Figures
Abstract
Objective
Heart failure (HF) is an important covariate and outcome in studies of elderly populations and cardiovascular disease cohorts, among others. Administrative data is increasingly being used for long-term clinical research in these populations. We aimed to conduct the first systematic review and meta-analysis of studies reporting on the validity of diagnostic codes for identifying HF in administrative data.
Methods
MEDLINE and EMBASE were searched (inception to November 2010) for studies: (a) Using administrative data to identify HF; or (b) Evaluating the validity of HF codes in administrative data; and (c) Reporting validation statistics (sensitivity, specificity, positive predictive value [PPV], negative predictive value, or Kappa scores) for HF, or data sufficient for their calculation. Additional articles were located by hand search (up to February 2011) of original papers. Data were extracted by two independent reviewers; article quality was assessed using the Quality Assessment of Diagnostic Accuracy Studies tool. Using a random-effects model, pooled sensitivity and specificity values were produced, along with estimates of the positive (LR+) and negative (LR−) likelihood ratios, and diagnostic odds ratios (DOR = LR+/LR−) of HF codes.
Results
Nineteen studies published from1999–2009 were included in the qualitative review. Specificity was ≥95% in all studies and PPV was ≥87% in the majority, but sensitivity was lower (≥69% in ≥50% of studies). In a meta-analysis of the 11 studies reporting sensitivity and specificity values, the pooled sensitivity was 75.3% (95% CI: 74.7–75.9) and specificity was 96.8% (95% CI: 96.8–96.9). The pooled LR+ was 51.9 (20.5–131.6), the LR− was 0.27 (0.20–0.37), and the DOR was 186.5 (96.8–359.2).
Citation: McCormick N, Lacaille D, Bhole V, Avina-Zubieta JA (2014) Validity of Heart Failure Diagnoses in Administrative Databases: A Systematic Review and Meta-Analysis. PLoS ONE 9(8): e104519. https://doi.org/10.1371/journal.pone.0104519
Editor: Yiru Guo, University of Louisville, United States of America
Received: April 9, 2014; Accepted: July 10, 2014; Published: August 15, 2014
Copyright: © 2014 McCormick 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: The authors confirm that all data underlying the findings are fully available without restriction. All relevant data are within the paper and its Supporting Information files.
Funding: This study was funded in part by the Canadian Arthritis Network (http://www.canradnetwork.ca). Natalie McCormick is supported by a Doctoral Research Award from the Canadian Institutes of Health Research. J. Antonio Avina-Zubieta held a salary award from the Canadian Arthritis Network and The Arthritis Society of Canada. He is currently the British Columbia Lupus Society Scholar and holds a Scholar Award from the Michael Smith Foundation for Health Research. Diane Lacaille holds the Mary Pack Chair in Arthritis Research from UBC and The Arthritis Society of Canada. The funders had no role in study design, data collection and analysis, decision to publish, or preparation of the manuscript.
Competing interests: Vidula Bhole is the sole proprietor of a consulting company, EpiSolutions Consultancy Services. There are no patents, products in development or marketed products to declare. This does not alter the authors' adherence to all the PLOS ONE policies on sharing data and materials, as detailed online in the guide for authors.
Introduction
Heart failure (HF) is a chronic condition that affects about 26 million people worldwide [1] and imposes a tremendous burden on these individuals and their families. The typical 40 year-old faces a 20% lifetime risk of developing HF [2], and the incidence of HF amongst adults 65 years of age and older is approximately 12.5 per 1,000 person-years [3]. About half of new cases are expected to die within five years of diagnosis [2], and estimates of the annual economic burden of HF have recently exceeded $30 billion in the United States [2], and $108 billion worldwide [4].
The European Society of Cardiology describes HF as a disorder of cardiac structure or function where the heart is unable to deliver adequate levels of oxygen to the tissues [5]. Cases often have primary left systolic HF, which is characterized by “reduced contraction and emptying of the left ventricle” [5]. Still, many cases have left diastolic HF, in which ventricular compliance and filling are impaired [6] but the contractile function of the ventricle is preserved. HF has some ‘classic’ signs and symptoms, including ankle oedema, and exertional dyspnoea and fatigue [5], [6]. However, HF is not considered to be a discrete condition but a “complex clinical syndrome” [6] that occurs in conjunction with other cardiovascular diseases such as coronary artery disease, valvular heart disease, hypertension, dilated cardiomyopathy [6], and conduction and rhythm disorders [5]. A significant source of morbidity on its own, HF frequently occurs in concordance with other chronic disorders such as renal disease [7]–[9], chronic obstructive pulmonary disease (COPD) [8], [10]–[12], and diabetes [7]–[11]. Thus when evaluating treatments for these and other chronic conditions, it is essential to adjust for diagnoses of HF.
Administrative databases have become excellent resources for the study of HF by allowing for long-term evaluation of large numbers of patients at relatively low cost. Some examples are the Medicare databases in the United States (USA) and health ministry databases from countries such as Canada where healthcare is funded by provincial governments and available to all residents. These data sources allow the patient-level linkage of health resource utilization data (including hospital separations, outpatient encounters, and sometimes, dispensed prescriptions) to demographic and vital statistics data. When studying clinic-based populations, patients with severe HF are likely to be overrepresented, but administrative databases provide a means for identifying risk factors for HF, and quantifying the effects of treatment in unselected populations.
However, administrative databases are only useful for HF research if the diagnostic codes contained within are valid; that is, if they can be used to distinguish those who actually have HF from those who do not. Their validity can be assessed by comparing the administrative database diagnosis to an accepted ‘gold standard’ reference diagnosis. This diagnosis is typically obtained through more resource-intensive processes such as patient self-report, retrospective chart review, or prospective clinical examination. Principal measures of validity include sensitivity (how many HF cases in the population are actually coded for HF) and specificity (how many of the non-HF cases in the population are, in turn, not coded for HF). Unfortunately, there is some uncertainty surrounding the validity of diagnoses recorded in administrative databases since most databases are not established for research purposes. Validity is of particular concern when studying HF patients, as they tend to have high comorbidity burdens and be hospitalized for other cardiovascular and respiratory conditions [13], [14]. While HF may have contributed to the need for these hospitalizations, this diagnosis may not be entered on the discharge record, leaving this potential confounding variable to go undetected in subsequent epidemiologic investigations. Although several assessments of the validity of HF codes in administrative databases have been published [15]–[17], there is considerable heterogeneity amongst them with regards to the clinical settings and reference standards used. Of note, many of these assessments were limited to specific populations (e.g. those diagnosed with atrial fibrillation [15] or myocardial infarction (MI) [16]) so may not be generalizable to the HF diagnoses recorded for other individuals.
As a part of a Canadian Rheumatology Network for establishing best practices in the use of administrative data for health research and surveillance (CANRAD) [18]–[22], we have conducted a systematic review of studies reporting on the validity of diagnostic codes for identifying cardiovascular diseases (CVD) in administrative data. Data from these studies were used to compare the validity of these codes, and to evaluate whether administrative health data can accurately identify CVD for the purpose of identifying these events as covariates, outcomes, or complications in future research. We recently reported our findings on the validity of codes for MI [23]. In the current paper, we focus on HF and undertake both a qualitative analysis, and for the first time, a quantitative synthesis of studies reporting on the validity of HF codes in administrative databases.
Methods
Literature Search
Comprehensive searches of the MEDLINE and EMBASE databases from inception (1946 and 1974, respectively) to November 2010 for all available peer-reviewed literature were conducted by an experienced librarian (M-DW). Two search strategies were employed: (1) All studies where administrative data was used to identify CVD; (2) All studies reporting on the validity of administrative data for identifying CVD. Our MEDLINE and EMBASE search strategies are available as (Text S1 and S2). To find additional articles, the authors hand-searched the reference lists of the key articles located through the database search. The Cited-By tools in PubMed and Google Scholar were also used to find relevant articles that had cited the articles located through the database search (up to February 2011). The titles and abstracts of each record were screened for relevance by two independent reviewers. No protocol for this systematic review has been published, though the review was conducted in accordance with the Preferred Reporting Items for Systematic Reviews and Meta-Analyses (PRISMA) [24] and Meta-Analysis of Observational Studies in Epidemiology (MOOSE) [25] statements; our completed checklists are provided as (Checklist S1 and S2).
Inclusion Criteria
We selected full-length, peer-reviewed articles published in English that used administrative data and reported validation statistics for the main International Classification of Diseases (ICD) codes for HF (ICD-8 and ICD-9 428, and ICD-10 I50), or provided sufficient data enabling us to calculate them. Any discrepancies were discussed until consensus was reached. When the conflict persisted a third reviewer (JAA-Z) was consulted.
Data Extraction
The full text of each selected record was examined by two independent reviewers (NM and VB) who abstracted data using a standardized collection form (a copy is provided in Text S3). While extracting data, particular attention was given to the study population, administrative data source, algorithm used to identify HF, validation method, and gold standard. Validation statistics comparing the HF codes to definite or possible cases were abstracted. These statistics included sensitivity, specificity, positive predictive value (PPV), negative predictive value (NPV), and kappa scores. Because hospital separations typically contain multiple diagnoses, with the primary or principal diagnosis in the first position followed by one or more secondary diagnoses, we abstracted statistics for each of these positions, where available. This was especially important given some recent studies of administrative databases that suggest hospitalizations with HF in the primary position are decreasing, while those with HF coded in secondary diagnostic positions are increasing [26],[27]. Data were independently abstracted by each reviewer who subsequently compared their forms to correct any errors and resolve discrepancies.
Quality Assessment
The design and methods used by each study, including the rigour of the reference standard, can directly influence the validity statistics produced. Thus, all studies were evaluated for quality, and the validation statistics were stratified by level of study quality. This was done using the Quality Assessment of Diagnostic Accuracy Studies (QUADAS) tool [28] (available as a part of Text S3), used previously by the CANRAD network in assessing the validity of codes for diabetes mellitus [21], osteoporosis and fractures [22], and myocardial infarction [23]. Briefly, it is a 14-item evidence-based quality assessment tool used in systematic reviews of diagnostic accuracy studies. Each item, phrased as a question, addresses one or more aspects of bias or applicability; however, there is no overall score. Instead, as done previously [22], [23], items were independently answered by each reviewer and used to qualitatively assess each study as High, Medium, or Low quality. Any disagreements were resolved by consensus.
Statistical Analysis
All validation statistics were abstracted as reported. Where sufficient data were available we calculated 95% confidence intervals (95% CI) and additional validity statistics not directly reported in the original publication. These were evaluated on aggregate, and, as pre-specified, stratified by geographic region and time period of publication. In evaluating the HF codes in administrative data, we considered the diagnosis assigned during the validation process to be the diagnostic gold standard; this meant, for instance, that cases coded for HF and classified as HF during validation were true-positive cases, while cases coded for HF but classified during validation as no-HF were false-positives. Sensitivity (the ability of the codes to identify true positive HF cases) was equal to the number of true positives divided by the sum of true positives and false negatives (all those with HF). Specificity (the ability of the HF codes to exclude false-positive cases) was equal to the number of true negatives divided by the sum of true negatives and false positives (all those without HF). Sensitivity and specificity were also used to calculate the positive and negative likelihood ratios (LR+ and LR−) and diagnostic odds ratios (DOR). The DOR (the ratio of the odds that coded individuals will actually have HF compared to the odds that non-coded individuals will have HF) was equal to the LR+ divided by the LR−.
The positive likelihood ratio (LR+), the ratio of true-positives to false-positives amongst all those coded for HF, was equal to the sensitivity divided by 1 – specificity. The negative likelihood ratio (LR−), the ratio of false-negatives to true-negatives amongst all those not coded for HF, was equal to 1 – sensitivity divided by the specificity. Thus, higher LR+ values (those greater than 1) mean the presence of an HF code is more indicative of true HF and lower LR- values (those closer to 0 than 1) mean the absence of an HF code is more indicative of non-disease (no HF). Specificity values typically fall close to 1, such that the denominator for LR+ (1 – specificity) is usually much smaller than the denominator for LR−. As a result, the values for LR+ (which range from 1 to 10 or more) are usually much larger than those for LR− (which range from 0 to 1). An LR+ of 5 to 10 means the codes are moderately good for detecting HF, and an LR+>10 means the codes are very good. Similarly, with an LR− of 0.1 to 0.2, the absence of an HF code corresponds moderately to non-disease (no HF), while an LR− of <0.1 corresponds very well to non-disease [29].
Three other validation statistics of interest were PPV, NPV, and kappa score. The PPV (the likelihood that the HF code corresponds to a true-positive case) was equal to the number of true positives divided by the total number of cases coded for HF (true-positives and false-positives). NPV (the likelihood that an individual not coded for HF is a true-negative case) was equal to the number of true negatives divided by the total number of cases not coded for HF (true-negatives and false-negatives). Kappa (a measure of the agreement, beyond that expected by chance, between how cases are classified in the administrative database and by the validation process) was equal to the observed agreement (the percent of cases classified as either true-positives or true-negatives) minus that expected by chance, divided by [100% - the agreement expected by chance]. Kappa scores greater than 0.60 indicate substantial/almost perfect agreement, 0.41–0.60 is considered as moderate agreement, 0.21–0.40 as fair agreement, and those 0.20 or lower as light/poor agreement [30].
Where available, we abstracted statistics for definite and possible cases of HF, though the number of categories reported depended on the choice of reference standard. In some studies, the reference standard is the presence of any notation of an HF diagnosis in the medical chart, and cases are classified simply as HF or no HF. The Framingham criteria [31] also classify cases as either HF or no HF; at least two of the major Framingham criteria (which include neck vein distension, cardiomegaly, and acute pulmonary edema) or one major criterion and two minor criteria (which include ankle oedema, hepatomegaly, and plural effusion) must be met for the diagnosis of HF. Other sets of standard criteria do allow for further classification. The Carlson criteria [32] use a points system in which potential cases are evaluated in three categories (history, physical examination, and chest radiography), and allocated a maximum of four points in each category, and a maximum overall score of 12. A score of 8 or more is considered Definite HF while 5–7 points are considered Possible HF, and 4 or fewer points are classified as Unlikely HF [32]. Under the European Society of Cardiology criteria [33], for a case to be classified as HF there must be both signs and symptoms of HF, and objective evidence of cardiac dysfunction. Some investigators [17], [34] have classified cases meeting both of these criteria as Definite HF, and those meeting only one of these criteria as Questionable, Possible, or Probable HF. It should be noted that while the New York Heart Association functional classification is used to measure the degree of functional limitation experienced by HF patients, and may assist in the selection of therapies [5], it is not used to make the initial diagnosis of HF.
Meta-Analysis
Studies that reported raw data for sensitivity and specificity were included in the meta-analysis. Forest plots and a summary receiver operating characteristic (ROC) curve were constructed, and pooled estimates (and 95% CI's) of the sensitivity and specificity values, LR+, LR−, and DORs were calculated. More informative diagnostic tests (in this case, being HF codes) - those with good sensitivity and good specificity - will produce ROC curves positioned in the top-left area of the ROC plane, well away from the positive diagonal line [35]. Two additional summary measures of test performance were determined from the ROC curve, the area under the curve (AUC) and Q*. The AUC ranges between 0 and 1, with 1 corresponding to a perfect test [36]. In the context of our research question, an AUC of 1 would mean that, given two cases, one with HF and one without, there is a 100% probability that the positive case will be coded for HF and the negative case will not. The Q*, the lower bound of the AUC, is the point at which the sensitivity and specificity are equal [36]. Higher Q* values indicate better-performing tests.
To assess for the presence of heterogeneity amongst the included studies, we visually inspected the forest plots and ROC curve, and calculated the χ2 statistic, Cochran's Q [37] and I2 [38] statistics. The I2 index, a measure of the degree of inconsistency across study findings, is expressed as the percentage of variation between studies due to heterogeneity as opposed to chance [38]. A value of 0% indicates no observed heterogeneity, while 25% is indicative of low heterogeneity, 50% moderate, and 75% high heterogeneity [38]. When there are a small number of studies, the I2 index is a preferred measure over Cochrane's Q [38]. In the absence of substantial heterogeneity, a fixed-effects model was to be applied. Otherwise, a random-effects model was to be applied, using the DerSimonian Laird method.
To assess the impact each individual study had on the pooled estimates, a jackknife sensitivity analysis [39] was performed in which one study was removed and all summary statistics were re-calculated. This process was repeated for all studies. The impact of publication bias was not evaluated as the common tests available to assess publication bias, including the Begg, Egger, and Macaskill tests, have been shown to be misleading for meta-analyses of test accuracy [40]. All analyses were conducted using Meta-Disc software, version 1.4 [41].
Results
Literature Search
After the removal of duplicates, 1,587 citations were identified through MEDLINE and EMBASE searches and screened for relevance to our study objectives. We then assessed 98 full-text articles for eligibility (Figure 1), of which 12 were selected for inclusion. We also assessed 30 full-text articles for eligibility that were identified from hand searches, and selected 7 additional articles therein. Thus, a total of 128 articles were assessed for eligibility, from which 109 were excluded, mainly because they reported on the validity of other CVD (n = 59), or did not actually validate HF diagnoses in administrative data (n = 20). Six articles were excluded because they were not published in English; their languages of publication were Danish, German, Italian, Japanese, Portuguese, and Spanish. Ultimately 19 articles were included for the qualitative systematic review of HF.
HF = heart failure; ICD = International Classification of Diseases
Study Characteristics
Of the 19 articles evaluating HF diagnoses that were included in the final review, nine (47%) were from the United States, six (32%) were from Canada, three (16%) from Europe, and one was from Australia. Characteristics of these studies are presented in Table 1. Validation was the primary objective in all but one [42] of these studies. Six studies [17], [34], [42]–[45] reported on the validity of HF exclusively, while 13 reported on the validity of other diagnoses as well. Overall, data were collected over a thirty-year period (1976–2005), though the studies were all published relatively recently (the earliest in 1999 [16]). PPV data were available from all but one [16] study, sensitivity and NPV data were available from 14 studies (74%), and specificity data from 13 studies (68%). Kappa scores were less frequently reported. Only four studies [17], [46]–[48] reported on the validity of ICD-10 codes separately from ICD-9. Most of the administrative databases pertained to hospitalizations though diagnoses recorded for outpatient encounters were included in five studies [42], [44], [45], [49], [50]. None of the studies reported on the validity of HF as a cause-of-death.
Chart reviews, sometimes in conjunction with unspecified diagnostic criteria, formed the basis of the gold standard in nine (47%) studies [15], [16], [43], [46]–[48], [50]–[52], and patient self-report was used in one [49]. Cardiac disease registries were used in two studies [53], [54], while a specific set of diagnostic criteria were incorporated in the reference standards of the seven remaining studies [17], [34], [42], [44], [45], [55], [56].
Study quality was evaluated based on the QUADAS tool [28], with 11 of 19 studies (58%) categorized as high quality, seven as medium (37%), and just one (5%) as low quality. A detailed breakdown of the quality assessment for each study is provided in Table S1. Of the seven medium-quality studies, two did not adequately describe the validation process [47], [48], and five used a less-reliable gold standard than published diagnostic criteria (being patient self-report in one [49] and chart review by an individual other than a clinician or trained hospital coder in four [15], [16], [50], [51]). The low-quality study [52] employed a very select source population (women at one institution undergoing vaginal hysterectomy), assessed only two potential cases of HF, and did not adequately describe the validation process.
Validity of Heart Failure Diagnoses
The validation statistics reported by each of the included studies are provided in Table 2. Sensitivity was reported by 14 studies, and was ≥69% in half of them (range: 0 to 87%). PPV was undefined (0/0) in one of the studies [52], but was at least 87% in nine of the 17 remaining studies (range: 34 to 100%). Specificity was ≥95% in all 13 studies reporting this statistic, and NPV was ≥88% in all but two of the 14 studies where this data was available. Kappa was only reported in six (32%) studies [43], [46], [47], [51], [53], [55]. The values in three of the studies (which ranged from 0.43 to 0.58) indicated there was moderate agreement between the diagnostic codes and reference standard, while those in the other three (range 0.72 to 0.94) indicated there was substantial to almost perfect agreement.
The Framingham criteria were used in three studies, with the PPV's reported as 65% [45], 82% [42], and 94% [56]. One of these studies [56] used both the Framingham and Carlson criteria, and found higher accuracy with the Framingham (PPV = 94%) than with the Carlson (PPV = 89%). The European Society of Cardiology criteria were used in two studies; the PPV for definite HF was 82% in one [34] but just 65% in the other [17]. Sex-stratified statistics were provided by two studies; one [56] reported a slightly higher PPV for ICD-9 428 in females, and the other [43] found that the sensitivity of ICD-9 428 was significantly better in females than males (66% vs. 61%). In that study, the sensitivity was also significantly better amongst Mexican Americans than Non-Hispanic whites (66% vs. 59%) [43].
The studies in Table 2 are ordered chronologically by publication year for the purpose of identifying any secular trends in the validity of HF codes. The nine-earliest studies included in this review were published between 1999 and 2004, with the ten remaining studies published from 2005 to 2009. However, no secular trends were observed for any of the validation statistics. Eleven (58%) of the studies included in this review were rated as high quality and seven (37%) as medium quality. Sensitivity ranged from 43% to 87% amongst the high quality studies, and from 58% to 87% amongst the medium quality. The PPV's for these two categories were also similar, ranging from 36% to 99% amongst the high quality studies, and from 34% to 100% amongst the medium quality. Any geographic comparisons were limited by the fact that 15 of the 19 studies were conducted in North America. The only difference observed was that the sensitivity values tended to be higher amongst the seven US studies than the five Canadian ones.
Meta-Analysis
Included in the quantitative synthesis were the 11 articles from which raw data on sensitivity and specificity were available. Forest plots of the pooled sensitivity and specificity values are illustrated in Figure 2. A random-effects model was used since the χ2, Q*, and I2 statistics indicated there was a high level of heterogeneity between studies. The pooled sensitivity was 75.3% (95% CI: 74.7–75.9) and the pooled specificity was 96.8% (95% CI: 96.8–96.9). The summary LR+ was 51.9 (95% CI: 20.5–131.6) and the summary LR- was 0.27 (95% CI: 0.20–0.37), giving a summary DOR of 186.5 (95% CI: 96.8–359.22). The summary ROC curve is illustrated in Figure 3, wherein the AUC was 0.93 (SE 0.0396) and the Q* was 0.86 (SE 0.0466).
95% CI = 95% confidence interval; DF = degrees of freedom.
AUC = Area Under the Curve; SROC = Summary Receiver Operating Characteristic; SE = standard error.
Results of the jackknife sensitivity analysis, wherein the pooled estimates were re-calculated after the removal of one study at a time, are shown in Table 3. The resulting pooled sensitivity estimates ranged mainly from 74% to 76%, and the specificities from 96.6% to 96.9%. The two most influential studies were those by Onofrei et al (sensitivity = 77.5% and specificity = 93.3% after its removal) and Austin et al (sensitivity = 71.8% and specificity = 99.1% after its removal).
Discussion
To our knowledge this is the first systematic review and meta-analysis on the validity of HF diagnoses in administrative data. Findings from this review suggest that the sensitivity of these codes is suboptimal, as sensitivity was ≤69% in 8 of the 14 studies reporting this statistic. However, the specificity and PPV of these codes appears much better: specificity was at least 95% in the 13 studies where this statistic was reported, and, in the majority of studies, the PPV was at least 87%. Further support was provided by the results of the meta-analysis, as the pooled specificity of HF codes was 97%, and the pooled LR+ was 52. This means an individual coded for HF is fifty-two-times more likely to actually have HF than someone not coded. However, the pooled sensitivity was modest, at just 75%, and the summary LR- value of 0.27 suggests that the absence of an HF code can rule out the diagnosis of HF only moderately.
The PPV's and NPV's amongst the studies included in this review were generally good, being at least 87% in the majority of studies reporting these statistics. A recently-published qualitative review of the validity of HF codes in North American databases also found the PPV to be generally high (>90% in most) [57]. However, it must be kept in mind that PPV and NPV are both dependent on the prevalence of the condition in the study population [35], and will be lower for rare conditions than for common conditions. This is important for HF because this condition differentially affects older individuals: for example, HF is reported to affect approximately 7.8% of US males aged 60–79 years, but only 1.5% of US males aged 40–59 years [2]. A higher baseline risk of HF in the study population may explain why several studies included in this review reported exceptionally high PPV's. For example, in the study by Szeto et al [50], which was conducted amongst a cohort of patients attending a Veteran's Affairs clinic, the prevalence of HF was 10%, and the PPV was 100%. So et al [48] examined the charts of patients hospitalized for MI, amongst whom the prevalence of HF was 29%, and the PPV in that study was 94%. Similarly, the prevalence of HF was 47% amongst the atrial fibrillation cohort studied by Birman-Deych et al [15], and the PPV was 97%. Consequently, if the exclusion of false-positive HF cases is of upmost priority for a particular study, the age and disease history of the study population must be taken into account when evaluating how accurately these codes will identify true HF cases.
Findings from our review suggest that administrative data codes are less-than-optimal for capturing HF cases, and this is consistent with another qualitative review of the validity of HF codes in which the sensitivity of HF diagnoses was highly-variable [58]. Instead of HF itself, some authors have suggested there is a tendency to list the underlying cause of the HF (such as MI or atrial fibrillation [17]), or another cardiac condition [53], in the primary position of the hospital discharge summary. Moreover, hospital coders generally report active conditions [51] such as MI, but may leave out chronic conditions such as HF if they were deemed not to have impacted the treatments provided in hospital or length-of-stay [47], [58]. Similarly, the study by Birman-Deych et al, where sensitivity for HF increased with disease severity (from 80% for mild cases to 94% for severe [15]), suggested that severe cases of HF may be recorded more often in administrative databases than mild ones. Thus, to maximize the capture of HF cases, authors are advised to broaden their search parameters by examining all diagnostic positions of the hospital record, considering the inclusion of more HF-related codes (other than ICD-9 428 or ICD-10 I50) in the search algorithm, and, where available, searching for HF cases in both hospitalization and outpatient databases.
Sources of Administrative Data
While the improvements were not substantial, some studies we reviewed suggested HF cases could be identified more accurately if algorithms combining hospital codes with prescription data were applied. For example, Rector et al [49] tested several algorithms to identify HF, some of which incorporated prescription claims for an angiotensin converting enzyme (ACE) inhibitor, angiotensin-II receptor antagonist, loop diuretic, or digoxin. When using an algorithm that required a healthcare encounter and HF-related prescription, the specificity was high (92%), though the sensitivity was modest (53%) [49]. While further research is needed in this area, findings from that study also suggested that HF cases could be identified from prescription data alone, as the specificity of an algorithm that included a single HF-related prescription, but no healthcare encounters, was 78% [49]. This occurred despite the fact that many medications used in the treatment of HF are also used to treat other conditions [49]. Hence, prescription medication data could be used to validate HF cases first identified from hospital or outpatient data, or used alone to identify HF cases in a sensitivity analysis. Requiring that cases be dispensed a combination of medications - for example, each of a diuretic, ACE inhibitor or angiotensin-II receptor antagonist, and beta blocker - may improve specificity. At this time the prescription databases in many countries only include government-subsidized prescriptions, limiting the potential of this data source for identifying cases. Thus, prescription medication data should only be used if the database contains records on all community-dispensed prescriptions, regardless of payer, or at least all prescriptions dispensed to senior citizens.
Laboratory databases may also be a useful source for identifying HF. Specifically, levels of B-type natriuretic peptide(BNP) are often elevated in patients with left ventricular HF [6], so individuals with high BNP values could be identified as HF cases. One study in this review, by Alqaisi et al [45], compared the accuracy of different algorithms for identifying HF, some of which included BNP levels, and the highest-sensitivity algorithm in that study was ≥2 outpatient encounters for HF, or ≥1 hospitalizations for HF, or a BNP level of ≥200 pg/ml. That algorithm achieved a sensitivity of 76% and a specificity of 75%. BNP levels can be elevated in conditions other than HF, such as pulmonary embolism and chronic obstructive pulmonary disease [6], which may limit the specificity of BNP levels for identifying HF. However, additional findings from the Alqaisi et al study [45], where the specificities of BNP levels of ≥100 pg/ml, 200 pg/ml, and 500 pg/ml (without considering any diagnoses from healthcare encounters) were 76%, 88%, and 95%, respectively, suggest this test is reasonably specific for HF. Any potential increases in sensitivity will be limited by the fact that BNP levels tend to be elevated more in HF patients with left systolic dysfunction than diastolic dysfunction [6]. Another caveat is that BNP is less sensitive a test in non-acute HF [5]. Where laboratory data are available, we suggest researchers incorporate BNP levels into their case definition and, in a sensitivity analysis, compare the HF cases identified with- and without BNP levels.
Reference Standards
Findings from our meta-analysis suggested a high degree of heterogeneity amongst the included studies; thus, a random-effects model was used to produce the summary measures. Part of this heterogeneity can be attributed to differences in the characteristics of the study populations. Some studies were community-based or conducted on a general hospitalized population while others were conducted on select populations (i.e. elderly people or those with a history of MI) in whom HF is more prevalent. Variations in the size of the study population may also have contributed, as there were changes, though not substantial, in the pooled sensitivity and specificity estimates after each of the two largest studies (n = 205,755 and n = 58,816) were removed.
More importantly, there was much heterogeneity in the reference standards used by different studies. This was not surprising as there is no single accepted gold standard for the diagnosis of HF, and a definitive diagnosis of HF is often difficult [53], [58], especially in elderly patients with multiple complications [34]. The reference standards used included patient self-report, chart reviews by clinicians and non-clinicians, two distinct disease registries, and the application of several sets of standard diagnostic criteria including the Framingham, Carlson, and European Society of Cardiology (ESC). One study included in our review, by Onofrei et al [44], reported both low sensitivity (44%) and low PPV (36%) for HF codes, which could be explained, in part, by their choice of reference standard. It consisted of a single measurement, left ventricular ejection fraction (LVEF) of either ≤55% or ≤40%. The LVEF is not typically used for HF diagnosis, but instead for classifying HF patients with left ventricular systolic or diastolic dysfunction [59]. Although the thresholds vary, an LVEF below 40% or 50% is usually indicative of systolic dysfunction, while higher LVEF values in HF patients are usually indicative of diastolic dysfunction but preserved systolic function [59]. It is possible that some of the false-positive cases in that study (coded for HF but whose LVEF measurement did not fall below the thresholds) exhibited other signs and symptoms that would fulfill the criteria for HF under the less-restrictive Framingham, Carlson, or ESC definitions. Thus, this choice of reference standard may have attenuated the PPV.
Furthermore, although the Framingham and Carlson criteria have been shown to be 100% sensitive to cases of definite HF [60], especially severe cases [61], the Framingham criteria are considered by some to be insensitive for detecting early HF [62], [63]. Therefore, the application of standard diagnostic criteria may also attenuate the PPV. In this review, we did observe a trend towards greater PPV (80-100%) when simply a physician's written confirmation of HF diagnosis or other notation in the medical chart was used as a gold standard [15], [42], [50]. In fact, Roger et al [42] compared two gold standards, physician diagnosis (as written in the chart) and the Framingham criteria, and found that the PPV from physician diagnosis was higher compared with the Framingham criteria (90% vs. 82%). Although the physician diagnosis may be more subjective, it may better reflect the diagnoses made in day-to-day clinical practice and thus be more meaningful to health researchers.
In addition to prescription medication and laboratory data, a third resource that could be used in conjunction with conventional administrative (billing) data to capture more HF cases is the electronic medical record (EMR), or electronic health record (EHR). The EMR or EHR is a digital file used by healthcare providers for patient care [64]. Though some authors use EMR when referring to the digital file maintained by a single practitioner, and EHR when referring to a digital file containing inpatient and outpatient data from multiple practitioners, for simplicity we will employ a single term, EMR, in this discussion. The materials available in the EMR can vary, but generally include clinical notes (similar to those recorded in a paper medical chart), prescription records, and laboratory and radiology reports [64]. With access to EMRs, researchers can identify HF cases by searching for an ICD code for HF amongst the patient's Problem List, a list maintained by the practitioner of all current and active diagnoses. In addition, researchers can also search for the term ‘heart failure’ amongst the entire free-text areas of the clinical notes, laboratory and radiological reports, and any correspondence from specialists. For example, the Mayo Clinic has used a natural language processing (NLP) algorithm containing the terms ‘cardiomyopathy’, ‘heart failure’, ‘congestive heart failure’, ‘pulmonary edema’, ‘decompensated heart failure’, ‘volume overload’ and ‘fluid overload’, along with 426 synonyms for these terms [65]. A potential case is eliminated if a negative term (such as ‘no’ or ‘unlikely’), or sometimes even a speculative term (such as ‘rule-out’ or ‘suspected’) is found within close proximity of the HF term [65], [66]. For chronic conditions like HF that may be superseded by other diagnoses on reimbursement claims, this EMR-based search strategy may be more sensitive than relying on the diagnostic codes in claims-based administrative databases, and may aid in capturing milder cases.
However, the EMR also has some limitations, many of which stem from the fact that, similar to most administrative databases, the EMR was not established for research purposes [64]. For example, when searching the free-text notes and reports, computer programs may have difficulty processing whether ambiguous phrases like “cannot be ruled out” [67] correspond to a positive case. In addition, while the information contained in administrative databases is already de-identified, the EMR does contain personally-identifying information. US law stipulates that, unless each patient provides consent [68], researchers cannot use data collected from the EMR without it undergoing a de-identification process [69]. Thus, it may be costly and time-consuming for researchers to access this data, especially as many hospitals do not use de-identification tools at present [68]. A lack of standardization across EMR systems [64] and challenges in linking EMRs from different hospitals or provider networks [70] may also limit the use of EMR. Finally, just as with ICD codes, the validity of the HF cases identified from the free-text areas of the EMR must be assessed before EMRs can be used for HF research. While the results of some validation studies [65], [67] have been promising, more validation studies conducted in different settings, and using different EMR platforms, are needed to confirm these findings.
Limitations
We acknowledge some limitations to our systematic review. There is the potential for a language bias as we could not consider articles whose full-texts were not available in English; articles published after the conclusion of our search period (February 2011) could not be considered either. Another potential limitation stems from the fact that, even though our database searches were conducted by an experienced librarian, administrative databases are not well catalogued in MEDLINE and EMBASE (e.g. no MeSH term pertaining to “administrative database”). Although most of the included studies were located through database searches, our subsequent hand search turned up several more relevant articles, most of which had not been indexed under terms relating to Administrative Data or Validation. As a result, despite our extensive hand search, we may have missed some relevant articles if they were not indexed in MEDLINE or EMBASE under a term relating to administrative data or validation. Our findings are also subject to publication bias, wherein reports of HF codes having poor validity may have been differentially withheld from publication. However, given the number of reports we located where the sensitivity of HF codes was suboptimal, we feel this is unlikely
Recommendations
After qualitative and quantitative analysis of the evidence, we conclude that the HF codes that do appear in administrative databases are highly predictive of true HF cases. At the same time, administrative databases fail to capture a non-negligible number of true cases, perhaps 25% to 30% of all diagnoses, and may differentially capture the most severe cases. Based on current evidence, we recommend several strategies for increasing the capture of HF cases in administrative data:
- Hospitalizations with HF in the primary position are decreasing, while those with HF in secondary positions are increasing [26], [27]. Thus, researchers should search amongst all available diagnostic positions in hospitalization data for HF codes.
- With many HF patients treated exclusively on an outpatient basis, data from both inpatient and outpatient encounters should be searched.
- Where available, researchers should supplement their data with searches of laboratory databases (specifically BNP values) and/or prescription medication data.
- Searching the free-text areas of the EMR for mentions of ‘heart failure’ and related terms, as well as the Problem List, should help identify cases whose HF diagnosis has not been recorded on an inpatient or outpatient billing record. This may particularly aid in the capture of mild HF.
Conclusions
The chronic and syndromic nature of HF creates difficulties for researchers studying this condition at the population level. To guide their efforts, we conducted a systematic review and meta-analysis of articles reporting on the validity of HF diagnoses in administrative data. Our findings suggest that, although the HF diagnoses identified using administrative data frequently correspond to true HF cases, this data source may not capture all cases. Administrative databases are increasingly being used to study long-term patient outcomes and disease burden; thus, to maximize the sensitivity of these data sources for all conditions, physicians and hospital coders are encouraged to record diagnoses of all comorbidities that may have contributed to a given healthcare encounter. In the meantime, the use of broader case definitions, potentially in combination with prescription medication and laboratory data, and searches of electronic medical records, may increase the sensitivity of this data source for HF, and in turn, its application in population-based health outcomes and economics research.
Supporting Information
Table S1.
Item-by-Item QUADAS Breakdown for Each Study.
https://doi.org/10.1371/journal.pone.0104519.s001
(DOC)
Acknowledgments
The authors wish to thank members of the CANRAD network, librarian Mary-Doug Wright (B.Sc., M.L.S.) for conducting the literature search, Reza Torkjazi, and Kathryn Reimer for their help during their administrative support and editing the manuscript.
Author Contributions
Conceived and designed the experiments: DL JAAZ. Analyzed the data: NM DL VB JAAZ. Contributed to the writing of the manuscript: NM DL VB JAAZ. Final approval of the version of the manuscript to be published: NM DL VB JAAZ.
References
- 1. Ambrosy AP, Fonarow GC, Butler J, Chioncel O, Greene SJ, et al. (2014) The global health and economic burden of hospitalizations for heart failure: lessons learned from hospitalized heart failure registries. J Am Coll Cardiol 63: 1123–1133
- 2. Go AS, Mozaffarian D, Roger VL, Benjamin EJ, Berry JD, et al. (2014) Heart disease and stroke statistics—2014 update: a report from the American Heart Association. Circulation 129: e28–e292
- 3. Chen Y-T, Vaccarino V, Williams CS, Butler J, Berkman LF, et al. (1999) Risk factors for heart failure in the elderly: a prospective community-based study. Am J Med 106: 605–612
- 4. Cook C, Cole G, Asaria P, Jabbour R, Francis DP (2014) The annual global economic burden of heart failure. Int J Cardiol 171: 368–376
- 5. McMurray JJV, Adamopoulos S, Anker SD, Auricchio A, Bohm M, et al. (2012) ESC Guidelines for the diagnosis and treatment of acute and chronic heart failure 2012: The Task Force for the Diagnosis and Treatment of Acute and Chronic Heart Failure 2012 of the European Society of Cardiology. Developed in collaboration with the Heart Failure Association (HFA) of the ESC. Eur Heart J 33: 1787–1847
- 6. Hunt SA, Abraham WT, Chin MH, Feldman AM, Francis GS, et al. (2009) 2009 focused update incorporated into the ACC/AHA 2005 Guidelines for the Diagnosis and Management of Heart Failure in Adults: a report of the American College of Cardiology Foundation/American Heart Association Task Force on Practice Guidelines: developed in collaboration with the International Society for Heart and Lung Transplantation. Circulation 119: e391–479
- 7. Van Deursen VM, Urso R, Laroche C, Damman K, Dahlström U, et al. (2014) Co-morbidities in patients with heart failure: an analysis of the European Heart Failure Pilot Survey. Eur J Heart Fail 16: 103–111
- 8. Wong CY, Chaudhry SI, Desai MM, Krumholz HM (2011) Trends in comorbidity, disability, and polypharmacy in heart failure. Am J Med 124: 136–143
- 9. Cleland JGF, Swedberg K, Follath F, Komajda M, Cohen-Solal A, et al. (2003) The EuroHeart Failure survey programme— a survey on the quality of care among patients with heart failure in Europe. Part 1: patient characteristics and diagnosis. Eur Heart J 24: 442–463.
- 10. Van Deursen VM, Damman K, van der Meer P, Wijkstra PJ, Luijckx G-J, et al. (2014) Co-morbidities in heart failure. Heart Fail Rev 19: 163–172
- 11. Braunstein JB, Anderson GF, Gerstenblith G, Weller W, Niefeld M, et al. (2003) Noncardiac comorbidity increases preventable hospitalizations and mortality among Medicare beneficiaries with chronic heart failure. J Am Coll Cardiol 42: 1226–1233.
- 12. Hawkins NM, Jhund PS, Simpson CR, Petrie MC, Macdonald MR, et al. (2010) Primary care burden and treatment of patients with heart failure and chronic obstructive pulmonary disease in Scotland. Eur J Heart Fail 12: 17–24
- 13. Dunlay SM, Redfield MM, Weston SA, Therneau TM, Hall Long K, et al. (2009) Hospitalizations after heart failure diagnosis a community perspective. J Am Coll Cardiol 54: 1695–1702
- 14. Dai S, Walsh P, Wielgosz A, Gurevich Y, Bancej C, et al. (2012) Comorbidities and mortality associated with hospitalized heart failure in Canada. Can J Cardiol 28: 74–79
- 15. Birman-Deych E, Waterman AD, Yan Y, Nilasena DS, Radford MJ, et al. (2005) Accuracy of ICD-9-CM codes for identifying cardiovascular and stroke risk factors. Med Care 43: 480–485.
- 16. Levy AR, Tamblyn RM, Fitchett D, McLeod PJ, Hanley JA (1999) Coding accuracy of hospital discharge data for elderly survivors of myocardial infarction. Can J Cardiol 15: 1277–1282.
- 17. Khand AU, Shaw M, Gemmel I, Cleland JG (2005) Do discharge codes underestimate hospitalisation due to heart failure? Validation study of hospital discharge coding for heart failure. Eur J Heart Fail 7: 792–797.
- 18. Bernatsky S, Lix L, O'Donnell S, Lacaille D (2013) CANRAD Network (2013) Consensus statements for the use of administrative health data in rheumatic disease research and surveillance. J Rheumatol 40: 66–73.
- 19. Widdifield J, Labrecque J, Lix L, Paterson JM, Bernatsky S, et al. (2013) Systematic review and critical appraisal of validation studies to identify rheumatic diseases in health administrative databases. Arthritis Care Res 65: 1490–1503
- 20. Barber C, Lacaille D, Fortin PR (2013) Systematic review of validation studies of the use of administrative data to identify serious infections. Arthritis Care Res 65: 1343–1357
- 21. Leong A, Dasgupta K, Bernatsky S, Lacaille D, Avina-Zubieta A, et al. (2013) Systematic review and meta-analysis of validation studies on a diabetes case definition from health administrative records. PloS One 8: e75256
- 22. Hudson M, Avina-Zubieta A, Lacaille D, Bernatsky S, Lix L, et al. (2013) The validity of administrative data to identify hip fractures is high—a systematic review. J Clin Epidemiol 66: 278–285
- 23. McCormick N, Lacaille D, Bhole V, Avina-Zubieta JA (2014) Validity of myocardial infarction diagnoses in administrative databases: a systematic review. PloS One 9: e92286
- 24. Moher D, Liberati A, Tetzlaff J, Altman DG (2009) PRISMA Group (2009) Preferred reporting items for systematic reviews and meta-analyses: the PRISMA statement. PLoS Med 6: e1000097
- 25. Stroup DF, Berlin JA, Morton SC, Olkin I, Williamson GD, et al. (2000) Meta-analysis of observational studies in epidemiology: a proposal for reporting. Meta-analysis Of Observational Studies in Epidemiology (MOOSE) group. JAMA 283: 2008–2012.
- 26. Blecker S, Paul M, Taksler G, Ogedegbe G, Katz S (2013) Heart failure–associated hospitalizations in the United States. J Am Coll Cardiol 61: 1259–1267
- 27. Fang J, Mensah GA, Croft JB, Keenan NL (2008) Heart failure-related hospitalization in the U.S., 1979 to 2004. J Am Coll Cardiol 52: 428–434
- 28. Whiting P, Rutjes AW, Reitsma JB, Bossuyt PM, Kleijnen J (2003) The development of QUADAS: a tool for the quality assessment of studies of diagnostic accuracy included in systematic reviews. BMC Med Res Methodol 3: 25.
- 29. Jaeschke R (1994) Users' Guides to the Medical Literature: III. How to Use an Article About a Diagnostic Test B. What Are the Results and Will They Help Me in Caring for My Patients? JAMA 271: 703
- 30. Landis JR, Koch GG (1977) The measurement of observer agreement for categorical data. Biometrics 33: 159–174.
- 31. McKee PA, Castelli WP, McNamara PM, Kannel WB (1971) The Natural History of Congestive Heart Failure: The Framingham Study. N Engl J Med 285: 1441–1446
- 32. Carlson KJ, Lee DC, Goroll AH, Leahy M, Johnson RA (1985) An analysis of physicians' reasons for prescribing long-term digitalis therapy in outpatients. J Chronic Dis 38: 733–739.
- 33. Dickstein K, Cohen-Solal A, Filippatos G, McMurray JJV, Ponikowski P, et al. (2008) ESC Guidelines for the diagnosis and treatment of acute and chronic heart failure 2008: the Task Force for the Diagnosis and Treatment of Acute and Chronic Heart Failure 2008 of the European Society of Cardiology. Developed in collaboration with the Heart Failure Association of the ESC (HFA) and endorsed by the European Society of Intensive Care Medicine (ESICM). Eur Heart J 29: 2388–2442
- 34. Ingelsson E, Arnlov J, Sundstrom J, Lind L (2005) The validity of a diagnosis of heart failure in a hospital discharge register. Eur J Heart Fail 7: 787–791.
- 35.
Kramer M (1988) Chapter 16: Diagnostic Tests. Clinical Epidemiology and Biostatics: A Primer for Clinical Investigators and Decision Makers. Berlin: Springer. pp. 236–253.
- 36. Walter SD (2002) Properties of the summary receiver operating characteristic (SROC) curve for diagnostic test data. Stat Med 21: 1237–1256
- 37. Cochran WG (1954) The Combination of Estimates from Different Experiments. Biometrics 10: 101
- 38. Higgins JPT, Thompson SG, Deeks JJ, Altman DG (2003) Measuring inconsistency in meta-analyses. BMJ 327: 557–560
- 39. Miller RG (1974) The jackknife-a review. Biometrika 61: 1–15
- 40. Deeks JJ, Macaskill P, Irwig L (2005) The performance of tests of publication bias and other sample size effects in systematic reviews of diagnostic test accuracy was assessed. J Clin Epidemiol 58: 882–893
- 41. Zamora J, Abraira V, Muriel A, Khan K, Coomarasamy A (2006) Meta-DiSc: a software for meta-analysis of test accuracy data. BMC Med Res Methodol 6: 31
- 42. Roger VL, Weston SA, Redfield MM, Hellermann-Homan JP, Killian J, et al. (2004) Trends in heart failure incidence and survival in a community-based population. JAMA 292: 344–350.
- 43. Goff DJ, Pandey DK, Chan FA, Ortiz C, Nichaman MZ (2000) Congestive heart failure in the United States: is there more than meets the I(CD code)? The Corpus Christi Heart Project. Arch Intern Med 160: 197–202.
- 44. Onofrei M, Hunt J, Siemienczuk J, Touchette DR, Middleton B (2004) A first step towards translating evidence into practice: heart failure in a community practice-based research network. Inform Prim Care 12: 139–145.
- 45. Alqaisi F, Williams LK, Peterson EL, Lanfear DE (2009) Comparing methods for identifying patients with heart failure using electronic data sources. BMC Health Serv Res 9: 237–6963–9–237.
- 46. Henderson T, Shepheard J, Sundararajan V (2006) Quality of diagnosis and procedure coding in ICD-10 administrative data. Med Care 44: 1011–1019.
- 47. Chen G, Faris P, Hemmelgarn B, Walker RL, Quan H (2009) Measuring agreement of administrative data with chart data using prevalence unadjusted and adjusted kappa. BMC Med Res Methodol 9: 5–2288–9–5.
- 48. So L, Evans D, Quan H (2006) ICD-10 coding algorithms for defining comorbidities of acute myocardial infarction. BMC Health Serv Res 6: 161.
- 49. Rector TS, Wickstrom SL, Shah M, Greeenlee NT, Rheault P, et al. (2004) Specificity and sensitivity of claims-based algorithms for identifying members of Medicare+Choice health plans that have chronic medical conditions. Health Serv Res 39: 1839–1857.
- 50. Szeto HC, Coleman RK, Gholami P, Hoffman BB, Goldstein MK (2002) Accuracy of computerized outpatient diagnoses in a Veterans Affairs general medicine clinic. Am J Manag Care 8: 37–43.
- 51. Humphries KH, Rankin JM, Carere RG, Buller CE, Kiely FM, et al. (2000) Co-morbidity data in outcomes research: are clinical data derived from administrative databases a reliable alternative to chart review? J Clin Epidemiol 53: 343–349.
- 52. Heisler CA, Melton LJ 3rd, Weaver AL, Gebhart JB (2009) Determining perioperative complications associated with vaginal hysterectomy: code classification versus chart review. J Am Coll Surg 209: 119–122.
- 53. Austin PC, Daly PA, Tu JV (2002) A multicenter study of the coding accuracy of hospital discharge administrative data for patients admitted to cardiac care units in Ontario. Am Heart J 144: 290–296.
- 54. Merry AH, Boer JM, Schouten LJ, Feskens EJ, Verschuren WM, et al. (2009) Validity of coronary heart diseases and heart failure based on hospital discharge and mortality data in the Netherlands using the cardiovascular registry Maastricht cohort study. Eur J Epidemiol 24: 237–247.
- 55. Heckbert SR, Kooperberg C, Safford MM, Psaty BM, Hsia J, et al. (2004) Comparison of self-report, hospital discharge codes, and adjudication of cardiovascular events in the Women's Health Initiative. Am J Epidemiol 160: 1152–1158
- 56. Lee DS, Donovan L, Austin PC, Gong Y, Liu PP, et al. (2005) Comparison of coding of heart failure and comorbidities in administrative and clinical data for use in outcomes research. Med Care 43: 182–188.
- 57. Saczynski JS, Andrade SE, Harrold LR, Tjia J, Cutrona SL, et al. (2012) A systematic review of validated methods for identifying heart failure using administrative data. Pharmacoepidemiol Drug Saf 21: 129–140
- 58. Quach S, Blais C, Quan H (2010) Administrative data have high variation in validity for recording heart failure. Can J Cardiol 26: 306–312.
- 59. Gaasch WH (1994) Diagnosis and treatment of heart failure based on left ventricular systolic or diastolic dysfunction. JAMA 271: 1276–1280.
- 60. Mosterd A, Deckers JW, Hoes AW, Nederpel A, Smeets A, et al. (1997) Classification of heart failure in population based research: an assessment of six heart failure scores. Eur J Epidemiol 13: 491–502.
- 61. Remes J, Reunanen A, Aromaa A, Pyörälä K (1992) Incidence of heart failure in eastern Finland: a population-based surveillance study. Eur Heart J 13: 588–593.
- 62. Marantz PR, Alderman MH, Tobin JN (1988) Diagnostic heterogeneity in clinical trials for congestive heart failure. Ann Intern Med 109: 55–61.
- 63. Senni M, Tribouilloy CM, Rodeheffer RJ, Jacobsen SJ, Evans JM, et al. (1999) Congestive heart failure in the community: trends in incidence and survival in a 10-year period. Arch Intern Med 159: 29–34.
- 64. Dean BB, Lam J, Natoli JL, Butler Q, Aguilar D, et al. (2009) Review: use of electronic medical records for health outcomes research: a literature review. Med Care Res Rev 66: 611–638
- 65. Pakhomov S, Weston SA, Jacobsen SJ, Chute CG, Meverden R, et al. (2007) Electronic medical records for clinical research: application to the identification of heart failure. Am J Manag Care 13: 281–288.
- 66. Friedman C, Hripcsak G, Shagina L, Liu H (1999) Representing information in patient reports using natural language processing and the extensible markup language. J Am Med Inform Assoc 6: 76–87.
- 67.
Friedlin J, McDonald CJ (2006) A natural language processing system to extract and code concepts relating to congestive heart failure from chest radiology reports. AMIA Annu Symp Proc: 269–273.
- 68.
Liu F, Weng C, Yu H (2012) Chapter 16: Natural Language Processing, Electronic Health Records, and Clinical Research. Clinical Research Informatics. Health Informatics. Springer.pp. 305–306.
- 69.
Guidance Regarding Methods for De-identification of Protected Health Information in Accordance with the Health Insurance Portability and Accountability Act (HIPAA) Privacy Rule (n.d.). Available: http://www.hhs.gov/ocr/privacy/hipaa/understanding/coveredentities/De-identification/guidance.html. Accessed 21 May 2014.
- 70. Bradley CJ, Penberthy L, Devers KJ, Holden DJ (2010) Health Services Research and Data Linkages: Issues, Methods, and Directions for the Future. Health Serv Res 45: 1468–1488