Pharmacokinetic and Pharmacodynamic Analysis of Bis-acetato-ammine-dichloro-cyclohexylamine-platinum(IV) (JM216) Administered Once a Day for Five Consecutive Days: A Phase I Study

doi:10.1093/jjco/hyd102

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Japanese Journal of Clinical Oncology 30:377-384 (2000)
© 2000 Foundation for Promotion of Cancer Research

Pharmacokinetic and Pharmacodynamic Analysis of Bis-acetato-ammine-dichloro-cyclohexylamine-platinum(IV) (JM216) Administered Once a Day for Five Consecutive Days: A Phase I Study

Takayasu Kurata¹, Tomohide Tamura¹, Yasutsuna Sasaki², Hirofumi Fujii², Shunichi Negoro³, Masahiro Fukuoka⁴ and Nagahiro Saijo¹

^,+ ¹Thoracic Oncology Division, National Cancer Center Hospital, Tokyo, ²Division of Oncology and Hematology, National Cancer Center Hospital East, Kashiwa, Chiba, ³Department of Respiratory Medicine and Oncology, Osaka City General Hospital, Osaka and ⁴Fourth Department of Internal Medicine, Kinki University School of Medicine, Osaka, Japan

Background: Bis-acetato-ammine-dichloro-cyclohexylamine-platinum(IV)(JM216) is the first orally given platinum complex that showsin vitro cytotoxicity comparable to that of cisplatin and invivo cytotoxicity superior to those of cisplatin and carboplatin.

Methods: We conducted an escalating-dose (50, 75, 100, 120 mg/m²)phase I study of JM216 administered orally once a day for fiveconsecutive days in patients with solid tumors to establishthe toxicity profile, maximum tolerated dose (MTD) and pharmacokineticprofile. Twenty-three patients were enrolled and all were assessablefor toxicity.

Results: The MTD was 120 mg/m²/day and the dose-limiting toxicitieswere leukopenia, thrombocytopenia, anemia and diarrhea. Becauseof the delayed hematological toxicities, it was difficult torepeat cycles every 26 days in some patients. Tumor shrinkagewas observed in two patients with breast cancer, both of whomwere resistant to doxorubicin. A pharmacokinetic study showedthat the areas under the concentration–time curve (AUC)and peak plasma concentrations (C_max) for total platinum (Pt)on days 1 and 5 and ultrafiltered Pt (UF-Pt) on day 1 increasedin proportion to the dose of JM216. The AUCs for both totaland UF-Pt on day 5 were higher than the AUCs on day 1. The AUCfor UF-Pt on day 5 showed the best correlation with percentagereduction in leukocyte count and in absolute neutrophil count.

Conclusion: The recommended dose for phase II studies is 100mg/m²/day every 4–6 weeks. The observation of tumor shrinkagein previously heavily treated breast cancer patients supportsa phase II investigation.

⁺ For reprints and all correspondence : Takayasu Kurata, ThoracicOncology Division, National Cancer Center Hospital, 1–1,Tsukiji 5-chome, Chuo-ku, Tokyo 104-0045, JapanAbbreviations:MTD, maximum tolerated dose; AUC, area under concentration–timecurve; C_max, peak plasma concentration; Pt, total platinum;UF-Pt, ultrafiltered platinum; CDDP, cis-diammine-dichloro-platinum;CBDCA, cis-diammine-cyclobutane-dicarboxylato-platinum; DLT,dose-limiting toxicity; PS, performance status; WBC, white bloodcell; plt, platelet count; AST, aspartate aminotransferase;ALT, alanine aminotransferase; GCP, Good Clinical Practice;⁵¹Cr-EDTA, chromium-51-edathamil; JCOG, Japan Clinical OncologyGroup; NCI-CTC, National Cancer Institute Common Toxicity Criteria;CR, complete response; PR, partial response; NC, no change;PD, progression disease; AAS, atomic absorption spectrometry;LOQ, lower limit of quantitation; t, half-life; ANC, absoluteneutrophil count; NSCLC, non-small cell lung cancer; pt, patient;BRM, biological response modifier; SD, standard deviation

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