Left Ventricular Global Function Index: A Potential Predictor of Mortality and Major Adverse Cardiovascular Events in NSTEMI Patients

Mesut Karatas; Cengiz Sabanoglu; Kader Eliz Sahin; Ibrahim Halil Inanc

doi:10.20944/preprints202502.1224.v1

Submitted:

14 February 2025

Posted:

18 February 2025

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Abstract

Background and Objectives: The Left Ventricular Global Function Index (LVGFI) is a comprehensive marker of cardiac performance that integrates volumetric and functional parameters of the left ventricle. While its prognostic value in chronic cardiovascular diseases is well-documented, limited evidence exists for its utility in non-ST elevation myocardial infarction (NSTEMI). This study aimed to evaluate LVGFI as a predictor of three-year mortality and major adverse cardiovascular events (MACE) in NSTEMI patients. Methods: This retrospective cohort study included 432 NSTEMI patients divided into tertiles based on LVGFI values: T1 (low), T2 (intermediate), and T3 (high). LVGFI values were derived from echocardiographic imaging. Kaplan-Meier survival analysis was used to assess outcomes, and Cox proportional hazards models, adjusted for demographics and clinical covariates (age, sex, body mass index, and cardiovascular risk factors), determined the association between LVGFI tertiles and three-year outcomes. Results: The average age and sex distribution were similar across tertiles (T1: 70 years, T2: 67 years, T3: 68 years) with no significant differences in cardiovascular risk factors or most laboratory parameters, including glucose and hematological counts. However, significant differences were noted in Body Surface Area (higher in T3), platelet counts (higher in T1), and triglyceride levels (lower in T3). The ROC analysis identified an optimal LVGFI cut-off of 23.22 for predicting three-year mortality, with a sensitivity of 72% and specificity of 75% (AUC: 0.81; 95% CI: 0.74-0.87, p < 0.001). Patients in the lowest LVGFI tertile (T1) exhibited a three-year mortality rate of 25%, compared to 2.1% in the highest tertile (T3). After adjustment, the hazard ratio (HR) for mortality was significantly elevated in T1 (HR 11.86; 95% CI: 3.60-39.10) compared to T3. Similarly, MACE rates were highest in T1 (27.1%) and lowest in T3 (7.6%), underscoring LVGFI’s prognostic value beyond traditional parameters. Conclusion: LVGFI is a significant independent predictor of three-year mortality and MACE in NSTEMI patients. It offers a holistic assessment of cardiac function and may enhance clinical risk stratification models for managing high-risk patients. Further prospective studies are warranted to validate its broader clinical utility.

Keywords:

Left ventricular global function index

;

cardiac function

;

non-ST elevation myocardial infarction

;

three-year mortality

;

major adverse cardiovascular events

Subject:

Medicine and Pharmacology - Cardiac and Cardiovascular Systems

Introduction

Left ventricular dysfunction is a key determinant of prognosis in patients with non-ST elevation myocardial infarction (NSTEMI), a common and clinically significant form of acute coronary syndrome (ACS) [1]. Despite advances in treatment strategies, NSTEMI patients remain at high risk for long-term adverse cardiovascular events, including mortality and major adverse cardiovascular events (MACE) [2,3]. Effective risk stratification is essential for identifying high-risk individuals and tailoring management strategies to reduce morbidity and mortality. However, traditional risk markers, such as left ventricular ejection fraction (LVEF), while helpful, have limitations in the acute setting, as they may not fully capture the complexity of left ventricular (LV) performance, particularly in the early phases of myocardial injury [4]. Moreover, LVEF primarily reflects systolic function and may fail to detect subtle abnormalities in diastolic function or the progressive changes in ventricular remodeling that occur after NSTEMI [5].

The Left Ventricular Global Function Index (LVGFI) is a novel composite marker that integrates multiple dimensions of LV function, including both volumetric and functional parameters. By combining stroke volume, LV total volume, and myocardial mass, LVGFI offers a more holistic assessment of cardiac performance, potentially providing more accurate prognostic information than traditional indices [6]. Previous studies have demonstrated the value of LVGFI in healthy population, chronic cardiovascular diseases, including heart failure, hypertrophic cardiomyopathy, and chronic kidney disease, where it has shown superior predictive power for adverse outcomes compared to traditional measures like LVEF [6,7,8,9]. Despite these findings, the role of LVGFI in predicting outcomes in acute settings, particularly in NSTEMI, remains underexplored. Given the dynamic nature of myocardial stress and recovery in NSTEMI, a more comprehensive index like LVGFI may have unique advantages for identifying patients at higher risk for adverse events in the short and long term.

This study aims to evaluate the predictive value of LVGFI for three-year mortality and MACE in NSTEMI patients, hypothesizing that LVGFI offers superior prognostic information compared to traditional markers.

Materials and Methods

Ethical approval for this retrospective cohort study was obtained from ethics committee and the study was conducted in accordance with the principles outlined in the Declaration of Helsinki. The study included a total of 432 patients diagnosed with NSTEMI. Patients were categorized into three groups based on their LVGFI values: T1 (low), T2 (intermediate), and T3 (high), with each group consisting of 144 patients. Baseline demographic and clinical characteristics, including age, sex, body mass index (BMI), and comorbidities such as hypertension, diabetes mellitus, and smoking status, were recorded for all patients. Laboratory parameters including glucose levels, lipid profiles, hemoglobin, platelet count, and creatinine levels were also collected.

Patients eligible for inclusion in this study were those aged 18 years or older with a diagnosis of NSTEMI, confirmed by clinical presentation, elevated cardiac biomarkers (such as troponins or creatine kinase MB), electrocardiographic findings indicative of ischemia without ST-segment elevation, received standard care for NSTEMI, including medical management (e.g., antiplatelet therapy, anticoagulants, and statins) and invasive procedures (e.g., coronary angiography and percutaneous coronary intervention) were included, provided they had complete follow-up data over a three-year period to assess clinical outcomes such as mortality and MACE. MACE was defined as cardiovascular death, myocardial infarction, target vessel revascularization (TVR), and stroke during follow-up.

Exclusion criteria included patients with ST-elevation myocardial infarction (STEMI), as it involves different pathophysiology and prognosis. Additionally, those with significant structural heart conditions including severe valvular diseases, hypertrophic cardiomyopathy (HCM), restrictive cardiomyopathy, and dilated cardiomyopathy (DCM), or advanced heart failure (defined as NYHA Class III/IV symptoms with LVEF< 35% and persistant symptoms despite optimal medical therapy) were excluded, as these could confound the assessment of LV function. Patients with inadequate echocardiographic data due to poor image quality, as well as those who could not provide informed consent due to cognitive impairment or other factors, were also excluded. Other exclusions included patients with active inflammatory or infectious diseases, end-stage renal disease (ESRD) requiring dialysis, and those who were lost to follow-up or had insufficient follow-up data.

The LVGFI was estimated using a comprehensive echocardiographic protocol based on established guidelines, specifically the American Society of Echocardiography (ASE) recommendations for chamber quantification [10]. Transthoracic echocardiography was performed using advanced imaging techniques with a Philips EPIQ 7G ultrasound system and a high-frequency 1-5 MHz transducer. Measurements were obtained from parasternal long-axis, short-axis, and apical four-chamber views to ensure accuracy and reproducibility. To calculate LVGFI, left ventricular volumes were measured using the biplane method of discs (modified Simpson’s rule) from the apical four-chamber and two-chamber views. Left ventricular end-diastolic volume (LVEDV) and end-systolic volume (LVESV) were derived by tracing the endocardial border in both diastole and systole, with the papillary muscles excluded. Stroke volume (SV) was calculated as the difference between LVEDV and LVESV. LVEF was derived by dividing the stroke volume by LVEDV, providing a measure of systolic function. Left ventricular mass (LVM) was calculated using the ASE formula: LVM = 1.04 × [(LVEDD + PWT + IVS)^3 - LVEDD^3] - 13.6 g, where LVEDD is the left ventricular end-diastolic diameter, PWT is the posterior wall thickness, and IVS is the interventricular septal thickness. The left ventricular mass index (LVMI) was calculated by dividing LVM by body surface area (BSA) to normalize for individual size. The LVGFI was calculated by multiplying the LVEF, the ratio of SV to LVEDV, and the LVMI, and then dividing the result by 100.

2.1. Statistical Analysis

Descriptive statistics were used to summarize baseline characteristics, with continuous variables presented as mean ± standard deviation and categorical variables as percentages. Between-group comparisons were made using one-way analysis of variance (ANOVA) for continuous variables and chi-square tests for categorical variables. The primary outcome measures were three-year mortality and MACE, with differences between groups assessed using Kaplan-Meier survival curves and log-rank tests.

To evaluate the independent associations between LVGFI tertiles and clinical outcomes, Cox proportional hazards models were used. Model 1 was unadjusted, while Models 2, 3, and 4 adjusted for various covariates, including demographic characteristics (age, sex, BMI), clinical factors (systolic blood pressure, heart rate, previous coronary artery disease), and laboratory values (creatinine, hemoglobin, CRP, LDL). Hazard ratios (HR) with 95% confidence intervals (CI) were reported for mortality and MACE. A p-value of less than 0.05 was considered statistically significant.

Results

This study included a total of 432 NSTEMI patients with a mean age of 68 years, and 65% were male. There were no significant differences in key cardiovascular risk factors, including the prevalence of hypertension, diabetes mellitus, and smoking status. BSA was higher in T3 compared to T1 and T2 (p = 0.003). Platelet counts were highest in compared to T2 and T3 (p = 0.049). Triglyceride levels were lowest in T3 relative to T1 and T2 (p = 0.011). Other laboratory parameters, such as glucose, hemoglobin, and lipid profiles, were not significantly different between the groups (Table 1).

Table 2 highlights the hemodynamic and echocardiographic characteristics of patients across LVGFI tertiles. Systolic and diastolic blood pressures, as well as heart rate, were similar among the groups (p > 0.05). LVEF showed no significant differences between groups (p = 0.901). However, SV was significantly lower in T1 (p < 0.001). LVM and LVMI showed a decreasing trend from T1 to T3, with LVM highest in T1 and lowest in T3, and LVMI declining from T1 to T3 (both p < 0.001). Left ventricular end-diastolic diameter (LVEDD) and LVEDV were consistent across tertiles (p = 0.167 and p = 0.407, respectively), while LVESV was slightly higher in T1, nearing significance (p = 0.050).

Three-year clinical outcomes across the LVGFI tertiles (T1, T2, T3) were presented in Table 3. The mean follow-up duration was 35 months. The rates of TVR and recurrent myocardial infarction (RMI) were similar among the three tertiles, with TVR occurring in 3.5% of patients in both T1 and T2, and 4.2% in T3 (p = 0.937), while RMI rates were 6.3%, 3.5%, and 2.8%, respectively (p = 0.296). In contrast, significant differences were observed in the rates of MACE and mortality. MACE occurred in 27.1% of patients in T1, 14.6% in T2, and 7.6% in T3 (p < 0.001), while mortality were significantly more frequent in T1 (25.0%) compared to T2 (9.7%) and T3 (2.1%) (p < 0.001) (Figure 1).

Cox proportional hazards analysis for three-year mortality and MACE based on LVGFI tertiles was presented in Table 4. For three-year mortality, the unadjusted HR was highest in T1, with a HR of 14.45 (95% CI: 4.44–46.98) compared to T3. After adjusting for age, sex, BMI, systolic blood pressure, heart rate, and previous coronary artery disease (CAD), the HR remained significantly elevated in T1 (HR 11.86; 95% CI: 3.60–39.10), indicating a substantially higher risk of mortality. The risk of mortality in T2 was also significantly increased compared to T3, with HRs ranging from 4.86 (95% CI: 1.39–16.94) to 4.36 (95% CI: 1.23–15.47) across different models. For MACE, T1 also had the highest risk, with an unadjusted HR of 4.33 (95% CI: 2.21–8.48), and after adjustment for covariates, the HR remained elevated at 3.44 (95% CI: 1.71–6.90). The HR for MACE was significantly lower in T2, ranging from 2.02 (95% CI: 0.97–4.21) in the unadjusted model to 1.86 (95% CI: 0.87–4.01) after full adjustment, while T3 remained the reference group with the lowest event risk.

The ROC analysis also demonstrated that a LVGFI cut-off value of 23.22 predicted three-year mortality with a sensitivity of 72% and specificity of 75% (AUC: 0.81; 95% CI: 0.74-0.87; p < 0.001) (Figure 2).

Discussion

In this study, we investigated the prognostic value of the LVGFI in predicting 3-year mortality and MACE among patients diagnosed with NSTEMI. Our findings demonstrate that a lower LVGFI is significantly associated with higher mortality and MACE rates, underscoring its potential as a valuable prognostic tool in clinical practice.

In our study, the LVGFI was selected over traditional indices, such as LVEF and global longutidunal strain (GLS), as it provides a more comprehensive assessment of cardiac function. Unlike LVEF, which primarily evaluates systolic function, LVGFI integrates multiple dimensions of left ventricular performance, encompassing volumetric and functional parameters [11]. The advantages of LVGFI also extend to its sensitivity in detecting early or subclinical left ventricular dysfunction, which is often missed by traditional metrics [6]. In a study, Diaz-Navarro et al. [5] characterized three patients groups including acute myocarditis, takotsubo cardiomyopathy, and acute myocardial infarction and found that the LVGFI offered incremental value over traditional metrics LVEF and GLS. Our study corroborates this advantage, as the LVEF did not differ significantly across tertiles, whereas LVGFI demonstrated significant predictive value for mortality and MACE.

Our results align with and extend the findings of several studies that have explored the prognostic value of LVGFI in ACS patients. Reinstadler et al. [12] demonstrated that LVGFI was a strong predictor of adverse events in patients with STEMI. In their study of 226 STEMI patients, they found that LVGFI independently predicted and had better prognostic value than traditional parameters such as LVEF. Eitel et al. [13] conducted a larger study with 795 STEMI patients and found that the LVGFI was strongly associated with markers of significant myocardial and microvascular injury in STEMI, providing superior prognostic value compared to traditional cardiac risk factors, including LVEF. Similar to our study, Doganay et al. [14] evaluated the prognostic role of the LVGFI in predicting MACE in patients with acute coronary syndrome after 3-year follow-up. Decreased LVGFI levels were identified as independent predictors of MACE in both STEMI and NSTEMI groups.

LVGFI has demonstrated its utility in various clinical settings, extending beyond its application in acute coronary syndrome. Studies have explored its prognostic value in diverse patient populations, including those with chronic kidney disease (CKD), heart failure, hypertrophic cardiomyopathy (HCM), and amyloidosis [7,8,9,15,16]. For instance, Liu et al.[7] investigated the association between the LVGFI and clinical outcomes in patients with DCM. They found that lower LVGFI was linked to higher rates of death and heart failure events. Similarly, Schober et al. [16] revealed that in patients with implanted cardioverter-defibrillators (ICD) for secondary prevention, a reduced LVGFI was identified as an independent predictor of both mortality and rehospitalization. A prospective study including 158 patients with ESRD undergoing maintenance dialysis showed that a 10% decrease in LVGFI increased the risk of MACE by 114%, and the predictive model including LVGFI had significantly better performance in forecasting MACE compared to other cardiac parameters like native T1 mapping and GLS, with these findings remaining consistent even in patients with LVEF above the median [9]. Huang et al [15] also demonstrated that LVGFI had excellent diagnostic performance in differentiating cardiac amyloidosis from HCM. Interestingly, a multicenter prospective cohort study evaluated the predictive value of the LVGFI for cardiovascular events in 5004 healthy participants with a median follow-up of 7.2 years. The results showed that LVGFI was significantly associated with heart failure, hard cardiovascular events, and all cardiovascular events, with lower LVGFI values independently predicting higher risk for these outcomes, highlighting its potential as a powerful prognostic tool in a multiethnic population without prior cardiovascular disease [6].

The primary distinction of our study lies in its focus on the prognostic value of LVGFI specifically within an acute NSTEMI patient population, whereas much of the existing literature has primarily explored LVGFI in more chronic or stable cardiovascular conditions. While LVGFI's ability to capture subtle left ventricular dysfunction in these chronic settings is well-established, the pathophysiological dynamics in acute NSTEMI patients, characterized by rapid and significant myocardial stress, require distinct prognostic approaches. Our study contributes to the current literature by demonstrating LVGFI's predictive value in an acute myocardial infarction context, thus broadening its clinical applicability. Notably, our findings highlight LVGFI's strong association with three-year mortality and MACE, complementing and extending previous research, and reinforcing its potential as a versatile prognostic tool across diverse cardiovascular conditions.

Despite these promising results, our study has limitations. First of all, the retrospective design and single-center setting may limit the generalizability of our findings. Second, we utilized echocardiographic measurements for LVGFI, which may have a lower degree of accuracy compared to MRI. However, this choice was deliberate, as LVGFI has the potential to be assessed using echocardiography, a more readily accessible imaging modality in the acute phase of NSTEMI. Third, while we adjusted for several confounders, the possibility of residual confounding cannot be entirely excluded. Multi-center, prospective studies would be valuable in confirming and extending our results.

Conclusion

Our findings suggest that LVGFI is an independent predictor of three-year mortality and MACE in patients with NSTEMI, supporting its potential integration into clinical risk stratification models. Unlike traditional markers, LVGFI provides a holistic assessment of ventricular function, making it a valuable tool for identifying high-risk patients and guiding post-NSTEMI management. Future prospective studies are warranted to validate LVGFI’s clinical utility across diverse populations and to optimize its application in acute care settings.

Author Contributions

Conceptualization, I.I, M.K.; Methodology, I.I, M.K, K.E.S.; Software, M.K.; Validation, , I.I, M.K, C.S.; Formal Analysis, K.E.S, M.K, K.E.S.; Investigation, C.S, I.I, M.K.; Resources, M.K, I.I, C.S.; Data Curation, K.E.S, M.K.; Writing – Original Draft Preparation, I.I, M.K, C.S.; Writing – Review & Editing, I.I, K.E.S, M.K, C.S.; Visualization, M.K, C.S.; Supervision, I.I.; Project Administration, M.K.; Funding Acquisition, I.I, M.K, C.S, K.E.S.

Funding

None.

Ethics approval

Approved by ethics committee (Date: 22.01.2025, Decision number: MSTH/20859).

Informed Consent

Informed written consent was obtained from all participants.

Availability of Data and Material

The datasets generated during and/or analyzed during the current study are available from the corresponding author upon reasonable request.

Conflict of Interests

The authors declare that they have no conflict of interests.

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Figure 1. Kaplan-Meier survival analysis of three-year mortality across LVGFI tertiles.

Figure 2. ROC analysis of LVGFI for predicting three-year mortality.

Table 1. Demographic, clinical, and laboratory characteristics of patients across LVGFI tertiles.

Characteristics	T1 (n=144)	T2 (n=144)	T3 (n=144)	p value
Age (mean±SD)	70 ± 12	67 ± 12	68 ± 13	0.238
Biological sex, male (n,%)	94 (65.3)	94 (65.3)	91 (63.2)	0.913
BMI (mean±SD)	27.8 ± 3.9	27.5 ± 4.2	28.4 ± 3.9	0.121
BSA (mean±SD)	1.78 ± 0.2	1.80 ± 0.2	1.86 ± 0.21	0.003
Hypertension (n,%)	83 (57.6)	85 (59.0)	80 (55.6)	0.835
Diabetes mellitus (n,%)	52 (36.1)	42 (29.2)	42 (29.2)	0.342
Smoking (n,%)	22 (15.3)	23 (16)	20 (13.9)	0.881
Previous CAD (n,%)	21 (14.6)	26 (18.1)	29 (20.1)	0.457
Laboratory parameters
Glucose, mg/dL (mean±SD)	124 ± 44	117 ± 38	119 ± 46	0.407
Hemoglobin, g/dL (mean±SD)	13.6 ± 2	13.8 ± 2	13.9 ± 2	0.483
White blood cell count, cells/µL (mean±SD)	9.1 ± 3	9.2 ± 3	9.8 ± 3	0.085
Platelet count, cells/µL (median,percentile)	226 (190 - 269)	215 (181 - 256)	209 (172 - 263)	0.049
Lymphocyte count, cells/µL (mean±SD)	2.3 ± 1	2.3 ±	2.5 ±	0.402
Neutrophil count, cells/µL (mean±SD)	6.5 ± 2	5.9 ± 2	6.0 ± 2	0.063
Creatinine, mg/dL (mean±SD)	0.98 ± 0.3	0.96 ± 0.3	0.97 ± 0.3	0.737
HDL (mean±SD)	41.1 ± 11	46.2 ± 16	45.1 ± 15	0.166
LDL (mean±SD)	118.4 ± 39	116.2 ± 35	116.4 ± 41	0.865
Trigliserid (median,percentile)	132 (99 - 176)	133 (85 - 186)	111 (81 - 154)	0.011
CRP (mean±SD)	4.2 (1.9 – 11.0)	4.2 (1.9 – 10.2)	5.5 (2.4 – 13.0)	0.215

*Abbreaviations: BMI:Body mass index, BSA:Body surface area, CAD:Coronary artery disease, CRP:C-reactive protein.

Table 2. Hemodynamic and echocardiographic characteristics of patients across LVGFI tertiles.

Parameter (mean±SD)	T1 (n=144)	T2 (n=144)	T3 (n=144)	p value
Systolic blood pressure, mmhg	131.7 ± 21.2	131.4 ± 21.4	129.4 ± 20.1	0.586
Diastolic blood pressure, mmhg	81.7 ± 15.7	81.4 ± 15.7	80.3 ± 16.4	0.747
Heart rate	74.3 ± 8.5	74.4 ± 8.3	73.3 ± 9.0	0.505
LVEF	54.53 ± 10.89	54.36 ± 11.04	53.95 ± 11.27	0.901
LVEDD	46.5 ± 4.62	47.44 ± 4.40	46.70 ± 4.34	0.167
LVEDV	86.66 ± 16.03	84.37 ± 13.76	85.87 ± 14.35	0.407
LVESV	45.51 ± 9.98	42.98 ± 10.42	45.65 ± 10.77	0.050
SV	57.43 ± 7.89	62.60 ± 7.67	65.17 ± 10.14	<0.001
LVM	216.22 ± 37.01	185.11 ± 39.79	176.13 ± 42.64	<0.001
LVMI	123.41 ± 26.92	103.59 ± 24.67	95.59 ± 24.64	<0.001

*Abbreaviations: LVEDD: Left ventricular end-diastolic diameter, LVEDV: Left ventricular end-diastolic volume, LVEF: Left ventricular ejection fraction, LVESV: Left ventricular end-systolic volume, LVM: Left ventricular mass, LVMI: Left ventricular mass index, SV: Stroke volume.

Table 3. Three-year clinical outcomes of patients across the LVGFI tertiles.

	T1 (n=144)	T2 (n=144)	T3 (n=144)	p value
TVR	5 (3.5)	5 (3.5)	6 (4.2)	0.937
RMI	9 (6.3)	5 (3.5)	4 (2.8)	0.296
Mortality	36 (25.0)	14 (9.7)	3 (2.1)	<0.001
MACE	39 (27.1)	21 (14.6)	11 (7.6)	<0.001

*Abbreaviations: MACE: Major adverse cardiovascular events, RMI:Recurrent myocardial infarction, TVR:Target vessel revascularization.

Table 4. Cox proportional analysis for 3-year mortality and 3-year MACE by LVGFI tertiles.

	T1 (n=144)	T2 (n=144)	T3 (n=144)
3-year mortality Number of deaths	36	14	3
Mortality, %	25	9.7	2.1
Mortality, HR (%95 CI) Model 1: unadjusted	14.45 (4.44 – 46.98)	4.86 (1.39 – 16.94)	1[Reference]
Model 2: adjusted for age, sex and BMI	14.18 (4.35 – 46.17)	4.85 (1.39 – 16.90)	1[Reference]
Model 3: adjusted for SBP, heart rate, previous CAD	13.28 (4.08 – 43.26)	4.66 (1.33 – 16.27)	1[Reference]
Model 4: adjusted for all covariates^a	11.86 (3.60 – 39.10)	4.36 (1.23 – 15.47)	1[Reference]
3-year MACE Number of events	39	21	11
Events, %	27.1	14.6	7.6
Event, HR (%95 CI) Model 1: unadjusted	4.33 (2.21 – 8.48)	2.02 (0.97 – 4.21)	1[Reference]
Model 2: adjusted for age, sex and BMI	4.27 (2.18 – 8.35)	2.00 (0.96 – 4.15)	1[Reference]
Model 3: adjusted for SBP, heart rate, previous CAD	4.04 (2.06 – 7.92)	1.94 (0.93 – 4.03)	1[Reference]
Model 4: adjusted for all covariates^a	3.44 (1.71 – 6.90)	1.86 (0.87 – 4.01)	1[Reference]
Abbreviations: SBP, systolic blood pressure; BMI, body mass index; CAD, coronary artery disease; HR, hazard ratio. ^aIncludes demographics (age, gender and BMI); first measurement during hospitalization of the following laboratory values (creatinine, hemoglobin, CRP, LDL) and comorbidities (hypertension, diabetes mellitus, smoking, previous CAD, systolic blood pressure, heart rate)

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