Date published: 2025-12-25

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HECA Inhibitors

Chemical inhibitors of HECA protein operate through various molecular pathways to modulate the activity of this protein. Staurosporine and Go6983, both protein kinase C inhibitors, can disrupt downstream signaling that involves HECA protein. By blocking protein kinase C, they reduce phosphorylation of targets that are presumably necessary for HECA protein's regulatory functions. Similarly, LY294002 and Wortmannin target phosphoinositide 3-kinase, resulting in the blockade of activation signals crucial for HECA protein's roles in cellular processes such as migration and adhesion. These inhibitors collectively act by impeding the phosphorylation cascade that would normally involve the HECA protein, thus inhibiting its activity.

Further along these lines, PD98059 and U0126, as inhibitors of MEK, suppress the MAPK/ERK signaling pathway, a route thought to be significant for HECA protein's involvement in organizing the actin cytoskeleton. SB203580's selective inhibition of p38 MAP kinase and SP600125's inhibition of c-Jun N-terminal kinase interfere with stress responses and transcriptional regulation, respectively, which are processes potentially regulated by HECA protein. Inhibition of these kinases can therefore reduce HECA protein's influence on these cellular responses. NF449, by selectively inhibiting the Gs-alpha subunit of G proteins, disrupts G protein-coupled receptor signaling that HECA protein may depend on. ML7, through its inhibition of myosin light chain kinase, can diminish HECA protein's role in cellular motility. Additionally, BAPTA-AM, by chelating intracellular calcium, can affect calcium-mediated activation of HECA protein, leading to a reduction in its activity in signaling pathways where calcium is a key secondary messenger. Collectively, these inhibitors provide a multifaceted approach to modulating HECA protein's activity within cells by targeting various signaling mechanisms and kinases that contribute to its function.

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