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Zymeworks Presents New Data from Multiple Development Programs at 2025 AACR Annual Meeting

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Zymeworks Inc.
Zymeworks Inc.

Six posters highlight continued progress across antibody-drug conjugate and T cell engager platforms

Novel T cell engager ZW209 demonstrates durable activity in small cell lung cancer; IND submission expected in 1H-2026

VANCOUVER, British Columbia, April 25, 2025 (GLOBE NEWSWIRE) -- Zymeworks Inc. (Nasdaq: ZYME), a clinical-stage biotechnology company developing a diverse pipeline of novel, multifunctional biotherapeutics to improve the standard of care for difficult-to-treat diseases, including cancer, inflammation, and autoimmune disease, today announced the presentation of six posters with new preclinical data from its preclinical, development-stage, and clinical programs at the American Association for Cancer Research (AACR) Annual Meeting being held April 25-30, 2025 in Chicago, IL.

“The breadth of data shared at AACR highlights the strength of our oncology portfolio across antibody-drug conjugates and T cell engagers, and demonstrates the novel approaches we employ using each modality,” said Paul Moore, Ph.D., Chief Scientific Officer at Zymeworks. “We’re particularly excited to share data on ZW209, the latest of our oncology nominated IND programs which has demonstrated promising anti-tumor activity in preclinical small cell lung cancer models by integrating CD28 co-stimulation into a trispecific T cell engager. We look forward to advancing ZW209 with an IND submission anticipated in the first half of 2026, while also progressing the differentiated programs in our wholly-owned pipeline.”

Presentation Highlights

T cell Engagers (TCE):

ZW171, a differentiated 2+1 T cell-engaging bispecific antibody with antitumor activity in a range of mesothelin expressing cancers
Abstract: 3503
Session Category: Immunology
Session Title: T Cell Engagers

ZW171 is a mesothelin (MSLN)-targeting TCE currently in a global Phase 1 clinical study (NCT06523803) in a range of difficult-to-treat, MSLN-positive tumor models including ovarian, pancreatic, and non-small cell lung cancer (NSCLC).

Key findings include:

  • ZW171 demonstrates cytolytic activity across a range of MSLN expressing tumor types including lung, ovarian and pancreatic cancers with anti-tumor activity correlating with MSLN cell surface expression and not related to soluble MSLN levels.

  • ZW171 exhibits strong anti-tumor activity in patient derived xenograft (PDX) models of NSCLC and pancreatic cancer, and in ex-vivo patient-derived ovarian cancer organoids with endogenous tumor-infiltrating lymphocytes (TIL).

  • Relative to other MSLN targeted T cell engagers in development, ZW171 exhibits reduced T cell binding but enhanced cytolytic activity.

  • These data reinforce the differentiated profile of ZW171 and demonstrate its enhanced anti-tumor activity compared to other MSLN-targeting bispecifics.