Date published: 2025-10-31

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TFB1M Inhibitors

TFB1M inhibitors encompass a range of chemicals that interfere with cellular and mitochondrial processes, which can indirectly affect the function of TFB1M, a mitochondrial transcription factor involved in mitochondrial DNA transcription and rRNA methylation. These compounds do not interact with TFB1M directly but can modulate the cellular environment or the mitochondrial processes in a way that influences the activity of TFB1M. For instance, several of these chemicals target the mitochondrial electron transport chain at various points: Rotenone, Antimycin A, and Azide inhibit different complexes, leading to a decrease in mitochondrial membrane potential, ATP synthesis, and overall mitochondrial function. This can create an environment that is less conducive to the functions TFB1M performs.

Other compounds listed, such as Oligomycin A, Atractyloside, and FCCP, have specific effects on the mitochondrial ATP synthesis and transmembrane potential, again impacting the energy status of the mitochondrion and indirectly the processes TFB1M is involved in. Actinonin, Chloramphenicol, and Doxycycline disrupt mitochondrial protein synthesis at different stages, from maturation to actual protein synthesis, which can have downstream effects on mitochondrial gene expression and hence on TFB1M's role. MitoPQ induces oxidative stress within the mitochondria, potentially affecting all mitochondrial processes including those governed by TFB1M. Lastly, Cerulenin and Tunicamycin affect lipid synthesis and protein glycosylation, respectively, which can alter the mitochondrial membrane integrity and protein import, indirectly influencing TFB1M's function in the mitochondria. These chemicals provide a diverse toolkit for modulating mitochondrial function and indirectly influencing the activity of TFB1M.

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