Date published: 2025-9-18

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C35 Inhibitors

Chemical inhibitors of C35 can exert their inhibitory effects through various mechanisms targeting the signaling pathways C35 is involved in. Palbociclib targets CDK4/6, which are kinases downstream of C35 signaling, and by inhibiting these kinases, it can lead to cell cycle arrest, thereby functionally inhibiting C35 by preventing its role in cell proliferation. Similarly, Trametinib and U0126 function as inhibitors of MEK, a critical kinase in the MAPK pathway. Since C35 is involved in MAPK signaling, the action of these inhibitors can lead to a decrease in ERK phosphorylation and activity, which is a necessary step for C35 to exert its function. LY294002 is another inhibitor that acts on the PI3K/AKT pathway, a pathway known to involve C35. By inhibiting PI3K, LY294002 can reduce AKT activation and thus functionally inhibit C35 by hindering the pathway's propagation.

Further down the line of signaling, Rapamycin inhibits mTOR, a central component of the mTOR signaling pathway that interacts with C35 function. Inhibition of mTOR by Rapamycin can suppress the protein synthesis and cell growth effects mediated by C35. Sorafenib's action is a bit broader; it targets several kinases that are part of signaling pathways in which C35 operates. By doing so, Sorafenib can reduce the functional activity of C35 by blocking several of its downstream effects. Erlotinib focuses on the EGFR tyrosine kinase, which, upon activation, can initiate a cascade that includes C35. By inhibiting EGFR, Erlotinib can prevent the activation of downstream components of the pathway, including C35. Selumetinib, like Trametinib and U0126, specifically inhibits MEK1/2 and thus impedes the MAPK/ERK signaling, which is necessary for C35 function. Dasatinib and Sunitinib, by inhibiting Src family kinases and multiple receptor tyrosine kinases respectively, can disrupt crucial signaling networks in which C35 participates, leading to an overall functional inhibition of C35. SP600125 inhibits JNK, which, by being involved in the same signaling pathways as C35, leads to a decrease in the functional role of C35 when JNK is inhibited. Lastly, PF-562271 targets FAK/Pyk2, which are involved in integrin signaling and cellular adhesion processes. By inhibiting these kinases, PF-562271 can disrupt the signaling cascades that facilitate C35's involvement in these processes, thus inhibiting its functional role.

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