Date published: 2025-10-29

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MORN1 Inhibitors

Chemical inhibitors of MORN repeat-containing protein 1 (MORN1) function through various mechanisms to disrupt the protein's involvement in cell morphology and actin cytoskeleton organization. Wiskostatin, CK 666, and SMIFH2 target crucial interactions and processes central to MORN1's function. Wiskostatin can inhibit MORN1 by altering its interaction with the actin cytoskeleton, thus impacting cell morphology and motility. CK 666 focuses on inhibiting MORN1 by targeting the Arp2/3 complex, which is essential for actin polymerization, a process in which MORN1 is potentially involved. SMIFH2's action on formin-mediated actin assembly further contributes to the inhibition of MORN1's role in organizing the actin cytoskeleton. Cytochalasin D and Latrunculin A, by inhibiting actin polymerization, directly affect the structural integrity of the actin cytoskeleton, thereby impacting MORN1's associated functions. Cytochalasin D achieves this by disrupting actin filament formation, while Latrunculin A binds to actin monomers, preventing their polymerization.

In the second aspect of inhibition, Jasplakinolide, Blebbistatin, Y-27632, ML-7, Wortmannin, LY 294002, and PD 98059 target various signaling pathways and interactions that influence MORN1's function. Jasplakinolide, by stabilizing actin filaments, alters actin dynamics crucial for MORN1's role in cell morphology. Blebbistatin inhibits MORN1 by affecting myosin II activity, thus influencing cellular processes where MORN1 collaborates with myosin II. Y-27632 and ML-7 disrupt Rho-associated kinase pathways and myosin light chain kinase, respectively, both of which are important for MORN1's involvement in actin-myosin interactions. Wortmannin and LY 294002, as PI3K inhibitors, affect the PI3K/Akt pathway, potentially impacting MORN1's role in cellular signaling. PD 98059, a MEK inhibitor, further contributes to the inhibition of MORN1 by affecting the MAPK/ERK pathway. Each of these chemicals, through their specific actions, contributes to the inhibition of MORN1, thereby impacting its role in cell morphology, actin cytoskeleton organization, and related signaling pathways.

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