BaseSpace
Correlation Engine 2.0
Import Your Data
Literature

FAQ

More FAQs

Back to top
Clear Search sequence regions
(e.g. EGFR, calcium channel activity, Hepatitis, Pancreas, Autoimmunity, Ciprofibrate)
Bookmark Forward

Enhanced delivery of cisplatin to intraperitoneal ovarian carcinomas mediated by the effects of bortezomib on the human copper transporter 1.

Danielle D Jandial, Salman Farshchi-Heydari, Christopher A Larson, Gregory I Elliott, Wolfgang J Wrasidlo, Stephen B Howell

Clinical cancer research : an official journal of the American Association for Cancer Research 2009 Jan 15


filter terms:
  • alleles (1)
  • bortezomib (13)
  • cation transport proteins (2)
  • cell kill (1)
  • cisplatin (11)
  • CTR1 (6)
  • female (1)
  • gene (1)
  • hCTR1 (5)
  • human (3)
  • human cells (1)
  • mice (1)
  • mice nude (1)
  • ovarian cancer (2)
  • ovarian carcinomas (2)
  • ovarian neoplasms (1)
  • plasma (2)
  • platinum (4)
  • protein human (1)
  • pyrazines (2)
  • slc31a1 protein, human (1)
  • western blot (1)
    • Sizes of these terms reflect their relevance to your search.

    The copper transporter 1 (CTR1) is a major influx transporter for platinum drugs. However, the accumulation of cisplatin in human ovarian carcinoma cells is limited by the fact that cisplatin triggers the down-regulation and proteasomal degradation of CTR1, thereby limiting its own uptake. We sought to determine whether proteasome inhibition using bortezomib would prevent human CTR1 (hCTR1) degradation and increase platinum accumulation in ovarian cancer cells. The effects of bortezomib on human hCTR1 expression and cisplatin accumulation were measured by Western blot, flow cytometric, and confocal digital imaging analyses. Platinum accumulation was measured by inductively coupled plasma mass spectrometry and bortezomib concentrations by liquid chromatography/mass spectrometry. Bortezomib blocked the cisplatin-induced down-regulation of hCTR1 in a concentration-dependent manner and increased cisplatin uptake 1.6- to 2.4-fold. Median effect analysis showed a combination index of 0.37 at 50% cell kill, indicating a high level of synergy. The effect of bortezomib was muted in cells lacking both alleles of CTR1, showing that bortezomib was working primarily through its effect on blocking hCTR1 degradation. I.p. administration of bortezomib produced a peritoneal/plasma area under the curve ratio of 252 in a murine model. I.p. administration of bortezomib before i.p. cisplatin increased platinum accumulation in peritoneal tumors by 33% (P = 0.006). Proteasomal inhibition prevented cisplatin-induced down-regulation of hCTR1 in ovarian cancer cells and enhanced drug uptake and cell killing in a synergistic manner. Bortezomib shows a large pharmacologic advantage when administered i.p. There is a strong rationale for the combined i.p. administration of bortezomib and cisplatin.

    Citation

    Danielle D Jandial, Salman Farshchi-Heydari, Christopher A Larson, Gregory I Elliott, Wolfgang J Wrasidlo, Stephen B Howell. Enhanced delivery of cisplatin to intraperitoneal ovarian carcinomas mediated by the effects of bortezomib on the human copper transporter 1. Clinical cancer research : an official journal of the American Association for Cancer Research. 2009 Jan 15;15(2):553-60

    Expand section icon Mesh Tags

    Expand section icon Substances


    PMID: 19147760

    View Full Text
    • Copyright © 2024 Illumina Inc. All rights reserved.