Spyre Therapeutics Announces Expected Acceleration of SPY003 (IL-23p19) Clinical Timelines and Presentations at UEGW supporting Spyre's Portfolio of Potentially Best-in-Class Antibodies and Combinations
SPY003, a novel half-life extended IL-23p19 monoclonal antibody (mAb), with first-in-human dosing now expected first quarter 2025
New data on SPY003 presented at UEGW demonstrating robust preclinical activity including comparable potency and a greater than three-fold extension in half-life in NHPs relative to risankizumab1. Spyre portfolio now uniquely includes extended half-life molecules targeting α4β7, TL1A, and IL-23 with potential Q8W-Q12W maintenance dosing.
Additional preclinical data on SPY003 in combination with SPY001 or SPY002 presented at UEGW showing enhanced preclinical efficacy and pharmacodynamics
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First-in-human dosing of SPY003 (anti-IL-23) in healthy volunteers is now expected to start during the first quarter of 2025. SPY003 is a novel, half-life extended mAb targeting IL-23p19 ("IL-23"). Approved inhibitors of IL-23 are effective and well tolerated treatments of moderate-to-severe IBD, with commercially available therapies dosed six times per year. SPY003 has the potential to be dosed quarterly or twice a year as a monotherapy in maintenance. The company expects to share interim data from the accelerated first-in-human trial in the second half of 2025.
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Spyre presented preclinical data on SPY003 for the first time at UEGW, expanding its portfolio of half-life extended antibodies to three validated targets in IBD. The presentation illustrated in vitro potency comparable to risankizumab1 and pharmacokinetics indicating that SPY003 has a half-life of ~30 days in non-human primates ("NHPs"), a greater than three-fold increase relative to risankizumab1. These data demonstrate that SPY003 exhibits high selectivity and affinity for IL-23 and potently inhibits downstream cellular signaling. With an extended half-life in NHPs, SPY003 demonstrates therapeutic potential for effective and well-tolerated treatment of Crohn's disease ("CD") and Ulcerative Colitis ("UC") with less frequent dosing than approved therapies. In conjunction with its previously disclosed SPY001 (anti-α4β7) and SPY002 (anti-TL1A) programs, the company has a unique portfolio of antibodies that have the potential to be delivered in combination on a unified, Q8W-Q12W dosing frequency in maintenance.
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Spyre presented preclinical data combining anti-IL-23 with either anti-α4β7 or anti-TL1A for the first time at UEGW. The presentation included in vitro studies and in vivo murine colitis model on anti-IL-23 combined with anti-TL1A and anti-α4β7, respectively. The models showed that IL-23 and TL1A have a synergistic effect on promoting IL-17 secretion from human and mouse immune cells, and that the combination of anti-IL-23 and anti-TL1A suppresses IL-17 secretion more effectively than either agent alone. In a T-cell transfer model of IBD, combination therapy with anti-IL-23 and anti-β7 improved body weight and reduced colonic CD4+ infiltration and IL-17 levels relative to monotherapy.
- Additional preclinical data for SPY001 (anti-α4β7) and SPY002 (anti-TL1A) presented at UEGW. These presentations included in vitro potency compared to benchmark antibodies, nonclinical safety data, and pharmacokinetics demonstrating extended half-life in NHPs. For SPY002, characterization of the two development candidates planned for first-in-human studies in Q4 2024 is further described. Human pharmacokinetic simulations for SPY001 and both SPY002 candidates support potential Q8-12W dosing regimens in IBD.
"The Spyre team has made significant progress in advancing its potentially best-in-class molecules into first-in-human studies within an expected nine-month window," said
The posters were presented at the
Title: A Novel Monoclonal Antibody Drug Candidate SPY001 Targeting Integrin ɑ4β7 for the Treatment of IBD: In
Poster #PP1103
Title: Characterization of Two Novel Extended Half-life Monoclonal Antibody Drug Candidates Targeting TL1A for the Treatment of IBD
Poster #MP450
Title: Development and Characterization of SPY003, a Novel Extended Half-life Monoclonal Antibody Drug Candidate Targeting IL-23 for the Treatment of IBD
Poster #MP118
Title: Combining IL-23 Blockade with Anti-ɑ4β7 or Anti-TL1A for the Treatment of IBD is Supported by In Vitro and Mouse IBD Model Experiments
Poster #PP1111
Full session details can be accessed via the UEGW program. New data disclosures are also available in Spyre's updated corporate presentation.
1Synthesized comparator antibody
About Spyre Therapeutics
Spyre Therapeutics is a clinical-stage biotechnology company that aims to create next-generation of inflammatory bowel disease (IBD) products by combining best-in-class antibody engineering, rational therapeutic combinations, and precision medicine approaches. Spyre's pipeline includes investigational extended half-life antibodies targeting α4β7, TL1A, and IL-23.
For more information, please visit http://spyre.com.
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