制备一种靶向PRLR和HER2的双特异性药物偶联抗体并改善内化

Huifang Zong, Baohong Zhang, Jianjia Zhu
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引用次数: 2

摘要

抗体药物偶联(ADC)治疗已成为肿瘤免疫治疗中最有前途的方法之一。双特异性靶向可以提高ADC分子的特异性、亲和力和内化能力。泌乳素受体(PRLR)和HER2在乳腺癌中具有串扰信号,与HER2相比,PRLR经历了快速的内化。为了提高HER2 ADC的疗效,增强其靶向特异性和内在化,我们构建了PRLR/HER2靶向双特异性ADC (BsADC)。我们从亲和和内化两方面评价了PRLR × HER2 BsADC的特性,并利用cell Count Kit-8分析进一步评估了其在人乳腺癌细胞系(BT474、T47D和MDA-MB-231)中的体外细胞毒性。我们的数据表明,与HER2 ADC相比,PRLR × HER2 BsADC在结合药物后保持了对两种靶向抗原的亲和力,并表现出更高的内化效率。此外,PRLR × HER2 BsADC在体外对人乳腺癌具有良好的抗肿瘤活性。总之,我们的研究结果表明,通过增加靶抗体的内化来增强抗肿瘤活性和治疗潜力是可行的,可以进一步在体内动物模型中进行评估。
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Generating a Bispecific Antibody Drug Conjugate Targeting PRLR and HER2 with Improving the Internalization
Antibody drug conjugate (ADC) therapy has become one of the most promising approaches in cancer immunotherapy. The bispecific targeting could improve the specificity, affinity, and internalization of the ADC molecules. Prolactin preceptor (PRLR) and HER2 have crosstalk signaling in breast cancer, and PRLR undergoes a rapid internalization compared with HER2. To improve the efficacy of HER2 ADCs with enhancing the target specificity and internalization, we constructed a PRLR/HER2-targeting bispecific ADC (BsADC). We evaluated the characterization of PRLR × HER2 BsADC from the affinity and internalization, and further assessed its in vitro cytotoxicity in human breast-cancer cell lines (BT474, T47D, and MDA-MB-231) using Cell Count Kit-8 analysis. Our data demonstrated that PRLR × HER2 BsADC kept the affinity to two targeting antigens after conjugating drugs and exhibited higher internalization efficiency in comparison to HER2 ADC. Furthermore, PRLR × HER2 BsADC demonstrated to have superior antitumor activity in human breast cancer in vitro. In conclusion, our findings indicate that it is feasible through increasing the internalization of target antibody to enhance the antitumor activity and therapeutic potential that could be further evaluated in in vivo animal model.
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24
审稿时长
15 weeks
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