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Mortality and adverse events associated with statin use in primary care patients with depression: a real-world, population-based cohort study
  1. Riccardo De Giorgi1,2,
  2. Franco De Crescenzo1,2,
  3. Edoardo Giuseppe Ostinelli1,2,3,
  4. Philip J Cowen1,2,
  5. Catherine J Harmer1,2,
  6. Seena Fazel1,2,
  7. Andrea Cipriani1,2,3
  1. 1 Department of Psychiatry, University of Oxford, Oxford, UK
  2. 2 Oxford Health NHS Foundation Trust, Oxford, UK
  3. 3 Oxford Precision Psychiatry Lab, NIHR Oxford Health Biomedical Research Centre, Oxford, UK
  1. Correspondence to Dr Riccardo De Giorgi, Psychiatry, University of Oxford, Oxford, UK; riccardo.degiorgi{at}psych.ox.ac.uk

Abstract

Background New National Institute for Health and Care Excellence (NICE) guidance endorses the prescription of statins in larger population groups for the prevention of cardiovascular and cerebrovascular morbidity and mortality, especially in people with severe mental illness. However, the evidence base for their safety and risk/benefit balance in depression is not established.

Objectives This study aims to assess the real-world mortality and adverse events of statins in depressive disorders.

Methods Population-based, nationwide (England), between-subject, cohort study. We used electronic health records (QResearch database) of people aged 18–100 years with first-episode depression, registered with English primary care practices over January 1998–August 2020 for 12(+) months, divided into statin users versus non-users.

Primary safety outcomes included all-cause mortality and any adverse event measured at 2, 6 and 12 months. Multivariable logistic regression was employed to control for several potential confounders and calculate adjusted ORs (aORs) with 99% CIs.

Findings From over 1 050 105 patients with depression (42.64% males, mean age 43.23±18.32 years), 21 384 (2.04%) died, while 707 111 (67.34%) experienced at least one adverse event during the 12-month follow-up. Statin use was associated with lower mortality over 12 months (range aOR2–12months 0.66–0.67, range 99% CI 0.60 to 0.73) and with lower adverse events over 6 months (range aOR2–6months 0.90–0.96, range 99% CI 0.91 to 0.99), but not at 1 year (aOR12months 0.99, 99% CI 0.96 to 1.03). No association with any other individual outcome measure (ie, any other neuropsychiatric symptoms) was identified.

Conclusions We found no evidence that statin use among people with depression increases mortality or other adverse events.

Clinical implications Our findings support the safety of updated NICE guidelines for prescribing statins in people with depressive disorders.

  • Depression
  • Adult psychiatry
  • Depression & mood disorders

Data availability statement

Data may be obtained from a third party and are not publicly available. To guarantee the confidentiality of personal and health information, only the authors have had access to the data during the study in accordance with the relevant licence agreements. Access to the QResearch data is according to the information on the QResearch website (https://qresearch.org/).

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WHAT IS ALREADY KNOWN ON THIS TOPIC

  • Updated guidance from the National Institute for Health and Care Excellence will expand the use of statins for the primary prevention of cardiovascular and cerebrovascular disease.

  • Concerns around neuropsychiatric adverse events possibly associated with statins are a barrier to their prescription in people with mental illness.

  • The evidence base supporting the safety and risk/benefit of statins in people with common mental disorders such as depression is not established.

WHAT THIS STUDY ADDS

  • Compared with non-use, statin use is associated with lower mortality and no increased adverse events, including neuropsychiatric ones, in people with first-episode depression.

HOW THIS STUDY MIGHT AFFECT RESEARCH, PRACTICE OR POLICY

  • Patients diagnosed with depressive disorders may benefit from statin prescription, similarly to other severe mental illnesses.

Background

Statins are a class of cholesterol-lowering drugs licensed for the prevention and treatment of cardiovascular and cerebrovascular (CVD) morbidity and mortality.1 They are the most prescribed medications worldwide, and more than 70 million prescriptions are dispensed in England alone, costing around £100 million to the National Health Service per year.2

New draft guidance from the National Institute for Health and Care Excellence (NICE) advises that a statin can be offered for the primary prevention of CVD to people above 40 years of age with a 10-year CVD event risk of <10% calculated on QRISK3,3 compared with prior ≥10%.4 This offer should follow an informed discussion between the clinician and the patient about the risk/benefit balance of statin treatment that takes into account patient preferences3 and comorbidities such as mental illness.5 For severe mental illness (SMI)—traditionally including schizophrenia, bipolar disorder and other psychoses, the importance of addressing the elevated mortality rates due to physical health conditions is established6 and reflected in clinical guidelines.3 5 This is less clear for more common mental disorders such as depression, despite evidence of robust bidirectional association with chronic ailments including CVD7 and ongoing high excess deaths associated with CVD, multimorbidity and health behaviours in people with depressive disorders.8

The overall benefit of statins has recently been challenged by studies showing small absolute risk reductions for all-cause mortality (0–0.8%) and CVD events (0.4–1.3%) adjusted for baseline risk,9 which would not overweigh the burden of adverse events.10 Recurring concerns about adverse events associated with statin use11 have determined a systematic underuse of these medications—a phenomenon especially seen in people with cognitive and mental disorders.12 However, the associations between statin use and adverse events, particularly neuropsychiatric ones, are not established.13 14 A long controversy on whether lowering cholesterol could result in increased depressive symptoms and suicide15 16 remains unsettled. Higher depression rates following statin use have been particularly observed in people with prior cerebrovascular events.17 18 Preclinical evidence suggests that statin administration can impair cognitive abilities while increasing anxiety levels in animals and humans, which can be explained by complex interactions between several biological and neuropsychological mechanisms.19

A clearer definition of the safety profile and risk/benefit balance of statins is necessary to guide a fully informed prescription of these drugs,20 especially in people with depression who are more at risk of premature CVD morbidity and all-cause mortality.7 8 Therefore, in this real-world, population-based cohort study, we investigate the mortality and adverse events associated with statin use versus non-use in a large, highly characterised sample of primary care patients with depression followed up for 12 months.

Methods

Protocol and full methodology are shown in online supplemental file 1.

Supplemental material

Database

QResearch is a primary care research registry (https://qresearch.org/), with anonymised electronic healthcare records of over 35 million patients registered with 1574 general practices in England, recording demographic data (eg, age), characteristics (eg, smoking status), death records, adverse events, diagnoses and prescribed medications.

Cohort construction

The study cohort was built according to the following inclusion/exclusion criteria to include a homogeneous population with first-episode depression (ie, no treatment-resistant depression) followed up for 12 months.

Inclusion criteria: patients aged 18–100 years, newly diagnosed with a depressive disorder (ie, study entry date) according to validated ‘Read codes’21 22 (list in online supplemental file 2), registered with eligible English general practices between 1 January 1998 and 15 August 2020 for at least 12 months.

Exclusion criteria: any prescription of antidepressants before the study entry date; a lifetime diagnosis of schizophrenia spectrum disorder or bipolar disorder; a diagnosis of postpartum depression within ±180 from the first diagnosis of depression; any prescription of antipsychotics, mood stabilisers or more than one antidepressant at baseline.

Exposure and comparison groups

The exposure under investigation was the concurrent use at baseline of any statin compared with non-exposure at baseline to a statin prescription: statin users versus statin non-users (drugs licensed in the UK according to the British National Formulary; list in online supplemental file 3).

Outcomes of interest

The primary safety outcomes included:

  • All-cause mortality: proportion of participants who had died during the eligible time of observation, identified using death data recorded on their general practice record.

  • Any adverse event: proportion of participants with at least one adverse event (excluding all-cause mortality, list in online supplemental file 4), according to validated ‘Read codes’,21 22 selected among those shown to be important to patients, carers and healthcare professionals in depression.23

Furthermore, we examined the proportion of participants with individual neuropsychiatric adverse events, recorded via the same ‘Read codes’ that have been shown to be a potential concern associated with statin use,13 14 including: any psychiatric symptom, anxiety, sleep disturbance, memory impairment, self-harm, suicidality, completed suicide. We also investigated the proportion of participants who remitted from their depressive episode, defined as a Patient Health Questionnaire (PHQ)-9 score <5 during the study period.

All outcomes were measured at 2, 6 and 12 months.

Confounders

Based on prior QResearch studies on depression and statins,21 22 we considered several confounding baseline variables (ie, possible risk factors associated with both the exposure and outcomes of interest). Suspected confounders included: age at study entry; sex; body mass index (BMI); year, type and severity of depression diagnosis; deprivation status (Townsend deprivation score); geographical area; smoking status; alcohol intake; ethnic group; comorbidities (eg, coronary heart disease, stroke, diabetes); antidepressant category (selective serotonin reuptake inhibitors (SSRIs), tricyclics, monoamine oxidase inhibitors, other antidepressants) and concomitant medications (eg, anticonvulsants, hypnotics/anxiolytics, antihypertensives) at baseline (list in online supplemental file 5).

Analysis

Baseline characteristics of the study cohort were reported with descriptive statistics.

Outcomes of interest were explored with multivariable logistic regression models, clustered by general practices, to compute ORs with 99% CIs for statin users versus statin non-users (ie, between-subject design), adjusted (aOR) for the above potential confounders. Multiple imputation by chained equations was employed for missing data: for each imputation, 10 imputed datasets were generated, and coefficient estimates across these were pooled using Rubin’s rule to calculate results for the primary full-set analysis (FSA, including imputed data).

As a sensitivity analysis, we reported results for the complete-case analysis (CCA), which does not include imputed data and only accounts for cases with no missing variables. Further, FSA data for statins were compared with those of the regression analyses for aspirin to probe whether results were non-specifically associated with another medication with comparable indication (ie, prevention and treatment of CVD) in a similar population.

All statistical analyses were conducted on Stata MP V.16.0.24

Findings

Study cohort

The cohort construction is in figure 1. The QResearch dataset included the electronic health records of 25 852 019 people registered with eligible general practices in England between 1 January 1998 and 15 August 2020 for at least 12 months. After the application of inclusion/exclusion criteria, the study cohort comprised 1 050 105 patients with a diagnosis of first-episode depression: 90 094 statin users and 960 011 statin non-users.

Figure 1

Cohort construction flow chart.

Baseline characteristics of the study cohort are in table 1. Across the whole sample, 55.06% were classified as suffering from major depression, 37.08% from minor depression and 7.86% with another ‘Read code’ for depression; the average depression severity measured with PHQ-9 at baseline was 16.15 (±5.49, moderately severe depression) and 12.94 (±6.76, moderate depression) at 12-month follow-up. The majority of the sample self-identified with white ethnicity (63.68%) and resided in London (24.13%), North West (18.52%) or South Central (11.92%) areas. The most prescribed antidepressants were SSRIs (54.94%), while antihypertensives (9.00%), hypnotics (6.68%) and contraceptives (6.00%) were the most common co-prescriptions. Compared with non-users, statin users included more males (males: 41.21% vs 57.84%), were older (mean age: 40.90 years vs 68.16 years), had more physical health comorbidities (particularly cardiovascular, cerebrovascular, metabolic and neoplastic), reported an average lower score of PHQ-9 (16.30 vs 14.33) and were taking more non-psychiatric medications (on antihypertensives: 56.52% vs 4.54%; on aspirin: 39.86% vs 2.01%; on anticoagulants: 7.71% vs 0.79%) aside from oral contraceptives (0.25% vs 6.54%), but fewer antidepressants (on antidepressants: 65.24% vs 51.99%).

Table 1

Baseline characteristics of the study cohort

Missing data, imputed for the FSA, are in online supplemental file 6. PHQ-9 values were the least available (81.26% missing), followed by alcohol consumption (48.68% missing), ethnic group (24.97% missing) and BMI (20.70% missing).

Study outcomes

Tables reporting the number of events for all outcomes per study group are in online supplemental file 7. A total of 21 384 (2.04%) people died, while most (67.34%, N=707 111) experienced at least one adverse event during the 12 months of study follow-up. Respectively, we observed 262 110 (24.96%) records for any psychiatric symptom, 167 274 (15.93%) for anxiety, 19 291 (1.84%) for sleep disturbance, 8524 (0.81%) for memory impairment, 6707 (0.64%) for self-harm, 16 427 (1.56%) for suicidality, 561 (0.05%) for completed suicide and 2364 (0.23%) patients remitted from the depressive episode by study endpoint.

On the FSA (N=1 050 105) adjusted model (figure 2), statin use was associated with reduced all-cause mortality at all time points (aOR2months 0.66, 99% CI 0.60 to 0.72; aOR6months 0.66, 99% CI 0.61 to 0.72; aOR12months 0.67, 99% CI 0.65 to 0.73). A lower number of statin users experienced any adverse events at 2 and 6 months (respectively aOR2months 0.93, 99% CI 0.91 to 0.96; aOR6months 0.97, 99% CI 0.94 to 0.99), but not at 12 months (aOR12months 0.99, 99% CI 0.96 to 1.03). No differences were identified at any time point for any psychiatric symptom (range aOR2–12months 0.92–0.97), anxiety (range aOR2–12months 1.05–1.07), sleep disturbance (range aOR2–12months 1.05–1.16), memory impairment (range aOR2–12months 0.89–1.32), self-harm (range aOR2–12months 0.76–0.82), suicidality (range aOR2–12months 1.00–1.02), completed suicide (range aOR2–12months 0.54–0.82) or depression remission (range aOR2–12months 1.03–1.11).

Figure 2

Study outcomes, full-set analyses (N=1 050 105), adjusted model. Green: beneficial association, red: harmful association, grey: no association. For depressive episode remission, an aOR >1 favours statin users, while for all outcomes, an aOR <1 favours statin users. 2mo, 2 months; 6mo, 6 months; 12mo, 12 months; aOR, adjusted OR.

In statin users, results from the sensitivity analysis on the CCA (N=88 227) adjusted model also showed lower all-cause mortality (range aOR2–12months 0.70–0.78) and any adverse events (range aOR2–6months 0.92–0.97), but with wide CIs that crossed the line of no association. Consistently with the FSA, any psychiatric symptom (range aOR2–12months 0.98–0.99), anxiety (range aOR2–12months 1.02–1.04), sleep disturbance (range aOR2–12months 0.95–1.02), suicidality (range aOR2–12months 0.95–1.10), completed suicide (range aOR2–12months 0.33–0.83) and depression remission (range aOR2–12months 0.89–1.19) were not different. However, a decrease in self-harm episodes (aOR12months 0.25, 99% CI 0.08 to 0.73) and higher memory impairment (aOR12months 1.13, 99% CI 1.04 to 1.23) in statin users at 12 months only was observed (tables including all analyses (FSAs and CCAs, both adjusted and unadjusted) are in online supplemental file 8).

Outcomes for the sensitivity analysis on aspirin (online supplemental file 9) only partially overlapped with those of statins: aspirin use was associated with worse all-cause mortality at 12 months (aOR12months 1.15, 99% CI 1.07 to 1.24) and adverse events at all time points (aOR2months 1.07, 99% CI 1.07 to 1.11; aOR6months 1.12, 99% CI 1.07 to 1.17; aOR12months 1.18, 99% CI 1.12 to 1.24), though also fewer anxiety reports over the follow-up period (aOR2months 0.90, 99% CI 0.84 to 0.96; aOR6months 0.91, 99% CI 0.86 to 0.97; aOR12months 0.91, 99% CI 0.85 to 0.96).

Discussion

This study examined an array of safety outcomes associated with statins in a large cohort of 1 050 105 patients with a new diagnosis of depressive disorder followed up for 12 months in real-world conditions. The FSA-adjusted model showed that statin use, compared with non-use, was associated with lower all-cause mortality and at least comparable risk of adverse events over the follow-up period. Results differed from those of the sensitivity analysis on aspirin use, which instead displayed higher mortality rates and adverse events compared with aspirin non-use. No differences for any neuropsychiatric adverse events were observed between statin users and non-users. A sensitivity analysis of the 88 227 cases with no missing data (CCA) supported the latter lack of associations but for lower self-harm and higher memory impairment at 12 months, and was linked with lower risk of mortality and total adverse events, although not statistically significant, which was likely due to the smaller sample size.

All-cause mortality

While the benefit of statins on all-cause mortality in the general population is being re-examined,3 9 10 we found a relative odds reduction between 33% and 34% across all time points in this large sample of primary care patients with depression. This finding has relevance to public health in the context of the 10–25 years of ‘mortality gap’, largely driven by physical comorbidities, in people with mental illness including depressive disorders.7 8 The updated tool for CVD risk scoring (QRISK3) now comprises items regarding the presence of SMI and the use of atypical antipsychotics. SMI usually involves schizophrenia, bipolar disorder and other psychoses, which tend to be the focus of CVD risk prediction studies.25 However, the QRISK3 development and validation cohort of people with SMI also included a high proportion of patients with moderate and severe depression (81.34%),26 which does not reflect the definition used in primary care electronic clinical systems.3 NICE concludes that QRISK3 should be used for people with ‘however defined severe mental illness’ and that clinical judgement should guide risk interpretation.3 Our findings that statin use is associated with reduced all-cause mortality in people with depressive disorders support the inclusion of depression within the ‘severe mental illness’ item of CVD risk prediction tools used in primary care, such as QRISK3, and call for an update of relevant UK government reports regarding the definition of physical health comorbidities and SMI,6 in line with other countries such as New Zealand.25 Specialised psychiatry services may consider implementing routine CVD risk screening for all patients diagnosed with depression within the at-risk age range of 40–74 years old,27 and regular cardiometabolic monitoring of individuals diagnosed with depressive disorders may be appropriate, as it is the case for other SMIs. More research is needed to understand and overcome potential barriers to statins’ uptake in people with depression.12

Overall, statins could helpfully treat or prevent cardiovascular and cerebrovascular conditions, thus lowering premature mortality in individuals with depression who are more at risk due to poor dietary habits and sedentary behaviour.7 8 In our study, this association was evident over a follow-up of 12 months, but statins are usually taken lifelong. An earlier epidemiological study of incident SSRI users (as compared with our sample of patients diagnosed with depression) with a follow-up of 642 058 person-years did not identify any association between concomitant SSRI and statin use, compared with SSRI use alone and changes in all-cause mortality (N=872 216, adjusted HR 1.04, 95% CI 0.96 to 1.12),28 which highlights the need for longer studies to corroborate our observations.

Adverse events

Findings for adverse events, which were lower in statin users compared with non-users, confirm the safety of statins in the general population, while also raising the possibility of a short-term protective association in this sample of people with depression. In line with this, a meta-analysis of randomised controlled trials in depressed participants had not observed any difference between statin treatment and placebo on adverse events (N=289, relative risk 1.07, 95% CI 0.66 to 1.73).29

In our sample of depressed participants, we did not find evidence either confirming or refuting an association between statin use and neuropsychiatric adverse events (including anxiety, sleep disturbance, self-harm and suicidal behaviour, memory impairment) or remissions of the depressive episode. In contrast with some preclinical evidence raising concerns about possible anxiogenic properties of statins,19 our results for anxiety align with those of other clinical studies that had not found these deleterious effects.30 The commonly reported sleep abnormalities associated with statins19 were not seen in this subgroup of individuals diagnosed with depression, therefore more likely to experience sleep difficulties. Likewise, the lack of association between statins and self-harming or suicidal behaviour, in a population who is more susceptible to experience these, further reduces previous concerns about increased impulsivity and suicidality in statin users.31 In fact, the sensitivity analysis on complete cases only (CCA) suggested that self-harm at 12 months was lower in depressed subjects using statins, which is in keeping with similar results previously described in patients with schizophrenia and bipolar disorder.32 Similar caution should be applied to the isolated finding that memory impairment was worse for statin users on the sensitivity CCA at 12 months. While more evidence is being gathered on this matter, with not always consistent results,14 some concerns about the potentially harmful effects of statins on cognitive function persist.

Regarding depressive episode remission, other epidemiological studies have thus far provided conflicting results, including higher (N=7 481 000, OR 1.22, 95% CI 1.20 to 1.25)33 or lower (N=1 149 384, HR 0.91, 95% CI 0.88 to 0.94)30 depression risk in individuals taking statins. Aside from differences in their design, inconsistencies among all these findings might be explained by the selection of different study populations and endpoints as well as difficulties in controlling for possible confounders due to the lack of detailed information about the sample characteristics in the datasets. Moreover, unlike our present study, none of these other investigations had been specifically conducted on people with a primary diagnosis of depression but probed a general population of statin users.

Limitations

Due to the observational design of this study, a lower internal validity can be anticipated as compared with an equivalent randomised controlled trial. We divided patients in an exposed and a comparison group depending on statin use at baseline; therefore, statin prescription had not been initiated at the time of entry in the study cohort (ie, when a new diagnosis of depression occurred). It could have occurred and stopped before study entry in statin non-users and may have been interrupted at any time point, as we followed an intention-to-treat principle (see protocol in online supplemental material 1)—these factors may however be responsible of selection bias. An alternative design that could be usefully employed in further studies would involve the identification of incident statin users in this population with first-episode depression and the use of a target trial emulation framework. Further, as for all analyses of electronic health records, undercoding/miscoding may occur, though the use of Read codes is established for studies on QResearch.17 Several baseline differences (eg, age, sex, comorbidities and concomitant medication use) could be observed between the two study cohorts, as expected for a comparison between statin users versus non-users; therefore, comparisons between these groups are challenging. However, our large and heterogeneous study population can ensure a wide overlapping across confounders, which supports the use of multiple logistic regression to control for these variables. We could not perform an additional propensity score matching analysis since this would not allow to use our imputation procedure,34 which may itself introduce bias. For depression severity (ie, PHQ-9 scores), alcohol use, ethnicity and BMI, a significant amount of data was missing and had to be imputed on the FSA. Specifically, PHQ-9 scores were only available for a minority of the sample (online supplemental material 6), and the large imputation procedure may have not fully captured and thus adequately adjusted for the severity of the depressive episode on the FSA. Altogether, these factors can lead to confounding by indication, which we attempted to control via multivariable logistic regressions that adjust for numerous potentially confounding variables.21 However, confounding variables may have differed between the physical and mental health outcomes measured. Furthermore, residual confounding remains a possibility for this study design. Because confounding cannot be completely removed, the higher short-term mortality in non-statin users versus statin users could be attributed to more deaths due to newly diagnosed depression rather than deaths due to CVDs or statins. Overall, limitations of the available database and of the study design employed advise caution in the interpretation of all our findings, and further confirmatory studies are necessary.

On the other hand, we could conduct a real-world assessment of the adverse outcomes associated with statin use in a large population of people with depression—including those with multiple comorbidities and co-occurring treatments oftentimes excluded from clinical trials, thus increasing the external validity of our results. However, statins are generally prescribed lifelong in the UK (https://www.nhs.uk/conditions/statins/); hence, it is possible that certain long-term benefits or harms would have not been observable during the 12-month follow-up. Similarly, our findings cannot be generalised beyond 12 months. We recognise that all-cause mortality measured within a 12-month time frame could be considered an uncommon occurrence; however, given the sizeable and diverse study cohort, we were still able to describe and analyse such rare event.

The primary safety outcomes (ie, all-cause mortality and proportion of participants with at least one adverse event) were assessed at three different time points (ie, at 2, 6 and 12 months) on the FSA, for a total of six main comparisons. Our assessment of the association estimates was conservative, since we used 99% CIs compared with more commonly reported 95% ones, in view of the large study sample and the several other comparisons for secondary outcomes and sensitivity analyses. Multiple comparisons might lead to an inflation of falsely positive results, but this possibility seems less relevant in the context of our findings generally showing little to no difference between the study groups on most of the additional analyses, while correcting for multiple comparisons would have spuriously lessened the chances of highlighting increases in adverse events. We did not use a time-to-event analysis, such as Cox proportional-hazard model, because the proportional-hazard assumption for the outcomes measured was not plausible when checked against available data. We used instead multiple logistic regression at prespecified time points, which does not rely on those assumptions while also allowing comparison with previous clinical trials.29

Our study focused on a homogeneous sample of people with a first episode of depression, often seen within primary care. It does not provide evidence, however, for those patients who have had several depressive episodes and trialled different courses of antidepressants—a condition known as ‘treatment-resistant depression’. Further research is needed to inform the prescription of statins in this population. Also, we did not assess for potentially diverse adverse event profiles associated with the use of different statins and concomitant medications. Clinical and preclinical evidence suggests that the effects of statins differ both centrally and peripherally depending on their lipophilicity19; therefore, our findings are not conclusive with regard to any individual statin, co-occurring drug use and their interactions.

Clinical implications

This real-world, population-based cohort study found that statins are associated with increased adverse events or overall mortality in people with depressive disorder. Taken together, our results do not substantiate prior concerns about statin-associated adverse outcomes.20 Instead, they contribute to a clearer evidence base which, if supported by further randomised studies, can inform the discussion between clinicians and people with depression about the risk/benefit balance of initiating statin treatment, in agreement with updated NICE guidelines.3

Data availability statement

Data may be obtained from a third party and are not publicly available. To guarantee the confidentiality of personal and health information, only the authors have had access to the data during the study in accordance with the relevant licence agreements. Access to the QResearch data is according to the information on the QResearch website (https://qresearch.org/).

Ethics statements

Patient consent for publication

Ethics approval

This study involves human participants and was independently reviewed and approved by the QResearch scientific committee (18/EM/0400). Participants gave informed consent to participate in the study before taking part.

References

Footnotes

  • X @rdegiorgi, @EGOstinelli, @And_Cipriani

  • Contributors RDG, FDC and AC conceived the study and acquired funding for it. RDG and FDC developed the study methodology, collected the data, conducted the study analyses and investigated its findings. AC, SF, PC, CJH and EGO validated the data, supported with the interpretation of the findings and supervised the overall project. RDG drafted the manuscript and designed the figures and tables. RDG is guarantor.

  • Funding The study was funded by the Wellcome Trust (grant 216452/Z/19/Z to RDG) and the National Institute for Health Research (grant RP-2017-08-ST2-006 to AC).

  • Disclaimer The funders did not have any role in the study design, in the collection, analysis and interpretation of data, in the writing of the report, and in the decision to submit the article for publication. The study authors are independent from the funders, they had full access to all the data (including statistical reports and tables), they are responsible for the integrity of the data and the accuracy of the data analysis, and they accept responsibility to submit for publication. The views expressed are those of the authors and not necessarily those of the Wellcome Trust, the NIHR, the MRC, the UK NHS or the UK Department of Health.

  • Competing interests All authors have completed the ICMJE uniform disclosure form at http://www.icmje.org/disclosure-of-interest/ and declare the following: RDG is supported by the Wellcome Trust (award 102176/Z/13/Z, grant 216452/Z/19/Z, title 'The effects of anti-inflammatory drugs on emotional and reward processing'). FDC is supported by the National Institute for Health Research (NIHR) Research Professorship to AC (grant RP-2017-08-ST2-006) and by the NIHR Oxford Health Biomedical Research Centre (grant BRC-1215-20005). EGO is supported by the NIHR Research Professorship to AC (grant RP-2017-08-ST2-006). PC is supported by the Medical Research Council (MRC) (grant MR/S003037/1, title 'Clinical Psychopharmacology of Depression'). CJH is supported by the NIHR Oxford Health Biomedical Research Centre. SF is supported by the NIHR Oxford Health Biomedical Research Centre. AC is supported by the NIHR Oxford Cognitive Health Clinical Research Facility, by an NIHR Research Professorship (grant RP-2017-08-ST2-006), by the NIHR Oxford and Thames Valley Applied Research Collaboration, by the NIHR Oxford Health Biomedical Research Centre (grant BRC-1215-20005) and by Wellcome Trust (GALENOS Project). CJH has received consultancy fees from P1vital, Lundbeck, Servier, UCB, Zogenix, J&J and Syndesi outside of the current work. AC has received research and consultancy fees from INCiPiT (Italian Network for Paediatric Trials), CARIPLO, Lundbeck and Angelini Pharma outside of the current work. The other authors declare that they have no conflict of interest.

  • Provenance and peer review Not commissioned; externally peer reviewed.

  • Supplemental material This content has been supplied by the author(s). It has not been vetted by BMJ Publishing Group Limited (BMJ) and may not have been peer-reviewed. Any opinions or recommendations discussed are solely those of the author(s) and are not endorsed by BMJ. BMJ disclaims all liability and responsibility arising from any reliance placed on the content. Where the content includes any translated material, BMJ does not warrant the accuracy and reliability of the translations (including but not limited to local regulations, clinical guidelines, terminology, drug names and drug dosages), and is not responsible for any error and/or omissions arising from translation and adaptation or otherwise.