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Targeting human telomerase for cancer therapeutics
Authors:Lionel Guittat  Patrizia Alberti  Dennis Gomez  Anne De Cian  Gaëlle Pennarun  Thibault Lemarteleur  Chafke Belmokhtar  Rajaa Paterski  Hamid Morjani  Chantal Trentesaux  Eliane Mandine  François Boussin  Patrick Mailliet  Laurent Lacroix  Jean-François Riou  Jean-Louis Mergny
Affiliation:(1) Laboratoire de Biophysique, Muséum National d’Histoire Naturelle USM503, INSERM U 565, CNRS UMR 5153, 43, rue Cuvier, 75231 Paris cedex 05, France;(2) Laboratoire d’Onco-Pharmacologie, JE 2428, UFR de Pharmacie,Université de Reims Champagne-Ardenne, 51096 Reims, France;(3) Laboratoire de Radiopathologie, CEA, 92265 Fontenay aux Roses, France;(4) Aventis Pharma SA, Centre de Recherche de Paris, Quai Jules Guesde, 94403 Vitry sur Seine, France
Abstract:The enzyme telomerase is involved in the replication of telomeres, specialized structures that cap and protect the ends of chromosomes. Its activity is required for maintenance of telomeres and for unlimited lifespan, a hallmark of cancer cells. Telomerase is overexpressed in the vast majority of human cancer cells and therefore represents an attractive target for therapy. Several approaches have been developed to inhibit this enzyme through the targeting of its RNA or catalytic components as well as its DNA substrate, the single-stranded 3′-telomeric overhang. Telomerase inhibitors are chemically diverse and include modified oligonucleotides as well as small diffusable molecules, both natural and synthetic. This review presents an update of recent investigations pertaining to these agents and discusses their biological properties in the context of the initial paradigm that the exposure of cancer cells to these agents should lead to progressive telomere shortening followed by a delayed growth arrest response.
Keywords:Apoptosis  Cancer  G-quadruplex ligands  G-quartets  Senescence  Telomerase  Telomere
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