P-glycoproteins and multidrug resistance

被引：268

作者：

Bellamy, WT

机构：

来源：

ANNUAL REVIEW OF PHARMACOLOGY AND TOXICOLOGY | 1996年 / 36卷

关键词：

cancer; MDR1; P-glycoprotein; MRP; chemosensitization;

D O I：

10.1146/annurev.pa.36.040196.001113

中图分类号：

R9 [药学];

学科分类号：

1007 ;

摘要：

Multidrug resistance represents a major obstacle in the successful therapy of neoplastic diseases. Studies have demonstrated that this form of drug resistance occurs both in cultured tumor cell lines as well as in human cancers. P-glycoprotein appears to play an important role in such cells by acting as an energy-dependent efflux pump to remove various natural product drugs from the cell before they have a chance to exert their cytotoxic effects. Expression of the MDR1 gene product has been associated with a poor prognosis in clinical studies. It has been demonstrated in the laboratory that resistance mediated by the P-glycoprotein may be modulated by a wide variety of compounds. These compounds, which include verapamil and cyclosporin, generally have little or no effect by themselves on the tumor cells, but when used in conjunction with antineoplastic agents, they decrease, and in some instances eliminate, drug resistance. Clinical trials to modulate P-glycoprotein activity are underway at the present time to determine if such strategies will be feasible. Although the P-glycoprotein is expressed in many cell lines and occurs in patient tumors, its expression is not a universal feature of multidrug resistance, suggesting that other mechanisms are operating.

引用

页码：161 / 183

页数：23

共 123 条

[41] THE BIOCHEMISTRY OF P-GLYCOPROTEIN-MEDIATED MULTIDRUG RESISTANCE
ENDICOTT, JA
LING, V
[J]. ANNUAL REVIEW OF BIOCHEMISTRY, 1989, 58 : 137 - 171
[42] ERLICHMAN C, 1993, CANCER RES, V53, P4837
[43] DECREASED NUCLEAR MATRIX DNA TOPOISOMERASE-II IN HUMAN LEUKEMIA-CELLS RESISTANT TO VM-26 AND M-AMSA
FERNANDES, DJ
DANKS, MK
BECK, WT
[J]. BIOCHEMISTRY, 1990, 29 (17) : 4235 - 4241
[44] A MONOCLONAL-ANTIBODY PSEUDOMONAS TOXIN CONJUGATE THAT SPECIFICALLY KILLS MULTIDRUG-RESISTANT CELLS
FITZGERALD, DJ
WILLINGHAM, MC
CARDARELLI, CO
HAMADA, H
TSURUO, T
GOTTESMAN, MM
PASTAN, I
[J]. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1987, 84 (12) : 4288 - 4292
[45] FLENS MJ, 1994, CANCER RES, V54, P4557
[46] ENHANCEMENT BY RECOMBINANT HUMAN INTERFERON-ALFA OF THE REVERSAL OF MULTIDRUG-RESISTANCE BY MRK-16 MONOCLONAL-ANTIBODY
FOGLER, WE
PEARSON, JW
VOLKER, K
ARIYOSHI, K
WATABE, H
RIGGS, CW
WILTROUT, RH
LONGO, DL
[J]. JOURNAL OF THE NATIONAL CANCER INSTITUTE, 1995, 87 (02) : 94 - 104
[47] FORD JM, 1990, PHARMACOL REV, V42, P155
[48] THE LEUKOTRIENE LTD(4) RECEPTOR ANTAGONIST MK571 SPECIFICALLY MODULATES MRP ASSOCIATED MULTIDRUG-RESISTANCE
GEKELER, V
ISE, W
SANDERS, KH
ULRICH, WR
BECK, J
[J]. BIOCHEMICAL AND BIOPHYSICAL RESEARCH COMMUNICATIONS, 1995, 208 (01) : 345 - 352
[49] HOMOLOGY BETWEEN P-GLYCOPROTEIN AND A BACTERIAL HEMOLYSIN TRANSPORT PROTEIN SUGGESTS A MODEL FOR MULTIDRUG RESISTANCE
GERLACH, JH
ENDICOTT, JA
JURANKA, PF
HENDERSON, G
SARANGI, F
DEUCHARS, KL
LING, V
[J]. NATURE, 1986, 324 (6096) : 485 - 489
[50] GERLACH JH, 1986, CANCER SURV, V5, P25

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