Epidermal Growth Factor, upon binding to its receptor, launches a signaling cascade with the potential to enhance the transcription of a range of proteins, possibly including ANKRD13B. Insulin, engaging its receptor pathway, orchestrates a symphony of changes in protein synthesis, in which ANKRD13B's function may be involved. Forskolin, by stimulating adenylate cyclase, raises cAMP levels within the cell, which can lead to a domino effect altering protein expression and function, affecting proteins like ANKRD13B.
PMA activates protein kinase C, a key player in the phosphorylation of various proteins, which might have implications for the modulation of ANKRD13B. Ionomycin increases intracellular calcium, another pivotal ion in cellular signaling, with the potential to impact ANKRD13B's activity. LY294002 specifically targets PI3K, causing a ripple effect in AKT signaling that might reach ANKRD13B. Similarly, the inhibition of p38 MAPK by SB203580, and JNK by SP600125, may lead to alterations in signaling pathways that could extend to the regulation of ANKRD13B. U0126 and PD98059, both inhibitors of MEK, could have downstream effects on the ERK pathway, potentially influencing how ANKRD13B functions. Dibutyryl cAMP, a synthetic analog of cAMP, directly activates PKA, which is known to regulate a plethora of proteins, potentially including ANKRD13B. Rapamycin, by inhibiting mTOR, affects protein synthesis and degradation pathways, which can have consequences for the levels and activity of ANKRD13B.
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| Product Name | CAS # | Catalog # | QUANTITY | Price | Citations | RATING |
|---|---|---|---|---|---|---|
Rapamycin | 53123-88-9 | sc-3504 sc-3504A sc-3504B | 1 mg 5 mg 25 mg | $62.00 $155.00 $320.00 | 233 | |
Inhibits mTOR, which can impact protein synthesis and degradation pathways, potentially affecting ANKRD13B levels. | ||||||