http://orcid.org/0000-0002-5896-4852
Figures
Abstract
Background
Current heart failure (HF) guidelines recommend titrating angiotensin-converting enzyme inhibitors (ACEIs)/angiotensin receptor blockers (ARBs) and beta-blockers (BBs) to target doses used in pivotal placebo-controlled randomized controlled trials (RCTs). Despite a number of RCTs comparing different doses (i.e. higher versus lower doses) of ACEIs, ARBs and BBs, the effects of higher versus lower doses on efficacy and safety remains unclear. For this reason, we performed a systematic review and meta-analysis to evaluate the efficacy and safety of higher versus lower doses of ACEIs, ARBs and BBs in patients with HFrEF.
Methods
We searched MEDLINE, Embase and the Cochrane Central Register of Controlled Trials (CENTRAL) via Ovid from inception to April 25th, 2018 and opentrials.net and clinicaltrials.gov for relevant trials that compared different doses of medications in heart failure. We analyzed trials by drug class (ACEIs, ARBs, and BBs) for efficacy outcomes (all-cause mortality, cardiovascular mortality, all-cause hospitalizations, HF hospitalizations, HF worsening). For safety outcomes, we pooled trials within and across drug classes.
Results
Our meta-analysis consisted of 14 RCTs. Using GRADE criteria, the quality of evidence for ACEIs and ARBs was assessed as generally moderate for efficacy and high for adverse effects, whereas overall quality for BBs was very low to low. Over ~2–4 years higher versus lower doses of ACEIs, ARBs or BBs did not significantly reduce all-cause mortality [ACEIs relative risk (RR) 0.94 (95% confidence interval 0.87–1.02)], ARBs RR 0.96 (0.87–1.04), BBs RR 0.25 (0.06–1.01)] or all cause hospitalizations [ACEIs relative risk (RR) 0.94 (95% confidence interval 0.86–1.02)], ARBs RR 0.98 (0.93–1.04), BBs RR 0.93 (0.39–2.24)]. However, all point estimates favoured higher doses. Higher doses of ARBs significantly reduced hospitalization for HF [RR 0.89 (0.80–0.99)– 2.8% ARR], and higher doses of ACEIs and ARBs significantly reduced HF worsening [RR 0.85 (0.79–0.92)– 5.1% ARR and 0.91 (0.84–0.99)– 3.2% ARR, respectively] compared to lower doses. None of the differences between higher versus lower doses of BBs were significant; however, precision was low. Higher doses of these medications compared to lower doses increased the risk of discontinuation due to adverse events, hypotension, dizziness, and for ACEIs and ARBs, increased hyperkalemia and elevations in serum creatinine. Absolute increase in harms for adverse effects ranged from ~ 3 to 14%.
Conclusions
Higher doses of ACEIs and ARBs reduce the risk of HF worsening compared to lower doses, and higher doses of ARBs also reduce the risk of HF hospitalization but the evidence is sparse and imprecise. Higher doses increase the chance of adverse effects compared to lower doses. Evidence for BBs is inconclusive. These results support initially always starting at low doses of ACEIs/ARBs and only titrating the dose up if the patient tolerates dose increases.
Citation: Turgeon RD, Kolber MR, Loewen P, Ellis U, McCormack JP (2019) Higher versus lower doses of ACE inhibitors, angiotensin-2 receptor blockers and beta-blockers in heart failure with reduced ejection fraction: Systematic review and meta-analysis. PLoS ONE 14(2): e0212907. https://doi.org/10.1371/journal.pone.0212907
Editor: Vinayak Shenoy, California Health Sciences University, UNITED STATES
Received: June 22, 2018; Accepted: February 12, 2019; Published: February 28, 2019
Copyright: © 2019 Turgeon et al. This is an open access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
Data Availability: All data is contained within the paper.
Funding: The authors received no specific funding for this work.
Competing interests: The authors have declared that no competing interests exist.
Introduction
Heart failure (HF) with reduced ejection fraction (HFrEF) is a prevalent condition with an overall poor prognosis.[1] The combination of an angiotensin-converting enzyme inhibitor (ACEI) or angiotensin-2 receptor blocker (ARB) plus a beta-blocker (BB) is first-line therapy for HFrEF management,[1],[2] as these medications reduce morbidity and mortality compared to placebo.[3],[4],[5] These results have led guideline authors to universally recommend starting these agents in most patients with (HFrEF).[1],[2]
The approach recommended by guidelines when initiating these medications is to start at a low-to-moderate dose and titrate as tolerated to the target doses used in placebo-controlled randomized controlled trials (RCTs).[1],[2] However, many patients are unable to achieve and maintain target doses due to adverse effects, with most patients only achieving ~50% of the target dose.[6] Despite a number of RCTs comparing different doses (i.e. higher versus lower doses) of ACEIs, ARBs and BBs, the effects of higher versus lower doses on efficacy and safety remains unclear. For this reason, we performed a systematic review and meta-analysis to evaluate the efficacy and safety of higher versus lower doses of ACEIs, ARBs and BBs in patients with HFrEF.
Methods
Design
Systematic review with meta-analysis in accordance with the Preferred Reporting Items for Systematic reviews and Meta-Analyses (PRISMA) statement.[7]
Search strategy
We searched MEDLINE, Embase and the Cochrane Central Register of Controlled Trials (CENTRAL) via Ovid from inception to April 25th, 2018 using keywords and subject headings for the following concepts: heart failure, ACEI, ARB, BB, dose, and randomized controlled trial (see S1 Appendix for MEDLINE search strategy). We also searched opentrials.net and clinicaltrials.gov for relevant RCTs, and hand-searched bibliographies of included studies.
Eligibility criteria and outcomes
We included parallel RCTs published in English evaluating different doses of the same drug within the class of ACEIs, ARBs, or BBs in patients with HFrEF as defined by study investigators. Eligible trials needed to report results for at least one of the following outcomes: all-cause mortality, cardiovascular mortality, all-cause hospitalizations, HF hospitalizations, HF worsening, serious adverse events, discontinuation due to adverse events, hypotension, lightheadedness/dizziness, hyperkalemia, renal dysfunction, and cough. While there is evidence some of these drug classes have dose-related hemodynamic and neurohormonal effects, we chose to only include trials whose clinical outcomes would likely be relevant to clinicians and patients.
Study selection and data collection
Three authors (MK, PL, JM) screened candidate articles for inclusion, identified missing data, and consulted original publications. The same authors individually extracted crude outcome data from full-text reports into a standardized database. For trials comparing >2 doses, we included the results from only the lowest and highest dose arms, hereafter referred to as “higher dose” and “lower dose”. Discrepancies and missing data were resolved by group discussion, reference to the original publication, and additional independent adjudication by all authors.
Risk of bias and quality of evidence assessment
Two authors (JM, PL) assessed individual trials for risk of bias using the Cochrane Collaboration Risk of Bias Tool.[8] For each trial, we classified trials as being at low, high, or unclear risk of bias in each of 5 domains: sequence generation, allocation concealment, blinding of participants and personnel, blinding of outcome assessors and incomplete outcome data. Disagreements were resolved by consensus with a third author (RT). We also rated the quality of evidence for individual outcomes from high to very low based on Grading of Recommendations Assessment, Development and Evaluation (GRADE) methodology, which incorporates risk of bias, consistency, directness, precision, and other considerations.[9]
Synthesis of results and assessment of heterogeneity
We performed all analyses using Review Manager 5.3 (Cochrane Collaboration). We pooled trials by drug class studied at the study level and calculated risk ratios (RRs) with 95% confidence intervals (CIs), and absolute risk difference per 1000 patients treated over the follow-up period. For efficacy outcomes, we analyzed trials by drug class (ACEIs, ARBs, and BBs). For safety outcomes, we pooled trials within and across drug classes. All comparisons used high dose as the experimental intervention and low dose as the control intervention. We evaluated for statistical heterogeneity by visually inspecting forest plots and by calculating the I2 statistic. For efficacy outcomes, we reported fixed-effects model results for analyses with I2<50% and the random-effects model results for an I2≥50%. We reported all safety outcomes using fixed-effects models to minimize type 2 error.
Results
Included studies
From 1923 articles identified, we included 14 RCTs with sample size ranging from 83 to 3846 participants (Fig 1). We identified evidence for the following interventions: ACEIs (7 studies, n = 5,817),[10],[11],[12],[13],[14],[15],[16] ARBs (3 studies, n = 4,908),[17],[18],[19] and BBs (4 studies, n = 1,018).[20],[21],[22],[23]
Characteristics of included trials
Table 1 summarizes key characteristics of the included trials. At baseline, the mean age across trials ranged from 54–70 years, approximately 75% of participants were male, and the majority had NYHA functional class 2 or 3 symptoms. Twelve trials required reduced ejection fraction (EF) at baseline, ranging from <30% to <50%. Eight trials compared >2 doses; seven studies (50%) compared a 4-fold increase in dose (between the groups receiving the lowest and highest dose), 4 studies (29%) compared 7 to 16-fold differences in doses, and three studies (21%) compared a 2 to 3-fold difference in dose. The weighted mean follow-up duration across included studies was 34 months (ACEIs 28 months, ARBs 45 months, BBs 17 months). Three studies that accounted for 63% of patients in this meta-analysis had follow-up greater than 12 months.[10],[18],[21]
Risk of bias and quality assessment
All trials except the HEAAL study had high or unclear risk of bias in at least 3 of the 5 domains (Fig 2). Quality of evidence for ACEIs and ARBs was generally moderate for efficacy and high for adverse effects, whereas overall quality for BBs was very low to low. Table 2 lists the quality of evidence for each outcome and reasons for downgrading. We did not assess for publication bias as the number of studies for each meta-analysis was insufficient according to accepted criteria.[24]
Statistically significant results are shown in bold text.
Efficacy
Figs 3–7 illustrate the meta-analyses for efficacy outcomes, and Table 2 summarizes the absolute and relative estimates for efficacy. Post-hoc analyses pooling studies of ACEIs and ARBs are shown in Figs 8 and 9.
Adverse effects
Figs 10–15 illustrate the meta-analyses for adverse effects, and Table 2 summarizes the absolute and relative estimates for adverse effects.
Discussion
In this systematic review and meta-analysis of RCTs, higher doses of ACEIs were not statistically superior to the lower doses studied in terms of mortality or hospitalizations, but point estimates were in favour of higher doses. Higher doses of ACEIs statistically-significantly reduced the proportion of patients with episodes of worsening HF compared to lower doses. Similarly, higher doses of ARBs did not statistically reduce mortality or all-cause hospitalizations compared to lower doses, but point estimates were again in favour of higher doses. However, higher doses of ARBs did statistically reduced HF hospitalization and episodes of worsening HF compared to the lower doses studied. We did not find statistically-significant differences between higher and lower doses of BBs for any efficacy outcome, though results were imprecise due to few events, limiting the certainty of these findings. Higher doses increased the risk of discontinuation due to adverse events, hypotension, dizziness, and for ACEIs and ARBs, increased hyperkalemia and elevations in serum creatinine compared to lower doses.
Based on these pooled results, treating 1000 patients with higher versus lower doses of ACEIs over a mean of 28 months would result in 51 fewer patients experiencing worsening HF and 23 fewer patients experiencing cough (possibly related to the lower incidence of worsening HF). These benefits would be offset by 30–51 more patients experiencing hypotension or dizziness, and 24–27 patients having laboratory abnormalities including hyperkalemia or an increase in serum creatinine. Treating 1000 patients with higher versus lower doses of ARBs over a mean of 45 months would lead to 28–32 fewer cases of HF hospitalization or worsening, 27 more patients experiencing symptomatic hypotension, 33 more patients with hyperkalemia and 62 more patients with increased serum creatinine. For BBs the data is too imprecise to estimate efficacy, but suggest 142 more cases of dizziness per 1000 patients treated with higher doses versus lower doses over 17 months.
Our results differ somewhat from those of a recent meta-analysis comparing higher versus lower doses of ACEIs/ARBs by Khan et al.[25] These authors reported that when the data from trials evaluating ACEIs and ARBs are combined, higher doses showed a reduced risk of all-cause mortality, but no difference in hospitalizations for HF or discontinuations due to adverse effects when compared to lower doses [25] Our meta-analysis included 4 additional trials not included in the Khan meta-analysis. In our post-hoc analysis pooling ACEIs plus ARBs for the outcome of all-cause mortality, we did not find a statistically significant difference between higher and lower doses. However, our results are quantitatively nearly identical (confidence interval 0.89–1.01 versus 0.89–1.00), and the apparent difference in the report of findings can be solely explained by dogmatic adherence to arbitrary dichotomous statistical significant thresholds.[26] Finally, for safety outcomes we used fixed-effects meta-analyses to minimize type 2 error which might account for some of the differences reported.
Applying the evidence
Given that the benefit of ACEIs, ARBs and BBs accrue over months, yet adverse effects typically occur early after starting or increasing doses, clinicians should initiate these agents at a low dose and titrate them gradually while assessing tolerability. American and Canadian HFrEF guidelines recommend this approach, with a goal of titrating the dose every 2–4 weeks as an outpatient to target doses used in the landmark placebo-controlled trials.[1],[2] Missing from these guidelines, however, is a discussion of the benefits and harms of dose titration. Ideally, HF guidelines would stress the important role that shared decision-making plays in this process, particularly when a patient experiences adverse effects and must decide on the value of maintaining their current dose or continuing to up-titrate. Clinicians can use the results of this review, as summarized in Table 2, to discuss what is known about the benefits and harms of higher versus lower doses of these agents, as well areas of uncertainty about clinically-important outcomes.
Limitations
Our meta-analysis has limitations stemming primarily from the included trials. First, included trials did not always report all outcomes of interest, especially for BBs, limiting available data and decreasing the certainty in pooled estimates. Furthermore, trials seldom reported the definitions for adverse effects such as hypotension and increase in serum creatinine, and it is therefore difficult to put their clinical significance into context without knowledge of their severity or consequence. Second, the ranges of doses studied varied widely between trials, limiting our ability to evaluate any specific dose intensity or compare lower doses to “target doses” recommended by guidelines. Additionally, for trials evaluating more than two dosages, we selected the highest and lowest daily doses for the intervention and control group, respectively, for our analyses. For instance, in one trial the higher-dose arm received enalapril 10 mg daily, which is a quarter of the maximum approved dose for this indication (40 mg) and half the recommended target dose, whereas in another the lower-dose arm received enalapril 20 mg daily (the recommended target dose) and the higher-dose arm received 60 mg daily (triple the target dose). Finally, we could not reliably assess for publication bias as there were too few studies (<10 trials) in each meta-analysis.[24]
Conclusion
Evidence comparing lower and higher doses of drugs in HFrEF is sparse and imprecise. Higher doses of ACEIs and ARBs reduce the risk of HF worsening compared to lower doses, and higher doses of ARBs also reduce the risk of HF hospitalization. Effects of higher versus lower doses of these agents on other outcomes, as well as the impact of higher versus lower doses of BBs on any efficacy outcome, remain unclear. Higher doses importantly increase the risk of hypotension and agent-specific adverse effects (e.g. hyperkalemia, cough, creatinine rise) compared to lower doses. These results reinforce recommendations to start these agents at low doses, involve patients in dose titration decisions, carefully monitor for adverse effects after dose changes, and not be averse to lowering doses when tolerability issues arise.
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