Copyright
©The Author(s) 2021.
World J Gastroenterol. Aug 28, 2021; 27(32): 5376-5391
Published online Aug 28, 2021. doi: 10.3748/wjg.v27.i32.5376
Published online Aug 28, 2021. doi: 10.3748/wjg.v27.i32.5376
Table 1 Incidence of severe hepatotoxicity by immunotherapy agent used as reported in key phase II and III clinical trials
| Class | Agent | Ref. | Indication | Incidence of hepatoxicity (all grades) % (no. of patients) | Incidence of ≥ grade 3 hepatoxicity % (no. of patients) |
| CTLA-4 | Ipilimumab (standard dose) 3 mg/kg | Hodi et al[71], 2018 | Melanoma | 0.3 (1/311) | 0 (0/311) |
| Weber et al[72], 2009 | Melanoma | 15.5 (9/58) | 10.3 (6/58) | ||
| Hodi et al[2], 2010 | Melanoma | 3.8 (5/131) | 0 (0/131) | ||
| Melanoma | 2.1 (8/380) Ipilimumab with gp100 | 1.1 (4/380) pilimumab with gp100 | |||
| Wolchok et al[73], 2010 | Melanoma | 26.4% (19/72) | 0 (0/72) | ||
| Robert et al[74], 2011 | Melanoma | 29.1 (72/247) | 20.6 (51/247) | ||
| Ipilimumab (high dose) 10 mg/kg | Wolchok et al[73], 2010 | Melanoma | 70.4 (50/71) | 15.5 (11/71) | |
| Tremelimumab | Ribas et al[75], 2013 | Melanoma | 0.6 (2/325) | 0.6 (2/325) | |
| Anti-PD-1 | Nivolumab | Hodi et al[71], 2018 | Melanoma | 0.3 (1/313) | 0.3 (1/313) |
| Weber et al[76], 2017 | Melanoma | 1.9 (11/576) | 0.7 (4/576) | ||
| Brahmer et al[77], 2015 | Squamous cell NSCLC | 1.5 (2/131) | 0 (0/131) | ||
| Borghaei et al[78], 2015 | Non-squamous NSCLC | 3.1 (9/287) | 0 (0/287) | ||
| Robert et al[79], 2014 | Melanoma | 1.1 (1/89) | 1.1 (1/89) | ||
| Pembrolizumab | Robert et al[79], 2014 | Melanoma | 0 (0/84) | 0 (0/84) | |
| Eggermont et al[80], 2018 | Melanoma | 1.8 (9/509) | 1.4 (7/509) | ||
| Cemiplimab | Migden et al[81], 2018 | Cutaneous Squamous-Cell Carcinoma | 8.5 (5/59) | 0 (0/59) | |
| Anti-PD-L1 | Atezolizumab | Jotte et al[82], 2020 | Squamous NSCLC | 17.4 (58/334) | 5.4 (18/334) |
| Atezolizumab + Bevacizumab (anti-VEGF antibody) | Finn et al[3], 2020 | HCC | 33.4 (110/329) | 10.6 (35/329) | |
| Avelumab | D’Angelo et al[83], 2020 | Metastatic Merkel cell carcinoma | 1.1 (1/88) | 1.1 (1/88) | |
| Durvalumab | Garassino et al[84], 2018 | Advanced NSCLC | 0.2 (1/444) | 0.2 (1/444) | |
| Combination Therapy | Ipilimumab + Nivolumab | Hodi et al[71], 2018 | Melanoma | 3.2 (10/313) | 2.6 (8/313) |
| Postow et al[85], 2015 | Melanoma | 22.3 (21/94) | 10.6 (10/94) | ||
| Larkin et al[86], 2015 | Melanoma | 17.6 (55/313) | 8.3 (26/313) | ||
| Wolchok et al[73], 2010 | Melanoma | 20.8 (11/53) | 11.3 (6/53) |
Table 2 Differential diagnosis and suggested investigations
| System | Differential diagnosis | Investigations |
| Drug-induced liver injury | (1) Other co-administered anti-cancer drugs; (2) Alcohol related liver disease; and (3) Acetaminophen toxicity | Medication history |
| Tumor-related | Metastatic disease | Abdominal imaging with ultrasound, CT or MRCP |
| Infectious | (1) Sepsis; (2) Acute HAV infection; (3) Acute HBV or flare of chronic HBV; (4) Chronic HCV; (5) Acute HEV; (6) Acute CMV or reactivation; and (7) Acute EBV | (1) Septic screen as appropriate; (2) Anti-HAV (IgM); (3) HBsAg, Anti-HBc IgG, IgM, ± HBV DNA; (4) Anti-HCV ± HCV RNA; (5) Anti-HEV (IgM); (6) CMV IgM and IgG ± CMV DNA; and (7) EBV IgM and IgG |
| Biliary disease | (1) Cholecystitis; (2) Cholangitis; and (3) Pancreatitis | (1) Abdominal imaging; and (2) Serum lipase |
| Autoimmune | Autoimmune hepatitis1 | ANA, Anti-SMA, Anti-LKM1, serum IgG levels |
| Musculoskeletal | (1) Myositis (potentially an irAEs); and (2) Rhabdomyolysis | Serum CK |
| Metabolic | Underlying NASH | (1) Metabolic risk factors; and (2) Abdominal imaging for hepatic steatosis |
| Vascular | (1) Portal-vein/hepatic vein thrombosis; and (2) Ischemic hepatitis | Abdominal imaging and clinical history |
Table 3 Comparison of common grading systems for inhibitor-related hepatotoxicity
| Grade | |||||
| Grade 1 | Grade 2 | Grade 3 | Grade 4 | Grade 5 | |
| CTCAE[87] | (1) Asymptomatic; (2) AST or ALT > 1-3 × more than ULN; and (3) T. Bil > 1-1.5 × more than ULN | (1) Asymptomatic; (2) AST or ALT > 3-5 × more than ULN; and (3) T. Bil > 1.5-3 × more than ULN | (1) Symptomatic liver dysfunction; (2) Fibrosis on biopsy; (3) Compensated cirrhosis; (4) Reactivation of chronic hepatitis; (5) AST or ALT > 5-20 × more than ULN; and (6) T. Bil > 3-10 × more than ULN | (1) Decompensated liver function (e.g., ascites, coagulopathy, encephalopathy, coma); (2) AST or ALT > 20 × more than ULN; and (3) T. Bil > 10 × more than ULN | Death due to hepatotoxicity |
| DILIN[73] | (1) Elevations in serum ALT and/or ALP levels; (2) T. Bil < 2.5 ULN; (3) INR < 1.5; and (4) Present with or without symptoms (fatigue, asthenia, nausea, anorexia, RUQ pain, jaundice, pruritus, rashes, or weight loss) | (1) Elevated serum ALT and/or ALP; (2) T. Bil ≥ 2.5 ULN or INR ≥ 1.5; and (3) Symptoms may become aggravated | (1) Elevated serum ALT and/or ALP; (2) T. Bil ≥ 5 ULN ± INR ≥ 1.5; (3) Symptoms are further aggravated; (4) Indication for hospitalization; and (5) No evidence of hepatic encephalopathy | (1) Coagulation abnormality indicated by INR ≥ 1.5; (2) Signs of hepatic encephalopathy; (3) T. Bil ≥ 10 ULN or daily elevation ≥ 1.0 mg/dL in 26 wk after the DILI onset; and (4) Ascites and DILI-related dysfunction of another organ | (1) Death due to DILI; and (2) Or need to receive liver transplantation for survival |
Table 4 Comparison of management recommendations for inhibitor-related hepatotoxicity by major expert societies
| Grade | FDA[88] | Society of Immunotherapy of Cancer[89] | American Society of Clinical Oncology[90] | European Society for Medical Oncology[91] | Australian (eVIQ Guidelines)[53] | European Association for the Study of Liver[52] |
| Grade 1 | (1) Monitor closely; (2) Continue ICI; and (3) Investigate for other causes of hepatitis | (1) Monitor closely; (2) Continue ICI; and (3) Investigate for other causes of hepatitis | (1) Monitor closely; (2) Continue ICI; (3) Check LFTs twice a week; and (4) Investigate for other causes of hepatitis | (1) Monitor closely; (2) Continue ICI; (3) Check LFTs weekly; and (4) Investigate for other causes of hepatitis | (1) Continue ICI; (2) Monitor LFTs more closely; and (3) Investigate for other causes of hepatitis | If irAEs are excluded (unlikely or unrelated) continue therapy with close follow-up. Start symptomatic treatment |
| Grade 2 | (1) Withhold ICI; (2) Investigate for other causes of hepatitis; (3) Start 0.5–1.0 mg/kg/d of prednisone Po until LFTs improve to < Grade 1 then wean steroids; and (4) Consider restarting when on less than equivalent of prednisone 7.5 mg/d | (1) Withhold ICI; (2) Investigate for other causes of hepatitis; (3) Start prednisone 0.5–1 mg/kg/d Po (or equivalent) with a 4-wk taper; (4) Monitor LFTs twice a week; (5) Liver biopsy optional; and (6) Resume ICI when steroids tapered to 10 mg/d and liver enzymes are grade 1 level or better | (1) Withhold ICI; (2) Investigate for other causes of hepatitis; (3) Monitor LFTs every 3 d and if no improvement start prednisone 0.5–1 mg/kg/d Po (or equivalent); and (4) Resume ICI when LFTs grade 1 level while on less than prednisolone 10 mg/d (taper over a month) | (1) Withhold ICI; (2) Investigate for other causes of hepatitis; (3) Recheck LFTs/INR every 3 d; (4) If LFTs increase on subsequent check after stopping checkpoint inhibitor, start oral prednisolone 1 mg/kg/d; (5) Once LFTs return to grade 1, start weaning steroids; and (6) Resume ICI when liver enzymes are grade 1 level or better while on less than prednisolone 10 mg/d | (1) Withhold ICI; (2) Monitor LFTs every 3 d; (3) Investigate for other causes of hepatitis; (4) Consider corticosteroid therapy for patients who are symptomatic or worsening LFTs; and (5) Resume ICI treatment once corticosteroid treatment is complete and tapered over 4 wk | (1) Skip dose and monitor liver parameters, INR and albumin twice weekly; (2) Start symptomatic treatment; (3) If abnormal liver parameters persist longer than 2 wk, start immunosuppression and discontinue the drug; and (4) Upon improvement immunotherapy could be resumed after corticosteroid tapering |
| Grade 3 | (1) Permanently cease ICI; (2) Start prednisone at 1–2 mg/kg/d Po (or equivalent); (3) Consider imaging and liver biopsy while assessing for alternative causes of hepatitis | (1) Permanently cease ICI; (2) Monitor complete metabolic panel every 1–2 d; (3) Start prednisone at 1–2 mg/kg/d (or equivalent); (4) If refractory to steroids, consider adding MMF. Once LFTs improve, taper over 4 wk; and (5) Consider liver biopsy | (1) Permanently discontinue medication; (2) Consider hospitalization and start IV 1–2 mg/kg/d methylprednisolone; (3) If no improvement in 3 d consider adding secondary agent; (4) Monitor LFTs daily/every other day; (5) Once LFTs improve will need to wean steroids over 4–6 wk; and (6) Do not offer infliximab | (1) Withhold ICI; (2) Investigate for other causes of hepatitis; (3) Recheck LFTs/INR daily; (4) Consider hospitalization; (5) Start prednisolone 1 mg/kg/d Po if ALT/AST < 400 U/L and normal bilirubin/albumin/INR OR start IV methylprednisolone 2 mg/kg/d if ALT/AST > 400 U/L or elevated bilirubin/INR or decreased albumin; (6) Once LFTs improve to grade 2, can switch to PO steroids and wean over 4 wk; (7) Consider rechallenge at discretion of consultant; (8) If no improvement on steroids, consider adding mycophenolate and/or tacrolimus; and (9) Do not offer infliximab | (1) Permanently discontinue treatment; (2) Investigate for other causes of hepatitis; (3) Consider liver biopsy; (4) Hospitalize patient if unwell; (5) Urgent administration of start IV 1–2 mg/kg/d methylprednisoloneFor 3 d, following high dose oral prednisolone; and (6) If no improvement on steroids, urgent referral to a gastroenterologist to prescribe other steroid-sparing agents | (1) Discontinue immunotherapy and monitor liver parameters. Consider permanent discontinuation of immunotherapy; (2) Start corticosteroids (methylprednisolone or equivalent) at a dose of 1–2 mg/kg/d depending on severity; (3) If there is no response to corticosteroids within 2–3 d, MMF should be added at 1000 mg twice daily; (4) Further immunosuppression: MMF, cyclosporine, tacrolimus, anti-thymocyte antibodies; and (5) Infliximab is not recommended |
| Grade 4 | (1) Permanently cease ICI; (2) Start prednisone at 1–2 mg/kg/d Po (or equivalent); and (3) Consider imaging and liver biopsy while assessing for alternative causes of hepatitis | (1) Permanently cease ICI; (2) Start prednisone at 1–2 mg/kg/d Po (or equivalent); (3) Monitor complete metabolic panel every 1–2 d; (4) If refractory to steroids, consider adding MMF. LFTs improve, taper over 4 wk; and (5) Consider liver biopsy | (1) Permanently discontinue medication; (2) Consider hospitalization and start IV 2 mg/kg/d methylprednisolone; (3) Add MMF if no improvement in 72 h; (4) Consider transfer to tertiary center with hepatology consultation if no improvement; (5) Do not offer infliximab; and (6) If LFTs improve, will need steroid wean over 4–6 wk | (1) Permanently discontinue medication; (2) Consider hospitalization and start IV methylprednisolone 2 mg/kg/d; (3) Formal hepatology consultation; (4) Consider liver biopsy; (5) If no improvement on IV steroids, add MMF and/or tacrolimus; (6) Do not offer infliximab; and (7) Once LFTs improve to > grade 2, can switch to oral steroids and wean over 4 wk | (1) Permanently discontinue treatment; (2) Investigate for other causes of hepatitis; (3) Consider liver biopsy; (4) Hospitalize patient if unwell; (5) Urgent administration of start IV 1–2 mg/kg/d Methylprednisolone. For 3 d, following high dose oral prednisolone; and (6) If no improvement on steroids, urgent referral to a gastroenterologist to prescribe other steroid-sparing agents |
- Citation: Remash D, Prince DS, McKenzie C, Strasser SI, Kao S, Liu K. Immune checkpoint inhibitor-related hepatotoxicity: A review. World J Gastroenterol 2021; 27(32): 5376-5391
- URL: https://www.wjgnet.com/1007-9327/full/v27/i32/5376.htm
- DOI: https://dx.doi.org/10.3748/wjg.v27.i32.5376