PO.ET02.03 · 实验与分子治疗

Preclinical assessment of HWK-206, a next-generation, biparatopic, SEZ6-targeting ADC with novel bioconjugation and linker-payload technology

编号 4440 展板 18 时间 4/21 09:00–12:00 区域 Section 12 主讲 Kathy Keegan
分会场 Antibody-Drug Conjugates and Linker Engineering 3
该海报暂无可访问的完整资料 AACR 官方页面 ↗

作者与单位

Kathy S. Keegan1, Shihe Hou1, Ashwini B. Pai1, Enrico Bellomo1, Erik Kratzer1, Victor Peykov1, Bryan Ball1, Lei Wu2, Mengmeng Sun2, Lu Jiang2, Jijie Gu2, David J. Lennon1, David Dornan1

1Whitehawk Therapeutics, Morristown, NJ,2WuXi Biologics, Shanghai, China

摘要 Abstract

Seizure-related 6 homolog (SEZ6) is a cell-surface transmembrane protein that plays a role in neuronal development. SEZ6 expression is highly elevated in neuroendocrine (NE) tumors, including, but not limited to, small cell lung cancer (SCLC), brain or central nervous system cancers, and NE tumors of prostate and bladder origin, and has limited expression in normal tissues. In SCLC, SEZ6 expression is correlated with worse survival outcomes. Single-epitope, SEZ6-directed antibody-drug conjugates (ADCs), such as ABBV-706, have shown initial promise in SCLC and NE neoplasms, but with some potential challenges attributed to side effects associated with these agents. HWK-206 is a next-generation ADC that utilizes a biparatopic antibody (bpAb) approach to target SEZ6, with an Fc effector-attenuated IgG1 antibody conjugated to the novel DNA topoisomerase I inhibitor, CPT116. HWK-206 was designed using novel bioconjugation (carbon bridge cysteine re-pairing) and advanced linker-payload technologies to maximize intracellular delivery while minimizing systemic exposure of free payload. The mechanism of action of the HWK-206 bpAb was investigated in preclinical SCLC models. Results showed that the HWK-206 bpAb bound to SEZ6 with higher affinity than the parental antibodies or that reported previously for ABBV-706. HWK-206 induced DNA damage and loss of SCLC tumor cell viability. Furthermore, the HWK-206 bpAb demonstrated superior binding, receptor-mediated internalization, and reduction in viability of SCLC tumor cells expressing varying levels of SEZ6, compared with the parental antibodies and historical benchmarks. Potent antitumor activity was observed in various SCLC xenograft tumor models, with tumor regression observed at single doses as low as 2 mg/kg. HWK-206 demonstrated a bystander killing effect in vitro , suggesting the ability to elicit activity against heterogeneous tumors. The pharmacokinetic (PK) and safety profiles of HWK-206 were evaluated in nonclinical toxicology studies. HWK-206 demonstrated a favorable PK profile and was well tolerated. In summary, HWK-206 is a highly potent and selective next-generation, biparatopic, SEZ6-targeted ADC that warrants further investigation. A planned phase I dose-escalation study will investigate HWK-206 in patients with advanced solid tumors.
利益披露 Disclosure
K. S. Keegan, Whitehawk Therapeutics Employment. S. Hou, Whitehawk Therapeutics Employment, Stock. BMS Stock. A. B. Pai, Whitehawk Therapeutics Employment. E. Bellomo, Whitehawk Therapeutics Employment. E. Kratzer, Whitehawk Therapeutics Employment. V. Peykov, Whitehawk Therapeutics Employment. ImmunityBio Stock. B. Ball, Whitehawk Therapeutics Employment. L. Wu, WuXi Biologics Employment. M. Sun, WuXi Biologics Employment. L. Jiang, WuXi Biologics Employment. J. Gu, WuXi Biologics Employment. D. J. Lennon, Whitehawk Therapeutics Employment. D. Dornan, Whitehawk Therapeutics Employment, Stock Option.

在会议检索中打开