Date published: 2025-9-17

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CMYA5 Inhibitors

Chemical inhibitors of CMYA5 can achieve functional inhibition through various mechanisms by targeting specific pathways integral to muscle function and structure. Blebbistatin, by inhibiting myosin II ATPase activity, disrupts the contractile machinery that CMYA5 is part of, leading to inhibition of CMYA5's role in force transduction within the muscle cells. Similarly, ML-7 targets myosin light chain kinase (MLCK), which is essential for phosphorylation processes that affect myofibril function. This inhibition can have a downstream effect on the structural integrity of myofibrils, thus affecting CMYA5's functionality. Y-27632, a ROCK inhibitor, can lead to decreased actomyosin contractility, which would upset the structural context in which CMYA5 operates, resulting in its functional inhibition. Gö6976, by inhibiting Protein Kinase C (PKC), might affect the phosphorylation of proteins within the sarcomere, impacting CMYA5's role and inhibiting its function. SB-203580 and PD 98059, by inhibiting p38 MAP kinase and MEK respectively, can disrupt the signaling pathways involved in muscle cell stress responses, which could in turn influence CMYA5's ability to respond to mechanical stress.

The second set of chemicals operates by influencing various signaling pathways that indirectly affect CMYA5's function within the muscle tissue. H-89 inhibits Protein Kinase A (PKA), which could alter the phosphorylation state of structural proteins in myocytes, thus affecting CMYA5. Wortmannin and LY294002, both PI3K inhibitors, can inhibit the downstream AKT signaling pathway, affecting cell survival and growth pathways that are crucial for maintaining the muscle cell architecture where CMYA5 is active. KN-93's inhibition of CaMKII affects calcium signaling, which is intimately linked to CMYA5's role in the muscle cells by disrupting calcium-dependent processes. U0126 disrupts the MEK/ERK pathway, which is known to regulate muscle cell function and growth, thus indirectly inhibiting CMYA5. Lastly, GF 109203X, another PKC inhibitor, affects CMYA5 by reducing PKC-mediated signaling, which is important for the maintenance of structural and functional integrity of the myocyte components associated with CMYA5.

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