Effect of angiotensin converting enzyme inhibitor and angiotensin II receptor blocker on the patients with sepsis
Article information
Abstract
Background/Aims
Inhibitors of the renin-angiotensin system, angiotensin-converting enzyme (ACE) inhibitors and angiotensin II receptor blockers (ARBs), reportedly have anti-inflammatory effects. This study assessed the association of prior use of ACE inhibitors and ARBs with sepsis-related clinical outcomes.
Methods
A population-based observational study was conducted using the Health Insurance Review and Assessment Service claims data. Among the adult patients hospitalized with new onset of sepsis in 2012, patients who took ARBs or ACE inhibitors at least 30 days prior to hospitalization were analyzed. Generalized linear models and logistic regression were used to examine the relation between the prior use of medication and clinical outcomes, such as in-hospital mortality, mechanical ventilation, and length of stay.
Results
Of a total of 27,628 patients who were hospitalized for sepsis, the ACE inhibitor, ARB, and non-user groups included 1,214 (4.4%), 3,951 (14.4%), and 22,463 (82.1%) patients, respectively. As the patients in the ACE inhibitor and ARB groups had several comorbid conditions, higher rates of intensive care unit admission, hemodialysis, and mechanical ventilation were observed. However, after covariate adjustment, the use of ACE inhibitor (odds ratio [OR], 0.752; 95% confidence interval [CI], 0.661 to 0.855) or ARB (OR, 0.575; 95% CI, 0.532 to 0.621) was significantly associated with a lower rate of in-hospital mortality.
Conclusions
Pre-hospitalization use of ACE inhibitors or ARBs for sepsis was an independent factor for a lower rate of in-hospital mortality.
INTRODUCTION
The renin-angiotensin system (RAS) is a complex endocrine system with a multi-dimensional enzymatic cascade to keep arterial blood pressure constant, which in turn helps maintain tissue perfusion and extracellular volume [1]. The RAS is known to be physiologically activated in rodents [1] and humans [2] during sepsis. Deficiency in the expression of angiotensin-converting enzyme (ACE) and angiotensin II is associated with high mortality rates in patients with severe sepsis [3]. Experimental studies have demonstrated the effectiveness of angiotensin II in restoring blood pressure and cardiac output in sheep [4] and pigs [5] during septic shock. In a recent randomized controlled trial for patients with vasodilatory shock, of which approximately 80% cases were due to sepsis, administration of angiotensin II elevated blood pressure in patients resistant to conventional catecholamines as well as permitted dose reduction of other vasopressors [6].
Although RAS activation is a physiological reaction counteracting septic shock, excessive activation may further aggravate pro-inflammatory responses and vascular dysfunction, resulting in worse clinical outcomes. In particular, a high degree of RAS activation was associated with micro-vascular dysfunction and organ failure in patients with sepsis [2]. Conversely, inactivation of RAS showed protective effects on acute pulmonary or renal injury [7,8] and decreased endotoxin-induced oxidative stress and endothelial dysfunction [9]. In animal models, the inhibition of angiotensin II improved mortality due to sepsis [10]. Accordingly, chronic suppression of RAS prior to an event of sepsis may be beneficial for clinical outcomes. In fact, one human observational study reported that the 30-day mortality rate due to sepsis was reduced in elderly male patients who ever received angiotensin II receptor blockers (ARBs) [11]. However, there is a lack of evidence evaluating the relationship between RAS suppression prior to an event of sepsis, and clinical prognoses.
ACE inhibitors or ARBs have been used to suppress RAS in patients with hypertension [12], cardiovascular diseases [13], and renal diseases [14]. ACE inhibitors interrupt ACE which catalyzes cleavage of angiotensin I to angiotensin II, while ARBs inhibit angiotensin II from binding to the angiotensin II receptor type I. There have been several studies to evaluate whether ACE inhibitors or ARBs can be beneficial in sepsis, but contradictory results have been reported [15-18].
The present study was conducted to determine the impact of prior RAS inhibition on the clinical prognosis during sepsis. The purpose of this study was to elucidate the effects of prior ACE inhibitor or ARB use on the in-hospital mortality rate in patients who were diagnosed with new onset of sepsis.
METHODS
Study design, setting, and data sources
We referred to The Strengthening the Reporting of Observational Studies in Epidemiology (STROBE) statement to report the results of our study [19]. A retrospective, population-based cohort study was conducted using the Health Insurance Review and Assessment Service (HIRA) annual claims data of the total population in South Korea from 2009 to 2013. The HIRA database consists of six domains: (1) general information, (2) healthcare services, (3) diagnosis, (4) outpatient prescription, (5) drug master, and (6) providers information. Detailed information concerning HIRA data was published previously [20]. Sepsis patients who were hospitalized in a tertiary care center or general hospital in 2012 were identified using the International Classification of Diseases 10th Revision (ICD-10) codes (A40 and A41). Considering that the definition of sepsis was revised in 2003 [21] and 2016 [22], the most recent delineation was applied to all patients in this study. No major epidemiological event or considerable change to nationwide policies was reported during this study period.
Participants
We identified all patients aged ≥ 18 years who experienced a new event of sepsis from January 01, 2012 to December 31, 2012. Patients with recent use of ACE inhibitors or ARBs before a new event of sepsis were operationally defined as the ACE inhibitor or ARB groups, respectively. Patients who did not use ACE inhibitors or ARBs were operationally defined as the non-user group. Recent use of ACE inhibitors or ARBs was defined as a prescription given at least 30 days or more prior to the onset of sepsis. Medications used by the ACE inhibitor group included alacepril, captopril, cilazapril, enalapril, fosinopril, imidapril, lisinopril, moexipril, perindopril, ramipril, and temocapril. Medications used by the ARB group included candesartan, eprosartan, fimasartan, irbesartan, losartan, olmesartan, telmisartan, and valsartan.
Measurement of variables
We evaluated demographic characteristics such as age and sex, baseline comorbidities, Charlson comorbidity index (CCI), and current medications of hospitalized sepsis patients. Baseline comorbidities included hypertension, diabetes mellitus, cerebrovascular disorder (CVD), chronic obstructive pulmonary disorder (COPD), congestive heart failure (CHF), coronary artery disease (CAD), liver cirrhosis, chronic kidney disease (CKD), pulmonary tuberculosis, and malignancy. Comorbidities were identified by reviewing the diagnosis code (ICD-10 code) up to 3 years before sepsis occurrence. Current medications other than ACE inhibitors and ARBs used within 30 days prior to the onset of sepsis, such as statins and beta-blockers, were identified. Clinical outcomes included the following events: intensive care unit (ICU) admission, mechanical ventilation, acute renal failure with hemodialysis, duration of mechanical ventilation, in-hospital mortality, hospital length of stay (LOS), and re-admission for sepsis. The event of re-admission for sepsis was followed-up until 31st December 2013. If a patient had multiple admissions to ICUs during the study period, the first episode was regarded as the major event.
Assessment of outcomes
The primary objective of our study was to evaluate the impact of current use of ACE inhibitors or ARBs on the incidence of in-hospital mortality in patients with sepsis.
Statistical methods
For comparisons among the ACE inhibitor, ARB, and non-user groups, categorical variables were analyzed using Pearson’s chi-square test and presented as a percentage. Continuous variables were evaluated using analysis of variance with post hoc analysis and presented as mean ± standard deviation. Univariate and multivariate logistic regression analyses were conducted to elucidate whether recent medication with ACE inhibitors or ARBs was associated with in-hospital mortality.
Ethics
The Institutional Review Board Committee of Seoul National University Hospital approved the present study and waived the need for informed consent for access to the HIRA data (IRB No. E-1607-004-771).
RESULTS
Demographic characteristics of the study population
A new episode of sepsis occurred in 27,365 patients in 2012. Among them, 1,207 (4.4%) were in the ACE inhibitor group, 3,951 (14.4%) were in the ARB group, and 22,463 (82.1%) were in the non-user group (Fig. 1). The three most commonly used drugs in the ACE inhibitor group were perindopril (34.0%), ramipril (33.1%), and captopril (19.7%). The three most commonly used drugs in the ARB group were losartan (25.5%), valsartan (19.0%), and candesartan (15.0%). The ACE inhibitor or ARB groups had a higher proportion of elderly and female patients than in the non-user group (Table 1). More patients in the ACE inhibitor or ARB group had a higher CCI than those in the non-user group. In terms of underlying conditions, more patients in the ACE inhibitor or ARB group had hypertension, diabetes mellitus, CVD, CAD, CHF, COPD, and CKD than those in the non-user group. Conversely, more patients with liver cirrhosis and malignancy were found in the non-user group. In the evaluation of current medications, a higher proportion of patients who used concurrent statins or beta-blockers was observed in the ACE inhibitor group than that in the ARB or non-user group.
In the post hoc analysis, age and sex were similar between the ACE inhibitor and ARB group (Table 2). Patients in the ARB group were more likely to have CCI > 8 than those in the ACE inhibitor or non-user group. The ACE inhibitor group showed a higher proportion of patients with cardiac disorders such as CHF and CAD than the ARB group. The ARB group showed a higher proportion of patients with disorders related to peripheral vascular disorder such as diabetes mellitus, CVD, and CKD than the ACE inhibitor group. In addition, more patients in the ACE inhibitor group had COPD, while more patients in the ARB group had malignancy.
Comparison of clinical outcomes according to ACE inhibitor, ARB, and non-user groups
We found significant differences in clinical outcomes among the ACE inhibitor, ARB, and non-user groups (Table 3). A higher ICU admission rate was found in the ACE inhibitor (57.3%) group in comparison to that in the ARB (42.7%) and non-user (36.1%) groups (p < 0.0001, both) (Table 4). Further, the ICU admission rate was higher in the ARB group than the non-user group (p < 0.0001). Hemodialysis was more frequently conducted in the ARB group (8.5%) than in the ACE inhibitor (5.5%) or non-user groups (3.1%) (p = 0.0010 and p < 0.0001, respectively) and more frequently in the ACE inhibitor group than in the non-user group (p < 0.0001). A greater number of patients were likely to have mechanical ventilation in the ACE inhibitor (46.1%) group than in the ARB (38.4%) or non-user (34.5%) groups (p < 0.0001, both). Furthermore, more mechanical ventilation was performed for the ARB group than for the non-user group (p < 0.0001). The ACE inhibitor group (3.0 days) showed a significantly shorter duration of mechanical ventilation than ARB group (3.6 days) or non-user group (3.7 days) (p < 0.0001, both). Hospital LOS was found to be about 17 days longer in the ACE inhibitor (41.9 days) and ARB (42.1 days) groups compared to that in the non-user group (25.0 days) (p < 0.0001, both). During hospitalization, 29.7% patients in the ARB group, 33.4% in the ACE inhibitor group, and 41.7% in the non-user group died. More deaths than ICU admissions were identified in the non-user group, while more ICU admissions than deaths were identified in the ACE inhibitor and ARB groups. The ARB group showed a significantly lower mortality rate than the ACE inhibitor group (p = 0.0153). The ICU re-admission rate due to sepsis was twice as high in the ACE inhibitor (1.08%) and ARB (1.04%) groups than in the non-user group (p < 0.0001, both). No difference in ICU re-admission rates was found between the ACE inhibitor and ARB groups.
In the univariate regression analysis to evaluate the risk factors for in-hospital mortality, age, sex, CCI, comorbidities including: hypertension, diabetes mellitus, CVD, COPD, CHF, CAD, liver cirrhosis, CKD, pulmonary tuberculosis, and malignancy, ICU admission, hemodialysis, use of ACE inhibitor, use of ARB, use of statin, and use of beta-blocker were significantly related to in-hospital mortality (Table 3). After multivariable adjustment, the use of ACE inhibitor before sepsis (odds ratio [OR], 0.752; 95% confidence interval [CI], 0.661 to 0.855) and ARB before sepsis (OR, 0.575; 95% CI, 0.532 to 0.621) were significantly correlated to a lower mortality rate (p < 0.001, both) (Table 5).
DISCUSSION
Our study showed that ACE inhibitor or ARB group were more likely to be elderly and have a higher number of comorbidities. Among them, CCI was higher in the ARB group. The ACE inhibitor group was associated with a greater number of underlying cardiac disorders, while the ARB group included diseases related to other vascular disorders such as cerebrovascular disease or CKD. The result that statin and beta-blockers were more often prescribed for ACE inhibitor or ARB groups also implies more underlying comorbidities in these population. Therefore, it is understandable that ICU admission, mechanical ventilation, and hemodialysis more frequently occurred in the ACE inhibitor or the ARB group. The rates of ICU admission and mechanical ventilation were the highest in the ACE inhibitor group, while the hemodialysis rate was the highest in the ARB group. The ACE inhibitor and ARB groups survived more and longer in hospital compared to non-user group. A higher mortality rate than ICU admission rate was found in the non-user group, while a higher ICU admission rate than mortality rate was found in the ACE inhibitor and ARB groups. In-hospital mortality was significantly lower in the ARB group than in the ACE inhibitor or non-user groups. Re-admission to the ICU for sepsis was more likely to occur in the ACE inhibitor and ARB groups.
Balancing RAS activation is an important consideration for cases of sepsis. In a study by Imai et al. [7] in 2005, the protective effects of ACE-2 on lung injury was demonstrated in ACE-deficient mice. Extremely low levels of RAS expression was associated with a poor prognosis in severe sepsis [3]. In a recent clinical study, infusion of angiotensin II in septic shock patients reduced the total use of vasopressors [6]. Conversely, endotoxin-induced lung injury and inflammatory response were reduced after ACE-2 inhibition in a rat model [23]. Micro-vascular dysfunction deteriorated after RAS activation during severe sepsis [2]. An observational study showed that the use of vasopressors for septic shock decreased in patients with chronic inhibition of RAS [24]. It is well known that sepsis abruptly elevates the level of RAS expression, which induces oxidative stress, vascular permeability, pro-inflammatory cytokine production, and pro-coagulant effects [25,26]. Although it would be best to modulate RAS according to the severity of sepsis or the presence of shock, to date, there is no clear guideline for implementation. Based on our results, there may be more sepsis patients in whom prevention of excessive RAS activation would lead to a beneficial outcome.
The benefit of ACE inhibitors on sepsis-related clinical outcomes has been previously demonstrated. In previous systematic reviews and meta-analyses, ACE inhibitors were shown to reduce total and cardiovascular deaths in hypertensive patients [27] as well as the incidence of pneumonia and pneumonia-related mortality [28]. This reduction in mortality is largely explained by an immunomodulatory effect, which lowers inflammatory cytokines in patients with chronic heart or kidney failure [29-31]. In an experimental study, enalapril reduced systemic inflammatory response and lung injury in endotoxin-induced sepsis [32]. Our results are consistent with those of previous studies.
The immunomodulatory effect of ARB on sepsis-related outcomes has also been previously studied. Lower levels of systemic or vascular inflammation were found in patients who took ARBs [33,34]. Although previous experimental studies have revealed the relationship between angiotensin II and inflammatory processes [35], the immunomodulatory effect on patients with sepsis after blocking angiotensin II receptor is unclear. In interventional studies with rat models, losartan partially helped ameliorate circulation dysfunction and/or improve lung injury in septic shock [36,37]. However, only observational studies have been conducted on humans in this regard. In a population with hypertension, longterm use of ARBs showed beneficial effects in terms of the incidence of sepsis requiring hospitalization and sepsis-related outcomes [38]. Lower 30-day mortality rates were reported in elderly male patients with sepsis, who were previously prescribed with ARBs or statins [11]. A recent cohort study showed better survival outcomes in the hypertensive patients who took an anti-hypertensive drug including ACE inhibitor and ARB [39]. In this study, the adjusted analysis showed that the ARB group had a significantly lower in-hospital mortality OR than the ACE inhibitor or non-user groups.
There has been a safety concern that ACE inhibitors or ARBs could further increase the incidence of acute kidney injury (AKI) among septic shock patients [16]. It is not a novel theory that RAS inhibition can increase AKI in critically ill patients [40]. ACE inhibitors and ARBs reduce efferent arteriolar resistance and promote renal hypoperfusion, leading to AKI [41]. Conversely, injecting angiotensin II may help reduce AKI with renal replacement therapy [42]. Therefore, ACE inhibitors or ARBs administration is usually stopped if a septic kidney is suspected, as AKI is more likely to occur in certain cases such as those with low blood pressure and intravascular hypovolemia. In our study, more events of hemodialysis due to AKI were noted in the ACE inhibitor and ARB groups. If RAS is suppressed in patients with sepsis, renal perfusion may not be enough even after hemodynamic stability is achieved.
Several well-designed cohort studies have been recently published [39,43], but this study has some important differences. First, in this study, the method of diagnosis and treatment of sepsis were relatively uniform because we included patients over a relatively short-time period. Kim et al. [39] compared the mortality rates due to sepsis among various medications for hypertension from 2003 to 2013. The strength of the study by Kim et al. [39] is the relatively homogeneous population of hypertensive patients with long-term follow-up. In contrast, the strength of this study is the relatively homogeneous diagnostic and treatment modality because all the sepsis events were diagnosed in 2012. Second, this study extended the inclusion criteria from hypertensive patients to patients who used hypertensive medications. Hypertension was only diagnosed in approximately 30% patients who used ACE inhibitors or ARBs, while other patients used these medications for other indications. Therefore, the study population of patients with hypertension may insufficient to evaluate the effects of ACE inhibitors or ARBs on sepsis. Third, we believe that our definition of drug use was more accurate. Hsieh et al. [43] defined a patient as a user of a certain drug if the patient took that drug for > 1 week within 3 months. Approximately 85% of all patients with sepsis were classified into the antihypertensive drug user group, and this rate was adjusted by matching the number of patients in the non-user group to the user group. Since this study only included patients who had been taking medication for at least 1 month before sepsis, the effect of taking the medication would be clearer.
Several limitations were identified in the current study. First, the present retrospective cohort study has a limitation in that clinical information was not available in the claims data. For example, the results of laboratory tests at admission or pathogen identification tests were not available. Therefore, discrepancy between actual sepsis and the disease code in the database cannot be excluded. Furthermore, clinical severity was not adjusted to evaluate clinical outcomes in this study. We could not fully explain why the ACE inhibitor or ARB groups showed better survival rates, even though these groups had more comorbidities, ICU admissions, hemodialysis treatments, and instances of mechanical ventilation. Further multicenter studies are needed to evaluate the positive effects of ACE inhibitors and ARBs on mortality rates under various clinical conditions. Second, the mechanism underlying the effect of RAS suppression on the clinical course according to the severity of sepsis cannot be evaluated at this stage. Furthermore, since the effect of ACE inhibitors and ARBs on sepsis is presumed to be based on an immunomodulatory function, further analysis with various inflammatory markers is necessary. Third, the prior-exposure period of ACE inhibitors or ARBs was not the same in the study population, although we set a minimum period of 30 days. However, no previously published studies exist reporting time-dependent immunomodulatory effects of these drugs. Fourth, survival analysis could not be conducted because long-term hospitalizations occurred even after sepsis events were found. In addition, an adjusted regression analysis with the Cox proportional hazards model was not used in this study because the hazard ratios of death among the three groups were not constant over time. Fifth, the health-related activities of patients could be different depending on the patients’ socioeconomic or educational status. Patients taking ACE inhibitors and ARBs are more likely to be interested in personal healthcare.
In conclusion, members of the population who were recently prescribed ACE inhibitors and ARBs at least 30 days prior to hospitalization for a new onset of sepsis had a lower rate of in-hospital mortality, although they had more comorbidities and higher rates of ICU admission, mechanical ventilation, and hemodialysis. Further clinical studies are required to determine which population segments can benefit from RAS inhibition during the early phase of sepsis.
KEY MESSAGE
1. More events of intensive care unit admission, hemodialysis, and mechanical ventilation were observed in the patients of angiotensin-converting enzyme (ACE) inhibitor and angiotensin II receptor blocker (ARB) groups who were older and had more comorbidities than those of non-user group.
2. However, the patients who used ACE inhibitor and ARB prior to hospitalization for a new onset of sepsis survived more and longer in hospital compared to non-user group.
Notes
No potential conflict of interest relevant to this article was reported.