Article Text
Abstract
Introduction Individuals with asthma breathe at higher operating lung volumes during exercise compared with healthy individuals, which contributes to increased exertional dyspnoea. In health, females are more likely to develop exertional dyspnoea than males at a given workload or ventilation, and therefore, it is possible that females with asthma may develop disproportional dyspnoea on exertion. The purpose of this study was to compare operating lung volume and dyspnoea responses during exercise in females with and without asthma.
Methods Sixteen female controls and 16 females with asthma were recruited for the study along with 16 male controls and 16 males with asthma as a comparison group. Asthma was confirmed using American Thoracic Society criteria. Participants completed a cycle ergometry cardiopulmonary exercise test to volitional exhaustion. Inspiratory capacity manoeuvres were performed to estimate inspiratory reserve volume (IRV) and dyspnoea was evaluated using the Modified Borg Scale.
Results Females with asthma exhibited elevated dyspnoea during submaximal exercise compared with female controls (p<0.05). Females with asthma obtained a similar IRV and dyspnoea at peak exercise compared with healthy females despite lower ventilatory demand, suggesting mechanical constraint to tidal volume (VT) expansion. VT-inflection point was observed at significantly lower ventilation and V̇O2 in females with asthma compared with female controls. Forced expired volume in 1 s was significantly associated with VT-inflection point in females with asthma (R2=0.401; p<0.01) but not female controls (R2=0.002; p=0.88).
Conclusion These results suggest that females with asthma are more prone to experience exertional dyspnoea, secondary to dynamic mechanical constraints during submaximal exercise when compared with females without asthma.
- Asthma
- Exercise
- Perception of Asthma/Breathlessness
Data availability statement
No data are available.
This is an open access article distributed in accordance with the Creative Commons Attribution Non Commercial (CC BY-NC 4.0) license, which permits others to distribute, remix, adapt, build upon this work non-commercially, and license their derivative works on different terms, provided the original work is properly cited, appropriate credit is given, any changes made indicated, and the use is non-commercial. See: http://creativecommons.org/licenses/by-nc/4.0/.
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WHAT IS ALREADY KNOWN ON THIS TOPIC
Individuals with asthma report exercise avoidance to a greater extent compared with healthy controls, with exertional dyspnoea being cited as a major contributor. Further, in health, females are more likely to report higher dyspnoea then males due to airway size.
WHAT THIS STUDY ADDS
Females with asthma reported significant dyspnoea at matched workloads compared with controls due to earlier tidal volume-inflection and higher operating lung volumes.
HOW THIS STUDY MIGHT AFFECT RESEARCH, PRACTICE OR POLICY
Females with asthma may be at a higher risk for symptom burden during exercise. Further research is needed to understand how this may affect perception around exercise and exercise avoidance in asthma.
Introduction
Asthma is a chronic airway disease characterised by recurrent episodes of wheezing and shortness of breath (commonly termed dyspnoea) brought on by pulmonary inflammation and bronchoconstriction.1 Although physical activity has been shown to reduce symptom burden,2 individuals with asthma perform less physical activity compared with individuals without asthma.3 The reasons for exercise avoidance in people with asthma are multifactorial and complex,4 and increased exertional dyspnoea has been cited as a major contributor to exercise avoidance in these individuals.3 5
During high-intensity exercise, increased ventilatory rate can result in expiratory flow limitation.6 The presence of expiratory flow limitation can lead to a compensatory increases in operating lung volume, which is reflected by a reduction in inspiratory capacity (IC) and inspiratory reserve volume (IRV).5 7–9 The increase in operating lung volume is advantageous as it facilitates greater airflow during high-intensity exercise. However, the elevated operating lung volume places tidal volume (VT) on the non-compliant portion of the sigmoidal pressure–volume curve, increasing the elastic load of the inspiratory muscles and ultimately heightening dyspnoea.9–12 Previous work has shown that individuals with controlled asthma develop greater expiratory flow limitation, breathe at higher operating lung volumes and report greater dyspnoea during exercise compared with age-matched and fitness-matched healthy individuals.5 Further, early VT-inflection points can mark significant ventilatory mechanical constraints and are closely related to increased perceived exertion in individuals with asthma.13–15
Females typically have smaller lungs and lower maximal expiratory flow rates than males of the same height.16 17 Healthy females have narrower airways, and during exercise they breathe at higher operating lung volumes, which increases the work of breathing and neural drive to breathe, when compared with males at similar ventilation rates.7 18 19 When expressed relative to maximal ventilation, males and females demonstrate similar work of breathing,7 18 19 suggesting the difference is predominantly driven by structure rather than function.20 As a result, females report greater dyspnoea at a given ventilatory rate,19 21 and female athletes typically report increased exertional dyspnoea compared with male athletes with asthma.22 Despite research evaluating sex differences in the dyspnoea response to exercise in health,19 21 the physiological underpinnings of increased exertional dyspnoea in females with asthma are poorly understood. Accordingly, the primary objective of the present study was to compare ventilatory and sensory responses during incremental exercise in females with and without asthma. It was hypothesised that females with asthma would experience greater dyspnoea compared with female controls and that the increased dyspnoea in females with asthma would be secondary to dynamic respiratory mechanical abnormalities, specifically elevated operating lung volumes, compared with female controls. As a comparison group, males with asthma and male controls were also examined in the study.
Materials and methods
Patient and public involvement
Patients were not involved in the concept, recruitment or design of the current trial.
Study design
This manuscript is part of a larger series of studies examining cardiopulmonary physiology in individuals with asthma, and some of the patient data has been published previously.5 23
The present study is a case–controlled observational study. The four sessions included: (1) a standardised pulmonary function test, including inhaled beta-agonist reversibility; (2) a methacholine challenge test; (3) an exercise challenge test and (4) an incremental cycle cardiopulmonary exercise test (CPET). On initial visit to the laboratory, each participant completed the Asthma Control Questionnaire (ACQ24) and the Physical Activity Readiness Questionnaire plus.25 In addition, medical history and demographic data were obtained prior to a pulmonary function test and CPET. The CPET was completed on a separate day as the pulmonary function test to avoid interference of beta-agonist inhalers on the CPET outcomes. Each participant completed three separate screening days to determine eligibility for participating including bronchodilator response following inhaled beta-agonist, a methacholine challenge and exercise challenge test in accordance with American Thoracic Society (ATS) guidelines.26
Participants
In accordance with previously listed ATS criteria,27 self-reported physician diagnosis of asthma was confirmed in 32 individuals (16 females with asthma, 16 males with asthma) by one of the following challenges: (1) ≥200 mL and 12% improvement in forced expired volume in 1 s (FEV1) following a beta-agonist administration, (2) ≥10% reduction in FEV1 following an exercise challenge test or (3) a 20% decrease in FEV1 following ≤4.0 mg/mL methacholine (PC20). For the control groups, 32 individuals (16 females and 16 males) without clinical history of asthma and who demonstrated no reversibility or hypersensitivity to the methacholine challenges were recruited. All individuals were free from any other known cardiovascular disease or lung disease. Patients with asthma were required to withhold inhaled corticosteroids for 48 hours prior to testing and short-acting beta-agonists 8 hours prior to testing. Participants were asked to abstain from physical activity, caffeine and alcohol 12 hours prior to testing. All participants who were identified as female reported contraception use and menstrual phase on the exercise day.
Pulmonary function
FEV1 and forced vital capacity (FVC) were evaluated using spirometry.28 On a separate day from the CPET, reversibility following an inhaled beta-agonist (4×100 µg salbutamol) was performed using a space chamber to ensure uniform dosing. Lung volumes were determined using plethysmography.29 Diffusing capacity was determined by measuring the single-breath diffusing capacity of carbon monoxide.30 All measurements were assessed using the V62J Body Plethysmography (Encore229 Vmax, SensorMedics, Yorba Linda, California, USA), and values were expressed as a percentage of predictive values, using Global Lung Initiative predictive equations.31–33
Methacholine challenge
ATS guidelines for the administration of methacholine have been previously published.34 35 In short, participants performed the tidal breathing method of administration and performed FEV1 manoeuvres at 30 and 90 s intervals. Individuals with asthma diagnosis started at a methacholine concentration of 0.125 mg/mL and doubling concentrations were administered until either a provocative concentration resulting in a 20% reduction in FEV1 (PC20) or a maximal concentration of 16 mg/mL was reached. Participants with no history of asthma (controls) performed the same procedure as above, though started at a concentration of 1.0 mg/mL as per recommendations.34
Exercise challenge test
ATS guidelines for the administration of an exercise challenge test have been previously published.36 Briefly, participants performed a cycle ergometer protocol such that each participant reached an exercise intensity to elicit a minute ventilation equivalent to 18–21 times their respective FEV1 within 3 min of initiating exercise and maintained that intensity for 6 min. During the entirety of the exercise session, participants breathed through a three-way, non-rebreathe mouthpiece which administered dry air (0% relative humidity) from a compressed gas cylinder through a Douglas bag apparatus (Hans Rudolph, Kansas, USA). Spirometry was conducted 1, 3, 5, 10, 15 and 20 min following the exercise session. A drop in FEV1 greater than or equal to 10% was used as criteria for a positive test.
Cardiopulmonary exercise test
The CPET consisted of a 4 min steady state rest period for baseline measurements. Initial work rate was set to 50 W and was increased by 25 W every 2 min to the limits of exercise tolerance.5 37 Participants rated their perceived breathing and leg discomfort using the modified Borg Scale38 at rest, within the last 30 s of every 2 min exercise interval and at the end of exercise, followed by an inspiratory capacity manoeuvre. Inspiratory capacity manoeuvre was used to calculate operating lung volumes including end-expiratory lung volume (EELV= total lung capacity (TLC)−IC) and inspiratory reserve volume (IRV=IC− VT).34 Dynamic hyperinflation was defined by a reduction in inspiratory capacity of >150 mL during exercise.39–41 Participants were asked to report the reason for exercise test termination immediately following completion of the protocol. The responses were broken down into four categories: breathing discomfort, leg discomfort, both breathing and leg discomfort, and other. All ventilatory and cardiovascular measurements were collected over the first 30 s of every second minute during the exercise test and were linked with the perceptual ratings and inspiratory capacity measurements collected in the final 30 s of the respective minute to avoid contamination of the expired gas data from the inspiratory capacity manoeuvre.42 43 Post-exercise spirometry was completed within 5 min of exercise cessation. VT-inflection points were derived using inverted Hey plots14 and verified by two independent collaborators. Briefly, all breath-by-breath VT data were averaged over 30 s and plotted relative to the corresponding minute ventilation (inverted Hey plot) for each participant. Consistent with previous work,15 44 45 the VT-inflection was then defined as the point at which the VT inflected or plateaued in each individual, despite a continual increase in ventilation. The associated physiological (eg, V̇E, IC, IRV) and sensory (eg, dyspnoea) data at this time point were compared between groups. Expiratory flow limitation was determined by placing the tidal breathing inside the maximal flow volume loop produced following the CPET.46 The minute ventilation relative to V̇CO2 production ratio (V̇E/V̇CO2)slope was calculated from the initiation of exercise to the respiratory compensation point,8 while V̇E/V̇CO2nadir was determined as the lowest 30 s average observed by each individual.
All exercise tests were performed on an electronically braked cycle ergometer (Ergoselect II 1200 Ergoline) using a cardiorespiratory metabolic measurement system (Encore229 Vmax, SensorMedics). Arterial oxygen saturation (SpO2) was estimated using finger pulse oximetry (N-595; Nellcor OxiMax). Heart rate was measured using electrocardiography (CardioSoft, GE Medical Systems). CPET measurements were expressed as per cent of predicted normal values.47
Statistical analysis
The sample size was calculated from previous work examining dyspnoea observed in stable asthma compared with controls during incremental exercise5 which found a 1.5 Borg unit (pooled SD of 1.4) difference between the two groups during submaximal exercise. An a priori sample size calculation determined that 16 females with asthma would be sufficient in detecting a difference in dyspnoea sensation compared with female controls (α=0.05, β=0.80) while accounting for a potential 5% drop-out. Thirty-two males (16 asthma and 16 controls) were also recruited as a comparison (total sample=64).
Baseline demographics and pulmonary function data were compared between controls and individuals with asthma using a one-way analysis of variance (ANOVA). A repeated measures ANOVA was used to evaluate physiological and sensory variables at standardised submaximal work rates. Additionally, a one-way ANOVA was used to analyse differences in peak exercise variables. A linear regression was used to determine associations between baseline pulmonary function and exercise outcomes. Reason for test termination was analysed using Fisher’s exact test. All statistical tests were performed using SPSS Statistics V.26.0 (IBM, Armonk, New York, USA). Statistical significance was set at p<0.05 a priori for all comparisons.
Results
Participant characteristics
Sixteen females with asthma were pairwise age, height and sex-matched to 16 healthy female controls (table 1). Sixteen males with asthma and matched controls were also recruited as a comparison group, and their characteristics and exercise data can be found in the supplement (online supplemental table 1). All participants were non-smokers and all participants with asthma were defined as well-controlled using the ACQ.24 Pulmonary function results for females are reported in table 2. Male pulmonary function results are found in the supplement (online supplemental table 2).
Supplemental material
Pulmonary responses to bronchial challenges are described in table 1 for females and online supplemental table 1 for males. The mean responses in FEV1 to reversibility, methacholine and exercise challenge test (regardless of whether the tests were positive) were 10±9%, −23±12% and −6±11% in females with asthma, respectively.
All participants reached peak exercise criteria, meeting at least three of the four conditions: volitional exhaustion, a respiratory exchange ratio greater than 1.1, increases in oxygen consumption <100 mL∙min−1 with further increase in power output and reaching age-predicted maximum heart rate48 as shown in online supplemental table 3 and 4. Relative peak oxygen consumption (V̇O2peak) was not significantly different between female controls and females with asthma (p=0.07).
Ventilatory and metabolic responses to exercise
Metabolic and ventilatory responses at highest equivalent workload (125W), VT-inflection point and peak exercise data for both female groups can be found in online supplemental table 4. Ventilation at submaximal exercise was significantly higher in females with asthma compared with female controls at matched workloads (100W: p=0.02, 125W: p=0.01) which was secondary to an increased breathing frequency (figure 1). Despite elevated ventilation at matched submaximal exercise intensities in females with asthma, the VT-inflection was determined to be at a significantly lower minute ventilation in females with asthma compared with female controls (Control: 70.2±16.5 L∙min−1 vs Asthma: 57.7±12.3 L∙min-1; (p=0.02). The VT-inflection also occurred at significantly lower power output (Control: 163±33 W vs Asthma: 128±26 W; p<0.01) and relative V̇O2 (Control: 35.7±6.7 mL∙kg-1∙min-1 vs Asthma: 30.6±6.2 mL∙kg-1∙min-1; p=0.03) in females with asthma as compared with controls. In contrast, males with asthma had similar minute ventilation at the VT-inflection point as male controls (Control: 93.7±25.3 L∙min-1 vs Asthma: 91.4±27.8 L∙min-1; p=0.81). Further, males with asthma reached similar relative V̇O2 and power output at VT-inflection as compared with male controls (p=0.75 and p=0.39, respectively) which highlights the differential response in females with asthma.
VT/inspiratory capacity and end inspiratory lung volume was not significantly different at the VT-inflection point (p=0.07 and p=0.12, respectively) between females with asthma and female controls. These results are consistent with previous respiratory mechanics studies in health and disease that showed close association between the VT-inflection and the mechanical load on the respiratory system (tidal oesophageal pressure swings, inspiratory elastic work of breathing).15 49 Interestingly, relative V̇O2 at VT-inflection was significantly associated with pre-bronchodilator FEV1 in females with asthma (R2=0.401; p<0.01) but not female controls (R2=0.002; p=0.88) (figure 2B).
Lung mechanics
Inspiratory capacity throughout submaximal exercise and at peak exercise was significantly lower in females with asthma compared with female controls (75W p=0.01, 100W p=0.03, 125W p=0.01, VT-inflection p=0.01, and peak p=0.04) (figure 1C); however, inspiratory capacity was not significantly different between groups when expressed as %TLC (online supplemental table 4). IRV was also significantly lower at matched workloads in females with asthma compared with controls (75W p=0.01, 100W p=0.01, 125W p=0.04), but no difference was detected at the VT-inflection (p=0.72) or peak exercise (p=0.34) (figure 1D). Differentially, males with asthma demonstrated no differences in both inspiratory capacity and IRV (p=0.20 and p=0.81, respectively) during submaximal exercise. Males with asthma did have a significantly lower inspiratory capacity at peak exercise compared with male controls (control: 3.89±0.41 L vs asthma: 3.46±0.47 L; p=0.02) (online supplemental figure 1).
Supplemental material
Consistent with previous literature in asthma,5 expiratory flow limitation was also significantly greater in both females and males with asthma at peak exercise compared with their respective controls (p=0.04 and p=0.01, respectively) (online supplemental table 3 and 4).
Perceptual responses to exercise
Dyspnoea responses to exercise are shown in figure 3. Exertional dyspnoea was significantly higher in females with asthma compared with controls at matched submaximal workloads (figure 3A) but was not significantly different at the VT-inflection point (p=0.64) or at peak exercise (p=0.75). Males with asthma however did not demonstrate significant differences in dyspnoea throughout submaximal (p=0.06) or peak exercise (p=0.34). Despite the significantly reduced IRV in females with asthma at submaximal workloads, the IRV/dyspnoea relationship to exercise was maintained in all four groups (figure 3B and online supplemental figure 2B).
Supplemental material
Discussion
The main findings from the study are threefold. First, females with asthma had elevated dyspnoea at submaximal workloads during incremental exercise, which was associated with decreased IRV compared with female controls. Second, females with asthma demonstrated a lower VT-inflection point compared with female controls. Third, the VT-inflection point was significantly associated with pre-bronchodilator FEV1 in females with asthma but not in healthy female controls. Consistent with other respiratory conditions,50 these findings demonstrate that dyspnoea is linked to reduced IRV in females with asthma and that the early VT-inflection point observed in females with asthma is largely due to mechanical constraint on VT expansion. Further, the above findings help to explain why females with controlled asthma consistently report greater dyspnoea during submaximal exercise compared with healthy females and males with asthma.
As previously mentioned, females have narrower conducting airways then males even when matched for lung size.17 The relatively narrower airways predispose even healthy females to greater airway resistance when ventilation is increased during exercise.6 51 52 In individuals with asthma, airway resistance may be further limited by baseline bronchoconstriction which further increases resistance and the prevalence of mechanical ventilatory constraint.5 53 Although lung size was not significantly associated with the VT-inflection point in females with asthma, baseline FEV1 was found to be significantly associated with relative V̇O2 at the VT-inflection point (figure 2B). These findings are consistent with Lougheed et al54 which similarly demonstrated a relationship between FEV1 and hyperinflation during bronchial challenges in asthma. The significantly early VT-inflection in females with asthma could be an attempt to minimise further increases in elastic work of breathing which is associated with large respiratory efforts during exercise. Altering breathing patterns by maintaining the VT and increasing breathing frequency allows for maintenance of minute ventilation without encroaching on maximal expiratory flow. In the current study, no between-group differences were observed in peak V̇E/V̇CO2 and end-tidal PCO2 was below 35 mm Hg at peak exercise in females with asthma (online supplemental table 4), suggesting sufficient compensatory alveolar hyperventilation at maximal exercise. Despite relative V̇O2peak not being significantly different between females with and without asthma, females with asthma had a lower absolute aerobic fitness compared with controls, and therefore, it is possible that the difference in VT-inflection point could be explained by fitness. However, a subanalysis conducted using the females with asthma who have the greatest aerobic fitness (ie, the top 50% V̇O2peak of females with asthma) were compared with controls, there is no difference between these two groups in V̇O2peak (control: 44.0±5.3 mL∙kg−1∙min−1 vs higher 50%: 44.6±4.1 mL∙kg−1∙min−1; p=0.76); however, the minute ventilation at VT-inflection was still lower in the females with asthma (control: 70.2±16.5 L∙min−1 vs higher 50%: 56.3±11.8 L∙min−1; p=0.03), suggesting the difference is not explained by fitness. The current study was observational, and future work examining interventions to improve respiratory mechanics, which presumably would positively affect VT-inflection, dyspnoea and exercise capacity, is required.
Expiratory flow limitation can be alleviated through increasing operating lung volumes (as demonstrated by reduced IRV).7 55 While reducing airflow resistance, breathing at higher operating lung volumes forces breathing to occur on the less compliant portion of the pressure–volume curve, which has been shown to increase elastic work of breathing and heighten dyspnoea sensation.15 56 Previous work in obstructive pulmonary diseases (ie, COPD and asthma) has shown that increased dyspnoea sensation with exercise is associated to reduced IRV.5 44 54 A reduced IRV reflects a decrease in the operating limit for VT expansion, as end-inspiratory lung volume approaches TLC, where further increase in volume is constrained. Further, a greater ventilation in the setting of a reduced resting and dynamic inspiratory capacity accelerates the decline in IRV to its critically low value, which would be corroborated by an earlier VT-inflection at a low work rate and onset of severe exertional dyspnoea.15 44 57 In the current study, females with asthma were found to experience more dyspnoea at matched absolute submaximal exercise intensities than healthy female controls. Exertional dyspnoea was associated with reduced IRV (figure 3A), which was consistent with previous work in health and other obstructive diseases.19 21 44 58 Further, the trajectory of perceived dyspnoea increases in both female groups as IRV approaches ~0.7 L which is consistent with previous work demonstrating the association between mechanical critical constraint (ie, a critically low IRV) and dyspnoea sensation.44 59
Dyspnoea is a distressing sensation that can have dramatic impact on quality of life. Previous work has suggested that females with obstructive lung disease report more dyspnoea during activities of daily living than their male counterparts.60–62 To our knowledge, no study to date has evaluated the lung mechanics and exertional dyspnoea responses in female patients with asthma. In the current study, females with asthma were found to experience more dyspnoea at matched absolute submaximal exercise intensities (figure 3A). Females with asthma had similar dyspnoea ratings at the VT-inflection point as female controls, despite breathing at significantly lower ventilation rate. These findings are consistent with Laveneziana et al13 which found a significant increased inflection of dyspnoea sensation at the VT-inflection point regardless of IRV in individuals with asthma. The observed reduced IRV during submaximal exercise coupled with the early onset of VT-inflection in females with asthma provides an explanation to the significantly elevated dyspnoea experienced in this group during exercise.
Although the primary focus of the study was to investigate ventilatory and dyspnoea responses in females with asthma, as a comparison, males with asthma and matched controls were also recruited for the current study and results can be found in online supplemental file. Despite similar asthma control to females, the VT-inflection was not significantly different between males with asthma and male controls. Further, operating lung volumes (IRV and inspiratory capacity) were not different between the two male groups during submaximal exercise. Similar to females with asthma, males with asthma demonstrated an adequate ventilatory response to exercise as V̇E/V̇CO2 and end-tidal PCO2 were not different compared with male controls. Lastly, males with asthma did not demonstrate significantly greater dyspnoea at submaximal exercise compared with controls which is in contrast to what was observed in females with asthma. These findings demonstrate that compared with males with asthma, females with asthma tend to demonstrate greater mechanical constraint during submaximal exercise as indicated by an earlier VT-inflection point and significantly reduced IRV compared with controls, contributing to increased dyspnoea sensation.
Limitations
The current study did not evaluate invasive measurements of diaphragmatic muscle effort,12 63 electrical activation of the diaphragm (reflecting inspiratory neural drive)19 64 or discriminate between qualitative descriptors of dyspnoea.21 Rather, the current study focused on non-invasive measurements of operating lung volumes and breathing pattern in females with asthma compared with female controls and its relationship to dyspnoea.
Asthma is a heterogeneous disease with varying severity and phenotypes. A much larger study would be required to describe the exercise responses across varying asthma phenotypes including those individuals with asthma who may demonstrate significant bronchodilation53 or bronchoconstriction65 during exercise. Although the current study tested individuals with asthma while withholding inhaler medications, previous work has demonstrated that administration of a short-acting inhaler prior to an incremental exercise test did not significantly alter operating lung volumes nor dyspnoea perception in individuals with mild to moderately controlled asthma.5 The current study included all patients with asthma as defined by ATS criteria; however, only 2 of the 16 females with asthma demonstrated evidence of exercise-induced bronchoconstriction. The low percentage of females with asthma who demonstrated significant exercise-induced bronchoconstriction most likely reflects a bias of recruitment to an exercise-based research study. Therefore, this small subsample size did not allow for further subanalysis.
Summary
This study examined the differences in breathing patterns, operating lung volumes and dyspnoea responses to exercise between females with asthma and healthy female controls. This is the first study to show that during submaximal exercise, females with asthma experience greater dyspnoea than female controls secondary to mechanical constraint. Further, our findings show that in females with asthma, but not female controls, baseline bronchoconstriction is strongly associated with VT-inflection point, further emphasising the importance of the mechanical ventilatory constraint on dyspnoea sensation in this group. Elevated exertional dyspnoea at submaximal intensities in females with asthma can lead to increased exercise avoidance and increased symptom burden.2 A more targeted approach is needed in females with asthma to help manage exertional dyspnoea, as physical activity is a crucial part of asthma management.1 3
Data availability statement
No data are available.
Ethics statements
Patient consent for publication
Ethics approval
This study involves human participants and was approved by Human Research Ethics Board of the University of Alberta (Biomedical Panel: Pro00047054). Participants gave informed consent to participate in the study before taking part.
References
Supplementary materials
Supplementary Data
This web only file has been produced by the BMJ Publishing Group from an electronic file supplied by the author(s) and has not been edited for content.
Footnotes
Twitter @AndrewBrotto, @mkstickland
Contributors ARB, DBP, LEM and MKS conceived the project. ARB, SR, LEM and EW acquired data set. ARB and DBP did the statistical analyses and drafted the initial manuscript. MKS obtained the funding. All authors participated in the interpretation of the results, edited and reviewed the manuscript. MKS is responsible for the overall content as guarantor.
Funding This work was supported by Canadian Institute of Health Research (grant number 407589). The corresponding author MKS obtained funding.
Competing interests None declared.
Patient and public involvement Patients and/or the public were not involved in the design, or conduct, or reporting, or dissemination plans of this research.
Provenance and peer review Not commissioned; externally peer reviewed.
Supplemental material This content has been supplied by the author(s). It has not been vetted by BMJ Publishing Group Limited (BMJ) and may not have been peer-reviewed. Any opinions or recommendations discussed are solely those of the author(s) and are not endorsed by BMJ. BMJ disclaims all liability and responsibility arising from any reliance placed on the content. Where the content includes any translated material, BMJ does not warrant the accuracy and reliability of the translations (including but not limited to local regulations, clinical guidelines, terminology, drug names and drug dosages), and is not responsible for any error and/or omissions arising from translation and adaptation or otherwise.