Your search keyword '"Provencher DM"' showing total 3 results

1. Chemosensitivity and radiosensitivity profiles of four new human epithelial ovarian cancer cell lines exhibiting genetic alterations in BRCA2, TGFbeta-RII, KRAS2, TP53 and/or CDNK2A.

Author

Samouëlian, V., Maugard, C.M., Jolicoeur, M., Bertrand, R., Arcand, S.L., Tonin, P.N., Provencher, DM., Mes-Masson, A.-M., Samouëlian, V, and Provencher, D M

Subjects

*OVARIAN diseases, *CELL lines, *EPITHELIAL cells, *CANCER radiotherapy, *DRUG therapy, *PACLITAXEL, *TUMOR treatment, *THERAPEUTICS, *ANTINEOPLASTIC agents, *CELL physiology, *CELL receptors, *COMPARATIVE studies, *RESEARCH methodology, *MEDICAL cooperation, *GENETIC mutation, *ONCOGENES, *OVARIAN tumors, *PROTEINS, *RADIATION, *RESEARCH, *TRANSFERASES, *EVALUATION research, *BRCA genes, *CANCER cell culture, *PHARMACODYNAMICS, *PHYSIOLOGICAL effects of radiation

Abstract

To address the cellular basis for the response to ovarian cancer treatment, we characterized the chemosensitivity and radiosensitivity of four human epithelial ovarian cancer cell lines that harbor different genetic alterations. The TOV-21G, TOV-81D, OV-90, and TOV-112D cell lines were derived from ovarian tumors (TOV) or ascites (OV) from chemotherapy- and radiotherapy-naive patients and were characterized by their mutation spectrum of BRCA2, TGFbeta-RII, KRAS2, TP53, and CDKN2A. Cells were monitored for survival following exposure at various concentrations to different cytotoxic agents including cisplatin, camptothecin or paclitaxel or to different doses of gamma-irradiation. At the lowest doses, the TGFbeta-RII-mutated and KRAS2-mutated cell line, TOV-21G, and the BRCA2-mutated cell line, TOV-81D, demonstrated a significantly higher sensitivity to cisplatin and gamma-irradiation than the TP53-mutated cell lines, TOV-112D and OV-90. At higher doses, differences between the TP53-mutated lines were observed with TOV-112D being less sensitive to cisplatin than OV-90 that also harbors a CDNK2A mutation. All cell lines were similarly sensitive to high doses of gamma-irradiation. In contrast, sensitivity to camptothecin or paclitaxel was not significantly different between all cell lines, irrespective of the mutation status of BRCA1, BRCA2, TGFbeta-RII, KRAS2, TP53, and CDKN2A. The observed responses to treatment are consistent with the current knowledge concerning BRCA2, TGFbeta-RII, KRAS2, TP53, and/or CDKN2A aberrant function. [ABSTRACT FROM AUTHOR]

Published

2004

2. Immunohistochemical profiling of benign, low malignant potential and low grade serous epithelial ovarian tumors.

Author

Ouellet V, Ling TH, Normandin K, Madore J, Lussier C, Barrès V, Bachvarov D, Rancourt C, Tonin PN, Provencher DM, Mes-Masson AM, Ouellet, Véronique, Ling, Tak Hay, Normandin, Karine, Madore, Jason, Lussier, Christian, Barrès, Véronique, Bachvarov, Dimcho, Rancourt, Claudine, and Tonin, Patricia N

Abstract

Background: Serous epithelial ovarian tumors can be subdivided into benign (BOV), low malignant potential (LMP) or borderline and invasive (TOV) tumors. Although the molecular characteristics of serous BOV, LMP and low grade (LG) TOV tumors has been initiated, definitive immunohistochemical markers to distinguish between these tumor types have not been defined.Methods: In the present study, we used a tissue array composed of 27 BOVs, 78 LMPs and 23 LG TOVs to evaluate the protein expression of a subset of selected candidates identified in our previous studies (Ape1, Set, Ran, Ccne1 and Trail) or known to be implicated in epithelial ovarian cancer disease (p21, Ccnb1, Ckd1).Results: Statistically significant difference in protein expression was observed for Ccnb1 when BOV tumors were compared to LMP tumors (p = 0.003). When BOV were compared to LG TOV tumors, Trail was significantly expressed at a higher level in malignant tumors (p = 0.01). Expression of p21 was significantly lower in LG tumors when compared with either BOVs (p = 0.03) or LMPs (p = 0.001). We also observed that expression of p21 was higher in LMP tumors with no (p = 0.02) or non-invasive (p = 0.01) implants compared to the LMP associated with invasive implants.Conclusion: This study represents an extensive analyse of the benign and highly differentiated ovarian disease from an immunohistochemical perspective. [ABSTRACT FROM AUTHOR]

Published

2008

3. Characterization of three new serous epithelial ovarian cancer cell lines.

Author

Ouellet V, Zietarska M, Portelance L, Lafontaine J, Madore J, Puiffe ML, Arcand SL, Shen Z, Hébert J, Tonin PN, Provencher DM, Mes-Masson AM, Ouellet, Véronique, Zietarska, Magdalena, Portelance, Lise, Lafontaine, Julie, Madore, Jason, Puiffe, Marie-Line, Arcand, Suzanna L, and Shen, Zhen

Abstract

Background: Cell lines constitute a powerful model to study cancer, and here we describe three new epithelial ovarian cancer (EOC) cell lines derived from poorly differentiated serous solid tumors (TOV-1946, and TOV-2223G), as well as the matched ascites for one case (OV-1946).Methods: In addition to growth parameters, the cell lines were characterized for anchorage independent growth, migration and invasion potential, ability to form spheroids and xenografts in SCID mice.Results: While all cell lines were capable of anchorage independent growth, only the TOV-1946 and OV-1946 cell lines were able to form spheroid and produce tumors. Profiling of keratins, p53 and Her2 protein expression was assessed by immunohistochemistry and western blot analyses. Somatic TP53 mutations were found in all cell lines, with TOV-1946 and OV-1946 harboring the same mutation, and none harbored the commonly observed somatic mutations in BRAF, KRAS or germline BRCA1/2 mutations found to recur in the French Canadian population. Conventional cytogenetics and spectral karyotype (SKY) analyses revealed complex karyotypes often observed in ovarian disease.Conclusion: This is the first report of the establishment of matched EOC cell lines derived from both solid tumor and ascites of the same patient. [ABSTRACT FROM AUTHOR]

Published

2008