The Role of Aldosterone in OSA and OSA-Related Hypertension

As we know, OSA brings great health burden in the general population. Higher incidence of OSA in PA patients was identified (Table 1). The RESIST-POL study found that OSA occurred more frequently in RHTN patients with PA than those without PA (59.4% vs. 42.4%) (15). In a population consisting of 3,003 consecutive patients with HTN, 321 were diagnosed with PA, among whom 45.8% were OSA patients (14). Then, a cross-sectional multiethnic study that screened for OSA in 207 patients with PA showed that the prevalence was 67.6% and there was no obvious difference of the prevalence between the white and Chinese (64.4% vs. 70%) (13). It was also reported the OSA prevalence of 55% among 71 Japanese patients with PA. Body mass index (BMI) and triglyceride content increased the risk of OSA in PA patients (OR = 1.27 and OR = 1.01, respectively) (11). Besides, an early retrospective study reported that among 3,428 hypertensive patients, patients with hyperaldosteronism had a higher prevalence of sleep apnea than those without hyperaldosteronism (18% vs. 9%), despite a lack of confirmation of PA (16). It should be mentioned that a much lower prevalence of OSA (10%) in a retrospective study including 677 PA patients may be attributed to the fact that polysomnography (PSG) was only conducted in those with snoring, which resulted in the underestimation of the actual prevalence of OSA in PA (12).

Management of PA improved OSA symptoms. Wolley et al. performed repeated PSG on 20 patients with PA pre- and post-treatment. Seven patients underwent adrenalectomy and 13 patients received treatment with spironolactone, amiloride, or both. The mean apnea–hypopnea index (AHI) was reduced from 22.5 to 12.3 events/h (P = 0.02) after an 8-month follow-up (17). A retrospective study including 83 PA patients (48 surgically managed and 35 medically managed) also showed a significant reduced OSA probability assessed by the Berlin questionnaire after PA treatment (from 64% to 35%, mean Berlin score 1.64 to 1.35, P < 0.001) with the follow-up duration up to 2.6 years. It seemed to be independent of BMI, for BMI remains unchanged before and after treatment for PA. Both obese and non-obese patients showed significant decreases in OSA probability (18).

PA was present in 2.6%–12.7% of the general HTN patients (19). Studies showed that the incidence of PA in OSA patients was at least 5% in OSA-HTN patients and up to 36% in RHTN patients with probable OSA (13, 14, 20–23) (Table 2). PA is likely to be more frequent in patients with OSA and HTN than in the general hypertensive population. Among 114 subjects with RHTN, 72 subjects had a high risk for sleep apnea based on the Berlin questionnaire who were more likely to have a diagnosis of PA than those with low risk of sleep apnea (36% vs. 19%) (20). Furthermore, the study of Di Murro et al., in which both PA and OSA were definitely confirmed, found that OSA patients (n = 53) had a higher prevalence of PA compared with non-OSA patients (n = 272) (34% vs. 9.2%) (21).

There was a high coexistence of PA and OSA, discrepancies in the results notwithstanding. The possible reason for the variation in prevalence should be considered such as sample sizes, differences in the criteria for the selection of patients, and different methodologies and criteria for the diagnosis of PA and OSA (Tables 1 and 2).

Several studies showed that aldosterone excess was present in OSA and suggested its involvement in the pathogenesis of OSA-related HTN. A meta-analysis showed that OSA patients tended to have a higher aldosterone level compared with the control group. A subgroup analysis further found that this effect was solely significant in OSA patients with HTN rather than in OSA patients without HTN (24). Later, a cross-sectional study with 534 primary RHTN patients (493 OSA and 41 non-OSA) demonstrated that the severe OSA group had elevated plasma aldosterone concentration (PAC) compared with those in the non-OSA group or mild/moderate OSA group. PAC and 24-h urine aldosterone level (24-h UAldo) were positively associated with AHI (β = 0.32 and β = 0.35, respectively, P < 0.05), after adjustment of age, gender, BMI, smoking status, plasma renin activity (PRA), diuretic and angiotensin-converting enzyme inhibitors (ACEI), and/or angiotensin receptor blocker (ARB) usage (9). Similarly, de Souza and colleagues found that higher PAC and 24-h UAldo were associated with severe OSA after adjustment for age, sex, BMI, 24 h BPs, and dipping status (25).

Studies have explored the impact of continuous positive airway pressure (CPAP), the gold-standard therapy for moderate to severe OSA, on aldosterone levels in OSA patients with a follow-up varying from 1 to 14 months (25–34) (Table 3). Concerning about normotensive population, two observational studies were conducted by Nicholl and colleagues to evaluate the effect of 1-month CPAP on renin–angiotensin–aldosterone system (RAAS) activity in OSA patients without HTN and diabetes in 2014 and 2021. Not only PAC was significantly reduced but also BP and renal function were improved after CPAP treatment (26, 28), especially in those with severe hypoxemia (26). Of note, patients in both studies were asked to keep a high-salt diet 3 days before the first visit until the second visit to avoid the impact of salt status on the aldosterone level. However, Møller and coworkers found that no laboratory data including PAC were changed in 13 symptomatic OSA patients without HTN after a successful 14-month CPAP treatment (29). A parallel randomized controlled trial (RCT) of 1-month CPAP enrolling 101 males with OSA was conducted, in which both the placebo and active treatment groups have similar use of CPAP. Unexpectedly, PAC rose by 30% in both groups and the sham/active difference was not significant (33). The result should be interpreted with caution due to lack of demographic information about coexisting diseases and drug usages.

The change of aldosterone level by CPAP treatment was also tested in OSA patients with HTN or RHTN. PAC in 11 hypertensive OSA subjects without any medications was found to be significantly decreased after 3 months of CPAP treatment (P = 0.046) (30). Improvement in nighttime mean BP was associated with changes of aldosterone. Lloberes et al. conducted one RCT, which showed that a 3-month CPAP treatment significantly decreased PAC and this change was independently associated with changes in office DBP (32). Intriguingly, Joyeaux-Faure and colleagues reported a significant increase in PAC during a 3-month sham CPAP compared with the active CPAP (P = 0.01) (34). The 24-h UAldo tended to decrease after 6 months of CPAP treatment in another RCT (P = 0.074) (25). This reduction was more noticeable in those with the non-dipping pattern, not using spironolactone, less obese, and with lowest sleep SaO₂ levels (25). Although some studies found unchanged PAC by CPAP (27, 31), a significant decrease of aldosterone-to-renin ratio (ARR) was observed in the responder group whose mean blood pressure (BP) was reduced by at least 4.5 mmHg after CPAP treatment (27).

In summary, a higher level of aldosterone was present in hypertensive OSA patients, and most studies indicated a decline of aldosterone level after CPAP treatment. Several factors blamed for some controversy in the results may belong to methodological concerns such as different demographic characteristics (OSA severity, BMI) and inconsistent control of variables (antihypertensive drugs, salt status, body position when sampling, etc.) known to influence aldosterone production.

Aldosterone is a hormone mainly secreted by the adrenal cortex that regulates electrolyte and water balance by increasing the renal retention of sodium and the excretion of potassium. Angiotensin II (Ang II) binds to its receptor (AT1R) on the zona glomerulosa cells of the adrenal cortex, which is one of major regulators of aldosterone synthesis. Chronic intermittent hypoxia (CIH)-induced sympathetic outflow to the kidney stimulates renin release and leads to elevated circulating levels of Ang II (35). It was demonstrated that Ang II was much higher in OSA patients than in healthy controls (24). CIH-treated rats also caused increasing levels of circulating renin activity and Ang II (36). In-vitro studies also confirmed that CIH directly upregulated the expression of renin (37). Besides, obesity, highly concomitant in OSA, has been found to participate in aldosterone excess in RHTN patients (38). Adipocyte-derived factors may be involved in adrenal aldosterone synthesis. Leptin was able to directly activate aldosterone synthase (CYP11B2) of the adrenal gland, resulting in increased production of aldosterone via a Ca²⁺-dependent mechanism which is independent of RAAS and sympathetic nervous systems (39). However, a subsequent experiment found the effect of leptin on aldosterone synthesis only happened in female mice (40). It was also observed that complement-C1q TNF-related protein-1 (CTRP-1), a secreted protein derived from adipocytes, could also enhance aldosterone production in cells of the human adrenal cortical cell line (41). Additionally, adipose tissue could secrete aldosterone itself (42). Nevertheless, studies are needed to clarify this mechanism in OSA.

In a 109 RHTN population, the severity of OSA was found to be greater in the high PAC (defined as PRA < 1 ng/ml/h and 24-h UAldo ≥ 12 µg) group than in the normal PAC group (AHI, 19.9 vs. 10.0 events/h). PAC and 24-h UAldo were positively and significantly correlated with AHI in the high PAC group, which was not found in the normal PAC group (43). Moreover, hyperaldosteronism [defined as ARR > 30 and PAC > 20 ng/dl or ARR > 50 (ng/dl: ng/ml/h)] was reported to independently increase the risk of OSA after adjustment of age, sex, BMI categories, diabetes mellitus, and chronic heart failure (OR = 1.8, 95% CI: 1.3–2.6) (16).

Two main mineralocorticoid receptor (MR) antagonists, spironolactone and eplerenone, are currently used as secondary agents in hypertensive patients (6). Several studies evaluated their effectiveness on OSA combined with uncontrolled HTN or RHTN (44–48) (Table 4).

Gaddam and coworkers recruited 12 individuals with OSA and RHTN, who administered additional spironolactone. All subjects were asked to remain on their baseline thiazide diuretic, ACEI, and ARB throughout the treatment period. After an 8-week therapy, the reduction in AHI was significant (39.8 ± 19.5 vs. 22.0 ± 6.8 events/h), with a significant decrease of body weight, clinic systolic and diastolic BP, and 24-h ambulatory blood pressure monitoring (AMBP) parameters (24-h systolic BP, for instance, 147 ± 13 vs. 130 ± 19 mmHg) (47). Thirty patients with OSA and RHTN were randomly assigned to a control group who received usual antihypertensive agents and a treatment group who received add-on therapy of spironolactone. After a 12-week follow-up, the reductions of clinic BP, AMBP parameters (mean differences of 24-h systolic BP in the two groups, 16.3 ± 10.0 vs. 5.3 ± 7.0 mmHg), and AHI (mean differences in the two groups, 21.8 ± 15.7 vs. 1.8 ± 12.8 events/h) were significant, as well as PAC (44). Similar results were also observed in 16 OSA patients with uncontrolled HTN. They took metolazone and spironolactone daily for 1 week after which the daily dose was force-titrated to double dose for another week. Then, a significant reduction of AHI, edema scale, body weight, total body fluid and leg fluid volume, and home BP parameters was observed (46).

Krasińska and coworkers led a 3-month observational study and a 6-month RCT in 2014 and 2019, respectively, in which additional use of eplerenone had similar benefits (significant reductions in the AHI, neck circumference, BP), along with improvement in aortic pulse wave, arterial wall stiffness, and left ventricular hypertrophy (45, 48).

The present observational and randomized trials consistently reported obvious improvement of AHI and BP after an add-on therapy of eplerenone or spironolactone in OSA patients with RHTN.

Aldosterone promotes sodium–water reabsorption and elevates overnight fluid shifting to the neck in the supine position, resulting in pharyngeal edema and upper airway obstruction. It was proven that OSA severity was strongly correlated with an overnight reduction of leg fluid volume and of calf circumference (49). Clinical studies showed that aldosterone blockade not only reduces PAC and BP but also AHI and neck girth significantly (44, 45, 47, 50). Aldosterone excess could damage the taste sensitivity for sodium chloride (NaCl) and favor more salt intake, further facilitating water–sodium retention (51). Besides, significantly increased secretion of cortisol in patients with PA, independent of PA subtype or adenoma tissue genotypes, could also increase risk of OSA (52, 53).

Aldosterone, which was related to sarcopenia (54), might affect the mass and function of upper dilator muscles. Lower skeletal muscle mass was found in female patients with PA than those with non-functional adrenal incidentaloma (55). It was also found that aldosterone impeded myogenesis in vitro and in vivo (56, 57). Both undifferentiated myoblasts and differentiated myotubes express aldosterone receptors (58). In Duchenne muscular dystrophy (DMD) mice model, the non-steroidal mineralocorticoid receptor antagonist (finerenone) brought significant improvements in clinically relevant functional parameters in skeletal muscle (normalized grip strength, lower susceptibility to limb muscle damage, normalized limb muscle force) (59) (Figure 1).