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Perspective
Nature Biotechnology  22, 1533 - 1537 (2004)
Published online: 6 December 2004; | doi:10.1038/nbt1042


There is a Corrigenda (January 2005) associated with this Perspective.

Antisense and siRNA as agonists of Toll-like receptors

Sudhir Agrawal & Ekambar R Kandimalla

Hybridon, Inc., 345 Vassar Street, Cambridge, Massachusetts 02139, USA.

Correspondence should be addressed to Sudhir Agrawal sagrawal@hybridon.com
About 25 years ago, researchers first demonstrated that a short synthetic oligodeoxynucleotide, referred to as antisense, can inhibit replication of Rous sarcoma virus through hybridization to viral RNA. Since then, several hybridization-based oligonucleotide approaches have been developed to elucidate the functions of genes and their potential as therapeutic agents. Short-interfering (si) RNA is the most recent example. To effectively inhibit gene expression, an antisense or siRNA must be resistant to nucleases, be taken up efficiently by cells, hybridize efficiently with the target mRNA and activate selective degradation of the target mRNA or block its translation without causing undesirable side effects. However, both antisense and siRNA agents have been shown to exert non-target-related biological effects including immune stimulation. Do antisense and siRNA agents work as ligands for Toll-like receptors (TLRs), a family of pathogen-associated, molecular pattern recognition receptors?

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Nature Biotechnology News and Views (01 Jan 2004)

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Nature Biotechnology
ISSN: 1087-0156
EISSN: 1546-1696
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