Cancer Chemother Pharmacol. 2017 Jan;79(1):9-16. doi: 10.1007/s00280-016-3193-5. Epub 2016 Nov 19.

Efficacy and safety of nab-paclitaxel in patients with previously treated metastatic colorectal cancer: a phase II COLO-001 trial.

Ducreux M^1,², Bennouna J³, Adenis A⁴, Conroy T⁵, Lièvre A^6,⁷, Portales F⁸, Jeanes J⁹, Li L⁹, Romano A¹⁰.

Author information

1: Gustave Roussy, Cancer Campus Grand Paris, Villejuif, France. Michel.DUCREUX@gustaveroussy.fr.
2: Université Paris-Saclay, Saclay, France. Michel.DUCREUX@gustaveroussy.fr.
3: Institut de Cancérologie de l'Ouest, Site Hospitalier Nord, Saint-Herblain, France.
4: Centre Oscar Lambret, Lille, France.
5: Institut de Cancérologie de Lorraine, Vandœuvre-lès-Nancy, France.
6: Institut Curie, Hôpital René Huguenin, Saint Cloud, France.
7: CHU Pontchaillou, Rennes, France.
8: Institut du Cancer de Montpellier, Montpellier, France.
9: Celgene Corporation, 86 Morris Avenue, Summit, NJ, USA.
10: Celgene International Sàrl, Boudry, Switzerland.

Abstract

PURPOSE:

This single-arm, phase II trial evaluated nab-paclitaxel monotherapy in pretreated patients with metastatic colorectal cancer (mCRC).

METHODS:

Patients with mCRC (RAS wild-type and RAS mutant cohorts) received nab-paclitaxel 125 mg/m² days 1, 8, and 15 (28-day cycle). The primary endpoint was investigator-assessed progression-free survival (PFS) rate at week 8; secondary endpoints included overall survival, overall response rate, and safety. Stage 1 planned enrollment was 15 patients per cohort per Simon 2-stage design. Stage 2 enrollment was to continue unless ≤8 of the first 15 patients per cohort achieved PFS at 8 weeks.

RESULTS:

Stage 1 enrolled 41 patients (RAS wild type: n = 18; RAS mutant: n = 23). In both RAS cohorts, 3 of 15 patients initially enrolled were progression-free at week 8 (20%; 95% CI 4.0-48.0). Median PFS was 8.1 weeks (95% CI 7.7-8.6) and 7.9 weeks (95% CI 7.6-8.0) for RAS wild-type and RAS mutant cohorts, respectively. There were no complete or partial responses. The overall disease control rate was 16% (95% CI 6.0-32.0), and rates were similar in the RAS wild-type and RAS mutant cohorts (18 and 15%, respectively). No new safety signals were reported; the most common grade ≥3 adverse events included neutropenia, asthenia, and peripheral neuropathy. This study did not progress to stage 2 per the preplanned statistical stopping rule.

CONCLUSIONS:

In patients with heavily pretreated mCRC, nab-paclitaxel did not demonstrate promising antitumor activity; further assessment of nab-paclitaxel monotherapy in this population of patients is not supported.