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>Navitoclax enhances the effectiveness of EGFR-targeted antibody-drug conjugates in PDX models of EGFR-expressing triple-negative breast cancer
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Navitoclax enhances the effectiveness of EGFR-targeted antibody-drug conjugates in PDX models of EGFR-expressing triple-negative breast cancer
Targeted therapies for triple-negative breast cancer (TNBC) are limited; however, the epidermal growth factor receptor (EGFR) represents a potential target, as the majority of TNBC express EGFR. The purpose of these studies was to evaluate the effectiveness of two EGFR-targeted antibody-drug conjugates (ADC: ABT-414; ABBV-321) in combination with navitoclax, an antagonist of the anti-apoptotic BCL-2 and BCL-XL proteins, in order to assess the translational relevance of these combinations for TNBC. The pre-clinical efficacy of combined treatments was evaluated in multiple patient-derived xenograft (PDX) models of TNBC. Microscopy-based dynamic BH3 profiling (DBP) was used to assess mitochondrial apoptotic signaling induced by navitoclax and/or ADC treatments, and the expression of EGFR and BCL-2/XL was analyzed in 46 triple-negative patient tumors. Treatment with navitoclax plus ABT-414 caused a significant reduction in tumor growth in five of seven PDXs and significant tumor regression in the highest EGFR-expressing PDX. Navitoclax plus ABBV-321, an EGFR-targeted ADC that displays more effective wild-type EGFR-targeting, elicited more significant tumor growth inhibition and regressions in the two highest EGFR-expressing models evaluated. The level of mitochondrial apoptotic signaling induced by single or combined drug treatments, as measured by DBP, correlated with the treatment responses observed in vivo. Lastly, the majority of triple-negative patient tumors were found to express EGFR and co-express BCL-XL and/or BCL-2. The dramatic tumor regressions achieved using combined agents in pre-clinical TNBC models underscore the abilities of BCL-2/XL antagonists to enhance the effectiveness of EGFR-targeted ADCs and highlight the clinical potential for usage of such targeted ADCs to alleviate toxicities associated with combinations of BCL-2/XL inhibitors and systemic chemotherapies.
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机译:针对三阴性乳腺癌(TNBC)的疗法有限;然而,表皮生长因子受体(EGFR)代表潜在的靶标,因为大多数TNBC Express EGFR。这些研究的目的是评估两种EGFR靶向抗体 - 药物缀合物(ADC:ABT-414; ABV-321)的有效性与Navitoclax,抗凋亡BCL-2和BCL-XL蛋白的拮抗剂组合,为了评估这些组合的TNBC的翻译相关性。在TNBC的多个患者衍生的异种移植物(PDX)模型中评价组合处理的前临床疗效。基于显微镜的动态BH3分析(DBP)用于评估Navitoclax和/或ADC处理诱导的线粒体凋亡信号传导,并在46个三阴性患者肿瘤中分析EGFR和Bcl-2 / X1的表达。用Navitoclax Plus ABT-414治疗导致七种PDX中的五种PDX中的肿瘤生长显着降低,并且在表达最高的EGFR的PDX中的肿瘤衰退中的显着肿瘤消退。 Navitoclax Plus ABBV-321,EGFR靶向ADC,显示更有效的野生型EGFR靶向,引发了评估的两个最高富尔表达模型中的更显着的肿瘤生长抑制和回归。通过DBP测量的单一或组合药物处理诱导的线粒体细胞凋亡信号的水平与体内观察到的治疗反应相关。最后,发现大多数三阴性患者肿瘤表达EGFR和Co-Express Bcl-XL和/或Bcl-2。在临床前TNBC模型中使用联合剂实现的戏剧性肿瘤回归强调了Bcl-2 / XL拮抗剂的能力,以提高EGFR靶向ADC的有效性,并突出了这种靶向ADC的使用临床潜力,以减轻与组合相关的毒性BCL-2 / XL抑制剂和全身化疗。
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