Green-Tripp Gabriela, Nattress Callum, Halldén Gunnel
Centre for Biomarkers and Biotherapeutics, Barts Cancer Institute, Queen Mary University of London, London, United Kingdom.
Cell Communication Lab, Department of Oncology, University College London Cancer Institute, London, United Kingdom.
Front Mol Biosci. 2022 Jun 24;9:901392. doi: 10.3389/fmolb.2022.901392. eCollection 2022.
Breast cancer (BC) is the most common cancer globally, accounting for 685,000 deaths in 2020. Triple-negative breast cancers (TNBC) lack oestrogen (ER) and progesterone (PR) hormone receptor expression and HER2 overexpression. TNBC represent 10-15% of all BC with high incidence in women under 50-years old that have mutations, and have a dismal prognosis. African American and Hispanic women are at higher risk partly due to the common occurrence of mutations. The standard treatment for TNBC includes surgery, radiotherapy, and chemotherapy although, resistance to all standard-of-care therapies eventually develops. It is crucial to identify and develop more efficacious therapeutics with different mechanisms of action to improve on survival in these women. Recent findings with oncolytic adenoviruses (OAds) may generate a new strategy to improve on the outcomes for women afflicted by TNBC and other types of BC. OAds are genetically engineered to selectively lyse, eliminate and recruit the host antitumour immune responses, leaving normal cells unharmed. The most common modifications are deletions in the early gene products including the E1B55 KDa protein, specific regions of the E1A protein, or insertion of tumour-specific promoters. Clinical trials using OAds for various adenocarcinomas have not yet been sufficiently evaluated in BC patients. Preclinical studies demonstrated efficacy in BC cell lines, including TNBC cells, with promising novel adenoviral mutants. Here we review the results reported for the most promising OAds in preclinical studies and clinical trials administered alone and in combination with current standard of care or with novel therapeutics. Combinations of OAds with small molecule drugs targeting the epidermal growth factor receptor (EGFR), androgen receptor (AR), and DNA damage repair by the novel PARP inhibitors are currently under investigation with reported enhanced efficacy. The combination of the PARP-inhibitor Olaparib with OAds showed an impressive anti-tumour effect. The most promising findings to date are with OAds in combination with antibodies towards the immune checkpoints or expression of cytokines from the viral backbone. Although safety and efficacy have been demonstrated in numerous clinical trials and preclinical studies with cancer-selective OAds, further developments are needed to eliminate metastatic lesions, increase immune activation and intratumoural viral spread. We discuss shortcomings of the OAds and potential solutions for improving on patient outcomes.
乳腺癌(BC)是全球最常见的癌症,2020年导致68.5万人死亡。三阴性乳腺癌(TNBC)缺乏雌激素(ER)和孕激素(PR)激素受体表达以及HER2过表达。TNBC占所有乳腺癌的10%-15%,在50岁以下有基因突变的女性中发病率较高,且预后较差。非裔美国人和西班牙裔女性风险更高,部分原因是常见的基因突变。TNBC的标准治疗包括手术、放疗和化疗,不过最终会对所有标准治疗产生耐药性。识别并开发具有不同作用机制的更有效疗法对于改善这些女性的生存率至关重要。溶瘤腺病毒(OAds)的最新研究结果可能为改善TNBC和其他类型乳腺癌女性的治疗效果带来新策略。OAds经过基因工程改造,可选择性地裂解、消除并激发宿主抗肿瘤免疫反应,而不损害正常细胞。最常见的改造是早期基因产物的缺失,包括E1B55KDa蛋白、E1A蛋白的特定区域,或插入肿瘤特异性启动子。使用OAds治疗各种腺癌的临床试验在乳腺癌患者中尚未得到充分评估。临床前研究表明,在包括TNBC细胞在内的乳腺癌细胞系中,有前景的新型腺病毒突变体具有疗效。在此,我们回顾临床前研究和临床试验中单独使用以及与当前标准治疗或新型疗法联合使用的最有前景的OAds的报告结果。目前正在研究OAds与靶向表皮生长因子受体(EGFR)、雄激素受体(AR)的小分子药物以及新型PARP抑制剂进行DNA损伤修复的联合使用,报告显示疗效增强。PARP抑制剂奥拉帕利与OAds联合使用显示出令人印象深刻的抗肿瘤效果。迄今为止最有前景的研究结果是OAds与免疫检查点抗体或病毒骨架中细胞因子表达的联合使用。尽管在众多针对癌症选择性OAds的临床试验和临床前研究中已证明其安全性和疗效,但仍需要进一步研发以消除转移病灶、增强免疫激活和肿瘤内病毒传播。我们讨论了OAds的缺点以及改善患者治疗效果的潜在解决方案。
