Date published: 2025-9-11

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OTTMUSG00000016698 Inhibitors

Synovial sarcoma, X member B family member (Gm14459), is a protein crucial for various cellular processes, and its inhibition can be achieved through several mechanisms involving specific chemical compounds. One approach involves direct inhibition using small molecules like Imatinib and Gefitinib. Imatinib, for instance, acts as a potent inhibitor by targeting the active site of Gm14459, thereby obstructing its enzymatic function within the cell. Similarly, Gefitinib directly inhibits Gm14459 by binding to its active site, effectively preventing the protein from carrying out its cellular roles. Alternatively, indirect inhibition of Gm14459 can be accomplished by targeting signaling pathways associated with its activity. Sorafenib is an example of such an inhibitor; it disrupts the signaling pathways that support Gm14459's function, leading to a reduction in its activity. Another indirect inhibitor, SB203580, modulates a crucial pathway linked to Gm14459, ultimately resulting in the functional inhibition of the protein. These indirect inhibitors demonstrate the ability to hinder Gm14459 by interfering with the cellular processes that regulate its activity.

Furthermore, molecules like Wortmannin and LY294002 inhibit Gm14459 by affecting post-translational modifications and blocking downstream effectors, respectively. Wortmannin disrupts the post-translational modifications essential for Gm14459's proper functioning, while LY294002 indirectly inhibits the protein by interfering with a downstream effector within the pathway associated with Gm14459's activity. These mechanisms showcase the diverse ways in which chemical compounds can effectively inhibit the function of Gm14459, shedding light on potential strategies for modulating its cellular roles. In summary, the inhibition of synovial sarcoma, X member B family member (Gm14459), can be achieved through various chemical compounds, both directly and indirectly. These compounds target specific aspects of Gm14459's function, ranging from its active site to key signaling pathways, thereby providing valuable insights into potential strategies for functional inhibition.

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