Date published: 2025-9-13

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OR1J4 Inhibitors

Caffeine and Quinine are both known to affect GPCR signaling, caffeine through adenosine receptor blockade and quinine through potassium channel inhibition, which can alter the signaling milieu in which OR1J4 operates. Chloroquine and verapamil, through their actions on endosomal acidification and calcium channels respectively, can impact the downstream signaling events that follow GPCR activation. This indirect modulation can alter OR1J4 activity. Similarly, pertussis toxin disrupts G protein signaling by inhibiting Gi/o proteins, potentially affecting OR1J4's ability to transduce signals. Compounds such as cholesterol affect the membrane environment and enzyme activity can lead to alterations in GPCR-mediated signaling processes, thereby influencing OR1J4 activity. Forskolin, with its ability to increase cAMP levels, impacts the signaling pathways downstream of GPCR activation, which can indirectly modulate OR1J4 receptor function. Yohimbine and haloperidol, by antagonizing alpha-2 adrenergic and dopamine receptors, can affect GPCR signaling cascades in a manner that potentially modulates the activity of OR1J4. Nifedipine, by inhibiting calcium channels, can also affect GPCR signaling, potentially altering the activity of the OR1J4 receptor.

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