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Mechanisms of exercise intolerance after COVID-19: new perspectives beyond physical deconditioning

Mecanismos de intolerância ao exercício após COVID-19: novas perspectivas além do descondicionamento físico

Eloara Vieira Machado Ferreira1, Rudolf K. F. Oliveira1

DOI: 10.36416/1806-3756/e20210406

The long-COVID-19 or post-COVID-19 syndrome is defined as the persistence of symptoms after four weeks of viral infection onset, in the absence of viral replication for 3 weeks.(1) Several studies have shown that approximately 60-70% of patients report persistence of symptoms for weeks to months after acute presentation. The primary symptoms include fatigue/muscle weakness, dyspnea, depression/anxiety, and sleep and cognitive disturbances. It remains unknown why several COVID-19 patients develop chronic symptoms following the acute event. Moreover, it seems that these chronic symptoms do not correlate well with the severity of the acute clinical presentation.(2,3) The main hypotheses to explain these findings relate to the viral toxicity itself, changes in the immune system, systemic inflammatory response, endothelial and microvascular injury and/or microthrombi, fibroblast proliferation due to diffuse alveolar damage, in addition to mechanical stretch from ventilation, medications (corticosteroids, neuromuscular blockers, etc.), prolonged hospitalization with immobility, and post-traumatic stress syndrome.
 
Considering this scenario, it would be expected, from a pathophysiological standpoint, that those patients would demonstrate reduced exercise tolerance with decreased aerobic capacity. However, according to the literature, few studies have investigated the role of cardiopulmonary exercise testing (CPET) in COVID-19 (Table 1). Based on those studies, it has been suggested that exercise intolerance could result from physical deconditioning. (4-6) But what is physical deconditioning? In the medical dictionary, it is defined as the “loss of physical fitness due to the inability to maintain an optimal level of physical activity or training. Inactivity for any reason can lead to deconditioning.” Regarding CPET findings, physical deconditioning can be described as the reduction of peak VO2 with or without slight tachycardia in the absence of known central and peripheral cardiocirculatory diseases. The presence of an early lactate threshold, for example, is only found in individuals without central cardiocirculatory diseases who are extremely sedentary and with high muscle impairment due to inactivity, as is the case of patients with debilitating chronic diseases.

 
In terms of the evaluation of exercise intolerance mechanisms by CPET, it is important to define whether the effort limitation is due to a central or peripheral cardiocirculatory origin and whether there is a ventilatory or gas exchange limitation alone or associated. Exercise limitations of central cardiocirculatory origin, for example, can occur even in the presence of normal cardiac exams at rest and can be related to low O2 delivery. Considering the hypothetical presence of myocarditis and endothelial/pulmonary microvascular lesions in the acute phase of COVID-19 infection, the exercise limitation in the post-COVID-19 syndrome related to central cardiovascular origin could be due to chronic inflammatory myocardial lesions - the prevalence of clinical and subclinical myocarditis in college athletes was 2.3% by cardiac MRI and may be one of the reasons for reduced performance in this population(7) - or pulmonary microvascular lesions. Pulmonary vascular disease, detected exclusively under physical stress, is also called exercise pulmonary hypertension’. In addition to cardiac pump impairment, the delivery of O2 could also be compromised by reduced O2 transport due to anemia, especially after discharge.(8)
 
From the peripheral standpoint, exercise intolerance may be due to impaired peripheral O2 utilization or reduced peripheral O2 extraction due to mitochondrial injury, with a consequent negative impact on energy production during cellular respiration for ATP formation. In keeping with this, Baratto et al.(8) demonstrated that post-COVID-19 patients at hospital discharge had a higher cardiac output (CO) at rest, lower arterial O2 content (reduced convective O2 transport), and a lower arteriovenous O2 difference compared to healthy controls, but with similar O2 extraction. During exercise, despite the higher CO, post-COVID-19 patients had lower muscle O2 extraction in the absence of increased pulmonary artery pressure and pulmonary vascular resistance, justifying the lower peak VO2.(8) When evaluating patients with persistent symptoms after COVID-19 infection, Singh et al.(3) elegantly demonstrated, through invasive CPET, that O2 delivery was normal and associated with reduced peripheral O2 extraction and elevated mixed venous O2 saturation compared to controls, resulting in reduced peak VO2, indicating lower diffusive O2 delivery to the mitochondria.(3) In their study, none of the patients presented central cardiocirculatory limitations. Corroborating with peripheral muscle impairment due to mitochondrial cellular respiration dysfunction, and not to peripheral muscle deconditioning, a recent case report with muscle biopsy performed after 3 weeks of mild COVID-19 infection evidenced a reduced actin:myosin ratio with loss of myosin filaments, thus confirming the presence of primary myopathy by COVID-19 as a cause of chronic fatigue.(9) These findings open a new perspective that suggests that myopathy due to viral injury might be responsible for the persistence of fatigue in long-COVID-19. Similarly, it is hypothesized that these patients may develop post-viral myalgic encephalomyelitis/chronic fatigue syndrome with possible associated small-fiber neuropathy, as previously described in other viral infections, or damage to olfactory sensory neurons, causing reduced cerebrospinal fluid flow, with congestion of the glymphatic system and subsequent toxic accumulation in the central nervous system.(10,11)
 
Reduced peak VO2 has not been the only finding described in post-COVID-19 syndrome. Some studies have reported mild hyperventilation due to an increase in the minute ventilation to carbon dioxide output ratio (V’E/V’CO2) during exercise, which could be justified by an increase in central chemosensitivity(3) or by dysfunctional breathing,(5,6) which would reduce the arterial CO2 pressure by increasing the ventilatory drive. It is noteworthy, however, that systemic stimuli of ventilation, such as activation of metabo- and mechanoreceptors during exercise, present in the peripheral muscles, can also justify the increase in V’E/V’CO2 in the absence of pulmonary and cardiac sequelae.(3) Another possible cause for ventilatory inefficiency would be the increase in dead space as a fraction of tidal volume (VD/VT), which may be present in patients with endothelial and/or microvascular injury, poor alveoli perfusion, and/or destruction of the pulmonary vascular bed in fibrotic areas, associated with reduced O2 diffusion through the blood-alveolar barrier.(3,8) This hypothesis would be plausible to justify, for example, the hypothetical presence of exercise pulmonary hypertension (not confirmed so far in the literature).(3,8) The VD/VT could also be elevated as a consequence of the reduction in VT during exercise due to the persistence of interstitial pulmonary fibrosis with consequent changes in ventilatory mechanics and ventilatory limitation, with possible associations with the extent of acute interstitial pulmonary involvement. (12) Finally, the presence of effort-induced hypoxemia could reduce muscle O2 delivery, causing limitations in gas exchange.(5)
 
Thus, considering the current pathophysiological knowledge of intolerance mechanisms and the range of systemic manifestations of the acute phase of COVID-19 infection, it would be simplistic for us to consider that all chronic symptoms of the long-COVID-19 syndrome are due to physical deconditioning by inactivity or prolonged hospitalization. The physical deconditioning theory does not explain the presence of persistent symptoms in patients who were affected by mild forms of the disease, many of whom did not even require hospitalization. Similarly, this theory does not explain the dissociation between the severity of hospitalization and the reduction in peak VO2 reported so far, nor does it explain the antagonism of the persistence of symptoms in patients with preserved peak VO2. (4-6) In light of the potential complexity and the lack of knowledge on the post-COVID-19 syndrome, it is unacceptable to be simplistic when attempting to unravel the post-COVID-19 syndrome exercise intolerance mechanisms. More robust scientific evidence is needed before drawing simple conclusions.
 
AUTHOR CONTRIBUTIONS
 
EVMF and RKFO: preparation, writing, and revision of the manuscript.
 
REFERENCES
 
1.            Nalbandian A, Sehgal K, Gupta A, et al. Post-acute COVID-19 syndrome. Nature Medicine 2021; 27: 601-615. https://doi.org/10.1038/s41591-021-01283-z.
2.            Rinaldo RF, Mondoni M, Parazzini EM, et al. Severity does not impact on exercise capacity in COVID-19 survivors. Respiratory Medicine 2021;187:106577. https://doi.org/10.1016/j.rmed.2021.106577.
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7.            Daniels CJ, Rajpal S, Greenshields JT, et al. Prevalence of Clinical and Subclinical Myocarditis in Competitive Athletes With Recent SARS-CoV-2 Infection Results From the Big Ten COVID-19 Cardiac Registry. JAMA Cardiol. 2021;6(9):1078-1087. https://doi.org/10.1001/jamacardio.2021.2065.
8.            Baratto C, Caravita S, Faini A, et al. Impact of COVID-19 on exercise pathophysiology: a combined cardiopulmonary and echocardiographic exercise study. J Appl Physiol 2021; 130: 1470-1478. https://doi.org/10.1152/japplphysiol.00710.2020.
9.            Belén Rodriguez, S. Nansoz, D.R. Cameron et al. Is myopathy part of long-Covid? Clinical Neurophysiology 2021;132:1241-1242. https://doi.org/10.1016/j.clinph.2021.03.008.
10.          Wostyn, P. COVID-19 and chronic fatigue syndrome: Is the worst yet to come? Medical Hypotheses 2021; 146:110469. https://doi.org/10.1016/j.mehy.2020.110469.
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