Effects of Endurance Training on Skeletal Muscle Bioenergetics in Chronic Obstructive Pulmonary Disease

Effects of Endurance Training on Skeletal Muscle Bioenergetics in Chronic Obstructive Pulmonary Disease

ERNEST SALA, JOSEP ROCA, RAMÓN M. MARRADES, JULI ALONSO, JOSÉ M. GONZALEZ de SUSO, ANGEL MORENO, JOAN ALBERT BARBERÁ, JOSEP NADAL, LLUIS de JOVER, ROBERT RODRIGUEZ-ROISIN, and PETER D. WAGNER

Servie de Pneumologia i Al·lèrgia Respiratòria, Departament de Medicina, IDIBAPS (Institut d'Investigacions Biomèdiques Pi i Sunyer), Hospital Clínic, Unitat de Medicina Preventiva i Salut Pública, Facultat de Medicina, Universitat de Barcelona, Centre Diagnòstic Pedralbes, Barcelona; Centre d'Alt Rendiment, Sant Cugat del Vallès, Spain; and Department of Medicine, Section of Physiology, University of California San Diego, La Jolla, California

ABSTRACT

TOP
ABSTRACT
INTRODUCTION
METHODS
RESULTS
DISCUSSION
REFERENCES

Physiologic adaptations after an 8-wk endurance training program were examined in 13 patients with chronic obstructive pulmonarydisease (COPD) (age, 64 ± 4 [SD] yr; FEV₁, 43 ± 9% pred; Pa_O₂,72 ± 8 mm Hg; and Pa_CO₂, 36 ± 2 mm Hg) and in eight healthy sedentarycontrol subjects (61 ± 4 yr). Both pre- and post-training studiesincluded: (1) whole-body oxygen consumption ( $V$ O₂) and one-legO₂ uptake ( $V$ O_2leg) during exercise; and (2) intracellular pH(pHi) and inorganic phosphate to phosphocreatine ratio ([Pi]/[PCr])during exercise; and half-time of [PCr] recovery. After training,the two groups increased peak $V$ O₂ (p < 0.05 each) and showeda similar fall in submaximal femoral venous lactate levels (p< 0.05 each). However, control subjects increased peak $V$ E (p< 0.01) and raised peak O₂ delivery (p = 0.05), not shown in patientswith COPD. Both groups increased post-training O₂ extraction ratio(p < 0.05). The most consistent finding, however, was in patientswith COPD, who had a substantial improvement in cellular bioenergetics:(1) half-time of [PCr] recovery fell from 50 ± 8 to 34 ± 7 s (p= 0.02); and (2) at a given submaximal work rate, [Pi]/[PCr] ratiodecreased and pHi increased (p < 0.05 each). We conclude thatbeneficial effects of training in patients with COPD essentiallyoccurred at muscle level during submaximalexercise.

	INTRODUCTION

TOP ABSTRACT INTRODUCTION METHODS RESULTS DISCUSSION REFERENCES

Respiratory rehabilitation, including lower limb exercise training, is recommended as part of the management for patientswith chronic obstructive pulmonary disease (COPD), because ithas been consistently shown that this relieves dyspnea and improveshealth-related quality of life (HRQL) (1). It is of note, however,that the physiologic mechanisms underlying the beneficial consequencesof training are poorly understood (1). In 1991, Casaburi andcolleagues (6) demonstrated that a relatively high-intensitytraining program was required to improve exercise endurance inpatients with moderate COPD. More recently, Maltais and coworkers(7, 8) reported that patients with COPD concurrently showedearly rise of blood lactate levels during exercise, together withlow concentration of skeletal muscle oxidative enzymes, as comparedwith normal subjects. The two findings were at least partiallycorrected after a controlled endurance training program (8).These two groups of investigators (6, 8) hypothesized thatreduction of blood lactate levels after training decreased ventilatoryrequirements during exercise, which in turn would relieve dyspneaand improve exercise tolerance. More recently, Casaburi and colleagues(9) reported that rigorous physical training in patients withsevere COPD, in whom blood lactate levels did not increase duringexercise, yielded a more efficient breathing pattern and reducedminute ventilation at a given submaximal work rate, hence improvingexercisetolerance.

An alternative hypothesis is that improvement of HRQL after endurance training is directly and mainly related to enhancementof skeletal muscle bioenergetics during submaximal exercise, ratherthan to changes in ventilation ( $V$ E). This notion may help toresolve the apparent discrepancies between the consistently beneficialeffects of physical training on HRQL (1) and the variabilityamong studies regarding the impact of rehabilitation on peak O₂uptake ( $V$ O₂ peak) (1). The present study examined the relationshipsamong oxygen consumption ( $V$ O₂), muscle O₂ transport, and cellularbioenergetics after an 8-wk endurance training program in 13 patientswith COPD and in eight healthy sedentary subjects used as controlsubjects.

	METHODS

TOP ABSTRACT INTRODUCTION METHODS RESULTS DISCUSSION REFERENCES

Study Group

Thirteen clinically stable male, steroid-free patients with COPD (mean age, 64 ± 4 [mean ± SD] yr; height, 167 ± 7 cm; andweight, 73 ± 8 kg) without recent history (6 mo) of an acute episodeof exacerbation, and eight healthy sedentary men (age, 61 ± 4yr; height, 170 ± 9 cm; and weight, 73 ± 7 kg) were enrolled inthe study. The patients with COPD were selected a priori becauseof their moderate-to-severe ventilatory impairment, but preservedsingle-breath carbon monoxide transfer capacity (DL_CO). All ofthem showed only moderate hypoxemia at rest without exercise-inducedoxyhemoglobin desaturation. Age, anthropometric variables, lungfunction measurements, therapy, and smoking habits of the twogroups are listed for each individual in Tables 1 and 2. Thecontrol group of sedentary subjects was carefully selected onthe basis of no previous history of regular or even occasionalphysical exercise above that required for average daily activities.In each subject, the same measurements described below were carriedout before and after the training period. All were informed ofany risks and discomfort associated with the experiment, and writteninformed consent was obtained in accordance with the Committeeon Investigations Involving Human Subjects at the Hospital Clínic,Universitat de Barcelona, which approved the study.

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TABLE 1

INDIVIDUAL ANTHROPOMETRIC DATA, HEMOGLOBIN CONCENTRATION, MEDICATION INTAKE, AND TOBACCO CONSUMPTION

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TABLE 2

PULMONARY FUNCTION AND PEAK EXERCISE DATA

³¹P-Magnetic Resonance Spectroscopy

In eight of the 13 patients with COPD and in all eight healthy sedentary subjects, ³¹P-magnetic resonance spectroscopy (³¹P-MRS) measurements in the quadriceps of the left thigh were carriedout less than 1 wk before the study with catheters as describedbelow. Exercise tests during MRS measurements were performed usingan ergometer made of nonmagnetic materials conceived to fit intoa standard whole-body magnet. The system allowed flexion and extensionof both legs by alternatively pressing two foot pedals connectedto a hydraulic-controlled resistance system while the subjectlay supine on the ergometer table (10). A piezoelectric forcetransducer (9251A model; Kistler Instruments AG, Winterthur, Switzerland)placed inside one of the pedals was used to provide an "on-line"measure of both strength and rate of pedaling during the exercisetest.

Each subject began with an incremental protocol that consisted of a maximum of five periods of 2-min of exercise each, pedalingat 60 rpm. The two first periods were set at 3 W · kg¹ muscle mass, with subsequent increases at 7, 9, and 11 W · kg¹ muscle mass. After a full 1-h recovery at rest, the subject performeda constant work rate exercise for 2 min. This second protocolwas designed to allow evaluation of [PCr] recovery from data collectedfor 8 min after exercise. The constant work rate used in eachsubject was chosen to produce a rise in [Pi]/[PCr] ratio of approximately1 ± 0.5 while keeping pHi higher than 6.90 units, as measuredin the first spectrum of the recovery period. The purpose wasto prevent a deleterious effect of low intracellular pH on therate of oxidative phosphorylation (11).

³¹P-MRS measurement details. Studies were carried out using a 1.5-T Signa System (Signa Advantage; General Electric MedicalSystems, Milwaukee, WI) operating at a frequency of 63.65 MHzand 25.86 MHz for the hydrogen-1 and the phosphorus-31 nucleus,respectively, connected to a SPARCStation 20 Workstation (SunMicrosystems, Mountain View, CA). Subjects were placed in themagnet in a supine position, head first, and the elliptical distributedcapacitance surface coil (14.5 cm × 6.5 cm), pretuned at the phosphorousresonant frequency, was positioned and fixed over the vastus medialismuscle of the left leg. Then the position of the surface coilwas checked with spin-echo T1-weighted images (10). Phosphorous-31spectra were obtained using 180° pulses as measured at the centerof the coil. A total of 1,024 data points were accumulated forthe measurements at rest, 12 scans for each work rate of the incrementalexercise, and blocks of eight scans were continuously recordedduring the 8-min recovery period form the constant work rateexercise.

Free induction decays were analyzed in the time domain with the magnetic resonance user interface software (14). All resonanceswere fitted to single lorentzian functions with the nonlinearleast-squares variable projection method (15, 16) and theestimated amplitudes of the time domain signals, which correspondto the area under each resonance in the frequency domain, andtheir chemical shifts were directly used for calculations. Theindividual half-time of phosphocreatine ([PCr]) recovery was calculatedby fitting the time domain amplitudes to a monoexponential function(Figure P; Biosoft, Cambridge, UK). The intracellular pH (pHi)was calculated using the formula: pHi = 6.75 + log [(d $-$ 3.27)/(5.69 $-$ d)], where di is the chemical shift distance in ppm betweenthe Pi and the PCr resonances (17).

Whole-body and One-leg O₂ Uptake Measurements

Subject preparation, safety precautions, and technical aspects of the central measurements (arterial and femoral venous bloodgases and femoral venous blood flow) have been described in detailelsewhere (18). Briefly, one catheter was placed in the radialartery of the nondominant arm to measure PO₂, PCO₂, pH, Sa_O₂,lactate, and hemoglobin in arterial blood. In the femoral veinof the left leg, a 7-F catheter was advanced 7 cm into the vesselwith the tip oriented distally and a 2.5-F thermistor was advanced5 cm proximally into the same vessel. Each subject performed anincremental cycle exercise test (10-watt [W] increments every2 min in patients with COPD and 20-W increments every 2 min inhealthy sedentary control subjects, without an initial periodcycling at zero watts) breathing room air (FI_O₂ = 0.21) untilexhaustion. The exercise protocol was done using an electromagnetically-brakedcyclo ergometer (CardiO₂ cycle; Medical Graphics Corporation,St. Paul, MN) with a mechanical assist to overcome the internalfrictionalresistances.

On-line calculations of whole-body $V$ O₂, CO₂ output ( $V$ CO₂), minute ventilation ( $V$ E), respiratory exchange ratio (RER), heartrate (HR), and respiratory rate (RR) were averaged sequentiallyover 15-s intervals and displayed on a screen monitor to observethe progress of the tests. In each subject, simultaneous arterialand femoral venous blood samples were collected at rest and duringthe second minute of each incremental work rate. Femoral venousblood flow measurements were made by short-term steady-state thermodilutionusing iced saline (18, 19) immediately after femoral venousblood sampling. In each instance, the following measurements weremade: (1) PO₂, PCO₂, pH (IL model 1302, pH/blood gas analyzerand tonometer model 237; Instrumentation Laboratories, Milan,Italy), oxyhemoglobin saturation, hemoglobin concentration (Hb)(IL 482 co-oximeter), and whole-blood lactate concentrations (YSI23L blood lactate analyzer; Yellow Springs Instruments, YellowSprings, OH) from simultaneous arterial and femoral venous bloodsamples; and (2) femoral venous blood flow ( $Q$ _leg) and arterialpressure. As indicated above, $V$ E, fraction of expired oxygen(FE_O₂), fraction of expired carbon dioxide (FE_CO₂), and HR werecontinuously monitored. Technical aspects of these measurementshave been previously provided in detail (18). In the pre-trainingstudies of five of the 13 patients with COPD, femoral venous flowwas measured only at approximately 30, 60, 80, and 100% of peakwork rate (as assessed in a preliminary incremental exercise protocoldone in all subjects before inclusion in the study). Measurementsof leg blood flow at each work rate were done in all the remainingpre- and post-training studies of the two groups of subjects (patientswith COPD and controlsubjects).

In the present study, blood O₂ content was calculated as follows: [(1.39 · Hb · measured oxyhemoglobin saturation) + (0.003· PO₂)]. This was done for arterial (Ca_O₂) as well as venous (Cfv_O₂)blood. The O₂ delivery to the exercising leg ( $Q$ O_2leg) was calculatedas the product of arterial O₂ content and leg blood flow [ $Q$ O_2leg= Ca_O₂ · $Q$ _leg]. Leg O₂ uptake ( $V$ O_2leg) was obtained as the productof $Q$ _leg and the arterial $-$ femoral venous difference of O₂ content[ $V$ O_2leg = $Q$ _leg · (Ca_O₂ $-$ Cfv_O₂)]. Leg O₂ extraction ratio (O₂ER)was calculated as the ratio of the arterial to femoral venousO₂ content difference and the arterial O₂ content [O₂ER = 100· (Ca_O₂ $-$ Cfv_O₂)/Ca_O₂]. In each subject, measured O₂ saturationand the corresponding PO₂ from all samples were used to estimatethe oxygen half-saturation pressure (P₅₀) ofhemoglobin.

Training Program

The two groups of subjects (patients with COPD and control subjects) exercised on a cycle ergometer (Monark model 810; Monark,Sweden) 5 d per week for 8 wk. The training sessions were directlysupervised by one of the members of the team (J.N.). The complianceof the subjects was excellent, with no withdrawals during thetraining period. During the cycling sessions, HR was continuouslymonitored (SportTester PE 3000 System; Polar Electro, Kemple,Finland). The training sessions, approximately 60-min duration,consisted of (1) 5 min of cycling at the low work rate, 40% ofthe peak work rate (40% W_peak) achieved in the previous control;(2) 20 min cycling at the high work rate, 70-90% W_peak; (3) 5min cycling at 40% W_peak; (4) 20 min cycling at 70-90% W_peak;and (5) 5 min at 40% W_peak. The rate of pedaling during the sessionswas kept at 60 rpm. The progress of work rate during the trainingperiod was decided on an individual basis to maximize the trainingeffect. During the first 3 wk of the program, cycling at the highwork rate was set at least 70% W_peak. Thereafter, it was increasedat least by 5% every week up to a maximum of 90% of the actualW_peak during the last 2 wk of the trainingprogram.

Data Analysis

Results are expressed as mean ± SD. Comparisons of pre- and post-training incremental exercise within each group (13 patientsversus eight control subjects) were done, unless otherwise stated,using Student's paired t test to examine the slopes (and intercepts)derived from individual least-squares regression lines of eachvariable versus work rate and $V$ O₂ (both whole-body $V$ O₂ and $V$ O_2leg).Comparisons of peak exercise values between pre- and post-trainingwere analyzed similarly. The effects of training on femoral venouslactate concentrations ([La]fv) compared post-training to pre-trainingvalues by regression analysis. Comparisons of pre-training databetween patients with COPD and control subjects were done usingStudent's unpaired t test to examine the slopes (and intercepts)derived from individual results. Comparison of the profiles ofthe O₂ extraction ratio (O₂ER) response to exercise was carriedout using a repeated measurements analysis of variance (MANOVA).Since we found that the O₂ER profile was substantially differentbetween groups (p = 0.03), the analysis of the O₂ER response duringexercise was done for each group separately. Statistical significancewas set up at p value equal or lower than 0.05.

	RESULTS

TOP ABSTRACT INTRODUCTION METHODS RESULTS DISCUSSION REFERENCES

Lung Function and Exercise Tolerance before Training

The characteristics of the patients with COPD and the healthy sedentary control subjects are depicted in Tables 1 and 2.The 13 patients with COPD presented moderate to severe airflowobstruction (FEV₁, 1.4 ± 0.3 L, 43 ± 9% predicted) (22), slightsingle-breath DL_CO impairment (79 ± 17% predicted) (25), andonly moderate hypoxemia at rest (72 ± 8 mm Hg). Arterial PO₂ didnot show significant changes from rest to peak exercise (+8.4± 9.5 versus +10.2 ± 8.4 mm Hg, patients with COPD and controlsubjects, respectively). While arterial PCO₂ did not change (from35.7 ± 2.4 to 34.1 ± 2.8 mm Hg) during exercise in control subjects,Pa_CO₂ significantly increased at peak exercise in patients withCOPD (from 35.5 ± 2.9 to 40.8 ± 4.4 mm Hg) (p = 0.0001). ArterialO₂ content (Ca_O₂) was similar in the two groups both at rest (19.6± 1.1 versus 19.5 ± 1.3 ml O₂ · 100 ml¹ blood, patients with COPD and control subjects, respectively)and at peak exercise (19.7 ± 1 versus 19.6 ± 1.2 ml O₂ · 100 ml¹blood).

As expected, the patients with COPD showed exercise intolerance as assessed by both lower peak work rate (85 ± 26 versus 131± 41 W) (p = 0.005) and peak whole-body O₂ uptake (1.4 ± 0.3 versus1.9 ± 0.6 L · min¹) (p = 0.008) than control subjects. Peak O₂ uptake expressedas percent of predicted values was 69 ± 16% and 85 ± 16% (p =0.04), respectively. The patients with COPD in the present studyshowed, at a given submaximal work rate (40 W), significantlyhigher whole-body $V$ O₂ (p < 0.009) and $V$ O_2leg (p < 0.02) thanthe healthy sedentary control subjects with similar slopes ofO₂ uptake versus work rate relationships in the two groups forboth whole-body O₂ uptake (12 ± 3 versus 12 ± 1 ml · min¹ · W¹, respectively), as shown in Figure 1.

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Figure 1. One-leg O₂ uptake ( $V$ O_2leg) and whole-body O₂ uptake ( $V$ O₂) plotted against work rate. Healthy subjects are indicated by triangles (pre-training study, open symbols, and post-training study, filled symbols). Patients with COPD are indicated by squares (pre-training study, open symbols, and post-training study, filled symbols). Results are expressed as mean (± SEM) data obtained at rest (zero watts) and at approximately 30%, 60%, 80%, and 100% peak work rate. Training effects on exercise response in the control subjects were those expected from the literature (26). Peak whole-body $V$ O₂ and peak work rate significantly increased after training in the two groups of subjects. Post-training peak $V$ O_2leg significantly increased in healthy sedentary subjects, but not in patients with COPD. In the patients, at given submaximal work rate, both pre- and post-training $V$ O_2leg (and also whole-body $V$ O₂) were significantly higher than in the control subjects (see text for further explanations).

The ventilatory and heart rate responses to exercise in patients with COPD were similar to those reported in the literature(30). Peak ventilation was lower in patients with COPD thanin control subjects (45.6 ± 7.1 versus 70.9 ± 22.2 L · min¹, respectively) (p = 0.001), but peak respiratory rate was similar(34.9 ± 8.4 versus 33.3 ± 10 min¹). At a given submaximal work rate (40 W), $V$ E was higher in patientswith COPD than in control subjects (28.8 ± 7.4 versus 21.5 ± 4.4L · min¹) (p = 0.02). The response of VT to exercise was also differentbetween groups; while in the control group mean VT rose progressivelythroughout exercise, the patients with COPD showed a well-definedplateau in VT above approximately 60 W. Mean peak heart rateswere not different between groups (133 ± 20 versus 145 ± 15 min¹, patients with COPD and control subjects, respectively), butHR at a given submaximal work rate (40 W) was significantly higherin patients with COPD than in control subjects (107 ± 17 versus93 ± 10 min¹) (p = 0.05). The RER at peak exercise was also significantlylower in patients with COPD than in control subjects (1.02 ± 0.08versus 1.16 ± 0.09) (p = 0.002).

Training Response

Muscle O₂ transport and O₂ uptake. Peak $V$ O_2leg (Figure 1, upper panel ) significantly increased after training in the controlgroup (by 0.18 ± 0.11 L · min¹) (p = 0.002). The difference in peak $V$ O_2leg of the patientswith COPD (0.07 ± 0.2 L · min¹) was not significant (p = 0.2). In contrast, peak whole-body $V$ O₂ (Figure 1, bottom panel ) rose in both groups (by 0.15 ±0.25 and by 0.27 ± 0.20 L · min¹, patients with COPD and control subjects) (p = 0.05 and p = 0.005,respectively). Likewise, peak work rate significantly increasedwith training in both groups (by 15 ± 12 W and by 33 ± 10 W, patientswith COPD and control subjects, respectively) (p < 0.01 each).RER at peak exercise did not change after training in patientswith COPD (from 1.02 ± 0.08 to 1.00 ± 0.1), but it increased inthe control group (from 1.16 ± 0.09 to 1.21 ± 0.09) (p = 0.04).As depicted in Figure 1, the slope of post-training $V$ O₂ (bothwhole-body $V$ O₂ and $V$ O_2leg) versus work rate was not differentbetween patients with COPD and control subjects, and in the twogroups it essentially overlaid the pre-trainingdata.

For both subject groups, the plots of both post-training one-leg blood flow ( $Q$ _leg) and post-training one-leg O₂ delivery( $Q$ O_2leg) versus work rate (or O₂ uptake) essentially overlaidthe pre-training data, as shown for $Q$ O_2leg in Figure 2 (upperpanel ). The normal subjects showed a significant increase inthese two variables at peak exercise: peak $Q$ _leg increased by1.15 ± 1.19 L · min¹ (p = 0.03) and peak $Q$ O_2leg rose by 0.19 ± 0.23 L · min¹ (p = 0.05). However, no changes were observed in the patientswith COPD after training (Table 3). Both leg blood flow and legO₂ delivery at a given submaximal work rate were not significantlydifferent between patients with COPD and control subjects in eitherof the studies (pre- and post-training). The arterial minus femoralvenous blood O₂ content gradient at peak exercise did not showsignificant changes with training in patients with COPD (from13.7 ± 1.7 to 14.2 ± 1.2 ml O₂ · 100 ml¹ blood) nor in the control group (from 13.2 ± 1.4 to 13.8 ± 1.5ml O₂ · 100 ml¹ blood). Peak oxygen extraction ratio (O₂ER, %) increased in boththe patients with COPD (from 69.6 ± 8.3 to 74 ± 5.4%) (p = 0.02)and the control group (from 67.4 ± 6.0 to 73.7 ± 6.0%) (p = 0.05),but did not differ between groups. O₂ER during submaximal exercisewas significantly higher in patients with COPD than in controlsubjects (p = 0.03) both in the pre- and post-training (Figure2, bottom).

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Figure 2. One-leg oxygen transport variables (top panel, O₂ delivery, and bottom panel, O₂ extraction ratio) plotted against work rate. Healthy subjects are indicated by triangles (pre-training study, open symbols, and post-training study, filled symbols). Patients with COPD are indicated by squares (pre-training study, open symbols, and post-training study, filled symbols). Results are expressed as mean (± SEM) data obtained at rest (zero watts) and at approximately 30%, 60%, 80%, and 100% peak work rate. In healthy sedentary subjects, one-leg O₂ delivery at peak exercise was significantly higher than pre-training data, but not in patients with COPD. The two groups of subjects showed a significant rise in peak O₂ extraction ratio after training. O₂ extraction ratio showed higher values at moderate submaximal exercise in patients with COPD than in control subjects, both in the pre- and post-training studies (see text for further explanations).

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TABLE 3

TRAINING RESPONSE IN HEALTHY SUBJECTS AND PATIENTS WITH COPD

Figure 3 (upper panel ) shows that while the normal subjects moderately decreased $V$ E at a given submaximal work rate (40W) from 22 ± 4.4 to 18 ± 3.5 L · min¹ (p = 0.02) and substantially increased peak $V$ E from 71 ± 22.2to 89 ± 27.2 L · min¹ (p = 0.004), no significant effects of training on submaximal $V$ E nor in peak $V$ E were observed in patients with COPD (Table3). It is of note, however, that submaximal $V$ E after trainingshowed a trend to fall, by $-$ 1.9 L · min¹ (p = 0.07, one tail). Control subjects significantly increasedpost-training peak HR (from 145 ± 15 to 158 ± 13 cycles · min¹) (p = 0.03), a change not seen in patients with COPD (133 ± 19compared with 133 ± 20 cycles · min¹). The COPD group did, however, show a significant reduction ofHR at a given submaximal work rate (40 W), by 10 ± 12 min¹ (p = 0.01). Despite the substantial differences in FEV₁ betweenpatients with COPD and control subjects, physical training decreasedfemoral venous lactate concentrations ([La]fv) at any work ratein a similar magnitude in the two groups, as indicated in Figure3 (lower panel ) (p < 0.05, each). After training, however, whiledifferences in base excess between patients with COPD and controlsubjects disappeared, [La]fv levels were still higher in patientswith COPD than in control subjects (at 40 W, 1.9 ± 0.36 versus1.2 ± 0.28 mM · L¹, respectively) (p = 0.0001).

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Figure 3. Minute ventilation (upper panel ) and lactate levels in femoral venous blood ([La]fv) (bottom panel ) plotted against work rate. Healthy subjects are indicated by triangles (pre-training study, open symbols, and post-training study, filled symbols). Patients with COPD are indicated by squares (pre-training study, open symbols, and post-training study, filled symbols). Results are expressed as mean (± SEM) data obtained at rest (zero watts), and at approximately 30%, 60%, 80%, and 100% peak work rate. Ventilation at peak exercise increased after training in healthy sedentary subjects, but not in patients with COPD. The control subjects, but not the patients with COPD, also reduced post-training ventilation at a given submaximal exercise. The two groups, however, showed a similar fall in post-training (La)fv at a given submaximal exercise (see text for further explanations).

Skeletal muscle bioenergetics. Pre-training half-time of [PCr] recovery was significantly longer in the patients with COPD(50 ± 8 s) than in control subjects (35 ± 7 s) (p = 0.02). Aftertraining, half-time of [PCr] recovery substantially fell to normallevels in patients with COPD (34 ± 7 s) (p = 0.02), but this variabledid not show significant changes in the healthy sedentary subjects(29 ± 8 s). The analysis of changes in half-time recovery wasdone in only six control subjects, since two of them (subjectsno. 1 and 2) had to be excluded because pHi fell below 6.9 eitherin the pre- or post-training study. Endurance training improvedthe skeletal muscle bioenergetic status to normal levels in patientswith COPD during incremental exercise (Figure 4), as shown bythe lesser increase in the [Pi] to [PCr] ratio and the lesserreduction in pHi at a given submaximal exercise. For example,at 27 W the [Pi]/[PCr] ratio fell from 2.8 to 1.3 (p = 0.05) andthe pHi increased from 6.83 to 6.98 (p = 0.04). In contrast, thenormal sedentary subjects did not show significant changes inthe [Pi]/[PCr] ratio nor in pHi at this level of exercise. Itis of note, however, that the control group showed a trend towardimprovement of the bioenergetic status after training at the laststep of the exercise protocol (Figure 4).

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Figure 4. Inorganic phosphate ([Pi]) to phosphocreatine [PCr] ratio and intracellular pH (pHi) plotted against work rate. Healthy subjects are indicated by triangles (pre-training study, open symbols, and post-training study, filled symbols). Patients with COPD are indicated by squares (pre-training study, open symbols, and post-training study, filled symbols). The results, expressed as mean (± SEM), were obtained during the incremental protocol carried out within the magnet. Data at zero watts are measurements done at rest. The three subsequent points in each line correspond to submaximal work rates achieved by all the subjects. The last measurement corresponds to peak exercise in the patients with COPD but not in the control group. In patients with COPD post-training [Pi]/[PCr] ratio and pHi markedly improved up to normal levels. Healthy sedentary subjects were explored only at very low work rates relative to their peak exercise (see text for further explanation).

	DISCUSSION

TOP ABSTRACT INTRODUCTION METHODS RESULTS DISCUSSION REFERENCES

Nature of the Training Response

The present study shows that patients with COPD and healthy sedentary control subjects presented clear physiologic trainingeffects both at peak work rate and during submaximal exercise.After training, peak whole-body $V$ O₂ and peak work rate significantlyincreased in the COPD group (by 10% and 15%, respectively) (p< 0.01 each) and in the control group (by 13% and 20%) (p = 0.05and p < 0.01). Likewise, post-training [La]fv during submaximalexercise (at 40 W) fell by $-$ 32% (p = 0.03) in the patients withCOPD and by $-$ 26% (p = 0.05) in the healthy sedentary control group.The two groups, however, showed quite different physiologic adaptationsto endurance training (Table 3). Whereas the healthy subjectsmarkedly increased the central factors governing convective O₂transport at peak exercise: (1) femoral venous blood flow andheart rate; (2) ventilation; and (3) O₂ delivery, no changes inany of these variables at peak exercise were observed in the patientswith COPD (Figures 2 and 3, upper panels ). In fact, similaritiesof pre- and post-training ventilatory responses to exercise (aswell as the observed plateau in tidal volume above 60% peak workrate) in the patients with COPD support the notion that ventilatorycapacity was one of the factors (albeit not the only one) limitingpeak exercise in these patients. The lack of a significant reductionof post-training $V$ E during submaximal exercise (by $-$ 1.9 L · min¹) should be attributed to a type II error. It is of note thatpost-training heart rate during submaximal exercise (at 40 W)fell by 8% (p = 0.01) in the COPDgroup.

The most consistent effects of the training program in patients with COPD were: (1) a significant increase in peak O₂ extractionratio (also seen in the control group); (2) reduced half-timeof [PCr] recovery; and (3) improved cellular bioenergetics duringsubmaximal exercise ([Pi]/[PCr] ratio and pHi) (Figure 4). Overall,the post-training findings in patients with COPD indicate thatthe physiologic changes provoked by endurance training essentiallytook place at the level of the skeletal muscle during submaximalexercise. The increase in peak whole-body $V$ O₂ after trainingin the patients can be interpreted as the end-result of the skeletalmuscle changes alluded toabove.

The O₂ extraction ratio ( $V$ O₂/ $Q$ O₂), at any given work rate, can be analyzed as the ratio of peripheral to central componentsof O₂ transport (18, 31). While the denominator ( $Q$ O₂) includesonly central components of O₂ transport (leg blood flow and arterialO₂ concentration), the numerator ( $V$ O₂) can be expressed as areflection of peripheral O₂ transfer. According to the laws ofdiffusion, $V$ O₂ is the product of muscle capillary O₂ conductanceand the PO₂ difference between muscle capillaries and mitochondria.In the present study, since peak $Q$ O₂ did not change (patientswith COPD) or even increased (healthy sedentary control subjects)(Figure 2, bottom panel), the rise in peak %O₂ ER after trainingshould be interpreted as an improvement of the muscle O₂ transfer.There are three potential mechanisms to explain such an increasein peak %O₂ ER with training: (1) higher capillary-to-muscle fiberratio due to training-induced angiogenesis, which would effectivelyenlarge the area for O₂ transfer in the muscle microcirculation;(2) improved mitochondrial oxidative capacity, which might potentiallyincrease the O₂ transfer gradient between capillary and mitochondria;and (3) the combined effects of these two phenomena. Unfortunately,the analysis of structural changes provoked by training was beyondthe scope of the present study. In the patients with COPD, however,since the half-time of [PCr] recovery fell to normal levels aftertraining, it can be hypothesized that physical training significantlyimproved mitochondrial oxidative capacity, as suggested by previousstudies (8). The half-time of [PCr] recovery is an overallmarker of the dynamics of muscle bioenergetics. It is well accepted,however, that when this variable is measured after a low-intensityconstant work rate exercise preventing a marked fall in pHi wouldotherwise negatively interfere oxidative phosphorylation, thehalf-time of [PCr] recovery reflects skeletal muscle mitochondrialoxidative capacity (11- 13,32).

A fundamental outcome of the post-training study in patients with COPD is the improvement of cellular bioenergetics ([Pi]/[PCr]ratio and pHi) during submaximal exercise up to normal levels,despite the lack of improvement in convective O₂ transport ( $Q$ O₂)(Figure 2, upper panel ). The results of the present study suggestthat physical deconditioning plays a key role in the impairmentof skeletal muscle bioenergetics in patients with COPD. The prominenceof the training effects on cellular bioenergetics in the COPDgroup may not be representative of the average training responseusually seen in the clinical setting. Both the intensity of thecontrolled training program and the inclusion criteria of thepatients can be important factors in explaining ourresults.

It is well accepted that healthy sedentary subjects show clear training effects on both cellular metabolism and muscle O₂transport (33). The lack of improvement in the cellular bioenergeticstatus ([Pi]/[PCr] ratio and pHi) during submaximal incrementalexercise in our control group can be largely attributed to thedesign of the ³¹P-MRS study. The use of an identical incremental protocol forthe two groups of subjects had some advantages, but only allowedexploration of very low work rates relative to the expected peakexercise for the control group. Post-training improvement of cellularbioenergetics in the healthy sedentary subjects likely would havebeen shown by exploring further steps in the incremental protocolwithin the magnet. This was not, however, a central aim of thepresent study. Moreover, the absence of a significant fall inhalf-time of [PCr] recovery after training (from 35 to 28 s) innormal subjects can be most likely attributed to a type II errorsince only six subjects could be included in the finalanalysis.

O₂ Uptake at Early Submaximal Exercise

It is well accepted that patients with COPD show relationships between O₂ uptake and work rate within the normal range suchthat O₂ uptake for a given submaximal work rate in these patientsis similar to that seen in healthy sedentary subjects (30).It is of note, however, that in the present study the patientswith COPD showed, at a given submaximal work rate, significantlyhigher whole-body $V$ O₂ (p < 0.009) and $V$ O_2leg (p < 0.02) thanthe healthy sedentary control subjects (Figure 1) with no differencesin the slopes of O₂ uptake (whole body and leg) versus work ratebetween groups. We can reasonably assume the reliability of ourresults because whole-body $V$ O₂ and $V$ O_2leg are independent measurements,and similar differences between the two groups were obtained inthe pre- and post-training studies. Since the problem appearsin the transitional zone from rest to slight exercise withoutmeasurements obtained during unloaded (zero watts) cycling, itis difficult to provide a clean explanation for such a differencein O₂ uptake at early submaximal exercise. The design of the incrementalexercise protocol without the recommended 3-min unloaded exercise(34, 35) could be considered a weakness of the study, butto our understanding it does not constrain the interpretationof the beneficial effects of physical training in patients withCOPD, which, in fact, is the main outcome of the presentinvestigation.

In summary, the present study suggests that the sedentary lifestyle of these patients with COPD due to psychological and/orphysiologic factors provokes functional changes in the skeletalmuscle that can be partly or completely reversed by physical rehabilitation,as shown by the improvement of cellular bioenergetics in skeletalmuscles to normal levels. The results of the investigation stressthe importance of physical deconditioning in the skeletal muscledysfunction observed in patients with COPD. It can be hypothesizedthat such an enhancement of the cellular bioenergetic status afterphysical rehabilitation may contribute to the underlying physiologicbasis of the improved HRQL observed in most of the studies (1).Physiologic adaptations to physical training essentially takeplace at muscle level, and they do not necessarily have an appreciableimpact on the ventilatory response to incremental exercise. Ourresults support the notion that improvement of the bioenergeticstatus of the skeletal muscle during submaximal exercise shouldconstitute one of the crucial components of the expected goalsof physical training. The findings of the present study may beof help in better identifying outcome variables for physical rehabilitationprograms.

	Footnotes

Correspondence and requests for reprints should be addressed to Josep Roca, M.D., Servei de Pneumologia, Hospital Clínic, Villarroel 170, Barcelona 08036, Spain. E-mail: roca{at}medicina.ub.es

(Received in original form April 28, 1998 and in revised form November 16, 1998).

Ernest Sala, M.D., was a Research Fellow supported by the Hospital Clínic(1997).

Acknowledgments: The authors are grateful to Felip Burgos, Jaume Cardús, and all the technical staff of the Lung Function Laboratory for theirskillful support during the study; to Vicky Cabestany, Lola Núñez,and Conxi Gistau for their outstanding support in the trainingprogram; to Narcis Gusí for his advice in conducting the trainingprogram; and to Mirjam Hillenius for typing themanuscript.

Supported by grants FIS 94-1106 and 97-0794 from the Fondo de Investigaciones Sanitarias; ALFA ETIR 2.42 (8) from the EuropeanUnion (DG XII); Comissionat per a Universitats i Recerca de laGeneralitat de Catalunya (1997 SGR-0086); and HL-17731 from theNational Heart, Lung, and BloodInstitute.

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