Mol Ther. 2009 Jun;17(6):954-63. Epub 2009 Mar 10.

Glycoengineered acid alpha-glucosidase with improved efficacy at correcting the metabolic aberrations and motor function deficits in a mouse model of Pompe disease.

Zhu Y, Jiang JL, Gumlaw NK, Zhang J, Bercury SD, Ziegler RJ, Lee K, Kudo M, Canfield WM, Edmunds T, Jiang C, Mattaliano RJ, Cheng SH.

Source

Genzyme Corporation, Framingham, Massachusetts 01701-9322, USA. yunxiang.zhu@genzyme.com

Abstract

Improving the delivery of therapeutics to disease-affected tissues can increase their efficacy and safety. Here, we show that chemical conjugation of a synthetic oligosaccharide harboring mannose 6-phosphate (M6P) residues onto recombinant human acid alpha-glucosidase (rhGAA) via oxime chemistry significantly improved its affinity for the cation-independent mannose 6-phosphate receptor (CI-MPR) and subsequent uptake by muscle cells. Administration of the carbohydrate-remodeled enzyme (oxime-neo-rhGAA) into Pompe mice resulted in an approximately fivefold higher clearance of lysosomal glycogen in muscles when compared to the unmodified counterpart. Importantly, treatment of immunotolerized Pompe mice with oxime-neo-rhGAA translated to greater improvements in muscle function and strength. Treating older, symptomatic Pompe mice also reduced tissue glycogen levels but provided only modest improvements in motor function. Examination of the muscle pathology suggested that the poor response in the older animals might have been due to a reduced regenerative capacity of the skeletal muscles. These findings lend support to early therapeutic intervention with a targeted enzyme as important considerations in the management of Pompe disease.

PMID:: 19277015; [PubMed - indexed for MEDLINE]
PMCID:: PMC2835178

Free PMC Article

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Figure 2

Biochemical characteristics of the unmodified and glycoengineered enzymes. (a) Chromatography of oxime-neo-rhGAA (open circle) and rhGAA (closed circle) over a CI-MPR column. Approximately 5 µg of the different enzymes were loaded onto a 2 ml column. After washing the column with binding buffer, the bound material was eluted (starting at fraction 11) with binding buffer containing 5 mmol/l M6P. Fractions (2 ml) were collected and assayed for GAA activity. (b) Uptake of the enzymes by L6 myoblasts in culture. Increasing amounts of either oxime-neo-rhGAA (open circle) or rhGAA (closed circle) were added to L6 myoblasts and incubated at 37 °C for 18 hours. After washing, the cells were lysed and the enzyme activity in the lysates assayed using the fluorogenic substrate, 4-methylumbelliferyl-α-D-glucopyranoside. Enzyme activity was expressed in relative units (RU). (c) Stability of oxime-neo-rhGAA at 4 °C (open square) and 25 °C (closed triangle). The modified enzyme was incubated at the respective temperatures for the times indicated after which they were subjected to analysis to determine the level of M6P. CI-MPR, cation-independent mannose 6-phosphate receptor; GAA, acid α-glucosidase; M6P, mannose 6-phosphate; rhGAA, recombinant human acid α-glucosidase.

Glycoengineered Acid α-Glucosidase With Improved Efficacy at Correcting the Metabolic Aberrations and Motor Function Deficits in a Mouse Model of Pompe Disease