The therapeutic efficacy of 5-ALA based photodynamic therapy and chemotherapy combination in triple negative breast cancer cells.

IF 2.1 4区 医学 Q3 ENGINEERING, BIOMEDICAL Lasers in Medical Science Pub Date : 2024-07-23 DOI:10.1007/s10103-024-04141-9
Beyzanur Erk, Ali Furkan Kamanli, Gamze Guney Eskiler
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Abstract

Triple negative breast cancer (TNBC) is one of the subtypes of breast cancer characterized by a heterogeneous and aggressive nature. Photodynamic therapy (PDT) has drawn significant attention in cancer treatment. However, solubility of photosensitizer, penetration problems into a target tissue and insufficient oxygen concentration limit the effectiveness of PDT. To overcome these limitations and to reduce the side effects of chemotherapy, combination treatment modalities play an essential role in cancer treatment. In this study, we aimed to investigate the combination efficacy of cisplatin-based chemotherapy and 5-Aminolevulinic acid (5-ALA)/PDT in TNBC cells and healthy breast cells in vitro. To determine the effect of the combination effects of cisplatin and 5-ALA/PDT on TNBC cells, two treatment protocols (simultaneous and sequential combination therapy) were evaluated compared with cisplatin and 5-ALA/PDT monotherapy and WST-1, Annexin V assay, acridine orange (AO) and mitochondrial staining were performed. Our findings showed that MDA-MB-231 TNBC cell viability was significantly decreased following simultaneous combination treatment compared to cisplatin and 5-ALA/PDT monotherapy. Additionally, simultaneous combination treatment was more effective than sequential combination treatment. The simultaneous combination treatment of 2.5 µM cisplatin and 5-ALA/PDT at 6 J/cm2 and 9 J/cm2 induced 46.78% and 53.6% total apoptotic death, respectively in TNBC cells compared with monotherapies (cisplatin (37.88%) and 5-ALA/PDT (6 J/cm2: 31.48% and 9 J/cm2: 37.78%). Additionally, cisplatin and 5-ALA/PDT combination treatment resulted in nuclear fragmentation and mitochondrial damage due to apoptosis. Our results suggest that cisplatin and 5-ALA/PDT simultaneous combination therapy could be a promising new alternative strategy for treating TNBC. However, further studies are required to assess the underlying molecular mechanisms of cisplatin and 5-ALA/PDT combination treatment at the molecular level.

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基于 5-ALA 的光动力疗法和化疗联合疗法对三阴性乳腺癌细胞的疗效。
三阴性乳腺癌(TNBC)是乳腺癌亚型之一,具有异质性和侵袭性的特点。光动力疗法(PDT)在癌症治疗中备受关注。然而,光敏剂的可溶性、对靶组织的穿透问题以及氧气浓度不足限制了光动力疗法的有效性。为了克服这些局限性并减少化疗的副作用,联合治疗模式在癌症治疗中发挥着至关重要的作用。本研究旨在体外研究顺铂化疗和 5-Aminolevulinic acid(5-ALA)/PDT 在 TNBC 细胞和健康乳腺细胞中的联合疗效。为了确定顺铂和5-ALA/PDT联合疗法对TNBC细胞的影响,我们评估了两种治疗方案(同步和序贯联合疗法)与顺铂和5-ALA/PDT单药疗法的比较,并进行了WST-1、Annexin V检测、吖啶橙(AO)和线粒体染色。我们的研究结果表明,与顺铂和 5-ALA/PDT 单药治疗相比,MDA-MB-231 TNBC 细胞活力在同时联合治疗后显著下降。此外,同时联合治疗比连续联合治疗更有效。与单药治疗(顺铂(37.88%)和5-ALA/PDT(6 J/cm2:31.48%和9 J/cm2:37.78%)相比,2.5 µM顺铂和5-ALA/PDT在6 J/cm2和9 J/cm2条件下同时联合治疗可分别诱导TNBC细胞46.78%和53.6%的凋亡。此外,顺铂和 5-ALA/PDT 联合治疗会导致细胞凋亡造成核破碎和线粒体损伤。我们的研究结果表明,顺铂和5-ALA/PDT同时联合治疗可能是治疗TNBC的一种很有前景的新替代策略。然而,要从分子水平评估顺铂和5-ALA/PDT联合治疗的潜在分子机制,还需要进一步的研究。
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来源期刊
Lasers in Medical Science
Lasers in Medical Science 医学-工程:生物医学
CiteScore
4.50
自引率
4.80%
发文量
192
审稿时长
3-8 weeks
期刊介绍: Lasers in Medical Science (LIMS) has established itself as the leading international journal in the rapidly expanding field of medical and dental applications of lasers and light. It provides a forum for the publication of papers on the technical, experimental, and clinical aspects of the use of medical lasers, including lasers in surgery, endoscopy, angioplasty, hyperthermia of tumors, and photodynamic therapy. In addition to medical laser applications, LIMS presents high-quality manuscripts on a wide range of dental topics, including aesthetic dentistry, endodontics, orthodontics, and prosthodontics. The journal publishes articles on the medical and dental applications of novel laser technologies, light delivery systems, sensors to monitor laser effects, basic laser-tissue interactions, and the modeling of laser-tissue interactions. Beyond laser applications, LIMS features articles relating to the use of non-laser light-tissue interactions.
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