Cardiovascular risk assessment in patients with a severe mental illness: a systematic review and meta-analysis

Cardiovascular disease is the leading cause of overall mortality, accounting for 24 % of deaths worldwide, while psychiatric diseases, led by major depressive disorder, are considered the eleventh most burdensome disease globally, with an increasing effect on overall mortality [1, 2].

Criteria for the definition of severe mental illness (SMI) differ, with some authors applying a narrow definition based on psychosis [3] and others also including a set of nosological entities of different types and clinical symptoms but with several common diagnostic criteria: severity, persistence over time (2 years or more), and a tendency toward clinical deterioration and difficulties in social and occupational function [4, 5].

It has been reported that cardiovascular risk (CVR) is higher in patients with SMI [6]. Studies in patients with bipolar disorder and schizophrenia indicate that they have a higher CVR than in the general population [7]. In patients with schizophrenia, the most prevalent CVR factors are hyperlipidaemia (61 %), smoking (55 %), obesity (41 %), diabetes (19 %) and hypertension (17 %)) [8]. Risk of metabolic syndrome is also higher among patients with schizophrenia and bipolar disorder [9]. Moreover, patients with anxiety and major depression have higher prevalence of hypertension compared to groups of similar age from the general population [10, 11].

Several factors may contribute to this raised CVR among patients with SMI, including unhealthy behaviours, difficulties in communication, barriers to medical care, poor treatment adherence and social deprivation [12]. Patients with SMI often receive fragmented medical care and fewer preventive measures, which leads to higher levels of underdiagnosis and lower rates of disease control [13]. Furthermore, antipsychotic drugs, antidepressants, and mood-stabilizing drugs have deleterious side effects, including important cardiometabolic consequences [14‐16].

However, to date no systematic analysis has investigated whether CVR is increased equally in all patients with SMI, making it difficult to design and implement effective, feasible, evidence-based interventions for CVR management in these patients. A summary of the observations about CVR in the different subgroups of patients with SMI would provide a better epidemiological description of the problem, inform more effective clinical and preventive strategies and help in the design of further studies.

The major aim of this review was to summarize the available evidence of CVR scores in patients with SMI. Furthermore, this review attempted to determine whether CVR differs between subgroups of SMI patients and compare the CVR between patients with SMI and the general or non-psychiatric population.

The Meta-analysis Of Observational Studies in Epidemiology (MOOSE) criteria were used to undertake this review and meta-analysis [17], together with Preferred Reporting Items for Systematic Reviews and Meta-Analyses (PRISMA) [18]. We conducted a systematic review of studies that reported CVR in patients with SMI.

The electronic and manual searches retrieved 3,608 articles, of which 67 full-text papers were assessed for eligibility and 35 studies were finally included in our review (Fig. 1), representing a total of 12,179 psychiatric patients and 225,951 controls. Sample size of psychiatric study groups ranged from 36 [22] to 1,942 [23] participants. Of the 35 studies, 19 studies in Eurasia (16 in Europe) and 16 studies were conducted in the Americas. The most common design was cross-sectional (22 studies); 8 studies were randomized controlled trials (RCT) and only 5 were case-control studies (Table 2). A 45.7 % of the studies were performed in secondary services exclusively and 31.4 % in the hospital setting. The most frequent diagnoses were schizophrenia and related diagnoses (45.7 %), depressive disorders (14.3 %), and bipolar disorders (8.6 %). Seven studies (20.0 %) included different psychiatric diagnoses and only 4 (11.4 %) showed data on SMI as a whole (Table 1).

In 30 studies, methodological quality was evaluated with STROBE and most showed a high quality score (median 21.00, SD: 6.40). Five were evaluated with CONSORT and most had a low quality score (median 18.57, SD: 2.72). The STROBE evaluation revealed two main weaknesses: insufficient efforts to address potential sources of bias and sparse information for each variable of interest on the number of participants with missing data. The CONSORT weaknesses were the method used to generate the random allocation sequence and type of randomisation; details of any restriction (such as blocking and block size); and information about where the full trial protocol can be accessed, if available (Additional file 1: Appendix 1).

Of the 35 studies included, only 7 studies had control groups [22, 24‐29]. These studies used different scores to evaluate CVR (Table 2). Three studies included only patients with schizophrenia and controls: two studies were based on FRS (CVD) scores: 10.7 vs. 8.5 p ≤ 0.01 [28] and 4.7 (4.7) vs. 3.1 (3.2), p = 0.002 [29] and one was based on FRS (CHD) scores: 8.6 (7.3) vs. 6.3 (6.0), p < 0.001 [24]. Two studies included psychiatric diagnoses and were based on FRS (CVD) scores: 11.3 (12.3) vs. 6.8 (6.4), p < 0.01 [25] and 8.3 (5.8) vs. 10.7 (5.9), p = 0.05 [26]. One study included depressive disorders: 10.3 (7.6) vs. 10.1 (7.7), p = 0.97 [22]. One study had insufficient data and was not included in the meta-analysis.

Table 3 synthesized the data about CVR scores found in studies by diagnosis groups of diseases. The CVR mean score assessed with FRS (CVD) in patients with depression ranged from 5.8 to 14.0, in patients with schizophrenia from 4.7 to 11.9, and was 13.7 in the only study of patients with bipolar disorder. Studies that addressed patients with SMI reported that CVR had been expressed in different forms (Table 3).

Subgroup analysis was performed in six studies (3 involving schizophrenia, 1 depressive disorder and 2 psychiatric diagnoses in general). Higher CVR was observed in patients with schizophrenia than in those with depressive disorder or general psychiatric diagnosis, with a pooled SMD (95 % CI) as follows: 0.63 (0.16, 1.09), 0.03 (−0.48, 0.54), and 0.02 (−0.82, 0.86), respectively (Table 4). The sensitivity analysis omitted one study at a time, showing a pooled SMD ranging from 0.19 to 0.50. Funnel plots did not suggest any publication bias (Additional file 2: Appendix 2).

Six studies that included 1,065 people with SMI who had a CVR assessment and 1,567 people without SMI were included in the meta-analysis [22, 24‐27, 29]. The total overall CVR between the psychiatric group and control group showed a SMD of 0.35 (95 % CI:−0.02–0.71, P = 0.06) with significantly high heterogeneity (I ² = 93 %; p < 0.001) (Fig. 2).

Data from studies that reported CVR scores did not support higher risk in patients with SMI than in the control population. Subgroup analysis showed a higher CVR associated with schizophrenia than with other SMIs. Only in patients with schizophrenia was there some evidence of higher CVR scores than in the control population.

To date it has been widely accepted that the prevalence of modifiable risk factors was increased in patients with SMI [30]. Nonetheless, several authors have suggested that not all risk factors were equally increased in these patients. A number of studies have found that smoking and diabetes rates were higher in the SMI population than in the reference population [31], while others observed that hypertension was not increased among SMI patients [31‐33]. Conversely, other authors did not detect significant differences in CVR factors between participants with and without SMI [34]. This could be the result of publication bias affecting CVR studies and therefore affecting CVR assessment. Chapman et al., in a meta-analysis of 42 studies on smoking in patients with schizophrenia, revealed that studies reporting low prevalence of this risk factor are cited less often than those reporting higher prevalence in this population [35].

Numerous previous studies have noted the importance of CVR factors in patients with SMI, but only a few of them incorporated CVR evaluation in the last 12 years. No other systematic review has been found in the literature on this topic. However, Osborn et al., in a systematic review which objective was to determine the relative risk of some CVR factors in people with SMIs, synthesized data about some studies that reported 10 year cardiovascular risk scores [31]. One controlled community study, including 74 SMI patients found that excess CVR scores showed that participants with SMI had higher FRS (CHD) than participants without SMI (median 10-year risk: 5 vs. 4 %) [36]. Another study, including 84 schizophrenic patients showed a significant increase of CVR only in males based on FRS (CHD) (10.4 vs. 6.4 %) [27]. And the last, involves 240 patients schizophrenia and schizoaffective disorders showed also an increased risk based on FRS (MI) score only in male patients compared to controls (8.9 vs. 6.3 %) [37]. Our review also showed that schizophrenia is the group that have more evidence of higher CVR than control groups and is consistent with other studies [38, 39].

However, the discrepancy between data showing higher CVR in SMI and the CVR assessment obtained in our review raises some questions. The tools to measure CVR that have been validated for general population may not apply to patients with SMI. In this sense, Osborn et al. proposed a CVR prediction model for this population [40]. In addition to the usual predictors, this model also included social deprivation, heavy alcohol use, SMI diagnosis, and prescriptions for antidepressants and antipsychotics [40]. Another key point is the influence of the prescribed medications on CVR. There is strong evidence that antipsychotic drugs, and to a more restricted degree antidepressants and mood stabilizers, are associated with an increased risk for several physical diseases, including obesity, dyslipidaemia, diabetes mellitus and so on [41]. Furthermore, unclear benefits of different kinds of antipsychotics (first vs. second-generation antipsychotics) have been reported [42], despite the superior efficacy and greater treatment persistence attributed to second-generation antipsychotics.

Our analysis showed that schizophrenia is the group at highest risk, in consonance with other studies that showed an increased risk in patients with schizophrenia and depression, compared to other SMIs [41, 42]. Of the three studies of schizophrenic patients included in the forest plot summary, McCreadie et al. [27] clearly had the highest SMD. This difference may be explained by the inclusion of older patients with a longer history of illness compared to the other two studies [24, 29].

A review of literature reporting CVR assessment in patients with SMI did not find sufficient evidence to determine whether or not there is a higher risk in these patients relative to the reference population. Subgroup analysis showed a higher CVR in patients with schizophrenia compared to those with depressive disorder or a psychiatric diagnosis. Only in patients with schizophrenia was there some evidence of higher CVR scores than in the control population. Instead of the generalized idea that SMI is associated with increased CVR, it is important to consider the complexity of summarizing the data because there is no universal definition of SMI or standard methods to describe CVR in this population. Further work is needed to elucidate whether new CVR charts that incorporate intrinsic determinants (as the effect of psychotropic drugs or social deprivation) should be established for risk assessment in this population.