Prion protein lowering is a disease-modifying therapy across prion disease stages, strains and endpoints. Issue 19 (10th August 2020)

Record Type:: Journal Article
Title:: Prion protein lowering is a disease-modifying therapy across prion disease stages, strains and endpoints. Issue 19 (10th August 2020)
Main Title:: Prion protein lowering is a disease-modifying therapy across prion disease stages, strains and endpoints
Authors:: Minikel, Eric Vallabh
Zhao, Hien T
Le, Jason
O'Moore, Jill
Pitstick, Rose
Graffam, Samantha
Carlson, George A
Kavanaugh, Michael P
Kriz, Jasna
Kim, Jae Beom
Ma, Jiyan
Wille, Holger
Aiken, Judd
McKenzie, Deborah
Doh-ura, Katsumi
Beck, Matthew
O'Keefe, Rhonda
Stathopoulos, Jacquelyn
Caron, Tyler
Schreiber, Stuart L
Carroll, Jeffrey B
Kordasiewicz, Holly B
Cabin, Deborah E
Vallabh, Sonia M
Abstract:: Abstract: Lowering of prion protein (PrP) expression in the brain is a genetically validated therapeutic hypothesis in prion disease. We recently showed that antisense oligonucleotide (ASO)-mediated PrP suppression extends survival and delays disease onset in intracerebrally prion-infected mice in both prophylactic and delayed dosing paradigms. Here, we examine the efficacy of this therapeutic approach across diverse paradigms, varying the dose and dosing regimen, prion strain, treatment timepoint, and examining symptomatic, survival, and biomarker readouts. We recapitulate our previous findings with additional PrP-targeting ASOs, and demonstrate therapeutic benefit against four additional prion strains. We demonstrate that <25% PrP suppression is sufficient to extend survival and delay symptoms in a prophylactic paradigm. Rise in both neuroinflammation and neuronal injury markers can be reversed by a single dose of PrP-lowering ASO administered after the detection of pathological change. Chronic ASO-mediated suppression of PrP beginning at any time up to early signs of neuropathology confers benefit similar to constitutive heterozygous PrP knockout. Remarkably, even after emergence of frank symptoms including weight loss, a single treatment prolongs survival by months in a subset of animals. These results support ASO-mediated PrP lowering, and PrP-lowering therapeutics in general, as a promising path forward against prion disease.
Is Part Of:: Nucleic acids research. Volume 48:Issue 19(2020)
Journal:: Nucleic acids research
Issue:: Volume 48:Issue 19(2020)
Issue Display:: Volume 48, Issue 19 (2020)
Year:: 2020
Volume:: 48
Issue:: 19
Issue Sort Value:: 2020-0048-0019-0000
Page Start:: 10615
Page End:: 10631
Publication Date:: 2020-08-10
Subjects:: Nucleic acids -- Periodicals
Molecular biology -- Periodicals
572.805
Journal URLs:: http://nar.oxfordjournals.org/ ↗
http://www.ncbi.nlm.nih.gov/pmc/journals/4 ↗
http://ukcatalogue.oup.com/ ↗
http://firstsearch.oclc.org ↗
DOI:: 10.1093/nar/gkaa616 ↗
Languages:: English
ISSNs:: 0305-1048
Deposit Type:: Legaldeposit
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Ingest File:: 15048.xml