key: cord-0704149-sz2zpuv9
authors: Singh, Ritu R.; Chhabra, Puneet; Kumta, Nikhil A.
title: Does Hyperlipasemia Predict Worse Clinical Outcomes in COVID-19? A Multicenter Retrospective Cohort Study
date: 2021-07-22
journal: J Clin Gastroenterol
DOI: 10.1097/mcg.0000000000001590
sha: 9163f3e853798c5b974101a6690d68655d4a2702
doc_id: 704149
cord_uid: sz2zpuv9

GOAL: We aim to perform a multicenter retrospective cohort study to determine if elevated serum lipase determines clinical outcomes in patients with coronavirus disease 2019 (COVID-19). BACKGROUND: Several cases of acute pancreatitis (AP) have recently been reported in association with severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) infection. Most of the evidence is based on elevated serum lipase values without objective demonstration of pancreatic inflammation or necrosis. MATERIALS AND METHODS: A population-based, multicenter, retrospective cohort study utilizing TriNetX was performed to obtain aggregated health records of ∼69 million patients from 49 health care organizations from January 1, 2020, to December 31, 2020. Adult patients (18 y and above) diagnosed with COVID-19 were identified using appropriate International Classification of Diseases, 10th Revision (ICD-10) codes and were stratified into 2 groups, with elevated (≥180 U/L) and with normal (≤80 U/L) serum lipase. The primary outcome was 30-day mortality; other outcomes were 30-day rehospitalization, need for mechanical ventilation, need for vasopressor use, acute kidney injury. RESULTS: A total of 435,731 adult patients with COVID-19 were identified, and 1406 of them had elevated serum lipase which was associated with higher 30-day mortality [risk ratio (RR)=1.53, P<0.001], risk of acute kidney injury (RR=1.5, P=0.003), and vasopressor use (RR=1.69, P<0.001) without any difference in 30-day rehospitalization (RR=0.98, P=0.54), or need for mechanical ventilation (RR=1.20, P=0.26). The negative predictive value of normal serum lipase for 3-month mortality in patients with COVID-19 was 91%. CONCLUSIONS: Patients with COVID-19 who have elevated serum lipase experience worse clinical outcomes even in the absence of AP. If these findings can be replicated in prospective studies, serum lipase can be utilized as a marker of disease severity in patients with COVID-19.

C oronavirus disease 2019 (COVID-19) is a serious disease caused by a novel strain of coronavirus, severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2). While acute respiratory illness predominates the clinical presentation of COVID-19, the spectrum of organ involvement and illness is broad. [1] [2] [3] Multiple studies have shown that gastrointestinal (GI) symptoms like abdominal pain, vomiting, and diarrhea can be the presenting manifestations of COVID-19. 4, 5 The biological plausibility of GI manifestations is understandable since angiotensin-converting enzyme II (ACE II) receptors, implicated in the SARS-CoV-2 viral entry pathway, are highly expressed in the enterocytes of the small bowel, colon, and upper esophageal stratified epithelial cells. 6 High expression of ACE II messenger RNA has also been demonstrated in pancreatic tissue and thus the potential for virus-induced pancreatic injury. 7 Retrospective studies have shown evidence of pancreatic injury in 1% to 2% of patients with nonsevere COVID-19 and in ∼17% of those with severe disease. 7, 8 Besides, there have been multiple case reports highlighting the role of SARS-CoV-2 as an etiologic agent for acute pancreatitis (AP). [9] [10] [11] [12] However, it is questionable whether these reports are true events of AP attributable to COVID-19 or represent the mere elevation of serum lipase without clinical consequences of AP. A recently published retrospective study has shown that elevated lipase is common in patients with SARS-CoV-2 infection without evidence of AP and without any influence on clinical outcome. 13 Here, we aim to perform a large multicenter retrospective study to determine the rate of elevated serum lipase in patients with COVID-19 and if it predicts worse clinical outcomes.

We performed a population-based, multicenter, retrospective cohort study utilizing TriNetX (Cambridge, MA), "A global federated health research network that provides deidentified data from electronic medical records. Protected Health information (PHI) is not available on this platform" (www.trinetx.com/page/4/#home-slider-3-copy). To fortify protected health information, TriNetX rounds up number of patients to the nearest 10 for analytic purposes. 14 We searched the TriNetX platform to obtain aggregated health records of ∼69 million patients from 49 health care organizations from January 1, 2020, to December 31, 2020. The study data was shared with all the authors who reviewed and approved the final manuscript.

Adult patients (18 y and above) diagnosed with COVID-19 were identified using appropriate ICD-10 codes, COVID-19 (U07.1), pneumonia due to SARS-associated coronavirus (J12.81) or Coronavirus infection, unspecified (B34.2). Patients with the most recent positive test result for SARS-CoV-2 RNA (TriNetX:LAB code 9088) was also identified. COVID-19 patients with elevated serum lipase above 3 times the upper limit of normal (ULN or ≥ 180 U/L) and those with normal serum lipase ( ≤ 80 U/L) were identified. Serum lipase levels within 1 week of COVID-19 diagnosis were identified using laboratory code (TriNetX: LAB code 9069). A subgroup of patients with idiopathic (K85.0), other (K85.8), or unspecified AP (K85.9) during acute illness due to COVID-19 was also identified. Common etiologies of AP were excluded. Serum ferritin level was considered markedly elevated when it was ≥ 1000 ng/mL and C-reactive protein was considered significantly elevated when it was ≥ 150 mg/L. The query builders for both the groups with elevated and normal serum lipase are available as Supplemental Files (Supplemental Digital Content 1, http://links.lww.com/JCG/A754).

We compared the group with normal serum lipase with those who had elevated serum lipase. A subgroup of patients with AP during acute illness from COVID-19 was analyzed and compared with patients who had elevated serum lipase. The primary outcome was 30-day mortality. Other outcomes were the need for mechanical ventilation, vasopressor use, acute kidney injury, and rehospitalization within 30 days. We also calculated the sensitivity, specificity, positive predictive value, and negative predictive value of elevated serum lipase in predicting mortality within 3 months in patients with COVID-19. The analyses were performed in the cohort of patients who had serum lipase value available during acute illness with COVID-19.

Mean and SD were calculated for continuous variables and proportion and percentage for dichotomous and categorical variables. Propensity score matching (1:1) was performed for baseline characteristics (age, gender, race) and common comorbidities (diabetes mellitus, obesity, malnutrition, chronic kidney disease, chronic pulmonary diseases, coronary artery disease, and heart failure). For clinical outcomes, relative risk, risk difference, and odds ratio were calculated, and Kaplan-Meir analysis with survival curve was obtained where appropriate. The statistical significance was set at a 2-sided P-value < 0.05. All the statistical analyses were performed using the TriNetX platform.

We found 435,731 adult patients from 45 health care organizations who were diagnosed with COVID-19 during the study period. Patients with elevated serum lipase values (N = 1406) and those with normal values (N = 15,849) were identified. Male patients (53% vs. 46%, P < 0.001) and those of black race (27% vs. 24%, P = 0.04) were more likely to have elevated serum lipase. Diabetes, chronic kidney disease, and chronic pulmonary disease were more frequent in patients with elevated serum lipase. A small proportion of patients with elevated serum lipase had documented abdominal pain (1.8%) and nausea or vomiting (3.2%) which was similar to those with normal serum lipase (Table 1) . AP was diagnosed in 11.8% of patients with elevated lipase compared with 1.9% of those with normal or mildly elevated lipase.

After propensity score matching, elevated serum lipase was associated with significantly higher 30-day mortality [11.31% vs. 7.40%; risk ratio (RR) = 1.53, P < 0.001] (Fig. 1) , risk of acute kidney injury (9.46% vs. 6.47%; RR = 1.52, P = 0.003), and vasopressor use (12.52% vs. 7.40%; RR = 1.69, P < 0.001) without any difference in 30-day rehospitalization (41.96% vs. 42.82%; RR = 0.98, P = 0.64), risk of acute respiratory failure or acute respiratory distress syndrome (11.45% vs. 12.02%; RR = 0.95, P = 0.64), or need for invasive mechanical ventilation (4.91% vs. 4.13%; RR = 1.2, P = 0.26). Frequency of 

This is the largest study looking at the relationship between hyperlipasemia and clinical outcomes in patients with COVID-19, to the best of our knowledge. We found that elevated serum lipase ( > 3 times ULN) in patients with COVID-19 predicts worse clinical outcomes including shortterm (30-d) mortality, acute kidney injury, and vasopressor use, even after propensity score matching for demographic characteristics and common chronic illnesses. We also performed separate analyses with serum lipase values 1 to 2 times ULN and 2 to 3 times ULN. However, there was no difference in mortality, rehospitalization, risk of acute kidney injury, or vasopressor use between those with either 1 to 2 times serum lipase elevation or 2 to 3 times serum lipase elevation compared with patients with normal serum lipase during acute COVID-19 illness (Supplement Table 1 , http:// links.lww.com/JCG/A754).

While our study adds to the emerging knowledge of hyperlipasemia in AP, its association with the worse clinical outcome has yet to be replicated in prospective studies. Our results are contrary to the results from prior retrospective studies that have shown no relationship between hyperlipasemia and clinical outcomes in patients with COVID-19; however, these results are limited by small patient samples (N < 10) and were conducted in a small geographic area. 8, 13 Our findings suggest that hyperlipasemia is not uncommon in patients with COVID-19, and there is no significant difference in the frequency of abdominal symptoms between patients who had elevated serum lipase and those with normal serum lipase. We found no difference in the clinical outcomes between COVID-19 patients who were labeled as having AP (idiopathic or other AP) when compared with all patients with elevated serum lipase. This is interesting as it might point towards overdiagnosis of AP in the setting of COVID-19 solely based on elevated serum lipase. Multiple cases of AP have been reported in association with COVID-19, however, most of these cases did not have any evidence of interstitial or necrotizing pancreatitis on cross-sectional imaging (computed tomography scan or magnetic resonance imaging). 9, 12, 15 The diagnoses were solely based on elevated serum pancreatic enzyme levels, which has been shown to be a common phenomenon in patients with COVID-19. Besides, COVID-19 is associated with several nonspecific GI symptoms making it difficult to correlate abdominal pain as a symptom of AP in the absence of imaging findings. 4,5 Some of the above cases had demonstration of AP on imaging without clear known etiology, nonetheless, it is likely that these patients represent 15% to 25% of patients with AP in whom the etiology is unknown. 16 A multicenter study has shown higher rate of idiopathic AP in patients with COVID-19 compared with those without COVID-19 (24% vs. 14%, P = 0.001). 17 Nonetheless, there are confounders and bias involved in the study that have to be considered before making any conclusions about this causal relation. Moreover, there has been a trend towards less frequent utilization of imaging modalities and invasive endoscopic procedures including endoscopic retrograde cholangiopancreatography and endoscopic ultrasound in patients with active COVID-19 to limit the transmission of the virus. This practice probably explains both, overreporting of AP solely based on elevated serum lipase and increased frequency of idiopathic AP due to missed cases of biliary sludge, microlithiasis, pancreatic cystic lesions, and early pancreatic cancer. 17 Furthermore, a multicenter, retrospective study from Spain reported a lower frequency of AP in patients with COVID-19 (odds ratio = 0.44, 95% confidence interval: 0.33-0.60). 18 Thus, the data on the incidence of AP in patients with COVID-19 appears to be inconsistent, questioning the probability of a true causal relationship.

Elevated serum lipase is considered more specific than serum amylase for the diagnosis of AP; nonetheless, there are conditions other than AP that can lead to mild to moderate lipase elevation. Among GI illnesses any form of bowel injury including enteritis, colitis or perforation can lead to hyperlipasemia without AP. Pancreatic ischemia due to systemic hypoperfusion can cause lipase elevation with or without AP. 19 Among non-GI acute illnesses, diabetic ketoacidosis has been shown to be associated with elevated lipase even in the absence of true AP. 20 We found that elevated serum lipase level had high specificity and negative predictive value for mortality (both > 90%) among patients who had serum lipase values available. This is an important finding as having a normal or near-normal serum lipase may predict better clinical outcomes and lower probability of short-term mortality in patients with COVID-19. Previous studies have shown adverse clinical outcomes in COVID-19 patients with hyperlipasemia (in the absence of AP) have not evaluated elevated serum lipase in predicting mortality or any other clinical outcome. 21, 22 While our findings are interesting and may have clinical implications in prognosticating some of the patients with COVID-19, the results must be validated in a prospective studies before clinical application.

We found that there was no difference in the rates of markedly elevated serum ferritin or C-reactive protein between patients who had elevated serum lipase compared with those who had normal serum lipase. This finding is interesting as serum lipase can complement other biomarkers of inflammation to predict disease course in patients with COVID-19.

Our study has some limitations. The retrospective study design brings with it an inherent risk of bias. Details on individual patients is lacking as the clinical data was extracted from a large database without access to protected health information. Besides, the cause of death or readmission cannot be determined in individual patients due to the study design. Nonetheless, the multicenter study design along with a large population size makes it a strong study.

Serum lipase is commonly elevated in patients with COVID-19, and it can serve as a predictor of disease severity. 

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