Expression of ADAMTS-8, a secreted protease with antiangiogenic properties, is downregulated in brain tumours

Dunn, Julie R.; Reed, James E.; Plessis, Daniel du; Shaw, Elisabeth; Reeves, Philip J.; Gee, A.; Warnke, Peter C.; Walker, Carol

doi:10.1038/sj.bjc.6603006

Cited by 92 publications

(85 citation statements)

References 32 publications

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“…Our data are in line with our previous report showing that ADAMTS-12 inhibits the formation of vascular endothelial growth factor-induced tubular structures in BAE-1 cells (Llamazares et al, 2007). The finding of antiangiogenic effects for a member of the ADAMTS family is not unprecedented as it has also been described for ADAMTS-1 and ADAMTS-8 (Vazquez et al, 1999;Dunn et al, 2006). However, the originality of our findings relies on the identification of a key host ADAMTS-12 contribution in the host protection toward the angiogenic response induced by tumor cells.…”

Section: Angiogenesis Insupporting

confidence: 93%

Higher sensitivity of Adamts12-deficient mice to tumor growth and angiogenesis

et al. 2010

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ADAMTS (a disintegrin and metalloproteinase domain with thrombospondin motifs) constitute a family of endopeptidases related to matrix metalloproteinases. These proteases have been largely implicated in tissue remodeling and angiogenesis associated with physiological and pathological processes. To elucidate the in vivo functions of ADAMTS-12, we have generated a knockout mouse strain (Adamts12) in which Adamts12 gene was deleted. The mutant mice had normal gestations and no apparent defects in growth, life span and fertility. By applying three different in vivo models of angiogenesis (malignant keratinocyte transplantation, Matrigel plug and aortic ring assays) to Adamts12 À/À mice, we provide evidence for a protective effect of this host enzyme toward angiogenesis and cancer progression. In the absence of Adamts-12, both the angiogenic response and tumor invasion into host tissue were increased. Complementing results were obtained by using medium conditioned by cells overexpressing human ADAMTS-12, which inhibited vessel outgrowth in the aortic ring assay. This angioinhibitory effect of ADAMTS-12 was independent of its enzymatic activity as a mutated inactive form of the enzyme was similarly efficient in inhibiting endothelial cell sprouting in the aortic ring assay than the wild-type form. Altogether, our results show that ADAMTS-12 displays antiangiogenic properties and protect the host toward tumor progression.

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Section: Angiogenesis Insupporting

confidence: 93%

Higher sensitivity of Adamts12-deficient mice to tumor growth and angiogenesis

et al. 2010

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“…These two proteases also cleave two other members of the lectican family, aggrecan [53] and versican [54], and have a restricted additional spectrum of ECM substrates [55][56][57]. Other members of the ADAMTS family have been shown or proposed to have aggrecanase activity (recently reviewed in [58]) but their expression in the CNS is low and there is currently no evidence for their role in B/b processing in gliomas [59][60][61][62][63].…”

Section: Discussionmentioning

confidence: 99%

BEHAB/brevican requires ADAMTS-mediated proteolytic cleavage to promote glioma invasion

2008

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Malignant gliomas are the most common and deadly primary brain tumors, due to their infiltrative invasion of the normal neural tissue that makes them virtually impossible to completely eliminate. We have previously identified and characterized the proteoglycan BEHAB/brevican in gliomas and have demonstrated that upregulation and cleavage of this CNS-specific molecule promote glioma invasion. Here, we have further investigated if the proteolytic processing of BEHAB/ brevican by metalloproteases of the ADAMTS family is a necessary step in mediating its proinvasive effect in glioma. By generating a site-specific ( 396 SRG 398 → NVY) mutant form resistant to ADAMTS cleavage, we have shown that the predominant proteolytic processing of BEHAB/ brevican by glioma cells occurs only at this site. More importantly, "uncleavable" BEHAB/ brevican is unable to enhance glioma cell invasion in vitro and tumor progression in vivo. In addition, our results suggest that the full-length protein and its cleavage products may act independently because the mutant form does not exert a dominant negative effect on normal BEHAB/brevican expression or cleavage. These results illustrate how the regulated processing of major components of the neural extracellular matrix has important functional implications in glioma progression. In addition, our findings underscore the relevance of the ADAMTS family of metalloproteases as attractive targets for novel pharmacological approaches in glioma therapy.

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“…Brain tumours, often invading surrounding parenchyma, could thus display a modulated proteinase expression facilitating tumour cell infiltration and/ or angiogenesis. Some ADAMTS proteinases (ADAMTS-8 and ADAMTS-13) display lower levels of expression in brain tumours as compared to normal brain tissue [118,119]. In sharp contrast, ADAMTS-4 and TS-5 are overexpressed in human glioblastomas and could be responsible for brevican cleavage and contribute to invasiveness of glioblastoma cells [120].…”

Section: Brain Tumoursmentioning

confidence: 99%

Emerging roles of ADAM and ADAMTS metalloproteinases in cancer

et al. 2008

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A disintegrin and metalloproteinases (ADAMs) are a recently discovered family of proteins that share the metalloproteinase domain with matrix metalloproteinases (MMPs). Among this family, structural features distinguish the membrane-anchored ADAMs and the secreted ADAMs with thrombospondin motifs referred to as ADAMTSs. By acting on a large panel of membrane-associated and extracellular substrates, they control several cell functions such as adhesion, fusion, migration and proliferation. The current review addresses the contribution of these proteinases in the positive and negative regulation of cancer progression as mainly mediated by the regulation of growth factor activities and integrin functions.

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Expression of ADAMTS-8, a secreted protease with antiangiogenic properties, is downregulated in brain tumours

Cited by 92 publications

References 32 publications

Higher sensitivity of Adamts12-deficient mice to tumor growth and angiogenesis

Higher sensitivity of Adamts12-deficient mice to tumor growth and angiogenesis

BEHAB/brevican requires ADAMTS-mediated proteolytic cleavage to promote glioma invasion

Emerging roles of ADAM and ADAMTS metalloproteinases in cancer

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