2002
DOI: 10.1016/s0925-4439(01)00105-3
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Erk 1/2 differentially regulates the expression from the 1G/2G single nucleotide polymorphism in the MMP-1 promoter in melanoma cells

Abstract: Matrix metalloproteinase-1 (MMP-1) breaks down interstitial collagens, a major component of stromal tissue and a barrier for invading tumor cells. The degradation of collagen by MMP-1 may, therefore, provide one mechanism for facilitating tumor invasion and metastasis. Because of the potential for excessive matrix degradation, the expression of MMP-1 is tightly regulated, often by the mitogen-activated protein kinase (MAPK) pathway. The MAPK signal cascade consists of three separate pathways, the extracellular… Show more

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Cited by 62 publications
(76 citation statements)
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“…The discovery of polymorphisms in MMP promoters that alter gene expression has revealed strong associations between these genetic variants and increased susceptibility to the development of malignancies and other diseases (Henney et al, 2000;Ye, 2000). The most extensively studied MMP SNP in relation to cancer is the À1607 bp insertion/deletion in the MMP-1 promoter (Rutter et al, 1998;Nishioka et al, 2000;Ghilardi et al, 2001;Zhu et al, 2001;Hinoda et al, 2002;Tower et al, 2002;Wyatt et al, 2002;Zinzindohoue et al, 2005;Elander et al, 2006). Similar studies have been conducted for the MMP-2 (Miao et al, 2003) and MMP-3 (Ghilardi et al, 2002;Hinoda et al, 2002) gene promoter polymorphism in relation to disease susceptibility and metastatic behaviour.…”
Section: Discussionmentioning
confidence: 99%
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“…The discovery of polymorphisms in MMP promoters that alter gene expression has revealed strong associations between these genetic variants and increased susceptibility to the development of malignancies and other diseases (Henney et al, 2000;Ye, 2000). The most extensively studied MMP SNP in relation to cancer is the À1607 bp insertion/deletion in the MMP-1 promoter (Rutter et al, 1998;Nishioka et al, 2000;Ghilardi et al, 2001;Zhu et al, 2001;Hinoda et al, 2002;Tower et al, 2002;Wyatt et al, 2002;Zinzindohoue et al, 2005;Elander et al, 2006). Similar studies have been conducted for the MMP-2 (Miao et al, 2003) and MMP-3 (Ghilardi et al, 2002;Hinoda et al, 2002) gene promoter polymorphism in relation to disease susceptibility and metastatic behaviour.…”
Section: Discussionmentioning
confidence: 99%
“…These studies confirmed that cells containing a 2G allele displayed enhanced transcriptional activity compared to cells harbouring the 1G allele. It was also noted that if MMP-1 transcriptional activity was not altered as a consequence of the MMP-1 polymorphism, then expression of this enzyme was likely to be differentially induced in response to cytokines and growth factors (Rutter et al, 1998;Tower et al, 2002;Wyatt et al, 2002). Investigations are currently underway in our laboratory to address this issue and to determine whether our observations are tumourspecific, or applicable to other adenocarcinomas such as breast and prostate.…”
Section: Discussionmentioning
confidence: 99%
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“…38 AP-1 is a protein dimer that consists of c-jun and c-fos. Increased c-fos gene expression correlated with induced AP-1 activation in UVB-exposed keratinocytes and is directed by specific MAPK pathways.…”
Section: C-jun and C-fos Expression In Cultured Pecs And Pterygium Timentioning
confidence: 99%
“…Increased c-fos gene expression correlated with induced AP-1 activation in UVB-exposed keratinocytes and is directed by specific MAPK pathways. 38 Given this background, PECs were irradiated with 20 mJ/cm 2 UVB, RNA was harvested, and analyzed by RT-PCR (Figure 4; A to D). Note the intermediate-early induction (2 to 6 hours) of both c-fos and c-jun transcripts after UVB (Figure 4, B and C, respectively).…”
Section: C-jun and C-fos Expression In Cultured Pecs And Pterygium Timentioning
confidence: 99%