细胞毒性
化学
伊布替尼
阿霉素
共价键
连接器
癌症研究
药理学
化疗
癌细胞
淋巴瘤
布仑妥昔单抗维多汀
共价结合
靶向给药
靶向治疗
生物化学
布鲁顿酪氨酸激酶
组合化学
药品
断点群集区域
联合化疗
程序性细胞死亡
配体(生物化学)
K562细胞
作者
Xinyue Zhao,Na Wei,Ziyang Fang,Yingyan Xie,X Y Yan,QiuQuan Wang
标识
DOI:10.1021/acs.jmedchem.5c02215
摘要
To address the low cytotoxicity and drug resistance issues of targeted covalent inhibitor (TCI) ibrutinib and severe side effects of chemotherapeutics doxorubicin (DOX), we developed a novel targeted covalently activated chemotherapy strategy. We designed and synthesized a targeted covalently activated chemotherapy drug, Ibt-DOX, which features a targeting ligand of ibrutinib, a DOX, an electrophilic warhead α-methylated acrylamide (α-MAA) and a self-immolative linker p-hydroxybenzyl alcohol. Upon specifically binding to BTK, Ibt-DOX inhibits the BTK-mediated BCR signaling, meanwhile releases DOX and induces immunogenic cell death (ICD), ultimately resulting in not only significantly enhanced targeted B-cell lymphoma cells death compared with ibrutinib, but also reduces the toxic side effects of DOX on BTK- cells. Our work offers a novel strategy through leveraging the synergistic effect of targeted covalent inhibition and the high cytotoxicity of chemotherapy drug, which will inspire the development of new targeted covalent chemotherapeutics for different cancers treatment.
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