Inflammation-induced upregulation of P2X4expression augments mucin secretion in airway epithelia

Author:

Winkelmann Veronika E.1ORCID,Thompson Kristin E.2,Neuland Kathrin1,Jaramillo Ana M.3,Fois Giorgio1,Schmidt Hanna1,Wittekindt Oliver H.1,Han Wei3,Tuvim Michael J.3,Dickey Burton F.3,Dietl Paul1,Frick Manfred1ORCID

Affiliation:

1. Institute of General Physiology, Ulm University, Ulm, Germany

2. Centre de Recherche Saint-Antoine, INSERM, Université Pierre et Marie Curie-Université Paris 06, Sorbonne Universités, Paris, France

3. Department of Pulmonary Medicine, MD Anderson Cancer Center, Houston, Texas

Abstract

Mucus clearance provides an essential innate defense mechanism to keep the airways and lungs free of particles and pathogens. Baseline and stimulated mucin secretion from secretory airway epithelial cells need to be tightly regulated to prevent mucus hypersecretion and mucus plugging of the airways. It is well established that extracellular ATP is a potent stimulus for regulated mucus secretion. Previous studies revealed that ATP acts via metabotropic P2Y2purinoreceptors on goblet cells. Extracellular ATP, however, is also a potent agonist for ionotropic P2X purinoreceptors. Expression of several P2X isoforms has been reported in airways, but cell type-specific expression and the function thereof remained elusive. With this study, we now provide evidence that P2X4is the predominant P2X isoform expressed in secretory airway epithelial cells. After IL-13 treatment of either human primary tracheal epithelial cells or mice, P2X4expression is upregulated in vitro and in vivo under conditions of chronic inflammation, mucous metaplasia, and hyperplasia. Upregulation of P2X4is strongest in MUC5AC-positive goblet cells. Moreover, activation of P2X4by extracellular ATP augments intracellular Ca2+signals and mucin secretion, whereas Ca2+signals and mucin secretion are dampened by inhibition of P2X4receptors. These data provide new insights into the purinergic regulation of mucin secretion and add to the emerging picture that P2X receptors modulate exocytosis of large secretory organelles and secretion of macromolecular vesicle cargo.

Funder

German Science Foundation

Ministry of Science, Research and the Arts of Baden Württemberg

Publisher

American Physiological Society

Subject

Cell Biology,Physiology (medical),Pulmonary and Respiratory Medicine,Physiology

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