Date published: 2025-10-11

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4921511M17Rik Inhibitors

Chemicals classified as indirect Samt1b inhibitors comprise a diverse group that can influence cell metabolism, protein folding and trafficking, cell signaling pathways, and gene expression. These compounds interact with various cellular mechanisms that can indirectly modulate the function or expression of Samt1b, which might be implicated in processes such as spermatogenesis. For instance, GW501516 and 2-Deoxy-D-glucose target metabolic pathways such as fatty acid oxidation and glycolysis, respectively. Changes in these metabolic pathways can alter the energy balance within the cell, which can influence processes related to Samt1b. Oligomycin A and Tunicamycin have the potential to disrupt ATP production and protein glycosylation, respectively. These disruptions can affect protein function and trafficking within the cell, which in turn, can influence the membrane localization or function of Samt1b.

The inhibitors MG132 and Chloroquine can impact protein turnover by interfering with proteasome-mediated degradation and autophagy, respectively. These processes are crucial for the regulation of protein levels in the cell, including Samt1b. Rapamycin, PD98059, and LY294002 target key signaling pathways such as mTOR, MAPK/ERK, and PI3K/AKT, respectively. The modulation of these pathways can affect cellular growth and division, as well as the response to external signals, which can have consequences for proteins involved in these processes, including Samt1b. Cyclopamine and Retinoic acid, by influencing the Hedgehog pathway and gene expression through retinoic acid receptors, respectively, can also affect cellular pathways where Samt1b may play a role.

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