Huntingtin suppression restores cognitive function in a mouse model of Huntington’s disease

Southwell, Amber L.; Kordasiewicz, Holly; Langbehn, Douglas R.; Skotte, Niels H.; Parsons, Matthew; Villanueva, Erika B.; Caron, Nicholas S.; Østergaard, Michael E.; Anderson, Lisa; Xie, Yuanyun; Cengio, Louisa Dal; Findlay-Black, Hailey; Doty, Crystal N.; Fitsimmons, Bethany; Swayze, Eric E.; Seth, Punit P.; Raymond, Lynn A.; Bennett, C. Frank; Hayden, Michael R.

doi:10.1126/scitranslmed.aar3959

Cited by 93 publications

(86 citation statements)

References 46 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Many technologies are being explored for gene modulation in the CNS, including adenoassociated virus (AAV) and ASOs 4,41,42 . AAV delivered by intra-parenchymal injections efficiently silenced HTT in minipig, sheep, and NHP 41,43,44 .…”

Section: Discussionmentioning

confidence: 99%

See 1 more Smart Citation

A divalent siRNA chemical scaffold for potent and sustained modulation of gene expression throughout the central nervous system

et al. 2019

View full text Add to dashboard Cite

show abstract

Section: Discussionmentioning

confidence: 99%

“…ASOs have enabled ~50% decrease of soluble mutant HTT in the CSF of patients following monthly intrathecal injections 45 . However, ASO delivery to deep brain structures is limited 4 , with no significant HTT silencing observed in NHP caudate after multiple injections 42 .…”

Section: Discussionmentioning

confidence: 99%

A divalent siRNA chemical scaffold for potent and sustained modulation of gene expression throughout the central nervous system

et al. 2019

View full text Add to dashboard Cite

show abstract

“…protein in the brain and are being advanced preclinically and clinically for several other neurodegenerative diseases (20)(21)(22)(23)(24)(25)(26)(27)(28)(29). These short (17-20 base) single-stranded oligonucleotides, chemically modified for pharmacokinetic stability, are capable of impacting disease biology through specific modulation of complementary target RNAs (30,31), including RNAse H-dependent degradation (32)(33)(34).…”

Section: Introductionmentioning

confidence: 99%

Antisense oligonucleotides extend survival of prion-infected mice

et al. 2019

Self Cite

View full text Add to dashboard Cite

Prion disease is a fatal, incurable neurodegenerative disease of humans and other mammals caused by conversion of cellular prion protein (PrPC) into a self-propagating neurotoxic conformer (prions; PrPSc). Strong genetic proofs of concept support lowering PrP expression as a therapeutic strategy. Antisense oligonucleotides (ASOs) can provide a practical route to lowering 1 target mRNA in the brain, but their development for prion disease has been hindered by 3 unresolved issues from prior work: uncertainty about mechanism of action, unclear potential for efficacy against established prion infection, and poor tolerability of drug delivery by osmotic pumps. Here, we test ASOs delivered by bolus intracerebroventricular injection to intracerebrally prion-infected WT mice. Prophylactic treatments given every 2–3 months extended survival times 61%–98%, and a single injection at 120 days after infection, near the onset of clinical signs, extended survival 55% (87 days). In contrast, a nontargeting control ASO was ineffective. Thus, PrP lowering is the mechanism of action of ASOs effective against prion disease in vivo, and infrequent — or even single — bolus injections of ASOs can slow prion neuropathogenesis and markedly extend survival, even when initiated near clinical signs. These findings should empower development of PrP-lowering therapy for prion disease.

show abstract

“…Antisense oligonucleotides (ASOs) hybridize by Watson–Crick base pairing to mRNAs, leading to degradation by ribonuclease H, inhibition of translation, or altered splicing. Dominant disorders can be treated with allele‐specific ASOs that specifically target the mutant transcript, or with non–allele‐specific ASOs that reduce both mutant and wild‐type transcript . The application of ASO therapy to neurological disorders is receiving increasing attention, and the US Food and Drug Administration has recently approved treatment for spinal muscular atrophy that uses intrathecal administration of an ASO at 6‐month intervals .…”

mentioning

confidence: 99%

“…Dominant disorders can be treated with allele-specific ASOs that specifically target the mutant transcript, or with non-allele-specific ASOs that reduce both mutant and wild-type transcript. 12,13 The application of ASO therapy to neurological disorders is receiving increasing attention, [14][15][16] and the US Food and Drug Administration has recently approved treatment for spinal muscular atrophy that uses intrathecal administration of an ASO at 6-month intervals. 17 The goal of the current work was to evaluate ASO therapy for SCN8A encephalopathy.…”

mentioning

confidence: 99%

Scn8a Antisense Oligonucleotide Is Protective in Mouse Models of SCN8A Encephalopathy and Dravet Syndrome

Lenk

Jafar‐Nejad

Hill

et al. 2020

Annals of Neurology

104

View full text Add to dashboard Cite

Objective SCN8A encephalopathy is a developmental and epileptic encephalopathy (DEE) caused by de novo gain‐of‐function mutations of sodium channel Nav1.6 that result in neuronal hyperactivity. Affected individuals exhibit early onset drug‐resistant seizures, developmental delay, and cognitive impairment. This study was carried out to determine whether reducing the abundance of the Scn8a transcript with an antisense oligonucleotide (ASO) would delay seizure onset and prolong survival in a mouse model of SCN8A encephalopathy. Methods ASO treatment was tested in a conditional mouse model with Cre‐dependent expression of the pathogenic patient SCN8A mutation p.Arg1872Trp (R1872W). This model exhibits early onset of seizures, rapid progression, and 100% penetrance. An Scn1a +/− haploinsufficient mouse model of Dravet syndrome was also treated. ASO was administered by intracerebroventricular injection at postnatal day 2, followed in some cases by stereotactic injection at postnatal day 30. Results We observed a dose‐dependent increase in length of survival from 15 to 65 days in the Scn8a‐R1872W/+ mice treated with ASO. Electroencephalographic recordings were normal prior to seizure onset. Weight gain and activity in an open field were unaffected, but treated mice were less active in a wheel running assay. A single treatment with Scn8a ASO extended survival of Dravet syndrome mice from 3 weeks to >5 months. Interpretation Reduction of Scn8a transcript by 25 to 50% delayed seizure onset and lethality in mouse models of SCN8A encephalopathy and Dravet syndrome. Reduction of SCN8A transcript is a promising approach to treatment of intractable childhood epilepsies. Ann Neurol 2020;87:339–346

show abstract

Huntingtin suppression restores cognitive function in a mouse model of Huntington’s disease

Cited by 93 publications

References 46 publications

A divalent siRNA chemical scaffold for potent and sustained modulation of gene expression throughout the central nervous system

A divalent siRNA chemical scaffold for potent and sustained modulation of gene expression throughout the central nervous system

Antisense oligonucleotides extend survival of prion-infected mice

Scn8a Antisense Oligonucleotide Is Protective in Mouse Models of SCN8A Encephalopathy and Dravet Syndrome

Contact Info

Product

Resources

About