Riant Florence, De Fusco Maurizio, Aridon Paolo, Ducros Anne, Ploton Claire, Marchelli Florence, Maciazek Jacqueline, Bousser Marie Germaine, Casari Giorgio, Tournier-Lasserve Elisabeth
Laboratoire de Génétique Moléculaire, Hôpital Lariboisière AP-HP, Paris, France.
Hum Mutat. 2005 Sep;26(3):281. doi: 10.1002/humu.9361.
Familial hemiplegic migraine (FHM) is an autosomal dominant form of migraine with aura. The disease is caused by mutations of at least three genes among which two have been identified, CACNA1A and ATP1A2. Very few mutations have been identified so far in ATP1A2. We screened the coding sequence of ATP1A2 in 26 unrelated FHM probands in whom CACNA1A screening was negative. A total of eight different mutations were identified in 11 of the probands (41%), including six missense mutations, one small deletion leading to a frameshift, and one in frame deletion. All were novel mutations. Two mutations were recurrent, in three and two families, respectively. Genotyping of 94 relatives of these 11 probands identified 47 mutation carriers, among whom 36 were clinically affected. Sequencing of all 23 exons in an ethnically matched panel detected only one exonic coding polymorphism.
家族性偏瘫性偏头痛(FHM)是一种常染色体显性遗传的伴先兆偏头痛。该疾病由至少三个基因的突变引起,其中两个已被鉴定出来,即CACNA1A和ATP1A2。到目前为止,在ATP1A2中仅鉴定出极少数突变。我们对26名无血缘关系的FHM先证者的ATP1A2编码序列进行了筛查,这些先证者的CACNA1A筛查结果为阴性。在11名先证者(41%)中总共鉴定出8种不同的突变,包括6种错义突变、1种导致移码的小缺失和1种框内缺失。所有均为新突变。有两种突变分别在三个和两个家族中出现。对这11名先证者的94名亲属进行基因分型,确定了47名突变携带者,其中36名有临床症状。在一个种族匹配的样本中对所有23个外显子进行测序,仅检测到一个外显子编码多态性。
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