The liver in times of COVID-19: What hepatologists should know

Ridruejo, Ezequiel; Soza, Alejandro

doi:10.1016/j.aohep.2020.05.001

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Abstract

The ongoing pandemic of coronavirus disease 2019 (COVID-19) pandemic poses a serious threat to healthcare systems globally. Information regarding how the infection affects the liver and relevance of pre-existing liver disease as a risk factor for acquiring the infection or having a severe disease are still scarce. Also, considerations in liver transplant patients, those having hepatocellular carcinoma or under immunosuppressive therapy are being matter of analysis as information is being generated. Different treatments for COVID-19 are currently under study, some of which may be associated to hepatotoxicity. In the present review we discuss current data on the COVID-19 and liver, aiming to provide hepatologists with updated information to face this pandemic.

Keywords:

SARS-CoV-2

Coronavirus

Liver disease

Transplantation

Cirrhosis

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1Overview

The global pandemic of novel coronavirus disease 2019 (COVID-19) caused by severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) began in Wuhan, China, in December 2019, and has since spread worldwide [1]. On March 11, 2020, the World Health Organization (WHO) declared the SARS-CoV-2 outbreak a pandemic due to the constantly increasing number of cases outside China [2]. As of April 20, nearly 2.5 million confirmed cases and more than 155,000 deaths in 213 countries and territories worldwide had been reported in the COVID-19 pandemic, according to WHO. However, despite these increases that are widely reported, many people are being discharged from hospitals and making a full recovery.

As the number of cases grows around the globe, both through increased detection and viral spread, it is essential to develop strategies to protect persons who are most vulnerable to have severe illness from SARS-CoV-2 infection. The Centers for Disease Control and Prevention (CDC) has issued specific guidance for persons at greater risk for serious morbidity and mortality from COVID-19, including patients with chronic liver diseases among many others [3].

In this article, we review current data on how COVID-19 may affect the liver in patients with and without previous liver disease and how a pre-existing liver disease may affect COVID-19 outcomes. We aim to provide clinical hepatologists with updated information to face this pandemic in daily practice.

2General considerations

The first and most evident consequence of COVID-19 pandemic is its impact on routine care of patients with chronic liver diseases. Traditional clinical care of patients with chronic diseases in ambulatory settings changed since the appearance of this pandemic. To avoid transmission, almost all face-to-face routine controls are suspended and follow-up by telemedicine or by phone is recommended[4,5]. Telemedicine may not be available in many countries, but any means of virtual consultation must be used to avoid clinical visits.

In patients with chronic liver disease all recommendations from local authorities for the general population should be applied. Since patients with cirrhosis may be at higher risk of poor outcome, counseling about warning symptoms should be provided. Immediate contact is recommended upon the appearance of signs or symptoms compatible with COVID-19 and/or decompensated cirrhosis for urgent referral and management [5].

3Evaluating patients with COVID-19 and abnormal liver tests

Liver dysfunction may be common in patients admitted for COVID-19. Elevated alanine aminotransferase (ALT) and aspartate aminotransferase (AST) levels were reported in 16–53% of patients [6]. Patients with severe COVID-19 seem to have higher rates of liver dysfunction. In a large study from China, AST/ALT were elevated in 18.2/19.8% of patients with mild and in 39.4/28.1% with severe disease [7]. Another smaller study from China found similar results: AST was elevated in 62% of patients in the intensive care unit (ICU) compared with 25% in those who did not require care in the ICU [8]. In patients with subclinical disease, AST and ALT were elevated in 8.7 and 8.9% of patients, respectively [9]. In a study from New York, including 5700 patients, 58.4% developed AST values >40U/L and 39% ALT >60U/L [10]. In this same cohort, 56 patients (2.1%) developed acute hepatic injury defined as an elevation in AST or ALT of >15 times the upper limit of normal. Of these 56 patients, 3 were 18–65 years old (3/1373, 0.2%) and discharged alive, and 53 died: 25 were 18–65 years old (25/134, 18.7%) and 28 were >65 years old (28/469, 6.7%) [10]. Therefore, the frequency of liver dysfunction increases the more severe is the COVID-19.

Liver damage in patients with coronavirus infections might be directly caused by the viral infection of liver cells since pathological studies in patients with SARS confirmed the presence of the virus in liver tissue. Angiotensin-converting enzyme 2 (ACE2), the entry cell receptor for SARS-CoV2, is expressed in both liver cells and bile duct cells [11]. Since its expression is much higher in bile duct cells, COVID-19 liver injury appears to be more related to its damage than to liver cells injury [11]. But this remains to be confirmed in COVID-19 patients [6]. ALT/AST elevation may also be explained by drug hepatotoxicity, cytokine storm and/or pneumonia-associated hypoxia [6,11].

In most studies, liver dysfunction appears to be mild, transient, not clinically significant and to have no impact on COVID-19 outcomes [12]. Despite these results, patients with abnormal liver test of hepatocellular type or mixed type at admission had higher risk of progressing to severe disease during hospitalization in a recent study [13].

4Cirrhosis and pre-existing liver diseases

The prevalence of pre-existing liver diseases in patients with COVID-19 ranges from 2 to 11% [6]. In the New York study only 0.4% of patients had pre-existing cirrhosis [10]. Even if its impact on COVID-19 disease is yet unknown, cirrhosis has been associated with increased mortality in patients with acute respiratory distress syndrome (ARDS) [14]. Given that cirrhotics have poor immune function and worse outcomes when critically ill, more intensive surveillance or individually tailored therapeutic approaches are needed for severe patients with COVID-19 with pre-existing liver diseases [6,14].

In a study from China including 202 patients, obesity and the presence of non-alcoholic fatty liver disease (NAFLD) were independently associated with an increased risk of COVID-19 disease progression and a higher likelihood of abnormal liver function from admission to discharge [15]. Other report from China including 214 patients showed that the presence of metabolic associated fatty liver diseases (MAFLD) and obesity were associated with increased risk of severe COVID-19 disease even after adjusting for age, sex, smoking, diabetes, hypertension, and dyslipidemia [16].

Besides the care of the critically ill, the care of compensated cirrhotics remains a challenge in this COVID-19 pandemic [5,17]. As previously mentioned, telemedicine/phone contact must be used, wherever possible. Visits to specialized centers and routine laboratory testing can be postponed and can be performed locally/off-site whenever needed.

There is some controversy regarding screening procedures for varices and hepatocellular carcinoma (HCC). Even if delayed screening is safe for most patients, it may increase the relative risk of complications like variceal hemorrhage at the population level or diagnosis of HCC at a later stage [5,17]. Decision should be made according to available resources at each center and individual risk assessment. Urgent endoscopic procedures, such as variceal bleeding, bacterial cholangitis or other life-threatening conditions should not be delayed and carried out according recommendations [18].

In case of decompensated disease, care should be maintained according to guidelines but considering minimal exposure to medical staff, by using telemedicine/visits by phone wherever possible/required to avoid admission [5]. It is recommended to testing for SARS-CoV-2 in patients with acute decompensation.

5Patients with hepatocellular carcinoma

There is no information about HCC and COVID-19. Nevertheless, patients with cancer may have a higher risk of COVID-19 and poorer outcomes from COVID-19 than individuals without cancer. It is recommended to pay more intensive attention in case of rapid deterioration in patients with cancer [19].

In patients with HCC, care and treatment should be maintained according to guidelines, including continuing systemic therapies, but considering minimal exposure to medical staff, by using telemedicine/visits by phone whenever possible/required [5]. The International Liver Cancer Association (ILCA) has released a guideline with recommendations for treatment of HCC during COVID-19 pandemic that can be consulted for further information [20].

6Liver transplant candidates

The main arguments for reducing liver transplantation during the COVID-19 pandemic are: 1) The unacceptable high morbidity and mortality (20.5%) of patients undergoing elective surgery in the incubation period of COVID-19 [21]; 2) The need to reserve ICU beds and related resources for COVID-19 patients; 3) The potential risk of starting potent immunosuppressive therapy in a time of high risk of SARS-CoV-2 infection. Accordingly, it is recommended that donors and recipients are routinely tested for SARS-CoV-2 before transplantation [5]. The potential risk of nosocomial COVID-19 should be part of the consent for procedures including liver transplantation.

The COVID-19 pandemic has completely changed the way we take care of patients with cirrhosis. Reserving health resources for the sickest in an attempt to reduce hospital utilization may result in an impact in the care of patients with cirrhosis unfolding in three waves: (1) A period of resource utilization only for emergencies among patients with liver disease; (2) A “return to normal” period with increase in decompensations and overload of deferred morbidity care; (3) A protracted period of suboptimal outcomes due to missed diagnoses, disease progression, increased waiting list mortality and loss to follow-up [17]. Liver transplantation activity has decreased in most centers, many completely halting living-donor liver transplantation (LDLT). Instead of a complete shutdown of liver transplant programs, a more individualized decision should be made based on the currently available local resources and the particular phase of the pandemic.

7Post-livertransplant and patients on immunosuppression

Patients on immunosuppressive drugs – either to avoid rejection in transplanted patients or for treatment of autoimmune liver disease – are considered at higher risk of severe illness [3]. Immunosuppression may increase risk for infection or reactivation of viral agents [22] and specifically for respiratory infections such as influenza, immunocompromised patients have an increased risk for more severe disease [23]. A report from Italy shows that mortality after liver transplantation is concentrated in patients older than 65 years and transplanted more than 10 years ago [24]. Nevertheless, it is interesting to note that small series have reported good clinical outcomes of patients infected with SARS-CoV-2 while in on immunosuppression, presumably because the cytokine release syndrome with increased serum levels of IL-6, IL-8 and TNF-α is blunted in these population [25,26]. It has been reported persistent viral shedding in posttransplant patients with COVID-19 [27].

Currently there is no rationale for reducing or adjusting immunosuppressive medications in stable patients in anticipation of COVID-19. Immunizations should be encouraged, with focus on influenza and Streptococcus pneumoniae. A different setting is the patient already infected with SARS-CoV-2, in whom it should be considered reducing corticosteroid dose to a dose sufficient to avoid adrenal insufficiency. Azathioprine or mycophenolate dose may be reduced if there is lymphopenia or pulmonary deterioration [28]. Minimizing in-person visits and prioritizing telemedicine is recommended.

8Potential treatments for COVID-19 and liver implications of such therapies

At the time of writing this article, 442 interventional trials for COVID-19 are listed in ClinicalTrials.gov (162 in phase 3 and 4), but no accepted specific drug therapy has been approved. When possible and available, patients should receive these experimental therapies in the context of a clinical study. Nonetheless, many drugs are being used either off label or in compassionate use programs, therefore an understanding of potential liver-related side-effects of these medications is required.

SARS-CoV-2 is an enveloped single-stranded RNA positive-sense virus with a genome comprising 29,903 nucleotides [29]. This RNA encodes for structural and 16 non-structural proteins. Among the structural proteins, S (spike), M (membrane), E (envelope) and N (nucleocapsid) [30] are critical for virion attachment and assembly and potentially susceptible for drug/antibody inhibition. Among the 16 non-structural proteins (nsp), two proteases (3-chymotrypsin-like protease and papain-like protease), and the RNA-dependent RNA polymerase (RdRp) are some targets for drug therapy [31]. The structure of the RdRp was recently resolved [32], a step toward design of new specific antivirals.

Targeting the host immune response to the viral infection is a different approach, aiming at controlling the systemic hyperinflammation (“cytokine storm”) [33] found in patients who progress to severe stages of the disease.

A database of periodically updated drug-drug interaction between experimental COVID-19 therapies and common drugs can be reviewed at the drug interactions site of the Liverpool University (covid19-druginteractions.org). Information regarding drug-induced liver injury can be obtained in the NIH maintained site LiverTox [34].

8.1Remdesivir

Remdesivir (GS-5734), interestingly for hepatologists, is a nucleotide analog pro-drug synthesized in the quest for finding anti-hepatitis C (HCV) treatments [35,36]. It has structural similarity to tenovofir. This compound was later found to have activity against Ebola virus in animal models [37], but failed in clinical trials [38]. Remdesivir has been used in more than 500 patients for Ebola virus disease (EVD). Liver toxicity was not reported, but this is difficult to rule out, given the frequent occurrence of abnormal liver enzymes at baseline as a feature of EBD. Robust in silico, in vitro and animal models data support the anti-viral activity of remdesivir against SARS-CoV-2 and related viruses [39–42]. A recent report of compassionate use of remdesivir for COVID-19 showed promising effectivity (68% clinical improvement and 18% mortality in severe patients) [43]. This report was not controlled and excluded patients with ALT or AST>5 times the upper limit of normal. In the 53 analyzed patients, 23% patients had increased liver enzymes, leading to remdesivir discontinuation in 2 patients. No report of bilirubin elevation was mentioned. Remdesivir is an intravenous drug and currently 5- and 10-day treatment duration are being explored. No hepatic or renal adjustments are recommended, but in trials it has been used mainly with creatinine clearance >30mL/min. The cyano group in the remdesivir molecule provides specificity of action, avoiding inhibition of host mitochondrial DNA polymerase, thus reducing the potential for lactic acidosis or mitochondrial toxicity. There are at least 6 ongoing clinical trials of remdesivir for COVID-19 with several thousands of patients enrolled, all excluding patients with ALT or AST >5 times the upper limit of normal. Based on current experience of other nucleoside/nucleotide analogs in patients with cirrhosis it may be anticipated a better safety profile compared to other drug classes. It has been suggested to control liver enzymes daily if remdesivir is used [44]. No relevant drug-drug interactions are predicted for this compound. Remdesivir is likely to be the first approved anti-viral treatment for SARS-CoV-2, so – if approved – it will require collecting real world experience in registries especially when used in a more diverse population, specifically in patients with liver disease or abnormal baseline liver enzymes and patients receiving other medications to reveal any important drug interaction.

8.2Other nucleoside/nucleotide analogs

Several nucleoside/nucleotide analogs have been proposed as therapies for COVID-19. Favipravir is an approved guanine analog approved in Japan for treating infuenza. It has been explored in a small clinical trial with inconclusive results [45]. Galidesivir is an iv nucleoside analog currently in a phase 1 trial for COVID-19 in Brazil. It has been proposed that anti-HCV drugs such as sofosbuvir and ribavirin could be re-purposed for treating SARS-CoV-2 [46,47]. The hepatic safety of these compounds is largely known to hepatologists, but unfortunately to date no conclusive data is available about effectivity against COVID-19.

8.3Protease inhibitors

Lopinavir/ritonavir is an approved protease inhibitor used for HIV infection. A randomized controlled trial showed that in hospitalized patients with FiO2<94%, lopinavir/ritonavir showed no clinical benefit [48]. Hepatotoxicity was reported in 2–10%. Lopinavir/ritonavir has numerous drug-drug interactions, especially with immunosuppressive drugs such as mTOR and calcineurin inhibitors. Most centers have discontinued its use.

8.4Chloroquine/hydroxychloroquine

Chloroquine and its derivative hydroxychloroquine are old antimalarial and immunomodulatory drugs that have shown in vitro activity against SARS-CoV-2 in tissue culture, with an EC50 in the micromolar range [42,49]. The proposed mechanism of action of chloroquine is not clear. Inhibition of glycosylation of host receptors and prevention of endosome acidification may play a role in entry inhibition, but immunomodulatory mechanisms have also been proposed [50]. Hydroxychloroquine with or without azithromycin was assessed in a study of 36 patients [51]. Due to the uncontrolled nature of the study and the small sample size, no conclusive evidence of clinical efficacy could be established. Chloroquine and hydroxychloroquine have been linked to arrhythmias due to QTc prolongation. In a pre-print article a high-dose chloroquine was linked to increased mortality and led to prematurely halting the study [52]. These drugs are not usually associated to liver toxicity [53], but there are significant drug-drug interactions, particularly with anti-rejection immunosuppressants.

8.5Host mediated treatments

Tocilizumab is a humanized monoclonal antibody against the interleukin 6 (IL-6) receptor that is being used in patients in advanced stages of the disease to treat the cytokine release syndrome [54]. Small series and case reports suggest beneficial effects [55,56], but there are no results of randomized controlled trials. Liver enzyme elevation is common with tocilizumab, but only rarely linked to severe liver injury [57]. Tocilizumab increases the risk of hepatitis B virus (HBV) reactivation [58].

9Teaching and research activities

Clinical activity is inseparable from teaching and research, and hepatology is no exception. Medical students and residents rotating in different departments are potential vectors of COVID-19. At the same time, they have an enormous opportunity to contribute to patient care and learn invaluable lessons from this pandemic [59]. In a bold move, Italy decided to rush 10,000 interns into service, as the medical services started to collapse [60]. Two main challenges arise in the current situation: (1) Ensuring adequate protection and safety of all health personnel, including medical students and residents. (2) Adapting medical education to flexible online methods to avoid important gaps in the medical curriculum. This requires flexibility and creativity.

A flood of publications regarding COVID-19 has emerged since January 2020. It has been criticized that in the pursuit of getting fast publication, the quality of the research and peer evaluation has suffered. Papers in preprint servers (not peer-reviewed) are being cited more than ever. Many investigators are turning their energy to study the effect of this infection in patients in their respective fields, organizing patient registries and writing recommendations for societies. It is advised that hepatologists maintain a high degree of skepticism while reading the medical literature. Engaging with journalists to accurately translate technical information and correcting erroneous information in social media is also advisable to fight misinformation and fake news.

Clinical research unrelated to COVID-19 has been greatly altered during this pandemic, due to quarantines and concerns regarding patient an research team safety. The FDA issued a guidance calling for ensuring safety of clinical trials participants and flexibility for amending clinical protocols, particularly for including alternatives to in-patient visits [61]. Basic research has been similarly affected. One potential positive side of the situation is that researchers in quarantine may have more time to focus on writing, which has resulted in an uptick in the number of new submissions for some journals [62] and also an increase in the request for reviewing papers.

10Conclusion

Pre-existing liver disease appears to have little impact on COVID-19 outcomes. ALT/AST abnormalities are common, especially in patients with severe disease, but its impact is unknown. There are many explanations for these abnormalities. Further research should focus on the causes of liver injury in COVID-19 and the effect of existing liver-related comorbidities on treatment and outcomes of COVID-19. Its outcomes and different factors influencing it may vary between countries and between continents. Local information from each country is particularly important to understand this heterogenous disease.

There is no doubt that COVID-19 is having a major impact on clinical practice and patient care. Although all attention is focused today on COVID-19, the care of patients with chronic diseases should not be neglected, since this could have catastrophic outcomes.AbbreviationsCOVID-19

coronavirus disease 2019

SARS-CoV-2

severe acute respiratory syndrome coronavirus 2

WHO

World Health Organization

CDC

Centers for Disease Control and Prevention

ALT

alanine aminotransferase

AST

aspartate aminotransferase

ICU

intensive care unit

ACE2

angiotensin-converting enzyme 2

ARDS

acute respiratory distress syndrome

NAFLD

non-alcoholic fatty liver disease

MAFLD

metabolic associated fatty liver diseases

HCC

hepatocellular carcinoma

ILCA

International Liver Cancer Association

IL

interleukin

TNF-α

tumor necrosis factor-alpha

nsp

non-structural proteins

RdRp

RNA-dependent RNA polymerase

NIDDK

National Institute of Diabetes and Digestive and Kidney Diseases

EVD

Ebola virus disease

HBV

hepatitis B virus

Conflict of interest

AS declares being the receiver of an investigator initiated research grant from Gilead and having stock ownership in Gilead Sciences Inc.

Funding

This study was funded by grant FONDECYT N°1191389 from CONICYT (Comité Nacional de Ciencia y Tecnología) to A.S.

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