Upregulation of elastase proteins results in aortic dilatation in mucopolysaccharidosis I mice

Ma, Xiucui; Tittiger, Mindy; Knutsen, Russell H.; Kovács, Attila; Schaller, Laura; Mecham, Robert P.; Ponder, Katherine P.

doi:10.1016/j.ymgme.2008.03.018

Cited by 46 publications

(68 citation statements)

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“…It is also known that accumulated dermatan sulfate can activate STAT proteins which increase productions of elastindegrading proteins, i.e., matrix metalloproteinase-12 (MMP-12) and cathepsin S. (Ma et al 2008). Reduction of elastin in myocardial cells, endocardium, and the coronary artery may lead to proliferation of connective tissues, resulting in fibrosis in the ventricular walls, endocardium, and vascular walls (Hinek and Wilson 2000;Karnik et al 2003).…”

Section: Discussionmentioning

confidence: 99%

The Transforming Growth Factor-Beta Signaling Pathway Involvement in Cardiovascular Lesions in Mucopolysaccharidosis-I

Yano

Pavlova

2012

JIMD Reports

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Mucopolysaccharidoses (MPS) are a group of genetic disorders due to deficiency of lysosomal enzymes resulting in impaired glycosaminoglycan metabolism. All types of MPS can present with cardiovascular manifestation, although MPS-I, II, and VI seem to have more severe involvement than the other types. Enzyme replacement therapy (ERT) is available for MPS-I, II, and VI. Cardiovascular changes including hypertrophic cardiomyopathy, thickened valvular lesions, and coronary artery lesions often poorly respond to ERT and are well known as leading causes of death in patients with MPS-I. The mechanisms to cause these changes in MPS-I have not been well characterized. Immunohistopathological studies were conducted on the cardiac specimens from a patient with MPS-I who died due to sudden cardiac failure.

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Section: Discussionmentioning

confidence: 99%

The Transforming Growth Factor-Beta Signaling Pathway Involvement in Cardiovascular Lesions in Mucopolysaccharidosis-I

Yano

Pavlova

2012

JIMD Reports

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“…Figure 2a and b Patient 2): CT images were of poor quality due to body habitus and breathing artefact; however, subsequent pathology specimens demonstrated bullous macroscopic changes and sub-pleural emphysema microscopically. The sub-pleural distribution of these changes was striking and has not previously been described in patients with MPS type I. Degradation of elastin secondary to increased cathepsin, elastase and matrix metalloproteinase activity has been demonstrated in cell culture and animal models of MPS I, and it seems likely that the same disease process is occurring here (Hinek and Wilson 2000;Ma et al 2008;Metcalf et al 2010). We suggest that screening for subpleural and paraseptal emphysema is warranted in adults with MPS I as there is a risk of lifethreatening spontaneous pneumothorax.…”

mentioning

confidence: 71%

Sub‐pleural bullous changes in two adults with Mucopolysaccharidosis type I (Hurler‐Scheie)

Tchan

Graf

Sillence

2011

J of Inher Metab Disea

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“…Treatment options currently available for MPS I have been shown to be very ineffective in treating some aspects of the disease, including the aorta, bone, joint and brain [Ma et al, 2008;Wraith, 2009]. Reaching these organs is imperative to improve the quality of life in MPS I patients.…”

Section: Discussionmentioning

confidence: 99%

Recombinant Encapsulated Cells Overexpressing Alpha-<i>L</i>-Iduronidase Correct Enzyme Deficiency in Human Mucopolysaccharidosis Type I Cells

Baldo

Mayer²,

Burin³

et al. 2011

Cells Tissues Organs

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Mucopolysaccharidosis I (MPS I) is an autosomal recessive lysosomal storage disease due to deficient α-L-iduronidase (IDUA) activity. It results in the accumulation of the glycosaminoglycans (GAGs) heparan and dermatan sulfate and leads to several clinical manifestations. Available treatments are limited in their efficacy to treat some aspects of the disease. Thus, new approaches have been studied for the treatment of MPS I. Here, we tested the ability of recombinant baby hamster kidney cells transfected with human IDUA cDNA in correcting skin fibroblasts from MPS I patients in vitro. Our results showed an increase in IDUA activity in MPS I fibroblasts after 15, 30 and 45 days of coculture with the capsules. Cytological analysis showed a marked reduction in GAG storage within MPS I cells. Enzyme uptake by the fibroblasts was blocked in a dose-dependent manner with mannose-6-phosphate (M6P), indicating that cells use the M6P receptor to internalize the recombinant enzyme. Capsules were effective in correcting MPS I cells even after a 12-month period of cryopreservation. Taken together, our results indicate that cell encapsulation is a potential approach for treatment of MPS I. This approach becomes particularly interesting as a complementary approach, since the capsules could be implanted in sites which current treatments available are not able to reach. Future studies will focus on the efficacy of this approach in vivo.

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Upregulation of elastase proteins results in aortic dilatation in mucopolysaccharidosis I mice

Cited by 46 publications

References 47 publications

The Transforming Growth Factor-Beta Signaling Pathway Involvement in Cardiovascular Lesions in Mucopolysaccharidosis-I

The Transforming Growth Factor-Beta Signaling Pathway Involvement in Cardiovascular Lesions in Mucopolysaccharidosis-I

Sub‐pleural bullous changes in two adults with Mucopolysaccharidosis type I (Hurler‐Scheie)

Recombinant Encapsulated Cells Overexpressing Alpha-<i>L</i>-Iduronidase Correct Enzyme Deficiency in Human Mucopolysaccharidosis Type I Cells

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