Hypoxemia in COVID‐19; Comment on: “The neuroinvasive potential of SARS‐CoV2 may play a role in the respiratory failure of COVID‐19 patients”
Matteo Coen, Gilles Allali, Dan Adler, Jacques Serratrice
Abstract
We read with interest the communications by Li et al1, 2 and Chigr et al,3 suggesting that the severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) targets the brainstem and plays a role in coronavirus disease 2019 (COVID-19) respiratory failure. Here, we hypothesize that asymptomatic hypoxemia (silent hypoxemia) presented by COVID-19 patients with severe pneumonia is related to a dysfunction of cortical rather than of subcortical structures. Patients with COVID-19 seldom complain of dyspnea.4, 5 Breathing control is a complex phenomenon. Sensory afferent information arising from chemoreceptors (sensing pH, PaO2, and PaCO2), upper airways stretch receptors (sensing inflation or deflation of the lungs), and chest wall mechanoreceptors (sensing muscles tension and contraction) reach the nucleus tractus solitarius (NTS) in the medulla oblongata. The NTS is the main autonomic brain center involved in breathing control (master regulator); it processes and projects the afferent signals to higher cortical centers, such as the insula, and the sensory and motor cortices (integrated system). Dyspnea is the subjective experience of breathing discomfort. It results from complex mechanisms, especially from a mismatch between efferent motor commands from the central nervous system (CNS) to the respiratory system, and afferent sensory informations (eg, expected airflow, cage movements) from the respiratory system to the CNS.6 The insular cortex is essential for conscious experience of visceral perceptions elicited by interoceptive stimuli.7 Perception of labored breathing involves the activation of the insula, insular lesions are associated with blunted perception of dyspnea.8 SARS-CoV-2 is a β-coronavirus, like HCoV-OC43 and SARS-CoV, to which is structurally homologous. These viruses are potentially neuroinvasive2; hence, the neuroinvasive potential of SARS-CoV-2 is probable. The olfactory disturbances common of COVID-19 can be due to virus-induced neuronal damage in the olfactory bulb.9 Retrograde axonal transport can then enable propagation of SARS-CoV-2 toward the insula. Animal studies support this hypothesis: HCoV-OC43 and SARS-CoV can reach the CNS via the olfactory bulb and cause neuronal death10, 11; moreover, the spreading of SARS-CoV to cortical structures occurs more rapidly compared to brainstem. The virus could also entry the CNS via an hematogenous route, of which endotheliitis can be the backbone.12 To note, brain tissue highly express SARS-CoV-2 cell receptor, the angiotensin-converting enzyme 2.13 To conclude, we hypothesize that la belle indifference (ie, the beautiful indifference) about breathlessness of COVID-19 depends on propagation of SARS-CoV-2 from the nose to the cortical regions, and subsequent virus-induced dysfunction. Isolated brainstem involvement as the sole and unique center involved in COVID-19 respiratory failure seems unconvincing. Brainstem mechanisms (necessary and sufficient to produce ventilator command and adapt it to the needs of the body) seem unaffected, as suggested by a normal to low pCO2 levels even in critically ill patients.6, 14 Nevertheless, since brainstem conveys information to higher CNS structures involved in breathing control, its dysfunction can affect this integrated system and contribute to the respiratory symptoms (or their absence) of COVID-19 patients. Interestingly, peripheral afferents could also play a role: virus-induced C fibers dysfunction could contribute to the absence of dyspnea in COVID-19 pneumonia.5 La belle indifference is more than a wink to Charcot and Freud: recent studies support a role of the insula (among other cortical areas) in the unawareness described in functional disorders.15