Subcellular Targeting as a Determinant of the Efficacy of Photodynamic Therapy | Zendy

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Subcellular Targeting as a Determinant of the Efficacy of Photodynamic Therapy

Author(s) -

Kessel David

Publication year - 2016

Publication title -

photochemistry and photobiology

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 0.818

H-Index - 131

eISSN - 1751-1097

pISSN - 0031-8655

DOI - 10.1111/php.12692

Subject(s) - photodynamic therapy , mitochondrion , autophagy , phototoxicity , calpain , photosensitizer , chemistry , microbiology and biotechnology , cleavage (geology) , lysosome , apoptosis , subcellular localization , biology , biochemistry , enzyme , in vitro , paleontology , organic chemistry , fracture (geology) , cytoplasm

In prior studies, we have identified the ability of low‐level lysosomal photodamage to potentiate the phototoxic effect of subsequent photodamage to mitochondria. The mechanism involves calpain‐mediated cleavage of the autophagy‐associated protein ATG 5 to form a proapoptotic fragment ( tATG 5). In this report, we explore the permissible time lag between the two targeting procedures along with the effect of simultaneously targeting both lysosomes and mitochondria. This was found to be as effective as the sequential protocol with no gap between the irradiation steps. Inhibition of calpain reversed the enhanced efficacy of the “simultaneous” protocol. It appears that even a minor level of lysosomal photodamage can have a significant effect on the efficacy of subsequent mitochondrial photodamage. We propose that these results may explain the efficacy of Photofrin, a photosensitizing product that also targets both lysosomes and mitochondria for photodamage.

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