Date published: 2025-9-19

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LIR-4 Inhibitors

Chemical inhibitors of LIR-4 act through various molecular mechanisms to disrupt the signaling pathways essential for the protein's function. Wortmannin, for instance, is a selective inhibitor of phosphoinositide 3-kinases (PI3Ks), which play a pivotal role in the activation and function of LIR-4 by regulating the Akt signaling pathway. Similarly, LY294002 functions by inhibiting PI3Ks, leading to the downregulation of Akt signaling, which is crucial for LIR-4 activity. These inhibitors interfere with the early stages of LIR-4 signaling, thereby impairing its overall functional capacity. Dasatinib, on the other hand, targets Src family kinases, which are responsible for phosphorylating several downstream proteins that may include substrates involved in LIR-4 pathways. Through this inhibition, Dasatinib can suppress LIR-4 activation. U0126 and PD98059 both act as inhibitors of the MEK1/2 kinases within the MAPK/ERK pathway, which is another signaling route that LIR-4 may utilize for its function. By blocking MEK1/2, these compounds prevent the activation of downstream targets necessary for LIR-4's activity.

Moreover, SB203580 and SP600125 disrupt LIR-4 function by targeting other kinases within the signaling network. SB203580 is a specific inhibitor of p38 MAP kinase, a kinase potentially involved in regulating LIR-4-related pathways. By inhibiting p38, SB203580 can interfere with the requisite signaling for LIR-4's function. SP600125 inhibits JNK, part of the stress-activated protein kinases that may regulate LIR-4, leading to suppression of LIR-4's functional activation. PP2, another inhibitor, targets Src family tyrosine kinases, which are upstream regulators in several signaling pathways, including those involving LIR-4. Rapamycin inhibits mTOR, which plays a central role in cell growth and metabolism that LIR-4 might interact with or depend upon for its function. Go6983 inhibits protein kinase C (PKC), which is implicated in a multitude of signaling pathways, potentially including those required for LIR-4 function. Lastly, Y-27632 and Gefitinib target Rho-associated protein kinase (ROCK) and EGFR respectively, both of which are involved in pathways that might be critical for the regulation and activation of LIR-4, with inhibition leading to the disruption of these pathways and, consequently, the inhibition of LIR-4 activity.

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