Date published: 2025-9-12

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PRX II Activators

Common PRX II Activators include, but are not limited to Sodium selenite CAS 10102-18-8, Dimethyl fumarate CAS 624-49-7, CDDO Methyl Ester CAS 218600-53-4, Curcumin CAS 458-37-7 and Quercetin CAS 117-39-5.

Peroxiredoxin II activators comprise a diverse group of chemicals that either directly enhance the activity of PRX II or indirectly promote its function by modulating related cellular pathways. PRX II, a member of the peroxiredoxin family, plays a critical role in cellular defense against oxidative stress by reducing hydrogen peroxide to water. Direct activators like Conoidin A interact with PRX II to facilitate its antioxidative activity. In contrast, indirect activators such as Sodium Selenite, RSL3, and Dimethyl Fumarate enhance PRX II activity by upregulating its expression or increasing oxidative stress, which triggers compensatory antioxidative responses. This category also includes several compounds that activate the Nrf2 pathway, a crucial regulator of antioxidative responses. Compounds like Sulforaphane, Bardoxolone Methyl, and tBHQ work through this mechanism, leading to increased expression of various antioxidative proteins, including PRX II.

Indirect activators often function by influencing cellular signaling pathways associated with oxidative stress. Compounds like Curcumin, Quercetin, Resveratrol, and Piperlongumine modulate oxidative stress levels, either by scavenging reactive oxygen species (ROS) or by influencing other cellular processes, which in turn leads to an upregulation of PRX II activity. This compensatory mechanism is vital in maintaining cellular redox balance and protecting cells from oxidative damage. Zinc Pyrithione is another example of an indirect activator that works by affecting the overall antioxidative response of cells. The diversity in the chemical structure and mode of action of these activators highlights the intricate network of pathways involved in regulating PRX II and its critical role in maintaining cellular homeostasis under stress conditions. By understanding these activators and their mechanisms, we can appreciate the complex regulation of antioxidative defenses in biological systems and the ability of these chemicals to influence PRX II activity.

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