Dual action of neurokinin-1 antagonists on Mas-related GPCRs
Ehsan Azimi, … , Paula Juliana Seadi Pereira, Ethan A. Lerner
Ehsan Azimi, … , Paula Juliana Seadi Pereira, Ethan A. Lerner
Published October 6, 2016
Citation Information: JCI Insight. 2016;1(16):e89362. https://doi.org/10.1172/jci.insight.89362.
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Research Article Dermatology Inflammation

Dual action of neurokinin-1 antagonists on Mas-related GPCRs

Abstract

The challenge of translating findings from animal models to the clinic is well known. An example of this challenge is the striking effectiveness of neurokinin-1 receptor (NK-1R) antagonists in mouse models of inflammation coupled with their equally striking failure in clinical investigations in humans. Here, we provide an explanation for this dichotomy: Mas-related GPCRs (Mrgprs) mediate some aspects of inflammation that had been considered mediated by NK-1R. In support of this explanation, we show that conventional NK-1R antagonists have off-target activity on the mouse receptor MrgprB2 but not on the homologous human receptor MRGPRX2. An unrelated tripeptide NK-1R antagonist has dual activity on MRGPRX2. This tripeptide both suppresses itch in mice and inhibits degranulation from the LAD-2 human mast cell line elicited by basic secretagogue activation of MRGPRX2. Antagonists of Mrgprs may fill the void left by the failure of NK-1R antagonists.

Authors

Ehsan Azimi, Vemuri B. Reddy, Kai-Ting C. Shade, Robert M. Anthony, Sebastien Talbot, Paula Juliana Seadi Pereira, Ethan A. Lerner

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Figure 3

The binding of substance P to Mrgprs is inhibited by QWF.

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The binding of substance P to Mrgprs is inhibited by QWF. (A) ELISA was ...
(A) ELISA was used to quantify the binding of substance P (SP) to nontransfected HEK293 cells and cells expressing human MRGPRX2, mouse MrgprB2, and mouse MrgprA1. SP binding is inhibited by QWF. P values for HEK293 SP vs. MRGPRX2 SP, MRGPRX2 SP vs. MRGPRX2 QWF+SP, HEK293 SP vs. MrgprB2 SP, MrgprB2 SP vs. MrgprB2 QWF+SP, HEK293 SP vs. MrgprA1 SP, and MrgprA1 SP vs. MrgprA1 QWF +SP are 0.0024, 0.0002, 0.0018, 0.0037, 0.0042, and 0.0012, respectively. HeLa cells were transfected with cDNAs encoding mouse MrgprB2 and mouse MrgprA1. A stably transfected HEK293 cell line was used for human MRGPRX2. *P ≤ 0.05, **P ≤ 0.01, ****P ≤ 0.001. (B) Concentration-effect curves with SP versus the indicated concentrations of QWF on a HEK293 cell line stably expressing human MRGPRX2. The results are consistent with QWF being a competitive antagonist of SP on human MRGPRX2. See Supplemental Figure 2 for the interaction of QWF with other GPCRs implicated in itch. The studies in A were performed 3 times and those in B were performed twice. 2-tailed unpaired Student’s t test was used.