Taylor Matthew R G, Ku Lisa, Slavov Dobromir, Cavanaugh Jean, Boucek Mark, Zhu Xiao, Graw Sharon, Carniel Elisa, Barnes Carl, Quan Dianna, Prall Ryan, Lovell Mark A, Mierau Gary, Ruegg Patsy, Mandava Naresh, Bristow Michael R, Towbin Jeffrey A, Mestroni Luisa
University of Colorado at Denver and Health Sciences Center, Aurora, CO, USA.
, 12635 East Montview Blvd. Suite 100, Aurora, CO, 80045, USA.
J Hum Genet. 2007;52(10):830-835. doi: 10.1007/s10038-007-0184-8.
X-linked dilated cardiomyopathy (XLCM) was first described in 1987 and associated with dystrophin gene (DMD) mutations a decade later in one of the original two families. Here we report long-term follow-up of the second family (XLCM-2), for which a DMD mutation was never found. Analysis of the lysosome-associated membrane protein-2 (LAMP-2) gene detected a novel mutation, confirming a diagnosis of Danon disease. The broad phenotype in this family included dilated and hypertrophic cardiomyopathy, cardiac pre-excitation, skeletal myopathy with high serum creatinine kinase, cognitive impairement (in males), and and a pigmentary retinopathy in affected females. Cardiac biopsy in a 13-month-old mutation-carrying male showed no vacuolization by standard histology. We conclude that XLCM may be the presenting sign of Danon disease and, in the presence of familial history of HCM, pre-excitation, skeletal muscle involvement and retinal pigmentary dystrophy should prompt LAMP-2 clinical testing. Furthermore, the absence of vacuolar myopathy in biopsies from young patients may not exclude Danon disease.
X连锁扩张型心肌病(XLCM)于1987年首次被描述,十年后在最初的两个家族之一中发现其与肌营养不良蛋白基因(DMD)突变有关。本文报告了第二个家族(XLCM-2)的长期随访情况,在该家族中从未发现DMD突变。对溶酶体相关膜蛋白2(LAMP-2)基因的分析检测到一个新的突变,从而确诊为丹农病。该家族的广泛表型包括扩张型和肥厚型心肌病、心脏预激、血清肌酸激酶升高的骨骼肌病、(男性)认知障碍以及受影响女性的色素性视网膜病变。一名携带突变的13个月大男性的心脏活检通过标准组织学检查未显示空泡形成。我们得出结论,XLCM可能是丹农病的首发症状,在存在肥厚型心肌病家族史、预激、骨骼肌受累和视网膜色素性营养不良的情况下,应促使进行LAMP-2临床检测。此外,年轻患者活检中无空泡性肌病可能不排除丹农病。
