To the Editor:
The catastrophic emergence of COVID-19 has led to large volumes of research from epicentres of infection, with some focusing on COVID-19-related liver impairment. In this regard, the study by Wang et al. published in the Journal intrigued us.1 The authors associate very minimal elevations in alanine (ALT) and aspartate aminotransferase (AST; ALT >AST) to disease severity and demonstrate ‘specific’ COVID-19-related cytopathic changes and virus-like particles on post-mortem liver histopathology (n = 2). They found that severe acute respiratory syndrome coronavirus 2 (SARS-Cov-2) caused massive apoptosis and binucleation of hepatocytes, resulting in liver enzyme abnormality and synthetic liver dysfunction, the latter in the form of hypoalbuminemia. Their painstaking work is commendable, but their assessment of clinical and investigational events may not reflect the reality. It is recommended that the ideal cut-off for diagnosing acute hepatic injury is 200 U/L and 300 U/L for AST and ALT, respectively.2 The degree of elevation in AST and ALT in the current study can only be considered an ‘altered’ liver test, not akin to acute hepatic injury. In hepatic impairment, there must be very clear evidence for metabolic (hypoglycaemia, hyperammonemia), secretory (hyperbilirubinemia) and synthetic (hypoalbuminemia, raised prothrombin time) dysfunction. Except for a mild rise in ALT and hypoalbuminemia, significant liver dysfunction is elusive in the current study. Importantly, hypoalbuminemia, in the absence of other significant liver test abnormalities, virtually rules out the hepatic origin of this abnormality. Acute liver injury is best identified by international normalized ratio >2.0, which was conspicuously absent in the current study.3 The liver biopsy findings of hepatocyte apoptosis, binuclear or occasional multinuclear syncytial hepatocytes, in the absence of viral inclusions and presence of moderate steatosis, with mild focal lobular or portal inflammation are non-specific findings that may not be related to viral cytopathy. These findings can undoubtfully be seen in sepsis and multi-organ dysfunction associated with critical illness (moderate to severe apoptosis, steatosis, lobular and portal inflammation), aging, drug-induced liver injury and fatty liver disease (binucleation or polyploidy– a feature of liver cell renewal and not injury).[4], [5], [6] The liver biopsy does not correlate with increased gamma-glutamyltransferase, which could have been secondary to the systemic illness or drug toxicity. CD68+ cellular infiltration of the hepatic sinusoids (a marker of macrophage activation) can be noted in any acute or chronic systemic inflammatory state affecting the liver, including non-alcoholic fatty liver disease (NAFLD).7 Finally, the ‘spiked’ inclusions and their degenerate components may not be of viral origin since confirmatory PCR testing for viral nucleic acids was not performed. Such ‘corona-like’ particles could be intrahepatic cholesterol crystals, lamellations, or ‘crown-like’ structures seen in patients with NAFLD. In the latter, Kupffer cells surround and engulf remnant lipid droplets (themselves granular or spiky cytoplasmic inclusions) of apoptotic hepatocytes. Moreover, associating mitochondrial changes to SARS-CoV-2 infection of hepatocytes could be erroneous. Electron microscopic changes of liver mitochondria in the form of enlarged mitochondria, intramitochondrial crystalline inclusions, mitochondrial matrix granules, vesicles containing electron-dense material in peribiliary Golgi-zone and electron-dense material accumulation in the space of Disse are notable in steatotic livers and drug-induced liver injury.8 , 9 In non-hepatotropic viral infection, such as cytomegalovirus-hepatitis, the liver involvement occurs as part of the disseminated systemic disease or secondary organ dysfunction that could be true for the SARS-CoV-2.10 To conclude, even though intriguing, the study by Wang et al. might have arrived at unfounded conclusions regarding SARS-CoV-2-related liver injury. Hepatic impairment is not confirmed, and multiple viral cytopathic effects described on liver histology may be misleading in the presence of multiple comorbidities. ‘COVID-19 induced liver injury’ may be illusory. Current research has not confirmed direct SARS-CoV-2-related liver injury, and the features described may only indicate hepatic involvement in a severe systemic inflammatory disease.
Financial support
The authors received no financial support to produce this manuscript.
Authors' contributions
CAP and RA designed the study; PA critically revised the manuscript; all authors approved the final version.
Conflict of interests
CAP received advisory and consulting fees from Cipla® (India) Ltd. RA and PA have nothing to disclose.
Please refer to the accompanying ICMJE disclosure forms for further details.
Footnotes
Supplementary data to this article can be found online at https://doi.org/10.1016/j.jhep.2020.05.025.
Supplementary data
References
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