Date published: 2025-11-22

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PRPSAP2 Activators

Compounds like Forskolin, IBMX, and Ionomycin elevate intracellular levels of critical second messengers-cAMP and calcium, respectively-which can lead to the activation of downstream kinases such as PKA that are pivotal in phosphorylation cascades. This can indirectly affect PRPSAP2, presuming that the protein is regulated by such phosphorylation events. PMA, acting through PKC, and growth factors like EGF, which trigger receptor tyrosine kinase pathways, can similarly initiate a series of phosphorylation events that may modulate PRPSAP2 activity.

On the other hand, metabolic regulators such as insulin and metformin can elicit broad effects on cellular signaling, touching upon pathways that could intersect with PRPSAP2 regulation. Insulin activates a well-known cascade that can influence numerous proteins, while 1,1-Dimethylbiguanide, Hydrochloride, by activating AMPK, modulates metabolic pathways that could have downstream effects on PRPSAP2. The influence of kinase inhibitors like LY294002, PD98059, SB203580, SP600125, and Rapamycin underscores the significance of phosphorylation in protein regulation. By selectively inhibiting kinases such as PI3K, MEK, p38 MAPK, JNK, and mTOR, these compounds can alter the phosphorylation landscape and, consequently, the activity of proteins within these pathways, which may include PRPSAP2.

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