Severe immune-related hepatitis induced by immune checkpoint inhibitors: Clinical features and management proposal - 20/04/21
PATIO groupa, b, c, d, f, g, h, i, j
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Highlights |
• | Extension of the indication of immune checkpoint inhibitors yielded to the emergence of specific liver toxicities. |
• | Liver biopsy is strongly recommended in case of grade≥3 immune-related hepatitis. |
• | The place of systemic steroids and immunosuppressive agents in severe immune-related hepatitis is controversial. |
• | Favorable outcomes may be achieved spontaneously and with no steroids in patients with severe immune-related hepatitis. |
• | Treatment with steroids should be discussed case by case with a multidisciplinary team, taken into account the bilirubin and prothrombin levels. |
• | A management algorithm for severe immune-related hepatitis is proposed. |
Summary |
Background |
Immune-related hepatitis (IRH) occurs in 1 to 18% of immune checkpoint inhibitor (ICI)-treated patients. Steroids are usually recommended for grade≥3 IRH, but their impact on IRH resolution and patient survival remains unclear.
Methods |
We retrospectively analyzed a prospective cohort of 339 patients treated at Saint-Louis Hospital (Paris, France) with ICIs for advanced melanoma. Cases of grade≥3 IRH were collected and analyzed. Two groups were compared for their biological features and time for IRH resolution and survival: patients who received steroids (steroids group: SG) and patients who did not (nonsteroids group: NSG).
Findings |
Grade≥3 IRH was observed in 21 patients. Thirteen were treated with steroids (SG), and 8 were not (NSG). The median time for toxicity resolution was 49 days in SG and 24 days in NSG (P=0.62). All but one patient showed a favorable outcome. Two-year survival was 56% in SG and 54% in NSG (P=0.83). Higher transaminase (P=0.002) and bilirubin (P=0.008) and lower prothrombin (P=0.035) levels were observed in SG than in NSG. For 8 (4 SG/4 NSG) patients, ICI was resumed without any hepatitis relapse.
Interpretation |
Favorable outcomes may be achieved spontaneously and with no steroids in patients with severe IRH. Steroid initiation should be discussed in cases of high bilirubin levels and decreased prothrombin levels. ICI could be resumed without hepatitis relapse. We propose a management algorithm for grade≥3 IRH that should be validated in larger and prospective cohorts.
Il testo completo di questo articolo è disponibile in PDF.Keywords : Melanoma, Cancer, Immune-related adverse events, Immune-related hepatitis, Immunotherapy, Ipilimumab
Abbreviations : AE, CD, CTCAE, CTLA-4, ESMO, ICI, IRAE, IRH, NSG, PD-1, PD-L1, SG
Mappa
Vol 45 - N° 2
Articolo 101491- Marzo 2021 Ritorno al numero
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