Goldman Sachs 47th Annual Global Healthcare Conference 2026
Logotype for Spyre Therapeutics Inc

Spyre Therapeutics (SYRE) Goldman Sachs 47th Annual Global Healthcare Conference 2026 summary

Event summary combining transcript, slides, and related documents.

Logotype for Spyre Therapeutics Inc

Goldman Sachs 47th Annual Global Healthcare Conference 2026 summary

8 Jun, 2026

Strategic priorities and pipeline focus

  • Aims to improve care in autoimmune diseases, initially focusing on inflammatory bowel disease (IBD) with three validated targets: alpha-4 beta-7, TL1A, and IL-23, developed as both monotherapies and advanced co-formulated combinations.

  • Exploring TL1A as a pipeline-in-a-product candidate for multiple rheumatic diseases, including rheumatoid arthritis, psoriatic arthritis, and axial spondyloarthritis.

  • Next 12 months will see five additional phase II readouts, including monotherapy and combination data in IBD and rheumatic diseases, with combination therapy readouts expected in 2027.

  • Anticipates multiple products could become indication-leading across large markets.

Differentiation and technology approach

  • Focuses on high-concentration, long-acting, co-formulatable antibodies, overcoming challenges in co-formulation and ensuring additive efficacy in a convenient format.

  • Unique ability to deliver both agents at high concentration in a single injection, unlike existing antibodies.

  • Chose co-formulation over bispecifics to independently block targets, avoid unwanted immune activation, and allow flexible dosing ratios.

  • Co-formulation may reduce immunogenicity compared to bispecifics, supported by external data.

Clinical data and expectations

  • Lead asset SPY001 targets alpha-4 beta-7, showing higher clinical remission rates at increased drug exposure, potentially matching or exceeding ENTYVIO efficacy.

  • Expects 002 and 003 to replicate first-generation efficacy with less drug due to long-acting modifications, enabling single-shot co-formulations.

  • Maintenance efficacy for TL1A may improve with better saturation, with data expected next year; IL-23 and alpha-4 beta-7 appear saturated in maintenance.

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