金纳米棒辅助光热疗法对乳腺癌和胰腺癌细胞的热效应和生物反应

IF 3.9 2区 生物学 Q2 BIOCHEMISTRY & MOLECULAR BIOLOGY
Leonardo Bianchi , Sara Baroni , Gabriela Paroni , Martina Bruna Violatto , Giulia Yuri Moscatiello , Nicolò Panini , Luca Russo , Fabio Fiordaliso , Laura Colombo , Luisa Diomede , Paola Saccomandi , Paolo Bigini
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引用次数: 0

摘要

为了提高纳米粒子(NP)辅助光热疗法(PTT)的疗效并使其过渡到临床应用,关键是要确定在癌细胞中诱导的热效应的特征,并将其与细胞生物反应(即细胞活力和细胞死亡途径)联系起来。本研究定量评估了金纳米棒(GNR)辅助近红外 PTT 对两种不同癌细胞系(4T1 三阴性乳腺癌细胞和 Pan02 胰腺癌细胞)的影响。研究人员从 GNR 的内化以及在不同 GNR 浓度下对细胞存活率的影响两个方面考察了纳米材料与生物基质之间的相互作用。为了进行直接比较,在相同的处理设置下对两种细胞系进行了 GNR 介导的 PTT,并通过热成像进行实时监测。根据各种参数(即最大绝对温度、最大温度变化、温度变化曲线、时间-温度变化曲线下面积、有效热增强(ETE)和时间常数)进行热分析,以评估处理的热结果。在选定的实验条件下,单独使用 GNR 处理和近红外激光照射不会导致细胞中毒,但两者结合使用会显著降低两种细胞系的细胞活力。在最佳实验条件下(即 6 μg/mL GNRs 和 4.5 W/cm2 激光功率密度),GNR 辅助 PTT 使 4T1 和 Pan02 细胞的存活率分别降低了 94% 和 87%,并且与 25 ℃ 和 29 ℃ 的最大温度变化有关(即、∼1.8 倍),4T1 和 Pan02 细胞的最高绝对温度分别为 55 ℃ 和 54 ℃,ETE 值分别为 78% 和 81%。此外,GNR 浓度的增加导致时间常数的下降,表明照射后的加热动力学更快。此外,热分析参数与细胞死亡程度相关。在近红外照射 12 小时后,发现 GNR 辅助 PTT 在两种细胞系中主要引发二次细胞凋亡。拟议的研究为 PTT 的温度历史与生物反应之间的关系提供了相关见解。这些发现有助于开发一种通用方法,用于评估 NP 辅助 PTT 对不同类型细胞的热敏感性,并为未来的转化研究奠定基础。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Thermal effects and biological response of breast and pancreatic cancer cells undergoing gold nanorod-assisted photothermal therapy

Thermal effects and biological response of breast and pancreatic cancer cells undergoing gold nanorod-assisted photothermal therapy

To increase the therapeutic efficacy of nanoparticle (NP)-assisted photothermal therapy (PTT) and allow for a transition toward the clinical setting, it is pivotal to characterize the thermal effect induced in cancer cells and correlate it with the cell biological response, namely cell viability and cell death pathways. This study quantitatively evaluated the effects of gold nanorod (GNR)-assisted near-infrared (NIR) PTT on two different cancer cell lines, the 4T1 triple-negative breast cancer cells and the Pan02 pancreatic cancer cells. The interaction between nanomaterials and biological matrices was investigated in terms of GNR internalization and effect on cell viability at different GNR concentrations. GNR-mediated PTT was executed on both cell lines, at the same treatment settings to allow a straightforward comparison, and real-time monitored through thermographic imaging. A thermal analysis based on various parameters (i.e., maximum absolute temperature, maximum temperature change, temperature variation profile, area under the time-temperature change curve, effective thermal enhancement (ETE), and time constants) was performed to evaluate the treatment thermal outcome. While GNR treatment and NIR laser irradiation alone did not cause cell toxicity in the selected settings, their combination induced a significant reduction of cell viability in both cell lines. At the optimal experimental condition (i.e., 6 μg/mL of GNRs and 4.5 W/cm2 laser power density), GNR-assisted PTT reduced the cell viability of 4T1 and Pan02 cells by 94% and 87% and it was associated with maximum temperature changes of 25 °C and 29 °C (i.e., ∼1.8-fold increase compared to the laser-only condition), maximum absolute temperatures of 55 °C and 54 °C, and ETE values of 78% and 81%, for 4T1 and Pan02 cells, correspondingly. Also, the increase in the GNR concentration led to a decrease in the time constants, denoting faster heating kinetics upon irradiation. Furthermore, the thermal analysis parameters were correlated with the extent of cell death. Twelve hours after NIR exposure, GNR-assisted PTT was found to mainly trigger secondary apoptosis in both cell lines. The proposed study provides relevant insights into the relationship between temperature history and biological responses in the context of PTT. The findings contribute to the development of a universal methodology for evaluating thermal sensitivity upon NP-assisted PTT on different cell types and lay the groundwork for future translational studies.

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来源期刊
CiteScore
12.10
自引率
1.90%
发文量
161
审稿时长
37 days
期刊介绍: The Journal of Photochemistry and Photobiology B: Biology provides a forum for the publication of papers relating to the various aspects of photobiology, as well as a means for communication in this multidisciplinary field. The scope includes: - Bioluminescence - Chronobiology - DNA repair - Environmental photobiology - Nanotechnology in photobiology - Photocarcinogenesis - Photochemistry of biomolecules - Photodynamic therapy - Photomedicine - Photomorphogenesis - Photomovement - Photoreception - Photosensitization - Photosynthesis - Phototechnology - Spectroscopy of biological systems - UV and visible radiation effects and vision.
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