Epigenetics dysfunction in morbid obesity with or without obstructive sleep apnoea: the EPIMOOSA study

The prevalence of obesity, defined as a body mass index (BMI) ≥ 30 kg/m², in the adult population of developed countries is greater than 25% and has reached epidemic levels [1]. Obesity increases the risk of death from many causes [2, 3], being an independent risk factor in the development of several chronic diseases (cardiovascular disorders, type 2 diabetes mellitus [DM2], hyperlipidaemia, cancer, high blood pressure, liver disease, etc.) and acute concurrent processes (e.g., accidents, infections) [4, 5].

Obesity is closely related to the development of obstructive sleep apnoea (OSA) [6] and obesity hypoventilation syndrome [7]. OSA is the most common sleep breathing disorder, affecting 20% of men and 8% of women in Spain [8]. This condition is characterized by repeated episodes of partial or total obstruction of the pharynx during sleep. The main clinical implications are sleep fragmentation and chronic intermittent hypoxia (CIH). OSA and obesity are both associated with high morbi-mortality rates, although the specific role of each condition in a given patient remains unclear.

Adipose tissue from obese patients, regardless of the coexistence of OSA, suffers chronic hypoxia due to its poor vascularization, which increases the level of hypoxia-inducible factor (HIF) [9, 10]. Recent studies have suggested that HIF, which is produced in hypoxic situations, activates different epigenetic mechanisms [11]. OSA has also been associated with the presence of systemic inflammation of as-yet unknown origin. This state may be influenced by epigenetic modifications induced by de-oxygenation/re-oxygenation phenomena, in which CIH is crucial [12, 13]. Both morbid obesity (MO) and OSA patients have an increase in several factors associated with endothelial damage triggered by CIH [14]. Epigenetic changes, especially overexpression of certain miRNAs that target the vascular endothelium (Fig. 1), are an intermediary mechanism that may connect CIH with endothelial damage. In OSA patients without MO, our group has identified an increased level of certain miRNAs in circulating exosomes associated with accelerated atherosclerosis and cardiovascular risk [15, 16]. Interestingly, some of these miRNAs reduced their expression after treatment with nocturnal continuous positive airway pressure (CPAP) [15]. In obese children with OSA, Khalyfa et al. found higher levels of miRNAs from circulating exosomes involved with endothelial dysfunction. Nevertheless, the effect of OSA therapy and weight loss was not evaluated in this study. In addition, no such studies have been performed in obese adults with OSA.

Circulating exosomes are extra-vesicular vesicles that contain lipids, proteins and miRNAs that contribute to remote cell signalling and communication mechanisms in both physiological [17] and pathological processes [18]. This methodological paper describes the aims and methods of the Epigenetics dysfunction in Morbid Obesity and Obstructive Sleep Apnoea (EPIMOOSA) research project, which hypothesizes that obesity and sleep apnoea pathogenically potentiate each other as independent risk factors for cardiovascular morbi-mortality through overexpression of dysregulated miRNAs in circulating exosomes.

Previous studies have evaluated the presence of epigenetic dysfunction in both children and adults with OSA (Table 4). However, most of these studies have assessed epigenetic dysfunction at the DNA methylation level [20, 21, 35, 36] or by using free miRNA in plasma [36, 37]. No such studies have been performed in obese patients with OSA, and no studies have evaluated the effect of CPAP or BS. The epigenetic changes occurring in obesity have also been widely studied, revealing that even perinatal alterations have an influence on the propensity to obesity in adulthood [38]. The authors of a study including 13 obese and non-obese adolescents found 55 different miRNAs (including miRNA 148b, miRNA 4269, miRNA 23b, miRNA 4429) in obese individuals compared to those with a BMI < 25 kg/m², and they were associated with an increase in insulin resistance, which is responsible for target organ damage in obesity [39]. The same group studied the effect of BS-induced weight loss on the exosomes and their content. Another study carried out on six African American women who underwent a gastric bypass examined the mircoRNAs before and 1 year after surgery and reported a change in the expression of 58 miRNAs, 10 of which were directly related to an improvement in insulin resistance [40]. None of these studies have considered the overlap effect of OSA.

The adipocytes of patients with MO present hyperplasia, hypertrophy and insufficient angiogenesis, which leads to tissue hypoxia and subsequently negative long-term metabolic and cardiovascular consequences [41]. Hypoxia also causes an increase in cell cytoplasm HIF 1α levels, demonstrating that such an increase activates, among other mechanisms, the release of different miRNAs such as miRNA 21 [42]. Similarly, patients with OSA who endure repeated episodes of nocturnal CIH experience a state of constant hypoxemia that lasts all night and triggers an increase in HIF 1α [43]. These pathophysiological coincidences are limited not only to the HIF but also to endothelial dysfunction in children with OSA and obese children without OSA. These studies revealed that children with endothelial dysfunction exhibited a significant decrease in 4 miRNAs (miRNA 16, miRNA 451, miRNA 5100, and miRNA 630), the last one being of particular interest given its association with endothelial dysfunction [34].

In the context of OSA, different epigenetic markers have been evaluated, specifically DNA methylation and, more recently, the role of miRNAs. Our group has previously studied non-obese (BMI < 30 kg/m²) adults with OSA and did not find any changes in methylation or FOXP3 expression. However, we found the dysregulation of certain miRNAs in circulating exosomes (miRNA320-5p and miRNA132-3p) associated with cardiovascular diseases that produced a non-uniform response to CPAP therapy [15]. Those findings explain the increasing interest in this field. On the one hand, epigenetic markers could be useful in identifying subjects at risk of developing certain comorbidities and could be used to monitor the progression of the underlying condition. On the other hand, there are already drugs that act on epigenetic changes, even reversing them and contributing to the treatment of several diseases, especially in the area of oncology [44].

The role of miRNA in OSA is currently a popular area of research. A sub-analysis of the HIPARCO clinical trial [37] revealed that a panel of miRNAs could be used to reliably predict which patients with refractory hypertension and OSA would respond better to CPAP therapy in terms of reducing their blood pressure. An experiment conducted by Khalyfa et al. [45] found a possible pathophysiological relationship among the circulating miRNAs of obese patients with OSA, adipocyte alterations, and the mechanisms of insulin resistance [45].

The relationship between OSA and MO has been well documented [46], showing that their coexistence greatly increases the harmful effects of both conditions on various target organs [47, 48] and that they have intrinsically linked mechanisms of action [43, 49]. Regarding the high prevalence of OSA among morbidly obese patients [7], we believe that the works cited in this article feature a significant methodological bias. The coexistence of two diseases whose close relationship has already been evidenced [50] means that any studies in this area must control both factors carefully.

Our study aims to evaluate, for the first time, whether patients with MO with/without OSA develop epigenetic dysfunction in circulating exosomes involved in accelerated incidents of cardiovascular diseases. Our study will provide a better understanding of the role of CPAP therapy in patients with MO/OSA overlap and the effect of BS-induced weight loss. The results could also give rise to new biomarkers to improve phenotyping in patients with either or both of the conditions and, possibly, novel therapeutic targets.