Date published: 2025-11-24

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AARSD1 Inhibitors

AARSD1 inhibitors like Cycloheximide and Emetine are known to interfere with protein synthesis, which would reduce the production of AARSD1 along with other proteins. Compounds like Halofuginone and Rapamycin target specific enzymatic activities or signaling pathways, such as aminoacyl-tRNA synthetase activity and the mTOR pathway, respectively. The inhibition of these pathways can decrease the functional availability of AARSD1 within the cell. Other compounds like Tunicamycin, Brefeldin A, and Thapsigargin affect the post-translational modification, trafficking, and stability of proteins. Tunicamycin's interference with glycosylation, Brefeldin A's disruption of protein transport, and Thapsigargin's perturbation of calcium homeostasis can lead to a less conducive environment for AARSD1's stability or trafficking, indirectly diminishing its functional presence.

Moreover, metabolic inhibitors like 2-Deoxyglucose can disturb the energy balance within the cell, potentially affecting the energy-dependent processes of protein synthesis, wherein AARSD1 is included. Chloroquine and MG132 can influence the degradation of proteins; Chloroquine by altering autophagic processes and MG132 by inhibiting the proteasome, which can result in an accumulation of dysfunctional AARSD1.

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