Different Serum Enzyme Levels Are Required to Rescue the Various Systemic Features of the Mucopolysaccharidoses

Overview

Journal Hum Gene Ther

Specialties Genetics
Pharmacology

Date 2009 Dec 22

PMID 20021231

Citations 17

Authors

Gabriella Cotugno

Alessandra Tessitore

Anita Capalbo

Patrizia Annunziata

Caterina Strisciuglio

Armida Faella

Michela Aurilio

Maurizio Di Tommaso

Fabio Russo

Antonio Mancini

Elvira De Leonibus

Luigi Aloj

Alberto Auricchio

Affiliations

Soon will be listed here.

Abstract

Mucopolysaccharidoses (MPSs) are lysosomal storage disorders characterized by progressive accumulation of glycosaminoglycans (GAGs) in various tissues. Enzyme replacement therapy (ERT) for several MPSs is available to date. However, the efficacy of ERT is limited, in particular in compartments such as bone, cartilage, the brain, and the eyes. We selected a rodent model of an MPS, with no central nervous system storage, to study the impact, on systemic features of the disease, of various stable levels of exogenous enzymes produced by adeno-associated viral vector (AAV)-mediated liver gene transfer. Low levels (6% of normal) of circulating enzyme were enough to reduce storage and inflammation in the visceral organs and to ameliorate skull abnormalities; intermediate levels (11% of normal) were required to reduce urinary GAG excretion; and high levels (>or=50% of normal) rescued abnormalities of the long bones and motor activity. These data will be instrumental to design appropriate clinical protocols based on either enzyme or gene replacement therapy for MPS and to predict their impact on the pathological features of MPS.

Citing Articles

Failures of Endochondral Ossification in the Mucopolysaccharidoses.

Jiang Z, Byers S, Casal M, Smith L Curr Osteoporos Rep. 2020; 18(6):759-773.

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Effects of gene therapy on cardiovascular symptoms of lysosomal storage diseases.

Poletto E, Pasqualim G, Giugliani R, Matte U, Baldo G Genet Mol Biol. 2019; 42(1 suppl 1):261-285.

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Non-clinical Safety and Efficacy of an AAV2/8 Vector Administered Intravenously for Treatment of Mucopolysaccharidosis Type VI.

Ferla R, Alliegro M, Marteau J, DellAnno M, Nusco E, Pouillot S Mol Ther Methods Clin Dev. 2017; 6:143-158.

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Prolonged Expression of Secreted Enzymes in Dogs After Liver-Directed Delivery of Sleeping Beauty Transposons: Implications for Non-Viral Gene Therapy of Systemic Disease.

Aronovich E, Hyland K, Hall B, Bell J, Olson E, Rusten M Hum Gene Ther. 2017; 28(7):551-564.

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Subcutaneous implantation of microencapsulated cells overexpressing α-L-iduronidase for mucopolysaccharidosis type I treatment.

Lagranha V, Zambiasi Martinelli B, Baldo G, Avila Testa G, Carvalho T, Giugliani R J Mater Sci Mater Med. 2017; 28(3):43.

PMID: 28150116 DOI: 10.1007/s10856-017-5844-4.