Federico Rossari, Toshifumi Tada, G. Suda, S. Shimose, Masatoshi Kudo, Changhoon Yoo, J. Cheon, F. Finkelmeier, H. Lim, J. Presa, Gianluca Masi, Francesca Bergamo, Elisabeth Amadeo, Francesco Vitiello, T. Kumada, Naoya Sakamoto, H. Iwamoto, T. Aoki, Hongjae Chon, V. Himmelsbach, Massimo Iavarone, G. Cabibbo, M. Montes, F. Foschi, C. Vivaldi, C. Soldà, T. Sho, T. Niizeki, N. Nishida, Christoph Steup, M. Hirooka, K. Kariyama, J. Tani, M. Atsukawa, K. Takaguchi, E. Itobayashi, Shinya Fukunishi, K. Tsuji, T. Ishikawa, K. Tajiri, H. Ochi, S. Yasuda, H. Toyoda, C. Ogawa, Takashi Nishimura, T. Hatanaka, Satoru Kakizaki, N. Shimada, K. Kawata, Atsushi Hiraoka, F. Tada, H. Ohama, K. Nouso, A. Morishita, A. Tsutsui, T. Nagano, N. Itokawa, T. Okubo, M. Imai, H. Kosaka, A. Naganuma, Y. Koizumi, Shinichiro Nakamura, Masaaki Kaibori, Hiroko Iijima, Y. Hiasa, M. Persano, S. Foti, S. Camera, Bernardo Stefanini, M. Scartozzi, S. Cascinu, A. Casadei‐Gardini, M. Rimini
{"title":"Disease etiology impact on outcomes of hepatocellular carcinoma patients treated with atezolizumab plus bevacizumab: a real-world, multicenter study","authors":"Federico Rossari, Toshifumi Tada, G. Suda, S. Shimose, Masatoshi Kudo, Changhoon Yoo, J. Cheon, F. Finkelmeier, H. Lim, J. Presa, Gianluca Masi, Francesca Bergamo, Elisabeth Amadeo, Francesco Vitiello, T. Kumada, Naoya Sakamoto, H. Iwamoto, T. Aoki, Hongjae Chon, V. Himmelsbach, Massimo Iavarone, G. Cabibbo, M. Montes, F. Foschi, C. Vivaldi, C. Soldà, T. Sho, T. Niizeki, N. Nishida, Christoph Steup, M. Hirooka, K. Kariyama, J. Tani, M. Atsukawa, K. Takaguchi, E. Itobayashi, Shinya Fukunishi, K. Tsuji, T. Ishikawa, K. Tajiri, H. Ochi, S. Yasuda, H. Toyoda, C. Ogawa, Takashi Nishimura, T. Hatanaka, Satoru Kakizaki, N. Shimada, K. Kawata, Atsushi Hiraoka, F. Tada, H. Ohama, K. Nouso, A. Morishita, A. Tsutsui, T. Nagano, N. Itokawa, T. Okubo, M. Imai, H. Kosaka, A. Naganuma, Y. Koizumi, Shinichiro Nakamura, Masaaki Kaibori, Hiroko Iijima, Y. Hiasa, M. Persano, S. Foti, S. Camera, Bernardo Stefanini, M. Scartozzi, S. Cascinu, A. Casadei‐Gardini, M. Rimini","doi":"10.1159/000537915","DOIUrl":null,"url":null,"abstract":"Introduction\nThe impact of etiology on response to immunotherapy in advanced hepatocellular carcinoma (HCC) is being debated, with contrasting findings between early and recent post-hoc analyses of IMbrave-150 and metanalyses of clinical trials of PD-1/PD-L1 blockers. As a results, it is not clear whether the first-line systemic treatment atezolizumab plus bevacizumab is equally effective in viral and non-viral patients.\nMethods\nWe retrospectively analyzed 885 HCC patients treated with first-line A + B from multiple centers from Eastern and Western countries, 53.9% having viral and 46.1% non-viral etiology. Baseline clinical and laboratory characteristics were analyzed with uni- and multi-variate models to explore potential differences on overall survival (OS), time to progression (TTP), disease control rates based on etiology and to identify putative prognostic factors in etiology subgroups. Treatment toxicities and access to second-line treatments and outcomes were also reported and compared between etiologies.\nResults\nOverall, no statistically significant differences were found in OS (mOS: viral 15.9 months; non-viral 16.3 months), TTP (mTTP: viral 8.3 months; non-viral 7.2 months), and disease control rates (DCR: viral 78.1%; non-viral 80.8%) based on etiology. Prognostic factors of survival and progression were mainly shared between viral and non-viral etiologies, including alpha-fetoprotein, aspartate transaminase, neutrophil-to-lymphocyte ratio (NLR) and ALBI score. Exploratory analyses highlighted a possible stronger association of immunological factors, i.e. NLR and eosinophil count, to treatment outcomes in viral patients.\nThe toxicity profile, the access to and type of second-line treatments and their outcome in terms of OS almost overlap in the two etiology subgroups. \nConclusion\nAtezolizumab plus bevacizumab efficacy does not vary according to underlying etiology of HCC in a multicenter, real-world population, matching recent post-hoc findings from the IMbrave-150 trial. Preliminary analyses suggest that some prognostic factors differ between viral and non-viral patients, potentially due to biological and immunological differences. \nProspective and comparative trials stratifying by etiology are warranted to validate these findings and guide clinical practice.","PeriodicalId":510489,"journal":{"name":"Liver Cancer","volume":"5 8","pages":""},"PeriodicalIF":0.0000,"publicationDate":"2024-04-10","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"","citationCount":"0","resultStr":null,"platform":"Semanticscholar","paperid":null,"PeriodicalName":"Liver Cancer","FirstCategoryId":"1085","ListUrlMain":"https://doi.org/10.1159/000537915","RegionNum":0,"RegionCategory":null,"ArticlePicture":[],"TitleCN":null,"AbstractTextCN":null,"PMCID":null,"EPubDate":"","PubModel":"","JCR":"","JCRName":"","Score":null,"Total":0}
引用次数: 0
Abstract
Introduction
The impact of etiology on response to immunotherapy in advanced hepatocellular carcinoma (HCC) is being debated, with contrasting findings between early and recent post-hoc analyses of IMbrave-150 and metanalyses of clinical trials of PD-1/PD-L1 blockers. As a results, it is not clear whether the first-line systemic treatment atezolizumab plus bevacizumab is equally effective in viral and non-viral patients.
Methods
We retrospectively analyzed 885 HCC patients treated with first-line A + B from multiple centers from Eastern and Western countries, 53.9% having viral and 46.1% non-viral etiology. Baseline clinical and laboratory characteristics were analyzed with uni- and multi-variate models to explore potential differences on overall survival (OS), time to progression (TTP), disease control rates based on etiology and to identify putative prognostic factors in etiology subgroups. Treatment toxicities and access to second-line treatments and outcomes were also reported and compared between etiologies.
Results
Overall, no statistically significant differences were found in OS (mOS: viral 15.9 months; non-viral 16.3 months), TTP (mTTP: viral 8.3 months; non-viral 7.2 months), and disease control rates (DCR: viral 78.1%; non-viral 80.8%) based on etiology. Prognostic factors of survival and progression were mainly shared between viral and non-viral etiologies, including alpha-fetoprotein, aspartate transaminase, neutrophil-to-lymphocyte ratio (NLR) and ALBI score. Exploratory analyses highlighted a possible stronger association of immunological factors, i.e. NLR and eosinophil count, to treatment outcomes in viral patients.
The toxicity profile, the access to and type of second-line treatments and their outcome in terms of OS almost overlap in the two etiology subgroups.
Conclusion
Atezolizumab plus bevacizumab efficacy does not vary according to underlying etiology of HCC in a multicenter, real-world population, matching recent post-hoc findings from the IMbrave-150 trial. Preliminary analyses suggest that some prognostic factors differ between viral and non-viral patients, potentially due to biological and immunological differences.
Prospective and comparative trials stratifying by etiology are warranted to validate these findings and guide clinical practice.
京公网安备 11010802042870号
京ICP备2023020795号-1
分享
求助内容:
应助结果提醒方式:
扫码关注我们
