What question did this study set out to answer?

To evaluate the efficacy of ITRI-148, a novel AR-NTD degrader, in overcoming resistance in advanced prostate cancer.

April 19, 2026

Abstract LB112: An orally bioavailable AR-NTD degrader that bypasses LBD-dependent resistance and prevents AR-V7-mediated feedback in advanced prostate cancer

Key Points

To evaluate the efficacy of ITRI-148, a novel AR-NTD degrader, in overcoming resistance in advanced prostate cancer.
Developed an orally bioavailable PROTAC targeting the AR N-terminal domain.
Utilized structure-guided modeling to identify binding sites.
Conducted proximity ligation assays to confirm AR-CRBN interaction.
Performed global proteomic profiling to assess target selectivity.
Conducted in vivo studies on tumor regression in xenograft models.
ITRI-148 effectively degraded full-length AR and AR-V7 splice variants.
Showed superior antiproliferative activity compared to enzalutamide.
Maintained suppression of AR signaling without causing adaptive resistance.
Induced significant tumor regression in castrated VCaP xenografts.
No significant toxicity observed in toxicokinetic studies.

Abstract

Abstract Resistance to second-generation antiandrogens in castration-resistant prostate cancer (CRPC) is frequently driven by androgen receptor (AR) splice variants such as AR-V7, which lack the ligand-binding domain (LBD) and evade current therapies. To address this unmet need, we developed ITRI-148, an orally bioavailable PROTAC that targets the AR N-terminal domain (NTD) to induce degradation of both full-length AR and AR splice variants. Structure-guided modeling identified a druggable pocket within the AR-NTD that accommodates ITRI-148, enabling recruitment of cereblon (CRBN) and formation of a productive ternary complex. Proximity ligation assays confirmed AR-CRBN interaction, leading to selective proteasomal degradation of AR, AR-V7, and clinically relevant resistant mutants. Global proteomic profiling demonstrated high target selectivity, with AR as the primary degraded protein. In enzalutamide-resistant C4-2B/MDVR cells, ITRI-148 exhibited superior antiproliferative activity compared with enzalutamide and the LBD-targeted degrader ARV-110. Notably, long-term enzalutamide treatment induced AR-V7 upregulation and PSA rebound, whereas ITRI-148 maintained durable suppression of AR signaling without triggering adaptive resistance. In vivo, oral ITRI-148 induced significant tumor regression in castrated VCaP xenografts and inhibited tumor growth in hormone-intact CWR22Rv1 models. Toxicokinetic studies in rats showed favorable systemic exposure without significant body weight loss or hematologic toxicity at therapeutic doses. Collectively, these findings establish ITRI-148 as a pan-AR degrader that bypasses LBD-dependent resistance mechanisms and prevents AR-V7-mediated feedback, supporting its potential as a next-generation therapy for advanced CRPC. Citation Format: Ling-Yu Wang, Chiu-Lien Hung, Wen-Ning Hsu, Tsan-Chun Wang. An orally bioavailable AR-NTD degrader that bypasses LBD-dependent resistance and prevents AR-V7-mediated feedback in advanced prostate cancer abstract. In: Proceedings of the American Association for Cancer Research Annual Meeting 2026; Part 2 (Late-Breaking, Clinical Trial, and Invited Abstracts) ; 2026 Apr 17-22; San Diego, CA. Philadelphia (PA): AACR; Cancer Res 2026;86 (8Suppl): Abstract nr LB112.

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Abstract LB112: An orally bioavailable AR-NTD degrader that bypasses LBD-dependent resistance and prevents AR-V7-mediated feedback in advanced prostate cancer

Key Points

Abstract

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