Date published: 2025-9-12

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BST-2 Inhibitors

BST-2 inhibitors belong to a specific class of molecules designed to target the cellular protein known as Bone Marrow Stromal Antigen 2 (BST-2), also commonly referred to as Tetherin or CD317. BST-2 is a crucial component of the innate immune system, primarily responsible for restricting the release of enveloped viruses from infected cells. To accomplish this, BST-2 is anchored in the cellular membrane, extending both extracellularly and intracellularly. On the extracellular side, it binds to the viral envelope proteins, hindering their incorporation into budding virions. Intracellularly, BST-2 interacts with cellular machinery to tether the virus to the host cell's surface. This dual role effectively traps the virus, limiting its spread. BST-2 inhibitors, on the other hand, are chemical compounds or molecules designed to interfere with the function of BST-2, thus facilitating the release of enveloped viruses from infected cells.

One of the primary mechanisms by which BST-2 inhibitors operate is by disrupting the protein-protein interactions necessary for BST-2's tethering function. These inhibitors can competitively bind to BST-2, stopping it from interacting with viral envelope proteins or the cellular machinery required for tethering. By doing so, BST-2 inhibitors weaken the cellular restriction on virus release, allowing newly formed virions to bud off from infected cells more easily. Researchers have developed a range of BST-2 inhibitors with varying mechanisms of action, including small molecules and peptides, to modulate BST-2's activity. These inhibitors hold promise as tools for better understanding the biology of virus-host interactions and may have implications in various research areas.

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