Date published: 2025-12-23

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PUS7L Inhibitors

Chemical inhibitors of PUS7L can exert their inhibitory effects through a variety of mechanisms that impact the protein's function in post-translational RNA modification. The compound 6-Diazo-5-oxo-L-norleucine, a glutamine antagonist, can impede glutamine-dependent enzymes that may be crucial for the activity of PUS7L. The nucleotide analog 5-Fluorouracil is incorporated into RNA, which can disrupt RNA modifications involving PUS7L. Methotrexate, by limiting dihydrofolate reductase, reduces tetrahydrofolate levels, thus affecting nucleotide synthesis that is essential for PUS7L's function in RNA modification. Cycloheximide's interference with the translocation step in protein elongation can result in a deficiency of necessary protein factors for PUS7L's functioning. Puromycin, which mimics aminoacyl-tRNA, can reduce the synthesis of proteins that are integral to PUS7L's role, leading to inhibition of PUS7L. Actinomycin D inhibits RNA synthesis by intercalating into DNA, thus potentially reducing the availability of RNA substrates for PUS7L. Alpha-amanitin, a potent inhibitor of RNA polymerase II, can decrease RNA synthesis, thereby limiting the RNA substrates required for PUS7L's action.

Furthermore, Rifampicin targets the beta subunit of RNA polymerase to inhibit RNA transcription, which can reduce RNA availability for PUS7L. Tunicamycin prevents N-linked glycosylation, potentially affecting the glycosylation status of proteins that interact with PUS7L or its RNA substrates, thereby inhibiting PUS7L. Anisomycin's inhibition of peptidyl transferase activity on ribosomes can indirectly inhibit PUS7L by disrupting the synthesis of essential proteins for PUS7L's activity. Chloramphenicol, though it mainly targets bacteria, can inhibit PUS7L by affecting protein synthesis in eukaryotic mitochondria, which is vital for PUS7L's function. Lastly, Emetine impedes protein synthesis by blocking ribosomal movement along mRNA, which can lead to a reduction in available proteins necessary for PUS7L's RNA modification functions, resulting in the inhibition of PUS7L. Each chemical, through its distinct mechanism, can inhibit the functional activity of PUS7L by limiting the production or availability of crucial proteins and RNA substrates necessary for PUS7L's role in cellular processes.

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