Topoisomerase I inhibitors: camptothecins and beyond

Topoisomerase I inhibitors: camptothecins and beyond

Key Points Topoisomerase I (TOP1) enzymes are essential in higher eukaryotes, as they are required to relax DNA supercoiling generated by transcription, replication and chromatin remodelling. Topoisomerases are particularly vulnerable to topoisomerase I inhibitors during their cleavage reaction, whi...

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Veröffentlicht in:Nature reviews. Cancer 2006-10, Vol.6 (10), p.789-802
1. Verfasser: Pommier, Yves
Format: Artikel
Sprache:eng
Schlagworte:
Adducts
Antimitotic agents
Antineoplastic agents
Antineoplastic Agents - pharmacology
Antineoplastic drugs
Antitumor agents
Apoptosis
Biomedical and Life Sciences
Biomedicine
Camptothecin
Camptothecin - pharmacology
Cancer Research
Chromatin remodeling
Colorectal carcinoma
Control
Cytotoxicity
Deoxyribonucleic acid
DNA
DNA biosynthesis
DNA Damage
DNA Repair
DNA Replication
DNA topoisomerase
DNA topoisomerase I
Dosage and administration
Enzyme Inhibitors - pharmacology
Enzymes
Humans
Intermediates
Irinotecan
Macromolecules
Natural products
Neoplasms - drug therapy
Neoplasms - enzymology
Neoplasms - genetics
Phenanthridine
Physiological aspects
Replication
review-article
Supercoiling
Topoisomerase I Inhibitors
Topotecan
Tumors
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Zusammenfassung:Key Points Topoisomerase I (TOP1) enzymes are essential in higher eukaryotes, as they are required to relax DNA supercoiling generated by transcription, replication and chromatin remodelling. Topoisomerases are particularly vulnerable to topoisomerase I inhibitors during their cleavage reaction, which is referred to as the 'cleavage complex'. TOP1 can be trapped by anticancer drugs as it cleaves DNA. Moreover, TOP1 can be trapped by endogenous alterations to DNA (mismatches, abasic sites, nicks and adducts) and apoptotic alterations to chromatin. Camptothecin is a natural product of which TOP1 is the only cellular target. Two camptothecin derivatives have recently been approved by the US Food and Drug Administration: topotecan for ovarian and lung cancers and irinotecan for colorectal cancer. Various non-camptothecin inhibitors of TOP1 are in development, including indolocarbazole, phenanthridine and indenoisoquinoline derivatives. Non-camptothecins are expected to be active in cancers that are currently resistant to camptothecins, and to have a greater therapeutic index. Co-crystal structures of TOP1 inhibitors illustrate the interfacial inhibition paradigm by which a small drug molecule can trap conformational intermediates of macromolecular complexes (in the case of TOP1 inhibitors, the TOP1 enzyme and its cleaved DNA substrate). The cytotoxic activity of TOP1 inhibitors is related to the interference of trapped TOP1 cleavage complexes with DNA replication and transcription. Deficiencies in both the checkpoint and DNA-repair pathways determine cellular sensitivity to TOP1 inhibitors. Therefore, the identification of such deficiencies in tumours should guide the rational use of TOP1 inhibitors. Targeting checkpoint and repair pathways should also increase the selectivity of TOP1 inhibitors in tumours that have pre-existing deficiencies in relevant redundant pathways. Nuclear DNA topoisomerase I (TOP1) is an essential human enzyme, and is the only known target of the camptothecin and its derivatives. The mechanisms and molecular determinants of the tumour response to TOP1 inhibitors are reviewed in the context of developing camptothecin and non-camptothecin derivatives that further increase anti-tumour activity but also reduce side effects. Nuclear DNA topoisomerase I (TOP1) is an essential human enzyme. It is the only known target of the alkaloid camptothecin, from which the potent anticancer agents irinotecan and topotecan are derived. As camptothecins
ISSN:1474-175X
1474-1768
DOI:10.1038/nrc1977