sciync

v0
Paper SpacePredictionsAI Sync
Your circlePrinciples
Join the waitlist
NoemesConsensusHeatPanels
All noemes
Trial · NCT00999609

Noeme · wixzyfis

Historical
gene-therapy

Published finding — does the expert body still believe it?

The LUXTURNA (voretigene) trial's stated primary conclusion — Subretinal AAV2-hRPE65 gene therapy improves functional vision in biallelic RPE65-associated inherited retinal dystrophy. — replicates in independent cohorts.

Sign in to follow
Open a pool

TL;DR · AI-generated

tldr@v2.0.0
semanticscholar.org

Voretigene neparvovec gene replacement improved functional vision in RPE65-mediated inherited retinal dystrophy previously medically untreatable.

Your position — does this noeme still stand given current evidence?

0% (impossible)

50%

100% (certain)

25
50
75

Proper-scoring-rule preview

If TRUE: Brier 0.250 · log 0.69 · +8 rep
If FALSE: Brier 0.250 · log 0.69 · -1 rep
Kelly 25.0% ≈ 250 rep

Your position is kept on this device until you sign in.

Evidence stream

2 events · 1 snapshot

posterior drift

71% → 71% (0pp · 1 point)

posterior drift: 71% → 71%
neutral

Registry data

NCT00999609

Apr 18, 2026

supports

Peer-reviewed paper

doi:10.1016/S0140-6736(17)31868-8

Apr 18, 2026

+21pp

Expert reactions · 0

Sign in to post a take, cite a related claim, or flag a methodological concern.

No reactions yet. Be the first expert to post a take, cite a related claim, or flag a methodological concern.

Source publication

Efficacy and safety of voretigene neparvovec (AAV2-hRPE65v2) in patients with RPE65 -mediated inherited retinal dystrophy: a randomised, controlled, open-label, phase 3 trial

Stephen Russell et al. · The Lancet · 2017

1.8k citations · S2 1.3k
58 influential
FWCI 60.7 · Landmark
Paywalled
36 authors · 64% ORCID

· openalex W2736065260 · s2 e00fcd8a

doi:10.1016/S0140-6736(17)31868-8
NCT00999609

Semantically related

Nearest claims in the expert-corpus vector space. Ordered by cosine distance — lower is closer.

Current

0.1092

Recent follow-up analyses of LUXTURNA (voretigene) are confirming the original effect size in real-world data.

Future

0.1769

By 2028, at least two additional subretinal gene therapies (beyond LUXTURNA) will be FDA-approved for monogenic retinal dystrophies.

Historical

0.1923

The HOPE-B (Hemgenix / etranacogene) trial's stated primary conclusion — AAV5 FIX-Padua gene therapy produces sustained Factor IX activity, reducing bleeds in severe hemophilia B. — replicates in independent cohorts.

Current

0.2031

Recent follow-up analyses of HOPE-B (Hemgenix / etranacogene) are confirming the original effect size in real-world data.

Historical

0.2037

The STR1VE (onasemnogene abeparvovec / Zolgensma) trial's stated primary conclusion — Single-dose IV AAV9-SMN1 gene therapy produces durable motor benefit in SMA type 1 infants. — replicates in independent cohorts.

Current

0.2096

Recent follow-up analyses of STR1VE (onasemnogene abeparvovec / Zolgensma) are confirming the original effect size in real-world data.