Increased antitumor activity, intratumor paclitaxel concentrations, and endothelial cell transport of cremophor-free, albumin-bound paclitaxel, ABI-007, compared with …
N Desai, V Trieu, Z Yao, L Louie, S Ci, A Yang… - Clinical cancer research …, 2006 - AACR
N Desai, V Trieu, Z Yao, L Louie, S Ci, A Yang, C Tao, T De, B Beals, D Dykes, P Noker…
Clinical cancer research: an official journal of the American Association for …, 2006•AACRAbstract ABI-007, an albumin-bound, 130-nm particle form of paclitaxel, was developed to
avoid Cremophor/ethanol-associated toxicities in Cremophor-based paclitaxel (Taxol) and
to exploit albumin receptor-mediated endothelial transport. We studied the antitumor activity,
intratumoral paclitaxel accumulation, and endothelial transport for ABI-007 and Cremophor-
based paclitaxel. Antitumor activity and mortality were assessed in nude mice bearing
human tumor xenografts [lung (H522), breast (MX-1), ovarian (SK-OV-3), prostate (PC-3) …
avoid Cremophor/ethanol-associated toxicities in Cremophor-based paclitaxel (Taxol) and
to exploit albumin receptor-mediated endothelial transport. We studied the antitumor activity,
intratumoral paclitaxel accumulation, and endothelial transport for ABI-007 and Cremophor-
based paclitaxel. Antitumor activity and mortality were assessed in nude mice bearing
human tumor xenografts [lung (H522), breast (MX-1), ovarian (SK-OV-3), prostate (PC-3) …
Abstract
ABI-007, an albumin-bound, 130-nm particle form of paclitaxel, was developed to avoid Cremophor/ethanol-associated toxicities in Cremophor-based paclitaxel (Taxol) and to exploit albumin receptor-mediated endothelial transport. We studied the antitumor activity, intratumoral paclitaxel accumulation, and endothelial transport for ABI-007 and Cremophor-based paclitaxel. Antitumor activity and mortality were assessed in nude mice bearing human tumor xenografts [lung (H522), breast (MX-1), ovarian (SK-OV-3), prostate (PC-3), and colon (HT29)] treated with ABI-007 or Cremophor-based paclitaxel. Intratumoral paclitaxel concentrations (MX-1-tumored mice) were compared for radiolabeled ABI-007 and Cremophor-based paclitaxel. In vitro endothelial transcytosis and Cremophor inhibition of paclitaxel binding to cells and albumin was compared for ABI-007 and Cremophor-based paclitaxel. Both ABI-007 and Cremophor-based paclitaxel caused tumor regression and prolonged survival; the order of sensitivity was lung > breast congruent with ovary > prostate > colon. The LD(50) and maximum tolerated dose for ABI-007 and Cremophor-based paclitaxel were 47 and 30 mg/kg/d and 30 and 13.4 mg/kg/d, respectively. At equitoxic dose, the ABI-007-treated groups showed more complete regressions, longer time to recurrence, longer doubling time, and prolonged survival. At equal dose, tumor paclitaxel area under the curve was 33% higher for ABI-007 versus Cremophor-based paclitaxel, indicating more effective intratumoral accumulation of ABI-007. Endothelial binding and transcytosis of paclitaxel were markedly higher for ABI-007 versus Cremophor-based paclitaxel, and this difference was abrogated by a known inhibitor of endothelial gp60 receptor/caveolar transport. In addition, Cremophor was found to inhibit binding of paclitaxel to endothelial cells and albumin. Enhanced endothelial cell binding and transcytosis for ABI-007 and inhibition by Cremophor in Cremophor-based paclitaxel may account in part for the greater efficacy and intratumor delivery of ABI-007.
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