Mechanism of Glycosaminoglycan-Mediated Bone and Joint Disease

Simonaro, Calogera M.; D’Angelo, Marina; He, Xingxing; Eliyahu, Efrat; Shtraizent, Nataly; Haskins, Mark E.; Schuchman, Edward H.

doi:10.2353/ajpath.2008.070564

Cited by 185 publications

(93 citation statements)

References 43 publications

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“…Alterations of several secondary cellular processes have been described as a consequence of the lysosomal accumulation of partially degraded substrates, which trigger different pathologic cascades [54,55].…”

Section: Discussionmentioning

confidence: 99%

Systems biology study of mucopolysaccharidosis using a human metabolic reconstruction network

Salazar

Rodríguez-López

Herreño

et al. 2016

Molecular Genetics and Metabolism

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Section: Discussionmentioning

confidence: 99%

Systems biology study of mucopolysaccharidosis using a human metabolic reconstruction network

Salazar

Rodríguez-López

Herreño

et al. 2016

Molecular Genetics and Metabolism

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“…There may be a clinical effect of ERT by reducing the proinfammatory factors that are induced when excessive KS results in an abnormal structure of extracellular matrix, relieving arthritis and pain in joints, enabling an increase in physical activity, as described in other types of MPS. 62 ERT with native enzyme could also improve hearing, reduce recurrent infection, and reduce airway narrowing (if the storage materials are released from the cartilage of the airway). While ERT with native enzyme may benefit some MPS IVA patients by arresting some aspects of disease progression, the fundamental problems associated with advanced skeletal deformity and laxity of joints are unlikely to be solved by current ERT with native enzyme.…”

Section: Current and Emerging Treatments For Mps Ivamentioning

confidence: 99%

Current and emerging treatments and surgical interventions for Morquio A syndrome: a review

Tomatsu¹,

Mackenzie²,

Theroux³

et al. 2012

RRED

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Patients with mucopolysaccharidosis type IVA (MPS IVA; Morquio A syndrome) have accumulation of the glycosaminoglycans, keratan sulfate, and chondroitin-6-sulfate, in bone and cartilage, causing systemic spondyloepiphyseal dysplasia. Features include lumbar gibbus, pectus carinatum, faring of the rib cage, marked short stature, cervical instability and stenosis, kyphoscoliosis, genu valgum, and laxity of joints. Generally, MPS IVA patients are wheelchair-bound as teenagers and do not survive beyond the second or third decade of life as a result of severe bone dysplasia, causing restrictive lung disease and airway narrowing, increasing potential for pneumonia and apnea; stenosis and instability of the upper cervical region; high risk during anesthesia administration due to narrowed airway as well as thoracoabdominal dysfunction; and surgical complications. Patients often need multiple surgical procedures, including cervical decompression and fusion, hip reconstruction and replacement, and femoral or tibial osteotomy, throughout their lifetime. Current measures to intervene in disease progression are largely palliative, and improved therapies are urgently needed. A clinical trial for enzyme replacement therapy (ERT) and an investigational trial for hematopoietic stem cell transplantation (HSCT) are underway. Whether sufficient enzyme will be delivered effectively to bone, especially cartilage (avascular region) to prevent the devastating skeletal dysplasias remains unclear. This review provides an overview of historical aspects of studies on MPS IVA, including clinical manifestations and pathogenesis of MPS IVA, orthopedic surgical interventions, and anesthetic care. It also describes perspectives on potential ERT, HSCT, and gene therapy.

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“…44 Studies of animal models of mucopolysaccharidosis VI suggest that proinflammatory cytokines alter expression of several matrix metalloproteinases, enzymes involved in ECM degradation. 45 In ML III, a variable fraction of lysosomal glycoproteins still acquires the M6P recognition marker and is correctly routed to, and functional within, lysosomes. It is apparently sufficient to maintain some statural growth and to postpone clinical expression of the abnormal ECM signalling.…”

Section: Phenotypeegenotype Correlationsmentioning

confidence: 99%

Phenotype and genotype in mucolipidoses II and III alpha/beta: a study of 61 probands

Cathey

Leroy

Wood

et al. 2009

Journal of Medical Genetics

130

163

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Objectives Mucolipidoses II and III alpha/beta (ML II and ML III) are lysosomal disorders in which the essential mannose-6-phosphate recognition marker is not synthesized onto lysosomal hydrolases and other glycoproteins. The disorders are caused by mutations in GNPTAB, which encodes two of three subunits of the heterohexameric enzyme, N-acetylglucosamine-1-phosphotransferase. Clinical, biochemical, and molecular findings in 61 probands (63 patients) are presented in order to provide a broad perspective of these mucolipidoses. Methods GNPTAB was sequenced in all probands and/or parents. Activity of several lysosomal enzymes was measured in plasma, and GlcNac-1-phosphotransferase was assayed in leukocytes. Thirty-six patients were studied in detail, allowing extensive clinical data to be abstracted. Results ML II correlates with near total absence of phosphotransferase activity resulting from homozygosity or compound heterozygosity for frameshift or nonsense mutations. Craniofacial and orthopedic manifestations are evident at birth, skeletal findings become more obvious within the first year, and growth is severely impaired. Speech, ambulation, and cognitive function are impaired. ML III retains a low level of phosphotransferase activity due to at least one missense or splice site mutation. The phenotype is milder with minimal delays in milestones, the appearance of facial coarsening by early school age, and slowing of growth after age four years. Conclusions Fifty-one pathogenic changes in GNPTAB are presented, including 42 novel mutations. Ample clinical information improves criteria for delineation of ML II and ML III. Phenotype-genotype correlations suggested in more general terms in earlier reports on smaller groups of patients are specified and extended.

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Mechanism of Glycosaminoglycan-Mediated Bone and Joint Disease

Cited by 185 publications

References 43 publications

Systems biology study of mucopolysaccharidosis using a human metabolic reconstruction network

Systems biology study of mucopolysaccharidosis using a human metabolic reconstruction network

Current and emerging treatments and surgical interventions for Morquio A syndrome: a review

Phenotype and genotype in mucolipidoses II and III alpha/beta: a study of 61 probands

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