Date published: 2025-9-15

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Olfr1107 Inhibitors

The chemical class of compounds potentially affecting Olfr1107 activity, termed Olfr1107 Inhibitors, encompasses a range of molecules primarily targeting the olfactory signal transduction pathways rather than directly binding to the Olfr1107 receptor. Given the complexity of the olfactory signaling system and the lack of specific inhibitors for many olfactory receptors, this approach considers the indirect modulation of Olfr1107 activity. Firstly, the ER-to-Golgi transport inhibitors like Brefeldin A and Monensin, along with Tunicamycin, a glycosylation inhibitor, play a critical role in the maturation and trafficking of olfactory receptors. Proper folding, glycosylation, and transport to the cell surface are critical for the functional expression of olfactory receptors. By disrupting these processes, these compounds could reduce the surface expression of Olfr1107, indirectly inhibiting its function.

Secondly, kinase inhibitors such as Genistein and Staurosporine, along with PI3K inhibitors like Wortmannin and LY294002, target key signaling molecules that are part of the downstream olfactory transduction pathways. These pathways are crucial for the translation of receptor activation into neuronal responses. By modulating these signaling pathways, these compounds can indirectly influence the functional activity of Olfr1107. Additionally, compounds affecting cAMP levels (Forskolin, IBMX) and calcium signaling (U73122, 2-APB, Ruthenium Red) are included due to their roles in olfactory signal modulation. The alteration of intracellular cAMP and calcium levels can significantly impact the signal transduction process initiated by olfactory receptors. In summary, Olfr1107 Inhibitors encompass a diverse range of chemicals that indirectly modulate the activity of Olfr1107 by targeting various aspects of olfactory receptor trafficking, maturation, and the downstream signaling pathways. This indirect approach provides a broader understanding of the potential modulation of olfactory receptor activities, especially in cases where direct inhibitors are not well-defined or available.

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