Date published: 2025-9-10

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β-defensin 135 Inhibitors

β-defensin 135 inhibitors are compounds that specifically interact with and inhibit the activity of the β-defensin 135 protein, a member of the β-defensin family. β-defensins are small, cysteine-rich cationic peptides that play important roles in various physiological processes, including immune responses and intercellular signaling pathways. β-defensin 135, like other members of its family, exhibits a structural framework defined by disulfide bonds that stabilize its three-dimensional conformation. These inhibitors typically work by binding to key regions on the β-defensin 135 protein, which may interfere with its ability to function in its native biological roles. The mechanisms of inhibition can vary based on the chemical nature of the inhibitor, ranging from small molecules that bind to specific active sites to larger peptides that can sterically hinder the functional regions of β-defensin 135.

The development and study of β-defensin 135 inhibitors require an understanding of both the structural properties of the protein and the inhibitors themselves. The chemical features of the inhibitors-such as their molecular weight, polarity, and the presence of functional groups capable of interacting with the amino acid residues of β-defensin 135-are crucial for their efficacy in inhibiting the protein's function. Additionally, computational modeling techniques such as molecular docking and dynamics simulations have proven invaluable in predicting the binding affinity and interaction modes between inhibitors and β-defensin 135. These studies help in identifying specific regions on the β-defensin 135 protein that are critical for inhibitor binding. Advanced spectroscopic techniques, including NMR and X-ray crystallography, are also employed to elucidate the exact molecular interactions between inhibitors and the β-defensin 135 protein, providing further insights into their inhibitory mechanisms.

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