Figure 7
Figure 7. Schematic summary of molecular events underlying O2−-mediated induction of S70pBcl-2 upon the downregulation of SOD1 in tumor cells. Augmented level of intracellular O2− as a result of SOD1 inhibition/downregulation could lead to an increase in the formation of ONOO− and the eventual tyrosine nitration of B56δ. This in turn inhibits the recruitment of PP2A-AC core subunits to Bcl-2, resulting in the accumulation of S70-phosphorylated Bcl-2 and the further inhibition of apoptotic stimuli. Redox modulators such as DPI, tiron, and FeTPPS may harbor the potential as chemosensitization agents by suppressing the levels of O2− or ONOO− in tumor cells.

Schematic summary of molecular events underlying O2-mediated induction of S70pBcl-2 upon the downregulation of SOD1 in tumor cells. Augmented level of intracellular O2 as a result of SOD1 inhibition/downregulation could lead to an increase in the formation of ONOO and the eventual tyrosine nitration of B56δ. This in turn inhibits the recruitment of PP2A-AC core subunits to Bcl-2, resulting in the accumulation of S70-phosphorylated Bcl-2 and the further inhibition of apoptotic stimuli. Redox modulators such as DPI, tiron, and FeTPPS may harbor the potential as chemosensitization agents by suppressing the levels of O2 or ONOO in tumor cells.

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