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Home: Papers of the Week
Annotation


Soutschek J, Akinc A, Bramlage B, Charisse K, Constien R, Donoghue M, Elbashir S, Geick A, Hadwiger P, Harborth J, John M, Kesavan V, Lavine G, Pandey RK, Racie T, Rajeev KG, Röhl I, Toudjarska I, Wang G, Wuschko S, Bumcrot D, Koteliansky V, Limmer S, Manoharan M, Vornlocher HP. Therapeutic silencing of an endogenous gene by systemic administration of modified siRNAs. Nature. 2004 Nov 11;432(7014):173-8. PubMed Abstract

  
Comments on Paper and Primary News
  Primary News: A Step Toward Therapeutic RNA Interference

Comment by:  Mark Cookson
Submitted 16 November 2004  |  Permalink Posted 16 November 2004

Many groups have adopted siRNA or shRNA technologies as the method of choice for gene knockdown since it was first demonstrated that these techniques work for mammalian cells. Although there are previous demonstrations that one can inject siRNA duplexes and evoke systemic effects, the paper by Soutschek et al. improves things further by increasing efficiency of delivery as well as duplex stability. For those of us who work on neurodegenerative diseases, the question now is, “Will it work in brain?” Perhaps not: most of the cholesterol in the brain is synthesized locally and relatively small amounts are taken up through the blood-brain barrier. However, it seems likely that the general concept may be useful. By using molecules that are permeable to the blood-brain barrier, one could imagine peripherally administered siRNA complexes being delivered to the brain quite efficiently. Given that the biodistribution of many natural and artificial molecules is known, one could even design compounds that act as postcodes for different organs. The challenge then would be to develop...  Read more

  Primary News: A Step Toward Therapeutic RNA Interference

Comment by:  Victor Miller, Henry Paulson
Submitted 18 November 2004  |  Permalink Posted 18 November 2004

Immediately following the description that RNA interference (RNAi) works in mammalian cells, it was recognized that such specific inhibitors of gene expression held tremendous potential as drugs (1). A wealth of papers describing the inhibition of disease-causing or disease-associated genes soon followed (reviewed in 2,3). As scientists sought to extend these successes to animal models, a predictable but nevertheless difficult obstacle arose: unmodified small interfering RNAs were not easily delivered to the relevant tissues in vivo. Even delivery to relatively accessible organs such as the liver required techniques not amenable to clinical application in humans. Now Soutschek et al. present evidence that small interfering RNA (siRNA), delivered via a clinically acceptable route (IV), can inhibit gene expression with predictable and physiologically relevant results in vivo (4). The large and frequent doses of siRNA required, coupled with the potentially confounding technique of administering a cholesterol-containing drug for a lipid disorder, make it unlikely that this...  Read more
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