Date published: 2025-11-24

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FNDC7 Inhibitors

FNDC7 Inhibitors are a diverse group of chemical compounds that impede FNDC7 activity through distinct yet interconnected cellular signaling pathways. Rapamycin serves as a potent FNDC7 inhibitor by suppressing the mTOR pathway, which is crucial for the synthesis of many proteins, including FNDC7. This suppression results in reduced functional activity of FNDC7 without directly altering its expression levels. Similarly, LY 294002 and Wortmannin exert their inhibitory effect on FNDC7 by irreversibly targeting PI3K, leading to the obstruction of the PI3K/Akt pathway, a signal transduction route that could affect FNDC7's downstream signaling processes. The inhibition of MEK by U0126 and PD 98059 disrupts the MAPK/ERK pathway, a key modulator of various cellular responses, thereby diminishing FNDC7's associated functional activities. Additionally, SB 203580, by selectively inhibiting p38 MAPK, and SP600125, by targeting JNK, each reduce FNDC7's role in their respective signaling pathways, thus indirectly reducing FNDC7 efficacy.

Further, the kinase inhibitor Staurosporine and the Src family kinase inhibitor Dasatinib disrupt multiple kinases that are likely to be involved in FNDC7's functional pathways, indirectly inhibiting FNDC7 by destabilizing its activation mechanisms. Sunitinib's role as a receptor tyrosine kinase inhibitor suggests its potential for indirectly diminishing FNDC7 activity by blocking signaling routes that lead to FNDC7's activation. The EGFR inhibitors Gefitinib and Erlotinib also contribute to the suppression of FNDC7 by inhibiting the EGFR signaling pathway, which may be intricately connected to FNDC7's functional roles within cells. Collectively, these FNDC7 inhibitors achieve their effects through a multifaceted approach, targeting various kinases and pathways to diminish the functional activity of FNDC7 without directly affecting its expression or translation.

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