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1661
Vol. 76.
(enero 2020)
ORIGINAL ARTICLE
Open Access
Changes in the neutrophil-to-lymphocyte and platelet-to-lymphocyte ratios before and after percutaneous coronary intervention and their impact on the prognosis of patients with acute coronary syndrome
Visitas
1661
Jianlong ShengI,
Autor para correspondencia
shengjianlong1982@163.com

Corresponding author.
, Nina LiuII, Fei HeI, Cheng ChengI, Shichun ShenI, Yuting SunI
I Department of Cardiology, The Second Affiliated Hospital of Anhui Medical University, Hefei, 230601, PR China.
II Department of Endocrinology, The Second Affiliated Hospital of Anhui Medical University, Hefei, 230601, PR China.
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OBJECTIVES:

This study aimed to prospectively observe the changes in the neutrophil-to-lymphocyte ratio (NLR) and platelet-to-lymphocyte ratio (PLR) before and after percutaneous coronary intervention (PCI) and their impact on the prognosis of patients with acute coronary syndrome (ACS).

METHODS:

Blood samples from 205 patients with ACS were collected at admission and at 24h and 30 days post-PCI to observe changes in the complete blood count. The Cox multivariate regression model was used to analyze the factors influencing major adverse cardiac events (MACE) after PCI in patients with ACS. A receiver operating characteristic (ROC) curve was used to evaluate the predictive value of inflammation indicators for MACE after PCI.

RESULTS:

Following PCI, NLR and PLR first increased postoperatively and then decreased within 30 days after PCI. Cox multivariate regression analysis showed that NLR and PLR at 24h post-PCI and acute ST-segment elevation myocardial infarction were independent influencing factors for the incidence of MACE after PCI. The ROC curve analysis showed that the NLR at 24h post-PCI was a better predictor of the incidence of MACE. The NLR at 24h post-PCI was significantly correlated with the number and length of implanted stents and operation duration.

CONCLUSIONS:

After PCI, patients with ACS had an increased neutrophil proportion and NLR. The NLR at 24h post-PCI was a better predictor of the incidence of postoperative MACE.

KEYWORDS:
Neutrophil-to-Lymphocyte Ratio
Platelet-to-Lymphocyte Ratio
Percutaneous Coronary Intervention
Acute Coronary Syndrome
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INTRODUCTION

Acute coronary syndrome (ACS) is a critical cardiovascular disease that can cause heart failure and arrhythmia and has a high mortality rate. Percutaneous coronary intervention (PCI) improves the prognosis of patients with ACS (1). However, among patients with ACS who receive PCI, some exhibit postoperative coronary revascularization, heart failure, cardiovascular death, and other adverse events (2,3). Inflammation plays an important role in the incidence of adverse events after PCI (4).

Previous studies have shown that the levels of inflammatory cytokines at admission are related to poor prognosis in patients with ACS (5-8). However, the results of other studies do not support this conclusion (9,10) because PCI further induces or promotes the inflammatory response (11,12). Elevated vascular inflammation may increase the risk of coronary thrombosis, restenosis in stents, unstable coronary plaque, and myocardial remodeling, thus influencing some of the postoperative benefits of PCI (13).

Theoretically, the level of inflammation after PCI may be strongly related to the prognosis after PCI. However, there are few studies regarding the impact of the levels of post-PCI inflammatory indicators on the prognosis of patients with ACS (14,15). In addition, dynamic changes in inflammatory indicators before and after PCI have rarely been reported (15,16). The neutrophil-to-lymphocyte ratio (NLR) and platelet-to-lymphocyte ratio (PLR) have been increasingly and extensively applied as inflammatory indicators in inflammation-related disease research because they are easy to use and are obtained using inexpensive tests (9,13–18). We conducted a prospective study to systematically observe the changing trends of NLR and PLR before and after PCI in patients with ACS and determine whether NLR and PLR affect the prognosis of patients undergoing PCI.

MATERIALS AND METHODSResearch patients

The ethical approval for this study was granted by the Ethics Committee of the Second Affiliated Hospital of the Anhui Medical University (PJ-YX2018-002). Each patient and/or his/her family provided written informed consent for participation in the study.

This study included 205 patients with ACS who underwent PCI at the Department of Cardiology of the Second Affiliated Hospital of Anhui Medical University (Anhui Province, China) between July 2018 and September 2019. The diagnostic criteria for ACS were in accordance with established guidelines (1,19). The exclusion criteria were as follows: 1) failure to follow the study protocol and complete the follow-up; 2) patients designated as having class IV heart failure according to the New York Heart Association classification before and during hospitalization, 3) patients with complications of severe infection, mixed connective tissue disease, or malignant tumors, or 4) patients receiving glucocorticoid therapy.

Research methodsACS patient grouping and PCI

In this study, patients were divided into three groups according to the ACS subtype: 1) unstable angina pectoris (UA), 2) acute non-ST-segment elevation myocardial infarction (non-STEMI), and 3) acute ST-segment elevation myocardial infarction (STEMI). Surgical indicators and PCI procedures were performed in accordance with the relevant PCI guidelines (20). The SYNTAX scores of patients with coronary lesions were calculated based on the coronary angiography results (21). PCI-related parameters, such as the number of treated coronary arteries, number of implanted stents, lengths of implanted stents, maximum pressure of balloon dilation during PCI, and operation duration, were recorded for each patient.

Whole blood count and NLR and PLR calculations

Peripheral venous blood samples were collected from each patient at admission, before PCI and at 24h and 30 days after PCI. All tests were performed in the laboratory of the Second Affiliated Hospital of Anhui Medical University. The complete blood count was performed using an XE-2100 automatic blood cell analyzer and matching reagents (Sysmex Corporation, Kobe, Japan). NLR was defined as the ratio of the neutrophil count to the lymphocyte count, and PLR was calculated as the ratio of the platelet count to the lymphocyte count.

Detection of high-sensitivity C-reactive protein and interleukin-6 after PCI

A peripheral venous blood sample was collected from each patient 24h post-PCI. High-sensitivity C-reactive protein (hsCRP) and interleukin 6 (IL-6) were detected using an AU5800 biochemical analyzer (Beckman Coulter Inc., Brea, CA, USA) and a Cobas601 biochemical analyzer (Roche Diagnostics, Indianapolis-Marion County, IN, USA), respectively.

MACE during follow-up

The patients were followed up via the clinic, WeChat app, telephone, or email according to their condition to observe the occurrence of major adverse cardiac events (MACE). MACE was defined as cardiovascular death, new myocardial infarction, unplanned PCI, and progression to class IV heart failure according to the New York Heart Association classification.

Statistical analysis

SPSS19.0 software (IBM Corp., Armonk, NY, USA) was used for statistical analysis. Normally distributed data are presented as the mean±standard deviation (x̄±S), and non-normally distributed data are presented as median and interquartile range. The comparison of measurement data that was normally distributed among groups was performed by one-way analysis of variance followed by a least significant difference post-hoc test. A non-parametric test was used for the statistical analysis of non-normally distributed data or non-uniform variance among groups (Kruskal Wallis H-rank sum test). Comparison of normally distributed measurement data before and after PCI was performed using the paired sample t-test. The Wilcoxon signed-rank test was used to compare the parameters of non-normally distributed measurement data before and after PCI. Correlation analysis of measurement data was performed using Pearson's correlation analysis (normally distributed data) or Spearman's correlation analysis (non-normally distributed data). The chi-square test was used to compare the count data among the groups. A multivariate Cox regression model was used to analyze the factors influencing the incidence of MACE in patients with ACS. A receiver operating characteristic (ROC) curve was used to evaluate the predictive value of inflammation indicators for the incidence of MACE after PCI in patients with ACS. Statistical significance was set at p<0.05.

RESULTSGeneral clinical indicators and PCI-related indicators

A total of 205 patients with ACS (138 male and 67 female) were enrolled in this study, including 156 patients with UA, 25 patients with non-STEMI, and 24 patients with acute STEMI. Table 1 shows the comparison of the general clinical data of patients with ACS. Patients with ACS with acute STEMI were older than patients with ACS with UA and non-STEMI (p=0.004). No statistical differences were found among the SYNTAX scores, number of treated coronary arteries, number of implanted stents, total length of implanted stents, and maximum pressure of balloon inflation in ACS subtypes.

Table 1.

Clinical characteristics of patients at baseline and post-PCI.

  UA  non-STEMI  STEMI  p-value 
Number of patients  156  25  24   
Sex (M/F)  108/48  18/7  12/12  0.151 
Age (years)  63.6±10.6  66.5±10.8  71.1±9.8*  0.004 
Hypertension, n (%)  113 (72.4)  16 (64.0)  13 (54.2)  0.163 
Heart failure, n (%)  8 (5.1)  1 (4.0)  2 (8.3)  0.769 
Cerebrovascular disease, n (%)  26 (16.7)  3 (12.0)  5 (20.8)  0.707 
Diabetes, n (%)  51 (32.7)  9 (36.0)  3 (12.5)  0.113 
CKD, n (%)  8 (5.1)  1 (4.0)  2 (8.3)  0.769 
Smoking, n (%)  31 (19.9)  3 (12.0)  3 (12.5)  0.480 
Drinking, n (%)  18 (11.5)  2 (8.0)  1 (4.2)  0.816 
Type of P2Y12 antagonist        0.120 
Ticagrelor  99 (63.5)  12 (48.0)  11(45.8)   
Clopidogrel  57 (36.5)  13 (52.0)  13 (54.2)   
β-blocker treatment  125 (80.1)  20 (80.0)  20 (83.3)  0.756 
ACEI/ARB treatment  112 (71.2)  19 (76.0)  18 (75.0)  0.876 
Statin treatment  149 (95.5)  24 (96.0)  23 (95.8)  0.992 
PPI treatment  120 (76.9)  22 (88.0)  20 (83.3)  0.635 
SYNTAX score  14.3±7.6  17.0±7.1  17.1±7.7  0.071 
Number of treated coronary artery (Median)  1 (1-1)  1 (1-1)  1 (1-2)  0.222 
Number of stents  1 (1-2)  2 (1-2)  2 (1-2)  0.071 
Total length of stents (mm)  36.0 (24.0-57.8)  52.0 (33.0-65.5)  46.0 (33.0-66.8)  0.296 
Maximum pressure of balloon dilation (MPa)  1.8 (1.6-2.0)  1.8 (1.6-2.0)  2.0 (1.8-2.0)  0.770 
Operation duration (min)  50.0 (36.0-66.0)  55.0 (42.5-65.5)  49.0 (40.0-60.0)  0.792 

Abbreviations: PCI, percutaneous coronary intervention; UA, unstable angina; non-STEMI, acute non-ST-segment elevation myocardial infarction; STEMI, acute ST-segment elevation myocardial infarction; M, male; F, female; CKD, chronic kidney disease; ACEI, angiotensin converting enzyme inhibitors; ARB, angiotensin receptor blocker; PPI, proton-pump inhibitor; mm, millimeter; min, minute; *p<0.05, compared with the UA group.

Changes in blood cell components, NLR, and PLR in patients with ACS before and after PCI

In patients with ACS, the neutrophil count and proportion at 24h post-PCI were significantly elevated as compared to those prior to PCI, and reduced to pre-PCI levels 30 days after PCI. The lymphocyte count and proportion in patients with ACS were reduced at 24h post-PCI as compared to those prior to PCI, and were restored to pre-PCI levels 30 days after PCI. As a result, the variation trends in NLR and PLR were similar to the changes in neutrophil proportion (Table 2).

Table 2.

Changes in the preoperative and postoperative blood cell counts in patients with ACS undergoing PCI (n=205).

  WBC, k/μL  Platelet, k/μL  Neutrophil, k/μL  Lymphocyte, k/μL 
ACS (n=205)         
Pre-PCI  7.15±2.19  199.64±58.09  4.66±1.98  1.82±0.67 
24h post-PCI  7.20±1.90  188.77±55.88*  5.06±1.61*  1.52±0.57* 
30 days post-PCI  6.60±1.42*  191.15±55.30*  4.28±1.13  1.72±0.58* 
UA (n=156)         
Pre-PCI  6.77±1.84  198.63±56.58  4.27±1.55  1.85±0.70 
24h post-PCI  7.07±1.72*  187.25±54.32*  4.92±1.43*  1.53±0.57* 
30 days post-PCI  6.50±1.43  190.23±54.80*  4.19±1.11  1.71±0.58* 
non-STEMI (n=25)         
Pre-PCI  7.60±1.55  188.08±48.85  5.19±1.39Δ  1.68±0.61 
24h post-PCI  7.55±1.96  185.56±48.19  5.32±1.56  1.58±0.67 
30 days post-PCI  7.07±1.45  185.88±56.56  4.67±1.21  1.82±0.68 
STEMI (n=24)         
Pre-PCI  9.12±3.46Δ  218.21±73.18  6.61±3.32Δ  1.78±0.58 
24h post-PCI  7.70±2.77*  201.96±72.01  5.65±2.51  1.38±0.42* 
30 days post-PCI  6.81±1.27*  202.63±58.11  4.47±1.13*  1.66±0.52 
  Neutrophil, percentage  Lymphocyte, percentage  NLR  PLR 
ACS (n=205)         
Pre-PCI  63.74±10.43  26.50±9.02  2.95±1.83  121.52±51.72 
24h post-PCI  69.65±7.69*  21.56±7.03*  3.75±1.88*  137.48±57.61* 
30 days post-PCI  64.56±8.08  26.22±7.21  2.77±1.20  122.54±52.55 
UA (n=156)         
Pre-PCI  62.21±9.94  27.92±8.88  2.68±1.68  120.04±52.84 
24h post-PCI  69.21±7.77*  21.99±7.24*  3.63±1.68*  135.82±58.22* 
30 days post-PCI  64.24±8.16*  26.51±7.16*  2.72±1.18  122.68±54.38 
non-STEMI (n=25)         
Pre-PCI  67.54±9.54  22.55±7.35  3.58±1.87  123.29±48.92 
24h post-PCI  70.31±7.75  21.21±6.96  3.85±1.75  133.10±51.72 
30 days post-PCI  65.74±7.78  26.42±8.58*  2.94±1.45*  114.64±47.66 
STEMI (n=24)         
Pre-PCI  69.69±11.65Δ  21.42±8.70Δ  4.02±2.24Δ  129.33±48.20 
24h post-PCI  71.78±6.96  19.08±5.21  4.40±2.97  152.83±59.35 
30 days post-PCI  65.42±8.02  24.14±5.81  2.91±1.06  129.86±45.48 

Abbreviations: ACS, acute coronary syndrome; PCI, percutaneous coronary intervention; UA, unstable angina; non-STEMI, acute non-ST-segment elevation myocardial infarction; STEMI, acute ST-segment elevation myocardial infarction; WBC, white blood cell count; NLR, neutrophil-to-lymphocyte ratio; PLR, platelet-to-lymphocyte ratio.

*

p<0.05, compared with Pre-PCI.

p<0.05, compared with 24h post-PCI.

Δ

p<0.05, compared with UA.

Changes in blood cell components, NLR, and PLR before and after PCI in patients with different ACS subtypes

No significant differences in the platelet count and PLR were found among the three ACS subtypes before and after PCI. In addition, the acute STEMI group showed a gradual decline in white blood cell and neutrophil counts at 24h and 30 days post-PCI relative to pre-PCI, which differed from the trend in the UA group, in which the counts first increased and subsequently decreased (Table 2 and Figure 1). The neutrophil proportion, NLR, and PLR before and after PCI showed a trend of first increasing and then decreasing in all groups. These changes suggested that PCI caused an increase in the levels of inflammatory indicators.

Figure 1.

Changes in the preoperative and postoperative blood cell counts in patients with different types of ACS (n=205). Abbreviations: ACS, acute coronary syndrome; non-STEMI, acute non-ST-segment elevation myocardial infarction; NLR, neutrophil-to-lymphocyte ratio; PLR, platelet-to-lymphocyte ratio; STEMI, acute ST-segment elevation myocardial infarction; UA, unstable angina; WBC, white blood cell count.

(0.1MB).
Factors influencing MACE after PCI in patients with ACS

Of the 205 patients with ACS who were followed up for an average of 15 months (median) after PCI, 19 patients (9.3%) experienced MACE. The multivariate Cox regression model (entry method) was used to analyze the possible influencing factors of MACE. The results showed that the NLR at 24h post-PCI (hazard ratio [HR]=3.84, p=0.005), PLR at 24h post-PCI (HR=1.05, p=0.034), and acute STEMI (HR=4.65, p=0.039) were independent factors affecting the incidence of MACE after PCI. As shown in Table 3, the NLR and PLR before and 30 days after PCI had no effect on the incidence of MACE after PCI.

Table 3.

Multiple Cox analysis of the factors predicting MACE in patients with ACS.

BWaldp-valueHR95% CI
Lower bound  Upper bound 
Sex  0.82  0.65  0.419  2.27  0.31  16.64 
Age  −0.07  1.31  0.253  0.93  0.82  1.05 
Hypertension  2.30  2.83  0.093  10.00  0.68  146.42 
Heart failure  0.08  0.00  0.959  1.08  0.05  21.23 
Cerebrovascular disease  1.56  2.69  0.101  4.76  0.74  30.63 
Diabetes  0.24  0.06  0.808  1.28  0.18  9.03 
CKD  −2.79  2.42  0.120  0.06  0.00  2.07 
Smoking  −0.34  0.04  0.840  0.71  0.03  18.53 
Type of P2Y12 antagonist  −2.18  1.39  0.239  0.11  0.00  4.25 
acute STEMI  1.54  4.26  0.039  4.65  1.08  20.02 
SYNTAX score  0.07  1.55  0.213  1.07  0.96  1.20 
NLR pre-PCI  −0.13  0.14  0.712  0.88  0.45  1.72 
PLR pre-PCI  0.02  1.47  0.225  1.02  0.99  1.05 
NLR 24h post-PCI  1.35  7.81  0.005  3.84  1.50  9.89 
PLR 24h post-PCI  0.04  4.48  0.034  1.05  1.01  1.10 
NLR 30 days post-PCI  0.68  2.14  0.143  1.97  0.80  4.86 
PLR 30 days post-PCI  0.02  1.50  0.221  1.02  0.99  1.05 

Abbreviations: MACE, major adverse cardiac events; ACS, acute coronary syndrome; PCI, percutaneous coronary intervention; NLR, neutrophil-to-lymphocyte ratio; PLR, platelet-to-lymphocyte ratio; STEMI, acute ST-segment elevation myocardial infarction; CKD, chronic kidney disease; CI, confidence interval.

ROC curve for the evaluation of predictive factors of incidence of MACE after PCI in patients with ACS

The results showed that the NLR and PLR at 24h post-PCI could be used to predict the incidence of MACE after PCI (p<0.01). However, the area under the curve for predicting the incidence of MACE was higher for NLR than that for PLR (0.862 vs. 0.703) (Table 4 and Figure 2). Moreover, the optimal cut-off point of the ROC curve for the NLR at 24h post-PCI was 3.0, with a sensitivity of 78.9% and a specificity of 67.7%, and the optimal cut-off point of the ROC curve for the PLR at 24h post-PCI was 107.01, with a sensitivity of 73.7% and a specificity of 47.8%.

Table 4.

ROC curves of NLR and PLR for predicting MACE.

Area under the curveStandard errorp-value95% CI of Area
Lower bound  Upper bound 
NLR  0.862  0.042  <0.001  0.779  0.945 
PLR  0.703  0.061  0.004  0.583  0.822 

Abbreviations: MACE, major adverse cardiac events; ROC, receiver operating characteristic; NLR, neutrophil-to-lymphocyte ratio; PLR, platelet-to-lymphocyte ratio; CI, confidence interval.

Figure 2.

ROC curves of inflammatory biomarkers for predicting MACE after PCI. Abbreviations: PCI, percutaneous coronary intervention; MACE, major adverse cardiac events; ROC, receiver operating characteristic.

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Correlation analysis of NLR and PLR

Correlation analysis showed that the NLR at 24h post-PCI significantly correlated with the number of implanted stents (p=0.046), length of implanted stent (p=0.014), operation duration (p=0.004), PLR (p<0.001), hsCRP (p<0.001), and IL-6 (p<0.001) (Table 5). There was no significant correlation between the PLR at 24h post-PCI and any of these PCI-related parameters. However, the PLR at 24h post-PCI was significantly correlated with hsCRP (p=0.001) and IL-6 (p=0.009) (Table 6).

Table 5.

Correlations between NLR and age, parameters in PCI and inflammatory factors (n=205).

  p-value 
Age  0.127  0.069 
SYNTAX score  0.055  0.434 
Number of interventional coronary arteries  0.055  0.430 
Number of stents  0.140  0.046 
Total length of stents (mm)  0.172  0.014 
Maximum pressure of balloon dilation (kPa)  0.071  0.308 
Operation duration (min)  0.199  0.004 
PLR 24h post-PCI  0.616  <0.001 
IL-6 24h post-PCI  0.286  <0.001 
hsCRP 24h post-PCI  0.248  <0.001 

Abbreviations: NLR, neutrophil-to-lymphocyte ratio; PLR, platelet-to-lymphocyte ratio; hsCRP, hypersensitive C-reactive protein; IL-6, interleukin-6.

Table 6.

Correlations between postoperative PLR and age, parameters in PCI and inflammatory factors (n=205).

  p-value 
Age  0.122  0.082 
SYNTAX score  0.056  0.422 
Number of treated coronary arteries  −0.007  0.919 
Number of stents  0.020  0.772 
Total length of stents (mm)  0.042  0.546 
Maximum pressure of balloon dilation (kPa)  0.060  0.393 
Operation duration (min)  0.106  0.132 
NLR 24h post-PCI  0.616  <0.001 
IL-6 24h post-PCI  0.183  0.009 
hsCRP 24h post-PCI  0.234  0.001 

Abbreviations: PLR, platelet-to-lymphocyte ratio; PCI, percutaneous coronary intervention; NLR, neutrophil-to-lymphocyte ratio; hsCRP, hypersensitive C-reactive protein; IL-6, interleukin-6.

DISCUSSION

Inflammation plays an important role in the occurrence and development of atherosclerotic cardiovascular disease and is related to the poor prognosis of ACS (5,6,22). NLR and PLR are inflammatory indicators that have been used to assess the levels of inflammation in cardiovascular diseases in recent years (15,18). One recent study has shown that in patients with coronary heart disease and hsCRP<2.0 mg/L, the pre-PCI NLR is an influencing factor affecting the long-term prognosis of patients after PCI (23). These findings suggest that NLR may have a better predictive value in the prognosis of patients with ACS after PCI.

In this study, we found that NLR and PLR increased in patients with ACS at 24h post-PCI and then decreased over the 30 days following the operation. These dynamic trends in the NLR and PLR before and after PCI have not been reported in previous studies. The results of the Cox regression analysis showed that the NLR and PLR at 24h post-PCI were independent risk factors for MACE after PCI. However, the NLR and PLR before and 30 days after PCI had no effect on the incidence of MACE after PCI. The area under the ROC curve for NLR was greater than that for PLR, which implied that the sensitivity and specificity of NLR were higher than those of PLR.

Significant positive correlations were observed between the NLR at 24h post-PCI, the number of stents implanted during PCI, the length of the stents, and the duration of the operation. These findings suggest that the NLR after PCI is related to the complexity of the interventional procedure. After PCI, neutrophils migrate, aggregate, and adhere to arterial endothelial cells; activate platelets; and further promote the inflammatory response (24). This excessive inflammatory response may promote the progression of atherosclerotic lesions, plaque instability, atherosclerotic thrombosis (25), lack of coronary reflow after PCI (26), and increased ventricular remodeling (14), all of which can lead to post-PCI in-stent restenosis (27), acute myocardial infarction, and deterioration of cardiac function (28).

These results suggest that the NLR at 24h post-PCI is a very good indicator of the inflammatory response after PCI and has better predictive value for the prognosis of PCI than PLR. We should pay attention to the treatment and follow-up of patients with elevated inflammatory indicators after PCI, especially in patients with ACS with NLR>3.0, after PCI. Anti-inflammatory treatment with IL-1β monoclonal antibodies or intensive statin treatments in patients with coronary heart disease has been shown to reduce the incidence of MACE (29,30). Therefore, inflammation is one of the targets that requires continuous therapeutic intervention in the treatment of ACS.

This study had some limitations, such as a short follow-up period and a small sample size from a single center. The results of this study need to be confirmed by a multicenter, large-sample, long-term follow-up clinical study. Because of the lack of relevant inflammatory marker data between 24h and 30 days after PCI, precise observation of the change in the trend of inflammatory indicators after PCI was not possible.

CONCLUSION

The neutrophil proportion and NLR of patients with ACS were elevated after PCI and were accompanied by a reduction in the lymphocyte count and proportion. In addition, compared with the PLR at 24h post-PCI, the NLR at 24h post-PCI had a better predictive value for the incidence of MACE after PCI.

AUTHOR CONTRIBUTIONS

Sheng J designed the study design and wrote the manuscript. Liu N and He F collected and analyzed data. Cheng C and Shen S contributed to patient follow-up. Sun Y and Shen S contributed to the experimental part of this study.

ACKNOWLEDGMENTS

This study was supported by the Clinical Research Cultivation Program of the Second Affiliated Hospital of Anhui Medical University (2020LCYB10).

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No potential conflict of interest was reported.

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