Functional ACE2 deficiency leading to angiotensin imbalance in the pathophysiology of COVID-19.

SARS-CoV-2, the virus responsible for COVID-19, uses angiotensin converting enzyme 2 (ACE2) as its primary cell-surface receptor. ACE2 is a key enzyme in the counter-regulatory pathway of the broader renin-angiotensin system (RAS) that has been implicated in a broad array of human pathology. The RAS is composed of two competing pathways that work in opposition to each other: the "conventional" arm involving angiotensin converting enzyme (ACE) generating angiotensin-2 and the more recently identified ACE2 pathway that generates angiotensin (1-7). Following the original SARS pandemic, additional studies suggested that coronaviral binding to ACE2 resulted in downregulation of the membrane-bound enzyme. Given the similarities between the two viruses, many have posited a similar process with SARS-CoV-2. Proponents of this ACE2 deficiency model argue that downregulation of ACE2 limits its enzymatic function, thereby skewing the delicate balance between the two competing arms of the RAS. In this review we critically examine this model. The available data remain incomplete but are consistent with the possibility that the broad multisystem dysfunction of COVID-19 is due in large part to functional ACE2 deficiency leading to angiotensin imbalance with consequent immune dysregulation and endothelial cell dysfunction.

Introduction

In January 2020, the world first began to hear of a cluster of cases of adult respiratory distress syndrome (ARDS) in Wuhan, China, marking the beginning of the COVID-19 pandemic. Soon thereafter, scientists isolated the culprit, a novel coronavirus known as severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) and confirmed that it primarily uses the same cell receptor as severe acute respiratory syndrome coronavirus 1 (SARS-CoV-1): angiotensin converting enzyme 2 (ACE2) [1-3]. Since this discovery, there has been renewed interest in defining the role of ACE2 in normal physiology in attempts to elucidate its potential involvement in COVID-19 pathology. As a critical component of the ubiquitous renin-angiotensin system (RAS), ACE2 is primarily involved in maintaining homeostasis within an array of normal physiologic functions ([4-8]. Furthermore, it is directly involved in bradykinin metabolism and has numerous non-catalytic functions in the gut [4, 6, 9]. Following the SARS pandemic, studies primarily in animal models confirmed that SARS-CoV-1 binding to ACE2 led to downregulation of the membrane-bound enzyme [10-12]. Extrapolating from this experience, a growing number of authors have posited that SARS-CoV-2 also induces downregulation of this critical enzyme, creating a functional ACE2 deficiency [4, 13–15]. In this review we will dissect the merits of this hypothesis. As we will discuss, there is evidence to suggest initial upregulation of ACE2 in airway cells, likely triggered by interferon signaling [16-19]. At the same time, mounting evidence suggests that COVID-19 phenocopies a functionally ACE2 deficient state. Taken together, these seemingly incongruous statements raise the distinct possibility that ACE2 deficiency occurs later in the disease course thereby driving the second, inflammatory phase of COVID-19 [20].

Overview of the renin-angiotensin system

The RAS is complex and incompletely understood, comprising two “arms” with both tissue-level and systemic components [4-8]. Historically, our understanding of the RAS has been limited to the angiotensin converting enzyme (ACE)-mediated pathway and its involvement in the regulation of intravascular volume. However, over the past two decades, a second, counterregulatory arm mediated by ACE2 has come into focus [4-8]. Given these additional complexities, it is now believed that the RAS is involved in an array of human physiology extending beyond its role in the maintenance of intravascular volume and that dysfunction of this system contributes to human disease, potentially including COVID-19 [4–8, 13–15, 21, 22].

The traditional RAS pathway involves numerous key peptides and enzymes: angiotensinogen, angiotensin 1 (AT1), angiotensin 2 (AT2), renin, ACE, and aldosterone [6, 21] (Fig. 1). Angiotensinogen, an inactive precursor peptide, is cleaved by renin to form AT1, which in turn is processed by ACE to AT2. Angiotensin-2 can be converted to angiotensin-3 and -4, but AT2 is considered the active signaling effector of the pathway [6, 21]. AT2 performs its multiple physiologic roles via signaling through two receptors: angiotensin-2 receptor type 1 (AT1R) and angiotensin-2 receptor type 2 (AT2R) [6, 23, 24]. Of the two, activation of AT1R is better studied and thought to be the primary mediator of angiotensin-2’s diverse biological effects [23]. Indeed, it is via AT1R that AT2 regulates aldosterone release from the adrenal cortex in response to changes in volume status [25]. In addition to its crucial role in fluid balance, AT2 activation of AT1R can promote vasoconstriction, angiogenesis, thrombosis, inflammation, and fibrosis [4, 23]. Interestingly, activation of AT2R may oppose the vascular actions of AT1R in certain contexts, but our understanding of this pathway is incomplete [23, 24].

Fig. 1

An overview of the renin angiotensin system pathways

Chymase, an endopeptidase primarily derived from mast cells, has also been shown to drive AT2 production [6, 26]. This ACE-independent mechanism of angiotensin-2 generation likely plays an important role in certain pathologic processes [6, 26]. In fact, in animal models there is a high level of compartmentalization between chymase and ACE [26]. Accumulating evidence indicates that chymase is the major regulator of tissue angiotensin-2 levels; in ACE-deficient mice, AT2 levels in the heart, lung, and kidneys are preserved despite undetectable levels in the circulation [26-28].

Although portrayed as a centralized mediator of systemic physiologic parameters, the spatial organization of the RAS is nested, featuring activities at the systemic, tissue, and cellular levels [6, 26, 29, 30]. Moreover, its activities may be differentially regulated among various tissues or cell types. As such, its local components can act independently from the central pathway [4–8, 29, 30]. The latter point may be critical to any potential RAS involvement in COVID-19 as tissue angiotensin-2 levels can be significantly higher than systemic values within multiple organ systems [6, 26, 31, 32].

The critical components of the second arm of the RAS include ACE2, angiotensin (1–9) [AT(1–9)], and angiotensin (1–7) [AT(1–7)] [4–8, 33]. ACE2 is an ectoenzyme present in most human tissues that is primarily membrane-bound but may be cleaved by protease ADAM17 to produce soluble ACE2 (sACE2), a process ramped up in certain disease states [4, 33]. ACE2 catalyzes the alternative conversion of AT1 to AT(1–9) – which subsequently is converted to AT(1–7) by a non-ACE2 mediated process – and of AT2 directly to AT(1–7) [33]. AT(1–7) likely binds to Mas receptors (MasR), promoting vasodilatory, anti-inflammatory, and anti-fibrotic effects [4, 23, 33]. Consequently, activation of this arm is thought to oppose the activity of the conventional ACE/AT2 pathway.

Secondarily, ACE2 acts in a non-catalytic fashion in the gut and participates in the enzymatic regulation of bradykinin (BK) signaling, which itself has been implicated in COVID-19 pathophysiology [4, 6, 9, 34]. ACE2 catabolizes bradykinin’s active metabolite, des-Arg9-bradykinin, and thus ACE2 deficiency is expected to disinhibit bradykinin signaling [9]. A detailed analysis of BK’s distinct impact on COVID-19 is beyond the scope of this review; however, given its role in vasodilation, inflammation, and vascular permeability, it is plausible that bradykinin dysregulation contributes to the overall clinical picture of ACE2 deficiency [34]. Additionally, BK likely increases chymase activity, providing additional avenues for AT2 production [35].

Under normal circumstances it is thought that the two arms of the RAS are balanced such that that an increase in ACE and AT2 is countered by a coordinate increase in ACE2 and AT(1–7) in order to maintain the physiologic status quo [21, 33]. However, in certain disease states, an imbalance between the two arms arises, typically in the form of unopposed ACE/AT2 activity [21]. In fact, we propose, as have others, a bipartite model for the pathogenesis of COVID-19: following an initial phase of illness resulting from direct viral toxicity to target cells, the disease enters an inflammatory phase in which SARS-CoV-2 induces functional ACE2 deficiency. This effective loss of ACE2, in turn, leads to an imbalanced RAS with a skewed ratio of AT2 to AT(1–7) [4, 13–15]. It has been argued that this imbalance is a driver of COVID-19 pathology [13-15]. Moving forward, we will examine the evidence in support of this theory first by exploring how ACE2 deficiency itself manifests.

Angiotensin imbalance causes widespread deleterious effects

Regulation of angiotensin balance by the systemic and local RAS has been confirmed to play a role in optimal functioning of most organ systems [6]. Numerous studies antedating COVID-19 have explored the physiologic consequences of angiotensin imbalance. We will review these data in order to highlight the diverse, multi-system failure that broad ACE2 deficiency incites (Table 1).

Table 1

Overview of renin angiotensin system involvement by organ system

Biological System	ACE Pathway	ACE2 Pathway
Pulmonary/ARDS	Causes volume expansion, vasoconstriction, increased vascular permeability, cytokine production, apoptosis of alveolar and epithelial cells and fibro-proliferation	Opposes ACE/AT2 effects ACE2 deficiency: risk factor in animal models via unopposed AT2/ AT1R activity rhACE2 improves ARDS in animal models
Cardiovascular	Causes left ventricular hypertrophy and cardiac dysfunction directly due to increased vasoconstriction and volume expansion	Compensated ACE2 deficiency: no clear deficits ACE2 deficiency with superimposed insult: cardiac dysfunction in part due to almandine deficiency
Renal	Causes increased sodium-retention, vasoconstriction, oxidative stress, fibrosis, inflammation	Causes vasodilatation, natriuresis/diuresis, reduction in oxidative stress + inflammation ACE2 or Mas Receptor knockouts: impaired renal function, alleviated with rhACE2
Endocrine	Causes reduction in blood flow to islet cells, increased oxidative stress and fibrosis, dose dependent impairment of insulin secretion	Opposes ACE pathway ACE2 or Mas receptor knockouts: glucose intolerance Ob/Ob mice: rhACE2 improves hyperglycemia and beta-cell function
Neurological	Causes vasoconstriction, inflammation, fibrosis, and oxidative stress increasing risk for stroke AT1R knockout mice: reduced risk for stroke Administration of AT2 vaccine reduces risk of stroke in animal models	Opposes ACE pathway AT(1–7)/MasR binding: vasodilatory, anti-inflammatory, antioxidant and angiogenic AT(1–7) therapy: centrally administered can reduce infarct size in animal model
Gastrointestinal	High dose AT2 impairs jejunal sodium-water reabsorption in animal model ACEIs/ARBs: impair intestinal inflammation in rodent models	Involved in tryptophan transport in non-catalytic fashion, likely alters gut microbiome and may impact cardio-pulmonary physiology
Hematological	Promotes thrombus formation in animal models, may activate microvascular thrombi ACEIs/ARBs: likely reduce thrombotic risk AT2 impairs endothelial cell function via reduction in NO production and activation of inflammatory pathways	Reduces platelet activation via promotion of NO and prostacyclin release in platelets and endothelial cells Protects endothelial cell function via stimulation of eNOS promoting increased NO synthesis
Immune System	Activates global inflammatory response primarily via NFκB pathway Stimulates cytokine production but may suppress some T-cell activity Could be involved in NETosis via NADPH oxidase-dependent manner May alter B-cell immunity	Less well studied but thought to oppose AT2 pathway thereby dampening the inflammatory response

Lungs

Cytokine signaling increases local ACE production, which in turn promotes the pathologic processes underpinning many features of ARDS: enhanced vasoconstriction and vascular permeability, further cytokine production, apoptosis of alveolar epithelial cells, and fibroproliferation [36, 37]. Indeed, ACE polymorphisms that augment its enzymatic activity correlate with increased mortality in ARDS [22, 38]. By contrast, ACE2 deficiency in the setting of superimposed illness can exacerbate acute lung injury or ARDS in animal models secondary to a relative increase in AT2 activation of AT1R [10, 36, 39–41], while administration of recombinant ACE2 improves lung pathology [10, 40]. Bronchoalveolar lavage (BAL) fluid from rats with lipopolysaccharide (LPS)-induced ARDS likewise contains upregulated ACE at the expense of ACE2, while recombinant AT(1–7) and the AT1R antagonist losartan decrease lung inflammation [41].

Cardiovascular system

AT2 promotes left ventricular hypertrophy and myocardial dysfunction, while pharmacologic blockade of this pathway has become a cornerstone of the management of both ischemic heart disease and congestive heart failure [23, 42]. Additionally, AT2 is thought to upregulate ADAM17, inducing a shift from membrane-bound to soluble ACE2, plausibly explaining the strong correlation between circulating sACE2 and cardiovascular morbidity and mortality [4, 43, 44]. To wit, high sACE2 levels in patients with cardiovascular disease (CVD) likely reflect an increased baseline AT2 tone rather than an active pathologic role for sACE2 per se. Downstream off AT2, aldosterone also causes deleterious effects on the cardiovascular system as evidenced by the all-cause mortality benefit conferred by mineralocorticoid receptor antagonists in patients with heart failure with reduced ejection fraction [45, 46]. The ACE2 pathway likely serves in a counter-regulatory capacity [4, 22]. Data on ACE2 deficiency in compensated states are mixed [47, 48]. However, superimposed insults such as volume overload or AT2 infusion can trigger more overt cardiac dysfunction [47-49]. The effect of ACE2 on heart function may proceed in part through conversion of AT(1–7) to almandine, as loss of the almandine receptor (MrgD) in an animal model results in severe cardiomyopathy [50].

Excretory (renal) system

Perhaps the best-known function of AT2 is its regulation of intravascular volume via its effects on renal water and sodium handling [51, 52]. However, a broader spectrum of ACE activity is implicated in chronic kidney disease, including increased oxidative stress, fibrosis, and inflammation [51]. On the other hand, the ACE2 arm largely opposes these effects, resulting in vasodilation, natriuresis and diuresis, and reduced oxidative stress and inflammation [51, 52]. An altered balance of ACE/ACE2 may be an important driver of renal pathology [51-53]. For example, murine knockout of the genes encoding ACE2 or the Mas receptor promotes proteinuria and renal inflammation that is attenuated by treatment with recombinant human ACE2 (rhACE2) [54-56]. The loss of ACE2 potentiates activation of AT1R by AT2, in turn upregulating the oxidative stress response; increased production of cytokines leads to inflammation and breakdown or malfunction of the glomerular filtration barrier [56].

Endocrine system

AT2 infusion has been shown to reduce blood flow to pancreatic islet cells, thereby hindering first-phase glucose-stimulated insulin secretion [57, 58]. At higher doses, AT2 may reduce both basal and pulsatile insulin secretion in humans [59-61]. The negative effects of the ACE pathway on insulin production likely result from β-cell damage from increased oxidative stress and fibrosis as well as specific impairments in insulin synthesis and secretion [59, 61]. Congruently, Ace2 and MasR knockout mice are glucose intolerant, while treatment of diabetic ob/ob mice with rhACE2 improves hyperglycemia along with indices of β-cell number and function [62-64]. Additionally, treatment with angiotensin(1–7) enhances insulin secretion in diabetic rats through improvements in β-cell microperfusion [65].

Neurological system

Activation of the ACE arm increases risk of stroke, perhaps secondary to increased vasoconstriction, inflammation, fibrosis, and oxidative stress [66]. Knockout of AT1R or administration of an AT2 “vaccine” reduces stroke risk in mice while increased angiotensin-2 levels in mice, via genetic manipulation of the renin and angiotensinogen genes, increases stroke risk [66-69]. The ACE2/AT(1–7) arm is less well characterized but has been identified as a neuroprotective pathway [66, 70]. In rats, both ACE2 and angiotensin(1–7) are increased within 48 h of an ischemic stroke, and intracerebroventricular infusion of AT(1–7) or administration of an ACE2 activator can reduce infarct size [71, 72].

Gastrointestinal system

The small intestine hosts the body’s highest tissue concentration of both ACE and ACE2 [73]. High doses of exogenous AT2 administered enterally to rats impair jejunal sodium-water reabsorption – potentially explaining the increased risk of diarrhea in COVID-19 – while ACE inhibitors and angiotensin receptor blockers (ARBs) reduce intestinal inflammation in rodent models [73, 74]. The effects of ACE2 in the gut are less well recognized but it appears to act in a non-catalytic manner to regulate tryptophan transport and the expression of antimicrobial peptides [4, 7, 73]. It has been more broadly hypothesized that ACE2’s impact on cardiovascular and pulmonary physiology may also proceed in part through alteration of the gut microbiome [4, 7].

Hematologic

The RAS modulates cardiovascular risk beyond the myocardium through direct effects on the vasculature, principally with regard to endothelial cell function and regulation of thrombotic pathways. A detailed accounting of the molecular pathways involved in the effects of the RAS on endothelial cell function is beyond the scope of this review. Nonetheless, activation of the ACE pathway has been shown to promote endothelial cell dysfunction [75-79]. The hallmark of endothelial cell dysfunction is failure to promote vasodilation by vascular smooth muscle cells, for example due to insufficient generation of nitric oxide (NO) by endothelial NO synthase (eNOS) [80]. AT2 and AT(1–7) have been shown to participate in the regulation of this process, as endothelial cells express both AT2 and Mas receptors [78, 81]. Local AT2 may act in a paracrine or endocrine fashion to impair production of NO by endothelial cells [76-79]. In an animal model, increasing doses of AT2 stimulated interleukin 6 (IL-6) production and promoted vascular macrophage accumulation, both of which correlated with increasing degrees of endothelial cell dysfunction [75]. By contrast, the ACE2 pathway is felt to protect endothelial cell function [4, 81–83]. AT(1–7) activation of Mas receptors has been shown to stimulate eNOS [83]; the resulting increase in NO synthesis promotes vasodilation as well as anti-fibrotic and anti-inflammatory effects, thereby helping to preserve endothelial cell function. The second major role of the RAS in vascular biology is regulation of thrombotic pathways by AT2 and AT(1–7) [13, 84]. ARBs and ACE inhibitors may reduce thrombosis in an AT(1–7)-dependent manner via enhanced fibrinolysis and reduced platelet activation [84, 85]. AT2 infusion in hypertensive rats promotes thrombus formation, particularly within the microvasculature, in an AT1R-independent manner [86]. The anti-thrombotic effect of AT(1–7) likely proceeds via activation of MasR on platelets that increases NO release as well as endothelial cell release of NO and prostacyclin (PC) [84]. Increased local NO and PC release reduces platelet activation and promotes vasodilation [84].

Immune system

The renin-angiotensin system is intricately involved in both innate and adaptive immunity [4–6, 87–91]. This interaction is highly complex and incompletely understood. Nevertheless, it is important to note some salient points to better contextualize the importance of a balanced RAS for normal immune function. In general, upregulation of the systemic ACE pathway – via activation of NFκB, a key regulator of inflammatory cytokine gene expression – leads to a pro-inflammatory state, while ACE2 dampens this inflammatory response [4–6, 89, 90, 92]. In reality, the interaction between the RAS and immune function is far more complex. For instance, more recent data suggest that activation of AT1R in lymphocytes tempers the inflammatory response, perhaps in an effort to brake the global inflammation triggered by AT2 [88]. As such, it is plausible that a functional ACE2 deficiency could simultaneously upregulate a systemic inflammatory response while inhibiting certain aspects of T-cell function.

Evidence for ACE2 downregulation model

Clinical similarities between COVID-19 and ACE2 deficiency

COVID-19 results in broad organ system dysfunction [93, 94]. In its severe form, it leads to life-threatening ARDS and extra-pulmonary manifestations are common [93, 94]. Studies have confirmed an increased risk for cardiovascular dysfunction, acute kidney injury, stroke, exacerbation of pre-existing diabetes or development of new-onset hyperglycemia, gastrointestinal pathology, and thrombosis [93, 94]. Additionally, in an animal model, SARS-CoV-2 has been shown to cause endothelial cell dysfunction via reduction in pulmonary artery endothelial NO synthase activity [95] suggesting that endothelial cell dysfunction plays an important role in COVID-19 pathology [96, 97]. These derangements phenotypically recapitulate functional ACE2 deficiency, solidifying the mechanistic plausibility of this model.

The parallels between the dysregulated immune function that characterizes COVID-19 and ACE2 deficiency are particularly compelling. Dysregulated immunity in COVID-19 may take various forms: cytokine storm, leukopenia, propagation of neutrophil extracellular traps (“NETosis”), and aberrant B-cell function [93, 98–101]. Intriguingly, a dysregulated RAS can produce a similar immunologic fingerprint. For example, unopposed AT2, likely via its functional interaction with NFκB and subsequent upregulation of IL-6, could play an active role in “cytokine storm” [102, 103]. Extrapolating from our discussion above, AT2 may exert direct inhibitory effects on T-cell function – perhaps an explanation for the leukopenia seen in COVID-19 patients [88]. AT2’s ubiquitous activation of AT1R may also be linked to the development of NETosis in an NADPH oxidase-dependent manner [104, 105]. Lastly, the lymph nodes of a subset of COVID-19 patients exhibit loss of germinal centers, thereby impairing durable immunity [100]. Interestingly, expression of B-cell lymphoma 6 protein (BCL6), a well-known regulator of germinal center dynamics, can be suppressed by AT2 [106-108]. Overall, experimental data support a negative impact of functional ACE2 deficiency on both innate and adaptive immunity.

Mechanisms of SARS-CoV-1 and -2 infection

The close resemblance of the multisystem pathology of COVID-19 to the physiologic consequences of angiotensin imbalance described above suggests but does not prove that SARS-CoV-2 infection causes functional ACE2 deficiency. However, the closely related SARS-CoV-1, which also caused both pulmonary and diffuse extra-pulmonary complications [109, 110], has been shown to downregulate ACE2 [10-12]. SARS-CoV-2 does appear more infectious perhaps secondary to its use of three additional viral co-factors: neuropilin-1 (NRP-1), HDL scavenger receptor B1 (SR-B1), and CD147 [111-113]. Interestingly, AT2 has been linked to upregulation of these co-receptors [114-118]. If these findings are confirmed in COVID-19, it would suggest a pathologic feed-forward cycle in which the SARS-CoV-2-mediated decrease in ACE2 leads to a downstream proliferation of viral co-receptors. Despite this important difference between SARS-CoV-1 and SARS-CoV-2, the similar clinical characteristics of the two viral infections is compelling. It may speak to ACE2’s ubiquity and simply reflect direct viral toxicity to a variety of target cell types but alternatively, the data could support the loss of ACE2 function per se as a key driver of disease.

To understand how SARS-CoV-2 could induce a functional ACE2 deficiency, one must look to its site of cell entry at the plasma membrane. SARS-CoV-2 binding to ACE2 activates two important enzymes: ADAM17 and transmembrane protease serine 2 (TMPSSR-2), both of which cleave membrane-bound ACE2 (mACE2) but do so at distinct sites [119]. Cleavage of ACE2 by ADAM17 results either in internalization of ACE2 by endocytosis or release of soluble ACE2 (sACE2), which retains some catalytic activity, into the extracellular fluid [119]. By contrast, TMPSSR-2 cleavage of ACE2 leads only to ACE2 internalization and, presumably, loss of function [119]. The reduction in mACE2 activity likely sets the stage for an imbalance between the key RAS effector peptides, AT2 and AT(1–7). Relatively unopposed AT2 activity can propagate the angiotensin imbalance by promoting further downregulation of mACE2 through its activation of ADAM 17 [4, 120]. Although plasma ACE2 activity rises during COVID-19 and may remain increased for weeks [121], it is not clear that this increase represents the full catalytic potential of ACE2 due to the possible presence of circulating endogenous inhibitors [122]. Additionally, the loss of mACE2’s obligatory localization once solubilized prevents the enzyme from acting efficiently in the original tissue microenvironment where it may be needed most. Interestingly, SARS-CoV-2 may also co-opt rising sACE2 levels in service of cell entry by forming ternary complexes with sACE2 and vasopressin that can be internalized upon binding to AT1R and vasopressin receptors [123]. Formation of such viral-protein complexes may further attenuate sACE2 activity, thereby compounding functional ACE2 deficiency.

In summary, there is good evidence to support SARS-CoV-1 downregulation of ACE2 [10-12]. Until recently, direct evidence for ACE2 downregulation by SARS-CoV-2 was lacking, but a new study reports that its spike protein is able to induce downregulation of ACE2 in hamster lung tissue and in human pulmonary artery endothelial cells [95]. To the best of our knowledge, this is the only study directly demonstrating ACE2 downregulation by SARS-CoV-2. Nonetheless, given the similarities between SARS-CoV-1 and SARS-CoV-2, coupled with the strong mechanistic possibility of ADAM17- and TMPSSR-2-mediated ACE2 shedding, it is reasonable to suspect that ACE2 downregulation occurs in COVID-19. Furthermore, given that COVID-19 closely phenocopies SARS – a disease state in which ACE2 downregulation is established – ACE2 downregulation is likely an important aspect of COVID-19 pathology. Indeed, multiple other lines of evidence that we will review support the ACE2 downregulation model.

Epidemiologic data

Additional support for the ACE2 deficiency model may lie in a more detailed examination of high-risk patient populations. Numerous groups have been identified as at high risk for poor COVID-19 outcomes: male gender, older age, obesity, and pre-existing co-morbidities with heart disease, hypertension, diabetes, and possibly vitamin D deficiency [93, 124–127]. These high-risk groups for COVID-19 share at least one common factor: elevated baseline ACE pathway tone, which may arise from the increased prevalence of chronic inflammation in many of these groups [87, 128–132]. Unsurprisingly, modulation of this pathway with ACE inhibitors or ARBs is common practice in many of these patient cohorts. Less well known but equally compelling is the evidence for direct interaction of both testosterone and vitamin D with the ACE pathway [133-140]. Studies predating COVID-19 have shown that testosterone can potentiate AT2 activity, in part via modulation of the relative levels of each angiotensin receptor [133-136]. Additionally, vitamin D deficiency may adversely impact on the RAS. Calcitriol suppresses renin gene expression and potentiates the angiotensin(1–7) arm, and was shown to improve LPS-induced ARDS in rats through favorable changes in both RAS arms [137-140].

Our understanding of baseline ACE2 activity in these high-risk populations is far less extensive due to an overall paucity of data, inconsistent reporting of endpoints across studies (e.g., ACE2 levels vs. activity, soluble vs. membrane-bound ACE2, angiotensin-2 vs. angiotensin (1–7) levels), and the innate complexity of ACE2 regulation. ACE2 activity can vary by organ system within a single disease state, as well as within an individual organ system based on clinical status (e.g., compensated or decompensated heart failure) [141, 142]. Definitively characterizing baseline ACE2 status, therefore, is challenging; any discussion must be tissue specific and clearly delineate the endpoint(s) under evaluation. For example, in nasal epithelium, a critical site of SARS-CoV-2 entry, ACE2 gene expression increases with age [143]. Similarly, a recent study found ACE2 gene expression in airway epithelial cells higher in older male patients, even as its expression pattern varied in other organs and in women [144, 145]. Lastly, sACE2 levels are elevated in numerous high-risk groups [43, 44, 146].

By contrast, epidemiologically low-risk groups – primarily women and younger patients – benefit from lower baseline ACE activity. Children generally lack chronic comorbidities that could drive inflammation-based activation of the RAS [87]. Direct assessment of ACE2 levels are complicated for reasons aforementioned but ACE2 expression may be lower in multiple organ systems in younger patients [143, 145]. The lower risk of women is likely attributable to a high ratio of estrogen to testosterone. The effects of estrogen on the RAS are complex but on the whole, in contrast to testosterone, it tilts the balance toward angiontensin(1–7), both via attenuation of the ACE pathway and upregulation of the ACE2 pathway [135, 136, 147–149]. The ACE2 gene promoter contains numerous estrogen and androgen receptor binding motifs – the former outnumbering the latter – suggesting direct regulation of the ACE2 pathway by sex steroids [145]. If ACE2 levels are upregulated in women, it is important to note this would reflect a non-compensatory, or “primary”, increase, in stark contrast to high-risk patients. As such, according to this model, higher ACE2 levels may increase risk for initial infection in women but, as with children, a favorable initial ratio of AT2 to AT(1–7) would position them to fare better once infected.

In summary, the critical difference between high- and low-risk groups relates to baseline ACE tone and the nature of their baseline ACE2 status. High-risk groups start out with a relatively high basal ACE tone while low-risk groups do not. Characterizing differences in ACE2 status is more difficult but the dynamic relationship between the two arms of the RAS is far more important than a single snapshot of ACE2 levels. Increased levels of ACE2 in high-risk patients, if present, likely reflect a compensatory attempt to counter a tonically activated ACE pathway. These patients have little or no ACE2 “buffer”, and any loss of ACE2 translates immediately into excess AT2, setting the stage for a more severe disease course. By contrast, for patients at lower risk, relatively elevated levels of ACE2 are “primary” rather than compensatory as their basal ACE tone is relatively low. As such, these low-risk patients benefit from a built-in AT(1–7) “buffer” that helps to forestall the development of relative AT2 excess.

Clinical trial data

The compendium of COVID-19 therapeutic trials performed within the past year also hint at involvement of the RAS in COVID-19 pathology. Each of the following agents require further study to confirm their true impact on COVID-19, and each may have RAS-independent effects that could help explain the findings. It is intriguing, however, that they all interact with the RAS; collectively these studies add to the body of evidence favoring a skewed RAS as a cardinal feature of COVID-19 pathophysiology.

ACEI/ARB studies

The most obvious candidates for demonstration of perturbations of the RAS in the pathophysiology of COVID-19 are ACE inhibitors (ACEI) and angiotensin receptor blockers (ARB). Unsurprisingly, multiple such studies have been conducted [150-160] (Table 2). Unfortunately, the data are mixed and significantly confounded for numerous reasons: most are observational studies, medications have typically been stopped once patients are hospitalized, and most authors combine ACEI and ARB use without considering differences between these two medication classes. Nonetheless, the overwhelming consensus that has emerged is that ACEIs and ARBs are not contraindicated despite the potential for upregulation of ACE2. A large meta-analysis assessed 86 studies involving 459,755 patients and found no increased risk for infection or severe infection among hypertensive patients on ACEIs or ARBs [156]. In fact, there appears to be a possible survival benefit with their use (OR 0.75, 0.61–0.92). Additional, smaller studies have also hinted at improved outcomes, especially among subgroup analysis of hypertensive patients, but this finding has not been universal [151, 153–155, 159].

Table 2

A sample of studies assessing ACE Inhibitor and Angiotensin 2 Receptor Blocker use in Covid-19

Study	Study Design/Description	Summary
Morales, DR et al. Lancet Digital Health, [160]*	International cohort analysis Compared out-patient use of ACE inhibitor or ARBs vs other hypertensive medications in 1.3 million patients Four primary endpoints: COVID diagnosis; admission; admission with pneumonia; admission with pneumonia and ARDS, acute kidney injury or sepsis	No association with ACE inhibitor or ARB use and diagnosis Moderately reduced risk with ACE inhibitors vs ARBs when used in duel therapy No association with more severe disease
Semenzato, L et al. Hypertension, [159]	Prospective cohort study Followed nearly 2 million patients with uncomplicated HTN × 16 weeks, compared ACE inhibitor or ARB users to CCB users Primary endpoint: time to hospitalization Secondary endpoint: time to intubation or death	Lower risk of hospitalization with ACE inhibitors (OR 0.74, 0.65–0.83) and ARBs (OR 0.84, 0.76–0.93) Lower risk of intubation/death for ACE inhibitors (OR 0.66, 0.51–0.84) and ARBs (OR 0.79, 0.64–0.98) ACE inhibitors with lower risk of hospitalization and intubation/death vs ARBs
Lopes, RD et al. JAMA, [158]	Randomized control trial of 659 patients Continuation vs discontinuation of ACE inhibitors/ARBs in mild to moderate COVID-19 Primary endpoint: mean days alive out of hospital	No difference in mean days alive and out of hospital No statistically significant difference in mortality, cardiovascular mortality, or progression of disease
An, J et al. J Am Heart Assoc, [157]	Analyzed outpatient records of 824,650 patients with HTN Assessed risk of COVID diagnosis in patients on ACE inhibitor or ARBs vs patients taking another HTN medication	No overall association between ACE inhibitor or ARB use and COVID infection Reduced risk of infection in patients > 85 years old on ACE inhibitors
Lee, MMY et al. Eur Heart J Cardiovasc Pharmacother, [156]	Meta-analysis of 86 studies including 459,755 patients Assessed ACE inhibitor or ARB use on risk of infection, severe disease, and mortality	No increased risk of infection or severity of infection Mortality reduced in HTN group (OR 0.75, 0.61–0.92)
Ren, L et al. J Cardiol, [155]	Meta-analysis of 53 case–control or cohort studies with 2,100,587 subjects Primary endpoint: association with prior HTN meds and COVID severity	No association between prior ACE inhibitor/ARB use and risk and severity of COVID Mortality reduced in patients with HTN (OR 0.77, 0.66–0.91)
Salah, HM et al. J Cardiovasc Pharmacol Ther, [154]	Meta-analysis of 12 studies including 16,101 patients with HTN Compared ACE inhibitor/ARB users vs non-users Primary endpoint: mortality	Lower mortality rate among ACE inhibitor/ARB users (12.15% vs 14.56%, OR 0.70, 0.53–0.91)
Yokoyama, Y et al. Med Virol, [153]	Two meta-analyses First: three studies analyzing ACE inhibitor/ARB use and COVID positivity rates Second: 14 studies assessing in-hospital mortality rates in ACE inhibitor/ARB use vs non-use	No association with COVID-positivity rates No overall effect on mortality OR 0.88 (0.64–1.20) Significant mortality reduction in hypertensive patients OR 0.66 (0.49–0.89)
Flacco, ME et al. Heart, [152]	Meta-analysis of 10 cohort or case-controlled trials involving 9890 hypertensive patients Endpoint: risk of severe or lethal COVID in ACE inhibitor or ARB users vs non-users	No statistically significant difference in either endpoint ACE inhibitors: OR 0.9 (0.65–1.26) ARBs: OR 0.92 (0.75–1.12)
Mehra, MR et al. NEJM, [151]	Assessed 8,910 patient records Analyzed independent risk factors for mortality	ACE inhibitor use: reduced mortality (OR 0.33, 0.20–0.54) ARB use: trend towards higher mortality (OR 1.23, 0.87–1.74)
Mancia, G et al. NEJM, [150]	Case-controlled study 6272 patients with severe COVID matched to 30,759 controls	No statistically significant association between ACE inhibitor or ARB use and infection or risk of severe infection

* These studies are referenced in primary text with reference number included here in brackets (references [150–160])

The relatively modest results with ACEIs and ARBs do raise some fundamental questions regarding the ACE2 downregulation hypothesis. Confounding aside, a clear reduction in mortality might be expected if the hypothesis is correct, but several additional factors must be considered. For example, ACE inhibitors alone do not completely curtail AT2 production: studies predating COVID-19 have confirmed ACE-independent production of AT2, most notably by chymase derived from mast cells [6, 22, 26, 161]. Perhaps not coincidentally, mast cell activity is thought to be increased in COVID-19, providing a viable alternative source for ongoing AT2 production in the face of ACE inhibition [162]. Furthermore, ACE inhibitors impair the ACE-mediated breakdown of bradykinin, compounding the effect of ACE2 depletion. Increased levels of bradykinin may further activate chymase pathways to establish a vicious feed-forward cycle [35]. Given these alternative mechanisms, ACE inhibition may not be sufficient to reduce AT2 activity.

Similarly, the modest effect of ARB treatment may be due to several additional factors. For one, their use is known to cause a compensatory rise in AT2 which has been shown to induce microvascular thrombosis in an AT1R-independent fashion [86]. Although AT1R is blocked, AT2 can also be converted to angiotensin-3 and angiotensin-4 [163]. These peptide fragments, though not well studied, may cause harm not suppressible by AT1R blockade. For instance, it is thought that angiotensin-4 raises thrombotic risk by increasing plasminogen activator inhibitor-1 [163, 164]. Furthermore, the downstream effects of AT1R activation entail certain subtleties that would be lost with wholesale blockade by ARBs. These include, first, the possibility of differential activation by “biased agonists” that bind AT1R and oppose the actions of classical AT2/AT1R signaling [23]. Second, activation of AT1R in lymphocytes appears to attenuate their immune response, contrary to the generally pro-inflammatory theme of AT1R activation, as a check against runaway inflammation [88]. At the same time, buildup of AT2 in the setting of AT1R blockade would be expected to translate into an increase in AT2R signaling that would oppose some of the effects of AT2/ AT1R activation [23, 24]. Overall, the complex interplay between the various peptides and receptors of the conventional ACE pathway poses challenges in predicting a straightforward response to AT1R blockade in the context of ACE2 deficiency.

Glucocorticoids

One of the most important milestones in the development of effective COVID-19 treatment was the discovery that dexamethasone reduces mortality in patients receiving supplemental oxygen or ventilator assistance [165]. Dexamethasone’s main impact on COVID-19 may be through its known anti-inflammatory effect. However, glucocorticoids also have a strong, albeit complicated, relationship with the RAS (Table 3). Glucocorticoids appear to upregulate the ACE pathway in animal models by inducing synthesis of ACE, angiotensinogen, and AT1R in smooth muscle cells, and by potentiating AT2-mediated vasoconstriction [166-168]. On the other hand, steroids may impair ACE-independent AT2 production by diminishing mast cell numbers and activity [169]. Glucocorticoids are also thought to upregulate neprilysin, a key ACE2-independent mediator of AT1 to AT(1–7) conversion, and may downregulate bradykinin receptors; reduction in bradykinin-stimulated chymase activity is thereby expected to further curb AT2 production [170-173]. Dexamethasone also favorably affects mineralocorticoid receptor activity. By suppression of adrenocorticotropic hormone (ACTH), dexamethasone can profoundly reduce the high levels of endogenous cortisol expected in critical illness that can cross-stimulate the mineralocorticoid receptor. Finally, glucocorticoids have been shown to inhibit NFκB, which mediates many of the pro-inflammatory actions of AT2 [89, 102, 174]. Thus, dexamethasone’s beneficial effect in COVID-19 could speak to its impact on the RAS through multifactorial rebalancing ACE/AT2 and ACE2/AT(1–7).

Table 3

Medications with positive endpoints in COVID-19 and their potential association with RAS

Drug Therapy	Study Design + Findings	Proposed Association to RAS
Dexamethasone	Design: randomized open label trial of 6,425 patients Protocol: Randomized to dexamethasone 6 mg × 10 days vs standard of care Findings: 28-day mortality improved in patients receiving oxygen and/or mechanical ventilation	ACE Pathway: –Induces synthesis of ACE, AT1 and AT1R –Potentiates AT2 vasoconstriction –Suppresses AT2 induced inflammation (via effects on NFκB) ACE2 Pathway –Suppress non-ACE mediated AT2 production –Increase AT(1–7) levels via NEP mediated activation
Aspirin	Design: retrospective, observational cohort study involving 412 patients Protocol: 98 patients received ASA within 24-h of admission or 7-days prior Findings: reduction in risk for mechanical ventilation, ICU-admission, and in-hospital mortality	ACE Pathway: –Protects against AT2-induced end organ damage via inhibition of NFKB and promotion of NO release in endothelial cells –Downregulates AT1R
Statin	Design: retrospective study of 648 matched COVID-19 patients vs controls Findings: significant reduction in mortality in COVID-19 patients taking statins	ACE Pathway: –Decreases AT1R expression –Inhibits AT2 down-stream signaling –Impairs AT2 and aldosterone production ACE2 Pathway –Upregulates ACE2 and AT(1–7) pathway
Metformin	Design: retrospective study 25,326 patients at one tertiary center Findings: significant reduction in mortality in DM patients	ACE Pathway: –Inhibits AT1R expression –Antagonizes AT2 pathways
Recombinant ACE2	Design: case study Findings: 45-year-old woman with DM2 admitted with 7-days cough, weakness, myalgia, fever, dyspnea and 4-days GI symptoms. Course worsened requiring intubation. Hospital day 2 started rhACE2 bid × 7 days. Defervesced after first dose. AT(-1–7) levels rose, AT2 levels fell. Markers of endothelial cell function and inflammatory markers improved as did overall clinical picture	ACE Pathway: –Retains ACE2 catalytic function –Decreases AT2 levels ACE2 Pathway: –Increases AT(1–7) levels
C21	Design: double-blind RCT of 106 patients Protocol: COVID-19 patients with high CRP but not on mechanical ventilation, randomized to C21 × 7 days or standard of care Finding: at day 14, 90% reduction in need for supplemental O2 NOT YET PEER REVIEWED	ACE Pathway –Stimulates AT2R receptors –Opposes some activity of AT-2/ AT1R signaling ACE2 Pathway: –May act as functional equivalent of a partial ACE2 activator

Aspirin

A retrospective observational cohort study of 98 patients who received aspirin within 24 h of admission or 7 days prior to admission found a reduced risk of mechanical ventilation, ICU admission, and mortality relative to 314 controls [175]. This finding has not yet been validated by a prospective clinical trial. It is presumed that the principal mechanism is via aspirin’s well-established anti-platelet or anti-inflammatory effects. However, aspirin may also counteract some deleterious effects of AT2, potentially through inhibition of NFκB activation and preservation of endothelial cell function through promotion of nitric oxide release [176-179]. Additionally there is evidence that aspirin can down-regulate AT1R [180, 181].

Statins

A recent large retrospective study of COVID-19 patients analyzed 648 statin users vs controls and found a significant reduction in mortality [182]. Considerable data support a direct link between statins and downregulation of the ACE pathway suggesting that statins decrease AT2 receptor expression, inhibit AT2-induced downstream signaling, reduce AT2-mediated oxidative stress, and potentially impair AT2 and aldosterone production [183]. Furthermore statins might potentiate the ACE2/AT(1–7) pathway [184].

Metformin

The authors of a retrospective analysis of 25,326 subjects tested for COVID-19 at one tertiary care center found a significant reduction in mortality in patients treated for diabetes with metformin [185]. If this benefit is proven in larger, prospective, randomized studies, the mechanism will likely be multifactorial. However, in numerous animal models, metformin has been shown to down-regulate AT1R and antagonize AT2 pathways [186-188].

Recombinant ACE2

Treatment of COVID-19 in a patient requiring mechanical ventilation with recombinant soluble human ACE2 quickly raised AT(1–7) levels at the expense of AT2 [189]. Viral load fell by two orders of magnitude within two days of starting treatment, while markers of endothelial function and levels of pro-inflammatory cytokines – as well as the overall clinical picture – markedly improved. Recombinant ACE2 likely restores healthier angiotensin balance while simultaneously serving as a decoy receptor for SARS-CoV-2. Although sACE2 may enhance SARS-CoV-2 cell entry via AT1R in cultured cells, this rhACE2 trial suggests that it may not be as significant a pathway in humans [123]. It is difficult to parse out the specific impact of this treatment within the overall intensive care milieu and the variable natural history of the illness but the striking temporal effect of the treatment lends credence to the ACE2 deficiency model

AT2R agonist

A recent randomized clinical trial employing a “first in class” agonist of AT2R has demonstrated reduced oxygen requirements and trends toward reduced intubation and mortality, although the data are not yet peer reviewed [Tornling G et al., 2021]. Our understanding of the AT2R remains very incomplete though evidence suggests that activation of this receptor opposes some functions of AT2/AT1R signaling thereby paralleling increased ACE2 activity [23, 24].

Evidence against the ACE2 deficiency model?

While we have shown the growing evidence in support of the theory that ACE2 down-regulation by SARS-CoV-2 is a critical driver of COVID-19 pathology, there are lingering, important concerns about the accuracy of the model.

Is ACE2 downregulated by SARS-CoV-2?

Most of the support for downregulation in vivo are limited to studies of the isolated SARS-CoV-2 spike protein [95] or of SARS-CoV-1 infection in mice [10-12]. However, human – but not mouse – airway epithelial cells appear capable of upregulating ACE2 in response to the burst of interferon signaling expected to accompany SARS-CoV-2 infection [19]. Beyond interferon, in vitro work has even suggested direct enhancement of ACE2 catalytic activity by SARS-CoV-2 or its isolated spike protein, particularly with regard to the active metabolite of bradykinin [190, 191]. It is difficult to extrapolate these data to the in vivo situation, however, as one study was performed in a cell-free system using only soluble ACE2 [190], and a second study confirmed the spike protein did downregulate ACE2 in vivo [95]. These divergent findings highlight that viral potentiation of ACE2 activity and downregulation of ACE2 need not be mutually exclusive, a distinction necessarily lost in a cell-free system. Crucially, despite a general increase in ACE2 activity, its metabolism of AT2 was minimally affected by the presence of the virus or its spike protein. Finally, the spike protein of SARS-CoV-1 was also found to accelerate ACE2 activity despite its likely ability to trigger downregulation of membrane-bound ACE2 [190].

Clinical Studies

We have only scanty, mixed data on the status of the RAS in humans with COVID-19. In one study, BAL fluid from patients with COVID-19 contained increased ACE2 mRNA relative to controls while that of ACE was decreased [34]. However, no assessment was made of protein levels or activity of ACE2 versus ACE, nor of AT2 versus AT(1–7) levels. The increase in ACE2 mRNA may therefore have been a compensatory mechanism occurring in the setting of already established ACE and AT2 excess. Moreover, ongoing ACE-independent production of AT2 may play an important role in angiotensin balance within the ARDS microenvironment [22, 26, 161]. A second study of SARS-CoV-2-infected lung tissue found increased ACE2 expression at up to 48 h, while prior studies suggested immediate ACE2 downregulation by SARS-CoV-1 [12, 16]. As previously mentioned, this study is supported by additional data showing upregulation of ACE2 in lung epithelial cells upon infection [17, 18]. However, the relatively short observation window in these studies may not be generalizable to later changes in ACE2 levels. Based on the previously mentioned bipartite nature of COVID-19, an early interferon-induced upregulation of ACE2 in response to initial viral infection may later give way to virus-induced ACE2 downregulation as viral multiplication overwhelms the stimulatory effects of interferon. This proposition is particularly salient given the latency period of up to two weeks between initial infection and onset of severe disease [20].

A related challenge to the model arises from difficulties in evaluating RAS peptides in COVID-19. This challenge may be more problematic insofar as AT2 and AT(1–7) are the main downstream effectors of the two RAS arms; thus their relative levels would be expected to better reflect the prevailing RAS tone than would levels of their upstream converting enzymes. Surprisingly, few such studies exist, but the data available do not convincingly or consistently demonstrate AT2/AT(1–7) imbalance [192-196]. In an early study, the authors found elevated AT2 levels in COVID-19 patients that correlated with degree of illness [193]. However, the study only contained 12 subjects, the authors compared values to healthy controls and the findings have since been questioned due to concerns about methodology [193, 195]. Two subsequent studies found no evidence for increased AT2 levels but critically neither measured AT(1–7), thus preventing interpretation of angiotensin balance in this setting [194, 195]. Another, more recent paper cited reductions in renin, AT1, AT2, and AT(1–7) in COVID-19 patients relative to patients with other respiratory illnesses; in this study, the decrease in AT2 exceeded that of AT(1–7) [192]. However, it is important to interpret these data in view of their limitations: 50% of the COVID-19 patients did not qualify for inclusion and the heart rate of the control group was statistically greater [192]. The latter could indicate a more severe degree of illness in the control group, as alterations in volume status or evolving sepsis are expected to stimulate the ACE pathway. Different interpretations of the data are also possible when taking into account the significant gaps in our knowledge of this complex system. These include, for example, inopportune timing of sample collection within the course of disease as previously mentioned, as well as the possibility that serum levels of the RAS peptides do not serve as a reliable surrogate for tissue or intracellular levels [6, 26]. With the potential upregulation of mast cell-derived chymase activity, it is conceivable AT2 levels within tissues are high in COVID-19 patients independent of serum levels [162]. As the authors found low AT(1–7) levels, prior systemic or ongoing local RAS imbalance remains plausible [192].

Further highlighting the enigmatic volatility of the RAS, another group has shown just the opposite of these studies: reduced levels of AT(1–7) while AT2 levels were preserved, albeit with the caveat that levels of the two angiotensins were reported in separate publications drawn from a single common batch of patient samples [195, 196]. This group also found decreased levels of AT1, which they construe as evidence of global RAS downregulation [196]. However, we can alternatively interpret the low AT1 levels as a reflection of rapid turnover in order to maintain the relatively high AT2 levels they report, particularly as angiotensinogen levels were not measured [196].

These mixed data do not unequivocally support the ACE2 downregulation model but limitations, both methodologic and inherent to the system itself, muddy interpretation of the data. We note in particular the considerable variability in AT2 levels, as some studies report a range of values spanning two orders of magnitude even within a single patient group. This may be due to technical issues with sample handling or non-standardized assay performance but also may simply reflect extreme biological variation within a notoriously mercurial system [192-196].

Overall, unanswered questions pertaining to the ACE2 deficiency model remain. Most importantly, more definitive data in support of actual downregulation are needed. Thus far the most relevant evidence emerges from mouse experiments in the SARS-CoV-1 literature, highlighting the need for human studies to quell any lingering doubt of ACE2 downregulation. If confirmed, additional studies demonstrating that such downregulation does drive the endothelial cell dysfunction and dysregulated immunity seen with COVID-19 would cement the ACE2 deficiency angiotensin imbalance hypothesis as a central explanatory model. To date, however, the current data support the possibility of a delayed ACE2 deficiency occurring later in the disease process.

Conclusions

SARS-CoV-2 is a novel coronavirus that causes COVID-19. Early studies confirmed the virus uses ACE2, a key regulatory enzyme in the RAS, as its primary cell receptor. Drawing from studies with SARS-CoV-1, many have speculated that SARS-CoV-2 downregulates ACE2, creating a functional deficiency that may define COVID-19. In this review, we have dissected the merits of this argument. Confirmatory evidence for this theory is clearly limited and the available data would suggest early upregulation of ACE2 by the immune response, even as ACE2 downregulation has also been demonstrated in endothelial cells exposed to the SARS-CoV-2 spike protein. It is therefore entirely conceivable that COVID-19 pathology simply reflects the ubiquity of the ACE2 receptor facilitating widespread viral cytotoxicity. Yet, on many levels the ACE2-downregulation hypothesis fits with the data currently available. The parallels between the clinical picture seen with COVID-19, as with SARS, and the expected consequences of multi-system ACE2 deficiency are striking. Unifying pathologic themes that may link the multiorgan pathology of COVID-19 to ACE2 deficiency include the endothelial cell dysfunction and immune dysregulation that arise in the setting of angiotensin imbalance. We feel that the preponderance of evidence points to RAS dysregulation – even if confined to individual tissues – occurring as a relatively late event in the pathogenesis of COVID-19, which would support its primacy in driving the deadly second, inflammatory phase of the disease.

Summary key points

This paper explores the hypothesis that ACE2 downregulation plays a central role in COVID-19 pathology

Data support a biphasic model of COVID-19 pathophysiology, in which initial interferon-driven upregulation of ACE2 during a phase of direct viral toxicity is later superseded by viral-induced ACE2 downregulation. ACE2 downregulation plays an important role in the second phase of COVID-19 pathology.

ACE2 deficiency, possibly confined to the tissue or cellular level, appears to drive the inflammatory phase of COVID-19

The inflammatory phase of COVID-19 phenocopies ACE2 deficiency

COVID-19 clinically parallels SARS-CoV-1 disease in which ACE2 downregulation is better established

High- and low-risk groups for COVID-19 can be risk stratified by baseline RAS balance

Multiple clinical studies have shown some benefit in COVID-19 with therapies expected to favorably alter RAS balance

Additional evidence particularly in human studies are needed to confirm this hypothesis