Raj S. Padwal, MD, MSc

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Comparing three different measures of frailty in medical inpatients: Multicenter prospective cohort study examining 30‐day risk of readmission or death

Author(s)

Sara Belga, MD

Sharry Kahlon, MD

Jenelle Pederson, BA

Darren Lau, MD, PhD

Mary Forhan, MHSc, PhD

Jeffrey A. Bakal, PhD

Frailty is a state of vulnerability that encompasses a heterogeneous group of people.[1] Because it lacks a precise definition, multiple tools have been developed to identify frailty in both clinical and research settings.[2, 3, 4] Prevalence of frailty depends on the frailty assessment tool used and the population studied, ranging from 4% to 17% when the Fried score[5, 6, 7] is used and from 5% to 44%[5, 7, 8] when cumulative deficit models like the Frailty Index are utilized, with the lower prevalences being in younger community‐dwelling elderly populations and the higher proportions being in older institutionalized populations.

The Frailty Index, also called the Burden or Cumulative Deficit Model, comprises 70 domains that include mobility, mood, function, cognitive impairment, and disease states. It is multidimensional and allows for patients to be categorized on a continuum of frailty, but it is extremely difficult to apply in clinical practice. Recognizing this, Rockwood et al.[9] developed and validated the Clinical Frailty Scale (CFS) in the Canadian Study of Health and Aging. The CFS classifies patients into 1 of 9 categories: very fit, well, managing well, vulnerable, mildly frail (needs help with at least 1 instrumental activity of daily living such as shopping, finances, meal preparation, or housework), moderately frail (needs help with 1 or 2 activities of daily living such as bathing and dressing), severely frail (dependent for personal care), very severely frail (bedbound), and terminally ill. Although this tool is easy to use in clinical practice, it reflects a gestalt impression and requires some clinical judgement.

The Fried score[6] is a prototypical phenotype tool based on 5 criteria that include weight loss, self‐reported exhaustion, low energy expenditure, slowness of gait, and weakness. Recent evidence has suggested that slow gait (or dysmobility) alone may also be a potential screening test for frailty.[10] A recent systematic review[11] demonstrated an association between slow gait (dysmobility) and increased mortality. Dysmobility negatively impacts quality of life and has a strong association with disability resulting in the need for an increased level of care.[12] The Timed Up and Go Test (TUGT) is one method of assessing mobility which is relatively easy to perform, does not require special equipment, and is feasible to use in clinical settings.[13] However, whether impaired mobility predicts outcomes within the first 30 days after hospital discharge (a timeframe highlighted in the Affordable Care Act and used by the Centers for Medicare and Medicaid Services as an important hospital quality indicator) is still uncertain.

The aim of this study was to compare frailty assessments using the CFS and 2 of the most commonly used phenotypic tools (a modified Fried score and the TUGT as a proxy for mobility assessment) to determine which tools best predict postdischarge outcomes.

METHODS

Study Design and Population

As described in detail elsewhere,[14] this was a prospective cohort study that enrolled adult patients (any age older than 18 years) at the time of discharge back to the community from 7 general internal medicine wards in 2 teaching hospitals in Edmonton, Alberta between October 2013 and November 2014. We excluded patients admitted from, or being discharged back to, long‐term care facilities or other acute care hospitals, or from out of the province; patients who were unable to communicate in English; patients with moderate or severe cognitive impairment (scoring 5 or more on the Short Portable Mental Status Questionnaire); or patients with projected life expectancy of less than 3 months. All patients provided written consent, and the study was approved by the Health Research Ethics board of the University of Alberta (project ID Pro00036880).

We assessed the degree of frailty within 24 hours of discharge in 3 ways. First, we used the CFS[9, 15] with patients being asked to rate their best functional status in the week prior to admission. As per the CFS validations studies, scores 5 were defined as frail.[9, 15] Second, we used the TUGT as a proxy for slow gait speed/dysmobility (with >20 seconds defined as abnormal).[13] The TUGT was recorded as the shortest recorded time of the 2 timed trials to get up from a seated position, walk 10 feet and back, and then sit in the chair again. Third, we also determined their Fried score[6] (using the modifications outlined below) and categorized the patients as frail if they scored 3 or more. Of the 5 Fried categories, we assessed weakness by grip strength in their dominant hand using a Jamar handheld dynamometer and weight loss of 10 lb or more in the past year based on patient self‐report; these are identical to the original Fried scale description. Grip strength in the lowest quintile for sex and body mass index was defined as weak grip strength as per convention in the literature, which corresponded to less than 28.5 kg for men and less than 18.5 kg for women.[16, 17] We assessed the other 3 Fried categories in modified fashion as follows. For slow gait, rather than assessing time to walk 15 feet as in the original study and assigning a point to those testing in the lowest quintile for their age/sex, we used the TUGT, because our research personnel were already trained in this test, and we were doing it already as part of the discharge package for all patients.[13] For the Fried category of low activity, we based this on patient self‐report using the relevant questions in the EuroQoL Questionnaire (EQ‐5D); the Fried score used self‐report with a different questionnaire. Finally, for self‐reported exhaustion we used the questions in the Patient Health Questionnaire 9 (PHQ‐9)[18] analogous to those used from the Center for Epidemiological Studies depression scale in the original Fried description. We did this as we were evaluating the PHQ‐9 in our cohort already, and did not want to increase responder burden by presenting them with 2 depression questionnaires.

We followed all patients until 30 days after discharge, and outcome data (all‐cause mortality or all‐cause readmission) were collected by research personnel blinded to the patient's frailty status at discharge using patient/caregiver self‐report and analysis of the provincial electronic health record. We included deaths in or out of the hospital, and all readmissions were unplanned.

We examined the correlation between the CFS score (5 vs <5) and (1) the modified Fried score (3 vs <3) and (2) TUGT (20 seconds vs >20 seconds) using chance corrected kappa coefficients. In our previous article[14] we reported the association between the CFS and readmissions/hospitalizations within 30 days of discharge. In this article we examine whether either the Fried score or TUGT accurately and independently predict postdischarge readmissions/deaths, and whether they add additional prognostic information to the CFS assessment by comparing models with/without each definition using the C statistic and the Integrated Discrimination Improvement index. All analyses were performed using SAS version 9.4 (SAS Institute, Cary, NC), with P values of <0.05 considered statistically significant. Subgroup analysis was done in patients older than 65 years.

RESULTS

Of 1124 potentially eligible patients, 626 were excluded because of patient refusal (n = 227); transfer to/from another hospital, long‐term care facility, or out of province (n = 189); moderate to severe cognitive impairment (n = 88); language barriers (n = 71); or foreshortened life expectancy (n = 51). Another 3 patients withdrew consent prior to outcome assessment. The 495 patients we recruited and had outcome data for had a mean age of 64 years, 19.6% were older than 80 years, 50% were women, and the patients had a mean of 4.2 comorbidities and mean Charlson score of 2.4. The 4 most common reasons for hospital admission were heart failure, pneumonia, chronic obstructive pulmonary disease, and urinary tract infection, and the median length of stay was 5 days (interquartile range: 49 days).

Prevalence of Frailty According to Different Definitions

Although the CFS assessment resulted in 162 (33%) patients being deemed frail, only 82 (51%) of those patients also met the phenotype frailty definition using either the Fried model or the TUGT, and 49 (10%) patients who were not classified as frail on the CFS met either of the phenotypic definitions of frailty (Figure 1). Overall, 211 (43%) patients were frail according to at least 1 assessment, and 46 (9%) met all 3 frailty definitions. In the subgroup of 245 patients older than 65 years, 137 (56%) were frail according to at least 1 assessment, 38 (16%) met all 3 frailty definitions, and 27 (11%) of those patients classified as not frail on the CFS met either phenotypic definition of frailty. Agreement between TUGT and CFS or CFS and Fried was relatively poor with kappas of 0.31 (95% confidence interval [CI]: 0.23‐0.40) and 0.33 (95% CI: 0.25‐0.42), respectively. It is noteworthy that some patients deemed nonfrail on the CFS had slow gait speeds, and most CFS‐frail patients had gait speeds in the nonfrail range (Figure 2).

Venn diagram illustrating the relationship between patients deemed frail using the Clinical Frailty Scale (CFS), Fried (FRIED), or Timed Up and Go Test (TUGT) assessments. The 284 nonfrail patients are represented by the space outside of the 3 intersecting circles, the 80 CFS frail patients are represented by the white space within the CFS circle, the 49 patients deemed frail using the modified Fried and/or TUGT but not the CFS are denoted by the hatched areas in the TUGT and Fried circles, and the 82 patients deemed frail using the CFS and either phenotype model are denoted by the grey area in the middle of the 3 circles.

Timed Up and Go Test (TUGT) times in adult patients stratified by their Clinical Frailty Scale (CFS) score.

Characteristics According to Frailty Status

Although frail patients were generally similar across definitions (Table 1) in that they were older, had more comorbidities, more hospitalizations in the prior year, and longer index hospitalization lengths of stay than nonfrail patients, patients meeting phenotypic definitions of frailty but not classified as frail on the CFS were younger, had lower Charlson scores, higher EQ‐5D scores, and were discharged with less medications (Table 1).

Table 1.Baseline Characteristics of Cohort Patients
	Not Frail on Any of the 3 Models, n = 284	Frail on the CFS Only, n = 80	Frail on the Fried and/or TUGT but Not the CFS, n = 49	Frail on CFS and Either Phenotype Model, n = 82	P Value Comparing the 3 Frailty Columns
NOTE: Definitions of frailty: scoring 5 on the CFS, 3 on the modified Fried score, >20 seconds on the TUGT. Abbreviations: CFS, Clinical Frailty Scale; CI, confidence interval; ICU, intensive care unit; IQR, interquartile range; EQ‐5D, EuroQoL Questionnaire; TUGT, Timed Up and Go Test.
Age, y, mean (95% CI)	57.3 (55.259.5)	69.1 (65.872.3)	63.1 (57.968.3)	75.8 (72.679.0)	<0.001
Sex, female, no (%)	118 (41.6)	49 (61.3)	27 (55.1)	56 (68.3)	0.3
No. of comorbidities, mean (95% CI)	4.2 (3.84.5)	6.0 (5.56.6)	4.0 (3.14.9)	6.5 (5.87.2)	<0.001
Charlson comorbidity score, mean (95% CI)	2.4 (2.12.6)	3.4 (3.03.9)	2.6 (2.03.2)	3.8 (3.34.2)	0.01
No. of patients hospitalized in prior 12 months, no (%)	93 (32.8)	44 (55.0)	27 (55.1)	54 (65.9)	0.3
Preadmission living situation, no (%)					0.01
Living at home independently	221 (77.8)	26 (32.5)	25 (51.0)	17 (20.7)
Living at home with help	59 (20.8)	43 (53.8)	19 (38.8)	48 (58.5)
Assisted living or lodge	4 (1.4)	11 (13.8)	5 (10.2)	17 (20.7)
EQ‐5D overall score, /100, mean (95% CI)	66.9 (65.068.9)	62.0 (57.666.4)	56.6 (51.361.8)	58.3 (53.962.7)	0.28
Goals of care in the hospital, no (%)					<0.0001
Resuscitation/ICU	228 (83.5)	41 (54.7)	39 (84.8)	29 (39.7)
ICU but no resuscitation	21(7.7)	17 (22.7)	1 (2.2)	16 (21.9)
No ICU, no resuscitation	23 (8.4)	17(22.7)	6 (13.0)	28 (37.8)
Comfort care	1 (0.4)	0	0	0
Timed Up and Go Test, s, mean (95% CI)	10.9 (10.411.3)	13.9 (12.914.9)	26.3 (19.033.6)	30.3 (26.833.7)	<0.0001
Grip strength, kg, mean (95% CI)	32.1 (30.733.5)	24.3 (22.3‐ 26.3)	22.1 (19.924.2)	17.7 (16.219.1)	<0.0001
Serum albumin, g/L, mean (95% CI)	34.2 (32.835.5)	35.0 (33.037.0)	31.1 (27.934.4)	33.1 (31.434.9)	0.07
No. of prescription medications at discharge, mean (95% CI)	5.2 (4.85.6)	8.8 (7.99.6)	6.1 (5.17.1)	8.2 (7.58.9)	<0.0001
Length of stay, d, median, [IQR]	5 [37]	6 [411]	7 [3.512]	7 [59]	0.02

Outcomes According to Frailty Status

The overall rate of 30‐day death or hospital readmission was 17.1% (85 patients), primarily as a result of hospital readmissions (81, 16.4%) (Table 2). Although patients classified as frail on the CFS exhibited significantly higher 30‐day readmission/death rates (24.1% vs 13.8% for not frail, P = 0.005) even after adjusting for age and sex (adjusted odds ratio [aOR]: 2.02, 95% CI: 1.19‐3.41) (Table 3), patients meeting either of the phenotypic definitions for frailty but not the CFS definition were not at higher risk for 30‐day readmission/death (aOR: 0.87, 95% CI: 0.34‐2.19) (Table 3). The group at highest risk for 30‐day readmissions/death were those meeting both the CFS and either phenotypic definition of frailty (25.6% vs 13.8% for those not frail, aOR: 2.15, 95% CI: 1.10‐4.19) (Tables 2 and 3). None of the Integrated Discrimination Improvement indices (for modified Fried added to CFS or TUGT added to CFS) were statistically significant, suggesting no net new information was added to predictive models, and there were no appreciable changes in C statistics (Table 3). Neither the modified Fried score nor the TUGT on their own added independent prognostic information to age/sex alone as predictors of postdischarge outcomes. It is noteworthy that the areas under the curve for models using any combination of the frailty definitions plus age and sex were not high (all ranged between 0.55 and 0.60 for the overall cohort and from 0.52 and 0.65 in the elderly). If the frailty definitions were examined as continuous variables rather than dichotomized into frail/not frail, the C statistics were not appreciably better: 0.65 for CFS, 0.58 for TUGT, and 0.60 for modified Fried. Of note, the CFS score with the published cutoff of 5 demonstrated the highest kappa, sensitivity, specificity, and positive predictive value in relation to outcomes.

Table 2.Outcomes for Patients Deemed Frail Using the CFS, Fried, or TUGT Assessments
Outcomes (Not Mutually Exclusive)	Not Frail on Any of the 3 Models	Frail on the CFS Only	Frail on the Fried and/or TUGT	Frail on CFS and Either Phenotype Model	P Value Comparing the 3 Frailty Columns
NOTE: Data are presented as no. (%). Definitions of frailty: scoring 5 on the CFS, 3 on the modified Fried score, >20 seconds on the TUGT. Abbreviations: CFS, Clinical Frailty Scale; ER = emergency room; TUGT, Timed Up and Go Test.
Entire cohort	n = 284	n = 80	n = 49	n = 82
Discharge disposition					<0.002
Live at home independently	203 (71.5)	16 (20.0)	19 (38.8)	10 (12.2)
Live at home with help	77 (27.1)	52 (65.0)	25 (51.0)	50 (61.0)
Assisted living or lodge	4 (9.3)	12 (15.0)	5 (10.2)	22 (26.8)
30‐day readmission or death	40 (14.1)	18 (22.5)	6 (12.2)	21 (25.6)	0.2
30‐day hospital readmission	39 (13.8)	18 (22.5)	6 (12.2)	18 (22.0)	0.31
Death	5 (1.8)	3 (3.8)	1 (2.0)	4 (4.9)	0.9
30‐day ER visit	66 (23.2)	30 (37.5)	12 (24.5)	23 (17.6)	0.25
Patients aged 65 years or older	n = 108	n = 47	n = 27	n = 63
Discharge disposition					0.03
Live at home independently	69 (63.9)	9 (19.2)	10 (37.0)	6 (9.5)
Live at home with help	36 (33.3)	30 (63.8)	13 (48.2)	39(61.9)
Assisted living or lodge	3 (3.8)	8 (17.0)	4 (14.8)	18 (28.6)
30‐day readmission or death	13 (12.0)	13 (27.7)	3 (11.1)	17 (27.0)	0.22
30‐day hospital readmission	12 (11.1)	13 (27.7)	3 (11.1)	14 (22.2)	0.26
Death	2 (1.9)	3 (6.4)	1 (3.7)	3 (4.8)	0.87
30‐day ER visit	20 (18.5)	17 (36.2)	6 (22.2)	18 (28.6)	0.45

Table 3.Predictive Ability of Different Frailty Assessment Methods Adjusted for Age and Sex
Frailty Definition	Adjusted Odds Ratio for 30‐Day Readmission/Death	95% CI	C Statistic for Model Predicting 30‐Day Readmission/Death Including Age, Sex, and Frailty Definition (95% CI)
NOTE: Definitions of frailty: scoring 5 on the CFS, 3 on the modified Fried score, >20 seconds on the TUGT. Abbreviations: CFS, Clinical Frailty Scale; CI, confidence interval; TUGT, Timed Up and Go Test.
Entire cohort
CFS (overall)	2.02	1.193.41	0.60 (0.530.65)
CFS (plus either phenotype model)	2.15	1.104.19	0.60 (0.520.64)
CFS (but neither phenotype model)	1.81	0.943.48	0.60 (0.520.64)
Fried	1.32	0.752.30	0.55 (0.560.58)
TUGT	1.34	0.732.44	0.55 (0.460.58)
Fried and/or TUGT	0.87	0.342.19	0.55 (0.470.58)
Patients aged 65 years or older
CFS (overall)	3.20	1.556.60	0.65 (0.560.73)
CFS (plus either phenotype model)	3.20	1.337.68	0.65 (0.550.72)
CFS (but neither phenotype model)	3.08	1.267.47	0.65 (0.550.72)
Fried	1.28	0.642.56	0.52 (0.390.53)
TUGT	1.44	0.702.97	0.52 (0.390.53)
Fried and/or TUGT	1.41	0.722.78	0.54 (0.420.56)

Outcomes According to Frailty Status in the Elderly Subgroup

Although absolute risks of readmission or death were higher in elderly patients than younger patients, the excess risk was largely seen in those elderly patients classified as frail on the CFS. In fact, all of the associations reported above for the entire cohort were in the same direction in the elderly subgroup (Tables 2 and 3).

DISCUSSION

In summary, we found that of patients being discharged from general medical wards who were frail according to at least 1 of the 3 tools we used, only 22% met all 3 frailty case definitions (including only 28% of elderly patients deemed frail by at least 1 definition). There was surprisingly poor correlation between phenotypic markers of frailty such as poor mobility (slow TUGT) or the modified Fried Index and the CFS, even amongt elderly patients. The most clinically useful of the frailty assessment tools (both overall and in those patients who are elderly) appears to be the CFS, because it more accurately identifies those at higher risk of adverse outcomes after discharge, does not require special equipment to conduct, and is faster to do than the phenotypic assessment models we tested. We have also previously demonstrated that the CFS, after a brief training period identical to that used in this study, is reproducible between observers[19] and remains an independent predictor of adverse 30‐day outcomes even after adjusting for age, sex, comorbidities, and the LACE (length of stay, acuity of the admission, comorbidity, emergency room visits during the previous 6 months) score.[14]

Although some[10] have advocated for the use of mobility assessments (such as gait speed) as a frailty marker due to its ease of measurement and objectivity, we found that slow TUGT (which is a marker for mobility and not just slow gait speed) was not an independent prognostic marker for postdischarge outcomes. We hypothesize that the phenotypic models of frailty performed less well than the CFS as they focus on the measurement of particular physical attributes and do not take into account cognitive or psychosocial characteristics or comorbidity burden that also influence postdischarge outcomes. As well, the CFS captures the patients' baseline status prior to acute illness, whereas the phenotypic measures were assessed just prior to discharge and thus may provide less information about eventual recovery potential. Some have suggested that repeating phenotype measures postdischarge might be more informative,[20] but this would reduce clinical applicability a great deal. Certainly, an analysis[21] of the Cardiovascular Health Study cohort demonstrated that cumulative deficit models of frailty (for which the CFS is an accurate proxy[9, 15]) better predicted risk of death than phenotypic models.

Although a number of published studies have shown similar results to ours in that frail patients are at greater risk for death and/or hospitalization,[22, 23, 24] there is surprisingly little literature on the comparative predictive performance of the different frailty instruments and the extent to which they overlap. Cigolle et al.[25] compared 3 frailty scales (the Functional Domain Model, the Burden Model, and the Fried score) in the Health and Retirement Study and, similarly to us, found that although 30.2% were frail on at least 1 of these scales, only 3.1% were deemed frail by all 3. The Conselice Study of Brain Aging[5] also reported that a deficit accumulation model defined a much higher prevalence of frailty (37.6%) than the 11.6% identified using the phenotypic Study of Osteoporotic Fractures (SOF) index based on weight loss, mobility, and level of energy. Another study[26] reported that risk models incorporating either the SOF index or the Fried score exhibited C statistics of only 0.61 for predicting falls in elderly females. A cohort study[27] from 2 English general medical units also found that none of the 5 frailty models was particularly accurate at predicting risk of readmission at 3 months, with C statistics ranging between 0.52 and 0.57. Although frailty assessment at time of hospital admission predicted in‐hospital mortality and length of stay in another English study, it was not independently associated with 30‐day outcomes after adjusting for age, sex, and comorbidities including dementia.[27] To our knowledge, these latter 2 are the only other studies reported to date performed in hospitalized patients to assess whether frailty assessment helps predict postdischarge outcomes. Thus, the poor C statistics we found for all of our frailty tools confirms prior literature that frailty assessment alone is inadequate to accurately identify those patients at highest risk for poor outcomes in the first 30 days after discharge. However, frailty assessment together with consideration of each individual's comorbidities, cognitive status, psychosocial circumstances, and environment can be useful to flag those individuals who may need extra attention postdischarge to optimize outcomes.

Strengths and Limitations

Although this was a prospective cohort study with blinded ascertainment of endpoints (30‐day outcome data were collected by observers who were unaware of the patients' CFS or phenotypic model scores), it is not without limitations. First, the only postdischarge outcomes we assessed were readmission and death, and it would be interesting to evaluate which frailty tools best predict those who are most likely to benefit from home‐care services in the community. Second, as we were interested in 30‐day readmission rates, we excluded long‐term care residents from our study and patients who had foreshortened life expectancy, in essence, the frailest of the frail. Although this reduced the size of any association between frailty and adverse outcomes, we focused this study on the situations where there is clinical equipoise and there is rarely a diagnostic dilemma around the identification of frailty and need for increased services in palliative or long‐term care patients. Third, we did not use exactly the same questionnaires or gait speed assessments as used in the original Fried score description, but as outlined in the Methods section, we used analogous questions on closely related questionnaires to extract the same information. Fourth, some might consider our comparisons biased toward the CFS, as it reflects gestalt clinical impressions (informed by patients and proxies) of frailty status before hospital admission while the Fried score and TUGT were based on patient status just prior to discharge, it may be that the former is a better measure of eventual recovery (and ongoing risk) than the latter measures. If this is the case, for the purposes of targeting interventions to prevent postdischarge complications, it would suggest to us that the CFS is better suited, whereas phenotype tools can be reserved for the postdischarge phase of recovery. By the same token, perhaps serial measures of the CFS and phenotypic tools are more important, as the trajectory of recovery may be most informative for risk prediction.[7] Certainly, if one were interested in changes in functional status during hospitalization,[29] then objective phenotypic measures such as grip strength or TUGT times would seem more appropriate choices. Fifth, some may perceive it as a weakness that we did not restrict our cohort to elderly patients; however, we actually view this as a strength, because frailty is not exclusive to older patients. Sixth, although we restricted this study to patients being discharged from general internal medicine wards, it is worth mentioning that previous studies have shown similar associations between frailty and outcomes in nonmedical hospitalized patients.[19, 22, 23, 24]

In conclusion, we looked at 3 different ways of screening for frailty, 1 being a subjective but well‐validated tool (the CFS) and the other 2 being objective assessments that look at specific phenotypic characteristics. There is a compelling need to find a standardized assessment to determine frailty in both research and clinical settings, and our study provides support for use of the CFS over the Fried or TUGT as screening tools. Standardized frailty assessments should be part of the discharge planning for all medical patients so that extra resources can be properly targeted at those patients at greatest risk for suboptimal transition back to community living.

Acknowledgements

The authors acknowledge Miriam Fradette and Debbie Boyko for their important contributions in data acquisition, as well as all the physicians rotating through the general internal medicine wards for their help in identifying the patients.

Disclosures: Author contributions are as follows: study concept and design: Finlay A. McAlister, Sumit R. Majumdar, and Raj Padwal; acquisition of patients and data: Sara Belga, Darren Lau, Jenelle Pederson, and Sharry Kahlon; analysis of data: Jeff Bakal, Sara Belga, Finlay A. McAlister; first draft of manuscript: Sara Belga and Finlay A. McAlister; critical revision of manuscript: all authors. Funding for this study was provided by an operating grant from Alberta InnovatesHealth Solutions. Alberta InnovatesHealth Solutions had no role in role in the design, methods, subject recruitment, data collections, analysis, or preparation of the article. Finlay A. McAlister and Sumit R. Majumdar hold career salary support from Alberta InnovatesHealth Solutions. Finlay A. McAlister holds the Chair in Cardiovascular Outcomes Research at the Mazankowski Heart Institute, University of Alberta. Sumit R. Majumdar holds the Endowed Chair in Patient Health Management from the Faculty of Medicine and Dentistry, and the Faculty of Pharmacy and Pharmaceutical Sciences, University of Alberta. The authors have no affiliations or financial interests with any organization or entity with a financial interest in the contents of this article. All authors had access to the data and played a role in writing and revising this article. The authors declare no conflicts of interest.

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Bagshaw SM, Stelfox HT, McDermid RC, et al. Association between frailty and short‐ and long‐term outcomes among critically ill patients: a multicenter prospective cohort study. CMAJ. 2013;186:e95–e102.
Dharmarajan K, Krumholz HM. Risk after hospitalization: we have a lot to learn. J Hosp Med. 2015;10:135–136.
Kulminski AM, Ukraintseva SV, Kulminskaya IV, Arbeev KG, Land K, Yashin AI. Cumulative deficits better characterize susceptibility to death in elderly people than phenotypic frailty: lessons from the Cardiovascular Health Study. J Am Geriatr Soc. 2008;56:898–903.
Dai YT, Wu SC, Weng R. Unplanned hospital readmission and its predictors in patients with chronic conditions. J Formos Med Assoc. 2002;101:779–785.
McAdams‐Demarco MA, Law A, Salter ML, et al. Frailty and early hospital readmission after kidney transplant. Am J Transplant. 2013;13:2091–2095.
Robinson TN, Wu DS, Pointer L, Dunn CL, Cleveland JC, Moss M. Simple frailty score predicts postoperative complications across surgical specialities. Am J Surg. 2013;206:544–550.
Cigolle CT, Ofstedal MB, Tian Z, Blaum CS. Comparing models of frailty: the Health and Retirement Study. J Am Geriatr Soc. 2009;57:830–839.
Ensrud KE, Ewing SK, Taylor BC, et al. Comparison of 2 frailty indexes for prediction of falls, disability, fractures, and death in older women. Arch Int Med. 2008;168:382–389.
Wou F, Gladman JR, Bradshaw L, Franklin M, Edmans J, Conroy SP. The predictive properties of frailty‐rating scales in the acute medical unit. Age Ageing. 2013;42:776–781.
Wallis SJ, Wall J, Biram RW, Romero‐Ortuno R. Association of the clinical frailty scale with hospital outcomes. QJM. 2015;108:943–949.
Covinsky KE, Pierluissi E, Johnston CB. Hospitalization‐associated disability: she was probably able to ambulate, but I'm not sure. JAMA. 2011;306:1782–1793.

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Journal of Hospital Medicine - 11(8)

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556-562

Read more about Frailty Evaluation in the Hospital

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Author(s)

Sara Belga, MD

Sharry Kahlon, MD

Jenelle Pederson, BA

Darren Lau, MD, PhD

Mary Forhan, MHSc, PhD

Jeffrey A. Bakal, PhD

Author(s)

Sara Belga, MD

Sharry Kahlon, MD

Jenelle Pederson, BA

Darren Lau, MD, PhD

Mary Forhan, MHSc, PhD

Jeffrey A. Bakal, PhD

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METHODS

Study Design and Population

RESULTS

Prevalence of Frailty According to Different Definitions

Characteristics According to Frailty Status

Table 1.Baseline Characteristics of Cohort Patients
	Not Frail on Any of the 3 Models, n = 284	Frail on the CFS Only, n = 80	Frail on the Fried and/or TUGT but Not the CFS, n = 49	Frail on CFS and Either Phenotype Model, n = 82	P Value Comparing the 3 Frailty Columns
NOTE: Definitions of frailty: scoring 5 on the CFS, 3 on the modified Fried score, >20 seconds on the TUGT. Abbreviations: CFS, Clinical Frailty Scale; CI, confidence interval; ICU, intensive care unit; IQR, interquartile range; EQ‐5D, EuroQoL Questionnaire; TUGT, Timed Up and Go Test.
Age, y, mean (95% CI)	57.3 (55.259.5)	69.1 (65.872.3)	63.1 (57.968.3)	75.8 (72.679.0)	<0.001
Sex, female, no (%)	118 (41.6)	49 (61.3)	27 (55.1)	56 (68.3)	0.3
No. of comorbidities, mean (95% CI)	4.2 (3.84.5)	6.0 (5.56.6)	4.0 (3.14.9)	6.5 (5.87.2)	<0.001
Charlson comorbidity score, mean (95% CI)	2.4 (2.12.6)	3.4 (3.03.9)	2.6 (2.03.2)	3.8 (3.34.2)	0.01
No. of patients hospitalized in prior 12 months, no (%)	93 (32.8)	44 (55.0)	27 (55.1)	54 (65.9)	0.3
Preadmission living situation, no (%)					0.01
Living at home independently	221 (77.8)	26 (32.5)	25 (51.0)	17 (20.7)
Living at home with help	59 (20.8)	43 (53.8)	19 (38.8)	48 (58.5)
Assisted living or lodge	4 (1.4)	11 (13.8)	5 (10.2)	17 (20.7)
EQ‐5D overall score, /100, mean (95% CI)	66.9 (65.068.9)	62.0 (57.666.4)	56.6 (51.361.8)	58.3 (53.962.7)	0.28
Goals of care in the hospital, no (%)					<0.0001
Resuscitation/ICU	228 (83.5)	41 (54.7)	39 (84.8)	29 (39.7)
ICU but no resuscitation	21(7.7)	17 (22.7)	1 (2.2)	16 (21.9)
No ICU, no resuscitation	23 (8.4)	17(22.7)	6 (13.0)	28 (37.8)
Comfort care	1 (0.4)	0	0	0
Timed Up and Go Test, s, mean (95% CI)	10.9 (10.411.3)	13.9 (12.914.9)	26.3 (19.033.6)	30.3 (26.833.7)	<0.0001
Grip strength, kg, mean (95% CI)	32.1 (30.733.5)	24.3 (22.3‐ 26.3)	22.1 (19.924.2)	17.7 (16.219.1)	<0.0001
Serum albumin, g/L, mean (95% CI)	34.2 (32.835.5)	35.0 (33.037.0)	31.1 (27.934.4)	33.1 (31.434.9)	0.07
No. of prescription medications at discharge, mean (95% CI)	5.2 (4.85.6)	8.8 (7.99.6)	6.1 (5.17.1)	8.2 (7.58.9)	<0.0001
Length of stay, d, median, [IQR]	5 [37]	6 [411]	7 [3.512]	7 [59]	0.02

Outcomes According to Frailty Status

Table 2.Outcomes for Patients Deemed Frail Using the CFS, Fried, or TUGT Assessments
Outcomes (Not Mutually Exclusive)	Not Frail on Any of the 3 Models	Frail on the CFS Only	Frail on the Fried and/or TUGT	Frail on CFS and Either Phenotype Model	P Value Comparing the 3 Frailty Columns
NOTE: Data are presented as no. (%). Definitions of frailty: scoring 5 on the CFS, 3 on the modified Fried score, >20 seconds on the TUGT. Abbreviations: CFS, Clinical Frailty Scale; ER = emergency room; TUGT, Timed Up and Go Test.
Entire cohort	n = 284	n = 80	n = 49	n = 82
Discharge disposition					<0.002
Live at home independently	203 (71.5)	16 (20.0)	19 (38.8)	10 (12.2)
Live at home with help	77 (27.1)	52 (65.0)	25 (51.0)	50 (61.0)
Assisted living or lodge	4 (9.3)	12 (15.0)	5 (10.2)	22 (26.8)
30‐day readmission or death	40 (14.1)	18 (22.5)	6 (12.2)	21 (25.6)	0.2
30‐day hospital readmission	39 (13.8)	18 (22.5)	6 (12.2)	18 (22.0)	0.31
Death	5 (1.8)	3 (3.8)	1 (2.0)	4 (4.9)	0.9
30‐day ER visit	66 (23.2)	30 (37.5)	12 (24.5)	23 (17.6)	0.25
Patients aged 65 years or older	n = 108	n = 47	n = 27	n = 63
Discharge disposition					0.03
Live at home independently	69 (63.9)	9 (19.2)	10 (37.0)	6 (9.5)
Live at home with help	36 (33.3)	30 (63.8)	13 (48.2)	39(61.9)
Assisted living or lodge	3 (3.8)	8 (17.0)	4 (14.8)	18 (28.6)
30‐day readmission or death	13 (12.0)	13 (27.7)	3 (11.1)	17 (27.0)	0.22
30‐day hospital readmission	12 (11.1)	13 (27.7)	3 (11.1)	14 (22.2)	0.26
Death	2 (1.9)	3 (6.4)	1 (3.7)	3 (4.8)	0.87
30‐day ER visit	20 (18.5)	17 (36.2)	6 (22.2)	18 (28.6)	0.45

Table 3.Predictive Ability of Different Frailty Assessment Methods Adjusted for Age and Sex
Frailty Definition	Adjusted Odds Ratio for 30‐Day Readmission/Death	95% CI	C Statistic for Model Predicting 30‐Day Readmission/Death Including Age, Sex, and Frailty Definition (95% CI)
NOTE: Definitions of frailty: scoring 5 on the CFS, 3 on the modified Fried score, >20 seconds on the TUGT. Abbreviations: CFS, Clinical Frailty Scale; CI, confidence interval; TUGT, Timed Up and Go Test.
Entire cohort
CFS (overall)	2.02	1.193.41	0.60 (0.530.65)
CFS (plus either phenotype model)	2.15	1.104.19	0.60 (0.520.64)
CFS (but neither phenotype model)	1.81	0.943.48	0.60 (0.520.64)
Fried	1.32	0.752.30	0.55 (0.560.58)
TUGT	1.34	0.732.44	0.55 (0.460.58)
Fried and/or TUGT	0.87	0.342.19	0.55 (0.470.58)
Patients aged 65 years or older
CFS (overall)	3.20	1.556.60	0.65 (0.560.73)
CFS (plus either phenotype model)	3.20	1.337.68	0.65 (0.550.72)
CFS (but neither phenotype model)	3.08	1.267.47	0.65 (0.550.72)
Fried	1.28	0.642.56	0.52 (0.390.53)
TUGT	1.44	0.702.97	0.52 (0.390.53)
Fried and/or TUGT	1.41	0.722.78	0.54 (0.420.56)

Outcomes According to Frailty Status in the Elderly Subgroup

DISCUSSION

Strengths and Limitations

Acknowledgements

METHODS

Study Design and Population

RESULTS

Prevalence of Frailty According to Different Definitions

Characteristics According to Frailty Status

Table 1.Baseline Characteristics of Cohort Patients
	Not Frail on Any of the 3 Models, n = 284	Frail on the CFS Only, n = 80	Frail on the Fried and/or TUGT but Not the CFS, n = 49	Frail on CFS and Either Phenotype Model, n = 82	P Value Comparing the 3 Frailty Columns
NOTE: Definitions of frailty: scoring 5 on the CFS, 3 on the modified Fried score, >20 seconds on the TUGT. Abbreviations: CFS, Clinical Frailty Scale; CI, confidence interval; ICU, intensive care unit; IQR, interquartile range; EQ‐5D, EuroQoL Questionnaire; TUGT, Timed Up and Go Test.
Age, y, mean (95% CI)	57.3 (55.259.5)	69.1 (65.872.3)	63.1 (57.968.3)	75.8 (72.679.0)	<0.001
Sex, female, no (%)	118 (41.6)	49 (61.3)	27 (55.1)	56 (68.3)	0.3
No. of comorbidities, mean (95% CI)	4.2 (3.84.5)	6.0 (5.56.6)	4.0 (3.14.9)	6.5 (5.87.2)	<0.001
Charlson comorbidity score, mean (95% CI)	2.4 (2.12.6)	3.4 (3.03.9)	2.6 (2.03.2)	3.8 (3.34.2)	0.01
No. of patients hospitalized in prior 12 months, no (%)	93 (32.8)	44 (55.0)	27 (55.1)	54 (65.9)	0.3
Preadmission living situation, no (%)					0.01
Living at home independently	221 (77.8)	26 (32.5)	25 (51.0)	17 (20.7)
Living at home with help	59 (20.8)	43 (53.8)	19 (38.8)	48 (58.5)
Assisted living or lodge	4 (1.4)	11 (13.8)	5 (10.2)	17 (20.7)
EQ‐5D overall score, /100, mean (95% CI)	66.9 (65.068.9)	62.0 (57.666.4)	56.6 (51.361.8)	58.3 (53.962.7)	0.28
Goals of care in the hospital, no (%)					<0.0001
Resuscitation/ICU	228 (83.5)	41 (54.7)	39 (84.8)	29 (39.7)
ICU but no resuscitation	21(7.7)	17 (22.7)	1 (2.2)	16 (21.9)
No ICU, no resuscitation	23 (8.4)	17(22.7)	6 (13.0)	28 (37.8)
Comfort care	1 (0.4)	0	0	0
Timed Up and Go Test, s, mean (95% CI)	10.9 (10.411.3)	13.9 (12.914.9)	26.3 (19.033.6)	30.3 (26.833.7)	<0.0001
Grip strength, kg, mean (95% CI)	32.1 (30.733.5)	24.3 (22.3‐ 26.3)	22.1 (19.924.2)	17.7 (16.219.1)	<0.0001
Serum albumin, g/L, mean (95% CI)	34.2 (32.835.5)	35.0 (33.037.0)	31.1 (27.934.4)	33.1 (31.434.9)	0.07
No. of prescription medications at discharge, mean (95% CI)	5.2 (4.85.6)	8.8 (7.99.6)	6.1 (5.17.1)	8.2 (7.58.9)	<0.0001
Length of stay, d, median, [IQR]	5 [37]	6 [411]	7 [3.512]	7 [59]	0.02

Outcomes According to Frailty Status

Table 2.Outcomes for Patients Deemed Frail Using the CFS, Fried, or TUGT Assessments
Outcomes (Not Mutually Exclusive)	Not Frail on Any of the 3 Models	Frail on the CFS Only	Frail on the Fried and/or TUGT	Frail on CFS and Either Phenotype Model	P Value Comparing the 3 Frailty Columns
NOTE: Data are presented as no. (%). Definitions of frailty: scoring 5 on the CFS, 3 on the modified Fried score, >20 seconds on the TUGT. Abbreviations: CFS, Clinical Frailty Scale; ER = emergency room; TUGT, Timed Up and Go Test.
Entire cohort	n = 284	n = 80	n = 49	n = 82
Discharge disposition					<0.002
Live at home independently	203 (71.5)	16 (20.0)	19 (38.8)	10 (12.2)
Live at home with help	77 (27.1)	52 (65.0)	25 (51.0)	50 (61.0)
Assisted living or lodge	4 (9.3)	12 (15.0)	5 (10.2)	22 (26.8)
30‐day readmission or death	40 (14.1)	18 (22.5)	6 (12.2)	21 (25.6)	0.2
30‐day hospital readmission	39 (13.8)	18 (22.5)	6 (12.2)	18 (22.0)	0.31
Death	5 (1.8)	3 (3.8)	1 (2.0)	4 (4.9)	0.9
30‐day ER visit	66 (23.2)	30 (37.5)	12 (24.5)	23 (17.6)	0.25
Patients aged 65 years or older	n = 108	n = 47	n = 27	n = 63
Discharge disposition					0.03
Live at home independently	69 (63.9)	9 (19.2)	10 (37.0)	6 (9.5)
Live at home with help	36 (33.3)	30 (63.8)	13 (48.2)	39(61.9)
Assisted living or lodge	3 (3.8)	8 (17.0)	4 (14.8)	18 (28.6)
30‐day readmission or death	13 (12.0)	13 (27.7)	3 (11.1)	17 (27.0)	0.22
30‐day hospital readmission	12 (11.1)	13 (27.7)	3 (11.1)	14 (22.2)	0.26
Death	2 (1.9)	3 (6.4)	1 (3.7)	3 (4.8)	0.87
30‐day ER visit	20 (18.5)	17 (36.2)	6 (22.2)	18 (28.6)	0.45

Table 3.Predictive Ability of Different Frailty Assessment Methods Adjusted for Age and Sex
Frailty Definition	Adjusted Odds Ratio for 30‐Day Readmission/Death	95% CI	C Statistic for Model Predicting 30‐Day Readmission/Death Including Age, Sex, and Frailty Definition (95% CI)
NOTE: Definitions of frailty: scoring 5 on the CFS, 3 on the modified Fried score, >20 seconds on the TUGT. Abbreviations: CFS, Clinical Frailty Scale; CI, confidence interval; TUGT, Timed Up and Go Test.
Entire cohort
CFS (overall)	2.02	1.193.41	0.60 (0.530.65)
CFS (plus either phenotype model)	2.15	1.104.19	0.60 (0.520.64)
CFS (but neither phenotype model)	1.81	0.943.48	0.60 (0.520.64)
Fried	1.32	0.752.30	0.55 (0.560.58)
TUGT	1.34	0.732.44	0.55 (0.460.58)
Fried and/or TUGT	0.87	0.342.19	0.55 (0.470.58)
Patients aged 65 years or older
CFS (overall)	3.20	1.556.60	0.65 (0.560.73)
CFS (plus either phenotype model)	3.20	1.337.68	0.65 (0.550.72)
CFS (but neither phenotype model)	3.08	1.267.47	0.65 (0.550.72)
Fried	1.28	0.642.56	0.52 (0.390.53)
TUGT	1.44	0.702.97	0.52 (0.390.53)
Fried and/or TUGT	1.41	0.722.78	0.54 (0.420.56)

Outcomes According to Frailty Status in the Elderly Subgroup

DISCUSSION

Strengths and Limitations

Acknowledgements

References

Fried LP, Ferrucci L, Darer J, Williamson JD, Anderson G. Untangling the concepts of disability, frailty, and comorbidity: implications for improved targeting and care. J Gerontol A Biol Sci Med Sci. 2004;59:255–263.
Sternberg SA, Wershof Schwartz A, Karunananthan S, Bergman H, Clarfield MA. The identification of frailty: a systematic literature review. J Am Geriatr Soc. 2011;59:2129–2138.
Clegg A, Young J, Iliffe S, Rikkert MO, Rockwood K. Frailty in elderly people. Lancet. 2013;381:752–762.
Vries NM, Staal JB, Ravensberg CD, Hobbelen JS, Rikkert MG, Sanden MW. Outcome instruments to measure frailty: a systematic review. Ageing Res Rev. 2011;10:104–114.
Forti P, Rietti E, Pisacane N, Olivelli V, Maltoni B, Ravaglia G. A comparison of frailty indexes for prediction of adverse health outcomes in a elderly cohort. Arch Gerontol Geriatr. 2012;54:16–20.
Fried LP, Tangen CM, Walston J, et al. Frailty in older adults: evidence for a phenotype. J Gerontol A Biol Sci Med Sci. 2001;56:M146–M156.
Collard RM, Boter H, Schoevers RA, Voshaar RC. Prevalence of frailty in community‐dwelling older persons: a systematic review. J Am Geriatr Soc. 2012;60:1487–1492.
Puts MT, Lips P, Deeg DJ. Sex differences in the risk of frailty for mortality independent of disability of chronic diseases. J Am Geriatr Soc. 2005;53:40–47.
Rockwood K, Andrew M, Mintnitski A. A comparison of two approaches to measuring frailty in elderly people. J Gerontol. 2007;62:738–743.
Cummings SR, Studenski S, Ferrucci L. A diagnosis of dismobility—giving mobility clinical visibility: a mobility working group recommendation. JAMA. 2014;311:2061–2062.
Studenski S, Perera S, Patel K, et al. Gait speed and survival in older adults. JAMA. 2011;301:50–58.
Afilalo J, Alexander KP, Mack MJ, et al. Frailty assessment in the cardiovascular care of older adults. J Am Coll Cardiol. 2014;63:747–762.
Podsiadlo D, Richardson S. The timed “Up and Go” test: a test of basic functional mobility for frail elderly persons. J Am Geriatr Soc. 1991;39:142–148.
Kahlon S, Pederson J, Majumdar SR, et al. Association between frailty and 30‐day outcomes after discharge from hospital. CMAJ. 2015;187:799–804.
Rockwood K, Song X, MacKnight C, et al. A global clinical measure of fitness and frailty in elderly people. CMAJ. 2005;173:489–495.
Cawthon PM, Fox KM, Gandra SR, et al. Do muscle mass, muscle density, strength, and physical function similarly influence risk of hospitalization in older adults? J Am Geriatr Soc. 2009;57:1411–1419.
Wang CY, Chen LY. Grip strength in older adults: test‐retest reliability and cutoff for subjective weakness of using the hands in heavy tasks. Arch Phys Med Rehabil. 2010;91:1747–1751.
Kroenke K, Spitzer RL. The PHQ‐9: a new depression measure. Psychiatr Ann. 2002;32:509–515.
Bagshaw SM, Stelfox HT, McDermid RC, et al. Association between frailty and short‐ and long‐term outcomes among critically ill patients: a multicenter prospective cohort study. CMAJ. 2013;186:e95–e102.
Dharmarajan K, Krumholz HM. Risk after hospitalization: we have a lot to learn. J Hosp Med. 2015;10:135–136.
Kulminski AM, Ukraintseva SV, Kulminskaya IV, Arbeev KG, Land K, Yashin AI. Cumulative deficits better characterize susceptibility to death in elderly people than phenotypic frailty: lessons from the Cardiovascular Health Study. J Am Geriatr Soc. 2008;56:898–903.
Dai YT, Wu SC, Weng R. Unplanned hospital readmission and its predictors in patients with chronic conditions. J Formos Med Assoc. 2002;101:779–785.
McAdams‐Demarco MA, Law A, Salter ML, et al. Frailty and early hospital readmission after kidney transplant. Am J Transplant. 2013;13:2091–2095.
Robinson TN, Wu DS, Pointer L, Dunn CL, Cleveland JC, Moss M. Simple frailty score predicts postoperative complications across surgical specialities. Am J Surg. 2013;206:544–550.
Cigolle CT, Ofstedal MB, Tian Z, Blaum CS. Comparing models of frailty: the Health and Retirement Study. J Am Geriatr Soc. 2009;57:830–839.
Ensrud KE, Ewing SK, Taylor BC, et al. Comparison of 2 frailty indexes for prediction of falls, disability, fractures, and death in older women. Arch Int Med. 2008;168:382–389.
Wou F, Gladman JR, Bradshaw L, Franklin M, Edmans J, Conroy SP. The predictive properties of frailty‐rating scales in the acute medical unit. Age Ageing. 2013;42:776–781.
Wallis SJ, Wall J, Biram RW, Romero‐Ortuno R. Association of the clinical frailty scale with hospital outcomes. QJM. 2015;108:943–949.
Covinsky KE, Pierluissi E, Johnston CB. Hospitalization‐associated disability: she was probably able to ambulate, but I'm not sure. JAMA. 2011;306:1782–1793.

References

Fried LP, Ferrucci L, Darer J, Williamson JD, Anderson G. Untangling the concepts of disability, frailty, and comorbidity: implications for improved targeting and care. J Gerontol A Biol Sci Med Sci. 2004;59:255–263.
Sternberg SA, Wershof Schwartz A, Karunananthan S, Bergman H, Clarfield MA. The identification of frailty: a systematic literature review. J Am Geriatr Soc. 2011;59:2129–2138.
Clegg A, Young J, Iliffe S, Rikkert MO, Rockwood K. Frailty in elderly people. Lancet. 2013;381:752–762.
Vries NM, Staal JB, Ravensberg CD, Hobbelen JS, Rikkert MG, Sanden MW. Outcome instruments to measure frailty: a systematic review. Ageing Res Rev. 2011;10:104–114.
Forti P, Rietti E, Pisacane N, Olivelli V, Maltoni B, Ravaglia G. A comparison of frailty indexes for prediction of adverse health outcomes in a elderly cohort. Arch Gerontol Geriatr. 2012;54:16–20.
Fried LP, Tangen CM, Walston J, et al. Frailty in older adults: evidence for a phenotype. J Gerontol A Biol Sci Med Sci. 2001;56:M146–M156.
Collard RM, Boter H, Schoevers RA, Voshaar RC. Prevalence of frailty in community‐dwelling older persons: a systematic review. J Am Geriatr Soc. 2012;60:1487–1492.
Puts MT, Lips P, Deeg DJ. Sex differences in the risk of frailty for mortality independent of disability of chronic diseases. J Am Geriatr Soc. 2005;53:40–47.
Rockwood K, Andrew M, Mintnitski A. A comparison of two approaches to measuring frailty in elderly people. J Gerontol. 2007;62:738–743.
Cummings SR, Studenski S, Ferrucci L. A diagnosis of dismobility—giving mobility clinical visibility: a mobility working group recommendation. JAMA. 2014;311:2061–2062.
Studenski S, Perera S, Patel K, et al. Gait speed and survival in older adults. JAMA. 2011;301:50–58.
Afilalo J, Alexander KP, Mack MJ, et al. Frailty assessment in the cardiovascular care of older adults. J Am Coll Cardiol. 2014;63:747–762.
Podsiadlo D, Richardson S. The timed “Up and Go” test: a test of basic functional mobility for frail elderly persons. J Am Geriatr Soc. 1991;39:142–148.
Kahlon S, Pederson J, Majumdar SR, et al. Association between frailty and 30‐day outcomes after discharge from hospital. CMAJ. 2015;187:799–804.
Rockwood K, Song X, MacKnight C, et al. A global clinical measure of fitness and frailty in elderly people. CMAJ. 2005;173:489–495.
Cawthon PM, Fox KM, Gandra SR, et al. Do muscle mass, muscle density, strength, and physical function similarly influence risk of hospitalization in older adults? J Am Geriatr Soc. 2009;57:1411–1419.
Wang CY, Chen LY. Grip strength in older adults: test‐retest reliability and cutoff for subjective weakness of using the hands in heavy tasks. Arch Phys Med Rehabil. 2010;91:1747–1751.
Kroenke K, Spitzer RL. The PHQ‐9: a new depression measure. Psychiatr Ann. 2002;32:509–515.
Bagshaw SM, Stelfox HT, McDermid RC, et al. Association between frailty and short‐ and long‐term outcomes among critically ill patients: a multicenter prospective cohort study. CMAJ. 2013;186:e95–e102.
Dharmarajan K, Krumholz HM. Risk after hospitalization: we have a lot to learn. J Hosp Med. 2015;10:135–136.
Kulminski AM, Ukraintseva SV, Kulminskaya IV, Arbeev KG, Land K, Yashin AI. Cumulative deficits better characterize susceptibility to death in elderly people than phenotypic frailty: lessons from the Cardiovascular Health Study. J Am Geriatr Soc. 2008;56:898–903.
Dai YT, Wu SC, Weng R. Unplanned hospital readmission and its predictors in patients with chronic conditions. J Formos Med Assoc. 2002;101:779–785.
McAdams‐Demarco MA, Law A, Salter ML, et al. Frailty and early hospital readmission after kidney transplant. Am J Transplant. 2013;13:2091–2095.
Robinson TN, Wu DS, Pointer L, Dunn CL, Cleveland JC, Moss M. Simple frailty score predicts postoperative complications across surgical specialities. Am J Surg. 2013;206:544–550.
Cigolle CT, Ofstedal MB, Tian Z, Blaum CS. Comparing models of frailty: the Health and Retirement Study. J Am Geriatr Soc. 2009;57:830–839.
Ensrud KE, Ewing SK, Taylor BC, et al. Comparison of 2 frailty indexes for prediction of falls, disability, fractures, and death in older women. Arch Int Med. 2008;168:382–389.
Wou F, Gladman JR, Bradshaw L, Franklin M, Edmans J, Conroy SP. The predictive properties of frailty‐rating scales in the acute medical unit. Age Ageing. 2013;42:776–781.
Wallis SJ, Wall J, Biram RW, Romero‐Ortuno R. Association of the clinical frailty scale with hospital outcomes. QJM. 2015;108:943–949.
Covinsky KE, Pierluissi E, Johnston CB. Hospitalization‐associated disability: she was probably able to ambulate, but I'm not sure. JAMA. 2011;306:1782–1793.

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Comparing three different measures of frailty in medical inpatients: Multicenter prospective cohort study examining 30‐day risk of readmission or death

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Comparing three different measures of frailty in medical inpatients: Multicenter prospective cohort study examining 30‐day risk of readmission or death

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Address for correspondence and reprint requests: Finlay A. McAlister, MD, 5‐134C Clinical Sciences Building, University of Alberta, 11350 83 Avenue, Edmonton, Alberta, Canada T6G 2G3; Telephone: 780‐492‐9824; Fax: 780‐492‐7277; E‐mail: [email protected]

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Similar Outcomes From Weekend Discharge

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Similar outcomes among general medicine patients discharged on weekends

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Erik Youngson, MMath

Hospitals typically reduce staffing levels and the availability of diagnostic, laboratory, and treatment services on weekends, and patients admitted on weekends exhibit poorer in‐hospital outcomes for several medical conditions.[1, 2, 3, 4, 5, 6, 7, 8, 9] Whether or not patients discharged on weekends have worse clinical outcomes has been less well studied.[10, 11, 12] Discharge rates on Saturday and Sunday are lower than for the other 5 days of the week,[12] but bed shortages and hospital overcrowding have increased the demand for maximizing 24/7 week‐round discharge efficiency. Given that the number of patients discharged on weekends is likely to continue to increase, it is important to assess the risk of weekend discharge on outcomes monitored as performance indicators by organizations such as the Centers for Medicare and Medicaid Services, the American Medical Association Physicians Consortium for Performance Improvement, the National Quality Forum, and the Joint Commission.

Thus, we designed this study to evaluate baseline characteristics, length of stay (LOS), and postdischarge outcomes for general internal medicine (GIM) patients in teaching hospitals discharged on weekends compared to weekdays. Our objective was to determine whether postdischarge outcomes differed for patients discharged on weekends versus weekdays.

METHODS

Study Setting

The Canadian province of Alberta has a single vertically integrated healthcare system that is government‐funded and provides universal access to hospitals, emergency departments (EDs), and outpatient physician services for all 4.1 million Albertans as well as all prescription medications for the poor, socially disadvantaged, disabled, or those age 65 years and older. This study received approval from the University of Alberta Health Research Ethics Board with waiver of informed consent.

Data Sources

This study used deidentified linked data from 3 Alberta Health administrative databases that capture vital status and all hospital or ED visits and have previously been shown to have high accuracy for medical diagnoses.[13] The Alberta Health Care Insurance Plan Registry tracks date of death or emigration from the province. The Discharge Abstract Database includes the most responsible diagnosis identified by the hospital attending physician, up to 25 other diagnoses coded by nosologists in each hospital, the admission and discharge dates, and the admission category (elective or urgent/emergent) for all acute care hospitalizations. Of note, unlike US studies, the hospital databases are able to distinguish in‐hospital (eg, adverse events) versus premorbid diagnoses (eg, preexisting comorbidities). The Ambulatory Care Database captures all patient visits to EDs with coding for up to 10 conditions per encounter.

Study Cohort

We identified all adults with an acute care hospitalization on the GIM services at all 7 Alberta teaching hospitals (ie, defined as those with Royal College of Physicians and Surgeons of Canadaapproved residency training programs in internal medicine, the equivalent of the Association of American Medical Colleges certification in the United States) between October 1, 2009 and September 30, 2010 and between April 1, 2011 and December 1, 2011 (these 20 months covered most of the pre/post intervals for a recently reported quality improvement initiative at 1 of the teaching hospitals that had no significant impact on postdischarge outcomes).[14] Patients from out of the province or transferred from/to another inpatient service (eg, the intensive care unit, a different service in the same hospital [such as surgery], another acute care hospital, or rehabilitation hospital) or with lengths of stay greater than 30 days were excluded. We only included the first hospitalization for any patient in our study timeframe and thus excluded repeat discharges of the same patient.

Explanatory Variable of Interest

The independent variable of interest was calendar day of discharge, stratified according to weekday (Monday thru Friday) versus weekend (Saturday and Sunday). Only 1.4% of weekday discharges occurred on a statutory holiday, and for the purposes of this study, these discharges were also considered weekend discharges. At the 7 teaching hospitals in Alberta, nursing staffing ratios do not differ between weekend and weekday, but availability of all other members of the healthcare team does. Physician census decreases from 4 to 5 per ward to 1 to 2, and ward‐based social workers, occupational therapists, physiotherapists, and pharmacist educators are generally not available on weekends.

Outcomes

Our primary outcome of interest was the composite outcome of death or all‐cause nonelective readmission within 30 days of discharge (ie, not including in‐hospital events prior to discharge or elective readmissions after discharge for planned procedures such as chemotherapy); hereafter we refer to this as death or readmission. This is a patient‐relevant outcome that is highlighted in the Affordable Care Act and for which there are several validated risk adjustment models.[15] We chose a composite outcome to deal with the issue of competing risks; if weekend discharges were more likely to die then we could observe a spurious association between weekend discharge and reduced readmissions if we focused on only that outcome.

Other Measures

Comorbidities for each patient were identified using International Classification of Diseases, Ninth Revision and Tenth Revision codes from the Discharge Abstract Database for the index hospitalization and any hospitalizations in the 12 months prior to their index admission, a method previously validated in Alberta databases.[13] We also recorded health resource use during their index hospitalization and calculated each patient's LACE score at the time of discharge, which is an index for predicting unplanned readmission or early death postdischarge previously validated in Canadian administrative databases.[15] The LACE index includes length of hospital stay (L), acuity of admission (A, based on the admission category variable described earlier), comorbidity burden quantified using the Charlson Comorbidity Index (C), and emergency department visits in the 6 months prior to admission (E); patients with discharge LACE scores >10 (total possible score is 19) are defined as being at high risk of death/readmission within 30 days.[16] As detailed below, to deal with potential concerns that LOS may be a mediator in the causal pathway, we ran 2 sensitivity analyses, 1 in which we excluded LOS from the analyses and 1 in which we included expected LOS rather than the actual LOS. Expected LOS is a data‐driven estimate based on the most current 2 years of patient LOS information available in the Canadian Institute for Health Information discharge abstract database (www.cihi.ca) for all acute care hospitals in Canada, and was generated for each patient independently of our study taking into account case mix group, age, and inpatient resource intensity weights.

Statistical Analysis

Baseline patient characteristics between weekend and weekday discharges were compared with t tests for continuous variables and [2] tests for binary or categorical variables. Logistic regression was used for comparison of death or readmission for weekend versus weekday discharges. Multivariable models were adjusted for age, sex, hospital, and LACE scores (as a continuous variable) at time of discharge; in sensitivity analyses we adjusted for (1) LACE score without including LOS and (2) LACE score using expected LOS rather than actual LOS. In further sensitivity analyses we (1) restricted the analysis to only those patients deemed to be at high risk for events due to LACE scores of 10 or greater and (2) included ED visits as part of the composite endpoint (ie, death, unplanned readmission, or unplanned ED visit within 30 days of discharge). Day of admission (weekend vs weekday) was also considered for the multivariable models, but was not found to be significant and thus was omitted from final models. We do not have any physician identifying variables in our dataset and thus could not investigate the potential correlation among patients discharged by the same physician. We did explore the hospital intraclass correlation coefficient, and as it was very small (0.001), we did not utilize models to account for the hierarchical nature of the data, but did include hospital as a fixed effect in the logistic models. The results were virtually identical whether we did or did not include hospital in the models. Adjusted odds ratios (aORs) are displayed with 95% confidence intervals (CI) and P values. Average LOS was calculated for weekend and weekday discharges with 95% CIs. P values for adjusted length of stay were calculated using multivariable linear regression adjusting for age, sex, day of admission, and Charlson score. All statistical analyses were done using SAS for Windows version 9.4 (SAS Institute, Inc., Cary, NC).

RESULTS

Patient Characteristics

Of the 7991 patients discharged during our study interval, 1146 (14.3%) were discharged on weekend or holiday days (Table 1). In contrast, 2180 of our cohort were admitted on a weekend (27.3%). The mean age of our study population was 62.1 years, 51.9% were men, mean Charlson score was 2.56, and 4591 (57.5%) had LACE scores of at least 10 at discharge.

Table 1.Characteristics of General Internal Medicine Patients Discharged From Seven Teaching Hospitals
Characteristic	Weekend Discharge	Weekday Discharge	P Value
NOTE: Abbreviations: COPD, chronic obstructive pulmonary disease; HIV, human immunodeficiency virus; LACE, length of hospital stay, acuity of admission, comorbidity burden quantified using the Charlson Comorbidity Index, and emergency department visits in the 6 months prior to admission; LOS, length of stay; SD, standard deviation. Numbers are n (%) unless specified otherwise.
No. of patients	1,146	6,845
Age, y, mean (SD)	57.97 (19.70)	62.77 (19.37)	<0.0001
Male	601 (52.4)	3,548 (51.8)	0.70
Top 5 most responsible diagnoses
COPD	74 (6.5)	507 (7.4)
Pneumonia	64 (5.6)	326 (4.8)
Heart failure	31 (2.7)	375 (5.5)
Urinary tract infection	39 (3.4)	254 (3.7)
Venous thromboembolism	31 (2.7)	259 (3.8)
Charlson score, mean (SD)	2.17 (3.29)	2.63 (3.30)	<0.0001
Comorbidities (based on index hospitalization and prior 12 months)
Hypertension	485 (42.3)	3,265 (47.7)	0.00
Diabetes mellitus	326 (28.4)	2,106 (30.8)	0.11
Fluid imbalance	332 (29.0)	1,969 (28.8)	0.89
COPD	255 (22.3)	1,790 (26.2)	0.01
Psychiatric disorder	179 (15.6)	1,459 (21.3)	<0.0001
Pneumonia	242 (21.1)	1,427 (20.8)	0.84
Anemia	167 (14.6)	1,233 (18.0)	0.00
Trauma	169 (14.7)	1,209 (17.7)	0.02
Atrial fibrillation	141 (12.3)	1,069 (15.6)	0.00
Heart failure	101 (8.8)	946 (13.8)	<0.0001
Drug abuse	188 (16.4)	966 (14.1)	0.04
Cancer	124 (10.8)	867 (12.7)	0.08
Renal disease	93 (8.1)	689 (10.1)	0.04
Dementia	49 (4.3)	564 (8.2)	<0.0001
Mild liver disease	99 (8.6)	587 (8.6)	0.94
Cerebrovascular disease	59 (5.1)	492 (7.2)	0.01
Gastrointestinal bleed	84 (7.3)	496 (7.2)	0.92
Asthma	83 (7.2)	426 (6.2)	0.19
Stroke	42 (3.7)	332 (4.9)	0.08
Prior myocardial infarction	47 (4.1)	329 (4.8)	0.30
Arthritis	42 (3.7)	309 (4.5)	0.19
Peripheral vascular disease	42 (3.7)	259 (3.8)	0.84
Severe liver disease	44 (3.8)	261 (3.8)	0.97
Valve disease	24 (2.1)	188 (2.7)	0.20
Paralysis	31 (2.7)	201 (2.9)	0.67
Skin ulcer	17 (1.5)	137 (2.0)	0.24
Shock	19 (1.7)	99 (1.4)	0.58
HIV	15 (1.3)	109 (1.6)	0.47
Protein calorie malnutrition	0 (0.0)	9 (0.1)	0.21
Features of index hospitalization
Resource intensity weight, mean (SD)	1.10 (0.82)	1.38 (1.24)	<0.0001
LACE score, mean (SD)	9.45 (2.85)	10.51 (3.03)	<0.0001
Expected LOS, mean (SD)	6.20 (4.08)	7.12 (4.89)	<0.0001
Acute LOS, mean (SD)	5.64 (4.99)	7.86 (6.13)	<0.0001
Weekend admission	244 (21.3)	1,936 (28.3)	<0.0001
Discharge disposition			<0.0001
Transferred to another inpatient hospital	14 (1.2)	189 (2.8)
Transferred to long‐term care facility	36 (3.1)	532 (7.8)
Transferred to other (except hospice)	5 (0.4)	24 (0.4)
Discharged to home setting with support services	125 (10.9)	1,318 (19.3)
Discharged home	926 (80.8)	4,646 (67.9)
Left against medical advice	40 (3.5)	136 (2.0)

Weekday Versus Weekend Discharge

Although patients admitted on weekdays and weekends were very similar (data available upon request), patients discharged on weekends (compared to those discharged on weekdays) were younger, more likely to be discharged home without additional support, and had fewer comorbidities (Table 1, Figure 1). Patients discharged on weekends had shorter lengths of stay than those discharged on weekdays (5.6 days vs 7.9 days, P<0.0001). In adjusted linear regression analyses, this 2.3‐day difference remained statistically significant (adjusted P value <0.0001).

Factors associated with day of discharge that potentially influence 30‐day outcomes.

Patients discharged on a weekend exhibited lower unadjusted 30‐day rates of death or readmission than those discharged on a weekday (10.6% vs 13.2%), but these differences disappeared after multivariable adjustment that accounted for differences in risk profile (aOR: 0.94, 95% CI: 0.771.16 (Table 2). Results were similar in sensitivity analyses adjusting for LACE scores without LOS included (aOR: 0.88, 95% CI: 0.711.08) or adjusting for LACE scores using expected LOS rather than actual LOS (aOR: 0.90, 95% CI: 0.731.10). Restricting the analysis to only those patients deemed to be at high risk for events due to LACE scores of 10 or greater confirmed that weekend and weekday discharges had similar outcomes in the first 30 days after discharge (aOR: 1.09, 95% CI: 0.851.41, Table 2). Similar patterns were seen when we included ED visits as part of the composite endpoint (ie, death, unplanned readmission, or unplanned ED visit within 30 days of discharge) (Table 2).

Table 2.Postdischarge Outcomes After a General Internal Medicine Hospitalization in a Teaching Hospital
	Weekend Discharge, n/N (%)	Weekday Discharge, n/N (%)	Unadjusted P Value	aOR* (95% CI)	Adjusted P Value
NOTE: Abbreviations: aOR, adjusted odds ratio; CI, confidence interval; ED, emergency department; LACE, length of hospital stay, acuity of admission, comorbidity burden quantified using the Charlson Comorbidity Index, and emergency department visits in the 6 months prior to admission. *Multivariable models adjust for age, sex, hospital, and LACE score at time of discharge from index hospitalization. Weekday discharge is reference group for odds ratios.
Death/readmission within 30 days
All 7 teaching hospitals, all patients	121/1146 (10.6)	901/6845 (13.2)	0.01	0.94 (0.77‐1.16)	0.58
All 7 teaching hospitals, but only patients with LACE <10	37/647 (5.7)	225/2753 (8.2)	0.04	0.72 (0.50, 1.03)	0.07
All 7 teaching hospitals, but only patients with LACE 10	84/499 (16.8)	676/4092 (16.5)	0.86	1.09 (0.85‐1.41)	0.49
Death/readmission/ED visit within 30 days
All 7 teaching hospitals, all patients	218/1146 (19.0)	1445/6845 (21.1)	0.11	0.98 (0.83‐1.15)	0.79
All 7 teaching hospitals, but only patients with LACE <10	90/647 (13.9)	460/2753 (16.7)	0.08	0.83 (0.64‐1.06)	0.13
All 7 teaching hospitals, but only patients with LACE 10	128/499 (25.7)	985/4092 (24.1)	0.44	1.12 (0.90‐1.39)	0.31
Death within 30 days
All 7 teaching hospitals, all patients	24/1146 (2.1)	215/6845 (3.1)	0.05	0.97 (0.63‐1.51)	0.89
All 7 teaching hospitals, but only patients with LACE <10	4/647 (0.6)	23/2753 (0.8)	0.58	0.89 (0.30, 2.62)	0.83
All 7 teaching hospitals, but only patients with LACE 10	20/499 (4.0)	192/4092 (4.7)	0.49	0.99 (0.61‐1.61)	0.98
Readmission within 30 days
All 7 teaching hospitals, all patients	105/1146 (9.2)	751/6845 (11.0)	0.07	0.94 (0.76‐1.17)	0.59
All 7 teaching hospitals, but only patients with LACE <10	33/647 (5.1)	211/2753 (7.7)	0.02	0.68 (0.46‐0.99)	0.04
All 7 teaching hospitals, but only patients with LACE 10	72/499 (14.4)	540/4092 (13.2)	0.44	1.14 (0.87‐1.49)	0.34
ED visit within 30 days
All 7 teaching hospitals, all patients	182/1146 (15.9)	1118/6845 (16.3)	0.70	1.00 (0.84‐1.19)	0.99
All 7 teaching hospitals, but only patients with LACE <10	83/647 (12.8)	412/2753 (15.0)	0.17	0.84 (0.65, 1.09)	0.20
All 7 teaching hospitals, but only patients with LACE 10	99/499 (19.8)	706/4092 (17.3)	0.15	1.17 (0.92‐1.48)	0.20

DISCUSSION

Our data suggest that patients discharged from the GIM teaching wards we studied on weekends were appropriately triaged, as they did not exhibit a higher risk of adverse events postdischarge. Although patients discharged on weekends tended to be younger and had less comorbidities than those discharged during the week, we adjusted for baseline covariates in analyses, and we did not find an association between weekend discharge and increased postdischarge events even among the subset of patients deemed to be at high risk for postdischarge adverse events (based on high LACE scores). To our knowledge, although we previously examined this issue in patients with a most‐responsible diagnosis of heart failure,[10] examining weekend versus weekday discharges in the full gamut of general medical patients admitted to teaching hospitals has not previously been examined.

In our previous study[10] of over 24,000 heart failure patients discharged over 10 years (up to June 2009, therefore no overlap with any patients in this study), we also found that patients discharged on the weekends were younger, had fewer comorbidities, and shorter lengths of stay. Although postdischarge death/readmission rates were higher for weekend discharged patients in our earlier study (21.1% vs 19.5%, adjusted hazard ratio: 1.15, 95% CI: 1.061.25), it is worth noting that this was almost entirely driven by data from nonteaching hospitals and cardiology wards. Thus, it is important to reiterate that the findings in our current study are for GIM wards in teaching hospitals and may not be generalizable to less‐structured nonteaching settings.

Although we did not study physician decision making, our results suggest that physicians are incorporating discharge day into their discharge decision making. They may be selecting younger patients with less comorbidities for weekend discharges, or they may be delaying the discharges of older patients with more comorbidities for weekday discharges. Either is not surprising given the realities of weekend inpatient care: reduced staffing and frequent cross‐coverage (of physicians, nurses, physiotherapists, pharmacists, and occupational therapists), limited support services (such as laboratory services or diagnostic imaging), and decreased availability of community services (including home care and social support services).[17] For example, in 1 large US heart failure registry, patients discharged on a weekend received less complete discharge instructions than those discharged on weekdays.[11] Given that early follow‐up postdischarge is associated with better outcomes,[18, 19] future studies should also explore whether patterns of patient follow‐up differ after weekend versus weekday discharges.

Although we were able to capture all interactions with the healthcare system in a single payer system with universal access, there are some limitations to our study. First, we used administrative data, which preclude fully adjusting for severity of diagnoses or functional status, although we used proxies such as admission from/discharge to a long‐term care facility.[20, 21] Second, we did not have access to process of care measures such as diagnostic testing or prescribing data, and thus cannot determine whether quality of care or patient adherence differed by the day of the week they were discharged on, although this seems unlikely. Third, although postdischarge follow‐up may be associated with better outcomes,[18, 19] we were unable to adjust for patterns of outpatient follow‐up in this study. Fourth, we acknowledge that death or readmission soon after discharge does not necessarily mean that the quality of care during the preceding hospitalization was suboptimal or that these deaths or readmissions were even potentially preventable. Many factors influence postdischarge mortality and/or readmission, and quality of inpatient care is only one.[22, 23, 24, 25] Fifth, although some may express concern that LOS may be a mediator in the causal pathway between discharge decision and postdischarge events, and that adjusting for LOS in analyses could thus spuriously obscure a true association, it is worth pointing out that our 2 sensitivity analyses to explore this (the 1 in which we excluded LOS from the analyses and the 1 in which we included expected LOS rather than the actual LOS) revealed nearly identical point estimates and 95% CI as our main analysis. Finally, as our study is observational, we cannot definitively conclude causality, nor can we exclude an 18% excess risk for patients discharged on weekends (or a 22% lower risk either), given our 95% CI for postdischarge adverse outcomes.

CONCLUSION

We found that the proportion of patients discharged on weekends is lower than the proportion admitted on weekends. We also found that lower risk/less severely ill patients appear to be preferentially discharged on weekends, and as a result, postdischarge outcomes are similar between weekend and weekday discharges despite shorter LOS and less availability of outpatient resources for patients discharged on a weekend. The reasons why more complicated patients are not discharged on weekends deserves further study, as safely increasing weekend discharge rates would improve efficiency and safety (by reducing unnecessary exposure to in‐hospital adverse events such as falls, unnecessary urinary catheterizations, and healthcare‐acquired infections). Although hospital admission has become a 24/7 business, we believe that hospital discharge processes should strive for the same level of efficiency.

ACKNOWLEDGMENTS

Disclosures: This study is based in part on data provided by Alberta Health. The interpretation and conclusions contained herein are those of the researchers and do not necessarily represent the views of the government of Alberta. Neither the government of Alberta nor Alberta Health express any opinion in relation to this study. F.A.M. and S.R.M. are supported by salary awards from Alberta Innovates‐Health Solutions (AIHS). F.A.M. holds the Capital Health Chair in Cardiology Outcomes Research. S.R.M. holds the Endowed Chair in Patient Health Management. This project was funded by AIHS through an investigator‐initiated peer reviewed operating grant. The funding agencies did not have input into study design, data collection, interpretation of results, or write up/approval for submission. The authors report no conflicts of interest.

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References

Bell CM, Redelmeier DA. Mortality among patients admitted to hospitals on weekends as compared with weekdays. N Engl J Med. 2001;345:663–668.
Magid DJ, Wang Y, Herrin J, et al. Relationship between time of day, day of week, timeliness of reperfusion, and in‐hospital mortality for patients with acute ST‐segment elevation myocardial infarction. JAMA. 2005;294:803–812.
Bell CM, Redelmeier DA. Waiting for urgent procedures on the weekend among emergently hospitalized patients. Am J Med. 2004;117:175–181.
Becker DJ. Do hospitals provide lower quality care on weekends? Health Serv Res. 2007;42:1589–1612.
Fonarow GC, Abraham WT, Albert NM, et al. Day of admission and clinical outcomes for patients hospitalized for heart failure: findings from the organized program to initiate lifesaving treatment in hospitalized patients with heart failure (OPTIMIZE‐HF). Circ Heart Fail. 2008;1:50–57.
Freemantle N, Richardson M, Wood J, et al. Weekend hospitalization and additional risk of death: an analysis of inpatient data. J R Soc Med. 2012;105:74–84.
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Hernandez AF, Greiner MA, Fonarow GC, et al. Relationship between early physician follow‐up and 30‐day readmission among Medicare beneficiaries hospitalized for heart failure. JAMA. 2010;303:1716–1722.
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Journal of Hospital Medicine - 10(2)

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Erik Youngson, MMath

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METHODS

Study Setting

Data Sources

Study Cohort

Explanatory Variable of Interest

Outcomes

Other Measures

Statistical Analysis

RESULTS

Patient Characteristics

Table 1.Characteristics of General Internal Medicine Patients Discharged From Seven Teaching Hospitals
Characteristic	Weekend Discharge	Weekday Discharge	P Value
NOTE: Abbreviations: COPD, chronic obstructive pulmonary disease; HIV, human immunodeficiency virus; LACE, length of hospital stay, acuity of admission, comorbidity burden quantified using the Charlson Comorbidity Index, and emergency department visits in the 6 months prior to admission; LOS, length of stay; SD, standard deviation. Numbers are n (%) unless specified otherwise.
No. of patients	1,146	6,845
Age, y, mean (SD)	57.97 (19.70)	62.77 (19.37)	<0.0001
Male	601 (52.4)	3,548 (51.8)	0.70
Top 5 most responsible diagnoses
COPD	74 (6.5)	507 (7.4)
Pneumonia	64 (5.6)	326 (4.8)
Heart failure	31 (2.7)	375 (5.5)
Urinary tract infection	39 (3.4)	254 (3.7)
Venous thromboembolism	31 (2.7)	259 (3.8)
Charlson score, mean (SD)	2.17 (3.29)	2.63 (3.30)	<0.0001
Comorbidities (based on index hospitalization and prior 12 months)
Hypertension	485 (42.3)	3,265 (47.7)	0.00
Diabetes mellitus	326 (28.4)	2,106 (30.8)	0.11
Fluid imbalance	332 (29.0)	1,969 (28.8)	0.89
COPD	255 (22.3)	1,790 (26.2)	0.01
Psychiatric disorder	179 (15.6)	1,459 (21.3)	<0.0001
Pneumonia	242 (21.1)	1,427 (20.8)	0.84
Anemia	167 (14.6)	1,233 (18.0)	0.00
Trauma	169 (14.7)	1,209 (17.7)	0.02
Atrial fibrillation	141 (12.3)	1,069 (15.6)	0.00
Heart failure	101 (8.8)	946 (13.8)	<0.0001
Drug abuse	188 (16.4)	966 (14.1)	0.04
Cancer	124 (10.8)	867 (12.7)	0.08
Renal disease	93 (8.1)	689 (10.1)	0.04
Dementia	49 (4.3)	564 (8.2)	<0.0001
Mild liver disease	99 (8.6)	587 (8.6)	0.94
Cerebrovascular disease	59 (5.1)	492 (7.2)	0.01
Gastrointestinal bleed	84 (7.3)	496 (7.2)	0.92
Asthma	83 (7.2)	426 (6.2)	0.19
Stroke	42 (3.7)	332 (4.9)	0.08
Prior myocardial infarction	47 (4.1)	329 (4.8)	0.30
Arthritis	42 (3.7)	309 (4.5)	0.19
Peripheral vascular disease	42 (3.7)	259 (3.8)	0.84
Severe liver disease	44 (3.8)	261 (3.8)	0.97
Valve disease	24 (2.1)	188 (2.7)	0.20
Paralysis	31 (2.7)	201 (2.9)	0.67
Skin ulcer	17 (1.5)	137 (2.0)	0.24
Shock	19 (1.7)	99 (1.4)	0.58
HIV	15 (1.3)	109 (1.6)	0.47
Protein calorie malnutrition	0 (0.0)	9 (0.1)	0.21
Features of index hospitalization
Resource intensity weight, mean (SD)	1.10 (0.82)	1.38 (1.24)	<0.0001
LACE score, mean (SD)	9.45 (2.85)	10.51 (3.03)	<0.0001
Expected LOS, mean (SD)	6.20 (4.08)	7.12 (4.89)	<0.0001
Acute LOS, mean (SD)	5.64 (4.99)	7.86 (6.13)	<0.0001
Weekend admission	244 (21.3)	1,936 (28.3)	<0.0001
Discharge disposition			<0.0001
Transferred to another inpatient hospital	14 (1.2)	189 (2.8)
Transferred to long‐term care facility	36 (3.1)	532 (7.8)
Transferred to other (except hospice)	5 (0.4)	24 (0.4)
Discharged to home setting with support services	125 (10.9)	1,318 (19.3)
Discharged home	926 (80.8)	4,646 (67.9)
Left against medical advice	40 (3.5)	136 (2.0)

Weekday Versus Weekend Discharge

Table 2.Postdischarge Outcomes After a General Internal Medicine Hospitalization in a Teaching Hospital
	Weekend Discharge, n/N (%)	Weekday Discharge, n/N (%)	Unadjusted P Value	aOR* (95% CI)	Adjusted P Value
NOTE: Abbreviations: aOR, adjusted odds ratio; CI, confidence interval; ED, emergency department; LACE, length of hospital stay, acuity of admission, comorbidity burden quantified using the Charlson Comorbidity Index, and emergency department visits in the 6 months prior to admission. *Multivariable models adjust for age, sex, hospital, and LACE score at time of discharge from index hospitalization. Weekday discharge is reference group for odds ratios.
Death/readmission within 30 days
All 7 teaching hospitals, all patients	121/1146 (10.6)	901/6845 (13.2)	0.01	0.94 (0.77‐1.16)	0.58
All 7 teaching hospitals, but only patients with LACE <10	37/647 (5.7)	225/2753 (8.2)	0.04	0.72 (0.50, 1.03)	0.07
All 7 teaching hospitals, but only patients with LACE 10	84/499 (16.8)	676/4092 (16.5)	0.86	1.09 (0.85‐1.41)	0.49
Death/readmission/ED visit within 30 days
All 7 teaching hospitals, all patients	218/1146 (19.0)	1445/6845 (21.1)	0.11	0.98 (0.83‐1.15)	0.79
All 7 teaching hospitals, but only patients with LACE <10	90/647 (13.9)	460/2753 (16.7)	0.08	0.83 (0.64‐1.06)	0.13
All 7 teaching hospitals, but only patients with LACE 10	128/499 (25.7)	985/4092 (24.1)	0.44	1.12 (0.90‐1.39)	0.31
Death within 30 days
All 7 teaching hospitals, all patients	24/1146 (2.1)	215/6845 (3.1)	0.05	0.97 (0.63‐1.51)	0.89
All 7 teaching hospitals, but only patients with LACE <10	4/647 (0.6)	23/2753 (0.8)	0.58	0.89 (0.30, 2.62)	0.83
All 7 teaching hospitals, but only patients with LACE 10	20/499 (4.0)	192/4092 (4.7)	0.49	0.99 (0.61‐1.61)	0.98
Readmission within 30 days
All 7 teaching hospitals, all patients	105/1146 (9.2)	751/6845 (11.0)	0.07	0.94 (0.76‐1.17)	0.59
All 7 teaching hospitals, but only patients with LACE <10	33/647 (5.1)	211/2753 (7.7)	0.02	0.68 (0.46‐0.99)	0.04
All 7 teaching hospitals, but only patients with LACE 10	72/499 (14.4)	540/4092 (13.2)	0.44	1.14 (0.87‐1.49)	0.34
ED visit within 30 days
All 7 teaching hospitals, all patients	182/1146 (15.9)	1118/6845 (16.3)	0.70	1.00 (0.84‐1.19)	0.99
All 7 teaching hospitals, but only patients with LACE <10	83/647 (12.8)	412/2753 (15.0)	0.17	0.84 (0.65, 1.09)	0.20
All 7 teaching hospitals, but only patients with LACE 10	99/499 (19.8)	706/4092 (17.3)	0.15	1.17 (0.92‐1.48)	0.20

DISCUSSION

CONCLUSION

ACKNOWLEDGMENTS

METHODS

Study Setting

Data Sources

Study Cohort

Explanatory Variable of Interest

Outcomes

Other Measures

Statistical Analysis

RESULTS

Patient Characteristics

Table 1.Characteristics of General Internal Medicine Patients Discharged From Seven Teaching Hospitals
Characteristic	Weekend Discharge	Weekday Discharge	P Value
NOTE: Abbreviations: COPD, chronic obstructive pulmonary disease; HIV, human immunodeficiency virus; LACE, length of hospital stay, acuity of admission, comorbidity burden quantified using the Charlson Comorbidity Index, and emergency department visits in the 6 months prior to admission; LOS, length of stay; SD, standard deviation. Numbers are n (%) unless specified otherwise.
No. of patients	1,146	6,845
Age, y, mean (SD)	57.97 (19.70)	62.77 (19.37)	<0.0001
Male	601 (52.4)	3,548 (51.8)	0.70
Top 5 most responsible diagnoses
COPD	74 (6.5)	507 (7.4)
Pneumonia	64 (5.6)	326 (4.8)
Heart failure	31 (2.7)	375 (5.5)
Urinary tract infection	39 (3.4)	254 (3.7)
Venous thromboembolism	31 (2.7)	259 (3.8)
Charlson score, mean (SD)	2.17 (3.29)	2.63 (3.30)	<0.0001
Comorbidities (based on index hospitalization and prior 12 months)
Hypertension	485 (42.3)	3,265 (47.7)	0.00
Diabetes mellitus	326 (28.4)	2,106 (30.8)	0.11
Fluid imbalance	332 (29.0)	1,969 (28.8)	0.89
COPD	255 (22.3)	1,790 (26.2)	0.01
Psychiatric disorder	179 (15.6)	1,459 (21.3)	<0.0001
Pneumonia	242 (21.1)	1,427 (20.8)	0.84
Anemia	167 (14.6)	1,233 (18.0)	0.00
Trauma	169 (14.7)	1,209 (17.7)	0.02
Atrial fibrillation	141 (12.3)	1,069 (15.6)	0.00
Heart failure	101 (8.8)	946 (13.8)	<0.0001
Drug abuse	188 (16.4)	966 (14.1)	0.04
Cancer	124 (10.8)	867 (12.7)	0.08
Renal disease	93 (8.1)	689 (10.1)	0.04
Dementia	49 (4.3)	564 (8.2)	<0.0001
Mild liver disease	99 (8.6)	587 (8.6)	0.94
Cerebrovascular disease	59 (5.1)	492 (7.2)	0.01
Gastrointestinal bleed	84 (7.3)	496 (7.2)	0.92
Asthma	83 (7.2)	426 (6.2)	0.19
Stroke	42 (3.7)	332 (4.9)	0.08
Prior myocardial infarction	47 (4.1)	329 (4.8)	0.30
Arthritis	42 (3.7)	309 (4.5)	0.19
Peripheral vascular disease	42 (3.7)	259 (3.8)	0.84
Severe liver disease	44 (3.8)	261 (3.8)	0.97
Valve disease	24 (2.1)	188 (2.7)	0.20
Paralysis	31 (2.7)	201 (2.9)	0.67
Skin ulcer	17 (1.5)	137 (2.0)	0.24
Shock	19 (1.7)	99 (1.4)	0.58
HIV	15 (1.3)	109 (1.6)	0.47
Protein calorie malnutrition	0 (0.0)	9 (0.1)	0.21
Features of index hospitalization
Resource intensity weight, mean (SD)	1.10 (0.82)	1.38 (1.24)	<0.0001
LACE score, mean (SD)	9.45 (2.85)	10.51 (3.03)	<0.0001
Expected LOS, mean (SD)	6.20 (4.08)	7.12 (4.89)	<0.0001
Acute LOS, mean (SD)	5.64 (4.99)	7.86 (6.13)	<0.0001
Weekend admission	244 (21.3)	1,936 (28.3)	<0.0001
Discharge disposition			<0.0001
Transferred to another inpatient hospital	14 (1.2)	189 (2.8)
Transferred to long‐term care facility	36 (3.1)	532 (7.8)
Transferred to other (except hospice)	5 (0.4)	24 (0.4)
Discharged to home setting with support services	125 (10.9)	1,318 (19.3)
Discharged home	926 (80.8)	4,646 (67.9)
Left against medical advice	40 (3.5)	136 (2.0)

Weekday Versus Weekend Discharge

Table 2.Postdischarge Outcomes After a General Internal Medicine Hospitalization in a Teaching Hospital
	Weekend Discharge, n/N (%)	Weekday Discharge, n/N (%)	Unadjusted P Value	aOR* (95% CI)	Adjusted P Value
NOTE: Abbreviations: aOR, adjusted odds ratio; CI, confidence interval; ED, emergency department; LACE, length of hospital stay, acuity of admission, comorbidity burden quantified using the Charlson Comorbidity Index, and emergency department visits in the 6 months prior to admission. *Multivariable models adjust for age, sex, hospital, and LACE score at time of discharge from index hospitalization. Weekday discharge is reference group for odds ratios.
Death/readmission within 30 days
All 7 teaching hospitals, all patients	121/1146 (10.6)	901/6845 (13.2)	0.01	0.94 (0.77‐1.16)	0.58
All 7 teaching hospitals, but only patients with LACE <10	37/647 (5.7)	225/2753 (8.2)	0.04	0.72 (0.50, 1.03)	0.07
All 7 teaching hospitals, but only patients with LACE 10	84/499 (16.8)	676/4092 (16.5)	0.86	1.09 (0.85‐1.41)	0.49
Death/readmission/ED visit within 30 days
All 7 teaching hospitals, all patients	218/1146 (19.0)	1445/6845 (21.1)	0.11	0.98 (0.83‐1.15)	0.79
All 7 teaching hospitals, but only patients with LACE <10	90/647 (13.9)	460/2753 (16.7)	0.08	0.83 (0.64‐1.06)	0.13
All 7 teaching hospitals, but only patients with LACE 10	128/499 (25.7)	985/4092 (24.1)	0.44	1.12 (0.90‐1.39)	0.31
Death within 30 days
All 7 teaching hospitals, all patients	24/1146 (2.1)	215/6845 (3.1)	0.05	0.97 (0.63‐1.51)	0.89
All 7 teaching hospitals, but only patients with LACE <10	4/647 (0.6)	23/2753 (0.8)	0.58	0.89 (0.30, 2.62)	0.83
All 7 teaching hospitals, but only patients with LACE 10	20/499 (4.0)	192/4092 (4.7)	0.49	0.99 (0.61‐1.61)	0.98
Readmission within 30 days
All 7 teaching hospitals, all patients	105/1146 (9.2)	751/6845 (11.0)	0.07	0.94 (0.76‐1.17)	0.59
All 7 teaching hospitals, but only patients with LACE <10	33/647 (5.1)	211/2753 (7.7)	0.02	0.68 (0.46‐0.99)	0.04
All 7 teaching hospitals, but only patients with LACE 10	72/499 (14.4)	540/4092 (13.2)	0.44	1.14 (0.87‐1.49)	0.34
ED visit within 30 days
All 7 teaching hospitals, all patients	182/1146 (15.9)	1118/6845 (16.3)	0.70	1.00 (0.84‐1.19)	0.99
All 7 teaching hospitals, but only patients with LACE <10	83/647 (12.8)	412/2753 (15.0)	0.17	0.84 (0.65, 1.09)	0.20
All 7 teaching hospitals, but only patients with LACE 10	99/499 (19.8)	706/4092 (17.3)	0.15	1.17 (0.92‐1.48)	0.20

DISCUSSION

CONCLUSION

ACKNOWLEDGMENTS

References

Bell CM, Redelmeier DA. Mortality among patients admitted to hospitals on weekends as compared with weekdays. N Engl J Med. 2001;345:663–668.
Magid DJ, Wang Y, Herrin J, et al. Relationship between time of day, day of week, timeliness of reperfusion, and in‐hospital mortality for patients with acute ST‐segment elevation myocardial infarction. JAMA. 2005;294:803–812.
Bell CM, Redelmeier DA. Waiting for urgent procedures on the weekend among emergently hospitalized patients. Am J Med. 2004;117:175–181.
Becker DJ. Do hospitals provide lower quality care on weekends? Health Serv Res. 2007;42:1589–1612.
Fonarow GC, Abraham WT, Albert NM, et al. Day of admission and clinical outcomes for patients hospitalized for heart failure: findings from the organized program to initiate lifesaving treatment in hospitalized patients with heart failure (OPTIMIZE‐HF). Circ Heart Fail. 2008;1:50–57.
Freemantle N, Richardson M, Wood J, et al. Weekend hospitalization and additional risk of death: an analysis of inpatient data. J R Soc Med. 2012;105:74–84.
Saposnik G, Baibergenova A, Bayer N, Hachinski V. Weekends: a dangerous time for having a stroke? Stroke. 2007;38:1211–1215.
Barnett MJ, Kaboli PJ, Sirio CA, Rosenthal GE. Day of the week of intensive care admission and patient outcomes: a multisite regional evaluation. Med Care. 2002;40:530–539.
Cram P, Hillis SL, Barnett M, Rosenthal GE. Effects of weekend admission and hospital teaching status on in‐hospital mortality. Am J Med. 2004;117:151–157.
McAlister FA, Au A, Majumdar SR, Youngson E, Padwal RS. Postdischarge outcomes in heart failure are better for teaching hospitals and weekday discharges. Circ Heart Fail. 2013;6:922–929.
Horwich TB, Hernandez AF, Liang L, et al. Weekend hospital admission and discharge for heart failure: association with quality of care and clinical outcomes. Am Heart J. 2009;158:451–458.
Walraven C, Bell CM. Risk of death or readmission among people discharged from hospital on Fridays. CMAJ. 2002;166:1672–1673.
Quan H, Li B, Saunders LD, Parsons GA, et al.; IMECCHI Investigators. Assessing validity of ICD‐9‐CM and ICD‐10 administrative data in recording clinical conditions in a unique dually coded database. Health Serv Res. 2008;43:1424–1441.
McAlister FA, Bakal J, Majumdar SR, et al. Safely and effectively reducing inpatient length of stay: a controlled study of the General Internal Medicine Care Transformation Initiative. BMJ Qual Saf. 2014;23:446–456.
Walraven C, Dhalla IA, Bell C, et al. Derivation and validation of an index to predict early death or unplanned readmission after discharge from hospital to the community. CMAJ. 2010;182:551–557.
Gruneir A, Dhalla IA, Walraven C, et al. Unplanned readmissions after hospital discharge among patients identified as being at high risk for readmission using a validated predictive algorithm. Open Med. 2011;5(2):e104–e111.
Wong HJ, Morra D. Excellent hospital care for all: open and operating 24/7. J Gen Intern Med. 2011;26:1050–1052.
Hernandez AF, Greiner MA, Fonarow GC, et al. Relationship between early physician follow‐up and 30‐day readmission among Medicare beneficiaries hospitalized for heart failure. JAMA. 2010;303:1716–1722.
McAlister FA, Youngson E, Bakal JA, Kaul P, Ezekowitz J, Walraven C. Impact of physician continuity on death or urgent readmission after discharge among patients with heart failure. CMAJ. 2013;185:e681–e689.
Jollis JG, Ancukiewicz M, DeLong ER, Pryor DB, Muhlbaier LH, Mark DB. Discordance of databases designed for claims payment versus clinical information systems. Implications for outcomes research. Ann Intern Med. 1993;119:844–850.
Pine M, Norusis M, Jones B, Rosenthal GE. Predictions of hospital mortality rates: a comparison of data sources. Ann Intern Med. 1997;126:347–354.
Calvillo‐King L, Arnold D, Eubank KJ, et al. Impact of social factors on risk of readmission or mortality in pneumonia and heart failure: systematic review. J Gen Intern Med. 2013;28(2):269–282.
Thomas JW, Holloway JJ. Investigating early readmission as an indicator for quality of care studies. Med Care. 1991;29(4):377–394.
Kansagara D, Englander H, Salanitro A, et al. Risk prediction models for hospital readmission: a systematic review. JAMA. 2011;306(15):1688–1698.
Walraven C, Bennett C, Jennings A, Austin PC, Forster AJ. Proportion of hospital readmissions deemed avoidable: a systematic review. CMAJ. 2011;183(7):E391–E402.

References

Bell CM, Redelmeier DA. Mortality among patients admitted to hospitals on weekends as compared with weekdays. N Engl J Med. 2001;345:663–668.
Magid DJ, Wang Y, Herrin J, et al. Relationship between time of day, day of week, timeliness of reperfusion, and in‐hospital mortality for patients with acute ST‐segment elevation myocardial infarction. JAMA. 2005;294:803–812.
Bell CM, Redelmeier DA. Waiting for urgent procedures on the weekend among emergently hospitalized patients. Am J Med. 2004;117:175–181.
Becker DJ. Do hospitals provide lower quality care on weekends? Health Serv Res. 2007;42:1589–1612.
Fonarow GC, Abraham WT, Albert NM, et al. Day of admission and clinical outcomes for patients hospitalized for heart failure: findings from the organized program to initiate lifesaving treatment in hospitalized patients with heart failure (OPTIMIZE‐HF). Circ Heart Fail. 2008;1:50–57.
Freemantle N, Richardson M, Wood J, et al. Weekend hospitalization and additional risk of death: an analysis of inpatient data. J R Soc Med. 2012;105:74–84.
Saposnik G, Baibergenova A, Bayer N, Hachinski V. Weekends: a dangerous time for having a stroke? Stroke. 2007;38:1211–1215.
Barnett MJ, Kaboli PJ, Sirio CA, Rosenthal GE. Day of the week of intensive care admission and patient outcomes: a multisite regional evaluation. Med Care. 2002;40:530–539.
Cram P, Hillis SL, Barnett M, Rosenthal GE. Effects of weekend admission and hospital teaching status on in‐hospital mortality. Am J Med. 2004;117:151–157.
McAlister FA, Au A, Majumdar SR, Youngson E, Padwal RS. Postdischarge outcomes in heart failure are better for teaching hospitals and weekday discharges. Circ Heart Fail. 2013;6:922–929.
Horwich TB, Hernandez AF, Liang L, et al. Weekend hospital admission and discharge for heart failure: association with quality of care and clinical outcomes. Am Heart J. 2009;158:451–458.
Walraven C, Bell CM. Risk of death or readmission among people discharged from hospital on Fridays. CMAJ. 2002;166:1672–1673.
Quan H, Li B, Saunders LD, Parsons GA, et al.; IMECCHI Investigators. Assessing validity of ICD‐9‐CM and ICD‐10 administrative data in recording clinical conditions in a unique dually coded database. Health Serv Res. 2008;43:1424–1441.
McAlister FA, Bakal J, Majumdar SR, et al. Safely and effectively reducing inpatient length of stay: a controlled study of the General Internal Medicine Care Transformation Initiative. BMJ Qual Saf. 2014;23:446–456.
Walraven C, Dhalla IA, Bell C, et al. Derivation and validation of an index to predict early death or unplanned readmission after discharge from hospital to the community. CMAJ. 2010;182:551–557.
Gruneir A, Dhalla IA, Walraven C, et al. Unplanned readmissions after hospital discharge among patients identified as being at high risk for readmission using a validated predictive algorithm. Open Med. 2011;5(2):e104–e111.
Wong HJ, Morra D. Excellent hospital care for all: open and operating 24/7. J Gen Intern Med. 2011;26:1050–1052.
Hernandez AF, Greiner MA, Fonarow GC, et al. Relationship between early physician follow‐up and 30‐day readmission among Medicare beneficiaries hospitalized for heart failure. JAMA. 2010;303:1716–1722.
McAlister FA, Youngson E, Bakal JA, Kaul P, Ezekowitz J, Walraven C. Impact of physician continuity on death or urgent readmission after discharge among patients with heart failure. CMAJ. 2013;185:e681–e689.
Jollis JG, Ancukiewicz M, DeLong ER, Pryor DB, Muhlbaier LH, Mark DB. Discordance of databases designed for claims payment versus clinical information systems. Implications for outcomes research. Ann Intern Med. 1993;119:844–850.
Pine M, Norusis M, Jones B, Rosenthal GE. Predictions of hospital mortality rates: a comparison of data sources. Ann Intern Med. 1997;126:347–354.
Calvillo‐King L, Arnold D, Eubank KJ, et al. Impact of social factors on risk of readmission or mortality in pneumonia and heart failure: systematic review. J Gen Intern Med. 2013;28(2):269–282.
Thomas JW, Holloway JJ. Investigating early readmission as an indicator for quality of care studies. Med Care. 1991;29(4):377–394.
Kansagara D, Englander H, Salanitro A, et al. Risk prediction models for hospital readmission: a systematic review. JAMA. 2011;306(15):1688–1698.
Walraven C, Bennett C, Jennings A, Austin PC, Forster AJ. Proportion of hospital readmissions deemed avoidable: a systematic review. CMAJ. 2011;183(7):E391–E402.

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Journal of Hospital Medicine - 10(2)

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Journal of Hospital Medicine - 10(2)

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69-74

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69-74

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Similar outcomes among general medicine patients discharged on weekends

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Similar outcomes among general medicine patients discharged on weekends

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Address for correspondence and reprint requests: Finlay A. McAlister, MD, Division of General Internal Medicine, 5–134C Clinical Sciences Building, 11350 83 Avenue, Edmonton, Alberta, Canada T6G 2G3; Telephone: 780‐492‐8115; Fax: 780‐492‐7277; E‐mail: [email protected]

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