- Research article
- Open access
- Published:
Predictors of hospital mortality among septic ICU patients with Acinetobacter spp.bacteremia: a cohort study
BMC Infectious Diseases volume 14, Article number: 572 (2014)
Abstract
Background
We hypothesized that among septic ICU patients with Acinetobacter spp. bacteremia (Ac-BSI), carbapenem-resistant Acinetobacter spp. (CRAc) increase risk for inappropriate initial antibiotic therapy (non-IAAT), and non-IAAT is a predictor of hospital death.
Methods
We conducted a retrospective cohort study of adult septic ICU patients with Ac-BSI. Non-IAAT was defined as exposure to initially prescribed antibiotics not active against the pathogen based on in vitro susceptibility testing, and having no exposure to appropriate antimicrobial treatment within 24 hours of drawing positive culture. We compared patients who died to those who survived, and derived regression models to identify predictors of hospital mortality and of non-IAAT.
Results
Out of 131 patients with Ac-BSI, 65 (49.6%) died (non-survivors, NS). NS were older (63 [51, 76] vs. 56 [45, 66] years, p = 0.014), and sicker than survivors (S): APACHE II (24 [19, 31] vs. 18 [13, 22], p < 0.001) and Charlson (5 [2, 8] vs. 3 [1, 6], p = 0.009) scores. NS were also more likely than S to require pressors (75.4% vs. 42.4%, p < 0.001) and mechanical ventilation (75.4% vs. 53.0%, p = 0.008). Both CRAc (69.2% vs. 47.0%, p = 0.010) and non-IAAT (83.1% vs. 59.1%, p = 0.002) were more frequent among NS than S. In multivariate analyses, non-IAAT emerged as an independent predictor of hospital death (risk ratio [RR] 1.42, 95% confidence interval [CI] 1.10-1.58), while CRAc was the single strongest predictor of non-IAAT (RR 2.66, 95% CI 2.43-2.72).
Conclusions
Among septic ICU patients with Ac-BSI, non-IAAT predicts mortality. Carbapenem resistance appears to mediate the relationship between non-IAAT and mortality.
Background
In its 2013 report titled “Antibiotic Resistance Threats in the United States, 2013”, the US Centers for Disease Control and Prevention rated carbapenem resistance as an urgent (among Enterobacteriaceae) or serious (among Acinetobacter spp.) threat [1]. Since anti-pseudomonal carbapenems often represent a last-resort option, emerging resistance to this class indeed reflects a grave concern. The growing prevalence of carbapenem-resistant pathogens makes it difficult for the clinician to choose reliably what will qualify as initially appropriate antibiotic therapy (IAAT).
Understandably, of greatest concern is carbapenem resistance among Enterobacteriaceae and Pseudomonas aeruginosa, as they typically comprise the dominant organisms encoding carbapenemases [2]-[5]. Acinetobacter spp., on the other hand, is a less frequently encountered pathogen. However, the proportion of carbapenem resistance among Acinetobacter spp. isolates is 2–5 times that seen in Pseudomonas aeruginosa and Klebsiella spp., and over an order of magnitude that among E. coli[3].
In the setting of many serious infections, one of the critical determinants of the outcome is early empiric coverage for the culprit organism [6]-[14]. Failing to administer in a timely manner an agent that is in vitro active against the offending pathogen(s) leads to increased mortality and morbidity. Acknowledgement of this observation has led to the practice of de-escalation where one often starts with an initially broad anti-infective (or a combination of agents) and later narrows the spectrum of coverage when culture results become available [15]. Unfortunately, for Acinetobacter spp. it is unclear if and how one can successfully execute this strategy, particularly in light of the fact that most isolates are resistant to last-resort treatment. Similarly, as a matter of health policy and antibiotic stewardship, it is necessary to appreciate the contribution of carbapenem resistance to the poor outcomes in infections with Acinetobacter spp. Gaining insight into the relationship between resistance and outcomes specifically as it relates to this pathogen may help clarify the urgency of the need for novel agents with which to treat it.
We hypothesized that in the setting of severe sepsis or septic shock due to Acinetobacter spp., failure to receive IAAT increased the risk of death, and that, as a corollary, carbapenem resistance is a strong determinant of exposure to non-IAAT.
Methods
Study design and ethical standards
We conducted a single-center retrospective cohort study from January 2002 to December 2012. Barnes-Jewish Hospital is a 1,200-bed urban academic medical center located in St. Louis, MO. The study was approved by the Washington University School of Medicine Human Studies Committee and informed consent was waived.
Study cohort
All consecutive adult ICU patients between January 2002 and December 2012 were enrolled if 1). They had a positive blood culture for Acinetobacter spp., and 2). There was an International Classification of Diseases, version 9, clinical modification (ICD-9-CM) code for an acute organ dysfunction [16]. Only the first episode of sepsis was included.
Definitions
To be included in the analysis patients had to meet criteria for severe sepsis based on discharge ICD-9-CM codes for acute organ dysfunction [16]. Septic shock was present if vasopressors (norepinephrine, dopamine, epinephrine, phenylephrine or vasopressin) were initiated within 24 hours of the blood culture collection date and time. Antimicrobial treatment was deemed IAAT if the initially prescribed antibiotic regimen was active against the identified pathogen based on in vitro susceptibility testing and administered within 24 hours following blood culture collection; all other regimens were classified as non-IAAT. Because the role of combination therapy in treating Acinetobacter spp. is not well defined, combination therapy was not a criterion for defining IAAT. We also required that antibiotics be prescribed for ≥24 hours. Prior antibiotic exposure occurred within the preceding 90 days, as did prior hospitalization, while prior bacteremia was defined within 30 days of the current episode. The bacteremia was deemed to be a healthcare-associated complication (HAC) if one of the following risk factors was identified: 1). Need for dialysis; 2). Immune suppression; 3). Prior hospitalization; 4). Prior antibiotics; 5). Current infection deemed hospital-acquired blood stream infection (HABSI; onset of infection ≥2 days after admission). Carbapenem-resistant Acinetobacter spp. (CRAc) was present if it was the organism that grew out in at least one blood culture specimen.
Antimicrobial susceptibility testing
The microbiology laboratory performed antimicrobial susceptibility of the isolates using the disk diffusion method according to guidelines and breakpoints established by the Clinical Laboratory and Standards Institute (CLSI) appropriate to the year the organism was isolated.
Data elements
Patient baseline characteristics and process of care variables were collected from the automated hospital medical record, microbiology database, and pharmacy database of Barnes-Jewish Hospital. Electronic inpatient and outpatient medical records available for all patients in the BJC Healthcare system were reviewed to determine prior antibiotic exposure. The baseline characteristics collected included: age, gender, race, past history of congestive heart failure, chronic obstructive pulmonary disease, diabetes mellitus, chronic liver disease, underlying malignancy, and end-stage renal disease requiring dialysis. The Acute Physiology and Chronic Health Evaluation (APACHE) II and Charlson comorbidity scores were calculated based on clinical data present during the twenty-four hours after the positive blood cultures were obtained [17]. This was done to accommodate patients with community-acquired and healthcare-associated community-onset infections who only had clinical data available after blood cultures were drawn. The primary outcome variable was hospital mortality. Because we were interested in understanding the contribution of CRAc to the risk of receiving non-IAAT, we examined it as a secondary endpoint in a logistic regression.
Statistical analyses
Continuous variables were reported as means with standard deviations when distributed normally, or medians with 25th and 75th percentiles when skewed. Differences between mean values were tested via Student’s t-test, while those between medians were examined using the Mann–Whitney U test. Categorical data were summarized as proportions, and the Chi-square test or Fisher’s exact test for small samples was used to examine differences between groups. We developed several multiple logistic regression models to identify clinical risk factors associated with hospital mortality. In the mortality models, all risk factors that were significant at ≤0.20 in the univariate analyses, as well as all biologically plausible factors even if they did not reach this level of significance, were included in the corresponding multivariable analyses. All variables entered into the models were examined to assess for co-linearity, and interaction terms were tested. The most parsimonious models were derived using the backward manual elimination method, and the best-fitting model was chosen based on the c-statistic. The model’s calibration was assessed with the Hosmer-Lemeshow goodness-of-fit test. To exclude the influence of time-dependent covariates on hospital mortality, we confirmed the risk factors in a Cox proportional hazards model. Similarly, the most parsimonious model for the predictors of non-IAAT was computed and its fit was tested with the c-statistic and the Hosmer-Lemeshow goodness-of-fit test.
Because both outcomes of interest in each of the models (mortality and non-IAAT) occurred with high frequency (overall mortality 49.6%, overall non-IAAT 71.0%), the adjusted odds ratios would overestimate the magnitude of the actual risk associated with each of the independent variables examined. For this reason we corrected the risk estimate according to the method of Zhang [18], and report the corrected risk ratios.
All tests were two-tailed, and a p value <0.05 was deemed a priori to represent statistical significance. All calculations were done in Stata/SE, version 9 (StataCorp, College Station, TX).
Results
One hundred and thirty-one patients with severe sepsis or septic shock due to Acinetobacter spp. met the inclusion criteria. Among these 76 (58.0%) were CRAc. (Table 1 lists additional drug susceptibilities stratified by carbapenem resistance). Overall hospital mortality was 49.6%. The patients’ baseline characteristics are listed in Table 2. Those who died were older and had a higher comorbidity burden, as signified by the Charlson comorbidity score, than those who survived their hospitalization. A higher proportion of those patients who died prior to discharge had dialysis (28.1% vs. 15.2%, p = 0.072), prior antibiotics (75.4% vs. 57.6%, p = 0.031) and HABSI (72.3% vs. 50.0%, p = 0.009) as risk factors for a HAC than those who were discharged alive.
During the hospitalization and prior to sepsis onset, patients who did not survive had a far longer pre-sepsis median hospital length of stay (LOS) (13 vs. 2 days, p = 0.002) (Table 3). All markers of severity of acute illness were higher in patients who died compared to those who survived; this included the APACHE II score, the presence of septic shock and the need for mechanical ventilation (Table 3). Urine and infected line were less likely and lung was more likely as a source of infection among non-survivors compared to survivors. In contrast to pre-sepsis LOS, post-sepsis onset median LOS was far shorter among those who did not than those who did survive their hospitalization (4.5 vs. 15 days, p < 0.001).
There were substantial differences between the two groups in terms of the likelihood of CRAc as the sepsis culprit (69.2% among non-survivors vs. 47.0%% among survivors, p = 0.010) (Table 3). Additionally, non-survivors were approximately 50% more likely to receive non-IAAT than those patients who survived their hospitalization (83.1% vs. 59.1%, p = 0.002). Notably, among those patients who harbored CRAc, the risk for being treated inappropriately was 96.1%, compared to 36.4% among those with a susceptible organism, p < 0.001.
Table 4 shows the results of a multiple logistic regression model derivation to examine the variables associated with hospital mortality in this population. In this model, receiving non-IAAT was the strongest predictor of hospital death, with the corrected risk ratio of 1.42 (95% confidence interval 1.10 to 1.58, p = 0.015). A Cox proportional hazards model, confirmed non-IAAT (hazard ratio 2.37, 95% confidence interval 1.16 to 4.85, p = 0.019) and APACHE II score (hazard ratio 1.08, 95% confidence interval 1.03 to 1.12, p < 0.001; per 1 point) as risk factors for hospital death. In an additional logistic regression model to examine factors that contribute to the inappropriate choice of therapy, CRAc as the etiology of sepsis was a strong predictor of inappropriate treatment, with the corrected risk ratio measuring 2.66 (95% confidence interval 2.43 to 2.72, p < 0.001). The only other predictor retained in the model was congestive heart failure, with the corrected risk ratio 1.89 (95% confidence interval 1.01 to 2.63, p = 0.048) (AUROC 0.884, Hosmer-Lemeshow p =0.513).
Discussion
In the current cohort of patients with sepsis due to Acinetobacter spp., the prevalence of carbapenem resistance was high at nearly 60%. More importantly, the risk for receiving non-IAAT in this setting was extreme. Specifically, the presence of CRAc as the infectious pathogen more than doubled the risk of receiving non-IAAT compared to having a carbapanem-susceptible isolate. Additionally, despite the high baseline rate of death in patients with Acinetobacter spp. sepsis, failure to receive appropriate therapy further increased the risk of hospital mortality.
A vast volume of research has emphasized the importance of early appropriate antimicrobial therapy in the setting of serious infections. Indeed, it has been shown in sepsis and pneumonia that the penalty for the wrong choice of empiric treatment is a 2-4-fold increase in the risk of death [6]-[8],[10]-[14], and that escalation of treatment in response to culture results fails to mitigate this increase in risk [9]. Our findings generally confirm this relationship. However, the current study adds to these earlier analyses by focusing specifically on a pathogen that is generally only sporadically found in US ICUs. The majority of earlier studies dealing with inappropriate therapy has addressed specific disease states (e.g., pneumonia), irrespective of the pathogen, or has not attempted to measure impact of inappropriate therapy in the setting of sepsis and septic shock as a syndrome. In this vein, few earlier efforts have dealt specifically with the issue of Acinetobacter spp. as a cause of bacteremia, and no other to the best of our knowledge has examined severe sepsis/septic shock. Indeed, the data on whether non-IAAT in the setting of Acinetobacter bacteremia as a contributor to the increase in the risk of death are conflicting. A small multi-center retrospective matched cohort study from Korea reported that non-IAAT was associated with a 6-fold increase in 30-day mortality [19]. Similarly, a single-center study from Turkey reported a nearly identical risk of 30-day morality to ours in association with non-IAAT (hazard ratio 2.1, 95% CI 1.2-3.7; P = 0.007) [20]. In contrast, several other studies failed to detect this relationship, though each suffered from a small sample size of bacteremia cases and other methodologic issues [21]-[24]. A cohort study from Turkey examining 100 cases of Acinetobacter bacteremia reported that carbapenem resistance was an independent risk factor for 14-day mortality [25]. However, while inappropriate empiric treatment was associated with an increase in mortality in the univariate analysis, it was not reported to be so in a multivariate analysis. It is unclear whether it was included in such and fell out or whether it was simply not examined. In either case, since we have demonstrated strong collinearity of non-IAAT with carbapanem resistance, including both in a single regression would not be statistically desirable. Another small cohort study conducted in the US examining the relationship between carbapenem resistance and mortality in A. baumanii bacteremia failed to detect an association, although appropriateness of treatment was an important determinant of hospital death [26]. However, such strong collinearity between non-IAAT and CRAc as we have detected in our study suggests that they may exist in the same causal pathway vis-à-vis outcomes. For this reason, it may be more statistically valid to examine them separately, as we have done, rather than in the same model.
Importantly, none of the above studies focused on the syndrome of sepsis. Because of the populations addressed in and limitations of earlier reports, ours expands upon past research exploring the mortality burden specifically related to Acinetobacter spp. severe sepsis and septic shock. Significantly, we illustrate that although outcomes are generally poor in persons infected with this organism, the additional impact of inappropriate therapy is substantial. As such, this suggests that there is an urgent need for agents that can provide empiric coverage for this pathogen. This last point is even more crucial in that the prevalence of drug-resistant Acinetobacter spp. is increasing both in the US and across the globe [27]. Thus, what may currently be of only a limited burden may in the future become much more of an issue. Conversely, our results emphasize the importance of public policy tools that foster drug development, such as the GAIN act, as well as the Food and Drug Administration’s attention to streamlining the development of antibacterial therapies in the setting of unmet medical needs [28].
Our results further suggest that carbapenem resistance is an important risk factor for receiving inappropriate empiric coverage. In other words, the key issue may not only be rapid identification of subjects specifically at risk for Acinetobacter spp., but may in fact be determining whether a patient is suffering from a potentially carbapenem-resistant pathogen. This not only highlights the urgent need for concerted efforts at preventing individual infections and curtailing the development and spread of resistant organisms, but also underscores the needs for novel rapid diagnostic tools. Moreover, these new diagnostics must provide clinicians up front with information about a pathogen’s likely susceptibilities rather than just simply identifying the organism.
Our study has a number of limitations. As a retrospective cohort it is prone to several forms of bias, most notably selection bias. We attempted to mitigate this by enrolling consecutive patients fitting the pre-determined enrollment criteria. Although we dealt with confounders by adjusting for those that were available, it is possible that some residual confounding remains, particularly confounding by indication. The fact that this is a single-center study in a very specific population of patients (those with Acinetobacter spp. sepsis) may diminish the generalizability of our results to other centers and populations. An additional potential threat to the generalizability of the findings is the fact that non-susceptibility to carbapanems was based on the corresponding year’s CLSI threshold for resistance. Applying higher MIC cut-offs either for carbapenems or other agents that have shown at least some in vitro susceptibilities at higher MICs would have reclassified some of the non-IAAT patients into the IAAT category [29],[30]. This reclassification would have the potential either to strengthen or to weaken the association between non-IAAT and mortality. It is important to note that, although our results strongly suggest that the association of carbapenem resistance with an increased risk of death is mechanistically related to the risk of receiving inappropriate empiric therapy, we cannot rule out that resistant Acinetobacter spp. may exert its lethal effect directly by virtue of higher virulence, as has been noted with other pathogens exhibiting higher MICs to certain antimicrobials [31],[32]. Because we examined hospital mortality rather than the more standard 28-day mortality as the primary outcome for our study, we may have underestimated the magnitude of this outcome.
Conclusions
In summary, our study sheds light on the mechanism for the detrimental effect on mortality of exposure to non-IAAT in the setting of Acinetobacter spp. sepsis. Namely, it is the pathogen’s resistance to carbapenems, the class of last resort, that appears to mediate at least in part this adverse outcome. In this way, this pathogen is an eloquent illustration of a recent World Health Organization’s statement: “A post-antibiotic era – in which common infections and minor injuries can kill – far from being an apocalyptic fantasy, is instead a very real possibility for the 21st Century” [33].
Authors’ contributions
MDZ participated in conception, design, analysis and interpretation of the data, drafted the manuscript and has given final approval for the version to be published. MDZ takes responsibility for data accuracy and analytic and reporting integrity of the study. AFS participated in conception, design, analysis and interpretation of the data. He was involved in revising the manuscript critically for important intellectual content, and has given final approval for the version to be published. STM participated in conception, design, acquisition and interpretation of the data. He was involved in revising the manuscript critically for important intellectual content, and has given final approval for the version to be published. MHK participated in conception, design, acquisition and interpretation of the data. He was involved in revising the manuscript critically for important intellectual content, and has given final approval for the version to be published. All authors read and approved the final manuscript.
References
Centers for Disease Control and Prevention: Antibiotic Resistance Threats in the United States, 2013. Available at Accessed May 29, 2014, [http://www.cdc.gov/drugresistance/threat-report-2013/pdf/ar-threats-2013-508.pdf#page=59]
Hidron AI, Edwards JR, Patel J, Horan TC, Sievert DM, Pollock DA, Fridkin SK: NHSN annual update: antimicrobial-resistant pathogens associated with healthcare-associated infections: annual summary of data reported to the National Healthcare Safety Network at the Centers for Disease Control and Prevention, 2006–2007. Infect Control Hosp Epidemiol. 2008, 29: 996-1011. 10.1086/591861.
Sievert DM, Ricks P, Edwards JR, Schneider A, Patel J, Srinivasan A, Kallen A, Limbago B, Fridkin S: Antimicrobial-resistant pathogens associated with healthcare-associated infections: Summary of data reported to the National Healthcare Safety Network at the Centers for Disease Control and Prevention, 2009–2010. Infect Control Hosp Epidemiol. 2013, 34: 1-14. 10.1086/668770.
Zilberberg MD, Shorr AF: Prevalence of multidrug-resistant Pseudomonas aeruginosa and carbapenem-resistant Enterobacteriaceae among specimens from hospitalized patients with pneumonia and bloodstream infections in the United States from 2000 to 2009. J Hosp Med. 2013, 8: 559-563.
Zilberberg MD, Shorr AF: Secular trends in gram-negative resistance among urinary tract infection hospitalizations in the United States, 2000–2009. Infect Control Hosp Epidemiol. 2013, 34: 940-946. 10.1086/671740.
Micek ST, Kollef KE, Reichley RM, Roubinian N, Kollef MH: Health care-associated pneumonia and community-acquired pneumonia: a single-center experience. Antimicrob Agents Chemother. 2007, 51: 3568-3573. 10.1128/AAC.00851-07.
Iregui M, Ward S, Sherman G, Fraser VJ, Kollef MH: Clinical importance of delays in the initiation of appropriate antibiotic treatment for ventilator-associated pneumonia. Chest. 2002, 122: 262-268. 10.1378/chest.122.1.262.
Alvarez-Lerma F: Modification of empiric antibiotic treatment in patients with pneumonia acquired in the intensive care unit. Intensive Care Med. 1996, 22: 387-394. 10.1007/BF01712153.
Zilberberg MD, Shorr AF, Micek MT, Mody SH, Kollef MH: Antimicrobial therapy escalation and hospital mortality among patients with HCAP: a single center experience. Chest. 2008, 134: 963-968. 10.1378/chest.08-0842.
Shorr AF, Micek ST, Welch EC, Doherty JA, Reichley RM, Kollef MH: Inappropriate antibiotic therapy in Gram-negative sepsis increases hospital length of stay. Crit Care Med. 2011, 39: 46-51. 10.1097/CCM.0b013e3181fa41a7.
Kollef MH, Sherman G, Ward S, Fraser VJ: Inadequate antimicrobial treatment of infections: a risk factor for hospital mortality among critically ill patients. Chest. 1999, 115: 462-474. 10.1378/chest.115.2.462.
Garnacho-Montero J, Garcia-Garmendia JL, Barrero-Almodovar A, Jimenez-Jimenez FJ, Perez-Paredes C, Ortiz-Leyba C: Impact of adequate empirical antibiotic therapy on the outcome of patients admitted to the intensive care unit with sepsis. Crit Care Med. 2003, 31: 2742-2751. 10.1097/01.CCM.0000098031.24329.10.
Harbarth S, Garbino J, Pugin J, Romand JA, Lew D, Pittet D: Inappropriate initial antimicrobial therapy and its effect on survival in a clinical trial of immunomodulating therapy for severe sepsis. Am J Med. 2003, 115: 529-535. 10.1016/j.amjmed.2003.07.005.
Kumar A, Roberts D, Wood KE, Light B, Parrillo JE, Sharma S, Suppes R, Feinstein D, Zanotti S, Taiberg L, Gurka D, Kumar A, Cheang M: Duration of hypotension before initiation of effective antimicrobial therapy is the critical determinant of survival in human septic shock. Crit Care Med. 2006, 34: 1589-1596. 10.1097/01.CCM.0000217961.75225.E9.
Dellinger RP, Levy MM, Rhodes A, Annane D, Gerlach H, Opal SM, Sevransky JE, Sprung CL, Douglas IS, Jaeschke R, Osborn TM, Nunnally ME, Townsend SR, Reinhart K, Kleinpell RM, Angus DC, Deutschman CS, Machado FR, Rubenfeld GD, Webb SA, Beale RJ, Vincent JL, Moreno R: Surviving Sepsis Campaign: international guidelines for management of severe sepsis and septic shock: 2012. Crit Care Med. 2013, 41: 580-637. 10.1097/CCM.0b013e31827e83af.
Angus DC, Linde-Zwirble WT, Lidicker J, Clermont G, Carcillo J, Pinsky MR: Epidemiology of severe sepsis in the United States: analysis of incidence, outcome, and associated costs of care. Crit Care Med. 2001, 29: 1303-1310. 10.1097/00003246-200107000-00002.
Knaus WA, Draper EA, Wagner DP, Zimmerman JE: APACHE II: a severity of disease classification system. Crit Care Med. 1985, 13: 818-829. 10.1097/00003246-198510000-00009.
Zhang J, Kai YF: What’s the Relative Risk?: A Method of Correcting the Odds Ratio in Cohort Studies of Common Outcomes. JAMA. 1998, 280: 1690-1691. 10.1001/jama.280.19.1690.
Kwon KT, Oh WS, Song JH, Chang HH, Jung SI, Kim SW, Ryu SY, Heo ST, Jung DS, Rhee JY, Shin SY, Ko KS, Peck KR, Lee NY: Impact of imipenem resistance on mortality in patients with Acinetobacter bacteraemia. J Antimicrob Chemother. 2007, 59: 525-530. 10.1093/jac/dkl499.
Erbay A, Idil A, Gozel MG, Mumcuoglu I, Balaban N: Impact of early appropriate antimicrobial therapy on survival in Acinetobacter baumannii bloodstream infections. Int J Antimicrob Agnets. 2009, 34: 575-579. 10.1016/j.ijantimicag.2009.07.006.
Sunenshine RH, Wright MO, Maragakis LL, Harris AD, Song X, Hebden J, Cosgrove SE, Anderson A, Carnell J, Jernigan DB, Kleinbaum DG, Perl TM, Standiford HC, Srinivasan A: Multidrug-resistant Acinetobacter infection mortality rate and length of hospitalization. Emerg Infect Dis. 2007, 13: 97-103. 10.3201/eid1301.060716.
Chen HP, Chen TL, Lai CH, Fung CP, Wong WW, Yu KW, Liu CY: Predictors of mortality in Acinetobacter baumannii bacteremia. J Microbiol Immunol Infect. 2005, 38: 127-136.
Choi JY, Park YS, Kim CO, Yoon HJ, Shin SY, Kim YA, Song YG, Yong D, Lee K, Kim JM: Mortality risk factors of Acinetobacter baumannii bacteraemia. Intern Med J. 2005, 35: 599-603. 10.1111/j.1445-5994.2005.00925.x.
Falagas ME, Kasiakou SK, Rafailidis PI, Zouglakis G, Morfou P: Comparison of mortality of patients with Acinetobacter baumannii bacteraemia receiving appropriate and inappropriate empirical therapy. J Antimicrob Chemother. 2006, 57: 1251-1254. 10.1093/jac/dkl130.
Metan G, Sariguzel F, Sumerkan B: Factors influencing survival in patients with multi-drug-resistant Acinetobacter bacteraemia. Eur J Intern Med. 2009, 20: 540-544. 10.1016/j.ejim.2009.05.005.
Esterly JS, Griffith M, Qi C, Manczynski M, Postelnick MJ, Scheetz MH: Impact of carbapenem resistance and receipt of active antimicrobial therapy on clinical outcomes of Acinetobacter baumannii bloodstream infections. Antimicrob Agents Chemother. 2011, 55: 4844-4849. 10.1128/AAC.01728-10.
Maragakis LL, Perl TM: Acinetobacter baumannii: epidemiology, antimicrobial resistance, and treatment options. Clin Infect Dis. 2008, 46: 1254-1263. 10.1086/529198.
US Department of Health and Human Services, Food and Drug Administration, Center for Drug Evaluation and Research: Guidance for Industry: Antibacterial Therapies for Patients With Unmet Medical Need for the Treatment of Serious Bacterial Diseases. 2013. Available at ; accessed June 18, 2014., [http://www.fda.gov/downloads/drugs/guidancecomplianceregulatoryinformation/guidances/ucm359184.pdf]
Kiratisin P, Apisarnthanarak A, Kaewdaeng S: Synergistic activities between carbapenems and other antimicrobial agents against Acinetobacter baumannii including multidrug-resistant and extensively drug-resistant isolates. Int J Antimicrob Agents. 2010, 36: 243-246. 10.1016/j.ijantimicag.2010.04.011.
Sheng WH, Wang JT, Li SY, Lin YC, Cheng A, Chen YC, Chang SC: Comparative in vitro antimicrobial susceptibilities and synergistic activities of antimicrobial combinations against carbapenem-resistant Acinetobacter species: Acinetobacter baumannii versus Acinetobacter genospecies 3 and 13TU. Diagn Microbiol Infect Dis. 2011, 70: 380-386. 10.1016/j.diagmicrobio.2011.03.003.
Holmes NE, Turnidge JD, Munckhof WJ, Robinson JO, Korman TM, O’Sullivan MV, Anderson TL, Roberts SA, Gao W, Christiansen KJ, Coombs GW, Johnson PD, Howden BP: Antibiotic choice may not explain poorer outcomes in patients with Staphylococcus aureus bacteremia and high vancomycin minimum inhibitory concentrations. J Infect Dis. 2011, 204: 340-347. 10.1093/infdis/jir270.
Cervera C, Castaneda X, de la Maria CG, del Rio A, Moreno A, Soy D, Pericas JM, Falces C, Armero Y, Almela M, Ninot S, Pare JC, Mestres CA, Gatell JM, Marco F, Miro JM: Effect of vancomycin minimal inhibitory concentration on the outcome of methicillin-susceptible Staphylococcus aureus endocarditis. Clin Infect Dis. 2014, 58: 1668-1675. 10.1093/cid/ciu183.
World Health Organization: Antimicrobial resistance: Global report on surveillance 2014. Available at URL: Please check that the following URLs are working. If not, please provide alternatives: http://www.who.int/drugresistance/documents/surveillancereport/en/; accessed June 5, 2014.
Acknowledgements
This study was supported by a grant from Tetraphase Pharmaceutical, Inc., Watertown, MA. The funder had no role in study design, analyses, data interpretation, or in the preparation or submission of the manuscript. Although the funder was given the opportunity to review the manuscript prior to submission, all of the editorial decisions resided with the authors. No one other than the listed authors contributed to the study.
Disclosure
This study was supported by a grant from Tetraphase Pharmaceuticals, Inc., Watertown, MA; Dr. Kollef’s time was in part supported by the Barnes-Jewish Hospital Foundation. These data in part have been accepted for presentation at ID Week 2014 meeting in Philadelphia, PA, USA.
Author information
Authors and Affiliations
Corresponding author
Additional information
Competing interests
MDZ has served as a consultant to and/or received research funding from Cubist, Astellas, Pfizer and CareFusion and Theravance. AFS has served as a consultant to and/or received research funding from Cubist, Astellas, Pfizer, Forest, Theravance and CareFusion. STM has served as a consultant to and/or received research funding from Cubist, Astellas and Pfizer. MHK has served as a consultant to and/or received research funding from Cubist, Astellas, Pfizer, Forest and Theravance.
Rights and permissions
Open Access This article is licensed under a Creative Commons Attribution 4.0 International License, which permits use, sharing, adaptation, distribution and reproduction in any medium or format, as long as you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons licence, and indicate if changes were made.
The images or other third party material in this article are included in the article’s Creative Commons licence, unless indicated otherwise in a credit line to the material. If material is not included in the article’s Creative Commons licence and your intended use is not permitted by statutory regulation or exceeds the permitted use, you will need to obtain permission directly from the copyright holder.
To view a copy of this licence, visit https://creativecommons.org/licenses/by/4.0/.
The Creative Commons Public Domain Dedication waiver (https://creativecommons.org/publicdomain/zero/1.0/) applies to the data made available in this article, unless otherwise stated in a credit line to the data.
About this article
Cite this article
Shorr, A.F., Zilberberg, M.D., Micek, S.T. et al. Predictors of hospital mortality among septic ICU patients with Acinetobacter spp.bacteremia: a cohort study. BMC Infect Dis 14, 572 (2014). https://0-doi-org.brum.beds.ac.uk/10.1186/s12879-014-0572-6
Received:
Accepted:
Published:
DOI: https://0-doi-org.brum.beds.ac.uk/10.1186/s12879-014-0572-6