Date published: 2025-9-15

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RPUSD1 Activators

Nucleoside analogs like 5-Azacytidine may incorporate into RNA, thereby engaging with the RNA maturation machinery and influencing the function of proteins such as RPUSD1. MG132 can raise the intracellular concentration of various proteins, including those that participate in RNA processing, possibly enhancing the functional role of RPUSD1. Compounds like Chloroquine alter lysosomal pH, which may reverberate through the pathways that RPUSD1 is a part of, affecting its activity. Leptomycin B, by inhibiting nuclear export, indirectly enriches the nuclear milieu with RNA processing factors, potentially optimizing the conditions for RPUSD1's role in tRNA maturation. Rapamycin modulates ribosomal biogenesis, a process closely linked to tRNA synthesis and processing, thereby indirectly influencing RPUSD1 activity. Actinomycin D, binding to DNA, impedes RNA synthesis, which could lead to adjustments in the processing dynamics of RPUSD1.

Compounds that induce stress responses, such as Sodium arsenite and Menadione, may tweak the signaling pathways and create a cellular state that affects RPUSD1, while antibiotics like Puromycin disrupt protein synthesis, impacting the processing proteins' demand and possibly RPUSD1's activity. Autophagy inducers like Spermidine may alter protein turnover, influencing the levels of RPUSD1 indirectly. DRB, as a transcription inhibitor, can modulate RNA levels and thus the operational context of RPUSD1, while β-Estradiol could influence the expression of genes and proteins involved in tRNA processing, potentially affecting RPUSD1 activity.

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