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首页> 外文期刊>Current drug targets-The International journal for timely in-depth reviews on drug targets >Phenothiazinium based photosensitisers--photodynamic agents with a multiplicity of cellular targets and clinical applications.
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Phenothiazinium based photosensitisers--photodynamic agents with a multiplicity of cellular targets and clinical applications.

机译:基于吩噻嗪鎓的光敏剂-具有多种细胞靶标和临床应用的光动力剂。

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摘要

PhBPs show selectivity for tumour and microbial cells, which appears to be based on electrostatic interactions between the positive charge generally carried by these molecules and the negative charge found on the outer surface of these target cells. In some cases, a site of action for photoactivated PhBPs is the outer membrane/envelope of the target cell. Such action can involve the modification of membrane lipid and/or lipopolysaccharide, and the inactivation of essential proteins and enzymes, with these effects usually leading to cell lysis and death. However, more often, PhBPs are internalised by target cells, promoted by a variety of factors, including low pH and enzymatic reduction, and upon photoactivation, internalised, PhBPs are able to inflict damage on a number of intracellular targets. In tumour cells, PhBPs can photodamage DNA and the membranes of organelles, thereby inducing necrosis and/or apoptosis. In bacterial cells, whilst DNA is generally a primary target of PhBPs, these compounds can exhibit multiple sites of action within a given cell and show different sites of action between different bacterial species. This variable targeting makes PhBPs attractive propositions as alternatives to conventional antibiotics in that the emergence of bacterial strains with acquired resistance to these compounds appears to be highly unlikely.
机译:PhBP对肿瘤和微生物细胞具有选择性,这似乎是基于这些分子通常携带的正电荷与这些靶细胞外表面上的负电荷之间的静电相互作用。在某些情况下,光活化PhBP的作用位点是靶细胞的外膜/包膜。这种作用可能涉及膜脂质和/或脂多糖的修饰,以及必需蛋白质和酶的失活,这些作用通常导致细胞裂解和死亡。但是,更多时候,PhBP被靶细胞内在化,并受到多种因素的促进,包括低pH和酶促还原,并且在光激活后,PhBP被内在化,能够对许多细胞内靶标造成损害。在肿瘤细胞中,PhBPs可以损伤DNA和细胞器的膜,从而引起坏死和/或凋亡。在细菌细胞中,尽管DNA通常是PhBP的主要靶标,但这些化合物在给定的细胞内可以显示多个作用位点,并且在不同细菌物种之间显示不同的作用位点。这种可变的靶向性使PhBPs成为替代常规抗生素的诱人命题,因为极不可能出现对这些化合物具有获得性耐药性的细菌菌株。

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