Date published: 2025-10-13

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T-Plastin Inhibitors

The chemical class of T-Plastin inhibitors consists of a diverse range of compounds that indirectly influence the function of T-Plastin by targeting the actin cytoskeleton and related cellular processes. These inhibitors interact with various components of the cytoskeletal architecture and modulate actin dynamics, impacting T-Plastin's role in cytoskeletal organization and cell signaling. Compounds such as Cytochalasin D, Latrunculin A, Jasplakinolide, and Swinholide A directly affect actin filament dynamics. Cytochalasin D and Latrunculin A inhibit actin polymerization, potentially disrupting the structural framework where T-Plastin operates. Jasplakinolide and Phalloidin stabilize actin filaments, which could alter T-Plastin's interactions with these structures. Swinholide A's actin-severing ability further influences the actin network that T-Plastin helps to organize and maintain.

In addition to actin-targeting compounds, inhibitors of kinases and proteins involved in actin cytoskeleton signaling pathways, such as Y-27632, ML-7, and Blebbistatin, play a significant role. Y-27632 inhibits the Rho-associated kinase (ROCK), crucial for actin cytoskeleton rearrangement, potentially affecting T-Plastin's activity. ML-7 targets myosin light chain kinase, and Blebbistatin inhibits myosin II, both influencing the contractile forces within the cytoskeleton, which can impact T-Plastin's role in cytoskeletal organization.

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