Annals of Hepatology (Dec 2024)

P-53 IMMUNE-MEDIATED ADVERSE EVENTS FOLLOWING ATEZOLIZUMAB PLUS BEVACIZUMAB IS ASSOCIATED WITH DECREASED SURVIVAL IN PATIENTS WITH CIRRHOSIS

  • FEDERICO PIÑERO,
  • Margarita Anders,
  • Carla Bermúdez,
  • Ezequiel Demirdjian,
  • Adriana Varón,
  • Daniela Perez,
  • Jorge Rodriguez,
  • Oscar Beltrán,
  • Javier Delgado García,
  • Leonardo Gomes da Fonseca,
  • Ezequiel Ridruejo,
  • Pablo Caballini,
  • Alexandre Araujo,
  • Juan Diego Torres Florez,
  • Juan Ignacio Marín,
  • Marina Villa,
  • Federico Orozco Ganem,
  • Jaime Poniachik,
  • Sebastián Marciano,
  • Fernando Bessone,
  • Marcelo Silva,
  • Manuel Mendizabal

Journal volume & issue
Vol. 29
p. 101667

Abstract

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Conflict of interest: No Introduction and Objectives: Clinical trials evaluating the efficacy of first line systemic immune therapies for patients with advanced hepatocellular carcinoma (HCC) have recruited a lower proportion of patients with cirrhosis. In this group of patients, immune related adverse events (irAEs) may lead to decreased prognostic outcomes. The aim of this study was describe the incidence rate of irAEs and its impact on survival. Patients / Materials and Methods: A multicenter prospective Latin-American cohort study was conducted including HCC patients who received A+B since its regional approval, either as first or sub-sequent systemic lines, to March 15, 2024. Overall survival since A+B, and survival since date of irAE was compared between patients developing and not developing irAEs (date since A+B), through Cox proportional hazard analysis (Harrell's c-index). Results and Discussion: Overall, 99 patients treated with A+B were included (n=8 received it as second line post sorafenib), 82.3% presented cirrhosis. The median treatment duration was 6 months [number of cycles 5 (range 3-11.5)], with a median overall survival of 17.0 months (range 12.6-19.8). Over a median follow-up of 7.7 months (range 4.5-17.2), the irAE incidence rate was 2.1 cases per 100 persons-months [cumulative incidence 18.1% (95% CI 11.1-27.2%); n=18]. Median time to irAE was 2.3 months (range 1.4-4.8), most frequently hepatitis (n=6), thyroiditis (n=5), and 8/18 required steroids (Table). Follow-up and treatment duration times were similar regardless irAEs occurrence. On multivariable Cox regression model, AFP values before A+B >400ng/ml [HR 2.9 (95% CI 1.1-7.6)], adjusted for HCC diffuse intrahepatic pattern was associated with irAE development (c-statistic 0.66). Patients developing irAEs presented decreased overall and post-irAE survival [median 2.9 months vs 18.5 months; HR 6.2 (95% CI 2.7-14.2); P<.0001] (Figure). Conclusions: Cautions management in patients with irAEs is of relevant importance in our region, highlighting the role of onco-hepatologists in the clinical-decision making process of these patients.