Lung volume dependence of respiratory function in rodent models of diabetes mellitus

Lung volume dependence of respiratory function in rodent models of diabetes mellitus

Abstract Background Diabetes mellitus causes the deterioration of smooth muscle cells and interstitial matrix proteins, including collagen. Collagen and smooth muscle cells are abundant in the lungs, but the effect of diabetes on airway function and viscoelastic respiratory tissue mechanics has not...

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Main Authors: Roberta Südy, Álmos Schranc, Gergely H. Fodor, József Tolnai, Barna Babik, Ferenc Peták
Format: Article
Language:English
Published: BMC 2020-04-01
Series:Respiratory Research
Subjects:
Forced oscillations
Hyperglycemia
Respiratory mechanics
Airway responsiveness
Tissue viscoelasticity
Online Access:http://link.springer.com/article/10.1186/s12931-020-01334-y
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spelling doaj-9adbd4e732af47ccb99e7167bc8400c82020-11-25T02:54:27ZengBMCRespiratory Research1465-993X2020-04-0121111210.1186/s12931-020-01334-yLung volume dependence of respiratory function in rodent models of diabetes mellitusRoberta Südy0Álmos Schranc1Gergely H. Fodor2József Tolnai3Barna Babik4Ferenc Peták5Department of Medical Physics and Informatics, University of SzegedDepartment of Medical Physics and Informatics, University of SzegedDepartment of Medical Physics and Informatics, University of SzegedDepartment of Medical Physics and Informatics, University of SzegedDepartment of Anaesthesiology and Intensive Therapy, University of SzegedDepartment of Medical Physics and Informatics, University of SzegedAbstract Background Diabetes mellitus causes the deterioration of smooth muscle cells and interstitial matrix proteins, including collagen. Collagen and smooth muscle cells are abundant in the lungs, but the effect of diabetes on airway function and viscoelastic respiratory tissue mechanics has not been characterized. This study investigated the impact of diabetes on respiratory function, bronchial responsiveness, and gas exchange parameters. Methods Rats were allocated randomly to three groups: a model of type 1 diabetes that received a high dose of streptozotocin (DM1, n = 13); a model of type 2 diabetes that received a low dose of streptozotocin with a high-fat diet (DM2, n = 14); and a control group with no treatment (C, n = 14). Forced oscillations were applied to assess airway resistance (Raw), respiratory tissue damping (G), and elastance (H). The arterial partial pressure of oxygen to the inspired oxygen fraction (PaO2/FiO2) and intrapulmonary shunt fraction (Qs/Qt) were determined from blood gas samples at positive end-expiratory pressures (PEEPs) of 0, 3, and 6 cmH2O. Lung responsiveness to methacholine was also assessed. Collagen fibers in lung tissue were quantified by histology. Results The rats in groups DM1 and DM2 exhibited elevated Raw, G, H, and Qs/Qt, compromised PaO2/FiO2, and diminished airway responsiveness. The severity of adverse tissue mechanical change correlated with excessive lung collagen expression. Increased PEEP normalized the respiratory mechanics, but the gas exchange abnormalities remained. Conclusions These findings indicate that diabetes reduces airway and lung tissue viscoelasticity, resulting in alveolar collapsibility that can be compensated by increasing PEEP. Diabetes also induces persistent alveolo-capillary dysfunction and abnormal adaptation ability of the airways to exogenous constrictor stimuli.http://link.springer.com/article/10.1186/s12931-020-01334-yForced oscillationsHyperglycemiaRespiratory mechanicsAirway responsivenessTissue viscoelasticity
collection DOAJ
language English
format Article
sources DOAJ
author Roberta Südy
Álmos Schranc
Gergely H. Fodor
József Tolnai
Barna Babik
Ferenc Peták
spellingShingle Roberta Südy
Álmos Schranc
Gergely H. Fodor
József Tolnai
Barna Babik
Ferenc Peták
Lung volume dependence of respiratory function in rodent models of diabetes mellitus
Respiratory Research
Forced oscillations
Hyperglycemia
Respiratory mechanics
Airway responsiveness
Tissue viscoelasticity
author_facet Roberta Südy
Álmos Schranc
Gergely H. Fodor
József Tolnai
Barna Babik
Ferenc Peták
author_sort Roberta Südy
title Lung volume dependence of respiratory function in rodent models of diabetes mellitus
title_short Lung volume dependence of respiratory function in rodent models of diabetes mellitus
title_full Lung volume dependence of respiratory function in rodent models of diabetes mellitus
title_fullStr Lung volume dependence of respiratory function in rodent models of diabetes mellitus
title_full_unstemmed Lung volume dependence of respiratory function in rodent models of diabetes mellitus
title_sort lung volume dependence of respiratory function in rodent models of diabetes mellitus
publisher BMC
series Respiratory Research
issn 1465-993X
publishDate 2020-04-01
description Abstract Background Diabetes mellitus causes the deterioration of smooth muscle cells and interstitial matrix proteins, including collagen. Collagen and smooth muscle cells are abundant in the lungs, but the effect of diabetes on airway function and viscoelastic respiratory tissue mechanics has not been characterized. This study investigated the impact of diabetes on respiratory function, bronchial responsiveness, and gas exchange parameters. Methods Rats were allocated randomly to three groups: a model of type 1 diabetes that received a high dose of streptozotocin (DM1, n = 13); a model of type 2 diabetes that received a low dose of streptozotocin with a high-fat diet (DM2, n = 14); and a control group with no treatment (C, n = 14). Forced oscillations were applied to assess airway resistance (Raw), respiratory tissue damping (G), and elastance (H). The arterial partial pressure of oxygen to the inspired oxygen fraction (PaO2/FiO2) and intrapulmonary shunt fraction (Qs/Qt) were determined from blood gas samples at positive end-expiratory pressures (PEEPs) of 0, 3, and 6 cmH2O. Lung responsiveness to methacholine was also assessed. Collagen fibers in lung tissue were quantified by histology. Results The rats in groups DM1 and DM2 exhibited elevated Raw, G, H, and Qs/Qt, compromised PaO2/FiO2, and diminished airway responsiveness. The severity of adverse tissue mechanical change correlated with excessive lung collagen expression. Increased PEEP normalized the respiratory mechanics, but the gas exchange abnormalities remained. Conclusions These findings indicate that diabetes reduces airway and lung tissue viscoelasticity, resulting in alveolar collapsibility that can be compensated by increasing PEEP. Diabetes also induces persistent alveolo-capillary dysfunction and abnormal adaptation ability of the airways to exogenous constrictor stimuli.
topic Forced oscillations
Hyperglycemia
Respiratory mechanics
Airway responsiveness
Tissue viscoelasticity
url http://link.springer.com/article/10.1186/s12931-020-01334-y
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