Iliac Artery Stenosis Clinical Trial
Official title:
A Non-invasive Exercise Test for Evaluating Sport-related Arterial Blood Flow Limitation in the Leg: an Exploratory Study (NIRS and Cycling Power in Patients With FLIA)
The research objectives of this project are to increase the understanding of pathophysiology and performance limitations related to sport-related flow limitation in the iliac artery (FLIA) using non-invasive measurement of muscle oxygenation at the working muscles of the leg and mechanical power output recorded during cycling exercise. Skeletal muscle oxygenation measured with Near-Infrared Spectroscopy (NIRS) is growing more accessible for use by coaches, teams, and individual athletes for use in performance testing. Describing how muscle oxygenation profiles in endurance athletes diagnosed with FLIA differ in comparison with healthy athletes may allow the use of this non-invasive, accessible measurement device for the screening of athletes at risk of developing FLIA. The relevance of this work is that FLIA imposes risk of irreversible injury to the main artery of the leg in endurance athletes, limiting their ability to participate in exercise, with further consequences for health, fitness, and quality of life. Currently, the early course of this progressive condition is poorly understood, as early detection is difficult and hence appropriate treatment is often delayed. If impairment becomes severe, often more invasive (and risky) treatment is necessary. Earlier detection and monitoring of FLIA may allow for improved patient management and outcomes. The design of this experiment will compare a patient group of trained cyclists diagnosed with FLIA, to healthy control subjects including cyclists of a similar fitness level without signs of FLIA. Both groups will perform an incremental ramp cycling test and an intermittent multi-stage cycling exercise test. Incremental ramp cycling testing is used as part of clinical diagnosis of FLIA, as well as performance (eg. VO2max) testing of healthy athletes. Multi-stage exercise protocols are also often used for performance testing of endurance athletes and allows for observation of (path)physiological responses during submaximal work stages. Outcome measures of muscle oxygenation kinetics with NIRS and cycling power will be analysed and compared between patients and healthy subjects.
Status | Not yet recruiting |
Enrollment | 60 |
Est. completion date | November 1, 2023 |
Est. primary completion date | May 1, 2023 |
Accepts healthy volunteers | Accepts Healthy Volunteers |
Gender | All |
Age group | 18 Years to 40 Years |
Eligibility | Inclusion Criteria: - Aged = 18 years and = 40 years - Trained cyclist or triathlete regularly training at least ~3/week for at least five years and identifying with a particular cycle-sport Exclusion Criteria: - Earlier vascular iliac surgery - Microvascular abnormalities (e.g. diabetes), - Vascular abnormalities outside of the iliac region, - Heart failure (New York Heart Association class >I), - Orthopedic/neurological entities potentially limiting exercise capacity, - Obesity. - Adipose tissue thickness > 7.5 mm These excluding conditions are considered as medical safety precautions to maximal exercise or as risk of unexpected pathophysiological effects confounding our primary outcome measures. It is known that a high level of adipose tissue thickness (ATT) influences the accuracy of NIRS measurement of underlying muscular tissue. A > 7.5 mm ATT cut-off point at the site of NIRS measurement determined with a skinfold caliper (Harpenden, Baty International West Sussex, UK) was chosen. The ATT is calculated as half the skinfold thickness. |
Country | Name | City | State |
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n/a |
Lead Sponsor | Collaborator |
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Maxima Medical Center |
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* Note: There are 26 references in all — Click here to view all references
Type | Measure | Description | Time frame | Safety issue |
---|---|---|---|---|
Primary | Power-deoxygenation (PD) profile | Power-deoxygenation (PD) profile: The ratio of power output to deoxygenation (eg. power/deoxy[heme]) as a proxy for the metabolic disturbance at the working muscle relative to the workload. | During cyclingtest day 1 | |
Primary | Near Infrared Spectroscopy (NIRS) deoxygenation parameters | Baseline: Average 60-second value before the start of exercise. min: the minimum 5-second mean value attained during exercise. max: the maximum 5-second mean value attained typically during the recovery after exercise.
?exercise amplitude: the difference between baseline and minimum values. |
During cyclingtest day 1 | |
Primary | Near Infrared Spectroscopy (NIRS) deoxygenation parameters | Baseline: Average 60-second value before the start of exercise. min: the minimum 5-second mean value attained during exercise. max: the maximum 5-second mean value attained typically during the recovery after exercise.
?exercise amplitude: the difference between baseline and minimum values. |
During cyclingtest day 2 | |
Primary | NIRS delta_recovery amplitude | The difference between minimum and maximum value. | During cyclingtest day 1 | |
Primary | NIRS delta_recovery amplitude | The difference between minimum and maximum value. | During cyclingtest day 2 | |
Primary | NIRS reoxygenation kinetics: tau | Time constant (tau, in seconds): the time constant parameter of a monoexponential curve fit to the reoxygenation profile after each work stage. | Immediately after exercise day 1 | |
Primary | NIRS reoxygenation kinetics: Time delay | Time delay (TD, in seconds): the delay before systematic rise in oxygenation after each work stage. | Immediately after exercise day 1 | |
Primary | NIRS reoxygenation kinetics: Mean Response Time | Mean response time (MRT, in seconds): the sum of TD and tau. | Immediately after exercise day 1 | |
Primary | NIRS reoxygenation kinetics: Half value time | Half value recovery time (HVT, in seconds): the time required to reoxygenate half of the total amplitude during recovery after each work stage. | Immediately after exercise day 1 | |
Primary | NIRS reoxygenation kinetics: Peak reoxygenation rate | Peak reoxygenation rate (SmO2/sec): a linear estimation of the peak resaturation slope, representing the magnitude of greatest mismatch between oxygen supply and utilization at the tissue during recovery kinetics, after each work stage. | Immediately after exercise day 1 | |
Primary | NIRS reoxygenation kinetics: Peak reoxygenation MRT | Peak reoxygenation MRT: an estimate of the time to occurrence of the peak reoxygenation rate, analogous to the MRT in a monoexponential curve, and representing the balance of recovery kinetics of oxygen supply and utilization in the tissue after each work stage. | Immediately after exercise day 1 | |
Primary | NIRS reoxygenation kinetics: tau | Time constant (tau, in seconds): the time constant parameter of a monoexponential curve fit to the reoxygenation profile after each work stage. | Immediately after exercise day 2 | |
Primary | NIRS reoxygenation kinetics: Time delay | Time delay (TD, in seconds): the delay before systematic rise in oxygenation after each work stage. | Immediately after exercise day 2 | |
Primary | NIRS reoxygenation kinetics: Mean response time | Mean response time (MRT, in seconds): the sum of TD and tau. | Immediately after exercise day 2 | |
Primary | NIRS reoxygenation kinetics: Half Value time | Half value recovery time (HVT, in seconds): the time required to reoxygenate half of the total amplitude during recovery after each work stage. | Immediately after exercise day 2 | |
Primary | NIRS reoxygenation kinetics: Peak reoxygenation rate | Peak reoxygenation rate (SmO2/sec): a linear estimation of the peak resaturation slope, representing the magnitude of greatest mismatch between oxygen supply and utilization at the tissue during recovery kinetics, after each work stage. | Immediately after exercise day 2 | |
Primary | NIRS reoxygenation kinetics: Peak reoxygenation MRT | Peak reoxygenation MRT: an estimate of the time to occurrence of the peak reoxygenation rate, analogous to the MRT in a monoexponential curve, and representing the balance of recovery kinetics of oxygen supply and utilization in the tissue after each work stage. | Immediately after exercise day 2 | |
Secondary | Recovery kinetics VO2/NIRS comparison | To describe skeletal muscle oxygenation kinetics vs pulmonary oxygen uptake kinetics in both healthy cyclists and patients with FLIA | After stages/maximal exercise. This is an offline analyses and therefore takes the time of the stage (1 minute for in between blocks; 5 minutes for maximal exercise) | |
Secondary | Vascular Occlusion Test - Reactive Hyperemia Area Under The Curve | Reactive Hyperemia area under the curve: the area of the NIRS signal (eg. SmO2·sec) will be calculated during the recovery from occlusion, as the total area under the curve and above the baseline value before cuff inflation during the first 4-minutes of recovery.
(This will be calculated from the same VOT for Outcome 1 |
Before cycling test day 1 | |
Secondary | Multiple reoxygenation kinetics - Primary Component Time constant tau | Primary component time constant (tau): the time constant parameter of a monoexponential curve fit to the rise in VO2 at the start of each work stage. | Between intervention day 1 (1-minute stages of block-protocol) and immediately after the intervention day 2 (ramp maximal test) | |
Secondary | Multiple reoxygenation kinetics - Cardiodynamic component time delay | Cardiodynamic component time delay (TD): the delay before systematic rise in VO2 at the start of each work stage. | Between intervention day 1 (1 minustages of block-protocol) and immediately after the intervention day 2 (ramp maximal test) | |
Secondary | Multiple reoxygenation kinetics - ?deoxy[heme] / ?VO2 onset kinetics | ?deoxy[heme] / ?VO2 onset kinetics: The oxygenation and VO2 curves will be normalized at the start of each work stage to a starting baseline and the eventual steady-state, as 0-100% of the response profile. The relative overshoot of ?deoxy[heme] vs ?VO2 can then be used to describe the matching of perfusive O2 delivery to O2 extraction. | During intervention day 1 (stages of block-protocol) | |
Secondary | Multiple reoxygenation kinetics - ?deoxy[heme] / ?VO2 recovery kinetics | ?deoxy[heme] / ?VO2 recovery kinetics: The same comparison of the response profiles of deoxy[heme] and VO2 will be performed during recovery after work stages. | Between intervention day 1 (stages of block-protocol) and immediately after the intervention day 2 (ramp maximal test) | |
Secondary | Vascular Occlusion Test (VOT): Microvascular Responsiveness | Microvascular Responsiveness (peak reoxygenation rate, eg. SmO2/sec): the linear slope of reoxygenation when the occlusion cuff is removed will be taken as the rate of reperfusion, representing microvascular responsiveness, a proxy for vasodilatory capacity and vascular function. | Before and after cycling test day 1 | |
Secondary | Vascular Occlusion Test (VOT): Reactive Hyperemia | Reactive Hyperemia area under the curve: the area of the NIRS signal (eg. SmO2·sec) will be calculated during the recovery from occlusion, as the total area under the curve and above the baseline value before cuff inflation during the first 4-minutes of recovery.
Calculated from same in VOT (Outcome 7) |
Before and after cycling test day 1 | |
Secondary | Clinical Assessment | Peak systolic velocity (PSV): Measurement of PSV at the external iliac artery with echo-Doppler ultrasound, before and after exercise, and with and without provocative maneuvers can be discriminative for FLIA. | During the same examination-appointment. The PSV will be measured following measurments of the arterial stiffness. This takes about 10 minutes for both sides. | |
Secondary | Clinical Assessment | Ankle brachial index (ABI): Blood pressures will be taken at bilateral ankles and from the arm both before and after exercise. The ratio of ankle and brachial pressures adjusted for height, and a bilateral difference can be discriminative for FLIA. | Immediately after maximal exercise day 1 | |
Secondary | Clinical Assessment | Ankle brachial index (ABI): Blood pressures will be taken at bilateral ankles and from the arm both before and after exercise. The ratio of ankle and brachial pressures adjusted for height, and a bilateral difference can be discriminative for FLIA. | Immediately after maximal exercise day 2 | |
Secondary | Clinical Assessment | Arterial stiffness with echo-Doppler: Arterial pulse wave velocities will be measured at the carotid and external iliac/femoral arteries with echo-Doppler ultrasound, before and after exercise. The velocity of propagation of the pulse wave is taken as an index of arterial stiffness. | Before exercise day 1, the arterial stiffness will be measured by the vascular technician. While this will be analyzed offline, this takes a few minutes. |
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