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  2. RNA interference-mediated silencing of the respiratory syncytial virus nucleocapsid defines a potent antiviral strategy

RNA interference-mediated silencing of the respiratory syncytial virus nucleocapsid defines a potent antiviral strategy

  • Antimicrob Agents Chemother. 2009 Sep;53(9):3952-62. doi: 10.1128/AAC.00014-09.
Rene Alvarez 1 Sayda Elbashir Todd Borland Ivanka Toudjarska Philipp Hadwiger Mathias John Ingo Roehl Svetlana Shulga Morskaya Rick Martinello Jeffrey Kahn Mark Van Ranst Ralph A Tripp John P DeVincenzo Rajendra Pandey Martin Maier Lubomir Nechev Muthiah Manoharan Victor Kotelianski Rachel Meyers
Affiliations

Affiliation

  • 1 Alnylam Pharmaceuticals, 300 Third Street, Cambridge, MA 02142, USA.
Abstract

We describe the design and characterization of a potent human respiratory syncytial virus (RSV) nucleocapsid gene-specific small interfering RNA (siRNA), ALN-RSV01. In in vitro RSV plaque assays, ALN-RSV01 showed a 50% inhibitory concentration of 0.7 nM. Sequence analysis of primary isolates of RSV showed that the siRNA target site was absolutely conserved in 89/95 isolates, and ALN-RSV01 demonstrated activity against all isolates, including those with single-mismatch mutations. In vivo, intranasal dosing of ALN-RSV01 in a BALB/c mouse model resulted in potent Antiviral efficacy, with 2.5- to 3.0-log-unit reductions in RSV lung concentrations being achieved when ALN-RSV01 was administered prophylactically or therapeutically in both single-dose and multidose regimens. The specificity of ALN-RSV01 was demonstrated in vivo by using mismatch controls; and the absence of an immune stimulatory mechanism was demonstrated by showing that nonspecific siRNAs that induce alpha interferon and tumor necrosis factor alpha lack Antiviral efficacy, while a chemically modified form of ALN-RSV01 lacking measurable immunostimulatory capacity retained full activity in vivo. Furthermore, an RNA interference mechanism of action was demonstrated by the capture of the site-specific cleavage product of the RSV mRNA via rapid amplification of cDNA ends both in vitro and in vivo. These studies lay a solid foundation for the further investigation of ALN-RSV01 as a novel therapeutic Antiviral agent for clinical use by humans.

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