loading page

Oral paclitaxel with encequidar compared to intravenous paclitaxel in patients with advanced cancer: a randomised crossover pharmacokinetic study.
  • +15
  • Christopher Jackson,
  • Tak Hung,
  • Eva Segelov,
  • Paula Barlow,
  • Hans Prenen,
  • Blair McLaren,
  • Noelyn Hung,
  • Katriona Clarke,
  • Tsu-Yi Chao,
  • Ming-Shen Dai,
  • Hsien-Tang Yeh,
  • David Cutler,
  • Douglas Kramer,
  • Jimmy He,
  • Jay Zhi,
  • Wing-Kai Chan,
  • Rudolf Kwan,
  • Sanjeev Deva
Christopher Jackson
University of Otago Medical School

Corresponding Author:[email protected]

Author Profile
Tak Hung
Zenith Technology Corporation Limited
Author Profile
Eva Segelov
Monash University
Author Profile
Paula Barlow
Auckland District Health Board
Author Profile
Hans Prenen
University Hospital Antwerp
Author Profile
Blair McLaren
Southern District Health Board
Author Profile
Noelyn Hung
University of Otago
Author Profile
Katriona Clarke
Capital and Coast District Health Board
Author Profile
Tsu-Yi Chao
Taipei Medical University
Author Profile
Ming-Shen Dai
Tri-Service General Hospital
Author Profile
Hsien-Tang Yeh
Lo-Hsu Medical Foundation Lotung Poh-Ai Hospital
Author Profile
David Cutler
Athenex Inc
Author Profile
Douglas Kramer
Athenex Inc
Author Profile
Jimmy He
Athenex Inc
Author Profile
Jay Zhi
Athenex Inc
Author Profile
Wing-Kai Chan
Athenex Inc
Author Profile
Rudolf Kwan
Athenex Inc
Author Profile
Sanjeev Deva
Auckland District Health Board
Author Profile

Abstract

Background and purpose: Paclitaxel is a widely used anti-neoplastic agent but has low oral bioavailability due to gut extrusion by P-glycoprotein (P-gp). Oral paclitaxel could be more convenient, less resource intensive, and more tolerable than intravenous administration. Encequidar (HM30181A) is a novel, minimally absorbed gut specific P-gp inhibitor. We tested whether administration of oral paclitaxel with encequidar (oPac+E) achieved comparable AUC to intravenous paclitaxel (IVP) 80mg/m2. Experimental approach: We conducted a multi-centre randomised crossover study with two treatment periods. Patients (pts) with advanced cancer received either oral paclitaxel 615mg/m2 divided over three days and encequidar 15mg orally one-hour prior, followed by IVP 80mg/m2, or the reverse sequence. PK blood samples were taken up to day 9 for oPac+E and day 5 for IVP. Key Results: 42 pts were enrolled; 35 completed both treatment periods. AUC0-∞was 5033.5 +/- 1401.1 ng.h/mL for oPac+E and 5595.9 +/- 1264.1 ng.h/mL with IVP. The geometric mean ratio (GMR) for AUC was 89.5% (90% CI 83.9-95.5). Mean absolute bioavailability of oPac+E was 12%. PK parameters did not change meaningfully after 4 weeks administration of oPac+E in an extension study. G3 treatment emergent adverse events occurred in 7 (18%) pts with oPac+E and 2 (5%) with IVP. 75% of pts preferred oPac+E over IVP. Conclusion and Implications: GMR for AUC was within the predefined acceptable range of 80%-125% for demonstrating equivalence. oPac+E is tolerable and there is no evidence of P-gp induction with repeat administration. With further study, oPac+E is a candidate to replace IVP.
Dec 2021Published in British Journal of Clinical Pharmacology volume 87 issue 12 on pages 4670-4680. 10.1111/bcp.14886