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Infrared laser pulse triggers increased singlet oxygen production in tumour cells

机译:红外激光脉冲触发肿瘤细胞单线态氧产生的增加

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摘要

Photodynamic therapy (PDT) is a technique developed to treat the ever-increasing global incidence of cancer. This technique utilises singlet oxygen (1O2) generation via a laser excited photosensitiser (PS) to kill cancer cells. However, prolonged sensitivity to intensive light (6–8 weeks for lung cancer), relatively low tissue penetration by activating light (630 nm up to 4 mm), and the cost of PS administration can limit progressive PDT applications. The development of quantum-dot laser diodes emitting in the highest absorption region (1268 nm) of triplet oxygen (3O2) presents the possibility of inducing apoptosis in tumour cells through direct 3O2 → 1O2 transition. Here we demonstrate that a single laser pulse triggers dose-dependent 1O2 generation in both normal keratinocytes and tumour cells and show that tumour cells yield the highest 1O2 far beyond the initial laser pulse exposure. Our modelling and experimental results support the development of direct infrared (IR) laser-induced tumour treatment as a promising approach in tumour PDT.
机译:光动力疗法(PDT)是一种用于治疗全球范围内不断增加的癌症发病率的技术。该技术利用激光激发光敏剂(PS)产生单线态氧( 1 O2)杀死癌细胞。但是,对强光的敏感性延长(对于肺癌为6-8周),通过激活光(630 nm至4 mm)相对较低的组织穿透力,以及PS的施用成本会限制PDT的逐步应用。在三重态氧( 3 O2)的最高吸收区域(1268 nm)发射的量子点激光二极管的发展提出了通过直接 3 O2→ 1 O2转换。在这里,我们证明了单个激光脉冲会在正常角质形成细胞和肿瘤细胞中触发剂量依赖性的 1 O2生成,并表明肿瘤细胞产生的最高 1 O2远超过初始值激光脉冲曝光。我们的建模和实验结果支持直接红外(IR)激光诱导的肿瘤治疗方法的开发,将其作为肿瘤PDT中的一种有希望的方法。

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