Slac2-c inhibitors are a class of chemical compounds that specifically target and inhibit the activity of the protein Slac2-c, also known as synaptotagmin-like protein 2-c. Slac2-c is a member of the Rab27A effector family and plays an essential role in vesicle transport and membrane trafficking within cells. It functions by interacting with Rab27A, a small GTPase involved in the regulation of vesicle docking and fusion, especially in secretory pathways. Slac2-c acts as an adaptor protein that connects Rab27A with molecular motors such as myosin, facilitating the transport of vesicles along actin filaments toward their target membranes. Inhibitors of Slac2-c work by binding to critical regions of the protein, disrupting its interaction with Rab27A or other molecular components, thus interfering with its role in vesicular trafficking.
The design and study of Slac2-c inhibitors are based on a thorough understanding of the protein's structure and its interactions with other molecules involved in vesicle transport. Researchers typically employ structural biology techniques such as molecular docking, X-ray crystallography, and computational modeling to identify potential binding sites on Slac2-c that are critical for its function. Inhibitors are developed to specifically bind to these sites, blocking the protein's ability to mediate vesicle transport. These inhibitors are evaluated using various biochemical assays to measure their binding affinity, specificity, and inhibitory effects on vesicle movement. By inhibiting Slac2-c, researchers can gain insights into the mechanisms underlying vesicle trafficking, membrane fusion, and how these processes contribute to cellular organization and function. The study of Slac2-c inhibitors expands the understanding of intracellular transport systems, revealing the importance of adaptor proteins like Slac2-c in coordinating vesicular dynamics and cellular cargo movement.
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