Expression of MDR1/P-glycoprotein,the multidrug resistance protein MRP,and the lung-resistance protein LRP in multiple myeloma |
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Authors: | Schwarzenbach Heidi |
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Affiliation: | (1) Department C on Internal Medicine, Kantonsspital St. Gallen, St. Gallen, Switzerland;(2) IHF Institute for Hormone and Fertility Research, Grandweg 64, 22529 Hamburg, Germany |
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Abstract: | The purpose of this study was to determine the incidence of three genes associated with multidrug resistance (MDR) in multiple myeloma in relation to treatment status. MDR1/Pgp (P-glycoprotein) expression was detected in 41% of 93 myeloma samples. Generally, the incidence of MDR1/Pgp expression was higher in pretreated samples, and treatments with doxorubicin and/or vincristine were more effective in MDR1/Pgp expression than with alkylating agents. A significant association was observed between MDR1/Pgp-positiveness and the ability of verapmil to increase doxorubicin sensitivity, suggesting functional relevance of MDR1/Pgp expression. MRP (multidrug resistance protein) expression was detected in 20.5% of 88 myeloma samples, in 26% at the mRNA level analyzed by quantitative reverse transriptase-polymerase chain reaction, and in only 3 of 79 samples by immunohistochemistry. LRP (lung-resistance protein) protein expression was observed in 12.5% of 72 myeloma samples. MRP and LRP expression was similar in samples with and without prior therapy. Approximately 80% of the myeloma samples with detectable mRNA expression of MDR1 and MRP exhibited low expression levels corresponding to <10% of the Pgp- and MRP-overexpressing multidrug-resistant human myeloma cell lines 8226/Dox6 and 8226/DOXint40c, respectively. Some normal bone marrow samples showed higher levels of MRP mRNA as compared to myeloma specimens, whereas MDR1 mRNA expression in normal bone marrow was much lower (≤ 5%) than that in 8226/Dox6. These findings indicate a requirement to develop single-cell assays for MRP detection in multiple myeloma that are more sensitive than immunohistochemistry and might be useful to evaluate the incidence of genes associated with MDR. |
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Keywords: | Bone marrow BMMCs overexpression RT-PCR doxorubicin verapamil alkylating agents |
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