BaseSpace
Correlation Engine 2.0
Import Your Data
Literature

FAQ

More FAQs

Back to top
Clear Search sequence regions
(e.g. Leukemia, Adipose tissue, Amniocentesis, Rosiglitazone, rs2476601, LEP, Apoptosis)
Bookmark Forward

Next generation topoisomerase I inhibitors: Rationale and biomarker strategies.

Beverly A Teicher

Genzyme Corporation, 1 Mountain Road, Framingham, MA 01701-9322, USA.

Biochemical pharmacology 2008 Mar 15


filter terms:
  • a gene (1)
  • animals (1)
  • antineoplastic agents (2)
  • arc 111 (1)
  • biological markers (2)
  • camptothecin (6)
  • carbazoles (2)
  • cells (1)
  • clinical trial (2)
  • diflomotecan (1)
  • dna (4)
  • dna break (2)
  • dna cleavage (1)
  • dna replication (1)
  • drug targeting (1)
  • edotecarin (2)
  • gimatecan (2)
  • H2AX (1)
  • homocamptothecin (2)
  • humans (1)
  • indenes (2)
  • indoles (2)
  • irinotecan (1)
  • isoquinolines (2)
  • lactone (2)
  • naphthyridines (2)
  • nsc 314622 (1)
  • patient (1)
  • ring- forms (1)
  • selection patients (1)
  • st 1481 (1)
  • strand break (1)
  • therapy (1)
  • TopoI (9)
  • topoi inhibitor (5)
  • topoisomerase i inhibitors (3)
  • topotecan (2)
    • Sizes of these terms reflect their relevance to your search.

    Topoisomerase I (TopoI), an essential enzyme, produces a DNA single strand break allowing DNA relaxation for replication. The enzymatic mechanism involves sequential transesterifcations. The breakage and closure reactions generate phosphodiester bonds and similar free energies, so the reaction is freely reversible. The TopoI reaction intermediate consists of enzyme covalently linked to DNA dubbed a 'cleavable complex'. Covalently bound TopoI-DNA complexes can be recovered. Camptothecin analogs, topotecan and irinotecan, are approved TopoI-targeted drugs. Both have limitations due to the equilibrium between the camptothecin lactone and ring-opened forms. Several strategies are being explored to develop improved TopoI inhibitors. Homocamptothecins, in which the metabolically labile camptothecin lactone is replaced with a more stable seven-membered beta-hydroxylactone, are potent anticancer agents. Gimatecan is a seven-position modified lipophilic camptothecin developed to provide rapid uptake and accumulation in cells and a stable TopoI-DNA-drug ternary complex. Diflomotecan, a homocamptothecin, and gimatecan are in Phase II clinical trial. Among non-camptothecins, edotecarin, an indolocarbazole that results in DNA C/T-G cleavage compared with T-G/A for camptothecins, is in Phase II clinical trial. Indenoisoquinolines were identified as TopoI inhibitors by the NCI 60-cell line COMPARE analysis. Co-crystal structures of two indenoisoquinolines with TopoI-DNA elucidated the structure of the ternary complex. Indenoisoquinolines are in preclinical development. Dibenzonaphthyridinone TopoI inhibitors have undergone extensive structure-activity examination. ARC-111 was selected for in-depth preclinical study. Biomarkers are under investigation to predict clinical efficacy from preclinical models, to allow determination of drug targeting in vivo and to aid selection of patients most likely to benefit from TopoI inhibitor therapy. gamma-H2AX formation may be a useful pharmacodynamic marker. A gene signature developed for topotecan sensitivity/resistance may have value in patient identification. Convergence of these efforts should result in clinically effective second generation TopoI inhibitors.

    Citation

    Beverly A Teicher. Next generation topoisomerase I inhibitors: Rationale and biomarker strategies. Biochemical pharmacology. 2008 Mar 15;75(6):1262-71

    Expand section icon Mesh Tags

    Expand section icon Substances


    PMID: 18061144

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