The inhibitors listed here target various signaling pathways and cellular mechanisms that may indirectly influence the activity and functions of LMO7. These compounds offer valuable insights into the complex biological roles and regulatory networks in which LMO7 is involved, particularly in relation to cytoskeletal dynamics and cell adhesion. Inhibitors such as Y-27632, Blebbistatin, and ML-7, targeting ROCK, myosin II, and MLCK respectively, are particularly significant for understanding LMO7's involvement in cytoskeletal organization. By influencing these elements of the cytoskeleton, these compounds can shed light on the role of LMO7 in cellular structure and motility.
Compounds like PD98059, LY294002, and SB203580, which inhibit various components of the MAPK, PI3K, and p38 MAPK pathways, provide insights into the signaling pathways that might intersect with LMO7's functions in cell signaling and adhesion. These pathways are crucial in transmitting external signals to the cellular machinery, impacting processes like gene expression and cellular response to environmental cues. Moreover, inhibitors such as CCG-1423 and NSC23766, targeting the RhoA/SRF and Rac1 pathways, respectively, underscore the importance of these pathways in cell adhesion and motility, processes where LMO7 may play a role. Additionally, Wiskostatin and Forskolin, affecting N-WASP and cAMP signaling, respectively, further highlight the broader cellular contexts and signaling environments that can influence LMO7's function.
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