AI Article Synopsis

  • Two cystic fibrosis rat models were studied to assess lung function, revealing that although they had CFTR mRNA reductions, they did not show typical signs of CF lung disease.
  • Using advanced imaging techniques, the study measured how localized physical obstructions affected lung ventilation and found increased ventilation issues in CF rats compared to healthy controls.
  • The findings highlighted that CF rats exhibit altered respiratory mechanics, necessitating more effort to breathe due to stiffer lungs, and demonstrated the effectiveness of XV imaging for assessing lung ventilation.

Article Abstract

Two cystic fibrosis (CF) rat models, one carrying the common Phe508del mutation and the other a nonsense cystic fibrosis transmembrane conductance regulator (CFTR) mutation (knockout) were previously characterised. Although relevant CFTR mRNA reductions were present in the lung, no overt CF lung disease was observed. This study used flexiVent lung mechanic assessment and regional ventilation assessment via X-ray velocimetry (XV) functional imaging to assess the lung phenotype in both models. To determine the sensitivity of XV regional ventilation imaging, the effect of a localised physical obstruction (delivery of agar beads to part of the lungs) on lung ventilation was examined. At baseline, Phe508del and knockout CF rats had a lower inspiratory capacity, total respiratory system compliance, and static compliance than wildtype rats. Following agar bead delivery all XV ventilation parameters were altered, with substantial increases in poorly ventilated regions and ventilation heterogeneity. XV ventilation maps accurately identified locations of bead-induced airflow changes. Despite unremarkable lung histopathology, this study indicated that CF rats display altered respiratory mechanics, with CF rats needing to exert additional effort to expand and deflate their lungs due to increased stiffness. This study demonstrated the utility of XV imaging providing spatial lung ventilation information.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC11405763PMC
http://dx.doi.org/10.1038/s41598-024-71632-8DOI Listing

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