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首页> 外文期刊>ACS Omega >Picolyl Porphyrin Nanostructures as a Functional Drug Entrant for Photodynamic Therapy in Human Breast Cancers
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Picolyl Porphyrin Nanostructures as a Functional Drug Entrant for Photodynamic Therapy in Human Breast Cancers

机译:普罗基卟啉纳米结构作为人乳腺癌光动力治疗的功能药物进入剂

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The major challenge in photodynamic therapy (PDT) is to discover versatile photosensitizers (PSs) that possess good solubility in biological media, enhanced singlet oxygen generation efficacy, and photodynamic activity. Working in this direction, we synthesized a picolylamine-functionalized porphyrin conjugate, compound 1, and its zinc complex compound 2. Compound 1 forms spherical structures in methanol, whereas compound 2 exhibited vesicular structures. Compared to the existing PSs like foscan and photofrin, compound 2 exhibited a high singlet oxygen generation efficiency and triplet quantum yield. The complex also showed good water solubility, and its PDT activity was demonstrated through in vitro studies using MDA-MB 231 breast cancer cells. The mechanism of biological activity evaluated using various techniques proved that the active compound 2 induced predominantly singlet oxygen-triggered apoptosis-mediated cancerous cell death. Our results demonstrate that zinc insertion in the picolyl porphyrin induces an enhanced triplet excited state, and the singlet oxygen yields quantitatively and imparts excellent in vitro photodynamic activity, thereby demonstrating their pertinence as a nanodrug in future photobiological applications.
机译:光动力治疗(PDT)中的主要挑战是发现在生物介质中具有良好的溶解性,增强的单线磷生成疗效和光动力活动,发现多功能光敏剂(PSS)。在此方向上工作,我们合成了吡喃胺官能化卟啉缀合物,化合物1及其锌复合化合物2.化合物1在甲醇中形成球形结构,而化合物2表现出凹形结构。与现有的PSS相比,如FOSCAN和Photofrin,化合物2表现出高态氧产生效率和三重态量子产率。该综合体还显示出良好的水溶性,通过使用MDA-MB 231乳腺癌细胞的体外研究证明了其PDT活性。使用各种技术评价的生物活性机制证明了活性化合物2主要诱导单线态氧引发的凋亡介导的癌细胞死亡。我们的结果表明,吡酰卟啉中的锌插入诱导增强的三重态激发状态,并且单向氧在定量上产生,并赋予优异的体外光动力活性,从而在未来的光生物学应用中展示其作为纳米凹面的优异。

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