PO.CH01.03 · 化学
A novel investigation of the cyclin A/B inhibitor ZMS-7506 demonstrates robust anti-tumor efficacy both in vitro and in vivo
作者与单位
摘要 Abstract
Cyclins A and B are critical regulators of the transition from the S phase to the G2/M phase of the cell cycle. Abnormal expression and activity of these cyclins are hallmarks of cancer. Disruption of the interaction between E2F and the cyclin A2-CDK2 complex results in hyperactivation of E2F, leading to apoptosis and synthetic lethality in E2F-driven tumors. Small cell lung cancer (SCLC) cell lines commonly exhibit dysregulated E2F activity due to near-universal loss-of-function mutations in RB1 and TP53. We have developed ZMS-7506, a potent oral Cyclin A/B inhibitor, which demonstrated a median IC 50 of approximately 40 nM in anti-proliferation assays using a panel of SCLC cell lines. Moreover, ZMS-7506 selectively inhibited the proliferation of ovarian cancer OVCAR3 cells, with a GI 50 value below 20 nM. In the meanwhile, ZMS-7506 exhibited a GI 50 greater than 10 μM in normal human embryonic lung fibroblasts (WI38), indicating a favorable therapeutic window. Mechanistically, ZMS-7506 induced G2/M cell cycle arrest and upregulated markers associated with apoptosis and mitotic arrest, including p-KNL1, p-HH3, p-PARP, and p-gamma-H2AX. These findings suggest that ZMS-7506 activates the spindle assembly checkpoint (SAC), thereby inducing mitotic arrest and apoptosis. ZMS-7506 also exhibited moderate oral bioavailability in pre-clinical species such as dogs, which supported the oral administration in human. Moreover, ZMS-7506 exhibited robust antitumor efficacy as a monotherapy in the SCLC NCI-H69 xenograft mouse model. In summary, ZMS-7506 is a highly selective oral Cyclin A/B inhibitor with promising therapeutic potential as a monotherapy for cancers characterized by elevated E2F activity.
利益披露 Disclosure
G. Yang,
State Key Laboratory of Neurology and Oncology Drug Development, Simcere Zaiming Pharmaceutical Co, Ltd. Employment.
R. Wang,
State Key Laboratory of Neurology and Oncology Drug Development, Simcere Zaiming Pharmaceutical Co, Ltd. Employment.
W. Wang,
State Key Laboratory of Neurology and Oncology Drug Development, Simcere Zaiming Pharmaceutical Co, Ltd. Employment.
L. Xue,
State Key Laboratory of Neurology and Oncology Drug Development, Simcere Zaiming Pharmaceutical Co, Ltd. Employment.
X. Qin,
State Key Laboratory of Neurology and Oncology Drug Development, Simcere Zaiming Pharmaceutical Co, Ltd. Employment.
R. Tang,
State Key Laboratory of Neurology and Oncology Drug Development, Simcere Zaiming Pharmaceutical Co, Ltd. Employment.
Z. Li,
State Key Laboratory of Neurology and Oncology Drug Development, Simcere Zaiming Pharmaceutical Co, Ltd. Employment.