The intricate molecular realm within cells hosts several chemicals capable of modulating the presence and function of Ribosomal Protein S17 (RPS17). For instance, Actinomycin D binds to DNA and restricts RNA synthesis, thereby establishing a heightened need for ribosomal proteins, encompassing RPS17. In a similar vein, Cycloheximide, which curtails peptide elongation during translation, can enhance the synthesis of ribosomal proteins, including RPS17. The action of 5-Azacytidine as a DNA methyltransferase inhibitor holds the potential to remodel gene expression, thereby having a bearing on the synthesis dynamics of RPS17.
Chemicals like Homoharringtonine, by intervening in the ribosomal machinery and halting protein synthesis, can catalyze a surge in RPS17 production. Anisomycin, through its activity on peptidyl transferase, interrupts protein synthesis, potentially driving RPS17 production. Furthermore, the influence of Rapamycin as an mTOR inhibitor sheds light on its potential to augment compensatory RPS17 synthesis, given mTOR's pivotal role in overseeing ribosome biogenesis. Such chemicals underscore the multifaceted molecular interventions that can decisively shape the cellular levels of RPS17.
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