Abstract
Background
We evaluated the burden of adverse events caused by β-blocker use after acute myocardial infarction (AMI) in frail, older nursing home (NH) residents.
Methods
This retrospective cohort study used national Medicare claims linked to Minimum Data Set assessments. The study population was individuals aged ≥65 years who resided in a U.S. NH for ≥30 days, had a hospitalized AMI between May 2007 and March 2010, and returned to the NH. Exposure was new use of β-blockers versus nonuse post-AMI. Orthostasis, general hypotension, falls, dizziness, syncope, and breathlessness outcomes were measured over 90 days of follow-up. Odds ratios (ORs) with 95% confidence intervals (CIs) for outcomes were estimated using multinomial logistic regression models after 1:1 propensity score-matching of β-blocker users to nonusers.
Results
Among the 10,992 NH propensity score-matched residents with an AMI, the mean age was 84 years and 70.9% were female. β-blocker users were more likely than nonusers to be hospitalized for hypotension (OR = 1.20, 95% CI 1.03–1.39) or experience breathlessness (OR = 1.10, 95% CI 1.01–1.20) after AMI. With the exception of falls, other outcome estimates, though imprecise, were compatible with a potential elevated risk of orthostasis (OR = 1.14, 95% CI 0.96–1.35), syncope, (OR = 1.24, 95% CI 0.55–2.77), and dizziness (OR = 1.28, 95% CI 0.82–1.99) among β-blocker users.
Conclusions
Considered alongside prior evidence that β-blockers may worsen functional outcomes in NH residents with poor baseline functional and cognitive status, our results suggest that providers should exercise caution when prescribing for these vulnerable groups, balancing the mortality benefit against the potential for causing adverse events.
Keywords: Nursing homes, Adrenergic beta-antagonists, Myocardial infarction, Activities of daily living, Drug-related side effects and adverse reactions
β-blockers are recommended for all adults without a contraindication after an acute myocardial infarction (AMI) (1,2). However, β-blockers may have side effects like hypotension and fatigue, which are particularly detrimental to frail, older adults (3,4). These adverse events (AEs) could, in part, explain the results from a recent study that found an association between β-blocker use and functional decline in nursing home (NH) residents after AMI (5). Regardless, symptoms and AEs of cardiovascular medications are often the outcomes that older adults notice and care about. Little is known about whether β-blockers cause these AEs in frail, older adults or the magnitude of these potential effects. Therefore, we used a unique national data set to evaluate the association between β-blockers and AEs that could result in functional decline among frail, older NH residents. We hypothesized that β-blockers would increase the risk of all AEs, including hypotension, syncope, dizziness, breathlessness, and falls.
Methods
Study Design and Data Source
We used a previously established national, retrospective cohort of NH residents who return to the NH after AMI (5). The data source was national Medicare data linked to the Minimum Data Set (MDS) version 2.0 and Online Survey Certification and Reporting System (OSCAR) data. The MDS is a quarterly assessment tool of resident characteristics that is required for all facilities that are certified to receive Medicare or Medicaid funding. The OSCAR data provides facility-level information on NH characteristics, staffing levels, and quality indicators. Medicare claims include information on inpatient care (Part A), outpatient care (Part B), and prescription drug dispensings (Part D). This study was approved by the institutional review boards of the University of California, San Francisco, and the Department of Veterans Affairs.
Study Population
Our study population consisted of U.S. NH residents aged 65 years or older who were hospitalized for AMI between May 1, 2007 to March 31, 2010; had resided in a NH for at least 30 days before AMI hospitalization; had not used a β-blocker for at least 4 months before hospitalization; and returned to the NH after hospital discharge. We defined hospitalization with AMI based on a Part A hospital claim with International Classification of Diseases, 9thRevision, Clinical Modification (ICD-9) code 410.XX or 411.1 as the primary or secondary diagnosis. Additional details about the study population have been previously published (5–8).
Exposures and Causal Contrast of Interest
Initiation of an oral β-blocker was ascertained using Medicare Part D claims. No prevalent (prior) β-blocker users were included. The causal contrast of interest was defined as the effect of initiating β-blocker versus not initiating β-blocker, regardless of subsequent treatment discontinuation or switching among treatment groups (ie, intention-to-treat).
Outcomes
We identified 90-day orthostasis and general hypotension outcomes using ICD-9 codes 458.0 and 458.XX, respectively, in any coding position on hospital claims (5). Falls were similarly identified using codes E880-E888 in any position on the Part A hospital claims. All coding positions were permitted because orthostasis, general hypotension, and falls are very rarely the principal cause for hospital admission. We ascertained 90-day dizziness, syncope, and breathlessness outcomes using checkboxes in Section J (Health Conditions) of the MDS version 2.0 assessments (5).
Baseline Characteristics
Potential common causes (or proxies of common causes) of β-blocker use and outcomes were prespecified based on existing literature (5,7,9–13) and measured prior to β-blocker use. Additional details about the measurement of baseline characteristics and which characteristics were included have been previously described (5). In brief, variables were measured in inpatient claims, outpatient claims, MDS records, and OSCAR data, and included demographic characteristics, medical history, medication use, risk factors for AMI, health services utilization, and NH facility characteristics (14). MDS data were used to generate several validated scales including the Cognitive Performance Scale (CPS), the Morris Activities of Daily Living (ADL) scale, and the Changes in Health, End-stage disease, Symptoms and Signs (CHESS) score, a measure of global prognosis.
Statistical Analyses
We adjusted for confounding by nearly 100 baseline covariates using methods that rely on estimating the propensity score (ie, the probability of receiving β-blocker vs not, conditional on covariates). Propensity scores were estimated using a logistic regression model. The model used restricted cubic splines with four knots for continuous variables and interaction terms wherever indicated based on prior literature (5,7,9–13). We included a pretreatment history of all AEs in the model. We also included concomitant medications that could be associated with the AEs, including antidepressants, opioids, sedative-hypnotics, antipsychotics, diuretics, and direct-acting vasodilators.
We used the propensity score to match one new user of β-blockers to one nonuser after the AMI. We applied a greedy 5-to-1 digit matching algorithm without replacement to do so. Propensity score distributions in each treatment group were examined using histograms and descriptive statistics. We used standardized mean differences after matching to assess covariate balance between treatment groups.
We estimated odds ratios (ORs) with 95% confidence intervals (CIs) using multinomial logistic regression models to compare β-blocker initiators to nonusers for all outcomes of interest while accounting for the competing risk of death.
In a noncausal preliminary analysis to begin to assess whether AE outcomes may have contributed to a previously observed association between β-blockers and functional decline (5), we estimated treatment effects within strata defined by post-AMI functional decline (had a 3-point increase on the 28-point MDS ADL scale vs did not). Specifically, we used a multinomial regression model with treatment (β-blocker initiation vs nonuse) term, post-AMI functional decline term, and a treatment × post-AMI functional decline term as independent variables.
Results
Study Cohort
Propensity score-matching yielded a cohort of 5,496 β-blocker users and an equal number of nonusers. The cohort had a mean (SD) age of 84 (8) years and 70.9% female. Of the 10,992 NH residents in the propensity score-matched cohort, 396 (3.6%) had a pre-β-blocker hospitalization with orthostasis, 526 (4.8%) with general hypotension, and 274 (2.5%) with falls; 109 (1.0%) individuals had a history of pretreatment dizziness, 30 (0.3%) had a history of syncope, and 916 (8.3%) has a history of breathlessness. Characteristics between β-blocker users and nonusers in the cohort were well-balanced after matching (Table 1). All standardized differences between treatment groups were ≤0.06. Further description of the cohort’s baseline characteristics has been previously published (5).
Table 1.
Characteristics of β-blocker Users and Nonusers After Propensity Score Matching
| n (%) | ||
|---|---|---|
| β-blocker Users (n = 5,496) | β-blocker Nonusers (n = 5,496) | |
| Age, mean (SD) years | 84 (8) | 84 (8) |
| Female sex | 3,901 (71.0) | 3,887 (70.7) |
| Race | ||
| Caucasian | 4,485 (81.6) | 4,497 (81.8) |
| African American | 644 (11.7) | 646 (11.8) |
| Other | 367 (6.7) | 353 (6.4) |
| Adverse events prior to AMI hospitalization | ||
| Breathlessness | 461 (8.4) | 455 (8.3) |
| Syncope | 15 (0.3) | 15 (0.3) |
| Dizziness | 54 (1.0) | 55 (1.0) |
| Falls | 124 (2.3) | 150 (2.7) |
| General hypotension | 264 (4.8) | 262 (4.8) |
| Orthostasis | 200 (3.6) | 196 (3.6) |
| ADL status prior to AMI hospitalization | ||
| Independent to limited assistance required | 1,834 (33.4) | 1,866 (34.0) |
| Extensive assistance required | 1,801 (32.8) | 1,778 (32.4) |
| Extensive dependency | 1,861 (33.9) | 1,852 (33.7) |
| Cognitive status prior to AMI hospitalization | ||
| Intact or borderline intact | 1,580 (28.8) | 1,585 (28.8) |
| Mild to moderate dementia | 3,294 (59.9) | 3,305 (60.1) |
| Moderately severe to very severe dementia | 622 (11.3) | 606 (11.0) |
| Chronic conditions prior to AMI hospitalization | ||
| Diabetes | 1,567 (28.5) | 1,582 (28.8) |
| Dyslipidemia | 297 (11.8) | 288 (11.9) |
| Hypertension | 3,055 (55.6) | 3,018 (54.9) |
| Renal failure | 297 (11.8) | 288 (11.9) |
| COPD | 1,498 (27.3) | 1,504 (27.4) |
| Heart failure | 2,554 (46.5) | 2,562 (46.6) |
| PVD | 409 (7.4) | 399 (7.3) |
| Number of medications prior to AMI hospitalization | 11 (8–15) | 12 (8–15) |
| Medication use prior to AMI hospitalization | ||
| Statins | 1,559 (28.4) | 1,580 (28.8) |
| Antiplatelets | 914 (16.6) | 916 (16.7) |
| Warfarin | 707 (12.9) | 723 (13.2) |
| Length of hospital stay for AMI, median (IQR) days | 6 (4–9) | 6 (4–9) |
| Number of days in ICU/CCU during AMI stay | ||
| None | 2,374 (43.2) | 2,361 (43.0) |
| 1–2 | 1,376 (25.0) | 1,396 (25.4) |
| 3 or more | 1,746 (31.8) | 1,739 (31.6) |
| PCI or CABG during AMI hospitalization | 126 (2.3) | 98 (1.8) |
Note: AMI = Acute myocardial infarction; ADL = Activities of daily living; CABG = Coronary artery bypass graft; HF = Heart failure; ICU/CCU = Intensive care unit/coronary care unit; IQR = Interquartile range; PCI = Percutaneous coronary intervention; PVD = Peripheral vascular disease; SD = Standard deviation.
Treatment Effects
After AMI, β-blocker users were more likely than nonusers to be hospitalized for hypotension (OR = 1.20, 95% CI 1.03–1.39) or experience breathlessness (OR = 1.10, 95% CI 1.01–1.20) (Table 2). With the exception of falls, other outcome estimates, though imprecise, were consistent with a potential elevated risk of orthostasis (OR = 1.14, 95% CI 0.96–1.35), syncope, (OR = 1.24, 95% CI 0.55–2.77), and dizziness (OR = 1.28, 95% CI 0.82–1.99) among β-blocker users.
Table 2.
Association of β-blocker Use Versus Nonuse With Potential Adverse Event Outcomes
| Adverse Event Outcome | Events, n | Risk, % | ||||
|---|---|---|---|---|---|---|
| β-blocker Users (n = 5,496) | β-blocker Nonusers (n = 5,496) | β-blocker Users | β-blocker Nonusers | OR (95% CI) | p Value | |
| Hypotension | 394 | 347 | 7.2 | 6.3 | 1.20 (1.03, 1.39) | .02 |
| Orthostatic Hypotension | 283 | 261 | 5.2 | 4.8 | 1.14 (0.96, 1.35) | .14 |
| Syncope | 13 | 11 | 0.2 | 0.2 | 1.24 (0.55, 2.77) | .60 |
| Dizziness | 44 | 36 | 0.8 | 0.7 | 1.28 (0.82, 1.99) | .27 |
| Breathlessness | 1,596 | 1,525 | 29.0 | 27.8 | 1.10 (1.01, 1.20) | .03 |
| Falls | 100 | 118 | 1.8 | 2.2 | 0.88 (0.68, 1.16) | .37 |
Note: CI = Confidence interval; OR = Odds ratio.
Stratification by Functional Decline
When the data were jointly stratified by post-AMI β-blocker use and functional decline, there was no evidence that the risk of AEs was substantially greater among those with β-blocker use and functional decline compared to those without (Table 3). This suggests that the AEs we evaluated were unlikely to be major mediators of the previously observed association between β-blockers and functional decline (5).
Table 3.
Risk (%) of Each Adverse Event Stratified by β-blocker Use and Functional Decline
| Adverse Event Outcome | Functional Decline (n = 1,328) | Alive With No Functional Decline (n = 8,201) | p Valuea | ||
|---|---|---|---|---|---|
| β-blocker users (n = 717) | β-blocker Nonusers (n = 611) | β-blocker users (n = 4,157) | β-blocker Nonusers (n = 4,044) | ||
| Hypotension | 7.4 | 7.3 | 7.1 | 6.1 | .55 |
| Orthostatic Hypotension | 5.1 | 4.9 | 5.0 | 4.6 | .88 |
| Syncope | 0.0 | <1.8b | 0.3 | <0.3b | .97 |
| Dizziness | <1.5b | <1.8b | 0.7 | 1.0 | .32 |
| Breathlessness | 30.1 | 29.3 | 26.5 | 26.2 | .88 |
| Falls | 1.6 | 2.0 | 1.8 | 2.1 | .95 |
a p value for whether the risk of an adverse event was different among β-blocker users versus nonusers for individuals with a functional decline versus without a decline;
bCells suppressed in compliance with the Centers for Medicare and Medicare Services Cell Size Suppression Policy stipulating that no cell can be reported that allows a value of 1 to 10 to be derived from other reported cells or information.
Discussion
In this retrospective cohort study, new use of β-blockers after AMI was associated with a slightly increased risk of hypotension and breathlessness in frail older adults, but not other AEs. Additionally, there was little evidence that potential AEs that we studied were likely to be responsible for the association between β-blockers and functional decline. Emerging evidence suggests that the benefits of β-blockers after AMI may be especially concentrated in individuals with reduced ejection fraction mediated by the AMI, and individuals with preserved ejection fraction may benefit less. Nonetheless, β-blockers remain the standard of care and are associated with reductions in mortality in the overall population of vulnerable older adults after AMI (5). For as long as β-blockers remain the standard of care, information on AEs that frail, older adults notice and care about is necessary to guide treatment decision-making.
Several pharmacokinetic and pharmacodynamic studies have suggested that frail older adults may experience more AEs from β-blockers, but few have examined the clinical significance of these findings in older adults by empirically examining outcomes (15). Meta-analyses of trials enrolling younger patients suggested that β-blockers were associated with dizziness, but conflicted on whether they were associated hypotension, breathlessness, or syncope (16,17).
Just one prior study examined the prevalence of orthostasis among NH residents and found that individuals with orthostasis received β-blockers more often than those without orthostasis (18). That study was not designed to analyze the effect of β-blockers on AEs, did not examine residents after AMI, and only examined orthostasis, but provides some of the only available prior evidence that a relationship may exist between β-blockers and important AEs among older NH residents. One other cross-sectional study using 2004 National Nursing Home Survey data found that β-blockers were associated with an increased likelihood of falls (OR = 1.14, 95% CI = 1.04–1.27), but the cross-sectional design precluded causal inference (19). Our study adds to the existing literature by providing the highest quality evidence to date on the relationship between β-blockers and AE outcomes among frail, older adults in NHs. In doing so, it provides information on outcomes that are important to a variety of geriatric healthcare professionals (3). Such information can be used to guide and support prescribing decisions in the NH setting.
Limitations of our study include the possibility of outcome misclassification due to a lack of validated outcome definitions for our data; the inability to look at fatigue and depression as outcomes despite their clinical importance; and the low incidence of the outcomes that limited our statistical power to detect a difference across subgroups of patient characteristics or by β-blocker type (ie, lipophilicity or cardioselectivity) (5). Another notable limitation of our study cohort was the lack of information on left ventricular ejection fraction (LVEF) since the data from younger individuals suggests that the mortality benefit is greatest for those with a LVEF of less than 40%. Due to the nature of our data, we were also unable to assess dose–response relationships with AE outcomes. Future studies using Veterans Affairs or other data should aim to address whether the harm-benefit balance of β-blockers in highly vulnerable older adults differs across strata of LVEF and by β-blocker dose.
Since this study is observational, we cannot rule out the possibility of confounding. In addition to the absence of information on LVEF, we were unable to accurately differentiate ST-elevation MI (STEMI) from non-ST-elevation MI (NSTEMI) or identify the infarct location. However, several factors support the robustness of our findings. First, our linked clinical and administrative databases provide detailed patient information beyond what is captured in administrative data alone. Second, we also obtained excellent balance on nearly 100 baseline covariates between treatment groups. We were also unable to assess whether AE outcomes differed between individuals who persisted with versus discontinued β-blockers. Such an analysis would likely be subject to substantial selection bias even with many covariates available for adjustment since β-blockers reduce the risk of mortality and death was the primary reason individuals “discontinued” β-blockers. Findings from previous work using our study cohort suggest that nearly all people in NHs who start on a β-blocker after AMI remain on them for at least the first 90 days, so questions about continuation versus discontinuation of β-blockers may be less relevant for NH residents in the immediate post-AMI period (5,7).
It is important to note that causal inference cannot be drawn from our analysis stratifying on post-AMI functional decline. Functional decline was not temporally ordered to occur after AEs and a formal causal mediation analysis was not conducted. The stratified analysis was only intended to provide preliminary information about the plausibility of the hypothesis that functional decline could be mediated by AEs. While there is not a strong empirical justification for proceeding with a formal causal mediation analysis, such future work could be conducted.
In summary, β-blockers were associated with a small relative and absolute increase in hypotension and breathlessness in frail older adults, but there was not strong evidence that these AEs mediate functional decline. Compared to younger individuals, frail, older adults often prioritize maintaining function and avoiding AEs, as opposed to maximizing longevity (20). We hope our results will encourage providers to consider the net benefit-harm balance when prescribing β-blockers to older adults. For the minority of patients and their caregivers who prefer to maximize longevity, our results should reassure them that the risk of AEs associated with starting β-blockers is modest. Nonetheless, the potential negative effects of β-blockers on functional outcomes in frail NH residents with poor baseline functional and cognitive status merit caution when prescribing for these vulnerable groups, balancing the mortality benefit against the potential for causing AEs (5).
Funding
Financial support for this study was provided by the National Institute on Aging (5R01AG045441; K24AG049057; and P30AG044281), the National Heart, Lung, and Blood Institute (5R01HL111032), the Agency for Healthcare Research and Quality (5K12HS022998), and the U.S. Department of Veterans Affairs.
Conflict of Interest
S.D.B. serves as an author for the “Falls” chapters in UpToDate and receives royalties from Wolters Kluwer for this. J.T. is a paid consultant for CVS Health. M.A.S. has served as a paid consultant for iodine.com. All other authors have no relevant conflicts of interest.
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