Date published: 2025-11-1

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FAM90A Activators

The activity of FAM90A can be influenced by several chemical activators through distinct signaling pathways. One such pathway involves the elevation of intracellular cAMP, which is a key second messenger in various cellular responses. The increase in cAMP levels is known to activate protein kinase A (PKA), a kinase that can target a multitude of proteins for phosphorylation. This activation cascade is initiated by compounds that directly stimulate adenylyl cyclase or mimic cAMP, leading to subsequent activation of PKA. As PKA becomes active, it may phosphorylate FAM90A, thereby increasing its functional activity. Additionally, the beta-adrenergic pathway, which also culminates in the elevation of cAMP levels, can be triggered by specific agonists, subsequently activating PKA and potentially enhancing the phosphorylation and activity of FAM90A. Furthermore, the modulation of intracellular calcium levels can activate calcium-dependent protein kinases, which in turn might target FAM90A for phosphorylation, serving as another mechanism for its activation.

Another route for the activation of FAM90A involves the inhibition of protein phosphatases such as PP1 and PP2A. Certain toxins that inhibit these phosphatases result in a general increase in the phosphorylation state of cellular proteins, which could include FAM90A, leading to its enhanced activity. Stress response pathways also play a role in the activation of FAM90A, as some compounds can activate stress-activated protein kinases like JNK, which are known to phosphorylate various target proteins. Additionally, the inhibition of specific enzymes such as GSK-3 can lead to the induction of signaling pathways that may indirectly influence the activity of FAM90A. GSK-3 is involved in a wide array of cellular functions, and its inhibition can result in the stabilization and activation of several proteins through the prevention of their degradation or through the initiation of alternative signaling cascades. For instance, the Wnt signaling pathway, when activated by inhibiting GSK-3, can lead to the accumulation and translocation of β-catenin to the nucleus, where it can influence the transcription of genes that may include those coding for FAM90A or proteins that modulate its activity.

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