Date published: 2025-9-16

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MRP-L11 Inhibitors

MRP-L11 inhibitors primarily refer to compounds that can influence the activity or function of the MRP-L11 protein, a component of the mitochondrial ribosome. While direct chemical inhibitors of MRPL11 might not be well-characterized, several compounds have been identified that can influence mitochondrial ribosomal function and translation, which can indirectly modulate MRPL11's activity. Antibiotics like Doxycycline, Tigecycline, Chloramphenicol, and Linezolid, for instance, possess the ability to inhibit mitochondrial protein synthesis by targeting bacterial-type ribosomes, which are evolutionarily similar to mitochondrial ribosomes. Dactinomycin, by binding to DNA, inhibits mitochondrial RNA synthesis, further hampering protein production in mitochondria.Then there are compounds affecting mitochondrial energetics. Valinomycin, for example, disrupts the mitochondrial membrane potential, crucial for ATP production. Oligomycin, Rotenone, and Antimycin A each target different complexes of the electron transport chain, thus impacting mitochondrial energy metabolism. CCCP operates by uncoupling oxidative phosphorylation, undermining ATP synthesis in mitochondria. Lastly, molecules such as Mdivi-1 and Tenofovir impact mitochondrial dynamics and DNA synthesis, respectively. Mdivi-1 inhibits mitochondrial division, affecting the organelle's overall dynamics and function. In contrast, Tenofovir, a nucleotide analog, affects mitochondrial DNA synthesis, which can influence the overall protein synthesis machinery, including ribosomal proteins like MRPL11.

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