Human Mast Cell Line HMC1 Expresses Functional Mas-Related G-Protein Coupled Receptor 2

Human Mast Cell Line HMC1 Expresses Functional Mas-Related G-Protein Coupled Receptor 2

The Mas-related G-protein-coupled receptor X2 (MRGPRX2) is prominently expressed by mast cells and induces degranulation upon binding by different ligands. Its activation has been linked to various mast cell-related diseases, such as chronic spontaneous urticaria, atopic dermatitis and asthma. There...

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Main Authors: Maud A. W. Hermans, Astrid C. van Stigt, Sanne van de Meerendonk, Benjamin Schrijver, Paul L. A. van Daele, Petrus M. van Hagen, Marloes van Splunter, Willem A. Dik
Format: Article
Language:English
Published: Frontiers Media S.A. 2021-03-01
Series:Frontiers in Immunology
Subjects:
mast cell (MC)
MRGPRX2
compound 48/80
qwf
HMC1
LAD2
Online Access:https://www.frontiersin.org/articles/10.3389/fimmu.2021.625284/full
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spelling doaj-cb6080b5e5f1497dab73576c78c44bba2021-03-15T05:01:23ZengFrontiers Media S.A.Frontiers in Immunology1664-32242021-03-011210.3389/fimmu.2021.625284625284Human Mast Cell Line HMC1 Expresses Functional Mas-Related G-Protein Coupled Receptor 2Maud A. W. Hermans0Astrid C. van Stigt1Sanne van de Meerendonk2Benjamin Schrijver3Paul L. A. van Daele4Paul L. A. van Daele5Petrus M. van Hagen6Petrus M. van Hagen7Marloes van Splunter8Willem A. Dik9Willem A. Dik10Section of Allergy & Immunology, Department of Internal Medicine, Erasmus MC, Rotterdam, NetherlandsLaboratory of Medical Immunology, Department of Immunology, Erasmus MC, Rotterdam, NetherlandsLaboratory of Medical Immunology, Department of Immunology, Erasmus MC, Rotterdam, NetherlandsLaboratory of Medical Immunology, Department of Immunology, Erasmus MC, Rotterdam, NetherlandsSection of Allergy & Immunology, Department of Internal Medicine, Erasmus MC, Rotterdam, NetherlandsLaboratory of Medical Immunology, Department of Immunology, Erasmus MC, Rotterdam, NetherlandsSection of Allergy & Immunology, Department of Internal Medicine, Erasmus MC, Rotterdam, NetherlandsLaboratory of Medical Immunology, Department of Immunology, Erasmus MC, Rotterdam, NetherlandsSection of Allergy & Immunology, Department of Internal Medicine, Erasmus MC, Rotterdam, NetherlandsSection of Allergy & Immunology, Department of Internal Medicine, Erasmus MC, Rotterdam, NetherlandsLaboratory of Medical Immunology, Department of Immunology, Erasmus MC, Rotterdam, NetherlandsThe Mas-related G-protein-coupled receptor X2 (MRGPRX2) is prominently expressed by mast cells and induces degranulation upon binding by different ligands. Its activation has been linked to various mast cell-related diseases, such as chronic spontaneous urticaria, atopic dermatitis and asthma. Therefore, inhibition of MRGPRX2 activity represents a therapeutic target for these conditions. However, the exact pathophysiology of this receptor is still unknown. In vitro research with mast cells is often hampered by the technical limitations of available cell lines. The human mast cell types LAD2 and HuMC (human mast cells cultured from CD34+ progenitor cells) most closely resemble mature human mast cells, yet have a very slow growth rate. A fast proliferating alternative is the human mast cell line HMC1, but they are considered unsuitable for degranulation assays due to their immature phenotype. Moreover, the expression and functionality of MRGPRX2 on HMC1 is controversial. Here, we describe the MRGPRX2 expression and functionality in HMC1 cells, and compare these with LAD2 and HuMC. We also propose a model to render HMC1 suitable for degranulation assays by pre-incubating them with latrunculin-B (Lat-B). Expression of MRGPRX2 by HMC1 was proven by RQ-PCR and flowcytometry, although at lower levels compared with LAD2 and HuMC. Pre-incubation of HMC1 cells with Lat-B significantly increased the overall degranulation capacity, without significantly changing their MRGPRX2 expression, phenotype or morphology. The MRGPRX2 specific compound 48/80 (C48/80) effectively induced degranulation of HMC1 as measured by CD63 membrane expression and β-hexosaminidase release, albeit in lower levels than for LAD2 or HuMC. HMC1, LAD2 and HuMC each had different degranulation kinetics upon stimulation with C48/80. Incubation with the MRGPRX2 specific inhibitor QWF inhibited C48/80-induced degranulation, confirming the functionality of MRGPRX2 on HMC1. In conclusion, HMC1 cells have lower levels of MRGPRX2 expression than LAD2 or HuMC, but are attractive for in vitro research because of their high growth rate and stable phenotype. HMC1 can be used to study MRGPRX2-mediated degranulation after pre-incubation with Lat-B, which provides the opportunity to explore MPRGRX2 biology in mast cells in a feasible way.https://www.frontiersin.org/articles/10.3389/fimmu.2021.625284/fullmast cell (MC)MRGPRX2compound 48/80qwfHMC1LAD2
collection DOAJ
language English
format Article
sources DOAJ
author Maud A. W. Hermans
Astrid C. van Stigt
Sanne van de Meerendonk
Benjamin Schrijver
Paul L. A. van Daele
Paul L. A. van Daele
Petrus M. van Hagen
Petrus M. van Hagen
Marloes van Splunter
Willem A. Dik
Willem A. Dik
spellingShingle Maud A. W. Hermans
Astrid C. van Stigt
Sanne van de Meerendonk
Benjamin Schrijver
Paul L. A. van Daele
Paul L. A. van Daele
Petrus M. van Hagen
Petrus M. van Hagen
Marloes van Splunter
Willem A. Dik
Willem A. Dik
Human Mast Cell Line HMC1 Expresses Functional Mas-Related G-Protein Coupled Receptor 2
Frontiers in Immunology
mast cell (MC)
MRGPRX2
compound 48/80
qwf
HMC1
LAD2
author_facet Maud A. W. Hermans
Astrid C. van Stigt
Sanne van de Meerendonk
Benjamin Schrijver
Paul L. A. van Daele
Paul L. A. van Daele
Petrus M. van Hagen
Petrus M. van Hagen
Marloes van Splunter
Willem A. Dik
Willem A. Dik
author_sort Maud A. W. Hermans
title Human Mast Cell Line HMC1 Expresses Functional Mas-Related G-Protein Coupled Receptor 2
title_short Human Mast Cell Line HMC1 Expresses Functional Mas-Related G-Protein Coupled Receptor 2
title_full Human Mast Cell Line HMC1 Expresses Functional Mas-Related G-Protein Coupled Receptor 2
title_fullStr Human Mast Cell Line HMC1 Expresses Functional Mas-Related G-Protein Coupled Receptor 2
title_full_unstemmed Human Mast Cell Line HMC1 Expresses Functional Mas-Related G-Protein Coupled Receptor 2
title_sort human mast cell line hmc1 expresses functional mas-related g-protein coupled receptor 2
publisher Frontiers Media S.A.
series Frontiers in Immunology
issn 1664-3224
publishDate 2021-03-01
description The Mas-related G-protein-coupled receptor X2 (MRGPRX2) is prominently expressed by mast cells and induces degranulation upon binding by different ligands. Its activation has been linked to various mast cell-related diseases, such as chronic spontaneous urticaria, atopic dermatitis and asthma. Therefore, inhibition of MRGPRX2 activity represents a therapeutic target for these conditions. However, the exact pathophysiology of this receptor is still unknown. In vitro research with mast cells is often hampered by the technical limitations of available cell lines. The human mast cell types LAD2 and HuMC (human mast cells cultured from CD34+ progenitor cells) most closely resemble mature human mast cells, yet have a very slow growth rate. A fast proliferating alternative is the human mast cell line HMC1, but they are considered unsuitable for degranulation assays due to their immature phenotype. Moreover, the expression and functionality of MRGPRX2 on HMC1 is controversial. Here, we describe the MRGPRX2 expression and functionality in HMC1 cells, and compare these with LAD2 and HuMC. We also propose a model to render HMC1 suitable for degranulation assays by pre-incubating them with latrunculin-B (Lat-B). Expression of MRGPRX2 by HMC1 was proven by RQ-PCR and flowcytometry, although at lower levels compared with LAD2 and HuMC. Pre-incubation of HMC1 cells with Lat-B significantly increased the overall degranulation capacity, without significantly changing their MRGPRX2 expression, phenotype or morphology. The MRGPRX2 specific compound 48/80 (C48/80) effectively induced degranulation of HMC1 as measured by CD63 membrane expression and β-hexosaminidase release, albeit in lower levels than for LAD2 or HuMC. HMC1, LAD2 and HuMC each had different degranulation kinetics upon stimulation with C48/80. Incubation with the MRGPRX2 specific inhibitor QWF inhibited C48/80-induced degranulation, confirming the functionality of MRGPRX2 on HMC1. In conclusion, HMC1 cells have lower levels of MRGPRX2 expression than LAD2 or HuMC, but are attractive for in vitro research because of their high growth rate and stable phenotype. HMC1 can be used to study MRGPRX2-mediated degranulation after pre-incubation with Lat-B, which provides the opportunity to explore MPRGRX2 biology in mast cells in a feasible way.
topic mast cell (MC)
MRGPRX2
compound 48/80
qwf
HMC1
LAD2
url https://www.frontiersin.org/articles/10.3389/fimmu.2021.625284/full
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