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Pulmonary oxygen uptake and muscle deoxygenation kinetics during heavy intensity cycling exercise in patients with emphysema and idiopathic pulmonary fibrosis

Melitta McNarry Orcid Logo, Nicholas K. Harrison, Tom Withers, Narendra Chinnappa, Michael Lewis

BMC Pulmonary Medicine, Volume: 17, Issue: 1

Swansea University Authors: Melitta McNarry Orcid Logo, Michael Lewis

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DOI (Published version): 10.1186/s12890-017-0364-z

Abstract

BackgroundLittle is known about the mechanistic basis for the exercise intolerance characteristic of patients with respiratory disease; a lack of clearly defined, distinct patient groups limits interpretation of many studies. The purpose of this pilot study was to investigate the pulmonary oxygen up...

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Published in: BMC Pulmonary Medicine
ISSN: 1471-2466
Published: 2017
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URI: https://cronfa.swan.ac.uk/Record/cronfa32958
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Abstract: BackgroundLittle is known about the mechanistic basis for the exercise intolerance characteristic of patients with respiratory disease; a lack of clearly defined, distinct patient groups limits interpretation of many studies. The purpose of this pilot study was to investigate the pulmonary oxygen uptake (V.V. O2) response, and its potential determinants, in patients with emphysema and idiopathic pulmonary fibrosis (IPF).MethodsFollowing a ramp incremental test for the determination of peak V.V. O2 and the gas exchange threshold, six emphysema (66 ± 7 years; FEV1, 36 ± 16%), five IPF (65 ± 12 years; FEV1, 82 ± 11%) and ten healthy control participants (63 ± 6 years) completed three repeat, heavy-intensity exercise transitions on a cycle ergometer. Throughout each transition, pulmonary gas exchange, heart rate and muscle deoxygenation ([HHb], patients only) were assessed continuously and subsequently modelled using a mono-exponential with (V.V. O2, [HHb]) or without (HR) a time delay.ResultsThe V.V. O2 phase II time-constant (τ) did not differ between IPF and emphysema, with both groups significantly slower than healthy controls (Emphysema, 65 ± 11; IPF, 69 ± 7; Control, 31 ± 7 s; P < 0.05). The HR τ was slower in emphysema relative to IPF, with both groups significantly slower than controls (Emphysema, 87 ± 19; IPF, 119 ± 20; Control, 58 ± 11 s; P < 0.05). In contrast, neither the [HHb] τ nor [HHb]:O2 ratio differed between patient groups.ConclusionsThe slower V.V. O2 kinetics in emphysema and IPF may reflect poorer matching of O2 delivery-to-utilisation. Our findings extend our understanding of the exercise dysfunction in patients with respiratory disease and may help to inform the development of appropriately targeted rehabilitation strategies.
Keywords: Respiratory disease, V.V. O2 kinetics, NIRS, Cycle
College: Faculty of Science and Engineering
Issue: 1

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