Date published: 2025-9-14

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KIAA1737 Inhibitors

KIAA1737 inhibitors employ a variety of biochemical mechanisms to achieve functional inhibition of this protein. Certain inhibitors target kinases that are crucial for the activity of KIAA1737, blocking ATP binding sites and thereby reducing its kinase activity. Others specifically inhibit phosphoinositide 3-kinases, leading to the deactivation of downstream targets such as AKT, which is necessary for the full functionality of KIAA1737. Additional mechanisms involve the disruption of mTOR signaling, which plays a vital role in regulating KIAA1737's function. There are also inhibitors that prevent the activation of the MAPK/ERK and p38 MAP kinase pathways, both of which are integral to the modulation of KIAA1737 activity. By blocking MEK1/2 or JNK, these inhibitors alter critical signaling processes, which can lead to a decrease in KIAA1737 activity.

Further inhibitory actions are achieved through different molecular pathways. The use of a proteasome inhibitor can lead to an accumulation of misfolded proteins, thereby affecting the stability and function of KIAA1737. Inhibitors targeting histone deacetylases can alter chromatin structure and gene expression patterns, which may indirectly impact the activity of KIAA1737. Another approach involves the inhibition of cyclin-dependent kinases, which are known to influence cell cycle progression and could thus affect the activity of KIAA1737. Moreover, inhibitors that interfere with mitotic processes, such as those targeting Aurora kinases, could affect KIAA1737, particularly if this protein has roles in cell division.

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