A phase II trial of the epothilone B analog, BMS-247550, in patients with previously treated advanced colorectal cancer

doi:10.1093/annonc/mdh236

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Annals of Oncology 15:928-932, 2004
© 2004 European Society for Medical Oncology

Original Paper

A phase II trial of the epothilone B analog, BMS-247550, in patients with previously treated advanced colorectal cancer

Received 17 February 2004; revised 25 February 2004; accepted 26 February 2004

Background:

The epothilone B analog, BMS-247550, is a non-taxane microtubulin-stabilizingagent with preclinical activity in taxane-resistant cell linesand phase I activity in colorectal cancer. We conducted a phaseII study of single-agent BMS-247550 in advanced colorectal cancerpatients who had disease progression following treatment withirinotecan–5-fluorouracil–leucovorin (IFL).

Patients and methods:

Patients were required to have histologically or cytologicallyconfirmed advanced or metastatic colorectal cancer; progressedon or after chemotherapy with IFL; Eastern Cooperative OncologyGroup performance status $≤$ 1; peripheral neuropathy grade $≤$ 1; andadequate laboratory parameters. BMS-247550 40mg/m² was administered intravenously over 3 h every 3 weeks.Patients were evaluated for response every 6 weeks.

Results:

Twenty-five patients were enrolled; all were evaluable for toxicityand 23 were evaluable for response. There were no complete orpartial responses. Thirteen patients (56%) had stable diseaseafter two cycles of therapy; five patients (20%) received sixor more cycles. The median time to progression was 11 weeks; median overall survival was 36 weeks. Therewas considerable grade 3/4 hematological toxicity, includingneutropenia (48%) and leukopenia (36%). Grade 3/4 non-hematologicaltoxicities included grade 3 hypersensitivity reaction (12%)and peripheral neuropathy (20%).

Conclusions:

Single-agent BMS-247550 (40 mg/m²) administered every 21 daysdemonstrated no activity in advanced colorectal cancer. Peripheralneuropathy was treatment-limiting.

C. Eng¹^,*, H. L. Kindler¹, S. Nattam³, R. H. Ansari⁴, K. Kasza², K. Wade-Oliver¹ and E. E. Vokes¹

¹ Department of Medicine, Section of Hematology/Oncology and ² Department of Health Studies, University of Chicago, Chicago, IL; ³ Fort Wayne Medical Center, Fort Wayne, IN; ⁴ Northern Indiana Cancer Research Consortium, South Bend, IN, USA

Key words: colorectal cancer, epothilone, phase II trial

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