Anne Marie Julia scite author profile

Anne Marie Julia

5Publications

37Citation Statements Received

64Citation Statements Given

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Institut Claudius Regaud, Inserm, Hôpital Purpan

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65 and 47 kDa forms of estrogen receptor in human breast cancer: relation with estrogen responsiveness

Jozan

Julia

Carretie

et al. 1991

Breast Cancer Res Tr

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In breast cancer nearly 40% of estrogen receptor (ER) positive patients do not respond to hormone therapy. As several species of ER have been described, we examined 41 breast cancers for: (1) the presence of ER and progesterone receptor (PR); (2) the molecular weight (Mr) of ER; (3) estrogen responsiveness, appreciated by the ability of a piece of tumor transplanted in nude mice to show an estrogen-induced protein synthesis (PR synthesis). We found that there are: two species of ER with different Mr (65 and 47 kDa), and three species of tumors (36% containing the highest form of ER alone, 49% bearing the two components in variable amounts, and 15% bearing only the minor species). Eleven of these 41 tumors could be assayed for PR synthesis induction, showing that estrogen responsiveness is correlated with the major component. Due to the limited number of samples (11) the data are preliminary, but they strongly suggest that the different forms of ER could exist in the living cell with different functional abilities.

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Multidrug resistance circumvention by a new triazinoaminopiperidine derivative S9788 in vitro: definition of the optimal schedule and comparison with verapamil

Julia

Roché²,

Berlion³

et al. 1994

Br J Cancer

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Summary The current work was undertaken to investigate the importance of exposure sequence and duration in achieving the maximum reversal action of S9788 on doxorubicin (DOX) cytotoxicity against cells that exhibit the (MDR) multidrug resistance phenotype: the MCF7/DOX cell line. Accumulation and release of DOX were examined in this cell line. The reversal effect was compared with that obtained with verapamil. S9788 activity was schedule dependent: when comparing incubation with S9788 before or after treatment with DOX, the best reversal factor was obtained in the case of a post-treatment incubation (65.6 ± 7.7 vs 20.8 ± 7.0). S9788 was a more potent modulating agent than verapamil, whatever the schedule of exposure of the cells to the reversal agent. The reversal of resistance after short-term DOX exposures was caused not only by prolonged cellular accumulation of DOX, but also by its prolonged retention after transfer of cells to DOX-free medium. A relationship was noted between cellular exposure to DOX and the cytotoxic effect, and so the reversal of resistance induced by S9788 appears to be directly linked to the level of cell exposure to DOX. This work provided a rationale for improving the schedule of administration of S9788 in clinical trials.

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Modulation of cisplatin cytotoxicity by human recombinant interferon-γ in human ovarian cancer cell lines

Nehmé

Julia

Jozan

et al. 1994

European Journal of Cancer

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Modulation of Cisplatin Cytotoxicity by Human Recombinant Gamma-Interferon in Human Ovarian Cancer Cell Lines

Nehmé¹,

Albin²,

Julia³

et al. 1995

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Mechanism of interaction between cisplatin and human recombinant interferon gamma in human ovarian‐cancer cell lines

Nehmé

Albin

Caliaro

et al. 1995

Intl Journal of Cancer

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Human ovarian carcinoma cells (2008 and its cisplatin-resistant sub-line 2008/C13*) were sensitized to cisplatin by treatment with human recombinant gamma interferon (IFN gamma). IFN gamma produced no significant change in the uptake of CDDP. Exposure of 2008 and 2008/C13* cells to IFN gamma resulted in a time-dependent decrease of cellular glutathione and total glutathione-S-transferase activity, principally the pi isoform. By contrast, the treatment of 2008 and 2008/C13* cell lines with IFN gamma induced rather than suppressed metallothionein IIA mRNA levels. IFN gamma changed neither the formation of total platinum-DNA adducts, nor DNA repair. A significant decrease in c-erbB-2 expression was observed both in sensitive and in resistant cell lines after treatment with IFN gamma, and this decrease was dose-dependent. Our results indicate that the mechanism of IFN gamma-induced sensitization in human ovarian-cancer cell lines is multifactorial.

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Anne Marie Julia

65 and 47 kDa forms of estrogen receptor in human breast cancer: relation with estrogen responsiveness

Multidrug resistance circumvention by a new triazinoaminopiperidine derivative S9788 in vitro: definition of the optimal schedule and comparison with verapamil

Modulation of cisplatin cytotoxicity by human recombinant interferon-γ in human ovarian cancer cell lines

Modulation of Cisplatin Cytotoxicity by Human Recombinant Gamma-Interferon in Human Ovarian Cancer Cell Lines

Mechanism of interaction between cisplatin and human recombinant interferon gamma in human ovarian‐cancer cell lines

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