Matrix Metalloproteinase 1 Is Necessary for the Migration of Human Bone Marrow-Derived Mesenchymal Stem Cells Toward Human Glioma

Ho, Ivy A. W.; Chan, K Y W; Ng, Wai-Hoe; Guo, Chang; Hui, Kam M.; Cheang, P.; Lam, Paula Yeng Po

doi:10.1002/stem.50

Cited by 137 publications

(107 citation statements)

References 34 publications

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“…Moreover, sST2 is secreted by metastatic breast cancer cells and found at high levels in the serum of patients with metastatic tumors. Among the genes most highly regulated by ErbB2, we found the MMPs MMP1 and MMP10 which have been involved previously in cell migration (Dufour et al, 2008;Ho et al, 2009). But MMP1 and MMP10 did not contribute to cell motility in our experimental system.…”

Section: Discussionmentioning

confidence: 45%

Gene expression profiling identifies sST2 as an effector of ErbB2-driven breast carcinoma cell motility, associated with metastasis

Gillibert-Duplantier¹,

Duthey²,

Sisirak³

et al. 2011

Oncogene

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Overexpression of the ErbB2 receptor tyrosine kinase in breast cancer contributes to tumor development and is associated with poor prognosis. However, the mechanism by which ErbB2 might contribute to metastasis is not well defined. To identify genes that mediate ErbB2-driven cell motility, we performed differential gene expression analysis of ErbB2-expressing migrating breast cancer cells vs mutant ErbB2-expressing non-migrating cells. Among the genes that were specifically induced in migrating cells were known transcriptional targets of ErbB2, such as matrix metalloproteinases, and novel ErbB2 targets. Contribution of selected candidate genes to ErbB2-driven cell motility was tested by small interfering RNA targeting. Knockdown of the soluble form of ST2 (sST2), also called interleukin-1 receptor-like 1, one of the most robustly induced genes, decreased ErbB2-induced cell motility in two different cell lines. In response to ErbB2 activation, sST2 protein expression and secretion were increased. Moreover, recombinant sST2 associated with the plasma membrane and sST2-blocking antibodies reduced ErbB2-induced motility. Interestingly, cells from metastatic breast tumors secreted higher levels of sST2 than primary tumor cells. Finally, sST2 was found at high levels in the serum of metastatic breast cancer patients. Our data suggest that sST2 contributes to breast cancer cell motility and that sST2 secretion is associated with metastasis.

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Section: Discussionmentioning

confidence: 45%

Gene expression profiling identifies sST2 as an effector of ErbB2-driven breast carcinoma cell motility, associated with metastasis

Gillibert-Duplantier¹,

Duthey²,

Sisirak³

et al. 2011

Oncogene

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“…TGF-a and EGFR overexpression in CP 13 is consistent with the observed upregulation of MMP-1 in CP in our study. The known involvement of MMP-1 in the migration of human mesenchymal stem cells 27 also supports a role for MMP-1 in PSC migration. As MMP-1 has a crucial role in tumor cell invasion, 24,28 and TGF-a is reportedly upregulated in several pancreatic cancer cell lines, 15 MMP-1 upregulation in TGF-a-activated PSCs may be important for pancreatic Figure 9 The partial colocalization of transforming growth factor (TGF)-b1 and TGF-a in the pancreatic tissues of a chronic pancreas sample.…”

Section: Tgf-a Activates Pscs H Tahara Et Almentioning

confidence: 61%

Transforming growth factor-α activates pancreatic stellate cells and may be involved in matrix metalloproteinase-1 upregulation

Tahara

Sato

Yamazaki

et al. 2013

Laboratory Investigation

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The role that transforming growth factor-a (TGF-a) has in chronic pancreatitis and pancreatic cancer has not been fully elucidated. We evaluated the effects of TGF-a on the human pancreatic stellate cell (PSC) line RLT-PSC and primary human PSCs, and the expression levels of TGF-a and metalloproteinase-1 (MMP-1) in human chronic pancreatitis and pancreatic cancer tissues. TGF-a stimulated the proliferation and migration of PSCs. Although the mRNA expression levels of tissue inhibitor of metalloproteinase-1 and a1(I) collagen were unchanged, the mRNA expression levels of MMP-1 increased concomitant with increases in MMP-1 protein levels and collagenase activity. TGF-a-stimulated migration of RLT-PSC cells was partially blocked by tissue inhibitor of metalloproteinase-1 protein and MMP-1 small interfering RNA. MMP-1 was also observed to stimulate the migration of PSCs. TGF-a-induced MMP-1 expression was completely blocked by gefitinib in PSCs. The Ras-ERK and PI3/Akt pathways appear to be involved in the activation of MMP-1 in PSCs. Immunohistochemical analyses showed that MMP-1 expression was significantly increased in the pancreatic interstitial tissues in case of chronic pancreatitis or pancreatic cancer compared with those in case of normal pancreas. In conclusion, TGF-a increased proliferation and migration of PSCs. TGF-a-induced migration of cells may be partly due to upregulation of MMP-1. TGF-a and MMP-1 upregulation may contribute to the pathogenesis of chronic pancreatitis and pancreatic cancer.

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“…Increased levels of inflammatory cytokines enhance in autocrine manner expression of proteases such as MMP-2, -9 and -14 in MSCs that promote MSC motility towards the tumour (Ries et al, 2007). Ho et al (2009) showed that MMP-1 is crucial for MSC migration toward glioma in vivo, as well as in vitro. MMP-1 cleaves G-proteincoupled receptor PAR1 on MSC surface, triggering intracellular signalling, which promotes MSC glioma tropism.…”

Section: Case Study: Interactions Between Mesenchymal Stem Cells and mentioning

confidence: 99%

Proteases and cytokines as mediators of interactions between cancer and stromal cells in tumours

Breznik

Motaln

Turnšek

2017

Biological Chemistry

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Proteolytic enzymes are highly relevant in different processes of cancer progression. Their interplay with other signalling molecules such as cytokines represents important regulation of multicellular cross-talk. In this review, we discuss protease regulation mechanisms of cytokine signalling in various types of cancer. Additionally, we highlight the reverse whereby cytokines have an impact on protease expression in an autocrine and paracrine manner, representing complex feedback mechanisms among multiple members of these two protein families. The relevance of the protease-cytokine axis is illustrated in glioblastoma, where interactions between normal mesenchymal stem cells and cancer cells play an important role in this very malignant form of brain cancer.

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Matrix Metalloproteinase 1 Is Necessary for the Migration of Human Bone Marrow-Derived Mesenchymal Stem Cells Toward Human Glioma

Cited by 137 publications

References 34 publications

Gene expression profiling identifies sST2 as an effector of ErbB2-driven breast carcinoma cell motility, associated with metastasis

Gene expression profiling identifies sST2 as an effector of ErbB2-driven breast carcinoma cell motility, associated with metastasis

Transforming growth factor-α activates pancreatic stellate cells and may be involved in matrix metalloproteinase-1 upregulation

Proteases and cytokines as mediators of interactions between cancer and stromal cells in tumours

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