Your search keyword '"Cianfriglia, M."' showing total 7 results

1. ORIGINAL RESEARCH Saquinavir induces stable and functional expression of the multidrug transporter P-glycoprotein in human CD4 T-lymphoblastoid CEMrev cells.

Author

Dupuis, M.L., Flego, M., Molinari, A., and Cianfriglia, M.

Subjects

LYMPHOBLASTOID cell lines, P-glycoprotein, MULTIDRUG resistance, ENZYME inhibitors, ANTINEOPLASTIC agents

Abstract

The multidrug transporter P-glycoprotein (P-gp) is expressed in HIV-1 target cells, in a range of pharmacological barriers and in AIDS-associated tumours. P-gp substrates include HIV-1 protease inhibitors (PIs) and anticancer drugs, which are efficiently effluxed from multidrug-resistant (MDR) cells. The aim of this study was to investigate the effect on human CD4 T-lymphoblastoid CEMrev cells of saquinavir and other PIs in terms of P-gp expression and to characterize the functional and biochemical patterns of PI-induced P-gp molecules. CEMrev cells no longer expressing detectable amounts of P-gp were cultured for a prolonged period in the presence of 10 μg/mL saquinavir (CEMsaq10) and tested for P-gp expression and function. Subsequently, CEMsaq10 cells were transferred into medium containing 15 μg/mL saquinavir (CEMsaq15) and cultured for several months. These cell lines were continuously monitored for P-gp expression, function and immunochemical patterns. A similar strategy was adopted to determine whether other PIs, such as ritonavir and indinavir, were able to induce P-gp expression in CEMrev cells. Compared with the drug-diluent control, the exposure of CEMrev cells to 10μg/mL saquinavir induced, in a consistent fraction of cells (45–50%), de novo expression of functioning P-gp molecules. The transfer of CEMsaq10 cells to 15μg/mL saquinavir was associated with a dramatic increase in P-gp expression and function (85–90% of CEMsaq15 cells expressed P-gp and effluxed P-gp dye substrates). These saquinavir-induced P-gp molecules included 75-kDa molecules as well as the classical 170-kDa form of P-gp, suggesting induction of a particular isoform of P-gp termed mini-P-glycoprotein. Conversely, ritonavir and indinavir induced transient P-gp expression in a small percentage of the CEMrev cells. Treatment of human CD4 T-lymphoblastoid CEMrev cells with saquinavir caused over-expression of functioning P-gp molecules. This de novo acquired MDR phenotype, which differed from that induced by other PIs, was stable, as expression and activity of P-gp were observed in CEMsaq10 and CEMsaq15 cells during prolonged in vitro culturing, even in drug-free conditions. [ABSTRACT FROM AUTHOR]

Published

2003

2. What is the relationship between P-glycoprotein and adhesion molecule expression in melanoma cells?

Author

Molinari, A., Calcabrini, A., Meschini, S., Marra, M., Stringaro, A., Toccacieli, L., Cianfriglia, M., and Arancia, G.

Published

2002

3. Cytolytically active murine T-cell hybrids.

Author

Nabholz, M., Cianfriglia, M., Acuto, O., Conzelmann, A., Haas, W., Boehmert, H. v., McDonald, H. R., Pohlit, H., and Johnson, J. P.

Published

1980

4. Quercetin potentiates the effect of adriamycin in a multidrug-resistant MCF-7 human breast-cancer cell line: P-glycoprotein as a possible target.

Author

Scambia, G., Ranelletti, F., Panici, P., Vincenzo, R., Bonanno, G., Ferrandina, G., Piantelli, M., Bussa, S., Rumi, C., Cianfriglia, M., Mancuso, S., Ranelletti, F O, Panici, P B, and De Vincenzo, R

Abstract

This study demonstrates that the flavonoid quercetin (Q), a plant-derived compound with low toxicity in vivo, greatly potentiates the growth-inhibitory activity of Adriamycin (ADR) on MCF-7 ADR-resistant human breast cancer cells. The effect of Q was dose-dependent at concentrations ranging between 1 and 10 microM. Since ADR resistance in these cells is associated with the expression of high levels of P-glycoprotein (Pgp), we evaluated the effect of Q and related flavonoids of Pgp activity in cytofluorographic efflux experiments with the fluorescent dye rhodamine 123 (Rh 123). Our results indicate that Q and 3-OMe Q (3',4',7-trimethoxyquercetin) but not the 3-rhamnosylglucoside of Q (rutin) inhibit the Pgp pump-efflux activity in a dose-related manner. Moreover, 10 microM Q reduces the expression of the immunoreactive Pgp in MCF-7 ADR-resistant cells as evaluated by cytofluorimetric assay. In conclusion, these findings provide a further biological basis for the potential therapeutic application of Q as an anti-cancer drug either alone or in combination with ADR in multidrug-resistant breast tumor cells. [ABSTRACT FROM AUTHOR]

Published

1994

5. Expression of lymphocyte homing receptor gene is lost in multi-drug-resistant variants of human T-lymphoblastoid CCRF-CEM cells.

Author

Cianfriglia, M., Yassen, A., Tombesi, M., Samoggia, P., Barca, S., and Caserta, M.

Published

1991

6. Murine monoclonal antibody recognizing a 90-kDa cell-surface determinant selectively lost by multi-drug-resistant variants of cem cells.

Author

Cianfriglia, M., Cenciarelli, C., Tombesi, M., Barca, S., Mariani, M., Morrone, S., Santoni, A., Samoggia, P., Alessio, M., and Malavasi, F.

Published

1990

7. The gene encoding for MC56 determinant (drug-sensitivity marker) is located on the short arm of human chromosome 11.

Author

Cianfriglia, M., Viora, M., Tombesi, M., Merendino, N., Esposito, G., Samoggia, P., Forsberg, U. H., and Schröder, J.

Published

1992