Jin W D, Jackson C E, Desnick R J, Schuchman E H
Division of Medical and Molecular Genetics, Mount Sinai School of Medicine, New York, NY 10029.
Am J Hum Genet. 1992 Apr;50(4):795-800.
Mucopolysaccharidosis type VI (MPS VI; Maroteaux-Lamy disease) results from the deficient activity of the lysosomal enzyme, arylsulfatase B (ASB; N-acetylgalactosamine-4-sulfatase E.C.3.1.6.1). The enzymatic defect leads to the accumulation of the glycosaminoglycan, dermatan sulfate, primarily in connective tissue and reticuloendothelial cell lysosomes. Although MPS VI patients have normal intelligence and no neurologic abnormalities, the disease is clinically heterogeneous: severely affected individuals expire in childhood or early adolescence while those with the mild or intermediate phenotypes have a slower, milder disease course and a longer life span. The recent isolation of the full-length cDNA-encoding human ASB permitted an investigation of the molecular lesions underlying the phenotypic heterogeneity in MPS VI. The ASB cDNA-coding sequences were determined from two unrelated MPS VI patients with the severe (proband 1) and mild (proband 2) phenotypes. These patients had about 2% and 7% of normal ASB activity in cultured fibroblasts, respectively. Proband 1 was homoallelic for a T-to-C transition in nucleotide (nt) 349, which predicted a cysteine-to-arginine substitution in the ASB polypeptide at residue 117 (C117R). Proband 2 was heteroallelic, having a T-to-C transition in nt 707, which predicted a leucine-to-proline replacement at ASB residue 236 (L236P), and having a G-to-A transition in nt 1214, which predicted a cysteine-to-tyrosine substitution at ASB residue 405 (C405Y). These mutations did not occur in three other unrelated MPS VI patients or in 120 ASB alleles from normal individuals, indicating that they were not polymorphisms. The identification of these three ASB mutations documents the first evidence of molecular heterogeneity in MPS VI and provides an initial basis for genotype/phenotype correlations in this lysosomal storage disease.
VI型黏多糖贮积症(MPS VI;马罗-拉米病)是由于溶酶体酶芳基硫酸酯酶B(ASB;N-乙酰半乳糖胺-4-硫酸酯酶,E.C.3.1.6.1)活性缺乏所致。这种酶缺陷导致糖胺聚糖硫酸皮肤素主要在结缔组织和网状内皮细胞溶酶体中蓄积。尽管MPS VI患者智力正常且无神经学异常,但该疾病在临床上具有异质性:严重受累个体在儿童期或青春期早期死亡,而具有轻度或中度表型的患者病程较慢、病情较轻且寿命较长。最近全长编码人ASB的cDNA的分离使得对MPS VI表型异质性潜在分子病变的研究成为可能。从两名具有严重(先证者1)和轻度(先证者2)表型的无关MPS VI患者中确定了ASB cDNA编码序列。这些患者培养的成纤维细胞中ASB活性分别约为正常活性的2%和7%。先证者1在核苷酸(nt)349处发生了T到C的转换,为纯合等位基因,这预测在ASB多肽第117位残基处半胱氨酸被精氨酸替代(C117R)。先证者2为杂合等位基因,在nt 707处发生了T到C的转换,这预测在ASB第236位残基处亮氨酸被脯氨酸替代(L236P),并且在nt 1214处发生了G到A的转换,这预测在ASB第405位残基处半胱氨酸被酪氨酸替代(C405Y)。这三个突变在其他三名无关的MPS VI患者或120个正常个体的ASB等位基因中均未出现,表明它们不是多态性。这三个ASB突变的鉴定记录了MPS VI分子异质性的首个证据,并为这种溶酶体贮积病的基因型/表型相关性提供了初步基础。
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