Date published: 2025-9-11

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ZBTB42 Activators

The realm of ZBTB42, a zinc finger protein associated with skeletal muscle development, has its intricacies intricately tied to various biochemical pathways. A notable pathway, the AMPK signaling route, has an instrumental role in maintaining muscle cell energy homeostasis. Chemicals like AICAR and Metformin actively engage with this pathway, creating a cellular environment conducive for the modulation of ZBTB42. The intrigue doesn't stop here. Delving deeper into muscle cell signaling, calcium homeostasis emerges as another pivotal player. Chemicals like Dantrolene can influence this delicate balance by targeting ryanodine receptors, thus setting the stage for an indirect influence on ZBTB42.

Further, the cyclic nucleotide signaling cascades, governed by cAMP and cGMP, are central to muscle cell differentiation and function. Chemicals such as Cilostazol, BAY 58-2667, and Rolipram can effectively modulate these pathways, thereby casting their indirect effects on proteins like ZBTB42. In the grand scheme of muscle cell function, metabolic regulators like Insulin and PPAR agonists (GW501516, Troglitazone) can steer the cellular dynamics, indirectly influencing the intricacies of ZBTB42's role. Lastly, autophagy and muscle contraction, cornerstones of muscle cell health and function, are influenced by chemicals like Chloroquine and Blebbistatin, respectively. These chemicals, by modifying the cellular milieu, can indirectly shape the activity and function of ZBTB42 in the skeletal muscle landscape. Through a systematic exploration of these chemicals and their associated pathways, the complex nexus of ZBTB42 activation is gradually unraveled, providing valuable insights into the broader matrix of muscle cell biology.

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