Your search keyword '"M F, Poupon"' showing total 9 results

1. Two- and three-dimensional cell structures govern epidermal growth factor survival function in human bladder carcinoma cell lines

Author

V, Dangles, F, Féménia, V, Lainé, M, Berthelemy, D, Le Rhun, M F, Poupon, D, Levy, and I, Schwartz-Cornil

Subjects

Cyclin-Dependent Kinase Inhibitor p21, Time Factors, Epidermal Growth Factor, Apoptosis, Protein-Tyrosine Kinases, Transforming Growth Factor alpha, Tyrphostins, Genistein, Isoflavones, Culture Media, Serum-Free, Neoplasm Proteins, Up-Regulation, ErbB Receptors, Urinary Bladder Neoplasms, Cyclins, Spheroids, Cellular, Nitriles, Quinazolines, Tumor Cells, Cultured, Humans

Abstract

Human bladder carcinomas often express high levels of the epidermal growth factor (EGF) receptor. In three human bladder carcinoma cell lines (OBR, T24, and 647V), we show that two EGF receptor ligands, namely EGF and transforming growth factor alpha, enhanced the apoptosis due to serum starvation on cells cultured as monolayers. Conversely, EGF and transforming growth factor alpha prevented apoptosis when the same serum-starved cells were cultured as three-dimensional spheroids. Both stimulation and inhibition of apoptosis by EGF were associated with p21 WAF1/CIP1 overexpression. In 647V spheroids, EGF protection against radiation-induced apoptosis was negated by genistein and tyrphostin AG1478, suggesting that blockade of the EGF signal transduction in patients with bladder cancer may improve the radiotherapy efficacy.

Published

1997

2. Antitumoral activity of bombesin analogues on small cell lung cancer xenografts: relationship with bombesin receptor expression

Author

F, Thomas, F, Arvelo, E, Antoine, M, Jacrot, and M F, Poupon

Subjects

Lung Neoplasms, Transplantation, Heterologous, Gene Expression, Mice, Nude, In Vitro Techniques, Receptors, Neurotransmitter, Receptors, Bombesin, Mice, Tumor Cells, Cultured, Animals, Humans, Bombesin, RNA, Messenger, Carcinoma, Small Cell, Cell Division, Neoplasm Transplantation

Abstract

Gastrin releasing peptide (GRP), the human homologue of bombesin (BN), is an autocrine growth factor for small cell lung cancer (SCLC) cells. The synthetic octapeptides [D-cpa1-beta-Leu8-des-Met9]litorin (BIM 26182) and [D-Phe6-Leu13-CH2NH-Cpa14]bombesin(6-14)NH2 (BIM 26189) are potent GRP/BN antagonists of the proliferation of 3T3 and rat pancreas cells. The effect of these analogues on the proliferation of four SCLC cell lines (SCLC 6, SCLC 41, SCLC 75, SCLC 74R) was tested in vitro and in vivo. Two of these SCLC lines (SCLC 41M and SCLC 75) had receptors for BN/GRP and expressed the prepro-GRP mRNA. BIM 26182 and BIM 26189 inhibited [3H]thymidine incorporation into the DNA of SCLC 41 cells, stimulated [3H]thymidine incorporation in SCLC 6, and had no effect on the two other cell lines. The SCLC implanted s.c. in nude mice were treated with either BIM 26182 or BIM 26189. BIM 26182 and BIM 26189 injected at the doses of 50 micrograms twice a day (s.c.) around the tumor for 10 to 21 days delayed the growth of SCLC 41 and of SCLC 75. The maximal effect was observed during the treatment period, after which the tumors regrew, suggesting a cytostatic effect of these peptides. No inhibitory effect of the peptides on SCLC 74R or SCLC 6 growth was observed. These data suggest that GRP antagonists are able to inhibit the in vitro and in vivo growth of BN/GRP receptors-positive SCLC.

Published

1992

3. Preclinical antitumor activity of a new Vinca alkaloid derivative, S 12363

Author

A, Pierré, L, Kraus-Berthier, G, Atassi, S, Cros, M F, Poupon, G, Lavielle, M, Berlion, and J P, Bizzari

Subjects

Mice, Inbred C57BL, Mice, Mice, Inbred DBA, Tumor Cells, Cultured, Animals, Humans, Drug Screening Assays, Antitumor, Vinca Alkaloids, Drug Administration Schedule

Abstract

S 12363 is a new Vinca alkaloid derivative obtained by appending an optically active alpha-aminophosphonate at the C23 position of O4-deacetyl vinblastine. S 12363 was evaluated for cytotoxic and antitumor activity against a spectrum of murine and human tumors. This compound was, respectively, on average, 72- and 36-fold more cytotoxic than were vincristine and vinblastine, when tested on a panel of 2 murine and 37 human tumor cell lines using the microculture tetrazolium assay. S 12363 exhibited significant antitumor activity against murine transplantable tumors (i.p. and s.c. P388 leukemia, i.p. L1210 leukemia, i.p. and i.v. B16 melanoma, i.p. M5076 sarcoma, and s.c. colon adenocarcinoma 38), while no activity was observed on s.c. Lewis lung carcinoma. S 12363, when administered i.p., showed moderate activity on human NCI-H460 lung and PANC-1 pancreas tumor xenografts in nude mice. However, when it was administered i.v., it exerted a significant activity against human HT-29 colon, NCI-H460 lung, NCI-H125 lung, PANC-1 pancreas, and A-431 vulvar tumor xenografts. S 12363 was also active in vivo against a P388 leukemia subline resistant to vincristine. On the in vivo panel of tumors used in this study, S 12363 was at least as active as reference compounds, while its optimal dosage was 10- to 40-fold lower than that of vinblastine, depending on the models studied. The effects of schedule and route of administration on the antitumor activity of S 12363 were studied in both i.p. inoculated P388 leukemia and B16 melanoma, in which the activity was improved by single and intermittent treatment (Days 1, 8, and 15) and i.p. route. S 12363, which differs only by the configuration of the asymmetric carbon atom of the side chain, was 300-fold less cytotoxic and 1000-fold less potent in vivo than was S 12363. These results suggest that S 12363 could present a therapeutic advantage over its congeners and deserves further pharmacological evaluations.

Published

1991

4. Heterogeneity of the growth and metastatic behavior of cloned cell lines derived from a primary rhabdomyosarcoma

Author

F L, Sweeney, J, Pot-Deprun, M F, Poupon, and I, Chouroulinkov

Subjects

Male, Lung Neoplasms, Lymphatic Metastasis, Rhabdomyosarcoma, Animals, Sarcoma, Experimental, Cell Division, Cell Line, Clone Cells, Rats

Abstract

In order to study the heterogeneity of the metastatic and tumorigenic behaviors of malignant neoplasms, we have isolated a series of cloned cell lines from a primary nickel-induced rat rhabdomyosarcoma. The growth characteristics in vitro and in vivo and metastatic capacity following s.c. or i.v. injection of cells were compared to those of the parental cell line. Differences between the cloned cell lines themselves and between the clones and the parental cells were found in the number of metastases provoked by both i.v. and s.c. injections, in the number of cells required to induce s.c. tumors, and in the growth rate of those tumors. In vitro, the doubling times and saturation densities of the different cell lines varied greatly. A direct correlation was observed between the 50% tumoral dose and the initial tumor growth phase. We found that there was a tendency for lines which were highly metastatic after s.c. injection to have a low metastatic capacity after i.v. injection and inversely. The two types of metastasis (spontaneous and experimental) appear therefore to depend on different characteristics of the cells used.

Published

1982

5. Cytostatic effect of spleen cells of tumor-bearing mice on syngenetic tumor cells

Author

G, Lespinats and M F, Poupon

Subjects

Immunity, Cellular, Mice, Inbred C3H, Fibrosarcoma, Neoplasms, Experimental, Thymus Gland, In Vitro Techniques, Cytotoxicity Tests, Immunologic, Mice, Antigens, Neoplasm, Animals, Female, Cell Division, Spleen, Methylcholanthrene

Abstract

Spleen cell suspensions of methylcholanthrene-induced tumor-bearing mice were tested for their ability to inhibit tumor growth in vitro. The level of cytostasis was correlated with tumor growth and disappeared rapidly after surgical removal of the tumor. Pretreatment by anti-Thy 1-2 antiserum and complement, or by carbonyl iron and a magnet, showed that adherent, non-T-cells were the main effector cells of the cytostatic antitumor effect. Thymus cells suspensions from tubor-bearing mice were not effective in inhibiting tumor growth. This cytostatic effect was not tumor specific, inasmuch as the same spleen cell suspension inhibited growth of tumor cells of different origin.

Published

1977

6. Fibroblast-dependent tumorigenicity of cells in nude mice: implication for implantation of metastases

Author

O, Picard, Y, Rolland, and M F, Poupon

Subjects

Mice, Lung Neoplasms, Macrophages, Cell Cycle, Rhabdomyosarcoma, Animals, Mice, Nude, Endothelium, Neoplasms, Experimental, Fibroblasts, Neoplasm Metastasis, Cell Line, Rats

Abstract

The inadequate nature of the microenvironment is one of several factors considered in the failure of tumor engraftment in athymic mice; in the present work, we have tried to more adequately reconstitute it by injecting tumor cells together with fibroblasts. We have demonstrated that the s.c. co-inoculation of fibroblasts with different kinds of tumor cells of animal origin [rat rhabdomyosarcoma (RMS) 9-4/0, rat hepato-carcinoma FAO] or human origin (colonic adenocarcinoma HT29, Ewing's sarcoma pleural metastasis EW-S1) is necessary for tumor take and growth when the number of tumor cells alone is below the tumorigenic dose. We have shown that the s.c. coinoculation of 10(6) fibroblasts and 10(2) RMS 9-4/0 tumor cells induced a tumor take in all the recipient mice, while 10(2) tumor cells alone never gave any tumor. With a tumorigenic number of RMS 9-4/0 tumor cells (10(4), addition of 10(6) fibroblasts decreased the delay between cell injection and tumor appearance, thereby increasing tumor take and growth rate. These results were observed not only in nude animals (mice and rats) used as recipient animals but also in normal WAG rats receiving the syngeneic RMS 9-4/0 tumor cells, and they were independent of the nature or origin of the different fibroblasts cells. This helper effect has also been observed in the normal WAG rats. I.v. injection of tumor cells from a poorly metastatic 9-4/8 subline, derived from the RMS 9-4/0 line and mixed with 10(6) fibroblasts, gave a high number of lung colonies. Addition of 10(6) irradiated 9-4/8 tumor cells instead of fibroblasts did not increase the lung colonizing potential. Fibroblast-conditioned medium mixed with tumor cells instead of fibroblasts also enhanced tumor take and size but to a lesser extent than did the fibroblasts themselves. Only endothelial cells cultured from porcine aorta had a similar helper effect among the cells tested. It is argued in the discussion that the proliferating state of cultivated fibroblasts is a determinant factor conferring upon them the ability to promote tumor cell growth, while fibroblasts very numerous at the implantation site but quiescent might not be efficient in cooperation. Changes in fibroblast morphology and physiology may be necessary in order for tumor cells to express their tumorigenicity.

Published

1986

7. Increased level of amplification of the c-myc oncogene in tumors induced in nude mice by a human breast carcinoma cell line

Author

N, Modjtahedi, C, Lavialle, M F, Poupon, R M, Landin, R, Cassingena, R, Monier, and O, Brison

Subjects

Mice, Transcription, Genetic, Transplantation, Heterologous, Gene Amplification, Animals, Chromosomes, Human, Humans, Mice, Nude, Breast Neoplasms, Female, Oncogenes, Neoplasm Transplantation, Cell Line

Abstract

Cell line SW 613-S, derived from a human breast carcinoma, contained double minute chromosomes (DMs) but lost them progressively upon in vitro cultivation. These cells were tumorigenic in nude mice. Cell lines were derived from the tumors and were found to have a high DM content. In three such cell lines, DMs were stably maintained upon in vitro cultivation, whereas in another they were progressively lost. We found that the c-myc oncogene is amplified 5- to 10-fold in SW 613-S and 20- to 90-fold in the different cell lines derived from the tumors. At least part of the additional c-myc copies were found associated with a purified DM fraction. In cell lines which lost the DMs during in vitro passages, the level of amplification was maintained. In situ hybridization experiments indicated that this loss was compensated by the acquisition of copies of the c-myc gene integrated into a chromosome. No major rearrangement of the amplified c-myc gene was detected. The amount of c-myc messenger RNAs is roughly proportional to the level of amplification. Our results indicate that growth of SW 613-S cells as tumors in nude mice selected cells with an increased level of amplification and expression of the c-myc oncogene.

Published

1985

8. Differential adhesiveness of rhabdomyosarcoma-derived cloned metastatic cell lines to vascular endothelial monolayers

Author

S, Korach, M F, Poupon, J A, Du Villard, and M, Becker

Subjects

Lung Neoplasms, Time Factors, Rhabdomyosarcoma, Cell Adhesion, Animals, Endothelium, Neoplasm Metastasis, Lung, Clone Cells, Fibronectins, Rats

Abstract

A series of 11 cloned cell lines derived from a primary, nickel-induced rat rhabdomyosarcoma was evaluated for their metastatic capacity (number of lung colonies following i.v. injection) and attachment kinetics to confluent pig endothelial cell monolayers grown in vitro. The morphology of the adhering cells was also studied by optical and scanning electron microscopy. Cells from all lines tested began to attach to the endothelial monolayers within 15 min of incubation at 37 degrees C, with 64% to 93% of the cells adhering after 2 h. Attachment rates at 30 min ranged from 29 to 48% for four lines classed as "weakly adhesive" (attachment, less than 50%) and from 53 to 78% for seven lines classed as "highly adhesive" (attachment, greater than 50%). Four clones of five displaying low lung-colonizing capacities also showed low attachment rates to endothelial monolayers in vitro. All of six highly colonizing lines studied had high attachment rates. A degree of positive correlation was observed between the amount of cell surface fibronectin as evaluated by immunofluorescence and the early phase attachment rates (and lung-colonizing capabilities) of the different cloned cell lines. Early (15 min) attachment of tumor cells to isolated extracellular matrix preparations proceeded at higher rates than to endothelial monolayers, and previously detected differences between high- and low-colonizing clones were less evident with these matrix substrates. Our results suggest possible interrelationships between specific cell adhesion properties and the metastatic potential of blood-borne tumor cells.

Published

1986

9. Correlation between reversion of a dedifferentiated rat hepatoma line and the recovery of tumorigenicity

Author

J, Maigné, K H, Ng, M, Meunier-Rotival, M F, Poupon, and J, Deschatrette

Subjects

Mice, Liver Neoplasms, Experimental, Phenotype, Transplantation, Heterologous, Animals, Mice, Nude, Cell Differentiation, Cell Division, Neoplasm Transplantation, Cell Line, Clone Cells, Rats

Abstract

The injection into athymic nude mice of well-differentiated cells of the H4IIEC3 rat hepatoma line leads to tumor take and growth. Animals given injections of cells of a "dedifferentiated" variant subclone, however, do not develop tumors, whereas revertant clones are malignant. Nevertheless, tumors are obtained by increasing the number of injected dedifferentiated cells, and the cells from these tumors do express liver-specific messenger RNAs. Finally, the differentiated state of these tumor cells is stable in vitro. This correlation between the differentiated state of the cells and tumorigenicity is also observed in somatic hybrids between the variant cells and the differentiated ancestors. These hybrids express the hepatic functions and give rise to tumors. The only in vitro character of transformation which distinguishes the two types of cells is anchorage independence of growth. Since two other independent variants develop tumors, it is established that the nonmalignant state is not simply due to the lack of expression of liver-specific traits. There is strong evidence that different mechanisms are responsible for the dedifferentiated state of the two classes of variants, and this supports the hypothesis that the correlation between the dedifferentiated state of the nonmalignant variant and its nontumorigenic phenotype relies on the level of regulation specifically affected in this clone.

Published

1988