Unique<i>O</i>-Methoxyethyl Ribose-DNA Chimeric Oligonucleotide Induces an Atypical Melanoma Differentiation-Associated Gene 5-Dependent Induction of Type I Interferon Response

Burel, Sebastien A.; Machemer, Todd; Ragone, Frank L.; Kato, Hiroki; Cauntay, Patrick; Greenlee, Sarah; Salim, Aneeza; Gaarde, William A.; Hung, Gene; Freier, Susan M.; Henry, Scott P.

doi:10.1124/jpet.112.193789

Cited by 29 publications

(26 citation statements)

References 56 publications

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“…Similar to ISIS 116847, no change in inflammatory signaling was observed in knockout animals deficient in MyD88 and TRIF. Interestingly, this study demonstrated that two cytosolic receptors, melanoma-differentiation associated-5 (MDA-5) and IFN-b promoter stimulator-1 (IPS-1) were involved in the inflammatory reaction to ISIS 147420, but retinoic acid inducible gene-1 (RIG-1) was not [64]. Both IPS-1 and RIG-1 are pattern recognition receptors that are capable of recognizing foreign nucleic acids.…”

Section: Second-and Third-generation Phosphorothioate Asosmentioning

confidence: 93%

“…For NATs, the majority of available studies have focused on TLRs (TLR3, TLR7/8 and TLR9) to explain observed immunostimulation [63,64,[165][166][167][168]. However in many cases, inhibiting or eliminating TLRs from test systems reduced immunostimulation but did not eliminate it, leaving a gap in the understanding of the mechanism(s) [63,64].…”

Section: Expert Opinionmentioning

confidence: 95%

“…Based on these findings, the authors suggested that 2¢-MOE non-CpG ASO induced cytokines through either TLR3 which functions through the My-D88-independent adaptor TRIF (Toll/IL-1R-containing adaptor protein inducing IFN-b), or another unidentified receptor. Another elegant study from this group showed a different 2¢-MOEmodified non-CpG ASO (ISIS 147420) induced high levels of type I interferons (IFN-b) independently from TLR3 [64]. Similar to ISIS 116847, no change in inflammatory signaling was observed in knockout animals deficient in MyD88 and TRIF.…”

Section: Second-and Third-generation Phosphorothioate Asosmentioning

confidence: 96%

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Immunological and hematological toxicities challenging clinical translation of nucleic acid-based therapeutics

Dobrovolskaia¹,

McNeil²

2015

Expert Opinion on Biological Therapy

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Section: Second-and Third-generation Phosphorothioate Asosmentioning

confidence: 93%

Section: Expert Opinionmentioning

confidence: 95%

Section: Second-and Third-generation Phosphorothioate Asosmentioning

confidence: 96%

See 1 more Smart Citation

Immunological and hematological toxicities challenging clinical translation of nucleic acid-based therapeutics

Dobrovolskaia¹,

McNeil²

2015

Expert Opinion on Biological Therapy

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“…The shorter basepair length of most LNA gapmers (based on their higher binding efficiency) seems to reduce their proinflammatory potential as compared to other backbones. The basis for the sequence specificity in rodents are sequence motifs that are recognized by pathogen-associated molecular pattern (PAMP) receptors, such as the nucleic acidsensing TLR receptors (Agrawal and Kandimalla 2004;Senn, Burel, and Henry 2005;Richardt-Pargmann and Vollmer 2009;Burel et al 2012;Burel et al 2013). These attributes have been exploited for immunomodulatory drug indications by industry (Krieg 1998(Krieg , 1999Henry et al 1999).…”

Section: Hybridization-independent Proinflammatory Effects (Challengementioning

confidence: 99%

Antisense Oligonucleotide Therapies

2014

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Many antisense oligonucleotides (ASOs) from several classes of molecules are currently in drug development. Despite over 20 years of pharmaceutical research, few ASOs have been marketed due to problems with clinical efficacy or preclinical toxicologic challenges. However, a number of recent developments have renewed interest in this class including the registration of mipomersen, the advent of successful screening strategies to eliminate more toxic molecules, and new understanding of the risks of off-target nucleotide binding and mitigation of potential off-target effects. Recent advances in backbone chemistries, conjugation to other moieties, and new delivery systems have allowed better tissue penetration, enhanced intracellular targeting, and less frequent dosing, resulting in fewer toxicities. While these new developments provide invigorated interest in these platforms, a few lingering challenges and preclinical/clinical toxicity issues remain to be completely resolved, including: (1) proinflammatory effects (vasculitis/inflammatory infiltrates); (2) nephrotoxicity and hepatotoxicity unrelated to lysosomal accumulation; and (3) thrombocytopenia. Recent investigative work by several laboratories have helped elucidate mechanisms for these issues, allowing a better understanding of the clinical relevance and implications of particular toxicities. It is important for toxicologists, pathologists, and regulatory reviewers to be familiar with new developments in the ASO field and their implications, as a greater number of new types of antisense molecules undergo preclinical toxicity testing.

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“…The microarray gene expression analysis showed several downregulated genes predicted to be because of off-target hybridization of HDO (Table 2). In addition, sequence-dependent and hybridization-independent immunestimulatory adverse effects mediated by activation of toll-like innate receptors 52,53 can also be a concern. Finally, a sequenceand hybridization-independent chemical property of nucleotide analogues and chemical modifications can cause liver dysfunction 51,[54][55][56][57] .…”

Section: Resultsmentioning

confidence: 99%

DNA/RNA heteroduplex oligonucleotide for highly efficient gene silencing

Yokota

2016

Clinical & Exp Neuroim

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Antisense oligonucleotides (ASOs) are recognized therapeutic agents for the modulation of specific genes at the post-transcriptional level. Similar to any medical drugs, there are opportunities to improve their efficacy and safety. Here we develop a short DNA/RNA heteroduplex oligonucleotide (HDO) with a structure different from double-stranded RNA used for short interfering RNA and single-stranded DNA used for ASO. A DNA/locked nucleotide acid gapmer duplex with an a-tocopherol-conjugated complementary RNA (Toc-HDO) is significantly more potent at reducing the expression of the targeted mRNA in liver compared with the parent single-stranded gapmer ASO. Toc-HDO also improves the phenotype in disease models more effectively. In addition, the high potency of Toc-HDO results in a reduction of liver dysfunction observed in the parent ASO at a similar silencing effect. HDO technology offers a novel concept of therapeutic oligonucleotides, and the development of this molecular design opens a new therapeutic field.

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UniqueO-Methoxyethyl Ribose-DNA Chimeric Oligonucleotide Induces an Atypical Melanoma Differentiation-Associated Gene 5-Dependent Induction of Type I Interferon Response

Cited by 29 publications

References 56 publications

Immunological and hematological toxicities challenging clinical translation of nucleic acid-based therapeutics

Immunological and hematological toxicities challenging clinical translation of nucleic acid-based therapeutics

Antisense Oligonucleotide Therapies

DNA/RNA heteroduplex oligonucleotide for highly efficient gene silencing

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