Date published: 2025-9-15

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TMEM34 Activators

The chemicals listed above are selected for their potential to modulate cellular processes that are generally relevant to the function or expression of transmembrane proteins, including TMEM34. While they are not direct activators of TMEM34, their influence on membrane dynamics, protein modifications, and cellular signaling pathways can indirectly affect the activity and function of transmembrane proteins. Cholesterol modulators like Simvastatin can influence membrane fluidity, which is crucial for the function of membrane proteins. Glycosylation inhibitors such as Tunicamycin may impact the glycosylation status of transmembrane proteins, affecting their stability and function.

Farnesyltransferase inhibitors, proteasome inhibitors, and palmitoylation inhibitors, like Tipifarnib, Bortezomib, and 2-Bromopalmitate, respectively, affect various post-translational modifications and degradation pathways that can be important for the function and regulation of transmembrane proteins. Compounds such as W-7 Hydrochloride and Src family kinase inhibitors like Dasatinib influence signaling pathways and phosphorylation processes that may impact transmembrane protein activity. PI3K/Akt pathway inhibitors, autophagy inhibitors, and ER stress modulators can also affect cellular processes and stress responses that are crucial for the function of membrane proteins. Lastly, HDAC inhibitors like Trichostatin A can modulate gene expression, potentially influencing the expression levels of transmembrane proteins. In summary, these chemicals represent a diverse range of compounds that can influence the cellular environment, post-translational modifications, and signaling pathways. While they do not specifically target TMEM34, their effects on these broader biological processes could potentially modulate the function or expression of TMEM34 and similar transmembrane proteins.

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