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Ozone mediates tumor-selective cell death caused by air plasma-activated medium independently of NOx
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Abstract
Cold atmospheric plasma and plasma-treated liquids (PTLs) are emerging promising tools for tumor-targeted cancer treatment, as they preferentially injure tumor cells more than non-malignant cells. Oxidative stress is critical to the antitumor effect, but the oxidant mediating the effect is debatable. Previously, we reported that air plasma-activated medium (APAM) has tumor-selective cytotoxicity in vitro and in vivo. Moreover, an unusual mitochondrial positioning named monopolar perinuclear mitochondrial clustering (MPMC) and nuclear damage proceeds to cell death. We noticed that air plasma generation was accompanied by ozone (O
3
) formation, leading to suppose the possible role of O
3
in the effect of APAM. In this study, we produced an O
3
-dissolved medium (ODM) and comparatively analyzed its biological effect with APAM. Both agents had comparable amounts of dissolved O
3
(dO
3
), while APAM, but not ODM, contained nitrite and nitrate. Like APAM, ODM could induce apoptosis, nonapoptotic cell death, tubulin remodeling, MPMC, and nuclear shrinkage. Catalase mitigated all these events. The increases in various intracellular and mitochondrial reactive oxygen species (ROS) and lipid peroxides proceeded to cell death, and catalase also prevented them. Conversely, suppressing cellular H
2
O
2
removal systems augmented mitochondrial ROS production and cell death. In contrast, like APAM, ODM minimally increased ROS production and MPMC in non-malignant cells. These results indicate that dO
3
is a critical mediator of the actions of APAM, including tumor-selective induction of MPMC and cell death. Our findings suggest ODM could be a more chemically-defined alternative to PTLs in cancer treatment.
Title: Ozone mediates tumor-selective cell death caused by air plasma-activated medium independently of NOx
Description:
Abstract
Cold atmospheric plasma and plasma-treated liquids (PTLs) are emerging promising tools for tumor-targeted cancer treatment, as they preferentially injure tumor cells more than non-malignant cells.
Oxidative stress is critical to the antitumor effect, but the oxidant mediating the effect is debatable.
Previously, we reported that air plasma-activated medium (APAM) has tumor-selective cytotoxicity in vitro and in vivo.
Moreover, an unusual mitochondrial positioning named monopolar perinuclear mitochondrial clustering (MPMC) and nuclear damage proceeds to cell death.
We noticed that air plasma generation was accompanied by ozone (O
3
) formation, leading to suppose the possible role of O
3
in the effect of APAM.
In this study, we produced an O
3
-dissolved medium (ODM) and comparatively analyzed its biological effect with APAM.
Both agents had comparable amounts of dissolved O
3
(dO
3
), while APAM, but not ODM, contained nitrite and nitrate.
Like APAM, ODM could induce apoptosis, nonapoptotic cell death, tubulin remodeling, MPMC, and nuclear shrinkage.
Catalase mitigated all these events.
The increases in various intracellular and mitochondrial reactive oxygen species (ROS) and lipid peroxides proceeded to cell death, and catalase also prevented them.
Conversely, suppressing cellular H
2
O
2
removal systems augmented mitochondrial ROS production and cell death.
In contrast, like APAM, ODM minimally increased ROS production and MPMC in non-malignant cells.
These results indicate that dO
3
is a critical mediator of the actions of APAM, including tumor-selective induction of MPMC and cell death.
Our findings suggest ODM could be a more chemically-defined alternative to PTLs in cancer treatment.
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