Simpson Michael A, Cross Harold, Proukakis Christos, Pryde Anna, Hershberger Ruth, Chatonnet Arnaud, Patton Michael A, Crosby Andrew H
Department of Medical Genetics, St. George's Hospital Medical School, University of London, London, United Kingdom.
Am J Hum Genet. 2003 Nov;73(5):1147-56. doi: 10.1086/379522. Epub 2003 Oct 16.
Mast syndrome is an autosomal recessive, complicated form of hereditary spastic paraplegia with dementia that is present at high frequency among the Old Order Amish. Subtle childhood abnormalities may be present, but the main features develop in early adulthood. The disease is slowly progressive, and cerebellar and extrapyramidal signs are also found in patients with advanced disease. Patients have a thin corpus callosum and white-matter abnormalities, as seen on magnetic resonance imaging. Using an extensive Amish pedigree, we have mapped the Mast syndrome locus (SPG21) to a small interval of chromosome 15q22.31 that encompasses just three genes. Sequence analysis of the three transcripts revealed that all 14 affected cases were homozygous for a single base-pair insertion (601insA) in the acid-cluster protein of 33 kDa (ACP33) gene. This frameshift results in the premature termination (fs201-212X213) of the encoded product, which is designated "maspardin" (Mast syndrome, spastic paraplegia, autosomal recessive with dementia), and has been shown elsewhere to localize to intracellular endosomal/trans-Golgi transportation vesicles and may function in protein transport and sorting.
马斯特综合征是一种常染色体隐性遗传的、伴有痴呆的复杂型遗传性痉挛性截瘫,在旧秩序阿米什人群中高发。儿童期可能存在细微异常,但主要特征在成年早期出现。该疾病进展缓慢,晚期患者还会出现小脑和锥体外系体征。磁共振成像显示,患者胼胝体薄且存在白质异常。利用一个庞大的阿米什家系,我们已将马斯特综合征基因座(SPG21)定位到15号染色体q22.31的一个小区域,该区域仅包含三个基因。对这三个转录本的序列分析显示,所有14例受累病例在33 kDa酸性簇蛋白(ACP33)基因中均为单个碱基对插入(601insA)的纯合子。这种移码导致编码产物过早终止(fs201 - 212X213),该产物被命名为“马帕丁”(马斯特综合征、痉挛性截瘫、常染色体隐性遗传伴痴呆),在其他地方已表明其定位于细胞内的内体/反式高尔基体运输小泡,可能在蛋白质运输和分选过程中发挥作用。
