Enzyme replacement therapy in a feline model of Maroteaux-Lamy syndrome

Allison C. Crawley; Doug A. Brooks; Vivienne J. Muller; Birgit A. Petersen; Elizabeth L. Isaac; Julie Bielicki; Barbara M. King; Christine D. Boulter; Alison J. Moore; Nick L. Fazzalari; Don S. Anson; Sharon Byers; John J. Hopwood

doi:10.1172/JCI118617

Enzyme replacement therapy in a feline model of Maroteaux-Lamy syndrome

Allison C. Crawley, Doug A. Brooks, Vivienne J. Muller, Birgit A. Petersen, Elizabeth L. Isaac, Julie Bielicki, Barbara M. King, Christine D. Boulter, Alison J. Moore, Nick L. Fazzalari, Don S. Anson, Sharon Byers, John J. Hopwood

Hopwood Centre For Neurobiology

Research output: Contribution to journal › Article › peer-review

124 Citations (Scopus)

Abstract

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 ~ 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.

Original language	English
Pages (from-to)	1864-1873
Number of pages	10
Journal	Journal of Clinical Investigation
Volume	97
Issue number	8
DOIs	https://doi.org/10.1172/JCI118617
Publication status	Published or Issued - 15 Apr 1996

Keywords

disease models, animal
dysostoses
genetics, medical
lysosomal storage diseases
mucopolysaccharidosis VI

ASJC Scopus subject areas

General Medicine

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10.1172/JCI118617

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title = "Enzyme replacement therapy in a feline model of Maroteaux-Lamy syndrome",

abstract = "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 ~ 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.",

keywords = "disease models, animal, dysostoses, genetics, medical, lysosomal storage diseases, mucopolysaccharidosis VI",

author = "Crawley, {Allison C.} and Brooks, {Doug A.} and Muller, {Vivienne J.} and Petersen, {Birgit A.} and Isaac, {Elizabeth L.} and Julie Bielicki and King, {Barbara M.} and Boulter, {Christine D.} and Moore, {Alison J.} and Fazzalari, {Nick L.} and Anson, {Don S.} and Sharon Byers and Hopwood, {John J.}",

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AU - Crawley, Allison C.

AU - Brooks, Doug A.

AU - Muller, Vivienne J.

AU - Petersen, Birgit A.

AU - Isaac, Elizabeth L.

AU - Bielicki, Julie

AU - King, Barbara M.

AU - Boulter, Christine D.

AU - Moore, Alison J.

AU - Fazzalari, Nick L.

AU - Anson, Don S.

AU - Byers, Sharon

AU - Hopwood, John J.

PY - 1996/4/15

Y1 - 1996/4/15

N2 - 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 ~ 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.

AB - 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 ~ 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.

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KW - lysosomal storage diseases

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Enzyme replacement therapy in a feline model of Maroteaux-Lamy syndrome

Abstract

Keywords

ASJC Scopus subject areas

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