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Elevated Liver Enzymes along with Comorbidity Is a High Risk Factor for COVID-19 Mortality: A South Indian Study on 1,512 Patients

  • Narayanasamy Krishnasamy1,*,
  • Karthick Rajendran2,* ,
  • Parimita Barua1,
  • Arunkumar Ramachandran2 ,
  • Priyadarshini Panneerselvam2  and
  • Muthukumaran Rajaram2
Journal of Clinical and Translational Hepatology   2022;10(1):120-127

doi: 10.14218/JCTH.2020.00100

Received:

Revised:

Accepted:

Published online:

 Author information

Citation: Krishnasamy N, Rajendran K, Barua P, Ramachandran A, Panneerselvam P, Rajaram M. Elevated Liver Enzymes along with Comorbidity Is a High Risk Factor for COVID-19 Mortality: A South Indian Study on 1,512 Patients. J Clin Transl Hepatol. 2022;10(1):120-127. doi: 10.14218/JCTH.2020.00100.

Abstract

Background and Aims

Liver enzyme abnormalities in coronavirus 2019 (COVID-19) are being addressed in the literature. The predictive risk of elevated liver enzymes has not been established for COVID-19 mortality. In this study, we hypothesized that elevated liver enzymes at admission can predict the outcome of COVID-19 disease with other known indicators, such as comorbidities.

Methods

This retrospective study included all the consecutive hospitalized patients with confirmed COVID-19 disease from March 4th to May 31st, 2020. The study was conducted in Rajiv Gandhi Government General Hospital, Chennai, Tamil Nadu, India. We assessed demography, clinical variables, COVID-19 severity, laboratory parameters, and outcome.

Results

We included 1,512 patients, and median age was 47 years (interquartile range: 34–60) with 36.9% being female. Liver enzyme level (aspartate aminotransferase and/or alanine aminotransferase) was elevated in 450/1,512 (29.76%) patients. Comorbidity was present in 713/1,512 (47.16%) patients. Patients with liver enzymes’ elevation and presence of comorbidity were older, more frequently hospitalized in ICU and had more severe symptoms of COVID-19 at the time of admission. Presence of liver enzymes’ elevation with comorbidity was a high risk factor for death (OR: 5.314, 95% CI: 2.278–12.393), as compared to patients with presence of comorbidity (OR: 4.096, 95% CI: 1.833–9.157).

Conclusions

Comorbidity combined with liver enzymes’ elevation at presentation independently increased the risk of death in COVID-19 by at least 5-fold.

Keywords

COVID-19, SARS-CoV-2, Liver enzyme, Comorbidity, Aspartate aminotransferase, Alanine aminotransferase

Introduction

Coronaviruses (CoVs) are a family of viruses that are known to cause both respiratory and intestinal diseases in various animal species and humans.1 The viruses are known to cause upper respiratory and lower respiratory tract infections, ranging from mild illnesses such as sore throat to severe pneumonia, leading to acute respiratory distress syndrome (ARDS), respiratory failure and death. To date, seven human coronaviruses have been identified, including the three epidemic viruses of severe acute respiratory syndrome (SARS)-CoV, middle east respiratory syndrome (MERS)-CoV and the newest, severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2).2 These three epidemic viruses have similar sequence identity, sharing more than 50% of genome sequences.3 In December 2019, there was an outbreak of pneumonia of unknown origin in the Central city of Wuhan, which rapidly spread to other parts of the world, leading to 44,888,869 cases and 1,178,475 deaths globally as of October 30, 2020.4 The World Health Organization labelled COVID-19 as a pandemic by March 2020. While most COVID-19 cases have been identified as mild, more extreme manifestations have led to respiratory failure, septic shock, and/or multiple organ dysfunctions.5

A number of reports have shown that COVID-19 patients have liver enzyme abnormalities.6 Our study aimed to determine the liver enzyme abnormality in patients with COVID-19 at the time of hospital admission and to evaluate the outcome of such patients. To our knowledge, this is the first study that analyzes the association of mortality and patients with liver enzyme elevation and comorbidity in Indian COVID-19 subjects.

Methods

The study was designed as a retrospective analysis of data collected from consecutive patients with COVID-19 admitted to the Rajiv Gandhi Government Hospital, Chennai, Tamil Nadu, India. The study period was from 4th March to 31st May 2020. Patients with COVID-19 admitted in the hospital were included in the study. Diagnosis of COVID-19 was confirmed by detection of SARS-CoV-2 RNA from nasopharyngeal/throat swabs using real-time reverse transcription-polymerase chain reaction. The study was approved by the institutional ethics committee of the Madras Medical College, Chennai, India.

Data collection

Demographics, clinical characteristics, laboratory findings, and radiography findings were collected from the medical records of the Community Medicine Department, Internal Medicine Department, pathology laboratory, biochemical laboratory, and Radiology Department by the Multidisciplinary Research Unit, Madras Medical College. The patient outcomes (discharge or death) were also collected for this analysis. Any uncertain or missing records were clarified and obtained by direct communication with patients and their families.

Biochemical and hematological parameters studied were complete blood count with differential count, white blood cell (WBC), red blood cell (RBC), hemoglobin, neutrophil-to-lymphocyte ratio (NLR), blood glucose, liver function test, and kidney function test. Markers of acute phase reaction proteins, such as lactate dehydrogenase (LDH), ferritin and C-reactive protein (CRP), were also collected. Creatine kinase (CK) and creatine kinase myocardial band (CK-MB) were also studied from the time of admission.

Clinical severity definitions

The clinical classification of COVID-19 was based on the Indian Ministry of Health and Family Welfare.7 Mild type was defined as without evidence of breathlessness or hypoxia (normal saturation). Moderate type was defined as a patient with pneumonia, without signs of severe disease and presence of clinical features of dyspnea and or hypoxia, fever, cough, including peripheral oxygen saturation (SpO2) <94% (range: 90–94%) on room air, respiratory rate (RR) more or equal to 24 per minute; fast breathing (in breaths/m) < 2 months was ≥60, for 2–11 months was ≥50 and for 1–5 years was ≥40. Severe type was defined as patients with clinical signs of pneumonia plus one of the following: respiratory rate >30 breaths/m, severe respiratory distress, or SpO2 <90% on room air. We graded severity of pneumonia based on computed tomography (CT) scan imaging of chest as percentage of total lung volume involved, with <25 as Grade 1, 25–50% as Grade 2, 51–75% as Grade 3, and >75% as Grade 4.

Inclusion criteria

All patients with COVID-19 diagnosed with swab test irrespective of age, and gender.

Patients were followed from the time of hospital admission till their death or discharge.

Exclusion criteria

Patients were excluded if they had preexisting liver diseases or liver enzyme abnormalities.

Definitions

Abnormal/elevated aspartate aminotransferase (AST) or alanine aminotransferase (ALT) was defined by taking the reference upper limit of normal as defined in male (ALT: 37 IU/L, AST: 41 IU/L) and in female (ALT: 37 IU/L, AST: 35 IU/L).8 Other test abnormalities were defined as the following reference: WBCs <3,800 or >11,000 cells/mm3; RBCs in male <4.2 or >5.6 (×106/µL) and in female <3.8 or >5.1 (×106/µL); hemoglobin in male <14 or >18 g/dL and in female <11 or >16 g/dL; packed cell volume (PCV) in male <40 or >52% and in female <35 or >47%; platelets <1.40 or <4.5 (×106/µL); neutrophils <50 or >81%; lymphocytes <14 or >44%; NLR <1 or >3; glucose (Random Blood Sugar) >140 mg/dL; urea <15 or >40 mg/dL; creatinine <0.5 or >1.3 mg/dL; sodium <136 or >146 m.eq/L; potassium <3.5 or >5.0 m.eq/L; triglyceride cholesterol (TGL-C) <40 or >170 mg/dL; CK <20 or >200 IU/L; CK MB <5 or >25 IU/L; LDH <125 or >220 IU/L; ferritin >400 ng/mL; CRP >10 mg/L; total bilirubin <0.3 or >1.3 mg/dL; direct bilirubin <0.0 or >0.4 mg/dL; total protein <6.5 or >8 g/dL; albumin <3.5 or >5.0 g/dL; alkaline phosphatase <32 or >110 U/L; pulse rate (PR) <60 or >100 beats/min; respiratory rate (RR) <14 or > 24 breaths per minute; saturation (SpO2) <94%. We graded severity of pneumonia based on computed tomography (CT) scan imaging of chest as percentage of total lung volume involved <25 as Grade 1, 25–50% as Grade 2, 51–75% as Grade 3, and >75% as Grade 4.

Results

Among 1,512 COVID-19 patients, 450 (29.76%) had elevated liver enzyme and 1,062 (70.24%) had normal range. The clinical characteristics of the patients were grouped based on discharged or death and presented in Table 1. Clinical characteristics and outcomes of COVID-19 stratified by elevated liver enzyme and comorbidity are presented in Table 2. To further understand the pattern of liver enzyme elevation, we classified these biomarkers into three distinct subtypes, such as AST elevation, ALT elevation, and both AST and ALT elevation, which showed a significant difference among survivors and non-survivors (Table 3).

Table 1

Characteristics of 1,512 patients with COVID-19 at admission grouped by survival

CharacteristicsTotal, n (%)Discharged, n (%)Death, n (%)p valuea
Age in years<1847 (3.1)47 (3.3)0 (0)0.0001
18–29229 (15.1)227 (15.8)2 (2.7)
30–39244 (16.1)239 (16.6)5 (6.8)
40–49298 (19.7)288 (20)10 (13.7)
50–59300 (19.8)284 (19.7)16 (21.9)
>60394 (26.1)354 (24.6)40 (54.8)
GenderMale954 (63.1)907 (63)47 (64.4)0.815
Female558 (36.9)532 (37)26 (35.6)
Chest CTNormal664 (43.9)647 (45)17 (23.3)0.0001
Abnormal848 (56.1)792 (55)56 (76.7)
Chest CT gradeGrade 1465 (30.8)450 (31.3)15 (20.5)0.0001
Grade 2248 (16.4)234 (16.3)14 (19.2)
Grade 3105 (6.9)89 (6.2)16 (21.9)
Grade 430 (2)19 (1.3)11 (15.1)
Normal664 (43.9)647 (45)17 (23.3)
SymptomsAbsent681 (45)668 (46.4)13 (17.8)0.0001
Present831 (55)771 (53.6)60 (82.2)
Disease severityAsymptomatic/Mild729 (48.2)723 (50.2)6 (8.2)0.0001
Moderate373 (24.7)358 (24.7)15 (20.5)
Severe410 (27.1)358 (27.1)52 (71.2)
ICUNot admitted1,029 (68.1)1,015 (70.5)14 (19.2)0.0001
Admitted483 (31.9)424 (29.5)59 (80.8)
WBCsNormal1,186 (78.4)1,154 (80.2)32 (43.8)0.0001
Abnormal326 (21.6)285 (19.8)41 (56.2)
RBCsNormal1,154 (76.3)1,106 (76.9)48 (65.8)0.029
Abnormal358 (23.7)333 (23.1)25 (34.2)
HemoglobinNormal887 (58.7)853 (59.3)34 (46.6)0.032
Abnormal625 (41.3)586 (40.7)39 (53.4)
PCVNormal929 (61.4)894 (62.1)35 (47.9)0.015
Abnormal583 (38.6)545 (37.9)38 (52.1)
PlateletsNormal1,303 (86.2)1,242 (86.3)61 (83.6)0.507
Abnormal209 (13.8)197 (13.7)12 (16.4)
NeutrophilsNormal1,072 (70.9)1,026 (71.3)46 (63)0.128
Abnormal440 (29.1)413 (28.7)27 (37)
LymphocytesNormal1,133 (74.9)1,094 (76)39 (53.4)0.0001
Abnormal379 (25.1)345 (24)34 (46.6)
NLRNormal907 (60)879 (61.1)28 (38.4)0.0001
Abnormal605 (40)560 (38.9)45 (61.6)
GlucoseNormal567 (37.5)545 (37.9)22 (30.1)0.183
Abnormal945 (62.5)894 (62.1)51 (69.9)
UreaNormal971 (64.2)937 (65.1)34 (46.6)0.001
Abnormal541 (35.8)502 (34.9)39 (53.4)
CreatinineNormal1,348 (89.2)1,286 (89.4)62 (84.9)0.234
Abnormal164 (10.8)153 (10.6)11 (15.1)
SodiumNormal911 (70.5)872 (70.7)39 (66.1)0.453
Abnormal382 (29.5)362 (29.3)20 (33.9)
PotassiumNormal838 (65.3)802 (65.4)36 (62.1)0.601
Abnormal446 (34.7)424 (34.6)22 (37.9)
TGL-CNormal1,156 (76.5)1,093 (76)63 (86.3)0.042
Abnormal356 (23.5)346 (24)10 (13.7)
CKNormal663 (67.4)640 (68)23 (53.5)0.047
Abnormal321 (32.6)301 (32)20 (46.5)
CK-MBNormal1,145 (75.7)1,097 (76.2)48 (65.8)0.042
Abnormal367 (24.3)342 (23.8)25 (34.2)
LDHNormal390 (33.2)386 (34.5)4 (7.3)0.0001
Abnormal783 (66.8)732 (65.5)51 (92.7)
FerritinNormal774 (65)749 (66)25 (45.5)0.002
Abnormal416 (35)386 (34)30 (54.5)
CRPNormal558 (46.7)550 (48.3)8 (14.3)0.0001
Abnormal637 (53.3)589 (51.7)48 (85.7)
Total bilirubinNormal1,437 (95)1,368 (95.1)69 (94.5)0.834
Abnormal75 (5)71 (4.9)4 (5.5)
Direct bilirubinNormal1,370 (90.6)1,307 (90.8)63 (86.3)0.196
Abnormal142 (9.4)132 (9.2)10 (13.7)
Total proteinNormal1,037 (97.6)993 (97.6)44 (97.8)0.952
Abnormal25 (2.4)24 (2.4)1 (2.2)
AlbuminNormal1,223 (80.9)1,173 (81.5)50 (68.5)0.006
Abnormal289 (19.1)266 (18.5)23 (31.5)
ASTNormal1,198 (79.2)1,153 (80.1)45 (61.6)0.0001
Abnormal314 (20.8)286 (19.9)28 (38.4)
ALTNormal1,166 (77.1)1,112 (77.3)54 (74)0.512
Abnormal346 (22.9)327 (22.7)19 (26)
ALPNormal763 (80.9)736 (81.6)27 (65.9)0.012
Abnormal180 (19.1)166 (18.4)14 (34.1)
PRNormal1,385 (91.6)1,331 (92.5)54 (74)0.0001
Abnormal127 (8.4)108 (7.5)19 (26)
RRNormal972 (64.3)940 (65.3)32 (43.8)0.0001
Abnormal540 (35.7)499 (34.7)41 (56.2)
SpO2Normal1,389 (91.9)1,348 (93.7)41 (56.2)0.0001
Abnormal123 (8.1)91 (6.3)32 (43.8)
Table 2

Characteristics of 1,512 patients with COVID-19 at admission grouped by comorbidity and liver function test

CharacteristicsAbsence of comorbidity and normal level of liver enzyme (n=586)Elevated liver enzyme (n=213)Presence of comorbidity (n=476)Elevated liver enzyme with presence of comorbidity (n=237)p valuea
Age in years<40 (n=520)327 (55.8)86 (40.4)78 (16.4)29 (12.2)0.0001
>40 (n=992)259 (44.2)127 (59.6)398 (83.6)208 (87.8)
GenderMale394 (67.2)136 (63.8)269 (56.5)155 (65.4)0.003
Female192 (32.8)77 (36.2)207 (43.5)82 (34.6)
Chest CTNormal362 (61.8)80 (37.6)151 (31.7)71 (30)0.0001
Abnormal224 (38.2)133 (62.4)325 (68.3)166 (70)
SymptomsAbsent324 (55.3)103 (48.4)174 (36.6)80 (33.8)0.0001
Present262 (44.7)110 (51.6)302 (63.4)157 (66.2)
Disease severityAsymptomatic/Mild408 (69.6)110 (51.6)146 (30.7)65 (27.4)0.0001
Moderate104 (17.7)51 (23.9)149 (31.3)69 (29.1)
Severe74 (12.6)52 (24.4)181 (38)103 (43.5)
ICUNot Admitted480 (81.9)135 (63.4)302 (63.4)112 (47.3)0.0001
Admitted106 (18.1)78 (36.6)174 (36.6)125 (52.7)
OutcomeDischarged578 (98.6)206 (96.7)441 (92.6)214 (90.3)0.0001
Death8 (1.4)7 (3.3)35 (7.4)23 (9.7)
Table 3

Elevated liver enzyme and its association with characteristics of patients with COVID-19

CharacteristicsCOVID-19 patients with elevated liver enzyme
TotalP valuea
AST (n=103, 22.9%)ALT (n=135, 30.0%)AST and ALT (n=212, 47.1%)n=450
Age in years<4021 (20.4%)53 (39.3%)41 (19.3%)115 (25.6%)0.0001
>4082 (79.6%)82 (60.7%)171 (80.7%)335 (74.4%)
GenderMale65 (63.1%)91(67.4%)135 (63.7%)291 (64.7%)0.725
Female38 (36.9%)44 (32.6%)77 (36.3%)159 (35.3%)
Chest CTNormal29 (28.2%)64 (47.4%)58 (27.4%)151 (33.6%)0.0001
Abnormal74 (71.8%)71(52.76%)154 (72.6%)299 (66.4%)
SymptomsAbsent37(35.9)58 (43)76 (35.8)171 (38)0.365
Present66 (64.1)77 (57)136 (64.2)279 (62)
Disease severityAsymptomatic/Mild35 (34.0%)67 (49.6%)73 (34.4%)175 (38.9%)0.030
Moderate28 (27.2%)34 (25.2%)58 (27.4%)120 (26.7%)
Severe40 (38.8%)34 (25.2%)81 (38.2%)155 (34.4%)
ICUNot admitted53 (51.5%)97 (71.9%)97 (45.8%)247 (54.9%)0.0001
Admitted50 (48.5%)38 (28.1%)115 (54.2%)203 (45.1%)
OutcomeDeath11 (10.7%)2 (1.5%)17 (8%)30 (6.7%)0.001
Discharged92 (89.3%)133 (98.5%)195 (92%)420 (93.3%)

Age group

In the study population, of 1,512 cases, the median age was 47 years (IQR: 34–60 years) and 63.1% cases were male. Compared to survivors, non-survivors were significantly older (44 years [IQR: 33-49] vs. median age 56 years [IQR: 52-73], p<0.001) and were more likely to have underlying comorbid illness with elevated liver enzyme. A majority of non-survivors (66/73) were in the more than 40 years of age group (Table 1). In the study population, patients with age >40 years were more likely to have elevated liver enzyme (127/992), comorbidity (398/992), and elevated liver enzyme with comorbidity (208/992), as compared to the younger age population (<40 years) (p>0.0001), as shown in the Table 2. It was also observed that, AST or ALT elevation was more common in the age group >40 years (p>0.0001), as shown in the Table 3.

Gender distribution

More than half of non-survivors were male (64.4%). However, mortality was not significantly different between genders (p>0.815). Males with elevated liver enzyme numbered 291/450 (64.7%) and females numbered 159/450 (35.3%). Gender-wise distribution of AST/ALT elevation also had not significantly differed (p>0.725). The analysis of gender-wise distribution of liver enzyme elevation and comorbidity was statistically significant. It was observed that males had high liver enzyme elevation (63.8%) and comorbidity (56.5%), and males also had both elevated liver enzyme and comorbidity (65.4%).

Comorbidity

The occurrence of comorbidities was: cardiovascular diseases including hypertension (180/713, 25.2%); diabetes (171/713, 24%); diabetes with hypertension (133/713, 18.7%); chronic kidney diseases (80/713, 11.2%); cancer (44/713, 6.2%); respiratory disease (34/713, 4.8%); and others (71/713, 10%). In the study population, mortality of patients with pre-existing comorbid illness with elevated liver enzyme was high at 23/73 (9.7%) when compared to patients with comorbidity alone (7.4%), patients with liver enzyme elevation alone (3.3%) or patients without liver enzyme elevation and comorbidity (1.4%). Patients with comorbidity and liver enzyme elevation had higher mortality than patients without.

Symptoms

Non-survivors were more likely to have symptoms than survivors (p<0.0001). Among symptomatic patients, the most common symptom is respiratory distress (33.6%), followed by fever with cough (9.6%), fever (6.9%), cough (4.7%), and other symptoms (2.7%). Symptomatic patients were more likely to have comorbidity with elevated liver enzyme (66.2%), with comorbid illness (63.4%), and with elevated liver enzyme (51.6%), as compared to patients without liver enzyme elevation or comorbidity (44.7%) (p<0.0001). Subgroup analysis of liver enzyme elevation did not find any statistically significant difference between the three groups.

Laboratory and clinical parameters

Various laboratory parameters and clinical parameters were assessed to study the association with outcome (discharge/death). Non-survivors had significantly higher median levels of AST (42.5 [31.25–70.25]) and ALT (32.5 [27.75–48.25]) than AST (26 [19–40]) and ALT (21 [14–34]) of survivors. The laboratory parameters such as WBC and RBC counts, hemoglobin, TGL-C, NLR, blood urea, CK-myoglobin fraction, ferritin, LDH, CRP and ALP were elevated in the poorer outcome group. Patients with lower serum albumin and lymphocyte count also had higher mortality. As shown in the Table 1, abnormal clinical parameters such as pulse rate (<60 or >100 beats/m), respiratory rate (<14 or >24 breaths per m) and low saturation (<94%) at the time of admission correlated with mortality.

Chest CT

On admission, lung involvement was more common in non-survivors than survivors (76.7% vs. 55%, p=0.001) (Table 1). The total severity CT grade was significantly higher in the non-survivor group than the survivor group (p<0.0001). By further characterizing the patients based on severity of lung involvement in non-survivors, Grade 1 was in 15/73 (20.5%), Grade 2 in 14/73 (19.2%), Grade 3 in 16/73 (21.9%) and Grade 4 in 11/73 (15.1%), suggesting severe lung involvement was common among non-survivors. A high frequency of patients [166/237 (70%)] had both elevated liver enzyme and comorbidity with abnormal chest CT than did patients with comorbidity 325/476 (68.3%) or liver enzyme elevation 133/213 (62.4%). Patients with abnormal chest CT had both AST and ALT elevated [154/212 (72.6%)] or AST elevated [74/103 (71.8%)] numbered more than patients with ALT elevated [71/135 (52.76%)].

Disease severity

Symptomatic patients with severe illness at the time of hospital admission had higher mortality (p<0.0001). A higher percentage of severe-symptom patients [103 (43.5%)] had elevated liver enzyme and presence of comorbidity than patients with comorbidity alone [181 (38%)] or liver enzyme elevation alone [52 (24.4%)]. Among patients with mild disease, 34% had elevated AST, 49.6% had elevated ALT, and 34.4% had both enzymes elevated. Among patients with moderate disease, 27.2% had elevated AST, 25.2% had elevated ALT, and 27.4% had both enzymes elevated. Whereas, among patients with severe disease, 38.8% had elevated AST, 25.2% had ALT elevation, and 38.2% had both enzymes elevated. Patients with severe disease had higher prevalence of both AST and ALT elevated or AST alone elevated than did those with ALT alone elevated (p<0.030).

Intensive care unit (ICU) admission

Most non-survivors were admitted to the ICU (80.8%). Patients with liver enzyme elevation and comorbidity were more frequently admitted to ICU (52.7%), while 47.3% of patients were managed in wards without ICU admission (54.9%). On further analysis, among patients who required ICU admission, 54.2% had both AST/ALT elevated and 48.5% had AST elevated.

Clinical outcome

AST/ALT subgroups showed a statistically significant difference between the groups for mortality. Patients with AST elevation [11/30 (10.7%)] or both AST and ALT [17/30 (8%)] elevation had higher mortality than those with only ALT elevation [2/30 (1.5%)]. Multiple variable logistic regression was assessed for poorer outcome (death). Compared with COVID-19 patients with presence of comorbidity (OR: 4.096; 95% CI: 1.833–9.157), patients with liver enzyme elevations and presence of comorbidity had higher observed death risk (OR: 5.314; 95% CI: 2.278–12.393) (Table 4).

Table 4

Multivariate analysis of elevated liver enzyme and comorbidity with COVID-19 mortality (age, gender adjusted)

CharacteristicsOR95% CI for EXP(B)p value
Normal level of liver enzyme and absence of comorbidityR
Liver enzyme elevated2.1250.7565.9740.153
Presence of comorbidity4.0961.8339.1570.001
Liver enzyme elevated with presence of comorbidity5.3142.27812.3930.0001

Discussion

In this study, clinical and laboratory parameters of 1,512 patients with COVID-19 were analyzed. We found that over 95% of the COVID-19 patients in the study population survived. Non-survivors with confirmed COVID-19 were older than 40 years of age and more likely to have elevated liver enzyme with comorbidity, compared to liver enzyme elevation or comorbidity alone. Consistent with findings reported by other authors, increased age was associated with mortality.9 It is postulated that the SARS-CoV-2 takes advantage of the natural decline in immunity in individuals with increasing age to cause severe and fatal infection. However, our study showed that age >40 years is associated with increased risk (p<0.0001). This warrants aggressive protective strategies for all persons >40 years of age to limit exposure, as active infection in such patients carries a very poor prognosis, at least for now, until a safe vaccine is developed and fully available. In this study, more than 67% (484/713) of patients had diabetes and/cardiovascular diseases as a common underlying comorbid illness. Meanwhile, a greater number of non-survivors had higher WBC count, neutrophils, NLR, and lower lymphocyte and platelet levels. This is consistent with previous findings that indicated severe patients with COVID-19 display higher neutrophil count and NLR, and lower lymphocyte count during the period of diseases.10–12 Elevated ALP is rare and has less commonly been observed among the COVID-19 liver injury patients.13 However, interestingly, our analysis found elevated ALP levels to be associated with mortality. The elevated clinical parameters such as PR, RR and decreased saturation at the time of admission were significantly associated with increased mortality. In this study, we observed that severely ill patients were more likely to die compared with the non-severe patients and that more than 71% (52/73) non-survivors were severely ill at the time of admission.

Liver enzyme abnormality is common in patients with COVID-19 at the time of hospital admission. We found that 450/1,512 (29.76%) had elevated liver enzyme. Our study showed that both AST and ALT represented the most frequently elevated pattern [212 (47.1%) of 450 patients], followed by ALT alone [135 (30%) of 450 patients] and AST alone [103 (22.9%) of 450 patients]. AST and ALT (both together) were elevated in 212/1,512 (14%) of patients at the time of hospital admission, as compared to the findings of many studies in which AST was found to be more frequently elevated than ALT.14–16 Additionally, symptomatic patients were more likely to have elevated liver enzyme (62%) at the time of hospital admission. The most common symptoms were respiratory distress, followed by cough and fever. In the present study, patients with lung involvement were more likely to have elevated liver enzyme at the time of presentation (66.4%, 299/450). Information regarding potential risks of severe conditions in COVID-19 associated with each type of liver enzyme elevation were calculated. Elevation of AST alone or ALT and AST (both together) was much more common in patients with severe disease than in patients with mild or moderate infection (p<0.030). Previous studies by Zhang et al.17 and Huang et al.18 also showed that liver enzyme abnormality was more common in patients with severe disease. A recently published meta-analysis reported pooled risk of AST elevation (OR: 3.4, 95% CI: 2.3–5.1) and risk of ALT elevation (OR: 2.8, 95% CI: 1.8–4.3) of severe COVID-19 patients.19 The findings reported may be explained by the fact that, apart from direct effects of SARS-CoV2 on liver, liver itself may also be involved in the development of Systemic Inflammatory Response Syndrome (SIRS) due to COVID-19. Further analysis showed that higher percentage of patients with AST and ALT (both together) elevated (115/212, 54.2%) needed ICU admission, suggesting that these enzyme elevation correlates with need for ICU admission, which may be revealed that hepatic dysfunction, being significantly higher in critically ill patients and associated with a poor outcome. Another study yielded similar results, showing elevated AST in 8/13 (62%) of patients in the ICU compared to 7/28 (25%) in the non-ICU setting.18 Patients with both AST and ALT elevation had a relatively higher death rate (17/30, 56.7%) and patients with AST elevated had the second-highest death rate (11/30, 36.7%), which was similar to the findings of a systematic review and meta-analysis study that found the presence of elevated liver enzyme also had statistical correlation with worse outcome (death).20

Most of the COVID-19 management protocols follow that patients with comorbidities should be closely monitored;21,22 however, specific recommendations for patients with elevated liver enzyme are sparse. The risk of comorbidities with elevated liver enzyme in COVID-19 patients had not been considered in most of the previous studies. In this large-sample-sized study, patients were categorized into four groups (patients with normal liver enzymes, liver enzyme elevation, comorbidity and liver enzyme elevation with comorbidity) and the mortality rates were 1.36%, 3.28%, 7.35%, and 9.7%, respectively. Multivariate logistic regression analysis of our study showed that liver enzyme elevation and comorbidity had the highest risk for death (OR: 5.314, 95% CI: 2.278–12.393) as compared to comorbidity alone (OR: 4.096, 95% CI: 1.833–9.157). In general, patients with liver enzyme elevated with comorbidity deteriorated more rapidly than those without liver damage and comorbidity, in which utility of liver enzyme elevation among the comorbid patients at the onset of the COVID-19 will be beneficial for stratification for aggressive early management of the disease. However, the mechanisms for increased risk for specified patients in COVID-19 should be thoroughly studied or explained in future.

Conclusions

From the present data analysis, we first conclude that comorbid illness with elevated liver enzyme at the early stage, associates with disease severity and worse clinical features. Second, we found that patients of age more than 40 years are at increased risk for severe disease, ICU admission, and mortality. Finally, logistic regression analysis suggested that elevated liver enzyme and presence of comorbidity could impart a 5-fold increase in risk for fatal outcomes of COVID-19.

Limitations

There were certain limitations in our study. First, serial liver enzyme levels during the course of hospitalization were not analyzed; as a result of which, a probability of drug-induced liver injury could not be ruled out with certainty. However, our major objective was to study patients with liver enzyme elevation at the time of hospital admission and its association with outcome. Second, patients were not followed prospectively with respect to their biochemical abnormality during their course of hospital admission; it is difficult to ascertain whether subsequent liver injury (due to sepsis, drug-induced liver injury, COVID-19 per se) affected the disease outcome and future studies should be undertaken to address this problem. Since, Covid-19 is a relatively new disease and we have limited knowledge, the full disease spectrum of the virus may unfold in the future.

Abbreviations

ALP: 

alkaline phosphatase

ALT: 

alanine aminotransferase

ARDS: 

acute respiratory distress syndrome

AST: 

aspartate aminotransferase

CI: 

confidence interval

CK: 

creatine kinase

CK-MB: 

creatine kinase myocardial band

CoV: 

coronavirus

COVID-19: 

coronavirus 2019

CRP: 

C-reactive protein

CT: 

computed tomography

ICU: 

intensive care unit

IQR: 

interquartile range

LDH: 

lactate dehydrogenase

MERS: 

middle east respiratory syndrome

NLR: 

neutrophil-to-lymphocyte ratio

OR: 

odds ratio

PCV: 

packed cell volume

PR: 

pulse rate

RBC: 

red blood cell

RR: 

respiratory rate

SARS-CoV-2: 

severe acute respiratory syndrome coronavirus 2

SpO2

oxygen saturation

TGL-C: 

triglyceride cholesterol

WBC: 

white blood cell

Declarations

Acknowledgement

We gratefully acknowledge the Government of India, Ministry of Health and Family Welfare, Department of Health Research, Multidisciplinary Research Unit (MRU), Virus Research and Diagnostic Laboratory (VRDL).

Data sharing statement

All data are available upon request.

Funding

None to declare.

Conflict of interest

The authors have no conflict of interests related to this publication.

Authors’ contributions

Overall study supervision (NK), conception of the study design, data analysis, drafting of the article, and statistical analysis (KR), assistance in drafting of the article (PB), and assistance in acquisition of data (AR, PP, MR).

References

  1. Ye ZW, Yuan S, Yuen KS, Fung SY, Chan CP, Jin DY. Zoonotic origins of human coronaviruses. Int J Biol Sci 2020;16(10):1686-1697 View Article PubMed/NCBI
  2. Hui DS, Azhar EI, Memish ZA, Zumla A. Reference Module in Biomedical Sciences. Elsevier; 2020 View Article PubMed/NCBI
  3. Lu R, Zhao X, Li J, Niu P, Yang B, Wu H, et al. Genomic characterisation and epidemiology of 2019 novel coronavirus: implications for virus origins and receptor binding. Lancet 2020;395(10224):565-574 View Article PubMed/NCBI
  4. World Health Organization. Coronavirus disease (COVID-19) weekly epidemiological update and weekly operational update. Available from: https://www.who.int/emergencies/diseases/novel-coronavirus-2019/situation-reports View Article PubMed/NCBI
  5. Wu Z, McGoogan JM. Characteristics of and important lessons from the coronavirus disease 2019 (COVID-19) outbreak in China: Summary of a report of 72,314 cases from the Chinese Center for Disease Control and Prevention. JAMA 2020;323(13):1239-1242 View Article PubMed/NCBI
  6. Guan GW, Gao L, Wang JW, Wen XJ, Mao TH, Peng SW, et al. Exploring the mechanism of liver enzyme abnormalities in patients with novel coronavirus-infected pneumonia. Zhonghua Gan Zang Bing Za Zhi 2020;28(2):100-106 View Article PubMed/NCBI
  7. Clinical management protocol: COVID-19. Available from: https://www.mohfw.gov.in/pdf/ClinicalManagementProtocolforCOVID19.pdf View Article PubMed/NCBI
  8. Annasamy C, Narayanasamy K, Karthick R. Prevalence of elevated serum aminotransferases among asymptomatic population of Tamil Nadu, India. Biomed Pharmacol J 2017;10(3):1249-1257 View Article PubMed/NCBI
  9. Price-Haywood EG, Burton J, Fort D, Seoane L. Hospitalization and mortality among black patients and white patients with Covid-19. N Engl J Med 2020;382(26):2534-2543 View Article PubMed/NCBI
  10. Qin C, Zhou L, Hu Z, Zhang S, Yang S, Tao Y, et al. Dysregulation of immune response in patients with coronavirus 2019 (COVID-19) in Wuhan, China. Clin Infect Dis 2020;71(15):762-768 View Article PubMed/NCBI
  11. Wang D, Hu B, Hu C, Zhu F, Liu X, Zhang J, et al. Clinical characteristics of 138 hospitalized patients with 2019 novel coronavirus-infected pneumonia in Wuhan, China. JAMA 2020;323(11):1061-1069 View Article PubMed/NCBI
  12. Qun S, Wang Y, Chen J, Huang X, Guo H, Lu Z, et al. Neutrophil-to-lymphocyte ratios are closely associated with the severity and course of non-mild COVID-19. Front Immunol 2020;11:2160 View Article PubMed/NCBI
  13. Cai Q, Huang D, Yu H, Zhu Z, Xia Z, Su Y, et al. COVID-19: Abnormal liver function tests. J Hepatol 2020;73(3):566-574 View Article PubMed/NCBI
  14. Guan WJ, Ni ZY, Hu Y, Liang WH, Ou CQ, He JX, et al. Clinical characteristics of coronavirus disease 2019 in China. N Engl J Med 2020;382(18):1708-1720 View Article PubMed/NCBI
  15. Richardson S, Hirsch JS, Narasimhan M, Crawford JM, McGinn T, Davidson KW, et al. Presenting characteristics, comorbidities, and outcomes among 5700 patients hospitalized with COVID-19 in the New York City Area. JAMA 2020;323(20):2052-2059 View Article PubMed/NCBI
  16. Xu L, Liu J, Lu M, Yang D, Zheng X. Liver injury during highly pathogenic human coronavirus infections. Liver Int 2020;40(5):998-1004 View Article PubMed/NCBI
  17. Zhang Y, Zheng L, Liu L, Zhao M, Xiao J, Zhao Q. Liver impairment in COVID-19 patients: A retrospective analysis of 115 cases from a single centre in Wuhan city, China. Liver Int 2020;40(9):2095-2103 View Article PubMed/NCBI
  18. Huang C, Wang Y, Li X, Ren L, Zhao J, Hu Y, et al. Clinical features of patients infected with 2019 novel coronavirus in Wuhan, China. Lancet 2020;395(10223):497-506 View Article PubMed/NCBI
  19. Wong YJ, Tan M, Zheng Q, Li JW, Kumar R, Fock KM, et al. A systematic review and meta-analysis of the COVID-19 associated liver injury. Ann Hepatol 2020;19(6):627-634 View Article PubMed/NCBI
  20. Sharma A, Jaiswal P, Kerakhan Y, Saravanan L, Murtaza Z, Zergham A, et al. Liver disease and outcomes among COVID-19 hospitalized patients - A systematic review and meta-analysis. Ann Hepatol 2021;21:100273 View Article PubMed/NCBI
  21. World Health Organization. Clinical management of severe acute respiratory infection (SARI) when COVID-19 disease is suspected: Interim guidance. Available from: https://www.who.int/docs/default-source/coronaviruse/clinical-management-of-novel-cov.%20pdf View Article PubMed/NCBI
  22. National Institutes of Health. Clinical spectrum of SARS-CoV-2 infection. Available from: https://www.covid19treatmentguidelines.nih.gov/overview/clinical-spectrum View Article PubMed/NCBI