Intravenous Cereport (RMP-7) Enhances Delivery of Hydrophilic Chemotherapeutics and Increases Survival in Rats with Metastatic Tumors in the Brain |
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Authors: | Emerich Dwaine F Dean Reginald L Marsh JoAnne Pink Melissa Lafreniere Denise Snodgrass Pamela Bartus Raymond T |
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Affiliation: | (1) Alkermes, Inc., Cambridge, Massachusetts;(2) Department of Pharmacology, Alkermes, Inc., 64 Sidney Street, Cambridge, Massachusetts, 02139;(3) Department of Pharmacology and Experimental Therapeutics, Tufts University Medical Center, Boston, Massachusetts |
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Abstract: | Purpose. The following experiments determined whether intravenous infusions of Cereport enhance delivery of chemotherapeutics and prolong survival in rats with metastatic tumors in the brain.Methods. Autoradiography and scintillation were used to examine uptake of the lipophilic (paclitaxel and carmustine) and the hydrophilic (carboplatin) chemotherapeutic agents, as well as the large hydrophilic marker, 70 kDa dextran. Cereport was also tested in combination with the chemotherapeutic drugs carboplatin, vinorelbine, gemcitabine and carmustine to determine if Cereport could enhance the survival benefit beyond that provided by chemotherapy alone.Results. Cereport enhanced the uptake of carboplatin and dextran, but not paclitaxel or carmustine. The pattern of Cereport's uptake effect with carboplatin revealed that Cereport selectively increased the proportion of highly permeable regions. Survival was significantly enhanced when Cereport was combined with either carboplatin, vinorelbine, or gemcitabine, but not carmustine, compared to each chemotherapeutic agent alone.Conclusions. These data provide the first evidence that Cereport, or any receptor-mediated approach intended to enhance the permeability of the blood-brain tumor barrier, can increase the delivery hydrophilic drugs to metastatic tumors in the brain, increasing survival in tumor-bearing rats. |
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Keywords: | blood-brain tumor barrier bradykinin brain metastases carboplatin carmustine paclitaxel vinorelbine gemcitabine |
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