Date published: 2025-9-14

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LZIC Inhibitors

Chemical inhibitors of LZIC function through various mechanisms by influencing the cellular pathways and processes with which this protein is associated. Staurosporine, a known inhibitor of protein kinase C (PKC), disrupts the Wnt/β-catenin pathway, crucial for cellular signaling and gene expression regulation. Since LZIC is associated with this pathway, Staurosporine's inhibition of PKC leads to a downstream effect on LZIC, impairing its functional role in the pathway. Rapamycin targets the mTOR pathway, integral for cell growth and cycle progression. Given LZIC's involvement in cell cycle regulation, the inhibition of mTOR by Rapamycin indirectly hinders LZIC's role in these processes. Similarly, LY 294002, by inhibiting PI3K, and PD 98059, by targeting MEK in the MAPK/ERK pathway, indirectly impact LZIC's function.

Additional chemicals, such as SB 203580 and SP600125, inhibit specific kinases like p38 MAPK and JNK, respectively. These kinases are involved in stress response and apoptosis, processes in which LZIC plays a part. Therefore, the inhibition of these kinases can indirectly reduce LZIC's effectiveness in regulating these cellular responses. U0126, another MEK inhibitor, further emphasizes the role of MAPK/ERK pathway inhibition in indirectly influencing LZIC function. Bortezomib's role in inhibiting proteasome activity impacts the degradation of proteins involved in the cell cycle, thereby indirectly inhibiting LZIC's function in these processes. Thapsigargin and Nutlin-3, by disrupting calcium signaling and the p53-MDM2 interaction respectively, also indirectly impair LZIC's role in cellular regulation. Lastly, HDAC inhibitors like Trichostatin A and Suberoylanilide Hydroxamic Acid, by altering gene expression patterns, have the potential to indirectly inhibit LZIC's function in the regulation of the cell cycle. These diverse chemicals, though not directly targeting LZIC, exert their influence on various cellular pathways and processes, resulting in the inhibition of LZIC's functional role within these contexts.

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