Date published: 2025-9-21

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Gm128 Inhibitors

Gm128 inhibitors can be classified into various types based on their primary mode of action. The majority of these inhibitors target kinases involved in different cell signaling pathways that are generally associated with cell proliferation. For instance, inhibitors such as Palbociclib and Gefitinib target cyclin-dependent kinases and tyrosine kinases, respectively, thereby affecting the progression of the cell cycle and cellular proliferation. Another category includes mTOR inhibitors like Everolimus and Rapamycin, which specifically target the mTOR pathway, affecting downstream processes involved in cell growth and proliferation. Proteasome inhibitors like Bortezomib affect protein degradation and thus could impact the stability or functionality of Gm128. Furthermore, inhibitors such as Azacitidine operate at the epigenetic level, altering the gene expression landscape relevant to cell proliferation and may affect Gm128 functions.

The methodological approaches to these inhibitors span from targeting surface receptors to affecting intracellular processes. For example, multi-kinase inhibitors like Sorafenib and Nilotinib are relatively less selective but impact a broad range of kinases that are key nodes in the pathways involving Gm128. On the other hand, highly targeted kinase inhibitors like Trametinib or Vemurafenib can offer precise modulation of specific pathways, such as the MAPK pathway, that may be intricately linked with Gm128 functions. These inhibitors act either by competitively inhibiting the ATP binding sites of kinases or by allosteric inhibition, ultimately affecting the downstream targets and the role that Gm128 plays in cell proliferation.

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