Pharmacokinetical Comparison of Anticancer Drugs in Cerebrospinal Fluid during Cerebrospinal Fluid Perfusion and Injection Chemotherapy
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概要
- 論文の詳細を見る
The present study examined the pharmacokinetics of anticancer drugs in the cerebrospinal fluid (CSF) during CSF perfusion or injection chemotherapy. A 69-year-old Japanese woman with disseminated glioblastoma received one course of both ventricular-lumbar (V-L) and lumbar-ventricular (L-V) CSF perfusion chemotherapy, and one course of both ventricular and lumbar injection chemotherapy with methotrexate (MTX), cytosine arabinoside (Ara-C), and nimustine (ACNU). Samples of CSF from the ventricles and lumbar spinal canal were obtained via the Ommaya reservoirs. The drug concentrations in the CSF were measured by either fluorescence polarization immunoassay or high performance liquid chromatography. In the V-L CSF perfusion chemotherapy, the maximum CSF concentrations of the three drugs in the lumbar spinal canal were lower than those in the ventricles. However, the concentrations of MTX and Ara-C in the lumbar spinal canal exceeded those in the ventricles 3 hours after the perfusion. The area under the CSF concentration versus the time curves (AUC) of MTX and Ara-C in the lumbar spinal canal were 175.7 and 76.2%, respectively, of those in the ventricles. In the L-V CSF perfusion chemotherapy, the CSF concentrations of the three drugs in the lumbar spinal canal were higher than those in the ventricle. The AUC_S of MTX and Ara-C in the ventricles were 15.5 and 18.4 %, respectively, of those in the lumbar spinal canal. In the ventricular CSF injection, the initial CSF concentrations of the three drugs in the ventricles were higher than those in the lumbar spinal canal. However, the CSF concentrations of MTX and Ara-C in the lumbar spinal canal exceeded those in the ventricles 12 hours after the injection. Although the concentration of ACNU in the ventricles was only detectable at 3 hours after the injection, no concentration in the lumbar spinal canal was detectable. The AUCS of MTX and Ara-C in the lumbar spinal canal were 84.6 and 29.l%, respectively, of those in the ventricles. In the lumbar CSF injection, the CSF concentrations of MTX and Ara-C in the ventricles were detectable but lower than those in the lumbar. Although the CSF concentration of ACNU in the lumbar spinal canal was only detect-able at 3 hours after the injection, no concentration in the ventricles was detectable. The AUC of MTX in the ventricles was 0.31% of that in the lumbar spinal canal. These results indicate that CSF perfusion chemotherapy may thus be a more useful treatment than CSF injection chemotherapy to patients with disseminated brain tumors.
- 日本医療薬学会の論文
- 1999-08-10
著者
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Hori S
Kyoto Pharmaceutical Univ. Kyoto Jpn
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Hori Shigeaki
Department Of Neurosurgery Oita Medical University
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TAKEYAMA MASAHARU
Department of Anesthesiology and Critical Care Medicine, Kagoshima University School of Medicine
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MORIKAWA Norifumi
Department of Clinical Pharmacotherapy, Division of Clinical Pharmacotherapeutics, Graduate School o
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MORI Teruaki
Department of Neurosurgery, Oita Medical University
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ABE Tatsuya
Department of Neurosurgery, Oita Medical University
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KAWASHIMA Hisanori
Department of Clinical Pharmacy, Oita Medical University
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FUJIKI MINORU
Department of Neurosurgery Oita Medical University
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Abe T
Tokyo Univ. Pharmacy & Life Sci. Tokyo Jpn
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Abe Tatsuya
Department Of Neurosurgery Oita University School Of Medicine
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Takeyama Masaharu
Department Of Anesthesiology And Critical Care Medicine Kagoshima University School Of Medicine
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Takeyama M
Oita Univ. Hospital
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Mori Teruaki
Neurosurgery Oita Medical University
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Mori Teruaki
Department Of Neurosurgery Oita Medical University
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Hori Shigeaki
Department Of Neurosurgery Medical College Of Oita
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Fujiki Minoru
Department Of Neurosurgery Medical College Of Oita
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Kawashima H
Department Of Clinical Pharmacy Oita Medical University
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Kawashima Hisanori
Department Of Clinical Pharmacy Oita Medical University
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Morikawa Norifumi
Department Of Clinical Pharmacotherapy Graduate School Of Biomedical Sciences Hiroshima University
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Morikawa N
Department Of Clinical Pharmacotherapy Hiroshima University
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Abe Tatsuya
Department Of Biochemistry Kyushu University School Of Medicine
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HORI SHIGEAKI
Department of Neurosurgery, Oita Medical University
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Mori Teruaki
Department of Neurology, Nishibeppu National Hospital
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