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Tumour-targeting photosensitisers for one- and two-photon activated photodynamic therapy

机译:靶向肿瘤的光敏剂,用于单光子和双光子激活的光动力疗法

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摘要

Despite the advantages of photodynamic therapy (PDT) over chemotherapy or radiotherapy such as low side effects, lack of treatment resistance and spatial selectivity inherent to light activation of the drug, several limitations especially related to the photosensitiser (PS) prevent PDT from becoming widespread in oncology. Herein, new folic acid-and biotin-conjugated PSs for tumour-targeting PDT are reported, with promising properties related to PDT such as intense absorption following one-photon excitation in the red or two-photon excitation in the near-infrared, and also high singlet oxygen quantum yield (close to 70% in DMSO). Cellular studies demonstrated that both targeted PSs induced phototoxicity, the folate-targeted PS being the most effective one with 80% of cell death following 30 min of irradiation and a phototoxicity four times higher than that of the non-targeted PS. This result is in accordance with the uptake of the folate-targeted PS in HeLa cells, mediated by the folate receptors. Moreover, this folate-targeted PS was also phototoxic following two-photon excitation at 920 nm, opening new perspectives for highly selective PDT treatment of small and deep tumours.
机译:尽管光动力疗法(PDT)优于化学疗法或放射疗法,例如副作用低,缺乏治疗抗性和药物光激活所固有的空间选择性,但一些特别是与光敏剂(PS)有关的局限性阻止了PDT在人体中的广泛传播。肿瘤学。本文中,报道了用于肿瘤靶向PDT的新型叶酸和生物素共轭PS,具有与PDT相关的有希望的性能,例如红色的单光子激发或近红外的两光子激发后的强烈吸收,以及单线态氧量子产率高(在DMSO中接近70%)。细胞研究表明,两种靶向PS均可诱导光毒性,以叶酸为靶向的PS是最有效的一种,照射30分钟后细胞死亡80%,光毒性比非靶向PS高四倍。该结果与叶酸受体介导的HeLa细胞中叶酸靶向PS的摄取相一致。此外,这种以叶酸为靶标的PS在920 nm处的双光子激发后也具有光毒性,为高选择性PDT治疗小而深的肿瘤开辟了新的前景。

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  • 来源
    《Organic & biomolecular chemistry》 |2019年第27期|6585-6594|共10页
  • 作者单位

    Univ Strasbourg, CNRS, Inst Chim Strasbourg UMR 7177, Lab Synth Assemblages Mol Multifunct, 4 Rue Blaise Pascal, F-67000 Strasbourg, France;

    Univ Strasbourg, CNRS, Inst Chim Strasbourg UMR 7177, Lab Synth Assemblages Mol Multifunct, 4 Rue Blaise Pascal, F-67000 Strasbourg, France;

    Univ Strasbourg, UdS CNRS, Fac Pharm, CAMB,UMR 7199, 74 Route Rhin, F-67401 Illkirch Graffenstaden, France;

    Ist ISOF CNR, Via P Gobetti 101, I-40129 Bologna, Italy;

    Univ Strasbourg, CNRS, Inst Chim Strasbourg UMR 7177, Lab Synth Assemblages Mol Multifunct, 4 Rue Blaise Pascal, F-67000 Strasbourg, France;

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