NEUTROPHIL-LYMPHOCYTE RATIO PREDICTS SHORT-TERM MORTALITY IN PATIENTS HOSPITALIZED FOR ACUTE DECOMPENSATION OF CIRRHOSIS

MACCALI, Claudia; AUGUSTINHO, Fernanda Cristina de; ZOCCHE, Tamara Liana; SILVA, Telma Erotides; NARCISO-SCHIAVON, Janaína Luz; SCHIAVON, Leonardo de Lucca

doi:10.1590/S0004-2803.202100000-23

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ORIGINAL ARTICLE • Arq. Gastroenterol. 58 (02) • Apr-Jun 2021 • https://doi.org/10.1590/S0004-2803.202100000-23 copy

NEUTROPHIL-LYMPHOCYTE RATIO PREDICTS SHORT-TERM MORTALITY IN PATIENTS HOSPITALIZED FOR ACUTE DECOMPENSATION OF CIRRHOSIS

Razão neutrófilo-linfócito prediz mortalidade em curto prazo em pacientes hospitalizados com cirrose hepática descompensada

Authorship SCIMAGO INSTITUTIONS RANKINGS

ABSTRACT

BACKGROUND:

Individuals with cirrhosis have a chronic systemic inflammation associated with an immune dysfunction, affecting the progression of the liver disease. The neutrophil-lymphocyte ratio (NLR) was proposed as a marker of systemic inflammatory response and survival in patients with cirrhosis.

OBJECTIVE:

Evaluate the prognostic role of NLR in cirrhotic patients and its relation with inflammatory cytokines(IL-6, IL-10 and IL-17).

METHODS:

In this prospective study two groups were evaluated: 1) Stable cirrhotic in outpatient follow-up (n=193); 2) Hospitalized cirrhotic for acute decompensation for at least 48 hours (n=334) with admission and 48 hours tests evaluation. Circulating inflammatory cytokines were available for 130 hospitalized patients.

RESULTS:

In outpatients with stable cirrhosis, NLR correlated with MELD score and other variables associated with severity of disease. However, after a median of 32 months of follow up NLR was not associated with mortality (HR 1.058, 95%CI 0.900-1.243; P=0.495). In hospitalized patients, NLR at 48-hour after admission was independently associated with 90-day survival (HR 1.061, 95%CI 1.020-1.103; P=0.003) in multivariate Cox-regression analysis. The 90-day Kaplan-Meier survival probability was 87% for patients with a 48-hour NLR <3.6 and 62% for NLR ≥3.6 (P<0.001). Elevation of NLR in the first 48 hours was also independently associated with mortality (HR 2.038, 95%CI 1295-3207; P=0.002). The 90-day Kaplan-Meier survival probability was 83% when NLR did not increase and 62% when NLR increased (P<0.001). IL-6, IL-10 and IL-17 at admission were positively correlated with both admission and 48-hour NLR. Lower levels of baseline IL-10 were associated with NLR increase during first 48-hour.

CONCLUSION:

NLR evaluated at 48 hours of hospitalization and its early increase after admission were independently associated with short-term mortality in patients hospitalized for acute decompensation of cirrhosis.

Keywords:
Liver cirrhosis; cytokines; prognosis; inflammation

Variables	Stable	Acute
	cirrhosis	decompensation
	(n=193)	(n=320)
Age (years), mean ± SD	54.36±12.48	55.67±10.77
Male gender, n (%)	131 (67.9)	235 (73.4)
Etiology of cirrhosis, n (%)
Alcohol	104 (53.9)	182 (56.9)
Hepatitis C	63 (32.6)	114 (35.6)
Hepatitis B	11 (5.7)	19 (6.0)
Cryptogenic	20 (10.4)	25 (7.8)
NAFLD	7 (3.6)	20 (6.3)
Autoimmune	8 (4.1)	10 (3.1)
Previous decompensation, n (%)	142 (73.6)	210 (66.2)
Active alcoholism, n (%)	11 (5.7)	102 (31.9)
Hepatocellular carcinoma	0	21 (7.2)
Esophageal varices	155 (81.2)	83 (74.1)^#
Propranolol, n (%)	110 (57.0)	102 (32.1)
Complications in the evaluation, n (%)
Ascites	43 (22.3)	167 (52.2)
Hepatic encephalopathy	20 (10.4)	158 (49.4)
Gastrointestinal bleeding	0	128 (40.0)
Bacterial infection	0	143 (44.7)
ACLF	NA	78 (24.4)
Laboratory data
Leukocyte Count (x 10⁹), median	4.78	7.51
Sodium (meq/L), mean ± SD	137.41±2.65	135.48±5.16
Creatinine (mg/dL), median	0.90	1.10
INR, median	1.20	1.44
Albumin (g/dL), mean ± SD	3.41±0.49	2.47±1.84
CRP (mg/L), median	3.50	15.10
Total bilirubin (mg/dL), median	1.00	2.10
NLR, median	2.10	4.05
Child-Pugh classification, n (%)
A	123 (63.7)	24 (7.5)
B	59 (30.6)	156 (49.1)
C	11 (5.7)	138 (43.4)
MELD, mean + SD	10.10±2.51	16.81±6.36
CLIF-SOFA, mean ± SD	NA	6.45±2.62

Variables	Survivors	Non-survivors	HR (CI 95%)	P
	(n=243)	(n=77)
Age (years), mean ± SD	55.39±10.76	56.56±10.82	1.008 (0.988-1.030)	0.428
Male gender, n (%)	180 (74.1)	55 (71.4)	0.903 (0.551-1.480)	0.685
Etiology of cirrhosis, n (%)
Alcohol	138 (56.8)	44 (57.1)	1.021 (0.650-1.603)	0.929
Hepatitis C	89 (36.6)	25 (32.5)	0.838 (0.520-1.350)	0.467
Hepatitis B	13 (5.4)	6 (7.8)	1.385 (0.602-3.186)	0.444
Cryptogenic	18 (7.4)	7 (9.1)	0.935 (0.583-1.500)	0.781
Active alcoholism, n (%)	54 (24.8)	23 (22.5)	0.898 (0.551-1.463)	0.666
Previous decompensation, n (%)	160 (65.8)	50 (64.9)	0.951 (0.596-1.519)	0.834
Complication in admission, n (%)
Ascites	108 (44.4)	59 (76.6)	3.545 (2.090-6.012)	<0.001
Hepatic encephalopathy	110 (45.3)	48 (62.3)	1.822 (1.149-2.889)	0.011
Gastrointestinal Bleeding	106 (43.6)	22 (28.6)	0.573 (0.349-0.939)	0.027
Bacterial infection	90 (37.0)	53 (68.8)	3.253 (2.007-5.272)	<0.001
ACLF, n (%)	39 (16.0)	39 (50.6)	4.154 (2.654-6.502)	<0.001
Laboratory data
Leukocyte count (x109), median	7.00	7.25	1.045 (1.008-1.083)	0.017
Sodium (meq/L), mean ± SD	135.97±4.88	133.96±5.74	0.938 (0.901-0.976)	0.002
INR, median	1.40	1.65	1.829 (1.462-2.288)	<0.001
Albumin (g/dL), mean ± SD	2.40 ± 0.61	2.00±0.55	0.256 (0.165-0.399)	<0.001
CRP (mg/L), median	10.90	28.30	1.007 (1.004-1.010)	<0.001
Bilirubin total (mg/dL), median	1.80	3.15	1.049 (1.022-1.077)	<0.001
Admission NLR, median	3.91	4.68	1.047 (1.021-1.073)	<0.001
Child-Pugh C, n (%)	83 (34.3)	55 (72.4)	4.013 (2.426-6.638)	<0.001
MELD score, mean ± SD	14.35±5.00	22.44±6.95	1.116 (1.087-1.146)	<0.001
CLIF-SOFA, mean ± SD	5.83±2.30	8.52±2.57	1.393 (1.290-1.503)	<0.001
Vital signs
MAP (mmHg), mean ± SD	85.70±15.24	83.98±16.58	0.922 (0.977-1.007)	0.319
Heart rate, mean ± SD	81.51±18.19	85.53±16.43	1.011 (0.999-1.023)	0.079
SpO2/FiO2, median	466.66	457.14	0.989 (0.986-0.993)	<0.001

Instituto Brasileiro de Estudos e Pesquisas de Gastroenterologia e Outras Especialidades - IBEPEGE. Rua Dr. Seng, 320, 01331-020 São Paulo - SP Brasil, Tel./Fax: +55 11 3147-6227 - São Paulo - SP - Brazil
E-mail: secretariaarqgastr@hospitaligesp.com.br

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[1] Corresponding author: Claudia Maccali. E-mail: maccalicm@gmail.com