Litcius/Paper detail

Defective CFTR modulates mechanosensitive channels TRPV4 and PIEZO1 and drives endothelial barrier failure

Jean-Pierre Amoakon, Jesun Lee, Pramodha Liyanage, Kavisha Arora, Anja Karlstaedt, Goutham Mylavarapu, Raouf Amin, Anjaparavanda P. Naren

2024iScience15 citationsDOIOpen Access PDF

Abstract

Cystic fibrosis (CF) is a genetic disease caused by a mutation in the cystic fibrosis transmembrane conductance regulator (CFTR) gene. Despite reports of CFTR expression on endothelial cells, pulmonary vascular perturbations, and perfusion deficits in CF patients, the mechanism of pulmonary vascular disease in CF remains unclear. Here, our pilot study of 40 CF patients reveals a loss of small pulmonary blood vessels in patients with severe lung disease. Using a vessel-on-a-chip model, we establish a shear-stress-dependent mechanism of endothelial barrier failure in CF involving TRPV4, a mechanosensitive channel. Furthermore, we demonstrate that CFTR deficiency downregulates the function of PIEZO1, another mechanosensitive channel involved in angiogenesis and wound repair, and exacerbates loss of small pulmonary blood vessel. We also show that CFTR directly interacts with PIEZO1 and enhances its function. Our study identifies key cellular targets to mitigate loss of small pulmonary blood vessels in CF.

Topics & Concepts

Mechanosensitive channelsPIEZO1Cystic fibrosisCystic fibrosis transmembrane conductance regulatorTRPV4LungAngiogenesisCell biologyMechanotransductionEndothelial stem cellBiologyMedicineChemistryIon channelInternal medicineGeneticsReceptorIn vitroErythrocyte Function and PathophysiologyBlood properties and coagulationIon Transport and Channel Regulation