Date published: 2025-9-16

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FAM98B Inhibitors

The proposed inhibitors for FAM98B primarily target protein synthesis and RNA metabolism, reflecting the known roles of this protein. Given FAM98B's involvement in these crucial cellular processes, affecting the broader mechanisms of protein and RNA dynamics could indirectly modulate its function. Cycloheximide, Puromycin dihydrochloride, Emetine, Harringtonin, Anisomycin, and Silvestrol are all inhibitors of protein synthesis, but they act at different stages of the translation process. For instance, Cycloheximide and Emetine inhibit the translocation step, Puromycin dihydrochloride causes premature chain termination, and Harringtonin blocks the initial elongation step. Silvestrol, targeting eIF4A, affects the initiation phase of protein synthesis. By disrupting these stages, these inhibitors could indirectly influence FAM98B's activity in the context of protein translation. In the realm of RNA metabolism, Actinomycin D and Fluorouracil are significant. Actinomycin D inhibits RNA polymerase, affecting RNA synthesis, while Fluorouracil interferes with the processing and function of RNA. KPT 330, by inhibiting XPO1, also impacts RNA transport, potentially affecting processes where FAM98B is involved. mTOR inhibitors like Rapamycin, AZD8055, and Torin 1 represent another approach, targeting the mTOR pathway which plays a crucial role in controlling protein synthesis. By modulating this pathway, these inhibitors can indirectly influence FAM98B's involvement in protein synthesis regulation. These inhibitors, through their action on protein synthesis and RNA metabolism, offer a way to indirectly affect FAM98B's function in cells. While they do not target FAM98B directly, their influence on the broader cellular processes in which FAM98B is involved provides valuable insight into the potential regulation and modulation of this protein's activity.

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