Introduction
Non-alcoholic fatty liver disease (NAFLD) is a collective term for a broad spectrum of liver diseases ranging from simple steatosis (non-alcoholic fatty liver, NAFL) to non-alcoholic steatohepatitis (NASH) and its complications fibrosis, cirrhosis and hepatocellular carcinoma [
1,
2]. With a prevalence of 25–30%, NAFLD has become the most common cause of chronic liver disease in the Western world [
3‐
5] and is expected to increase dramatically in the future with the growing epidemics of obesity and type 2 diabetes (T2DM) [
5].
It is associated with increased all-cause mortality, less due to liver complications than to non-hepatic comorbidities and their complications [
6,
7], with cardiovascular events being the most common cause of death in NAFLD [
8,
9]. In this context, NAFLD has been related to an increased risk of developing coronary heart disease, T2DM, chronic kidney disease and certain extrahepatic cancers [
10‐
12]. More recently, accumulating evidence suggests a strong and independent association between NAFLD and an increased risk of functional, structural and arrhythmic cardiac complications that promote the development of heart failure (HF) [
8‐
10,
13]. While the mechanisms linking NAFLD and HF remain largely unknown [
10], NAFLD and HF share many risk factors, including T2DM, obesity, hypertension, and metabolic syndrome [
10,
14,
15]. Although several studies have found an association between NAFLD and HF, the results are sometimes conflicting, and most studies had small samples or limited populations or did not adequately adjust for potential confounders [
10,
16,
17].
As both NAFLD and HF are associated with high morbidity and mortality worldwide and thus represent a major economic and public health burden, the aim of this work was to investigate the incidence of HF as a function of NAFLD as the primary outcome after adjustment for HF risk factors in a large real-world cohort from Germany.
Methods
Discussion
This retrospective study using the DA database (IQVIA) included a large real-world cohort of more than 173,966 adult outpatients in Germany and compared individuals with and without NAFLD in a 1:1 matched cohort for the risk of new-onset HF as the primary outcome. It was found that NAFLD was associated with a significantly increased risk of developing HF in all age groups, in both sexes and in patients with and without diabetes at baseline. As such, during the 10-year follow-up period, 13.2% of patients with NAFLD were newly diagnosed with HF compared to 10.0% of patients without NAFLD. Notably, the comparison of patients with and without NAFLD was adjusted for sex, age, and diagnoses considered risk factors for HF, such as obesity, diabetes, hypertension, ischemic heart disease, atrial fibrillation, chronic kidney disease and chronic obstructive pulmonary disease (COPD).
Our study supports the findings of a recently published large meta-analysis by Li et al. which included a total of 6 cohort studies with approximately 11 million participants and found a 36% increased relative risk of future HF in patients with NAFLD compared with patients without NAFLD after adjustment for other cardiometabolic risk factors. Of interest, even simple steatosis was associated with an increased risk of HF [
16]. Similarly, in an updated meta-analysis of 11 observational cohort studies with aggregated data from about 11 million middle-aged individuals from various countries, Mantovani et al. examined new-onset HF as the primary outcome in relation to NAFLD over a median of 10 years. The authors found that NAFLD was significantly associated with a 1.5-fold long-term risk of new-onset HF that was independent of age, sex, obesity, diabetes, hypertension, and other common cardiovascular risk factors [
19]. Of note, in our study, although a significant association between NAFLD and incident HF was found in all age groups studied, interestingly, this association was particularly pronounced in patients with NAFLD aged 18 to 50 years, whereas it was weaker in older patients. Possible hypotheses that could at least partially explain this observation are, first, that older age, which is a strong risk factor for HF, may attenuate the effect of NAFLD itself as a risk factor for new-onset HF and, second, that older people are more likely to be treated with medication, which in turn may reduce the risk of cardiovascular disease and the development of HF. Further research, particularly with prospective study designs, is needed to better understand this age-related association.
The development of HF is a process of cardiac remodeling based on molecular, cellular, and interstitial changes in the heart induced by hemodynamic stress, neurohormonal activation, and other factors yet to be elucidated, which manifests clinically as alterations in cardiac structure and function [
20]. In this regard, several studies have found a strong association between NAFLD and an increased risk of left ventricular (LV) diastolic dysfunction, LV hypertrophy, or left atrial enlargement independent of obesity, hypertension, and T2DM [
9,
21].
Recently, a meta-analysis of 16 cross-sectional studies involving 32,000 subjects showed that NAFLD is associated with subclinical changes in left heart structure and function. Interestingly, the association between NAFLD and subclinical cardiac remodeling remained significant in most of the studies included in the meta-analysis when adjusted for established cardiometabolic risk factors [
21]. In addition, Chiu et al. examined a Framingham Heart Study sample of 2,356 participants who had undergone echocardiography and standardized computed tomography (CT) to measure liver fat [
22]. They demonstrated that liver fat was associated with several imaging markers of subclinical cardiac dysfunction after correction for a number of demographic and HF risk factors. Similar conclusions were reached in the population-based cohort study CARDIA (Coronary Artery Risk Development in Young Adults), which included 1827 adults and prospectively examined whether NAFLD was linked to short-term changes in echocardiographic measures of LV structure and function over a 5-year period. Again, NAFLD was found to be associated with subclinical changes in LV structure and function independent of traditional risk factors for HF [
23].
While the association between NAFLD and HF risk remains largely unclear, several potential pathophysiological mechanisms by which NAFLD may increase the risk of HF development and progression have been discussed [
10,
19]. Although our study did not elucidate the mechanisms linking NAFLD to HF, it suggests that NAFLD, beyond its phenotype, is a systemic disease whose pathophysiology is determined by the involvement of multiple organ systems. These mechanisms are thought to be determined by a variety of metabolic, genetic, epigenetic, and nutritional factors [
19]. In particular, factors associated with T2DM and obesity have been discussed as a possible link between NAFLD and the development of HF [
24]. Thus, insulin resistance and impaired glucose and lipid metabolism, which are among the major pathophysiological features of NAFLD, are thought to play a role in alterations in cardiac energy metabolism and cardiac dysfunction [
10]. In this context, circulating free fatty acids (FFAs) and triglycerides have been reported to lead to increased myocardial fatty acid oxidation and inefficient metabolism in both liver and cardiac myocytes in patients with NAFLD, which may contribute to the development of HF [
10,
20]. In addition, a role for atherogenic dyslipidemia, particularly in mediating NAFLD-associated cardiovascular risk through an increased hepatic synthesis of very low-density lipoprotein (VLDL) in NAFLD, has been described [
10]. Furthermore, hepatic and cardiac mitochondrial dysfunction has been linked to the development of progressive NAFLD [
9,
11,
25,
26], which in turn leads to increased production of reactive oxygen species (ROS) [
27]. There is also evidence that increased activation of the renin–angiotensin–aldosterone system (RAAS), known to be an important mediator of cardiac remodeling and progression of HF, may play an additional role in NAFLD [
28]. In this context, an increased activation of the RAAS in combination with cardiac ROS is thought to be involved in the interaction between NAFLD and HF [
10,
28]. It has also been suggested that the proinflammatory cytokines interleukin-6 (IL-6), interleukin-1beta (IL-1β), and tumor necrosis factor-alpha (TNF-α), as well as decreased plasma adiponectin concentrations resulting from increased or dysfunctional visceral adipose tissue, may not only be involved in the development and progression of NAFLD through effects on glucose and lipid metabolism and insulin resistance but may also affect the coronary arteries and cause HF [
29,
30]. Recently, intestinal dysbiosis has received increasing attention as a factor linking NAFLD and HF. In this context, gastrointestinal factors such as the endotoxin lipopolysaccharide (LPS), metabolites of aromatic acids, ethanol, short-chain fatty acids, incretins, and modified bile acids are known to contribute to the severity of liver disease [
31,
32] and may also have direct effects on the cardiovascular system, potentially influencing HF [
33]. Increased intestinal permeability may also enhance the potential of LPS to enter the portal circulation and promote a proinflammatory response in the liver. In this regard, trimethylamine oxide (TMAO) has also been discussed as having a potential adverse effect on cardiac disease [
33,
34]. Also of interest are genetic variants, such as the presence of gene polymorphisms, e.g. for patatin-like phospholipase domain-containing protein-3 (PNPLA3) and trans-membrane 6 superfamily 2 (TM6SF2) [
10,
19,
35], which have been implicated in predisposing to the development and severity of liver disease in NAFLD [
35‐
37]. Although both genotypes increase the risk of more severe liver disease in NAFLD, there is evidence that both genotypes also decrease plasma concentrations of VLDL, which may attenuate the strength of the association between NAFLD and the risk of coronary heart disease in particular [
9]. However, to our knowledge, no study has examined whether and to what extent these genetic polymorphisms influence the strength of the association between NAFLD and the risk of heart failure, and further evidence is needed.
To date, no specific pharmacotherapy has been approved for NAFLD, and treatment of NAFLD is primarily based on lifestyle changes (e.g., weight reduction, physical activity) [
38]. However, there is evidence that certain medications used to treat T2DM may also reduce the risk of HF in patients with NAFLD. In this context, scientific interest in the relationship between these two conditions is increasing as newer antihyperglycemic agents, particularly sodium-glucose cotransporter-2 (SGLT2) inhibitors and glucagon-like peptide-1 receptor (GLP1R) agonists, have shown some benefit on liver fat content and histologic regression of NASH [
39], but also clinically significant benefits on cardiovascular outcomes, including the risk of hospitalization for HF, independent of T2DM status [
39,
40].
We would like to point out some limitations of our study, which are mainly due to the study design and are therefore unavoidable. First, our study is subject to the limitations of a retrospective analysis of a database. Secondary data analyses may be limited by the incompleteness of the underlying data. Because all diagnoses are based on ICD-10 codes, misclassification and undercoding of certain diagnoses cannot be excluded, which may have resulted in some selection bias. In addition, certain information about important health determinants that would have allowed further analysis was not available, such as socioeconomic status, family history, ethnic background/race, environmental conditions, lifestyle factors (e.g., physical activity, nicotine or alcohol consumption, diet), and genetic information. Another limitation of our study is that the DA database does not yet include imaging (including sonography/elastography/fibroscan and echocardiography) or histopathologic data in addition to ICD-10 codes, and it does not include clinical follow-up information that would have allowed more accurate stratification of NAFLD and HF. In particular, it would have been interesting to investigate whether the severity of liver disease in NAFLD would have further exacerbated the increased risk of developing HF. At this point, we would like to refer to previously published cohort studies using liver biopsy or non-invasive scores for advanced fibrosis, showing that the risk of developing HF seems to further increase with the severity of NAFLD, especially with higher fibrosis stages [
19,
41,
42]. As mentioned above, because echocardiographic data were not available for our analyses, we were also unable to examine the association between NAFLD and HF as a function of left ventricular ejection fraction (HF with preserved ejection fraction (HFpEF) versus HF with reduced ejection fraction (HFrEF)). Furtherrmore, we should be aware that our study is purely descriptive and can only show associations, but cannot draw any causal conclusions. Nevertheless, we would like to emphasize the strengths of our study, which are the large number of patients included, the use of representative population data, and the overall long follow-up period. Our observations in a large real-world cohort in Germany are of particular importance for the generalizability of the results of previously published cohort studies to Western countries. Moreover, this study used data from the representative IQVIA DA database, which has been validated in several studies [
18] and has already been used in studies on NAFLD [
43,
44] and HF [
45,
46].
In conclusion, the present study provides strong evidence for a positive association between NAFLD and subsequent HF. Given the dramatic increase in the prevalence of NAFLD and the high morbidity and mortality of HF, the results of our study are of major clinical relevance. Therefore, we propose a multidisciplinary approach that includes prevention and screening strategies for further patient-centered risk stratification using echocardiography or serum biomarkers to identify the early stages of HF in patients with NAFLD. The results of our study should stimulate further research efforts to understand the complex pathophysiological mechanisms by which NAFLD may contribute to the risk of new-onset HF and to determine whether amelioration of NAFLD may prevent or slow the development and progression of HF.