Phase I and Pharmacokinetic Study of PKC412, an Inhibitor of Protein Kinase C

医学 恶心 呕吐 腹泻 胃肠病学 药代动力学 内科学 毒性 中性粒细胞减少症
作者
David Propper,A. C. McDonald,A. Man,P. Thavasu,Frances R. Balkwill,J P Braybrooke,F. Caponigro,P. Graf,C. Dutreix,R. Blackie,Stan B. Kaye,Trivadi S. Ganesan,Denis C. Talbot,Adrian L. Harris,Chris Twelves
出处
期刊:Journal of Clinical Oncology [Lippincott Williams & Wilkins]
卷期号:19 (5): 1485-1492 被引量:209
标识
DOI:10.1200/jco.2001.19.5.1485
摘要

N-Benzoyl staurosporine (PKC412) is a protein kinase C inhibitor with antitumor activity in laboratory models. We determined the toxicity of oral PKC412 administered daily for repeat cycles of 28 days.Thirty-two patients with advanced solid cancers were treated at seven dose levels (12.5 to 300 mg daily) for a total of 68 cycles.The most frequent treatment-related toxicities were nausea, vomiting, fatigue, and diarrhea. At the two top dose levels (225 and 300 mg/d), 15 of 16 patients experienced nausea/vomiting (common toxicity criteria [CTC], version 1), grade 2 in nine of 16 and grade 3 in three of 16 patients; and six of 16 patients developed CTC grade 2 diarrhea. After 1 month of treatment, there were significant reductions in circulating lymphocyte (P <.02) and monocyte (P <.01) counts in patients receiving doses > or = 100 mg/d. Nevertheless, only two patients developed myelosuppression (both grade 2). Of two patients with progressive cholangiocarcinoma, one attained stable disease lasting 4.5 months and one a partial response lasting 4 months. There was a linear relationship between PKC412 dose and area under the curve (0-24 hours) and maximum plasma concentration with marked interpatient variability. The estimated median elimination half-life was 1.6 days (range, 0.9 to 4.0 days), and a metabolite with a median half-life of 36 days was detected. Steady-state PKC412 plasma levels at the top three dose cohorts (150 to 300 mg) were five to 10 times the cellular 50% inhibitory concentration for PKC412 of 0.2 to 0.7 micromol/L.PKC412 can be safely administered by chronic oral therapy, and 150 mg/d is suitable for phase II studies. The pharmacokinetics and lack of conventional toxicity indicate that pharmacodynamic measures may be additionally needed to optimize the drug dose and schedule.

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