Deruxtecan(DXd,MC-GGFG-DXD,AbMole,M10396)是一种带有连接子(Linker)的强效的拓扑异构酶I抑制剂,常用于新型抗体偶联物(ADC)的构建。其特点是具有较高的抑制剂-抗体比(Drug-to-Antibody Ratio, DAR)和稳定的可切割连接子(Tetrapeptide-based cleavable linker)。基于Deruxtecan(CAS No.:1599440-13-7)构建的ADC包括Trastuzumab deruxtecan (针对HER2)、Patritumab deruxtecan (针对HER3)、Datopotamab deruxtecan (针对TROP2)等,它们在细胞实验(如体外细胞毒性测试)和动物实验(如异种移植模型)中展现出显著的抗肿瘤活性。此外,这些ADC还具有“旁观者效应”(bystander effect),即在靶向肿瘤细胞后,释放的DXd能扩散至邻近低抗原表达细胞,提高对异质性肿瘤的疗效[1]。其中,Trastuzumab deruxtecan是针对HER2阳性细胞系(如JIMT-1乳腺癌细胞)的ADC,该ADC显示出显著的细胞毒性。实验表明,Trastuzumab deruxtecan能有效降低细胞活力(viability),并通过诱导拓扑异构酶I抑制导致DNA断裂,最终触发细胞凋亡。具体来说,在平行实验中,该ADC的细胞毒性优于其他对照组,并在HER2表达细胞中展现出强靶向驱动活性[2]。Patritumab deruxtecan则是针对HER3表达的肿瘤细胞。该ADC通过结合HER3受体实现内化,释放Deruxtecan。细胞实验显示,Patritumab deruxtecan能显著降低癌细胞活力,并诱导钙网蛋白重定位,这标志着免疫原性细胞死亡的激活。这种机制在非小细胞肺癌(NSCLC)细胞系中尤为明显,证实了其对HER3突变肿瘤的针对性作用。综上所述,以Deruxtecan(DXd,MC-GGFG-DXD,AbMole,M10396)为基础的ADC具有强效肿瘤杀伤与旁观者效应,并且已经显著改善了HER2、TROP2、HER3等靶点阳性肿瘤的增殖[3]。

参考文献及鸣谢

[1] Jalali, P.; Saeed, A.; Taher, S.; et al. Trastuzumab deruxtecan: Redefining precision oncology across HER2-driven cancers. Critical reviews in oncology/hematology 2026, 217, 105019.

[2] Valsasina, B.; Orsini, P.; Caruso, M.; et al. Novel Thienoduocarmycin-Trastuzumab ADC Demonstrates Strong Antitumor Efficacy with Favorable Safety Profile in Preclinical Studies. Molecular cancer therapeutics 2023, 22 (12), 1465-1478.

[3] Forveille, S.; Zhao, L.; Sauvat, A.; et al. Patritumab deruxtecan induces immunogenic cell death. Oncoimmunology 2025, 14 (1), 2514050.