Diagnostic sensitivity of 2-day cardiopulmonary exercise testing in Myalgic Encephalomyelitis/Chronic Fatigue Syndrome

ME/CFS is a chronic condition of unexplained onset, characterised by both physical and mental fatigue, muscle and joint pain, and increased levels of post-exertional malaise when compared with healthy individuals [1]. The prevalence of ME/CFS has been estimated at 0.8 to 3.3% of the population [2]. The condition represents a significant challenge to patients and healthcare providers given that many patients are unable to maintain their occupation and there is no widely accepted treatment [3].

In addition to the lack of an accepted treatment for ME/CFS, difficulties also exist with its diagnosis. Many studies have attempted to identify a single, objective bio-marker to aid with diagnosis (e.g. [4‐6]), however, to date, none has been identified. As a result, diagnosis has been performed on the basis of clinical criteria which aim to confirm a set of core symptoms and exclude other factors which might otherwise explain these symptoms. These clinical criteria have typically required the presence of fatigue exacerbated by exercise, sore throat, headaches, and unrefreshing sleep, among other symptoms [1, 3]. The 1994 Centre for Disease Control and Prevention (CDC) criteria [1] was the first widely accepted of these clinical criteria, and required patients to present with clinically evaluated, unexplained, persistent or relapsing fatigue persistent for 6 months. The fatigue reported by the patient must be: of new or definite onset; not the result of ongoing exertion; not substantially alleviated by rest; and results in substantial reduction in previous levels of occupational, educational social or personal activities. Additionally, the fatigue must be accompanied by four or more of the following symptoms: impaired short term memory or concentration; sore throat; tender cervical or axillary lymph nodes; muscle pain; multi-joint pain without arthritis; headaches of a new type, pattern, or severity; unrefreshing sleep; and post-exertional malaise lasting more than 24 h [1]. This clinical criteria was followed by the 2003 ‘Canadian Consensus Criteria’ [3] which required patients to meet the criteria for fatigue, post exertional malaise and/or fatigue, sleep dysfunction and pain, together with two or more neurological/cognitive manifestations and one or more symptoms from two of the categories of autonomic, neuroendocrine and immune manifestations, with the illness required to have persisted for at least 6 months [3]. The most recent widely used clinical criteria is the 2011 ‘International Consensus Criteria’ [7], which requires a number of pathological neurological impairments, immune/gastro-intestinal/genitourinary impairments, and energy metabolism/ion transport impairments, with an increased focus on the requirement for patients to demonstrate post-exertional malaise as a key feature of the condition [7] in an attempt to better differentiate ME/CFS from other similar conditions (e.g. fibromyalgia).

In line with the requirement by the 2011 International Consensus Criteria for patients to demonstrate post-exertional malaise, physiological differences between ME/CFS patients and healthy controls following physical exertion have been investigated [8, 9] as potential biomarkers of the condition. In particular, the effects of cardiopulmonary exercise tests (CPET) performed over 2 consecutive days (2-day CPET) have been evaluated in an attempt to identify post-exertional, fatigue-induced biomarkers that can discriminate between ME/CFS patients and controls [10‐13]. Multiple studies [8, 10, 11, 14] have identified that ME/CFS patients experience an earlier onset of VT on the 2nd day of the 2-day CPET protocol, a change that is not present in healthy controls. Although this earlier onset of VT may represent an objective biomarker of ME/CFS, results have been inconsistent in relation to the magnitude of change in the onset of VT (ranging from negligible [12], to large [8]). However, although requiring patients with ME/CFS to complete graded exercise tests to exhaustion on 2 consecutive days may exacerbate symptoms, and is therefore not ideal for assisting with the diagnosis of ME/CFS, due to the lack of reliable and objective biomarkers to aid in the diagnosis of ME/CFS, 2-day CPET represents an increasingly popular method for attempting to differentiate between patients and controls [13]. Indeed, ME/CFS management practices [13] and legal processes (e.g. insurance claims [15]) are being based on this reported phenomenon, despite the current research being limited to a small number of studies, indicating further confirmation of these findings is required.

Presently, despite the increasing use of 2-day CPET to differentiate between patients and controls, further evidence is needed to confirm the usefulness of this technique. Additionally, in previous studies no diagnostic cut-off values have been established for the change in the onset of VT which limits its validity in clinical practice. Establishing such values would allow for the confirmation of the ability for 2-day CPET to reliably differentiate between ME/CFS patients and healthy controls, and therefore potentially be useful for assisting with the diagnosis of ME/CFS. Accordingly, this study had two aims: (1) to determine if 2-day CPET is able to differentiate between ME/CFS patients and healthy controls, and (2) to establish cut-off values which can be used in differentiating between ME/CFS patients and healthy controls.

Participant physical characteristics are shown in Table 1. There were no differences in any physical characteristics between the ME/CFS patients and controls. ME/CFS patients had been diagnosed with the condition for 8.1 ± 4.7 years, with durations ranging from 2 to 18 years.

Ventilatory, subjective and HR parameters from the 2-day CPET are provided in Table 2. All participants met at least two of the three criteria required for determination of a valid maximal effort during exercise testing. ME/CFS patients reported higher scores than controls on the Chalder Fatigue Scale on Day 1 (p < 0.01), with a significant group × time interaction effect following Day 2, due to a greater increase in their scores compared with controls (p < 0.01). Significant effects of time for HR at VT (p = 0.03), WR at VT (p < 0.01) and RER at VT (p = 0.02) were also identified, with estimated marginal means indicating that all three parameters were lower on Day 2 irrespective of group. Significant group effects were found for RPE (p < 0.01), and RPE at VT (p < 0.01), with ME/CFS patients having higher values for both. Importantly, there was a significant group × time interaction for WR at VT (p < 0.01), with WR at VT decreasing by a greater extent from Day 1 to Day 2 for ME/CFS patients compared with healthy controls.

Receiver operator characteristic analysis of absolute and percentage changes in WR at VT (Fig. 1) showed an area under the curve of 87.8% for the absolute change (p < 0.01, standard error: 7.1%), and 89.4% for the percentage change (p < 0.01, standard error: 6.8%). Absolute change data revealed that greater absolute and percentage reductions in WR at VT occurred in patients with ME/CFS compared with controls, with thresholds for optimal sensitivity and specificity for distinguishing between ME/CFS and controls represented by an absolute difference in reduction in WR at VT of between 7.5 W (sensitivity = 75%, specificity = 90%) and 12.5 W (sensitivity = 50%, specificity = 100%). For percentage changes in WR at VT, sensitivity and specificity were optimal at differences in reductions of between − 6.3% (sensitivity = 87.5%, specificity 90%) and − 9.8% (sensitivity = 68.8%, specificity = 100%). For the percentage change in WR at VT, 12 out of the 16 patients experienced a decrease in this parameter of greater than 10%, while such a change was only observed in one control participant.

This study aimed to (1) determine if 2-day CPET is a useful method for differentiating between ME/CFS patients and healthy controls, and (2) establish cut-off values which can be used to aid in the diagnosis of ME/CFS. The main finding of the present study was that during the 2nd day of the 2-day CPET, WR at VT was decreased for ME/CFS patients, confirming previous findings that an earlier onset of VT during the presence of post-exertional malaise is a potential biomarker of ME/CFS [8, 10, 11]. The change in WR at VT was paired with larger self-reported increases in fatigue in ME/CFS patients compared with controls on Day 2, while there were no differences in peak WR or peak VO₂ from Day 1 to Day 2 for either patients or controls. ROC analysis identified that the decrease in WR at VT of 6.3–9.8% on the 2nd day of 2-day CPET may represent an objective biomarker of ME/CFS, with high sensitivity and specificity.

In the current study, there were no differences between patients and controls for RHR, SSHR, peak HR, peak V̇O₂ or peak WR, suggesting that the patients and controls were well matched for their general fitness levels. Previous literature has suggested that ME/CFS patients may be affected by significant deconditioning compared to healthy, sedentary individuals [24], or kinesiophobia [25, 26], which may impact on their ability to produce a maximal effort. However, given the similarities between the patients and controls for peak V̇O₂, SSHR, peak HR, and that all ME/CFS patients were able to produce a criteria-defined valid maximal effort, this does not appear to be the case in the current study. These findings are in agreement with the those of Sargent et al. [27] who reported no difference in V̇O₂ max between ME/CFS patients and controls when accepted criteria were applied to define the attainment of a maximal value. Importantly, the fact that ME/CFS patients produced the same WR and V̇O2 as controls on both days of testing implies that the change in any ventilatory or HR parameters as a result of the 2-day CPET were not due to a change in physical performance in the ME/CFS patients.

Receiver operator characteristic analysis performed on the change in WR at VT between Day 1 and Day 2 of testing revealed that an absolute decrease in WR at VT of 7.5–12.5 W or a percentage decrease of between − 6.3% and − 9.8% provided optimal specificity and sensitivity for differentiating between patients and controls. However, given the large variation in WR at VT for ME/CFS patients (ranging from 50 to 140 W in the current study), it is likely more appropriate to use the percentage, rather than absolute change in VT, as a method for differentiating between the two groups. It is important to acknowledge that CPET may exacerbate symptoms of post-exertional malaise and is therefore not an ideal method for determining the presence of ME/CFS, and markers that can be assessed under resting conditions would be preferable. However, while not ideal, evaluation of the change in WR at VT during 2-day CPET may be a valid and sensitive marker that can be used to aid in the diagnosis of ME/CFS. Based on the ROC analysis performed in the present study, we would propose that the more conservative measure of at least a 9.8% reduction in WR at VT be used for diagnosis, given this provided 100% specificity, indicating that a reduction of this magnitude is not likely to occur in a person who does not have ME/CFS.

Numerous previous studies have also found an earlier onset of VT in ME/CFS patients on the 2nd day of 2-day CPET. VanNess, Snell and Stevens [10] found a 30% reduction in V̇O2 at VT from the first to the 2nd day, while Keller, Pryor and Giloteaux [11] found a 15% decrease in V̇O₂ at VT and a 21% decrease in WR at VT, Snell et al. [8] found a 55% decrease in WR at VT and Hodges, Nielsen and Backen [14] found a 12% decrease in WR at VT for ME/CFS patients while controls experienced a 9% increase. While these results suggest that ME/CFS patients experience an earlier occurrence of VT on the 2nd day of 2-day CPET, the mechanism responsible for this effect is currently unknown. Potentially, the alterations in VT during the 2-day CPET may result from metabolic abnormalities. Metabolic abnormalities have been reported in skeletal muscle of ME/CFS patients related to impairment of oxygen delivery to skeletal muscle during exercise and inability to recover from exercise-induced reductions in pH [28‐30]. Derangement of pH homeostasis might have resulted in a more rapid decrease in blood pH during the 2nd day of exercise in the present study. This would in turn lead to an increased CO₂ production through buffering of H⁺ ions by carbonic anhydrase, leading to stimulation of chemoreceptors with a subsequent increase in ventilation. However, while some studies have reported derangement of pH homeostasis in patients with ME/CFS, others have found such abnormalities are present in less than 50% of patients [31, 32]. In the present study though, VT occurred earlier in all but one ME/CFS patients (i.e. in 15/16 patients). Keller et al. [11] found a decrease in maximal O₂ pulse during the 2nd day of their 2-day CPET, indicating a compromised oxygen delivery in ME/CFS patients in the presence of post-exertional malaise, while Vermeulen et al. [12] found a non-significant 5% decrease in the same parameter on the 2nd day of testing. A lack of O₂ delivery/uptake may lead to an earlier transition to anaerobic energy systems and therefore a more rapid increase in lactic acid production and reduction in pH. Future studies employing a 2-day maximal testing protocol in patients with ME/CFS should endeavour to measure lactic acid and pH. Interestingly, the change in WR at VT from Day 1 to Day 2 in the current study was smaller than that seen in previous studies which have assessed this parameter in ME/CFS patients [8, 10, 11]. This is likely due to a difference in the protocols used to elicit a maximal effort. In the current study all participants were given regular verbal encouragement to help elicit a valid maximal effort. Conversely, it was not explicitly stated if verbal encouragement was provided in two of the three pervious studies [10, 11], and it has been shown that frequent verbal encouragement results in higher peak WR’s and prolonged maximal exercise tolerance [18] than when no encouragement is provided. This potential lack of encouragement may have resulted in a premature cessation of exercise on Day 2 of the 2-day CPET in ME/CFS patients, resulting in a greater exacerbating in the change in WR at VT.

This study is limited by a possible selection bias as a result of the 2-day CPET protocol used within the study. Given the potential for symptom exacerbation as a result of the 2-day CPET, patients with severe ME/CFS may be less likely to volunteer, whereas patients with mild-moderate ME/CFS may be more likely. Anecdotally, none of the included participants classified themselves as a severe sufferer of the condition, and so the inclusion of patients with a more severe form of ME/CFS may have produced a different result. Future research should attempt to include sufferers with severe ME/CFS in the study design; however the authors acknowledge the potential for severe symptom exacerbation for these people and hence the clinical and ethical considerations. Additionally, ME/CFS patients exhibited a wide range of time periods since initial diagnosis (ranging from 2 to 18 years). This may have affected the results as patients who have been suffering from the condition for longer periods may experience increased levels of physical detraining that are common in ME/CFS patients compared to those who had been diagnosed more recently.

ME/CFS patients exhibit a decrease in WR at VT on the 2nd day of 2-day CPET, which was accompanied with increases in self-reported increases in fatigue that were not present in healthy controls. Importantly, the decreases in WR at VT was not accompanied by any change in performance on the maximal exercise test on Day 2 of testing (as demonstrated by unchanged peak HR and peak VO2), indicating that the change in WR at VT in ME/CFS may represent an objective biomarker of the condition, with a decrease in WR at VT of at least 9.8% providing the greatest specificity for distinguishing between ME/CFS patients and healthy controls. Future research should attempt to determine the mechanism for the earlier onset of VT in ME/CFS patients.