Anti‐integrin antibodies induce type IV collagenase expression in keratinocytes

Larjava, Hannu; Lyons, J. Guy; Salo, Tuula; Mäkelä, M; Koivisto, Leeni; Birkedal‐Hansen, Henning; Sk, Akiyama; Yamada, Katsushi; Heino, Jyrki

doi:10.1002/jcp.1041570125

Cited by 82 publications

(40 citation statements)

References 70 publications

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“…Also, MAb 13, directed against ␤1 integrin, 23 induced pro-MMP-9 expression, possibly by acting as the natural ligand on its receptor, in agreement with studies of keratinocytes showing pro-MMP-9 induction by the same antibody. 28 Since collagen I is a ubiquitous component of the prostate and bone stroma, a major site of PC metastasis, our data suggest that specific interactions of PC cells with the collagenous ECM may facilitate matrix breakdown and eventually tumor invasion through the induction of proteolytic enzymes in tumor cells. We speculate that collagen I in bone, whether as a part of the ECM or in soluble form, may stimulate the expression of MMP-9 by PC cells, leading to increased bone turnover and release of collagen I, resulting in a vicious cycle of bone matrix degradation and tumor cell proliferation.…”

Section: Discussionmentioning

confidence: 81%

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Differential regulation of matrix metalloproteinase-9, tissue inhibitor of metalloproteinase-1 (TIMP-1) and TIMP-2 expression in co-cultures of prostate cancer and stromal cells

et al. 2001

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Tumor-stromal interactions have been suggested to be a critical factor in both tumor invasion and tumor metastasis. Here, we examined the role of tumor-stromal interactions using co-cultures of prostate cancer (PC) cells derived from primary and metastatic tumors with primary or immortalized stromal (fibroblast and smooth muscle) cells and their effect on matrix metalloproteinase (MMP) and tissue inhibitor of metalloproteinase (TIMP) expression. Co-cultures of PC and stromal cells showed enhanced levels of pro-MMP-9 and reduced levels of TIMP-1 and TIMP-2. Whereas enhanced expression of pro-MMP-9 occurred in PC cells, the TIMPs were down-regulated in stromal cells. Induction of pro-MMP-9 and reduction of TIMP expression did not require cell-cell contact and were mediated by a soluble factor(s) present in the conditioned medium of the effector cell. Collagen I is a potent inducer of pro-MMP-9 in PC cells. Consistently, preliminary characterization of the soluble factor in the fibroblast conditioned medium revealed m.w. of approximately 100 to 250 kDa, and its effect on pro-MMP-9 expression was partly inhibited by an anti-␣2 integrin antibody, a major collagen I receptor. Expression of pro-MMP-9 protein and mRNA was also induced in metastatic PC-3 cells grown in human fetal bone implants in SCID mice. Metastasis formation is the hallmark of cancer and the major cause of mortality. Tumor metastasis involves extensive interactions of the invasive cancer cells with host stromal components, and such interactions promote degradation of the extracellular matrix (ECM) by specialized proteolytic enzymes produced by both the cancer and the stromal cells. These interactions are likely to occur in both primary and metastatic sites. Among the proteases involve in ECM degradation during tumor invasion, the family of matrix metalloproteinases (MMPs) has been shown to play a key role due to their ability to degrade a variety of ECM and basement membrane components. 1-3 All MMPs are specifically inhibited by the tissue inhibitors of matrix metalloproteinases (TIMPs), a family of proteins that presently includes TIMP-1, TIMP-2, TIMP-3 and TIMP-4. 4 The TIMPs inhibit all active MMPs, albeit with different affinities, by binding to the active site of the enzyme. Consequently, the balance between MMP and TIMP levels has been considered to be a critical determinant of the net proteolytic activity at any given time. 5 In tumor tissues, differential expression of MMPs and TIMPs in the tumor and stromal cells may tilt the balance and thus influence MMP activity and eventually tumor cell invasion. However, little is known about the regulation of MMP and TIMP levels in tumor and stromal tissues.Prostate cancer (PC) is the most common cancer and the second leading cause of cancer death in American men. 6 Metastatic PC cells invade initially into the prostate stroma, where they intimately interact with stromal cells and ECM components. Eventually, PC cells metastasize preferentially to bone tissues, where they interact with bone stromal cell...

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Section: Discussionmentioning

confidence: 81%

“…7c), suggesting that binding of the MAb to its receptor triggers a signaling pathway in PC cells similar to that elicited by collagen I and leading to pro-MMP-9 secretion. 28 As controls, anti-␣5 (MAb 16) (Fig. 7d) and non-immune IgG (Fig.…”

Section: Effect Of Anti-integrin Antibodies On Pro-mmp-9 Expressionmentioning

confidence: 99%

Differential regulation of matrix metalloproteinase-9, tissue inhibitor of metalloproteinase-1 (TIMP-1) and TIMP-2 expression in co-cultures of prostate cancer and stromal cells

et al. 2001

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“…a3b1 integrin was shown to participate in phagocytosis of extracellular matrix (Coopman et al, 1996). a2b1, a3b1, a4b1, and a5b1 integrin were found to be involved in the regulation of matrix metalloprotease expression (Larjava et al, 1993;Huhtala et al, 1995;Riikonen et al, 1995). In addition, activation of a6b1 integrin increased invasiveness of LOX human melanoma cells correlating with a 2 ± 3-fold elevation of extracellular matrix degradation and invadopodial activity (Nakahra et al, 1996).…”

Section: Discussionmentioning

confidence: 99%

β1 integrin promotes but is not essential for metastasis of ras-myc transformed fibroblasts

Brakebusch

Wennerberg

Krell³

et al. 1999

Oncogene

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To investigate the role of b1 integrin during tumor metastasis, we established a ras-myc transformed ®broblastoid cell line with a disrupted b1 integrin gene on both alleles (GERM 11). Stable transfection of this cell line with an expression vector encoding b1A integrin resulted in b1A integrin-expressing sublines. Tumors were induced by subcutaneous injection of GERM 11 cells and 3 independent b1 integrin expressing sublines (GERM 116, 1A10, 2F2) into syngeneic mice. After 10 days tumors were surgically removed. While average weights of GERM 11 and GERM 116 tumors were similar, tumors induced by the high expressing clones 1A10 and 2F2 were markedly smaller, suggesting an inverse correlation of tumor growth and b1 integrin expression. The metastasis potential of all three b1 integrin-expressing GERM 11 sublines tested was signi®cantly higher than that of the b1-de®cient GERM 11 cells. GERM 116 tumors led in all animals to severe metastasis in lung and liver, while GERM 11 tumors induced only a few metastatic foci in the lung. Stroma of both tumors contained nidogen and high amounts of tenascin C, but only a few very low levels of ®bronectin, laminin-1, and collagen type I. b1 integrin, therefore, increases but is not essential for metastasis of ras-myc transformed ®broblasts.

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“…It was initially observed that antibodies blocking α 5 β 1 integrin-mediated adhesion induced MMP expression in fibroblasts (Werb et al, 1989). Later studies revealed that integrin-mediated signals are general regulators of MMP expression, as α 2 β 1 integrin regulates MMP-1 expression (Riikonen et al, 1995;Dumin et al, 2001), antibodies to α 3 β 1 integrin-tetraspanin complexes induce MMP-2 expression (Sugiura and Berditchevski, 1999), and α M β 2 and α 3 β 1 integrin ligation stimulates MMP-9 expression (Wize et al, 1998;Larjava et al, 1993). The effects on MMP expression are very specific.…”

Section: Expression and Secretion Of Gelatinases And Other Mmpsmentioning

confidence: 99%