Crawley A C, Brooks D A, Muller V J, Petersen B A, Isaac E L, Bielicki J, King B M, Boulter C D, Moore A J, Fazzalari N L, Anson D S, Byers S, Hopwood J J
Department of Chemical Pathology, Women's and Children's Hospital, North Adelaide, Australia.
J Clin Invest. 1996 Apr 15;97(8):1864-73. doi: 10.1172/JCI118617.
We report studies that suggest enzyme replacement therapy will result in a significant reduction in disease progression and tissue pathology in patients with Maroteaux-Lamy syndrome (Mucopolysaccharidosis type VI, MPS VI). A feline model for MPS VI was used to evaluate tissue distribution and clinical efficacy of three forms of recombinant human N-acetylgalactosamine-4-sulfatase (rh4S, EC 3.1.6.1). Intravenously administered rh4S was rapidly cleared from circulation. The majority of rh4S was distributed to liver, but was also detected in most other tissues. Tissue half-life was approximately 2-4 d. Three MPS VI cats given regular intravenous infusions of rh4S for up to 20 mo showed variable reduction of storage vacuoles in Kupffer cells and connective tissues, however cartilage chondrocytes remained vacuolated. Vertebral bone mineral volume was improved in two MPS VI cats in which therapy was initiated before skeletal maturity, and increased bone volume appeared to correlate with earlier age of onset of therapy. One cat showed greater mobility in response to therapy.
我们报告的研究表明,酶替代疗法将显著降低马罗-拉米综合征(黏多糖贮积症VI型,MPS VI)患者的疾病进展和组织病理学变化。使用MPS VI的猫模型来评估三种形式的重组人N-乙酰半乳糖胺-4-硫酸酯酶(rh4S,EC 3.1.6.1)的组织分布和临床疗效。静脉注射的rh4S迅速从循环中清除。大部分rh4S分布到肝脏,但在大多数其他组织中也可检测到。组织半衰期约为2-4天。三只MPS VI猫接受长达20个月的rh4S定期静脉输注,库普弗细胞和结缔组织中的储存空泡有不同程度的减少,然而软骨软骨细胞仍有空泡。在两只骨骼成熟前开始治疗的MPS VI猫中,椎体骨矿物质含量有所改善,骨体积增加似乎与治疗开始的年龄较早有关。一只猫在接受治疗后活动能力增强。
