Abstract
This review summarizes evidence that most of cell protein degradation is maintained by pathways transferring energy from glucose to reduction of enzymic and nonenzymic proteins (redox-responsive). In contrast, a major subcomponent of proteolysis is simultaneously independent of the cell redox network (redox-unresponsive). Thus far, direct and indirect redox-responsive proteolytic effector mechanisms characterized by various investigators include: several classes of proteases, some peptide protease inhibitors, substrate conjugation systems, substrate redox and folding status, cytoskeletal-membrane kinesis, metal homeostasis, and others. The present focus involves redox control of sulfhydryl proteases and proteolytic pathways of mammalian muscle; however, other mechanisms, cell types, and species are also surveyed. The diversity of redox-responsive catabolic mechanisms reveals that the machinery of protein turnover evolved with fundamental dependencies upon the cell redox network, as observed in many species. The net redox status of a reversible proteolytic effector mechanism represents the balance between combined oxidative inactivating influences versus reductive activating influences. Similar to other proteins, redox-responsive proteolytic effectors appear to be oxidized by mixed disulfide formation, nitrosation, reactive oxygen species, and associations or reactions with metal ions and various pro-oxidative metabolites. Systems reducing the proteolytic machinery include major redox enzyme chains, such as thioredoxins or glutaredoxins, and perhaps various reductive metabolites, including glutathione and dihydrolipoic acid. Much of mammalian intracellular protein degradation is reversibly responsive to noninjurious experimental intervention in the reductive energy supply-demand balance. Proteolysis is reversibly inhibited by diamide or dehydroascorbic acid; and such antiproteolytic actions are strongly dependent on the cell glucose supply. However, gross redox-responsive proteolysis is not accompanied by ATP depletion or vice versa. Redox-responsive proteolysis includes Golgi-endoplasmic reticulum degradation, lysosomal degradation, and some amount of extravesicular degradation, all comprising more than half of total cell proteolysis. Speculatively, redox-dependent proteolysis exhibits features expected of a controlling influence coordinating distinct proteolytic processes under some intracellular conditions.
Highlights
Intracellular proteolysis is critical to maintain timely degradation of altered proteins including oxidized proteins
Evolution has used oxygen to modify certain proteins, termed redox switches, as a cell signaling mechanism in survival [5] and regeneration [6] among other pathways. This clever use of reactive oxygen species (ROS) is best exemplified by NADPH oxidases (NOX), situated in the plasma membrane, whose main role is to generate superoxide and hydrogen peroxide (H2O2) as second messengers [7]
We summarize the most relevant findings about the degradation of oxidized proteins, here termed oxyproteins, and the impact of oxidative stress on proteolytic cell systems, and gene expression
Summary
Autophagy refers to any intracellular process that leads to degradation of cytosolic components inside lysosomes [43,44]. Redox-mediated signaling or oxidative modification of macromolecules up-regulate the autophagy flux, leading to elimination of non-functional and potentially damaging protein aggregates and affected organelles (Fig. 5A and B). Since NRF2 promotes the expression of proteasome and autophagy-genes it is not surprising that tunicamycin-induced ER stress significantly up-regulates proteasomal activity [96]. Tunicamycin treatment of myc-tagged NRF1 transfected cells resulted in higher levels of the 110 kDa Nrf fragment in the nucleus when compared with untreated cells Another group later reported that this isoform does not have the ability to transactivate ARE-containing genes [96]. ROS production and oxidative stress can be considered an integral component of the UPR, triggering both transcriptional and post-translational responses which in turn lead to cell adaptation and survival or cell death by apoptosis
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