Date published: 2025-9-27

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FYCO1 Activators

FYCO1 Activators consist of a range of compounds that amplify its function primarily by influencing the autophagic process. Forskolin, by raising cAMP levels, indirectly enhances FYCO1's role in autophagosome trafficking through PKA activation, which is integral to autophagy. Curcumin further augments FYCO1's function by modulating autophagic pathways, potentially upregulating FYCO1's involvement in autophagosome trafficking. Rapamycin and Torin 1, both mTOR inhibitors, directly initiate autophagy, which is likely to increase the activity of FYCO1 in autophagosome-lysosome fusion. Lithium's inhibition of inositol monophosphatase, Resveratrol's induction of autophagy via SIRT1, and Spermidine's autophagy enhancement all serve to potentiate FYCO1's autophagic functions. Piperlongumine's and Trehalose's roles in autophagy induction, along with Verapamil's ability to induce autophagy via Ca2+ channel blocking, further underscore the diverse yet convergent mechanisms by which these compounds can elevate FYCO1 activity.

Nicotinamide mononucleotide elevates NAD+ levels, supporting cellular energy processes and potentially increasing the autophagic activity where FYCO1 operates as an adaptor. Additionally, 2-Deoxy-D-glucose, by inducing energy stress, also fosters an autophagic response, indirectly supporting the physiological roles of FYCO1. Collectively, these chemical compounds, by targeting various steps and signaling pathways that culminate in autophagy, indirectly yet significantly bolster the functional activity of FYCO1.

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