Date published: 2025-10-11

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ANKRD61 Activators

Chemical activators of ankyrin repeat domain 61 can engage various intracellular signaling pathways to enhance the functional activity of this protein. Forskolin acts by directly stimulating adenylate cyclase, leading to an increase in cyclic AMP (cAMP) levels within the cell. The elevated cAMP subsequently activates protein kinase A (PKA), which is known to phosphorylate a wide array of proteins. The phosphorylation by PKA can target ankyrin repeat domain 61, culminating in its activation. Another chemical, IBMX, operates by inhibiting phosphodiesterases, which are enzymes responsible for the breakdown of cAMP. By preventing cAMP degradation, IBMX effectively amplifies the signal initiated by forskolin, leading to sustained PKA activity and prolonged phosphorylation and activation of ankyrin repeat domain 61.

In parallel to the cAMP-PKA axis, other signaling molecules like PMA and 4-Phorbol activate protein kinase C (PKC), which phosphorylates numerous substrates within the cell. The activation of PKC can lead to the phosphorylation of ankyrin repeat domain 61, enhancing its activity. Calcium signaling is another pivotal pathway; chemicals like Ionomycin and A23187 increase intracellular calcium levels, which can activate calmodulin-dependent kinases (CaMK). These kinases are capable of phosphorylating an array of proteins, and this cascade has the capacity to include ankyrin repeat domain 61 as a substrate, resulting in activation. Thapsigargin, by inhibiting the SERCA pump, also induces a rise in cytosolic calcium, potentially engaging the same calcium-dependent kinases to activate ankyrin repeat domain 61. Additionally, inhibitors of protein phosphatases such as Calyculin A and Okadaic Acid lead to increased phosphorylation states of proteins by preventing their dephosphorylation. This biochemical blockade could maintain ankyrin repeat domain 61 in a phosphorylated, hence active, state. Anisomycin, a stress-activated protein kinase activator, and Cantharidin, a phosphatase inhibitor, can also contribute to the phosphorylation and consequent activation of ankyrin repeat domain 61. Finally, 8-Br-cAMP, a synthetic analogue of cAMP, binds and activates PKA, thus potentially phosphorylating and activating ankyrin repeat domain 61 in a manner akin to the natural cAMP response.

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