Date published: 2025-9-15

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Vmn1r103 Activators

Vomeronasal 1 receptor 103 (V1R103) activators encompass a variety of chemical compounds that can enhance the receptor's functional activity through distinct biochemical and cellular pathways. Compounds such as calcium chloride and ionomycin directly increase intracellular calcium levels, a pivotal step in activating calcium-dependent signaling mechanisms that are vital for V1R103 function. Adenine, through its conversion to cAMP, and compounds like forskolin and isoproterenol, which stimulate adenylate cyclase, raise the levels of cAMP within the cell. This enhanced cAMP concentration activates PKA, leading to the phosphorylation of specific proteins that are critical for V1R103 activation. Similarly, GTPγS binds to and persistently activates G-proteins, maintaining the activation of signaling pathways that are essential for the functional activity of V1R103.

Furthermore, compounds that modulate the intracellular environment or receptor conformation, such as sodium bicarbonate, can influence the functional state of V1R103 by enhancing its ability to bind ligands. Magnesium sulfate contributes to the stability and proper functioning of the receptor and associated signaling molecules, thus facilitating the activation of kinases and G-proteins involved in V1R103 signaling. Zinc sulfate acts as a positive allosteric modulator, potentially heightening the receptor's sensitivity and activation potential. Piperine's role in increasing the bioavailability of V1R103's ligands or necessary cofactors serves to enhance the overall activity of the receptor. Additionally, barium chloride's effect on potassium channels and the subsequent activation of voltage-dependent calcium channels can indirectly potentiate V1R103 activation. Cobalt(II) chloride, by inducing a hypoxic-like state, may lead to the stabilization of HIFs and the upregulation of signaling components that indirectly augment V1R103 activity.

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