CHEST Original Research

HEALTH-CARE-ASSOCIATED PNEUMONIA

Why Mortality Is Increased in

Health-Care-Associated Pneumonia
Lessons From Pneumococcal Bacteremic Pneumonia
Jordi Rello, MD, PhD; Manel Luján, MD; Miguel Gallego, MD; Jordi Vallés, MD, PhD;
Yolanda Belmonte, MD; Dionisia Fontanals, PhD; Emili Diaz, MD, PhD;
and Thiago Lisboa, MD, PhD; for the PROCORNEU Study Group*

Background: A cohort of patients with bacteremic Streptococcus pneumoniae pneumonia was

reviewed to assess why mortality is higher in health-care-associated pneumonia (HCAP) than in
community-acquired pneumonia (CAP).
Methods: A prospective cohort of all adult patients with bacteremic pneumococcal pneumonia
attended at the ED was used.
Results: One hundred eighty-four cases were classified as CAP and 44 (19%) as HCAP. Fifty-two
(23%) were admitted to the ICU. Three (1.5%) isolates were resistant to b-lactams, and only two
patients received inappropriate therapy. The CAP cohort was significantly younger (median age
68 years, interquartile range [IQR] 42-78 vs 77 years, IQR 67-82, P , .001). The HCAP cohort
presented a higher Charlson index (2.81 6 1.9 vs 1.23 6 1.42, P , .001) and had higher severity of
illness at admission (altered mental status, respiratory rate . 30/min, Pao2/Fio2 , 250, and multi-
lobar involvement). HCAP patients had a lower rate of ICU admission (11.3% vs 25.5%, P , .05),
and a trend toward lower mechanical ventilation (9% vs 19%, P 5 .17) and vasopressor use (9% vs
18.4%, P 5 .17) were documented. More patients in the HCAP cohort presented with a pneumo-
nia severity index score . 90 (class IV-V, 95% vs 65%, P , .001), and 30-day mortality was signifi-
cantly higher (29.5% vs 7.6%, P , .001). A multivariable regression logistic analysis adjusting for
underlying conditions and variables related to severity of illness confirmed that HCAP is an inde-
pendent variable associated with increased mortality (odds ratio 5 5.56; 95% CI, 1.86-16.5).
Conclusions: Pneumococcal HCAP presents excess mortality, which is independent of bacterial sus-
ceptibility. Differences in outcomes were probably due to differences in age, comorbidities, and
criteria for ICU admission rather than to therapeutic decisions. CHEST 2010; 137(5):1138–1144

Abbreviations: aOR 5 adjusted odds ratio; CAP 5 community-acquired pneumonia; CLSI 5 Clinical and Laboratory
Standards Institute; CURB-65 5 confusion, urea nitrogen, respiratory rate, BP, 65 years of age or older; HCAP 5 health-
care-associated pneumonia; IQR 5 interquartile range; MIC 5 minimum inhibitory concentration; OR 5 odds ratio;
PSI 5 pneumonia severity index

Health-care-associated pneumonia (HCAP) is cur-

rently considered a distinct subset of pneumonia
associated with severe disease, long hospital stay, and
high mortality rates.1,2 HCAP has not been exten-
sively studied or clarified, especially in terms of its
etiology and management. It is not clear whether the
poor outcome observed in patients with HCAP is
related to the presence of more comorbidities or to a
higher incidence of antibiotic-resistant bacteria and
inappropriate empirical antibiotic treatment.3 There-
fore, a study comparing pneumococcal HCAP and
pneumococcal community-acquired pneumonia (CAP)
may be of interest.
Moreover, patients with severe HCAP or CAP may
need intensive care or mechanical ventilation and
their condition may be complicated by shock or mul-
tiple organ failure. Unfortunately, the information
available on severe HCAP is limited. We therefore
decided to analyze the implications of HCAP in a
cohort of patients with bacteremic pneumococcal
pneumonia.
The key question that we address in this article is
whether classifying someone as HCAP adds any
information that is not captured by existing severity
indices. Prior studies4,5 clearly show that patients with
HCAP are older and have more comorbidities, and

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© 2010 American College of Chest Physicians
therefore have higher pneumonia severity index
(PSI) scores.6 However, this information is already
captured by the PSI. It would be interesting to assess
predicted and actual mortality based on the actual
PSI score. If mortality in patients with HCAP is pre-
dicted by standard CAP severity indexes, there is no
real justification for categorizing them separately.
Our objectives were to compare differences in epi-
demiology, use of vasopressors, need for mechanical
ventilation, and ICU admission. We also aimed to
establish whether differences in outcomes for HCAP
were due to differences in age, comorbidities, thera-
peutic decisions, or criteria for ICU admission.
Materials and Methods
Study Population
Patients admitted between January 1999 and June 2007 to an
800-bed teaching hospital (500 beds for acute care patients and
300 for long-term hospitalization) were prospectively identified
by one of the authors (M. L.). All patients aged ⱖ 18 years who
received a diagnosis of pneumonia (fever, productive cough, chest
pain, shortness of breath, and crackles on auscultation in addition
to a chest radiograph interpreted as pneumonia), and whose blood
cultures obtained within the first 48 h of hospitalization showed
growth of Streptococcus pneumoniae, were included. Exclusion
criteria were bacteremia from other sources, presence of concur-
rent meningitis or endocarditis at admission, and HIV infection.
Cases were retrospectively considered HCAP in accordance
with the Infectious Disease Society of America/American Tho-
racic Society guidelines,3 if one of the following criteria was met:
hospitalization in an acute-care hospital for a minimum of 2 days
within 90 days of the infection, residence in a nursing home or
long-term care facility, recent IV antibiotic therapy, chemother-
apy, wound care within the past 30 days of the current infection,
or attendance at a hospital or hemodialysis clinic. The study was
approved by the institutional review board, and informed consent
was waived.
Demographic and clinical data of the CAP and HCAP cohorts
were compared. The following variables were recorded at admis-
Manuscript received September 15, 2009; revision accepted
November 9, 2009.
Affiliations: From the Critical Care Department (Drs Rello,
Diaz, and Lisboa), Joan XXIII University Hospital, IISPV, Rovira i
Virgili University; the Pneumology Service (Drs Luján, Gallego,
and Belmonte), Critical Care Service (Dr Vallés), and UDIAT
Centre diagnòstic (Dr Fontanals), Corporació Parc Tauli, Institut
Universitari Parc Taulí, Departament de Medicina, Universitat
Autònoma de Barcelona, Sabadell, Spain.
*A complete list of participants is located in the appendix.
Funding/Support: This study was supported in part by CIBER
enfermedades respiratorias (CIBERes) 06/06/36, AGAUR 2009/
SGR/1226, FISS 08/0452, and FISS 04/1500. The Proyecto Cor-
porativo de Neumonía (PROCORNEU) Study Group is supported
by CIBERes, Instituto de Salud Carlos III.
Correspondence to: Jordi Rello, MD, PhD, Critical Care
Department, Joan XXIII University Hospital, Carrer Mallafre
Guasch, 4, Tarragona 43007, Spain; e-mail: [email protected]
© 2010 American College of Chest Physicians. Reproduction
of this article is prohibited without written permission from the
American College of Chest Physicians (www.chestpubs.org/
site/misc/reprints.xhtml).
DOI: 10.1378/chest.09-2175
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© 2010 American College of Chest Physicians
sion: age, sex, origin, alcohol abuse and tobacco consumption,
hospitalization and antibiotic therapies in last 3 months, CURB-65
(Confusion, urea nitrogen, respiratory rate, BP, 65 years of age or
older) score, underlying diseases including Charlson comorbidity
index,7 vaccination status with the 23-valent polysaccharide
vaccine (patients who received their last administration of the
vaccine in the 5 years before pneumonia were considered as vac-
cinated), symptoms in the days prior to and at admission, relevant
physical signs, blood gases, WBC and RBC counts, serum creati-
nine, and chest radiograph pattern. The PSI was calculated using
a validated prognostic scoring system,6 with PSI . 90 (class IV-V)
being considered as severe pneumonia.
During hospitalization, the following variables were also
recorded: in vitro susceptibility for strains, need for ICU admis-
sion, vasoactive drugs and mechanical ventilation, major compli-
cations, outcome (30-day mortality), length of stay for survivors,
and antibiotic therapy prescribed. Antibiotic therapy and decision
for ICU admission were not standardized and were left to the cri-
teria of the attending physician.
Microbiologic Evaluation
Blood samples were processed using the BacT-Alert system
(BioMerieux; Lyon, France). Identification was carried out by
colony morphology on blood agar, Gram stain, Optochin-disk sus-
ceptibility, and the results of a latex agglutination test.
Minimum inhibitory concentration (MIC) values were deter-
mined by the microdilution method in cation-adjusted Mueller-
Hinton broth, supplemented with 5% lysed horse blood.
Susceptibility was assessed post hoc, converting MIC values to
categories of susceptibility according to the 2008 Clinical and
Laboratory Standards Institute (CLSI) breakpoints.8 All strains
were sent to the Pneumococcus Reference Laboratory of the
Instituto de Salud Carlos III in Majadahonda for verification of
sensitivity to the antibiotics and serotyping using the Quellung
reaction and/or dot blot assay, with the use of antisera provided by
the Statens Serum Institut (Copenhagen, Denmark).
Definitions
Definitions were underlying conditions: alcohol consumption
. 60 g/d; history of lung comorbidity including COPD and inter-
stitial lung disease; cardiac comorbidity: diagnosis of congestive
heart failure, coronary artery disease, or advanced valvulopathy; renal
disease: chronic renal failure, with creatinine levels ⱖ 1.5 mg/dL;
liver disease: biopsy-proven cirrhosis or diagnosis of viral or toxic
chronic liver disease; diabetes mellitus: treatment with oral antidi-
abetics or insulin; immunocompromise: corticosteroid therapy
with 4 mg prednisolone/d or equivalent for . 1 month, or history
of cancer chemotherapy over the past 6 months. Antibiotic treat-
ment was considered concordant if the isolated strain was fully
sensitive in vitro to at least one of the antibiotics administered.9
Empyema was defined as a pleural fluid with macroscopic pus or
bacterial growth of the sample.
Statistical Analysis
Quantitative variables for age, median values, and interquartile
range (IQR) were reported and compared with the Mann-Whitney
U test. For Charlson index, mean 6 SD was given and compared
with the Student t test. For categorical variables, frequencies and
percentages were reported and compared using the x2 test and
Fisher exact test when appropriate. The risk of death was assessed
by multivariable logistic regression analysis, considering variables
with P , .1 in the univariate analysis. We restricted the number of
variables included in the multivariable model following the rule of
at least five to seven events (deaths) per variable.10 Thus, variables
CHEST / 137 / 5 / MAY, 2010 1139
showing colinearity (multilobar involvement, respiratory rate and Table 1—Demographic Data, Underlying Conditions,
Pao2/Fio2 ratio, and shock, need for vasopressors, and ICU Clinical, Radiologic, and Microbiologic Findings in
admission) were not included in the model. Similarly, comorbidi- 228 Patients With Bacteremic Community-Acquired
ties were grouped as the Charlson index. The appropriateness of Pneumonia and Health-Care-Associated Pneumonia
the model was assessed by Hosmer-Lemeshow goodness-of-fit.11
Moreover, the survival was analyzed with the Kaplan-Meier Variables Data
method, and curves for HCAP vs CAP were compared with the
Median age (IQR) 70 (49-79)
log-rank analysis. The significance level of all analyses was HCAP 44 (19)
defined as P , .05. Data were analyzed using the SPSS-15 statis- 23-Valent pneumococcal polysaccharide 21/172 (12)
tical package (SPSS, Inc.; Chicago, IL). vaccinea
Alcoholism 30 (13)
Comorbidities
Results Cardiomyopathy 52 (23)
Lung disease 63 (27)
During the study period, all consecutive patients Hepatic disease 26 (11)
Renal 22 (9)
with bacteremic pneumococcal pneumonia were Charlson index, mean 6 SD 1.54 6 1.65
identified at the ED. Twenty were excluded because ICU admission 52 (23)
of HIV infection. Forty-four (19%) had HCAP and Pao2/Fio2 ratio , 250 74 (32)
184 had CAP. Hospitalization in the previous 90 days Vasopressor use 38 (16)
(25 patients, 56.8%) was the most common condition Multilobar involvement 101 (44)
Pleural effusion 71 (31)
in the HCAP cohort, with 16 (38.5%) patients admit- Empyema 18 (8)
ted from long-term care facilities. Only eight were Therapy
receiving cancer chemotherapy, and one patient was Discordant therapy 2 (1)
receiving hemodialysis. Six patients met more than Combination therapy 118 (51)
one condition. PSI score I–III 65 (28)
PSI score IV-IV 163 (72)
The demographic features are presented in Table 1. CURB-65 score
Two distinct populations from the community pre- 0-2 141 (61.8)
sented with pneumococcal pneumonia (Table 2). The ⱖ3 87 (38.2)
HCAP cohort presented more frequently with base- 30-d mortality 27 (12)
line comorbidities (84% vs 60%, P , .01) and had Data given as No. (%) unless otherwise specified. CAP 5 community-
higher Charlson index. Overall, 72% of the entire acquired pneumonia; CURB-65 5 confusion, urea nitrogen, respira-
cohort presented a risk of class IV or V PSI score; tory rate, BP, 65 years of age or older; HCAP 5 health-care-associated
pneumonia; IQR 5 interquartile range; PSI 5 pneumonia severity
however, the HCAP cohort presented more severe index.
illness overall and a significantly higher PSI score aThose vaccinated within the last 5 y.

(Table 2). A trend toward higher hypoxemia was

associated with HCAP but did not correlate with
greater mechanical ventilation requirement. At same
time, there was a trend toward less use of vasopres-
sors in HCAP, with the distribution of hypotensive
patients not different among patients with HCAP and
CAP. Indeed, most patients with HCAP were admit-
ted to medical wards, with a significantly less frequent
ICU hospitalization in the HCAP (11.3%) than in the
CAP cohort (25.5%, P , .05). Finally, medical orders
about therapeutic limitation were explicitly stated in
22 patients, 15 in the HCAP group and seven in the
CAP group (34% vs 3.8%, P , 0,001).
The most frequently prescribed antibiotic thera-
pies in patients with HCAP were combination ther-
apy, including third-generation cephalosporin and
macrolides (36%) or amoxicillin-clavulanate (25%).
In patients with CAP, the combination therapy with
third-generation cephalosporin and macrolides was
administered in 46%, amoxicillin-clavulanate in 21%,
and nonpseudomonal fluoroquinolones in 11%.
Using the 2008 CLSI breakpoints, nonsusceptibility
to penicillin (MIC ⱖ 4 mg/mL) was documented in
only three of 228 (1.5%) episodes. Three isolates were
also documented as resistant to cephalosporins (one
patient in the HCAP cohort). Resistance to mac-
rolides was 36% in the HCAP cohort vs 13% in the
CAP cohort (P , .01, Table 2). However, only two
patients (one in each group) received inappropriate
therapy (2.3% vs 0.5%, P 5 .34). Available records
documented that exposure to the 23-valent pneumo-
coccal vaccine in the prior 5 years was uncommon.
Indeed, 4.5% of HCAP patients were vaccinated
compared with 10% of CAP (P 5 .45). Complications
and outcomes are shown in Table 2. CAP and HCAP
cohorts again presented differences. Patients with
HCAP had higher rates of complications, which were
generally associated with S pneumoniae bacteremia.
Interestingly, among HCAP subgroups, patients with
prior hospitalization achieved the highest mortality
(12 out of 25, 48%), being 18% in elderly care group
(three of 18) and 12% (one of eight) in the chemotherapy
group. No significant differences in age, comor-
bidities, and severity of illness were documented among
subgroups. Univariate analysis (Table 3) revealed that
30-day mortality was influenced by several underlying

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© 2010 American College of Chest Physicians
Table 2—Univariate Analysis for Conditions Associated With HCAP vs CAP in Bacteremic Pneumococcal Pneumonia

Variable HCAP, n 5 44 CAP, n 5 184 P Value

Median age (IQR) 77 (68-83) 68 (42-79) , .001
Charlson index 2.81 6 1.9 1.23 6 1.42 , .001
Comorbidities
Cardiomyopathy 14 (31.8) 39 (21.1) .16
Lung disease 21 (47.7) 42 (22.8) , .01
Liver disease 9 (20.4) 18 (9.7) .06
Renal disease 6 (13.6) 16 (8.6) .39
Pao2 /Fio2 (, 250) 18 (40.9) 56 (30.4) .21
Shock 11 (25) 53 (28.8) .71
Vasopressor use 4 (9) 34 (18.4) .17
ICU admission 5 (11.3) 47 (25.5) , .05
Multilobar involvement 18 (40.9) 83 (45) .73
Mechanical ventilation 4 (9) 35 (19) .17
Pleural effusion 17 (38.6) 54 (29.3) .27
Macrolide resistance 16 (36.3) 22 (11.9) , .01
PSI score class IV-V 42 (95.4) 121 (65.7) , .001
CURB-65 ⱖ 3 22 (50) 65 (35) .08
30-d mortality 13 (29.5) 14 (7.6) , .001
LOS . 10 d 12/29 (41.3) 84/167 (50.2) .82
Data given as No. (%) unless otherwise noted. LOS 5 length of stay. See Table 1 for expansion of other abbreviations.

conditions, reflected by higher Charlson index. Other
complications (level of consciousness, vasoactive
drugs use, multilobar involvement, Pao2/Fio2 ratio)
were also associated with 30-day mortality. The
HCAP cohort suffered a higher mortality rate (29.5%
vs 7.6%, P , .001). The Kaplan-Meier survival curves
(Fig 1) of HCAP vs CAP cohorts showed statistically
significant differences (P 5 .001). After adjustment for
PSI class (class I-III vs class IV-V), patients with HCAP
had a significantly higher 30-day mortality (adjusted
Table 3—Univariate Analysis of Potential Predisposing
Factors for 30-d Mortality Among 228 Patients With
Bacteremic Pneumococcal Pneumonia
OR [aOR] 5 3.65, 95% CI, 1.54-8.66; Hosmer-
Lemeshow goodness-of-fit P 5 .942) than patients
with CAP. After adjustment for CURB-65 score (0-2
vs ⱖ 3) patients with HCAP had a significantly higher
30-day mortality (aOR 5 4.58; 95% CI, 1.91-10.94;
Hosmer-Lemeshow goodness-of-fit P 5 .550) than
patients with CAP.
When only class IV-V patients (n 5 163) were ana-
lyzed, HCAP was associated with higher mortality in
the univariate analysis (OR 5 3.72; 95% CI, 1.56-8.90)
and after adjustment for age (aOR 5 3.76; 95% CI,
1.54-9.15; Hosmer-Lemeshow goodness-of-fit P 5 .830)
compared with CAP. Figure 2 shows the estimated

Predisposing Factors OR for Death (95% CI) P Value

Age . 65 y 2.09 (0.84-5.17) .14

Alcoholism 2.70 (1.03-7.10) .05
HCAP 5.09 (2.18-11.87) , .001
Comorbidity
Cardiomyopathy 1.83 (0.77-4.37) .22
Lung disease 2.35 (1.03-5.35) .05
Liver disease 2.58 (0.93-7.15) .10
Renal disease 0.72 (0.16-3.28) 1.00
Charlson index 1.41 (1.13-1.76) , .01
Severity at admission
Altered mental status 3.37 (1.44-7.91) , .01
RR . 30/min 3.30 (1.38-7.91) , .01
Pao2 /Fio2 , 250 6.30 (2.60-15.23) , .01
Acute renal failure 1.23 (0.55-2.77) .68
Multilobar involvement 6.79 (2.47-18.60) .001
Vasopressor use 4.43 (1.86-10.55) .001
ICU admission 3.22 (1.39-7.41) , .01
Antibiotic therapy
Monotherapy 1.68 (0.73-3.85) .22
Figure 1. Kaplan-Meier survival curve for HCAP vs CAP cohorts
OR 5 odds ratio; RR 5 respiratory rate. See Table 1 for expansion of (censored at 30 days). CAP 5 community-acquired pneumonia;
other abbreviation. HCAP 5 health-care-associated pneumonia.

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© 2010 American College of Chest Physicians
 monia, and evaluates the implications of HCAP in
the ICU. Our findings endorse the concept that
patients with pneumococcal HCAP present signifi-
cant differences in terms of demographics, severity of
illness, and complications. These differences are not
only of academic interest, since HCAP was associated
with higher mortality. Interestingly, inappropriate
therapy was uncommon when isolates were classified
using 2008 CLSI breakpoints.8 Although PSI was pri-
mary designed to assess severity in patients with CAP,
when patients with HCAP were analyzed we found
an excess of mortality comparing with the original
studies evaluating this score (Fig 2). A lower ICU
admission and a trend toward lower rates of mech-
anical ventilation and need for vasopressors were
reported for patients having HCAP.
Figure 2. Estimated and observed mortality for patients with PSI
In a retrospective cohort study, Kollef et al12
classes IV and V. PSI 5 pneumonia severity index. See Figure 1 reviewed a large multi-institutional database of more
legend for expansion of other abbreviations. than 4,500 positive-culture patients and identified
20% of patients as having HCAP. S pneumoniae was
and observed mortality for patients with PSI classes documented in 16% of patients with CAP and 5% of
IV and V. Finally, a multivariable logistic regression patients with HCAP. In a study in Spain that used a
analysis (Table 4) identified a significantly higher similar design,4 HCAP was identified in 17.3% of the
30-day mortality in patients with HCAP (OR 5 5.56; cohort, S pneumoniae being the predominant organism.
95% CI, 1.86-16.5), patients with Pao2/Fio2 ratio In an Italian study,1 increased severity, longer hospi-
, 250 (OR 3.90; 95% CI, 1.42-10.71), and need for talization, and higher mortality were reported for the
vasopressor therapy (OR 5 4.22; 95% CI, 1.37-12.9); HCAP cohort. Unfortunately, this study reported
Hosmer-Lemeshow goodness-of-fit P 5 .360. The only limited information on organisms and ICU care.
model did not change when patients receiving discor- A recent study reported that patients with HCAP
dant therapy were excluded. Also, when patients with were more likely to receive inappropriate empirical
CURB-65 ⱖ 3 were analyzed (n 5 87), HCAP was also antibiotic coverage than those with CAP.2 The same
associated with higher mortality in the univariate anal- group found an association between inappropriate
ysis (OR 5 3.14; 95% CI, 1.04-9.43) and after adjust- empirical initial therapy and mortality in a logistic
ment for age (aOR 5 3.15; 95% CI, 1.01-9.83; regression analysis (OR 5 2.88; 95% CI, 1.46-5.67).
Hosmer-Lemeshow goodness-of-fit P 5 .605) com- Late escalation did not improve survival.13 Accord-
pared with CAP. When patients not admitted to the ing to the 2005 American Thoracic Society/Infec-
ICU were analyzed, patients with HCAP were older, tious Disease Society of America guidelines, patients
had higher Charlson index and more hypoxemia, and
were more likely to be class IV/V PSI score (Table 5).
Table 5—Characteristics of 176 Patients With
Bacteremic Pneumococcal Pneumonia Not Admitted to
ICU
Discussion
HCAP, CAP,
This article compares CAP with HCAP specifically Variable n 5 39 n 5 137 P Value
in monomicrobial bacteremic pneumococcal pneu- Median age (IQR) 77 (72-83) 70 (46-79) .001
Charlson index, mean 6 SD 2.92 6 1.99 1.13 6 1.36 , .001
Comorbidities 32 (82) 81 (59) , .01
Table 4—Results of the Multivariable Regression Cardiomyopathy 13 (33) 23 (17) , .05
Logistic Analysis for 30-d Mortality Lung disease 18 (46) 34 (25) , .05
Liver disease 8 (20.5) 11 (8) , .05
Variable OR (95% CI) P Value
Renal disease 6 (15) 9 (6.5) .10
HCAP 5.56 (1.86-16.59) , .05 Pao2/Fio2 (, 250) 13 (33) 23 (17) , .05
Need for vasopressors 4.22 (1.37-12.99) .01 Multilobar involvement 13 (33) 43 (31) .84
Pao2/Fio2 , 250 3.90 (1.42-10.71) , .01 PSI score class IV-V 37 (94) 79 (57) , .001
Alcoholism 2.04 (0.61-6.74) .24 CURB-65 ⱖ 3 18 (46) 35 (25) .01
Altered mental status 1.56 (0.57-4.24) .38 30-d Mortality 10 (26) 5 (3.6) , .001
Charlson comorbidities index 1.24 (0.94-1.63) .11
Data given as No. (%) unless otherwise specified. See Table 1 for expansion
See Tables 1 and 3 for expansion of abbreviations. of abbreviations.

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 Table 6—Relationship Between Death/ICU Admission in Different Health-Care Associated Infections Studies
Current Study
Variable HCAP CAP
Mortality, No. (%) 13 (29.5) 14 (7.6)
ICU admission, No. (%) 5 (11.3) 47 (25.5)
Death/ICU ratio 2.6 0.3
CAI 5 community-acquired infection; HCAI 5 health-care-associated infection. See Table 1 for expansion of other abbreviations.
with HCAP and CAP are at risk for infection with
the same multidrug-resistant pathogens.3 However,
in the HCAP group a substantial number of patients
were also infected with microorganisms that cause
CAP (pneumococcus, Legionella, and even virus).
Many recent publications have reviewed the role of
gram-negative bacilli or Staphylococcus aureus,14-17
but acceptance of the HCAP definition is still
controversial. A recent respiratory forum18 suggested
describing different categories based on the following:
(1) need for mechanical ventilation, (2) prior antibi-
otics for more than 3 days within the past 6 months,
and (3) poor functional status, defined as an activi-
ties of daily living score of . 12.5. Wunderink19 also
noted that the distinction between HCAP and CAP
has never been totally clear.
In the present study, only five patients with HCAP
received mechanical ventilation. The diagnosis of
HCAP was significantly associated with increased
30-day mortality but did not increase the probability
of receiving discordant therapy when assessed using
2008 CLSI breakpoints. Previous reports have classi-
fied resistant organisms as nonsusceptible, based on
older breakpoints.8 Therefore, the number of patients
receiving therapies classified as inappropriate was
substantially higher in the past, at least for pneumo-
coccal HCAP.
An important issue is that of nonaggressive or lim-
ited treatment. The HCAP group was more severely
ill, but made much lower use of advanced care
modalities. How much of the excess mortality was
because of physician or patient preference for limit-
ing the extent of support given due to “terminal”
comorbidities? Although in the HCAP group mortal-
ity risk was more than twice the ICU admission rate
(29.5% vs 11.3%), in patients with CAP the risk for
mortality was one-third of ICU admission rate (7.6%
vs 25.5%). This information is concordant with find-
ings reported for HCAP4 and bacteremia,20 suggest-
ing that these patients are less likely to be admitted in
the ICU despite higher mortality (Table 6) and should
be considered as a separate entity.
Our study has some strengths and limitations.
One is its sample size: although the HCAP cohort
contained fewer than 50 patients from a single cen-
ter, it was large enough to identify distinctions in
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© 2010 American College of Chest Physicians
Carratalà et al4 McDonald et al20
HCAP CAP HCAI CAI
13 (10.3) 26 (4.3) 35 (19.7) 18 (13.6)
8 (6.3) 52 (8.7) 40 (22.5) 28 (21.2)
1.6 0.5 0.9 0.6
terms of predisposing factors and outcomes. Another
strength was that it focused on one pathogen with
definite diagnosis (blood cultures), but a full picture
of pneumococcal disease requires inclusion of non-
bacteremic cases. An additional strength is that our
study is a prospective analysis and the diagnosis was
based on clinical grounds. This contrasts with many
reported HCAP studies in which the diagnosis was
retrospective and based on administrative records.
One limitation, which is also inherent to prior stud-
ies on HCAP,1,2,4,5,9,12-14 is the fact that the distribu-
tion of HCAP in other geographical areas is expected
to be different. Other limitations include lack of a
measure of patient mobility and that the HCAP
patient population is skewed to patients with a his-
tory of previous hospitalization and those coming
from long-term facilities. In addition to these prior
reports on HCAP, our study provides additional
insight into the demographics of S pneumoniae HCAP
and is relevant as it provides additional evidence in
the field of health-care-associated infections, in the
light of recently published guidelines for manage-
ment of HCAP.3
In summary, HCAP accounts for a significant num-
ber of cases of pneumococcal pneumonia, which,
using traditional definitions, would be classified as
CAP. The HCAP cohort was significantly older, had
more comorbidities, higher mean PSI scores, and a
significantly higher mortality rate. HCAP accounts
for a significantly lower proportion of patients admit-
ted to the ICU, probably because most of these
HCAP patients were elderly and had more comor-
bid conditions. Our findings suggest that, at least for
pneumococcal HCAP, excess mortality was due in
part to the decision of the physician or patient to limit
the extent of support given to patients of advanced
age and with comorbidities.
Appendix
The Proyecto Corporativo de Neumonía (PROCORNEU)
Study Group is formed by E. Bouza (Hospital Gregorio
Marañon); J. Liñares (Hospital Bellvitge); J. Rello (IISPV);
A. Torres (Hospital Clinic i Provincial); E. Perez-Trallero
(Hospital Donosti); V. Ausina (Hospital Germans Trias I Pujol);
J. Valles (Hospital Parc Taulí); E. Garcia (CSIC); and A. Gonzalez
de la Campa (ISCIII).
CHEST / 137 / 5 / MAY, 2010 1143
 Acknowledgments
Author contributions: Dr Rello: contributed to study design,
analysis of data, writing the first draft, and creating the final ver-
sion of the manuscript.
Dr Luján: contributed to study design, enrolling patients, rec-
ording variables, conducting follow-up, collecting samples,
analyzing data, writing the first draft, and creating the final version
of the manuscript.
Dr Gallego: contributed to study design, analysis of data, writing
the first draft, and creating the final version of the manuscript.
Dr Vallés: contributed to enrolling patients, recording variables,
conducting follow-up, collecting samples, and creating the final ver-
sion of the manuscript.
Dr Belmonte: contributed to enrolling patients, recording vari-
ables, conducting follow-up, collecting samples, and creating the
final version of the manuscript.
Dr Fontanals: contributed to enrolling patients, recording var-
iables, conducting follow-up, collecting samples, and creating the
final version of the manuscript.
Dr Diaz: contributed to study design and creating the final version
of the manuscript.
Dr Lisboa: contributed to analysis of data, writing the first draft,
and creating the final version of the manuscript.
Financial/nonfinancial disclosures: The authors have reported
to CHEST that no potential conflicts of interest exist with any
companies/organizations whose products or services may be dis-
cussed in this article.
Other contributions: We are indebted to Michael Maudsley for
help in editing the manuscript and David Suárez for statistical
support.
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Original Research