Abstract
Purpose
Power output at the moderate-to-heavy-intensity transition decreases during prolonged exercise, and resilience to this has been termed ‘durability’. The purpose of this study was to assess the relationship between durability and the effect of prolonged exercise on severe-intensity performance, and explore intramuscular correlates of durability.
Methods
On separate days, 13 well-trained cyclists and triathletes (V̇O2peak, 57.3 ± 4.8 mL kg−1 min−1; training volume, 12 ± 2.1 h week−1) undertook an incremental test and 5-min time trial (TT) to determine power output at the first ventilatory threshold (VT1) and severe-intensity performance, with and without 150-min of prior moderate-intensity cycling. A single resting vastus lateralis microbiopsy was obtained.
Results
Prolonged exercise reduced power output at VT1 (211 ± 40 vs. 198 ± 39 W, ∆ -13 ± 16 W, ∆ -6 ± 7%, P = 0.013) and 5-min TT performance (333 ± 75 vs. 302 ± 63 W, ∆ -31 ± 41 W, ∆ -9 ± 10%, P = 0.017). The reduction in 5-min TT performance was significantly associated with durability of VT1 (rs = 0.719, P = 0.007). Durability of VT1 was not related to vastus lateralis carnosine content, citrate synthase activity, or complex I activity (P > 0.05).
Conclusion
These data provide the first direct support that durability of the moderate-to-heavy-intensity transition is an important performance parameter, as more durable athletes exhibited smaller reductions in 5-min TT performance following prolonged exercise. We did not find relationships between durability and vastus lateralis carnosine content, citrate synthase activity, or complex I activity.
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Introduction
Performance outcomes in stochastic endurance events, such as road cycling, are often determined by the ability to produce high work outputs in the severe-intensity domain following multiple hours of exercise, primarily performed in the moderate-intensity domain (Fernández-García et al. 2000; Sanders et al. 2019). Physiological profiling characteristics are estimated in well-rested athletes during routine laboratory assessments and used for the assessment of performance capabilities, within-session intensity regulation, and monitoring training load and adaptation (Maunder et al. 2021b). Prolonged exercise elicits progressive physiological changes, such as increased core and muscle temperature (Febbraio et al. 1994), depletion of endogenous fuel stores (Gonzalez et al. 2016; Areta and Hopkins 2018; Stokie et al. 2023), accumulation of muscle damage (Stevens et al. 2018), and cellular stress (Morton et al. 2009; Peake et al. 2017). Consequently, physiological profiling characteristics, such as work output at the moderate-to-heavy (Stevenson et al. 2022b) and heavy-to-severe (Clark et al. 2018, 2019a, 2019b)-intensity transitions, gross cycling efficiency (Passfield and Doust 2000; Hopker et al. 2017) and the peak rate of oxygen consumption (V̇O2peak) (Brownstein et al. 2022) may, in some instances, degrade during prolonged exercise. ‘Durability’ is defined as an individual’s resilience to deteriorations in physiological profiling characteristics during prolonged exercise, and has been proposed as a key endurance performance parameter (Maunder et al. 2021b). However, the influence of durability on performance outcomes has not been well-characterised.
Like physiological profiling characteristics, severe-intensity performance decreases with prolonged exercise (Spragg et al. 2023a, b). Durability of the intensity domain transitions may promote resilience to the effects of prolonged exercise on severe-intensity performance. As power output at the moderate-to-heavy-intensity transition decreases during prolonged exercise (Stevenson et al. 2022b), an initially moderate-intensity power output may drift into the heavy-intensity domain. Heavy-intensity exercise elicits distinct physiological responses compared to the moderate-intensity domain, such as greater plasma K+ accumulation, reduced intramuscular pH, and phosphocreatine depletion (Black et al. 2017). Therefore, greater time spent in the heavy-intensity domain may result in reduced subsequent capacity for work outputs in the severe-intensity domain. This ‘domain drift’ may also be present during prolonged exercise initially in the heavy intensity domain, where exercise may drift into the severe domain. Accordingly, better durability of the intensity transitions may promote resilience to the effects of prolonged exercise on subsequent severe-intensity performance. However, the relationship between these variables has not been assessed.
The effect of prolonged exercise on subsequent severe-intensity performance may also be related to glycogen depletion. Glycogen depletion may impair Na+,K+-ATPase pump activity, and therefore the ability to regulate K+ homeostasis and maintain muscle contractile function (Jensen et al. 2020). Specifically, Na+,K+-ATPase function appears dependent on intramyofibrillar glycogen (Nielsen et al. 2022), and intramyofibrillar glycogen depletion has been implicated in impaired muscle contractile function (Nielsen et al. 2009, 2014; Ørtenblad et al. 2011, 2013). Furthermore, recent work in mouse muscle suggests glycogen depletion increases the number of inexcitable muscle fibres unable to contribute to force and power production, and therefore performance (Cairns and Renaud 2023). Therefore, it is plausible that athletes capable of oxidising fat at high rates to preserve glycogen during submaximal exercise may be better able to maintain severe-intensity performance following prolonged exercise. Indeed, fat oxidation rates during submaximal exercise have been associated with durability of the heavy-to-severe-intensity transition and severe-intensity performance (Spragg et al. 2023b). The capacity for fat oxidation during exercise has been quantified using the peak fat oxidation rate (PFO) observed during an incremental exercise test (Maunder et al. 2018, 2023), and PFO has been related to endurance performance outcomes (Frandsen et al. 2017; Maunder et al. 2022). However, the relationship between PFO and the effect of prolonged exercise on severe-intensity performance has not been assessed.
Similarly, the physiological determinants of durability are not well-explored. Plausibly, skeletal muscle fibre type composition may influence durability, as type I fibres are more fatigue resistant (Thorstensson and Karlsson 1976). Likewise, possessing a larger mitochondrial pool may spread the oxidative burden of a given work rate, and therefore reduce negative effects on the function of individual mitochondria during prolonged exercise (Sahlin et al. 2010; Trewin et al. 2017; Layec et al. 2018; Lewis et al. 2021). This may promote durability by delaying deteriorations in mitochondrial function, and therefore the oxidative capacity of muscle. Heat shock protein 70 (HSP70) availability may also relate to durability. HSP70 is an intracellular chaperone involved in managing protein aggregation and cellular stress (Krüger et al. 2019). Greater HSP70 abundance may, therefore, augment the capacity to manage the cellular stress generated during prolonged exercise, and therefore promote durability. Understanding the mechanistic determinants of durability may allow for the development of targeted interventions to improve it.
Therefore, the primary aims of the present investigation were to: (i) determine if durability of the moderate-to-heavy transition is related to the magnitude of prolonged exercise-induced reductions in severe-intensity performance, (ii) assess the relationship between prolonged exercise-induced reductions in severe-intensity performance and PFO and (iii) quantify relationships between various intramuscular characteristics and durability of the moderate-to-heavy-intensity transition. We hypothesised that cyclists who have greater durability of the moderate-to-heavy-intensity transition would be more resilient to the effect of prolonged exercise on severe-intensity performance, that resilience to the effects of prolonged exercise on severe-intensity performance would be related to PFO, and that durability of the moderate-to-heavy-intensity transition would be related to various oxidative properties of skeletal muscle.
Methods
Ethical approval
The study was performed in accordance with the Declaration of Helsinki, 2013. The Auckland University of Technology Ethics Committee approved all procedures (22/163), and all participants provided written informed consent prior to participation. This study was not registered in a database. Raw data are available upon request.
Participants
Thirteen well-trained endurance cyclists and triathletes completed the present investigation (eleven males, two females; age, 29 ± 7; height, 182.6 ± 8 cm; mass, 78.1 ± 11.7 kg; V̇O2peak, 57.3 ± 4.8 mL kg−1 min−1; training volume, 12 ± 2.1 h week−1). A-priori calculations indicated that 15 participants were required to detect a significant bivariate correlation of r = 0.6, assuming a null hypothesis correlation of r = 0, and a one-tailed test, with 80% statistical power and a type I error rate of 0.05. All participants were free of recent (< 3 months) illness and musculoskeletal injury, free of cardiovascular disease, and training > 8 h week−1 in endurance cycling, with a peak oxygen uptake > 55 mL kg−1 min−1 and self-reported best-effort 20-min power output of > 3.5 W kg−1. All participants provided written informed consent. Three participants dropped out after the first visit due to the inclusion criteria of remaining free of illness for > 3 months.
Study design
Participants visited the laboratory on four separate occasions, ~ 5–14 days apart, at ~ 6:00 am (Fig. 1). The first visit was a characterisation trial, involving an incremental cycling test for estimation of power output at the first ventilatory threshold (VT1) for use in subsequent trials and peak oxygen uptake (V̇O2peak), and a familiarisation 5-min time trial. The second and third visits took place in random, counterbalanced order and involved either (i) PRE: a submaximal incremental test to determine the moderate-to-heavy-intensity transition, and performance and V̇O2peak in a 5-min time trial, or (ii) POST: 150 min of cycling at 90% of the first ventilatory threshold (VT1) power output estimated in the characterisation trial, followed by the submaximal incremental test to determine the moderate-to-heavy-intensity transition, and performance and V̇O2peak in a 5-min time trial. The 5-min time trials were used to mimic a decisive effort in a road cycling event, and because these fall within the severe-intensity domain (Jones et al. 2019). Fixed-duration cycling time trials also produce reliable data, particularly in trained cyclists following a familiarisation trial (Hopkins et al. 2001; Paton and Hopkins 2001; Leo et al. 2022). The remaining visit was for a resting vastus lateralis microbiopsy.
Characterisation trial
Participants reported to the laboratory for an initial incremental cycling test and 5-min familiarisation time trial, after having fasted overnight for ~ 10 h and having ingested 1–2 L of plain water before arrival. After providing written informed consent, height and mass were determined. Cycling commenced with a 5-min warm-up at 100 W on personal road bicycles mounted to a direct-drive smart indoor trainer (Kickr, Wahoo Fitness, GA, USA). Subsequently, the incremental cycling test began at 95 W, with the power output increasing by 35 W every 3 min. Expired gases and heart rate were collected continuously using indirect calorimetry (TrueOne 2400, ParvoMedics, UT, USA) and a chest-strap heart rate monitor (Polar Electro Oy, Kempele, Finland). When the respiratory exchange ratio reached 1.0, power output was increased by 35 W every minute until volitional exhaustion. The V̇O2peak was accepted as the highest 15-s average V̇O2, and VT1 was identified as the first V̇O2 breakpoint in the V̇O2 vs. V̇E.V̇O2−1 relationship. This V̇O2 was converted to power output by linear regression of the V̇O2 vs. power output relationship, using the last minute of V̇O2 data from each 3-min stage. The last minute of expired gas data in each 3-min stage was also used to quantify whole-body rates of carbohydrate and fat oxidation using standard equations (Eq. 1) (Jeukendrup and Wallis 2005). The highest observed rate of whole-body fat oxidation was identified as the peak fat oxidation rate (PFO) (Maunder et al. 2022).
where V̇O2 and V̇O2 are in L.min-1
Following completion of the incremental test, participants rested for 15 min before completing a 5-min performance time trial at maximal effort, with the goal of achieving the highest possible average power output. Expired gases and heart rate were collected throughout; however, participants were blinded to all data other than elapsed time. Verbal encouragement was not provided to control the influence of this variable on performance outcomes (McCormick et al. 2015). We have refrained from providing verbal encouragement during time trials previously (Maunder et al. 2021a). The importance of providing a maximum effort during time trials was stressed to participants at the beginning of the study, and participants were reminded of this ahead of each time trial. The highest 15-s average of V̇O2 was accepted as the time trial V̇O2peak. If this value exceeded the V̇O2peak achieved during the maximal, incremental cycling test, it was used as the characterisation trial V̇O2peak. Following the time trial, participants were provided with blank 7-d exercise and 2-d diet record sheets, which were completed in advance of the second trial, and replicated in advance of the third trial.
Visits two and three: PRE and POST assessments
Participants returned to the laboratory 5–14 days following the characterisation trial to complete the first of the two subsequent trials. Participants arrived having consumed a standardised breakfast containing ~ 2 g kg−1 of carbohydrate and ~ 800 mL of water 1 h beforehand. Participants were fitted with a chest-strap heart rate monitor, and a wireless near-infrared spectroscopy device for estimation of muscle oxygenation (SmO2) on their right leg (Moxy Monitor, Fortiori Design LLC, Hutchinson, MN, USA). The device was placed over the mid-belly of the vastus lateralis, half the distance between the tibial tuberosity and greater trochanter. The precise site of the device was recorded such that it could be repeated in the remaining trial. Heart rate and muscle oxygenation were measured continuously throughout the trial.
The PRE and POST trials began with a 5-min warm-up at 100 W. Following warm-up, participants cycled for 150 min at 90% of their estimated VT1 power output in the POST but not PRE trial, with expired gases collected for 4 min every 15 min. Expired gases were used to quantify rates of whole-body rates of energy expenditure, carbohydrate oxidation, and fat oxidation during the 150-min preload using standard equations (Jeukendrup and Wallis 2005). In POST, participants consumed 150 mL of water every 15 min in a solution made with electrolyte mix (LMNT) containing 125 mg Na+, 25 mg K+, and 7.5 mg Mg2+ during the first 120 min of the 150-min preload.
Subsequently, the moderate-to-heavy-intensity transition was estimated precisely using a five-step incremental test with continuous collection of expired gases. The first step began 50 W below the VT1 power output estimated in the first laboratory visit, and increased by 25 W every 4 min, such that the fifth and final step was 50 W above the VT1 power output estimated in the first laboratory visit. The moderate-to-heavy-intensity transition power output was estimated using the methods described for determining VT1 in the first laboratory visit, but with greater precision given the greater density of data around the transition. This method has been used to estimate the moderate-to-heavy-intensity transition previously, producing similar results to blood lactate-derived measurements (Stevenson et al. 2022b). Following the five-step incremental test, participants cycled at 100 W for 5 min before completing a 5-min performance time trial according to the procedures described above. The effect of prolonged exercise on the moderate-to-heavy-intensity transition power output, 5-min time trial performance, and V̇O2peak during the 5-min time trial was determined by subtracting PRE from POST values. We used this exercise protocol as we previously observed reduced power output at the moderate-to-heavy-intensity transition after 150 min of initially moderate-intensity cycling (Stevenson et al. 2022b), and to simulate a road cycling event, in which a severe-intensity effort near the finish may follow a longer period of lower intensity cycling (Fernández-García et al. 2000; Sanders et al. 2019).
Visit four: resting vastus lateralis microbiopsy
Approximately 5–14 days following the third visit, participants returned to the laboratory having consumed breakfast and having refrained from vigorous exercise for 24 h. A ~ 15–30 mg resting microbiopsy sample was obtained from the mid-belly of the vastus lateralis of the dominant leg, ~ 10–15 cm above the patella. Local anaesthesia was applied to the skin and superficial muscle fascia. A microbiopsy needle was then inserted into the mid-belly of the vastus lateralis to a depth of ~ 2 cm to recover ~ 20–40 mg of tissue using a spring-loaded mechanism (14G Ultimate Biopsy Needle, Zamar Care, Croatia). Muscle tissue was immediately frozen on dry ice and stored at −80 °C until further analysis.
Muscle analyses
Frozen muscle was cut and rinsed using cold phosphate-buffered saline (PBS) and then suspended to ~ 25 mg.mL−1 in PBS. Samples were then ground manually and thoroughly using a pre-cooled Dounce homogeniser. Homogenate was solubilised in extraction buffer (ab260490, Abcam®) to ~ 5 mg mL−1 and incubated on ice for 20 min prior to centrifugation at 16,000 g for 10 min at 4 °C. Supernatant was extracted and stored at −80 °C prior to further analysis. Supernatant was thawed and assayed in duplicate for carnosine concentration (MBS721162, MyBioSource®; our laboratory-specific coefficient of variation [CV], 12.6%), citrate synthase enzyme activity (ab119692, Abcam®; CV, 11.4%), and complex I enzyme activity (ab109721, Abcam®; CV, 12.1%). All outcome measures were expressed relative to sample protein concentration using a Bradford assay, performed in triplicate (ab102535, Abcam®; CV, 6.1%). Carnosine concentrations, as assessed by 1H-magnetic resonance spectroscopy, have been related to fibre type profile (Baguet et al. 2011). Lower carnosine concentrations are observed in type I compared to type II skeletal muscle fibres (Harris et al. 1998). We, therefore, used our measures of muscle carnosine as an indicator of muscle fibre type profile. CS and complex I activities are related to mitochondrial protein content (Larsen et al. 2012). We, therefore, used our measures of CS and complex I activities as markers of mitochondrial protein content.
Statistical analyses
Data are expressed as mean ± standard deviation, unless otherwise stated. Normality of datasets was assessed using Shapiro–Wilk tests. Simple PRE vs. POST comparisons of the moderate-to-heavy-intensity transition power output, V̇O2peak, and time trial performance were made using paired t tests or Wilcoxon signed-rank tests, depending on normality, and used to verify the effect of prolonged exercise on these parameters. The effect of time on whole-body rates of energy expenditure, carbohydrate oxidation, fat oxidation, SmO2, and heart rate during the 150 min preload in POST was analysed using one-way repeated measures analyses of variance.
Bivariate relationships between (i) the magnitude of the PRE vs. POST change in moderate-to-heavy-intensity transition power output and the magnitude of the PRE vs. POST change in time trial performance, (ii) the magnitude of the PRE vs. POST change in V̇O2peak and the magnitude of the PRE vs. POST change in time trial performance, (iii) the magnitude of the PRE vs. POST change in time trial performance and PFO, (iv) the magnitude of the PRE vs. POST change in moderate-to-heavy-intensity transition power output and skeletal muscle characteristics were assessed using Pearson’s or Spearman’s rank-order correlation coefficients (depending on normality), and expressed with 95% confidence intervals. The strength of correlations were assessed according to the following qualitative criteria: < 0.10, trivial; 0.10–0.29, small; 0.30–0.49, moderate; > 0.50, large (Cohen 1992). The PRE and POST values for SmO2 at the moderate-to-heavy-intensity transition were compared using paired t tests or Wilcoxon signed-rank tests, depending on normality, and intra-class correlation coefficients and coefficient of variation statistics were computed. All analyses were performed in GraphPad Prism Version 9.3.1. Significance was inferred when P ≤ 0.05.
Results
Prolonged exercise phase
The estimated power output at VT1 in the initial assessment was 208 ± 30 W. The 150-min prolonged phase in POST was, therefore, completed at 187 ± 27 W. During the prolonged phase, there was an effect of time on heart rate, EE, carbohydrate oxidation, and fat oxidation (P < 0.05). Significant effects of time on V̇O2 and SmO2 were not observed (Fig. 2).
Effects of prolonged exercise
Power output at VT1 (211 ± 40 W vs. 198 ± 39 W, ∆ -13 ± 16 W, ∆ -6 ± 7%, P = 0.013) and 5-min time trial performance (333 ± 75 W vs. 302 ± 63 W, ∆ -31 ± 41 W, ∆ -9 ± 10%, P = 0.017) significantly decreased from PRE to POST. The V̇O2peak (4.37 ± 0.85 vs. 4.28 ± 0.78 L.min−1, P = 0.252) and SmO2 at VT1 (37 ± 13 vs. 40 ± 16%, P = 0.139) were not significantly different between PRE and POST (Fig. 3). The within-subject CV for SmO2 at VT1 in PRE and POST was 13.0%, with an intra-class correlation of 0.874.
Correlational analyses
The change in power output at VT1 from PRE to POST was strongly associated with PRE-to-POST change in 5-min time trial power output and V̇O2peak (P < 0.05). The PRE-to-POST change in V̇O2peak was not significantly associated with the change in 5-min time trial power output, nor was PFO (Fig. 4). No significant relationships were observed between the PRE-to-POST change in power output at VT1 and vastus lateralis carnosine concentration (24.0 ± 12.2 µg.g−1 protein), CS activity (16.1 ± 5.1 µmol −1 min−1 mg−1 protein), or complex I activity (5.8 ± 3.2 µmol −1 min−1 mg−1 protein) (Fig. 5).
Discussion
Our primary observations were that: (i) prolonged exercise-induced reductions in severe-intensity time trial performance were strongly related to durability of the moderate-to-heavy-intensity transition, (ii) prolonged exercise-induced reductions in severe-intensity time trial performance were not related to PFO, (iii) no relationships were observed between vastus lateralis CS activity, complex I activity, or carnosine concentration and durability of the moderate-to-heavy-intensity transition. These observations provide the first direct support for the hypothesis that durability of the moderate-to-heavy-intensity transition is an important endurance performance parameter, and therefore further support that durability of the moderate-to-heavy-intensity transition might be monitored at an individual level. The physiological determinants of durability remain to be identified.
In line with our hypothesis and previous work (Stevenson et al. 2022a; Spragg et al. 2023a, b), prolonged exercise led to a reduction in power output at the moderate-to-heavy-intensity transition and 5-min time trial performance (Fig. 3). Our novel observation is that those exhibiting larger reductions in power output at the moderate-to-heavy-intensity transition with prolonged exercise exhibited the largest reductions in 5-min time trial performance (Fig. 3). The strong relationship between the effects of prolonged exercise on the moderate-to-heavy-intensity transition and 5-min time trial performance could plausibly be mechanistically related. Athletes demonstrating greater reductions in power output at the moderate-to-heavy-intensity transition likely spent more time in the heavy domain during the prolonged phase. Heavy-intensity exercise results in greater extracellular K+ accumulation than moderate-intensity exercise (Black et al. 2017). Extracellular K+ accumulation depresses muscle force production, and therefore induces fatigue in vitro (Cairns et al. 1997; de Paoli et al. 2007). It is, therefore, plausible the more durable athletes were better able to maintain 5-min time trial performance due to better ability to maintain K+ homeostasis. However, given an incremental exercise test and 5-min recovery period occurred between the end of the prolonged phase and the 5-min time trial, it is possible that extracellular K+ concentrations were restored (Mohr et al. 2011). We suggest that this mechanism is interrogated in studies with measurement of plasma and interstitial K+ concentrations.
Second, prolonged exercise-induced reductions in 5-min time trial performance were not related to PFO (Fig. 4d). As muscle glycogen is an important fuel for high-intensity exercise (Vigh-Larsen et al. 2022), and glycogen availability is implicated in muscle fibre excitability and sensitivity to K+ disturbance (Cairns and Renaud 2023), we hypothesised that athletes with a higher PFO would better maintain muscle glycogen availability during the prolonged phase, and that this would be favourable for mitigating the fatiguing effects of K+ disturbances and maintaining muscle fibre excitability during the subsequent 5-min time trial. Despite the lack of association between the effect of prolonged exercise on 5-min time trial performance and PFO, it remains possible that glycogen availability may at least partially mediate the effects of prolonged exercise on severe-intensity performance. Although PFO during incremental exercise relates to fat oxidation rates during prolonged exercise (Maunder et al. 2022), PFO is not a direct measure of glycogen utilisation or availability. In support, fat oxidation rates during submaximal exercise have been associated with durability of the heavy-to-severe-intensity transition and severe-intensity performance (Spragg et al. 2023b). We, therefore, recommend that future studies interrogate the relationship between the effects of prolonged exercise on severe-intensity performance and muscle glycogen availability using direct measures of glycogen content, ideally with subcellular analyses.
In contrast to our hypothesis, durability of the moderate-to-heavy-intensity transition was not related to vastus lateralis carnosine concentration, citrate synthase activity, or complex I activity (Fig. 5). The absence of relationships between these variables and durability of the moderate-to-heavy-intensity transition may indicate that these variables are not mechanistically related, or may be due to the variability in these outcome measures, relatively low sample size, and/or relatively homogenous participant group. We did attempt to measure HSP70 in our muscle samples, but unfortunately this assay did not produce usable results (measured concentrations exceeded the detectable range of the assay). Due to budgetary constraints, we were unable to repeat the assay. We recommend that the relationship between intramuscular HSP70 abundance and durability is assessed in future studies.
As power output at the moderate-to-heavy-intensity transition declines during prolonged exercise, identification of a marker that can be viewed live during prolonged exercise and used to assess proximity to the moderate-to-heavy-intensity transition would be useful for within-session training intensity regulation (Maunder et al. 2021b). Here we measured muscle oxygenation (SmO2) using a non-invasive, wireless near-infrared spectroscopy device that could theoretically be used for this purpose. Measures of SmO2 reflect the balance between local oxygen use and supply (Wittekind et al. 2012; Yogev et al. 2023). The exercise intensity domains show distinct SmO2 responses to prolonged exercise (Kirby et al. 2021), and the SmO2 response to incremental exercise can be used to identify intensity domain transitions (Batterson et al. 2023). We found that the SmO2 coinciding with the moderate-to-heavy-intensity transition was not systematically different between PRE and POST (Fig. 3d). This supports the live monitoring of SmO2 for within-session intensity regulation, as estimates of the SmO2 associated with the moderate-to-heavy-intensity transition derived in routine physiological profiling assessments appear to hold over time during prolonged exercise. However, the within-subject CV for SmO2 at the moderate-to-heavy-intensity transition was ~ 13%, which suggests these measurements should be applied to prolonged exercise with caution. This variability may be due to movement of the device and therefore measurement site (Crum et al. 2017). Nevertheless, our data support further exploration of how SmO2 can be applied to within-session intensity regulation during prolonged exercise. We recommend that other SmO2 indices such as deoxygenated haemoglobin are also explored.
This study is limited by the sample size. We may have been insufficiently powered to detect relationships between durability and the intramuscular variables, given the known variability in the assays performed. In a between-subject analysis, this variability is further exacerbated by minor between-subject differences in the biopsy site, given previous research showing variability in intramuscular parameters within an individual at different sites along a muscle tissue (Horwarth et al. 2021). Furthermore, we cannot determine if the results observed within this study readily translate to elite athletes, to prolonged exercise with carbohydrate ingestion, or during stochastic-intensity prolonged exercise protocols, that may be more reflective of real-world road cycling events (Fernández-García et al. 2000; Sanders et al. 2019). We, therefore, recommend that the implications of durability for endurance performance are studied using a range of prolonged exercise protocols, athlete populations, and sports to provide a more detailed understanding of how durability influences real-world endurance performance outcomes.
In conclusion, we observed that durability of the moderate-to-heavy-intensity transition was related to the effect of prolonged exercise on severe-intensity time trial performance. However, we were unable to identify intramuscular variables that related to durability of the moderate-to-heavy-intensity transition. This study provides the first direct support that durability of the moderate-to-heavy-intensity transition is an important endurance performance parameter, and therefore that individual monitoring of durability of the moderate-to-heavy-intensity transition may be valuable.
Data availability
Data are available from the corresponding author upon reasonable request.
Code availability
None used.
Abbreviations
- CS:
-
Citrate synthase
- CV:
-
Coefficient of variation
- EE:
-
Energy expenditure
- PFO:
-
Peak fat oxidation rate
- SmO2 :
-
Muscle oxygen saturation
- rs :
-
Spearman’s rank-order correlation coefficient
- V̇O2 :
-
Rate of oxygen consumption
- V̇O2peak:
-
Peak rate of oxygen consumption
- VT1 :
-
First ventilatory threshold
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K.H., A.E.K., D.J.P., M.J.M., M.W., and E.M. conceived and designed the research. K.H., Tobias H. Cox, Thanchanok Charoensap, M.J.B., W.L.B., and E.M. undertook the experiments. K.H. and E.M. analysed samples. K.H. completed data analyses. K.H. and E.M. drafted the manuscript. All authors revised the manuscript.
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Hamilton, K., Kilding, A.E., Plews, D.J. et al. Durability of the moderate-to-heavy-intensity transition is related to the effects of prolonged exercise on severe-intensity performance. Eur J Appl Physiol 124, 2427–2438 (2024). https://doi.org/10.1007/s00421-024-05459-6
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DOI: https://doi.org/10.1007/s00421-024-05459-6