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Hepatic Injury Induced by a Single Dose of Nivolumab – a Case Report and Literature Review


Authors: J. Kopecký 1;  O. Kubecek 1;  T. Geryk 2;  M. Podhola 2;  M. Ziaran 1;  P. Priester 1;  M. Hanisova 1;  S. Borilova 1
Authors‘ workplace: Department of Oncology and Radiotherapy, Faculty of Medicine, University Hospital Hradec Kralove 1;  The Fingerland Department of Pathology, Faculty of Medicine, University Hospital Hradec Kralove 2
Published in: Klin Onkol 2019; 32(2): 133-138
Category: Case Report
doi: https://doi.org/10.14735/amko2019133

Overview

Background: The use of nivolumab in the treatment of metastatic melanoma has become well established during past years. Despite its undeniable efficacy, immune-related side effects may occur, including acute liver injury. Liver toxicity caused by nivolumab is usually observed as liver enzyme elevation with mild or no symptoms; further, there is limited information regarding any histopathological findings.

Case:We report a case of a 38-year-old woman with metastatic melanoma who developed unusual nivolumab-induced hepatic injury after a single dose of nivolumab. A liver biopsy was performed to assess the aetiology of hepatic lesions as no other analysis concerning biochemistry, virology, autoantibodies, nor imaging studies revealed any pathology. The histopathological analysis showed an oedema in the portal fields and mixed inflammation consisting of eosinophilic and neutrophilic granulocytes. The major finding was a prominent, predominantly intracellular, cholestasis.

Conclusion:To our knowledge, no such histopathological pattern of liver injury has been described in relation to nivolumab therapy elsewhere. This type of liver injury shows higher resistance to corticosteroids, which may warrant upfront high-dose corticotherapy combined with other immunosuppressive agents, including mycophenolate mofetil. This case highlights a necessary awareness regarding immunotherapy-related adverse events, which could be severe and potentially life-threatening.

Keywords:

nivolumab – hepatitis – toxicity – corticosteroids – autoimmunity

Introduction

The use of nivolumab in the treatment of metastatic melanoma has become well established during past years [1]. Nivolumab, a human monoclonal antibody targeting the programmed cell death receptor 1 (PD-1), has proven to be of great benefit in overall survival in patients with metastatic malignant melanoma; however, despite its undeniable efficacy, major side effects may occur. These are usually immune-related and may be present in various forms, including acute liver injury, a potentially serious and life-threatening event. Although the liver toxicity of nivolumab has been reported in clinical trials, it is usually described as increased liver enzyme, with none or limited information regarding histopathological observations. The risk of severe immune-related hepatic injury is generally considered to be lower and less common with anti-PD-1 therapy when compared to anti-CTLA-4 antibodies [2,3].

Herein, we report a case of unusual onset of nivolumab-induced hepatic injury after a single dose of nivolumab. Furthermore, we provide a thorough histopathological study of the liver tissue specimen and discuss possible pathogenesis and treatment options.

Case report

The present study concerns the case of a 38-year-old woman with metastatic melanoma (Schema 1) who developed severe hepatic injury after the first dose of nivolumab. Fourteen days following the introduction of nivolumab therapy, the patient visited the outpatient clinic to obtain a second dose; she had no symptoms of immune-related adverse events (irAE). However, the laboratory tests revealed severe increment of liver enzymes and bilirubin (alanine aminotransferase – ALT, aspartat aminotransferase – AST, bilirubin, and gamma-glutamyl transferase – GGT) shown in Graph 1 leading to immediate hospital admission. The patient had no past medical history of liver disease, elevated liver enzymes, drug-induced liver injury, autoimmune disorders or any other significant comorbidities. There were no signs of metastatic involvement of the liver on previous computed tomography (CT) and current ultrasound imaging studies. Her medication did not include any drugs with known liver toxicity except for levetiracetam 1,500 mg/day, administered as antiepileptic prophylaxis for brain metastases. Taking into account that rare cases of levetiracetam-induced hepatic failure were reported [4], the medication was switched to a less hepatotoxic drug, lamotrigine. However, considering that the liver functions did not resolve after cessation of levetiracetam, it was ruled out as a possible cause of liver toxicity and returned to the patient’s medication.

Schema 1. Disease history timeline.
Schema 1. Disease history timeline.

1. 1. Development of liver enzymes and therapeutical interventions.
1. Development of liver enzymes and therapeutical interventions.
Arrows indicate day and manner of intervention: 1) methylprednisolon 2 mg/kg/day; 2) corticosteroids 4 mg/kg/day + mycophenolate mofetil 2 g/day; 3) methylprednisolon 6 mg/kg/day; 4) tapering of methylprednisolon to 2 mg/kg/day; 5) methylprednisolon 4 mg/kg/day.

In order to exclude all possible causes of liver injury, we performed a broad evaluation spectrum. At the beginning, drug or herbal intoxication was excluded, and the patient was tested for a panel of viral infections (human immunodeficiency virus – HIV, cytomegalovirus – CMV, Epstein-Barr virus – EBV, herpes simplex virus type 1 – HSV-1, herpes simplex virus type 2 – HSV-2, hepatitis A virus – HAV, hepatitis B virus – HBV, hepatitis C virus – HCV, hepatitis E virus – HEV) with negative results. A screening for possible iron and copper metabolism disorders was also negative. The imaging methods showed no biliary tree distension, no signs of new liver metastases, nor brain metastases progression. Taking a step further, the patient was tested for possible autoimmune diseases, involving the assessment of autoantibodies (i.e. anti-neutrophil cytoplasmic antibodies – ANCA, anti-mitochondrial antibodies – AMA, anti-nuclear antibodies – ANA, antibodies to smooth muscle – SMA, anti-liver-kidney microsome antibodies – anti-LKM, anti-soluble liver antigen antibodies – anti-SLA, antibody to liver cytosol – anti-LC-1, and rheumatoid factor), all of which were negative.

Considering that none of the previous tests provided any significant information regarding the aetiology of the hepatic lesion, the decision to perform a liver biopsy was made. The histopathological evaluation showed an oedema in the portal fields and mixed inflammation consisting of eosinophilic and neutrophilic granulocytes. The major finding was a perivenular (zone 3) cholestasis. Fig. 1 shows the presence of bile both within the liver cell cytoplasm and the dilated canaliculi.

1. Histological samples of liver tissue.
Histological samples of liver tissue.
Hematoxylin and eosin staining showing the portal fields with mixed inflammation and predominantly intracelullar and canalicular cholestasis.

Following the recommendations for irAE management, the patient was started on methylprednisolone i.v. 2 mg/kg/day. Considering that the laboratory results and symptoms did not improve after a week of therapy, the dose of methylprednisolone was raised to 4 mg/kg/day and further to 6 mg/kg/day. Because of further deterioration of the clinical symptoms (jaundice, itching), the case was discussed within a multidisciplinary board, including gastroenterologists and a neurologist, and the patient was started on mycophenolate mofetil 1g BID and acidum ursodeoxycholicum 1,500 mg/day (Graph 1).

While on combined immunosuppressive therapy, the patient developed multiple side effects, including blood count alteration (thrombocytopenia and neutropenia), thyroid function alteration (decreased thyroid-stimulating hormone), muscle weakness, loss of appetite, and mental discomfort. Considering this, together with partial restoration of liver function, we started to gradually taper the doses of corticosteroids and mycophenolate mofetil (Graph 1).

Despite the use of antibiotics and antimycotics prophylaxis (fluconazole, co-trimoxazole) during the immunosuppressive therapy, the patient developed a mild respiratory infection, which was promptly managed with antibiotics (cefotaxime).

Because of neurological symptoms (epileptic seizures, weakness of muscles with hemiplegic left upper extremity) recurring despite sufficient plasma levels of anti-epileptic drugs, progression of GGT and bilirubin serum levels, we performed brain magnetic resonance imaging and a chest, abdomen, and pelvis CT scan. There were no new metastatic lesions in the brain. However, the CT scan revealed metastases progression in lungs, adrenal glands and liver. The limited therapeutic possibilities and unfavourable prognosis was thoroughly discussed with the patient and her family. The consensus was made to provide the best supportive care. The patient eventually died 74 days following the first dose of nivolumab due to tumour progression.

Discussion

The introduction of immune checkpoint inhibitors has dramatically improved the prognosis of patients with metastatic melanoma; in this regard, nivolumab has significantly improved overall survival when compared to ipilimumab or to chemotherapy [1,5].

Despite the important clinical benefits of nivolumab, immune checkpoint inhibition is associated with a broad spectrum of side effects, usually termed as irAEs, resulting from its mechanism of action, i.e. immune response enhancement [6].

Overall, the safety profile of nivolumab is favourable and any possible AEs are manageable and generally consistent. IrAEs include dermatologic, gastrointestinal, hepatic, endocrine, and other less common inflammatory events. There is no obvious pattern in the incidence, severity, or relation to nivolumab dosage. Most irAEs are of low-grade (i.e. grade 1–2) with relatively few of high-grade (i.e. grade 3–4). Most high-grade events are managed with corticosteroids, tumour necrosis factor-alpha antagonists, or mycophenolate mofetil [7].

Although nivolumab-related liver toxicity has been reported in the past, it was usually present in low-grade form. In this regard, patients treated with nivolumab monotherapy within clinical trials (CA209066, CA209037, CA209067, CA209017, CA209057, CA209063, CA209025, CA209205, and CA209039), showed a 6.9% incidence of liver function abnormalities. An estimated 5.1% of patients presented usually mild effects (i.e. grade 1 or 2), whereas only 1.9% were classified as grade 3 or 4. The onset of liver toxicity was usually observed after two to six cycles 1–3 months after treatment initiation (median 1.9 month). With appropriate medical therapy, most of these irAEs were resolved within a median of 5.4 weeks. Permanent discontinuation of the treatment was required in only 0.9% of patients [1,8–14].

Hepatic AEs induced by PD-1 inhibitors commonly shown as an asymptomatic increment of AST and ALT, and rarely of total bilirubin. Symptoms such as fatigue, fever, and hepatomegaly, detected by imaging methods, may also occur [15].

A correct diagnosis, along with the assessment of a hepatic lesion aetiology, requires the combination of laboratory tests and a liver biopsy; however, it may still be challenging to reveal the aetiology of the hepatic lesion. Clinical data may provide further information and aid in determining the diagnosis, i.e. the relation between therapy start and hepatotoxicity onset, resolution time after drug cessation, time of recurrence upon re-challenge, and previous evidence of drug hepatotoxicity [16]. The differential diagnosis includes drug-induced liver injury, idiopathic autoimmune hepatitis, acute viral hepatitis, and acute alcoholic liver disease. Distinguishing between idiopathic autoimmune hepatitis and drug-induced liver injury is much more challenging in case of immunotherapy, as these two forms of liver injury have similar clinical features [17].

Further information regarding any histopathological findings in patients with anti-PD-1 induced liver injury is rather scarce. Although there are some reports (usually individual case reports or small case series) of anti-CTLA-4 monoclonal antibodies induced liver toxicity [18,19] with a similar pattern of liver injury caused by anti-PD-1 therapy. Histopathological findings of liver injury associated with anti-CTLA-4 therapy are usually described as acute hepatitis-like pattern with focal or confluent necrosis and prominent portal inflammation. However, other pathological patterns have been reported and some proportion of cholestasis may also be present in some cases. The inflammatory infiltrate is composed predominantly of CD8+ T-lymphocytes, admixed histiocytes, scattered plasma cells, and eosinophils [18–20].

To the best of our knowledge, there are only two reported cases, including the histopathological findings of nivolumab-induced liver injury in a patient with lung cancer and glioblastoma [21,22], but none in melanoma. In the first case, the liver biopsy showed a moderate lymphocytic inflammatory infiltrate with bile duct injury and mild periportal necrosis. Immunohistochemical staining revealed the prevalence of CD3+CD8+ lymphocytes in the portal tract. In the latter case, the hepatocytes showed a diffuse cytoplasmic clearing, with occasional macro-vacuolar steatosis in the centrilobular area. The steatotic hepatocytes were surrounded by a rich inflammatory infiltrate, while in the portal tract, only a minimal fibrosis and scattered inflammatory cells were found. Again, the inflammatory infiltrate was represented mostly by CD8+ cytotoxic lymphocytes, diffusely scattered within the parenchyma.

In our case, the evaluation of the liver tissue by CD3/CD8 immunohistochemical staining and PD-L1 expression analysis showed only a small number of CD8+ cells in liver sinusoids and portal fields, whereas CD3+ cell presence was much richer at these sites. The CD3: CD8 ratio was 5: 1 in favour of CD3+ cells. PD-L1 expression was mainly detected in the endothelial cells of liver sinusoids and, sporadically, in Kupffer cells; however, it was absent in hepatocytes.

Taking into account our findings with available case reports, it could be suggested that anti-PD-1 induced liver injury likely represents heterogeneous forms of disease, ranging from autoimmune hepatitis to other forms with predominant cholangitic liver disease. In contrast to both cases mentioned above, we present a new histopathological pattern involving intracellular and canalicular cholestasis with only a mild inflammatory infiltrate. In a similar manner to the case with cholangitic hepatitis [21], we also observed a worse response to corticosteroids; therefore suggesting that a predominant cholangiolitic pattern of liver injury might require different and much more intensive therapeutic strategies. However, the specific mechanisms involved in nivolumab-induced liver injury are currently unknown.

Hepatitis with cholestasis may be induced by a wide spectrum of drugs [17]. Cholestatic patterns of liver injury can be divided into three basic categories – acute (bland or intrahepatic) cholestasis, chronic cholestasis, and a type of cholestasis termed as “cholestatic hepatitis”. The histopathological findings in acute cholestasis usually involve bile plugs in canaliculi and bile accumulation in hepatocytes, particularly in zone 3, accompanied with mild inflammation. Chronic cholestasis pattern shows cholate stasis and periportal copper accumulation with some degree of induct injury. Histopathological findings of cholestatic hepatitis show a variable spectrum of inflammation and cholestasis, ranging from cases of acute hepatitis, involving a cholestatic component, to cases with minimal inflammation. The degree of inflammation in cholestatic hepatitis, predominantly consisting of neutrophilic infiltrates, tends to be less severe compared with a case of pure acute or chronic hepatitis [23].

In order to identify the correct cause of liver injury, cooperation within a multidisciplinary team, involving gastroenterologists, radiologists and preferably also pathologists, is important. The symptoms and findings might mimic other conditions, such as autoimmune hepatitis, primary biliary cholangitis, primary sclerosing cholangitis, viral hepatitis, or tumour progression, which need to be ruled out before being able to diagnose nivolumab induced immune-related liver injury.

Corticosteroids therapy is the mainstay of irAE management, in which the dose depends on a toxicity grade ranging from 0.5 to 2 mg/kg/day [24–26]. The response to corticosteroid therapy in immune mediated liver injury can be variable, especially in presence of a non-typical cholangitic pattern. When concerning our case (or a previously reported lung cancer case) [21], the response seems to be slower and the condition more resistant to immunosuppressive therapy; therefore, a higher initial dose of corticosteroids may be required. Alternatively, other immunosuppressive drugs, such as mycophenolate mofetil can be used. Regardless, it must be emphasised that patients treated with corticosteroids i.v. therapy are especially prone to infectious complications and adequate care should be paid to this issue.

Conclusion

Our case report shows the importance of vigilance from the first application of nivolumab and the necessity of regular follow-up. Special attention must be given to the fact that hepatotoxicity might represent a severe complication of immunotherapy with a potentially fatal outcome. In concordance with previously published data, we demonstrate that cholestatic hepatitis shows a poor response to corticosteroid therapy and may justify more potent upfront immunosuppressive treatment. In order to collect more data regarding histopathological patterns associated with anti-PD-1 therapy induced liver toxicity, liver biopsy in patients with severe hepatotoxicity is warranted.

The study was supported by the Charles University Faculty of Medicine in Hradec Kralove grant SVV- 2016-260286 and UK Progres Q40/06.

The authors declare they have no potential conflicts of interest concerning drugs, products, or services used in the study.

The Editorial Board declares that the manuscript met the ICMJE recommendation for biomedical papers.

 MUDr. Jindřich Kopecký, Ph.D.

Department of Oncology and Radiotherapy University Hospital Hradec Kralove

Sokolska 581 50 005 Hradec Kralove

e-mail: kopecjin@fnhk.cz

Submitted: 31. 12. 2018

Accepted: 20. 2. 2019


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