用于光动力疗法的光敏剂缀合物的合成、生物分析及生物分布
Synthesis, bioanalysis and biodistribution of photosensitizer conjugates for photodynamic therapy.
作者信息
St Denis Tyler G, Hamblin Michael R
机构信息
Department of Chemistry, Columbia University, NY, USA.
出版信息
Bioanalysis. 2013 May;5(9):1099-114. doi: 10.4155/bio.13.37.
Abstract
Photodynamic therapy (PDT) was discovered in 1900 by Raab, and has since emerged as a promising tool for treating diseases characterized by unwanted cells or hyperproliferating tissue (e.g., cancer or infectious disease). PDT consists of the light excitation of a photosensitizer (PS) in the presence of O(2) to yield highly reactive oxygen species. In recent years, PDT has been improved by the synthesis of targeted bioconjugates between monoclonal antibodies and PS, and by investigating PS biodistribution and PD. Here, we provide a comprehensive review of major developments in PS-immunoconjugate-based PDT and the bioanalysis of these agents, with a specific emphasis on anticancer and antimicrobial PDT.
摘要
光动力疗法(PDT)于1900年由拉布发现,此后已成为一种有前景的治疗工具,用于治疗以不需要的细胞或过度增殖组织为特征的疾病(如癌症或传染病)。PDT包括在氧气存在下对光敏剂(PS)进行光激发,以产生活性很强的氧物种。近年来,通过合成单克隆抗体与PS之间的靶向生物共轭物以及研究PS的生物分布和光动力作用,PDT得到了改进。在此,我们全面综述了基于PS免疫共轭物的PDT的主要进展以及这些药物的生物分析,特别强调了抗癌和抗菌PDT。
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