Pfizer Worldwide Research and Development, Oncology Research and Development, Pearl River, NY, USA.
BioMedicine Design, Cambridge, MA, USA.
Cell Rep Med. 2021 May 18;2(5):100279. doi: 10.1016/j.xcrm.2021.100279.
Aberrant NOTCH3 signaling and overexpression is oncogenic, associated with cancer stem cells and drug resistance, yet therapeutic targeting remains elusive. Here, we develop NOTCH3-targeted antibody drug conjugates (NOTCH3-ADCs) by bioconjugation of an auristatin microtubule inhibitor through a protease cleavable linker to two antibodies with differential abilities to inhibit signaling. The signaling inhibitory antibody rapidly induces ligand-independent receptor clustering and internalization through both caveolin and clathrin-mediated pathways. The non-inhibitory antibody also efficiently endocytoses via clathrin without inducing receptor clustering but with slower lysosomal co-localization kinetics. In addition, DLL4 ligand binding to the NOTCH3 receptor mediates transendocytosis of NOTCH3-ADCs into ligand-expressing cells. NOTCH3-ADCs internalize into receptor and ligand cells independent of signaling and induce cell death in both cell types representing an atypical mechanism of ADC cytotoxicity. Treatment of xenografts with NOTCH3-ADCs leads to sustained tumor regressions, outperforms standard-of-care chemotherapy, and allows targeting of tumors that overexpress NOTCH3 independent of signaling inhibition.
异常的 NOTCH3 信号和过表达是致癌的,与癌症干细胞和耐药性有关,但治疗靶点仍然难以捉摸。在这里,我们通过蛋白酶可切割接头将微管抑制剂奥瑞他汀与两种具有不同抑制信号能力的抗体进行生物偶联,开发了针对 NOTCH3 的抗体药物偶联物(NOTCH3-ADC)。信号抑制抗体通过网格蛋白和小窝蛋白介导的途径快速诱导配体非依赖性受体聚集和内化。非抑制性抗体也通过网格蛋白有效地内吞,但不诱导受体聚集,而是具有较慢的溶酶体共定位动力学。此外,DLL4 配体与 NOTCH3 受体的结合介导了 NOTCH3-ADC 向配体表达细胞的转胞吞作用。NOTCH3-ADC 可内化到受体和配体细胞中,而不依赖于信号,并诱导两种细胞类型的细胞死亡,这代表了 ADC 细胞毒性的一种非典型机制。用 NOTCH3-ADC 治疗异种移植瘤可导致肿瘤持续消退,优于标准治疗化疗,并允许针对表达 NOTCH3 的肿瘤进行靶向治疗,而无需抑制信号。
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