Differential effects of glucose-dependent insulinotropic polypeptide receptor/glucagon-like peptide-1 receptor heteromerization on cell signaling when expressed in HEK-293 cells.

The incretin hormones: glucose-dependent insulinotropic polypeptide (GIP) and glucagon-like peptide-1 (GLP-1) are important regulators of many aspects of metabolism including insulin secretion. Their receptors (GIPR and GLP-1R) are closely related members of the secretin class of G-protein-coupled receptors. As both receptors are expressed on pancreatic ß-cells there is at least the hypothetical possibility that they may form heteromers. In the present study, we investigated GIPR/GLP-1R heteromerization and the impact of GIPR on GLP-1R-mediated signaling and vice versa in HEK-293 cells. Real-time fluorescence resonance energy transfer (FRET) and bioluminescence resonance energy transfer (BRET) saturation experiments confirm that GLP-1R and GIPR form heteromers. Stimulation with 1 µM GLP-1 caused an increase in both FRET and BRET ratio, whereas stimulation with 1 µM GIP caused a decrease. The only other ligand tested to cause a significant change in BRET signal was the GLP-1 metabolite, GLP-1 (9-36). GIPR expression had no significant effect on mini-Gs recruitment to GLP-1R but significantly inhibited GLP-1 stimulated mini-Gq and arrestin recruitment. In contrast, the presence of GLP-1R improved GIP stimulated mini-Gs and mini-Gq recruitment to GIPR. These data support the hypothesis that GIPR and GLP-1R form heteromers with differential consequences on cell signaling.

Correction: Al-Zamel, N., et al. A Dual GLP-1/GIP Receptor Agonist Does Not Antagonize Glucagon at Its Receptor but May Act as a Biased Agonist at the GLP-1 Receptor. Int. J. Mol. Sci. 2019, 20, 3532.

The author wishes to make the following correction to this paper [...].

A single bout of vigorous-intensity aerobic exercise affects reactive, but not proactive cognitive brain functions.

The literature on aerobic exercise and neurocognition reports acute post-exercise enhancement of neural activity linked to motor preparation in the premotor area and inhibitory control in the frontoparietal areas. However, the acute effect of vigorous-intensity aerobic exercise (VIAE) on the prefrontal, the insular, and the occipito-parietal activities linked to proactive control, early perceptual, and attentional processing is indeterminate. Thus, the present study investigated the acute effect of VIAE on the neurobehavioral correlates of these proactive and reactive neurocognitive functions. Young, healthy subjects participated in two separate experimental sessions: 30 min of VIAE and 30 min of internet browsing. Before and immediately after the two sessions, we recorded high-resolution electroencephalograms while performing a visuomotor discriminative response task. For testing the effect of VIAE on cognitive processing, we analyzed the behavioral performance and event-related potentials (ERPs). The analysis of behavioral data did not reveal any VIAE effect on task performance. The analysis of ERPs showed no significant VIAE effect on the proactive functions in the premotor and the prefrontal areas, but significant effects on the reactive functions related to selective attention in parietal areas (indexed by the N1 amplitude) and perceptual awareness in the anterior insula (indexed by the pN1 latency). We concluded that a single bout of VIAE does not affect the proactive functions in the premotor and the prefrontal areas, but modulates the early reactive neural mechanisms underlying perceptual awareness of stimuli in the insular cortex and selective attention in the parieto-occipital areas.

A Dual GLP-1/GIP Receptor Agonist Does Not Antagonize Glucagon at Its Receptor but May Act as a Biased Agonist at the GLP-1 Receptor.

Glucagon-like peptide-1 (GLP-1) and glucose-dependent insulinotropic polypeptide (GIP) are important regulators of metabolism, making their receptors (GLP-1R and GIPR) attractive targets in the treatment of type 2 diabetes mellitus (T2DM). GLP-1R agonists are used clinically to treat T2DM but the use of GIPR agonists remains controversial. Recent studies suggest that simultaneous activation of GLP-1R and GIPR with a single peptide provides superior glycemic control with fewer adverse effects than activation of GLP-1R alone. We investigated the signaling properties of a recently reported dual-incretin receptor agonist (P18). GLP-1R, GIPR, and the closely related glucagon receptor (GCGR) were expressed in HEK-293 cells. Activation of adenylate cyclase via Gαs was monitored using a luciferase-linked reporter gene (CRE-Luc) assay. Arrestin recruitment was monitored using a bioluminescence resonance energy transfer (BRET) assay. GLP-1, GIP, and glucagon displayed exquisite selectivity for their receptors in the CRE-Luc assay. P18 activated GLP-1R with similar potency to GLP-1 and GIPR with higher potency than GIP. Interestingly, P18 was less effective than GLP-1 at recruiting arrestin to GLP-1R and was inactive at GCGR. These data suggest that P18 can act as both a dual-incretin receptor agonist, and as a G protein-biased agonist at GLP-1R.