A phase I trial of a Bcl-2 antisense (G3139) and weekly docetaxel in patients with advanced breast cancer and other solid tumors

doi:10.1093/annonc/mdh317

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Annals of Oncology 15:1274-1283, 2004
© 2004 European Society for Medical Oncology

A phase I trial of a Bcl-2 antisense (G3139) and weekly docetaxel in patients with advanced breast cancer and other solid tumors

Purpose: Expression of the Bcl-2 protein confers resistanceto various apoptotic signals. G3139 [oblimersen sodium (Genasense^TM)]is a phosphorothioate antisense oligodeoxynucleotide that targetsBcl-2 mRNA, downregulates Bcl-2 protein translation, and enhancesthe antitumor effects of subtherapeutic doses of docetaxel (Taxotere^TM).

Patients and methods: We performed a phase I trial to determinethe maximum tolerated dose (MTD) and safety profile of combinedtherapy with G3139 and weekly docetaxel in patients with advancedBcl-2-positive solid tumors. Cohorts of three to six patientswere enrolled to escalating doses of G3139 and a fixed doseof weekly docetaxel using either of two schedules. In part I,G3139 was administered by continuous infusion for 21 days (D1–22),and docetaxel (35 mg/m²) was given weekly on days 8, 15 and22. In part II, G3139 was given by continuous infusion for 5days before the first weekly dose of docetaxel, and for 48 hbefore the second and third weekly docetaxel doses. For bothschedules, cycles were repeated every 4 weeks.

Results: Twenty-two patients were enrolled. Thirteen patientswere treated on the part I schedule with doses of G3139 escalatedfrom 1 to 4 mg/kg/day. Nine patients were on the part II scheduleof shorter G3139 infusion at G3139 doses of 5–9 mg/kg/day.Hematologic toxicities were mild, except for one case of persistentgrade 3 thrombocytopenia in part I. The most common adverseevents were cumulative fatigue and transaminase elevation, whichprevented further dose escalation beyond 4 mg/kg/day for 21days with the part I schedule. In part II of the study, usingthe abbreviated G3139 schedule, even the highest daily doseswere tolerated without dose-limiting toxicity or the need fordose modification. Objective tumor response was observed intwo patients with breast cancer, including one whose cancerpreviously progressed on trastuzumab plus paclitaxel. Four patientshad stable disease. Pharmacokinetic results for G3139 were similarto those of other trials.

Conclusions: G3139 in combination with standard-dose weeklydocetaxel was well tolerated. The shortened and intermittentG3139 infusion had less cumulative toxicities and still allowedsimilar total G3139 delivery as the longer infusion. Furtherstudies should examine the molecular effect of the regimen,as well as clinical activities in malignancies for which taxanesare indicated.

J. Marshall¹^,*, H. Chen², D. Yang³, M. Figueira¹, K. B. Bouker¹, Y. Ling¹, M. Lippman³, S. R. Frankel⁴ and D. F. Hayes³

¹ Division of Oncology/Hematology, Lombardi Comprehensive Cancer Center, Georgetown University Medical Center, Washington, DC; ² Investigational Drug Branch, Cancer Treatment Evaluation Program, National Cancer Institute, Bethesda, MD; ³ Division of Hematology/Oncology, Department of Medicine, University of Michigan Health System, Ann Arbor, MI; ⁴ Medical Operations, Genta Inc., Berkeley Heights, NJ, USA

^* Correspondence to: Dr J. L. Marshall, Lombardi Comprehensive Cancer Center, 3800 Reservoir Rd NW, Washington, DC 20007, USA. Tel: +1-202-444-7064; Fax: +1-202-444-1229; Email: marshalj{at}georgetown.edu

Key words: advanced breast cancer, Bcl-2, docetaxel, G3139, solid tumors

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