Logotype for Opus Genetics Inc

Opus Genetics (IRD) R&D Day 2026 summary

Event summary combining transcript, slides, and related documents.

Logotype for Opus Genetics Inc

R&D Day 2026 summary

8 Jul, 2026

Pipeline overview and program updates

  • Advancing seven AAV gene therapy assets for inherited retinal diseases, targeting bestrophinopathies, Leber's congenital amaurosis (LCA), and retinitis pigmentosa, with a platform approach enabling parallel development and capital efficiency.

  • Two lead programs (BEST1 and LCA5) are in clinical trials, with five more expected in the clinic by 2027.

  • LCA5 phase III enrollment ongoing; BEST1 phase I-II cohort 1 completed; RDH12, MERTK, and RHO programs entering clinic over the next 12-18 months, with up to four clinical trial readouts expected in 2027.

  • Multi-asset pipeline and first-mover advantage in several indications, with meaningful ex-U.S. market opportunities.

  • Cash runway extends into 2029, supporting five clinical programs through multiple inflection points.

Clinical trial data and development milestones

  • LCA5 gene therapy shows significant improvements in visual acuity and functional endpoints in both adult and pediatric cohorts, with meaningful patient-reported outcomes.

  • LCA5 Phase 1/2 trial demonstrated improvement in visual acuity and full-field stimulus test in 5 of 6 participants, with effects lasting up to 18 months in adults and 6 months in pediatric patients.

  • BEST1 program completed first cohort enrollment; microperimetry and imaging endpoints are being used to correlate structural and functional improvements.

  • Early BEST1 results show favorable safety (no ocular inflammation or adverse events) and initial efficacy (12-letter gain in visual acuity, 23% reduction in central subfield thickness).

  • Preclinical data for RDH12, MERTK, and RHO demonstrate restoration of enzyme/protein function and photoreceptor preservation in relevant animal models.

R&D strategy and innovation priorities

  • Focus on diseases with preserved retinal structure, rapid proof-of-concept potential, and availability of animal/cell models.

  • Use of mutation-independent, single AAV constructs for silence-and-replace strategies (notably for RHO).

  • Data-driven dose exploration and adaptive clinical trial designs, leveraging independent data monitoring committees.

  • Streamlined, cost-effective development leverages rare disease regulatory advantages and a validated delivery approach.

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