Antisense therapy for cancer

ME Gleave, BP Monia - Nature Reviews Cancer, 2005 - nature.com
ME Gleave, BP Monia
Nature Reviews Cancer, 2005nature.com
Improved understanding of the molecular mechanisms that mediate cancer progression and
therapeutic resistance has identified many therapeutic gene targets that regulate apoptosis,
proliferation and cell signalling. Antisense oligonucleotides offer one approach to target
genes involved in cancer progression, especially those that are not amenable to small-
molecule or antibody inhibition. Better chemical modifications of antisense oligonucleotides
increase resistance to nuclease digestion, prolong tissue half-lives and improve scheduling …
Abstract
Improved understanding of the molecular mechanisms that mediate cancer progression and therapeutic resistance has identified many therapeutic gene targets that regulate apoptosis, proliferation and cell signalling. Antisense oligonucleotides offer one approach to target genes involved in cancer progression, especially those that are not amenable to small-molecule or antibody inhibition. Better chemical modifications of antisense oligonucleotides increase resistance to nuclease digestion, prolong tissue half-lives and improve scheduling. Indeed, recent clinical trials confirm the ability of this class of drugs to significantly suppress target-gene expression. The current status and future directions of several antisense drugs that have potential clinical use in cancer are reviewed.
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