The community effect in FGF-1 mediated tumor progression of a rat bladder carcinoma does not involve a direct paracrine signaling

Jouanneau, Jacqueline; Moens, G; Thiery, Jean Paul

doi:10.1038/sj.onc.1202285

Cited by 13 publications

(7 citation statements)

References 29 publications

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“…Non-resistant tumor cells also favor the growth of TSP1-resistant ones: when TSP1 was turned on after 18 d in tumors, when cells had divided about 12 times and the heterogeneity of the cell population had thus increased, resistance developed more rapidly than when TSP1 was expressed starting on day 0. Multiple clonal variants would cooperate during tumor progression through "community" effects (Jouanneau et al 1999) involving secreted factors, cell-cell interactions, or both. Resistance to TSP1, as it results among others in an increased secretion of angiogenic factors, would be one of the mechanisms involved in these community effects.…”

Section: Discussionmentioning

confidence: 99%

In vivo mechanisms by which tumors producing thrombospondin 1 bypass its inhibitory effects

Filleur¹,

Volpert²,

Degeorges³

et al. 2001

Genes Dev.

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Thrombospondin 1 (TSP1) is a multifunctional protein able to activate TGF␤ and to inhibit angiogenesis in vivo. Although usually thought of as an inhibitor of tumor growth, TSP1 may sometimes be present at high levels during tumor progression, suggesting that tumors can eventually overcome their anti-tumor effects. Using a tet-repressible expression system, we demonstrate that murine TSP1 delayed the onset of tumor growth when produced in the tumor bed by rat fibrosarcoma tumor cells or by stromal fibroblasts coinjected with unmodified C6 glioma tumor cells. Yet upon prolonged exposure to TSP1, tumors came to grow at the same rate in the presence as in the absence of TSP1 and transplantation experiments showed that they had become insensitive to inhibition by TSP1 in both syngeneic and immune compromised hosts. Tumor resistance to TSP1 developed as a result of the in vivo outgrowth of pre-existing tumor cell variants that (1) secreted increased amounts of angiogenic factors that counterbalanced the inhibitory effect of TSP1 on neovascularization and (2) grew more efficiently in the presence of TSP1-activated TGF␤. These results indicate that prolonged and continuous local delivery of a single multifunctional angiogenesis inhibitor like TSP1 to fast-growing tumors can lead to tumor resistance in vivo by fostering the outgrowth of subpopulations that are a by-product of the genetic instability of the tumor cells themselves.

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Section: Discussionmentioning

confidence: 99%

In vivo mechanisms by which tumors producing thrombospondin 1 bypass its inhibitory effects

Filleur¹,

Volpert²,

Degeorges³

et al. 2001

Genes Dev.

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“…The fact that the episialin-negative cells are not refractory to ET-18-OMe can be due to the "community effect" described for mixed cell populations with one type of cell dominating the other via cell-cell interactions. 41 Indeed, in a mixture with a minority of MCF7/AZ and a majority of MCF7/6 cells, the MCF-7/AZ phenotype dominates and cells become adhesion-proficient (M. Bracke, personal communication).…”

Section: Discussionmentioning

confidence: 99%

Alkyl-lysophospholipid 1-O-octadecyl-2-O-methyl- glycerophosphocholine induces invasion through episialin-mediated neutralization of E-cadherin in human mammary MCF-7 cellsin vitro

et al. 2001

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1-O-octadecyl-2-O-methyl-glycerophosphocholine (ET-18 Key words: alkyl-lysophospholipid; E-cadherin; episialin; adhesion; invasion1-O-octadecyl-2-O-methyl-glycerophosphocholine (ET-18-OMe) interacts with cell membranes, thereby modulating phospholipid metabolism, interfering with signal transduction, inducing apoptosis and differentiation and regulating invasion. 1 On solid substrate, the E-cadherin/catenin complex is implicated in the cell-cell adhesion of 2 variants of the MCF-7 human breast cancer cell line family, coined MCF-7/AZ and MCF-7/6. In suspension, however, MCF-7/6 cells are adhesion-deficient while MCF-7/AZ cells are adhesion-proficient. Treatment with ET-18-OMe caused antithetic effects on the 2 types of MCF-7 cells. ET-18-OMe restored the E-cadherin function in the adhesiondeficient MCF-7/6 cells, whereas it caused a decrease in cellular aggregation of the adhesion-proficient MCF-7/AZ cells. The latter effects could not be explained by changes in sialylation of Ecadherin. 2 Antithetic effects on invasion have also been reported: ET-18-OMe inhibited invasion of constitutively invasive cells, [3][4][5][6] whereas it induced invasion of otherwise noninvasive cells. 7,8 Inhibition of invasion in the presence of ET-18-OMe was explained by induction of host tissue resistance, 9 but the antithetic effects on cell-cell adhesion and the invasion-promoting effect of ET-18-OMe have not been explained.Adhesion and invasion are the result of a balance between promoter and suppressor molecules modulated by multiple intraand extracellular factors. The presence of the anti-adhesion molecule episialin on the 2 types of MCF-7 cells was observed in a previous study. 2 The aim of our study was to see whether ET-18-OMe affects invasion and adhesion through modulation of episialin and E-cadherin.Episialin is a heterodimeric molecule composed of a membrane anchor and an extracellular moiety. The membrane anchor consists of a cytoplasmatic domain of 68 amino acids and a transmembrane domain. The extracellular moiety consists of a large mucin domain containing a large number of O-linked glycans. 10 The carbohydrate side chains carry many sialic acid residues conveying a highly negative charge upon episialin. 11 Episialin is located at the apical surface of most glandular epithelial cells; it is over-expressed in carcinomas, often distributed over the entire cell surface. 11 Overexpression of episialin inhibits integrin-mediated cell adhesion to

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“…The constitutive expression of FGF-1 or FGF-2 by these carcinoma cells generates cells that secrete the corresponding growth factor and that in vivo allow the growth of highly vascularized tumors as well in autocrine or nonautocrine NBT-II-expressing cells (Jouanneau et al, 1997;Billottet et al, 2002). However, a major difference in growth rate was observed: tumors developing NBT-II cells expressing FGF-2 grew like the control, whereas the growth rate of FGF-1-expressing cells was much faster (Jouanneau et al, 1997(Jouanneau et al, , 1999. Although constitutive expression of the high-affinity receptor FGFR-1 gave cells that have acquired the capacity to be activated by exogenous FGF-2, these cells induced tumors with growth properties similar to that of parental cells (Moscatelli, 1992); conversely, when they are engineered to constitutively express FGFR-1 and FGF-2, they behave like FGF-1-producing cells (Billottet et al, 2002).…”

Section: Introductionmentioning

confidence: 74%

“…Previously, we showed that tumors derived from FGF-1-transfected NBT-II cells grew faster than tumors obtained with control or FGF-2-transfected cells, irrespective of their angiogenic status (Jouanneau et al, 1997(Jouanneau et al, , 1999. Furthermore, NBT-II cellsengineered autocrine for FGF-2 became highly tumorigenic but present the same tumor vascularization (Billottet et al, 2002).…”

Section: Discussionmentioning

confidence: 99%

Direct FGF receptor 1 activation through an anti-idiotypic strategy mimicks the biological activity of FGF-2 and inhibits the progression of the bladder carcinoma derived from NBT-II cells

et al. 2004

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The community effect in FGF-1 mediated tumor progression of a rat bladder carcinoma does not involve a direct paracrine signaling

Cited by 13 publications

References 29 publications

In vivo mechanisms by which tumors producing thrombospondin 1 bypass its inhibitory effects

In vivo mechanisms by which tumors producing thrombospondin 1 bypass its inhibitory effects

Alkyl-lysophospholipid 1-O-octadecyl-2-O-methyl- glycerophosphocholine induces invasion through episialin-mediated neutralization of E-cadherin in human mammary MCF-7 cellsin vitro

Direct FGF receptor 1 activation through an anti-idiotypic strategy mimicks the biological activity of FGF-2 and inhibits the progression of the bladder carcinoma derived from NBT-II cells

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