercholesterolemia (ADH), one of the most frequent hereditary disorders, is characterized by an isolated elevation of LDL particles that leads to premature mortality from cardiovascular complications. It is generally assumed that mutations in the LDLR and APOB genes account for ADH. We identified one large French pedigree (HC2) and 12 additional white families with ADH in which me excluded linkage to the LDLR and APOB, implicating a new locus we named "FH3." A LOD score of 3.13 at a recombination fraction of 0 was obtained at markers D1S2892 and D1S2722. We localized the FH3 locus to a 9-cM interval at 1p34.1-p32. We tested four regional markers in another set of 12 ADH families. Positive LOD scores were obtained in three pedigrees, whereas linkage was excluded in the others. Heterogeneity tests indicated linkage to FH3 in similar to 27% of these non-LDLR/non-APOB ADH families and implied a fourth locus. Radiation hybrid mapping located four candidate genes at 1p34.1-p32, outside the critical region, showing no identity with FH3. Our results show that ADH is genetically more heterogeneous than conventionally accepted.
引用
收藏
页码:1378 / 1387
页数:10
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