The signaling signature of the neurotensin type 1 receptor with endogenous ligands

Élie Besserer-Offroy; Rebecca L Brouillette; Sandrine Lavenus; Ulrike Froehlich; Andrea Brumwell; Alexandre Murza; Jean-Michel Longpré; Éric Marsault; Michel Grandbois; Philippe Sarret; Richard Leduc

doi:10.1016/j.ejphar.2017.03.046

The signaling signature of the neurotensin type 1 receptor with endogenous ligands

Eur J Pharmacol. 2017 Jun 15:805:1-13. doi: 10.1016/j.ejphar.2017.03.046. Epub 2017 Mar 22.

Authors

Affiliations

¹ Department of Pharmacology-Physiology, Faculty of Medicine and Health Sciences, Institut de Pharmacologie de Sherbrooke, Université de Sherbrooke, Sherbrooke, Québec, Canada J1H 5N4. Electronic address: Elie.Besserer-Offroy@USherbrooke.ca.
² Department of Pharmacology-Physiology, Faculty of Medicine and Health Sciences, Institut de Pharmacologie de Sherbrooke, Université de Sherbrooke, Sherbrooke, Québec, Canada J1H 5N4. Electronic address: Rebecca.Brouillette@USherbrooke.ca.
³ Department of Pharmacology-Physiology, Faculty of Medicine and Health Sciences, Institut de Pharmacologie de Sherbrooke, Université de Sherbrooke, Sherbrooke, Québec, Canada J1H 5N4. Electronic address: Sandrine.Lavenus@USherbrooke.ca.
⁴ Department of Pharmacology-Physiology, Faculty of Medicine and Health Sciences, Institut de Pharmacologie de Sherbrooke, Université de Sherbrooke, Sherbrooke, Québec, Canada J1H 5N4. Electronic address: Ulrike.Froehlich@USherbrooke.ca.
⁵ Department of Pharmacology-Physiology, Faculty of Medicine and Health Sciences, Institut de Pharmacologie de Sherbrooke, Université de Sherbrooke, Sherbrooke, Québec, Canada J1H 5N4. Electronic address: Andrea.Brumwell@USherbrooke.ca.
⁶ Department of Pharmacology-Physiology, Faculty of Medicine and Health Sciences, Institut de Pharmacologie de Sherbrooke, Université de Sherbrooke, Sherbrooke, Québec, Canada J1H 5N4. Electronic address: Alexandre.Murza@USherbrooke.ca.
⁷ Department of Pharmacology-Physiology, Faculty of Medicine and Health Sciences, Institut de Pharmacologie de Sherbrooke, Université de Sherbrooke, Sherbrooke, Québec, Canada J1H 5N4. Electronic address: Jean-Michel.Longpre@USherbrooke.ca.
⁸ Department of Pharmacology-Physiology, Faculty of Medicine and Health Sciences, Institut de Pharmacologie de Sherbrooke, Université de Sherbrooke, Sherbrooke, Québec, Canada J1H 5N4. Electronic address: Eric.Marsault@USherbrooke.ca.
⁹ Department of Pharmacology-Physiology, Faculty of Medicine and Health Sciences, Institut de Pharmacologie de Sherbrooke, Université de Sherbrooke, Sherbrooke, Québec, Canada J1H 5N4. Electronic address: Michel.Grandbois@USherbrooke.ca.
¹⁰ Department of Pharmacology-Physiology, Faculty of Medicine and Health Sciences, Institut de Pharmacologie de Sherbrooke, Université de Sherbrooke, Sherbrooke, Québec, Canada J1H 5N4. Electronic address: Philippe.Sarret@USherbrooke.ca.
¹¹ Department of Pharmacology-Physiology, Faculty of Medicine and Health Sciences, Institut de Pharmacologie de Sherbrooke, Université de Sherbrooke, Sherbrooke, Québec, Canada J1H 5N4. Electronic address: Richard.Leduc@USherbrooke.ca.

PMID: 28341345
DOI: 10.1016/j.ejphar.2017.03.046

Abstract

The human neurotensin 1 receptor (hNTS1) is a G protein-coupled receptor involved in many physiological functions, including analgesia, hypothermia, and hypotension. To gain a better understanding of which signaling pathways or combination of pathways are linked to NTS1 activation and function, we investigated the ability of activated hNTS1, which was stably expressed by CHO-K1 cells, to directly engage G proteins, activate second messenger cascades and recruit β-arrestins. Using BRET-based biosensors, we found that neurotensin (NT), NT(8-13) and neuromedin N (NN) activated the Gα_q-, Gα_i1-, Gα_oA-, and Gα₁₃-protein signaling pathways as well as the recruitment of β-arrestins 1 and 2. Using pharmacological inhibitors, we further demonstrated that all three ligands stimulated the production of inositol phosphate and modulation of cAMP accumulation along with ERK1/2 activation. Interestingly, despite the functional coupling to Gα_i1 and Gα_oA, NT was found to produce higher levels of cAMP in the presence of pertussis toxin, supporting that hNTS1 activation leads to cAMP accumulation in a Gα_s-dependent manner. Additionally, we demonstrated that the full activation of ERK1/2 required signaling through both a PTX-sensitive G_i/o-c-Src signaling pathway and PLCβ-DAG-PKC-Raf-1-dependent pathway downstream of G_q. Finally, the whole-cell integrated signatures monitored by the cell-based surface plasmon resonance and changes in the electrical impedance of a confluent cell monolayer led to identical phenotypic responses between the three ligands. The characterization of the hNTS1-mediated cellular signaling network will be helpful to accelerate the validation of potential NTS1 biased ligands with an improved therapeutic/adverse effect profile.

Keywords: G protein; G protein-coupled receptor (GPCR); Neuromedin N; Neuromedin N (PubChem CID: 9940301); Neurotensin; Neurotensin (1-13) (PubChem CID: 25077406); Neurotensin (8-13) (PubChem CID: 5311318); Neurotensin receptor 1; SR48692 (PubChem CID: 119192); β-arrestin.

MeSH terms

Amino Acid Sequence
Animals
CHO Cells
Cricetinae
Cricetulus
Enzyme Activation
GTP-Binding Proteins / metabolism
Humans
Ligands
Mitogen-Activated Protein Kinase 1 / metabolism
Mitogen-Activated Protein Kinase 3 / metabolism
Neurotensin / chemistry
Neurotensin / metabolism
Peptide Fragments / chemistry
Peptide Fragments / metabolism
Receptors, Neurotensin / metabolism*
Signal Transduction*
beta-Arrestin 1 / metabolism
beta-Arrestin 2 / metabolism

Substances

Ligands
Peptide Fragments
Receptors, Neurotensin
beta-Arrestin 1
beta-Arrestin 2
neurotensin type 1 receptor
neuromedin N
Neurotensin
neurotensin (8-13)
Mitogen-Activated Protein Kinase 1
Mitogen-Activated Protein Kinase 3
GTP-Binding Proteins