2011
DOI: 10.1523/jneurosci.0141-11.2011
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MMP2-9 Cleavage of Dystroglycan Alters the Size and Molecular Composition of Schwann Cell Domains

Abstract: Myelinating glial cells exhibit a spectacular cytoarchitecture, because they polarize on multiple axes and domains. How this occurs is largely unknown. The dystroglycan-dystrophin complex is required for the function of myelin-forming Schwann cells. Similar to other tissues, the dystroglycan complex in Schwann cells localizes with different dystrophin-family members in specific domains, thus promoting polarization. We show here that cleavage of dystroglycan by matrix-metalloproteinases 2 and 9, an event that i… Show more

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Cited by 46 publications
(60 citation statements)
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References 69 publications
(109 reference statements)
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“…4A,C and Table 3). Finally, -dystroglycan glycosylation, which increases as nerves mature (Court et al, 2011), was significantly reduced in 1 integrin-null nerves. Collectively, these data suggest that dystroglycan acts after 1 integrin during axonal sorting.…”
Section: Research Article Dystroglycan In Axonal Sortingmentioning
confidence: 91%
“…4A,C and Table 3). Finally, -dystroglycan glycosylation, which increases as nerves mature (Court et al, 2011), was significantly reduced in 1 integrin-null nerves. Collectively, these data suggest that dystroglycan acts after 1 integrin during axonal sorting.…”
Section: Research Article Dystroglycan In Axonal Sortingmentioning
confidence: 91%
“…Changes in -Dg glycosylation may also play a role in cancer progression [16,17], which may have an important anti-tumorigenic function [14]; in addition, aberrant degradation of -Dg through MMP-2 and MMP-9 has been recorded as a relevant event observed in several tumor cell lines and in inflammatory diseases [16,18].…”
Section: Introductionmentioning
confidence: 99%
“…laminin) from degradation, suppressing the algesic action of MMP-2 (21), and stimulating the regenerative program in the sensory neurons, the selective, local, and short term inhibition of MMP-14 activity promoted axonal growth and reversed the established hypersensitivity arising from PNS damage. Caution, however, is required in developing the sustained or late stage MMP-14 inhibitor therapy as this therapy may also target certain functions that are beneficial to nerve repair, such as the MMP-2-mediated degradation of inhibitory CSPGs (25,26) and myelination (20,64,65).…”
Section: Discussionmentioning
confidence: 99%