The pathophysiology of ‘happy’ hypoxemia in COVID-19

This review describes the pathophysiological abnormalities in COVID-19 that might explain the disconnect between the severity of hypoxemia and the relatively mild respiratory discomfort reported by the patients.

In early December 2019, the first cases of a pneumonia of unknown origin were identified in Wuhan, the capital of Hubei province in China. The pathogen responsible for coronavirus disease 2019 (COVID-19) has been identified as a novel member of the enveloped RNA betacoronavirus family and named severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), due to similarities with SARS-CoV and Middle East Respiratory Syndrome (MERS) viruses. Although much is known about the epidemiology and the clinical characteristics of COVID-19, little is known about its impact on lung pathophysiology. COVID-19 has a wide spectrum of clinical severity, data classifies cases as mild (81%), severe (14%), or critical (5%) [1‐3]. Many patients present with pronounced arterial hypoxemia yet without proportional signs of respiratory distress, they not even verbalize a sense of dyspnea [4‐8]. This phenomenon is referred as silent or ‘happy’ hypoxemia. Tobin et al. recently presented three cases of happy hypoxemia with P_aO₂ ranging between 36 and 45 mmHg in the absence of increased alveolar ventilation (P_aCO₂ ranging between 34 and 41 mmHg) [5]. In patients with COVID-19, the severity of hypoxemia is independently associated with in-hospital mortality and can be an important predictor that the patient is at risk of requiring admission to the intensive care unit (ICU) [9, 10]. Since correct recognition of hypoxemia has such an impact on prognosis and timely treatment decisions, we here offer an overview of the pathophysiological abnormalities in COVID-19 that might explain the disconnect between hypoxemia and patient sensation of dyspnea.

Breathing is centrally controlled by the respiratory center in the medulla oblongata and pons regions of the brainstem (see Fig. 1) that control the ‘respiratory drive’ to match respiration to the metabolic demands of the body [11, 12]. The main input affecting the respiratory drive is derived from chemical feedback among peripheral and central chemoreceptors. The center is, however, also influenced by higher brain cortex, hypothalamic integrative nociception, feedback from mechanostretch receptors in muscle and lung, and metabolic rate. The output of the respiratory center can be divided into rhythm- (e.g. respiratory rate) and pattern generating (e.g. depth of breathing effort) signals, and these outputs may be controlled independently [11, 13, 14]. Dyspnea is generally defined as a sensation of ‘uncomfortable, difficult, or labored’ breathing and occurs, in general, when the demand for ventilation is out of proportion to the patient’s ability to respond. It should be distinguished from tachypnea (rapid breathing) or hyperpnea (increased ventilation). Dyspnea grading relates to whether this feeling occurs in rest or upon exercise. This semi-quantitative approach of scoring is best exemplified by the frequently used modified Medical Research Council (MRC) dyspnea scale, which categorizes dyspnea from grade 0 (dyspnea only with strenuous exercise) to grade 4 (too dyspneic to leave house or breathless when dressing) in relation to subjects of the same age [15, 16].

Various sensory, pain and emotional stimuli affect the sensation of breathing via the cerebral cortex and hypothalamus [17, 18]. The abnormal sense of muscle effort is another contributor to dyspnea. Conscious awareness of the activation of respiratory muscles is absent in healthy breathing. However, when the respiratory muscles are fatigued or weakened due to altered lung mechanics (e.g. decreased thoracic compliance), breathing may be perceived as a substantial effort [12]. Dyspnea can also be caused by input from the mechanoreceptors in the respiratory tract and the chest wall. Stimulation of vagal irritant receptors (e.g. bronchoconstriction, breathing through an external resistance) appears to intensify dyspnea [12, 19, 20]. The contribution of metabolic rate in modulating sense of dyspnea in critically ill patients remains unclear, despite its well-established role during exercise [11, 21]. The best-known determinants of the respiratory drive are the central and peripheral chemoreceptors. Changes in partial gas pressure of dissolved carbon dioxide in the blood (PaCO₂) seem the most important component, causing shifts in pH at the level of both the peripheral and central chemoreceptors [11, 12, 22]. At steady state, the arterial PaCO₂ is determined by the following equation:

The normal response to hypercapnia (caused by increased V_D, hypoventilation or increased VCO₂) is an increase in respiratory drive and minute volume ventilation [23]. Hypoxemia itself rather plays a limited role in the sensation of breathlessness experienced by patients with cardiopulmonary disease on the opposite of hypercapnia that creates per se dyspnea [12, 24, 25]. In healthy subjects, the respiratory drive shifts minimally in mild hypoxemia (PaO₂ 60–65 mmHg), such as resulting from stays at high altitude or experimental hypoxic chambers [11, 26]. Many patients with dyspnea are not hypoxemic, while those who are, usually experience only a slight improvement in symptoms after hypoxemia is corrected with supplemental oxygen therapy [12]. When arterial P_aO₂ drops below 40 mmHg, dyspnea often occurs [12]. Of note, the normal response to hypoxemia is a rise in minute ventilation, primarily by increasing tidal volume and respiratory rate. Increased respiratory rate (tachypnea) and tidal volume (hyperpnea) - and not dyspnea - are therefore the most important clinical signs of impending hypoxemic respiratory failure [11, 27]. Furthermore, PaCO₂ serves as one of the fundamental regulators of cerebral blood flow. Hyperventilation causes decreased PaCO2 which subsequently leads to arterial vasoconstriction thus lowering cerebral blood flow and intracranial pressure. In contrary, increase in PaCO₂ leads to increased intracranial pressure ultimately leading to deteriorating level of consciousness, altered brainstem reflexes, and altered postural and motor responses [28, 29]. At the bedside, a profound understanding of the pathophysiological determinants of respiratory drive and hypoxemia may promote a more complete comprehension of a COVID-19 of a patient’s clinical presentation and timely management [11].

The disconnect between the severity of hypoxemia and the relatively mild respiratory discomfort reported by the COVID-19 patients contrasts with the experience of physicians usually treating critically ill patients in respiratory failure [30]. Guan reported dyspnea in only 18.7% of 1099 hospitalized COVID-19 patients, despite low PaO2/FiO2 ratios, abnormal CT scans (86%) and common requirement for supplemental oxygen (41%) [31]. Happy or silent hypoxemia is not exclusively seen in COVID-19, but may also occur in patients with atelectasis, intrapulmonary shunt (i.e. arterio-venous malformations) or right-to-left intracardiac shunt. The adequacy of gas exchange is primarily determined by the balance between pulmonary ventilation and capillary blood flow, referred as ventilation/perfusion (V/Q) matching [32]. In the initial phase of COVID-19, several mechanisms contribute to the development of arterial hypoxemia (see Fig. 2), without a concomitant increase in work of breathing. Rapid clinical deterioration may occur.

At the stage that COVID-19 patients are admitted to the hospital with hypoxemia, viral replication is well underway and in addition to giving antiviral medication, optimization of the V/Q mismatch and reduction of cytokine storm remain the major therapeutic goals. Regarding perfusion, avoiding microthrombi and ongoing fibrin deposition is one of the therapeutic strategies. It seems prudent to use thromboprophylaxis in all COVID-19 patients, particularly in those with high D-dimers on admission [59, 66, 74]. Moore et al. recently suggested the use of tissue plasminogen activator (tPA) to treat ARDS in COVID-19 [75]. In addition, tackling the systemic prothrombotic complication using anti-inflammatory medications (such as anti-IL6R tocilizumab or sarilumab, or the anti-IL6 antibody siltuximab or complement inhibiting strategies) to prevent macro- and microthrombi represents another potential approach and several trials are currently verifying this hypothesis [54]. Effective hypoxic pulmonary vasoconstriction may be another target to improve the matching of regional perfusion and ventilation in the lung. There is an excessive release of inflammatory mediators that disturbs the balance between nitric oxide (NO), endothelin, and prostanoids in the pulmonary capillaries [76], although inhaled NO has consistently failed to show an improvement in mortality in ARDS [53‐55, 84]. RAS modulation (e.g. angiotensin receptor blockers, recombinant soluble ACE2, and inhibition of the bradykinin system) may have a potential role in restoring lung perfusion regulation, and trials are ongoing [50‐52].

Regarding ventilation, supplemental oxygen is the first step in facilitating oxygenation. In patients with refractory hypoxemic respiratory failure (increasing shunt fraction), timely but not premature intubation and invasive ventilation support may be superior to non-invasive ventilation in boosting transpulmonary pressure, opening collapsed alveoli, improving oxygenation, decreasing oxygen debt, avoiding P-SILI and offering a better chance for the lungs to heal [61, 76, 77]. Considering the critical cases, most patients fulfil the Berlin criteria of ARDS, where lung-protective ventilation, prone ventilation, effective sedation and analgesia, and high positive end-expiratory pressure (PEEP) are key [54, 61, 70, 77]. COVID-19 patients are exquisitely PEEP sensitive [78‐80]. Tolerance for modest permissive hypercapnia minimizes ventilator-induced lung injury (VILI) [61]. Since prone position recruits the dorsal lung regions and diverts blood flow to these caudal regions, it may have particular importance in COVID-19 when used early and in relatively long sessions [42]. Although further trials are needed to evaluate the impact on disease severity and mortality, several authors confirmed that awake proning can improve oxygenation in COVID-19 [81‐83].

The remarkable dissociation between profound hypoxemic respiratory failure and a clinically ‘happy’ patient is frequently seen and should prompt physicians and health care workers not only to rely on the patient’s apparent wellbeing but closely monitor respiratory rate, signs of hyperventilation, oxygen saturation and invasive measurements of hypoxemia/hypocapnia at regular time intervals. Pulse oximetry should be interpreted with caution, because left-sided shifting of the oxyhemoglobin dissociation curve. The arterial hypoxemia is induced by intrapulmonary shunting, dysregulated hypoxic pulmonary vasoconstriction, impaired lung diffusion, and formation of intravascular microthrombi. As in the first days of the disease, the lung mechanics are well-preserved and there is no increased airway resistance or dead space ventilation. The respiratory center thus does not sense an uncomfortable sensation of breathing. However, sudden and rapid respiratory decompensation may occur, and tachypnea and hyperpnea might be the most important clinical warning signs of impending respiratory failure in COVID-19 patients.