Local Distribution into Brain Tumor and Pharmacokinetics of 4-Pyridoxate Diammine Hydroxy Platinum, a Novel Cisplatin Derivative, after Intracarotid Administration in Rats with 9L Malignant Glioma : Simultaneous Brain Microdialysis Study

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概要

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• Local distribution into brain tumor and the pharmacokinetics of 4-pyridoxate diammine hydroxy platinum (PyPt), a novel cisplatin derivative, were examined using rats implanted with 9L glioma and compared with cisplatin. PyPt (5.0 mg/kg) and cisplatin (3.5 mg/kg) were administered as selective intracarotid infusions for 30 min to the rats. Dialysates from extracellular fluid (ECF) in tumor and non-tumor brain tissues were collected by simultaneous microdialysis. The amount of platinum was determined by atomic absorption spectrophotometry, as representative of the drug administered. Plasma concentration of total and protein unbound platinum, and urinary excretion amount and tissue distribution of total platinum were also determined. Unbound platinum was accumulated preferentially in the brain tumor tissue ECF aftwer administration, while there was little distribution into normal tissue ECF of the brain. In the brain tumor, the values of the unbound platinum AUC and MRT, where AUC is the area under the concentration-time curve and MRT is the mean residence time, for PyPt were 1.7 and 1.3 times larger than with cisplatin, respectively. The brain tumor distribution coefficient (the ratio of brain tumor ECF platinum AUC to plasma protein unbound platinum AUC) for PyPt (0.85) was higher than that for cisplatin (0.69), indicating that the local amount of platinum distributed into the glioma is enhanced by PyPt rather than by cisplatin. The binding to plasma proteins of PyPt (23%) was lower than that of cisplatin (65%). The total platinum concentration in tissues after administration of PyPt was significantly lower than that of cisplatin in the kidney, liver and spleen. In addition, the urinary excretion amount of total platinum after the administration of PyPt was significantly larger than that of cisplatin. These results suggested that PyPt is easily eliminated by rapid urinary excretion because of its reduced interaction with plasma proteins and poor distribution to the kidney or reticuloendothelial tissues such as the liver and spleen.It is concluded that PyPt is an effective cisplatin derivative for the treatment of gliomas with the added advantage of enhancing local distribution of drug into the brain tumor and reducing its accumulation in the kidney, which has previously caused severe nephrotoxicity.

• 公益社団法人日本薬学会の論文
• 2000-12-01

著者

• 中島 幹夫

  佐賀大学医学部附属病院 手術部

• NAKASHIMA Mikiro

  Department of Hospital Pharmacy, Nagasaki University Hospital of Medicine and Dentistry

• SASAKI Hitoshi

  Department of Hospital Pharmacy, Nagasaki University Hospital of Medicine and Dentistry

• Nakashima M

  Dep. Of Clinical Pharmacy Graduate School Of Biomedical Sciences Nagasaki Univ.

• Nakashima Mikiro

  Department Of Hospital Pharmacy Nagasaki University School Of Medicine

• Sasaki H

  Dep. Of Hospital Pharmacy Nagasaki Univ. Hospital

• ICHIKAWA Masataka

  Department of Respiratory Medicine, Graduate School of Medicine, Kyoto University

• Nakano M

  Department Of Laboratory Medicine Nagasaki University School Of Medicine

• Kaminogo Makio

  Department of Neurosurgery, Nagasaki University School of Medicine

• Kaminogo Makio

  長崎大学 医学部脳神経外科学

• Kaminogo Makio

  Department Of Neurosurgery Nagasaki University School Of Medicine

• Shibata S

  Department Of Neurosurgery Nagasaki University School Of Medicine

• Shibata Shobu

  Department Of Neurosurgery Nagasaki University School Of Medicene

• Shibata Shobu

  Department Of Neurosurgery

• Sasaki Hitoshi

  長崎大学 医歯学部病院薬剤部

• Sasaki Hitoshi

  Department Of Basic Pharmaceutics Faculty Of Pharmaceutical Sciences Kyoto University

• Tomiyama Naoki

  武庫川女子大学 薬学研究科

• Tomiyama Naoki

  Departrment Of Neurosurgery University Of The Ryukyus School Of Medicine

• NAKASHIMA Mihoko

  Department of Analytical Research for Pharmacoinformatics, Graduate School of Pharmaceutical Science

• TOKUNAGA Yoshiharu

  Department of Neurosurgery Nagasaki University School of Medicine

• Tomiyama Naoki

  Department Of Hospital Pharmacy Nagasaki University School Of Medicine

• Ichikawa Masataka

  Department Of Hospital Pharmacy Nagasaki University School Of Medicine

• Ichikawa Masataka

  Department Of Pharmacy Nagasaki University Hospital

• Tokunaga Yoshiharu

  Department Of Neurosurgery Nagasaki Prefectural Shimabara Hospital

• Nakashima Mihoko

  Department Of Analytical Research For Pharmacoinformatics Graduate School Of Pharmaceutical Sciences

• ICHIKAWA MASATAKA

  Department of Hospital Pharmacy, Nagasaki University School of Medicine

• Nakashima Mikiro

  Department of Clinical Pharmacy, Graduate School of Biomedical Sciences, Nagasaki University

• ICHIKAWA MASATAKA

  Department of Chemical Engineering, Kyushu University

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