BGB-21447, a next-generation Bcl-2 inhibitor, demonstrates superior potency and overcomes Venetoclax resistance in preclinical models of hematologic malignancies
Presenter: Shuran Li, PhD Session: Cell Death Regulation and Therapeutic Resistance in Cancer Time: 4/21/2026 9:00:00 AM → 4/21/2026 12:00:00 PM
Authors
Shuran Li 1 , Shasha Yang 1 , Xiaolong Yang 1 , Yanwen Ma 1 , Shining Nie 1 , Longbo Yin 1 , Qin Wang 1 , Haimei Xing 1 , Zhu Mei 1 , Ali Wang 1 , Xiaolin Liu 1 , Ying Guo 1 , Haitao Wang 1 , Weiwei Song 1 , Lin Li 1 , Lu Lyu 1 , Yiwen Wang 1 , Jin Wei 1 , Chuanxiu Wang 1 , Ye Liu 1 , Xi Yuan 1 , Yunhang Guo 1 , Yu Shen 2 , Lai Wang 2 , Xiaomin Song 1 1 BeOne Medicines (Beijing) I GmbH, Beijing, China, 2 BeOne Medicines (Shanghai) Research & Development I GmbH, Beijing, China
Abstract
Bcl-2 is a key anti-apoptotic gatekeeper that controls intrinsic apoptosis pathway. Its overexpression or aberrant activation is frequently observed in hematologic malignancies, where it promotes tumorigenesis and confers resistance to chemotherapy. Venetoclax (VEN), the first-in-class Bcl-2 inhibitor approved for R/R CLL and AML, shows modest efficacy in non-Hodgkin lymphoma and is compromised by acquired BCL2 mutations (e.g., G101V, D103Y). Herein, we report the preclinical characterization of BGB-21447, a highly potent and selective next-generation Bcl-2 inhibitor that demonstrates remarkably better potency than VEN across multiple hematologic cancer cell lines and effectively targets a broad spectrum of VEN-resistant Bcl-2 mutations. BGB-21447 displays ≥121-fold higher selectivity for Bcl-2 over Bcl-xL, Bcl-W, Mcl-1 and Bcl2A1. Across a panel of 9 hematologic lines, it consistently achieved lower IC 50 values than VEN (0.18-6.6 nM vs 4.8-238 nM for Ven). In RS4;11 cells overexpressing Bcl2 mutants, BGB-21447 achieved IC 50 values of 11-44 nM IC 50 s, including G101V (15 nM vs 3854 nM for VEN) and D103Y (44 nM vs 4731 nM for VEN). Its anti-proliferative effects were accompanied by hallmark features of intrinsic apoptosis, including caspase-3/7 activation, phosphatidylserine externalization (Annexin V positivity), and sub-G0/G1 DNA accumulation. In PK/PD studies, oral administration of BGB-21447 demonstrated a clear exposure-response relationship in both RS4;11 wild-type and Bcl-2-G101V knock-in xenograft models, with cleaved caspase-3 levels correlating with intratumoral drug concentration. At 1.5 mg/kg, BGB-21447 showed superior antitumor efficacy compared to VEN at 15 mg/kg and ABBV-453 (AbbVie’s selective Bcl-2 inhibitor) at 1.5 mg/mL. in the RS4;11 WT model. Notably, BGB-21447 showed robust antitumor effects in VEN-insensitive models, including the Toledo (DLBCL), RS4;11 Bcl2-G101V, and RS4;11 Bcl2-D103Y xenografts. No significant weight loss or laboratory toxicities were observed. In conclusion, BGB-21447 surpasses VEN in potency and mutant coverage, and durably inhibits VEN-resistant tumors at well-tolerated doses in preclinical models. These findings support the ongoing Phase 1 clinical trials (NCT05828589, NCT06756932) evaluating BGB-21447 in B-cell malignancies and metastatic breast cancer.
Disclosure
S. Li, BeOne Medicines (Beijing) I GmbH Employment. S. Yang, BeOne Medicines (Beijing) I GmbH Employment. X. Yang, BeOne Medicines (Beijing) I GmbH Employment. Y. Ma, BeOne Medicines (Beijing) I GmbH Employment. S. Nie, BeOne Medicines (Beijing) I GmbH Employment. L. Yin, BeOne Medicines (Beijing) I GmbH Employment. Q. Wang, BeOne Medicines (Beijing) I GmbH Employment. H. Xing, BeOne Medicines (Beijing) I GmbH Employment. Z. Mei, BeOne Medicines (Beijing) I GmbH Employment. A. Wang, BeOne Medicines (Beijing) I GmbH Employment. X. Liu, BeOne Medicines (Beijing) I GmbH Employment. Y. Guo, BeOne Medicines (Beijing) I GmbH Employment. H. Wang, BeOne Medicines (Beijing) I GmbH Employment. W. Song, BeOne Medicines (Beijing) I GmbH Employment. L. Li, BeOne Medicines (Beijing) I GmbH Employment. L. Lyu, BeOne Medicines (Beijing) I GmbH Employment. Y. Wang, BeOne Medicines (Beijing) I GmbH Employment. J. Wei, BeOne Medicines (Beijing) I GmbH Employment. C. Wang, BeOne Medicines (Beijing) I GmbH Employment. Y. Liu, BeOne Medicines (Beijing) I GmbH Employment. X. Yuan, BeOne Medicines (Beijing) I GmbH Employment. Y. Guo, BeOne Medicines (Beijing) I GmbH Employment. Y. Shen, BeOne Medicines (Shanghai) Research & Development I GmbH Employment. L. Wang, BeOne Medicines (Shanghai) Research & Development I GmbH Employment. X. Song, BeOne Medicines (Beijing) I GmbH Employment.
Cited in
Control: 864 · Presentation Id: 6097 · Meeting 21436