Abstract
Olfactory receptors (ORs) are expressed in the olfactory epithelium, where they detect odorants, but also in other tissues with additional functions. Some ORs are even overexpressed in tumor cells. In this study, we identified ORs expressed in enterochromaffin tumor cells by RT-PCR, showing that single cells can co-express several ORs. Some of the receptors identified were already reported in other tumors, but they are orphan (without known ligand), as it is the case for most of the hundreds of human ORs. Thus, genes coding for human ORs with known ligands were transfected into these cells, expressing functional heterologous ORs. The in vitro stimulation of these cells by the corresponding OR odorant agonists promoted cell invasion of collagen gels. Using LNCaP prostate cancer cells, the stimulation of the PSGR (Prostate Specific G protein-coupled Receptor), an endogenously overexpressed OR, by β-ionone, its odorant agonist, resulted in the same phenotypic change. We also showed the involvement of a PI3 kinase γ dependent signaling pathway in this promotion of tumor cell invasiveness triggered by OR stimulation. Finally, after subcutaneous inoculation of LNCaP cells into NSG immunodeficient mice, the in vivo stimulation of these cells by the PSGR agonist β-ionone significantly enhanced metastasis emergence and spreading.
Highlights
Olfactory receptors (ORs) are G protein-coupled receptors mainly expressed in olfactory sensory neurons (OSNs) of the olfactory epithelium, where they detect and discriminate myriads of odorants according to a combinatorial code in which an OR can be activated by various odorants and an odorant can stimulate various ORs [1,2]
Because BON cells were derived from a metastasis, we explored whether activation of ORs by agonist odorants could have a role in tumor progression
We showed that contrary to OSNs, individual BON tumor cells (BON) co-express various ORs transcripts
Summary
Olfactory receptors (ORs) are G protein-coupled receptors mainly expressed in olfactory sensory neurons (OSNs) of the olfactory epithelium, where they detect and discriminate myriads of odorants according to a combinatorial code in which an OR can be activated by various odorants and an odorant can stimulate various ORs [1,2]. A more physiological model was used in vitro, the LNCaP prostate cancer cells which overexpress the PSGR (Prostate Specific G protein-coupled Receptor), an endogenous and deorphanized OR considered as a tumor marker, and wich was described to inhibit the proliferation of these cells in vitro [12]. This model was used in vivo to analyze the role of ORs stimulation in tumor progression, that is in metastasis emergence and spreading
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