紧身衣
化学
光毒性
光动力疗法
生物正交化学
光敏剂
共焦显微镜
毒性
单线态氧
组合化学
荧光
肽
点击化学
生物物理学
光化学
生物化学
细胞生物学
氧气
有机化学
体外
生物
物理
量子力学
作者
Greta Linden,Olalla Vázquez
标识
DOI:10.1002/chem.202001718
摘要
Abstract Photodynamic therapy (PDT) leads to cancer remission via the production of cytotoxic species under photosensitizer (PS) irradiation. However, concomitant damage and dark toxicity can both hinder its use. With this in mind, we have implemented a versatile peptide‐based platform of bioorthogonally activatable BODIPY‐tetrazine PSs. Confocal microscopy and phototoxicity studies demonstrated that the incorporation of the PS, as a bifunctional module, into a peptide enabled spatial and conditional control of singlet oxygen ( 1 O 2 ) generation. Comparing subcellular distribution, PS confined in the cytoplasmic membrane achieved the highest toxicities (IC 50 =0.096±0.003 μ m ) after activation and without apparent dark toxicity. Our tunable approach will inspire novel probes towards smart PDT.
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