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Antagonizing cholecystokinin A receptor in the lung attenuates obesity-induced airway hyperresponsiveness.

Nature communications (2023-01-05)
Ronald Allan M Panganiban, Zhiping Yang, Maoyun Sun, Chan Young Park, David I Kasahara, Niccole Schaible, Ramaswamy Krishnan, Alvin T Kho, Elliot Israel, Marc B Hershenson, Scott T Weiss, Blanca E Himes, Jeffrey J Fredberg, Kelan G Tantisira, Stephanie A Shore, Quan Lu
RÉSUMÉ

Obesity increases asthma prevalence and severity. However, the underlying mechanisms are poorly understood, and consequently, therapeutic options for asthma patients with obesity remain limited. Here we report that cholecystokinin-a metabolic hormone best known for its role in signaling satiation and fat metabolism-is increased in the lungs of obese mice and that pharmacological blockade of cholecystokinin A receptor signaling reduces obesity-associated airway hyperresponsiveness. Activation of cholecystokinin A receptor by the hormone induces contraction of airway smooth muscle cells. In vivo, cholecystokinin level is elevated in the lungs of both genetically and diet-induced obese mice. Importantly, intranasal administration of cholecystokinin A receptor antagonists (proglumide and devazepide) suppresses the airway hyperresponsiveness in the obese mice. Together, our results reveal an unexpected role for cholecystokinin in the lung and support the repurposing of cholecystokinin A receptor antagonists as a potential therapy for asthma patients with obesity.

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Sigma-Aldrich
Anticorps monoclonal de souris anti-α-actine de muscle lisse-Cy3, clone 1A4, purified from hybridoma cell culture
Sigma-Aldrich
Anti-Goat IgG (H+L), highly cross-adsorbed, CF 488A antibody produced in donkey, ~2 mg/mL, affinity isolated antibody