Disease Etiology Impact on Outcomes of Hepatocellular Carcinoma Patients Treated with Atezolizumab plus Bevacizumab: A Real-World, Multicenter Study

Federico Rossari; Toshifumi Tada; Goki Suda; Shigeo Shimose; Masatoshi Kudo; Changhoon Yoo; Jaekyung Cheon; Fabian Finkelmeier; Ho Yeong Lim; José Presa; Gianluca Masi; Francesca Bergamo; Elisabeth Amadeo; Francesco Vitiello; Takashi Kumada; Naoya Sakamoto; Hideki Iwamoto; Tomoko Aoki; Hong Jae Chon; Vera Himmelsbach; Massimo Iavarone; Giuseppe Cabibbo; Margarida Montes; Francesco Giuseppe Foschi; Caterina Vivaldi; Caterina Soldà; Takuya Sho; Takashi Niizeki; Naoshi Nishida; Christoph Steup; Masashi Hirooka; Kazuya Kariyama; Joji Tani; Masanori Atsukawa; Koichi Takaguchi; Ei Itobayashi; Shinya Fukunishi; Kunihiko Tsuji; Toru Ishikawa; Kazuto Tajiri; Hironori Ochi; Satoshi Yasuda; Hidenori Toyoda; Chikara Ogawa; Takashi Nishimura; Takeshi Hatanaka; Satoru Kakizaki; Noritomo Shimada; Kazuhito Kawata; Atsushi Hiraoka; Fujimasa Tada; Hideko Ohama; Kazuhiro Nouso; Asahiro Morishita; Akemi Tsutsui; Takuya Nagano; Norio Itokawa; Tomomi Okubo; Michitaka Imai; Hisashi Kosaka; Atsushi Naganuma; Yohei Koizumi; Shinichiro Nakamura; Masaaki Kaibori; Hiroko Iijima; Yoichi Hiasa; Mara Persano; Silvia Foti; Silvia Camera; Bernardo Stefanini; Mario Scartozzi; Stefano Cascinu; Andrea Casadei-Gardini; Margherita Rimini

doi:10.1159/000537915

Disease Etiology Impact on Outcomes of Hepatocellular Carcinoma Patients Treated with Atezolizumab plus Bevacizumab: A Real-World, Multicenter Study

Federico Rossari, Toshifumi Tada, Goki Suda, Shigeo Shimose, Masatoshi Kudo, Changhoon Yoo, Jaekyung Cheon, Fabian Finkelmeier, Ho Yeong Lim, José Presa, Gianluca Masi, Francesca Bergamo, Elisabeth Amadeo, Francesco Vitiello, Takashi Kumada, Naoya Sakamoto, Hideki Iwamoto, Tomoko Aoki, Hong Jae Chon, Vera HimmelsbachMassimo Iavarone, Giuseppe Cabibbo, Margarida Montes, Francesco Giuseppe Foschi, Caterina Vivaldi, Caterina Soldà, Takuya Sho, Takashi Niizeki, Naoshi Nishida, Christoph Steup, Masashi Hirooka, Kazuya Kariyama, Joji Tani, Masanori Atsukawa, Koichi Takaguchi, Ei Itobayashi, Shinya Fukunishi, Kunihiko Tsuji, Toru Ishikawa, Kazuto Tajiri, Hironori Ochi, Satoshi Yasuda, Hidenori Toyoda, Chikara Ogawa, Takashi Nishimura, Takeshi Hatanaka, Satoru Kakizaki, Noritomo Shimada, Kazuhito Kawata, Atsushi Hiraoka, Fujimasa Tada, Hideko Ohama, Kazuhiro Nouso, Asahiro Morishita, Akemi Tsutsui, Takuya Nagano, Norio Itokawa, Tomomi Okubo, Michitaka Imai, Hisashi Kosaka, Atsushi Naganuma, Yohei Koizumi, Shinichiro Nakamura, Masaaki Kaibori, Hiroko Iijima, Yoichi Hiasa, Mara Persano, Silvia Foti, Silvia Camera, Bernardo Stefanini, Mario Scartozzi, Stefano Cascinu, Andrea Casadei-Gardini^*, Margherita Rimini

^*この論文の責任著者

内科学（第三）講座

研究成果: ジャーナルへの寄稿 › 学術論文 › 査読

6 被引用数 (Scopus)

抄録

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 (A + B) is equally effective in viral and nonviral patients. Methods: We retrospectively analyzed 885 HCC patients treated with the first-line A + B from multiple centers from Eastern and Western countries, 53.9% having viral and 46.1% nonviral etiology. Baseline clinical and laboratory characteristics were analyzed with uni- and multivariate models to explore potential differences on overall survival (OS), time-to-progression (TTP), disease control rates (DCRs) based on etiology and to identify putative prognostic factors in etiology subgroups. Treatment toxicities and access to the second-line treatments and outcomes were also reported and compared between etiologies. Results: Overall, no statistically significant differences were found in median OS (mOS: viral 15.9 months; nonviral 16.3 months), TTP (mTTP: viral 8.3 months; nonviral 7.2 months), and DCRs (viral 78.1%; nonviral 80.8%) based on etiology. Prognostic factors of survival and progression were mainly shared between viral and nonviral 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 the 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 nonviral 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.

本文言語	英語
ページ（範囲）	522-536
ページ数	15
ジャーナル	Liver Cancer
巻	13
号	5
DOI	https://doi.org/10.1159/000537915
出版ステータス	出版済み - 2024/04/10

ASJC Scopus 主題領域

肝臓学
腫瘍学

UN SDG

この成果は、次の持続可能な開発目標に貢献しています

文献へのアクセス

10.1159/000537915

フィンガープリント

「Disease Etiology Impact on Outcomes of Hepatocellular Carcinoma Patients Treated with Atezolizumab plus Bevacizumab: A Real-World, Multicenter Study」の研究トピックを掘り下げます。これらがまとまってユニークなフィンガープリントを構成します。

引用スタイル

Rossari, F., Tada, T., Suda, G., Shimose, S., Kudo, M., Yoo, C., Cheon, J., Finkelmeier, F., Lim, H. Y., Presa, J., Masi, G., Bergamo, F., Amadeo, E., Vitiello, F., Kumada, T., Sakamoto, N., Iwamoto, H., Aoki, T., Chon, H. J., ... Rimini, M. (2024). Disease Etiology Impact on Outcomes of Hepatocellular Carcinoma Patients Treated with Atezolizumab plus Bevacizumab: A Real-World, Multicenter Study. Liver Cancer, 13(5), 522-536. https://doi.org/10.1159/000537915

@article{54d34c07abf644f6b942678174f45dcd,

title = "Disease Etiology Impact on Outcomes of Hepatocellular Carcinoma Patients Treated with Atezolizumab plus Bevacizumab: A Real-World, Multicenter Study",

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 (A + B) is equally effective in viral and nonviral patients. Methods: We retrospectively analyzed 885 HCC patients treated with the first-line A + B from multiple centers from Eastern and Western countries, 53.9% having viral and 46.1% nonviral etiology. Baseline clinical and laboratory characteristics were analyzed with uni- and multivariate models to explore potential differences on overall survival (OS), time-to-progression (TTP), disease control rates (DCRs) based on etiology and to identify putative prognostic factors in etiology subgroups. Treatment toxicities and access to the second-line treatments and outcomes were also reported and compared between etiologies. Results: Overall, no statistically significant differences were found in median OS (mOS: viral 15.9 months; nonviral 16.3 months), TTP (mTTP: viral 8.3 months; nonviral 7.2 months), and DCRs (viral 78.1%; nonviral 80.8%) based on etiology. Prognostic factors of survival and progression were mainly shared between viral and nonviral 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 the 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 nonviral 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.",

keywords = "Atezolizumab, Bevacizumab, Etiology, Hepatocellular carcinoma, Immunotherapy, Non-alcoholic steatohepatitis, Viral hepatitis",

author = "Federico Rossari and Toshifumi Tada and Goki Suda and Shigeo Shimose and Masatoshi Kudo and Changhoon Yoo and Jaekyung Cheon and Fabian Finkelmeier and Lim, {Ho Yeong} and Jos{\'e} Presa and Gianluca Masi and Francesca Bergamo and Elisabeth Amadeo and Francesco Vitiello and Takashi Kumada and Naoya Sakamoto and Hideki Iwamoto and Tomoko Aoki and Chon, {Hong Jae} and Vera Himmelsbach and Massimo Iavarone and Giuseppe Cabibbo and Margarida Montes and Foschi, {Francesco Giuseppe} and Caterina Vivaldi and Caterina Sold{\`a} and Takuya Sho and Takashi Niizeki and Naoshi Nishida and Christoph Steup and Masashi Hirooka and Kazuya Kariyama and Joji Tani and Masanori Atsukawa and Koichi Takaguchi and Ei Itobayashi and Shinya Fukunishi and Kunihiko Tsuji and Toru Ishikawa and Kazuto Tajiri and Hironori Ochi and Satoshi Yasuda and Hidenori Toyoda and Chikara Ogawa and Takashi Nishimura and Takeshi Hatanaka and Satoru Kakizaki and Noritomo Shimada and Kazuhito Kawata and Atsushi Hiraoka and Fujimasa Tada and Hideko Ohama and Kazuhiro Nouso and Asahiro Morishita and Akemi Tsutsui and Takuya Nagano and Norio Itokawa and Tomomi Okubo and Michitaka Imai and Hisashi Kosaka and Atsushi Naganuma and Yohei Koizumi and Shinichiro Nakamura and Masaaki Kaibori and Hiroko Iijima and Yoichi Hiasa and Mara Persano and Silvia Foti and Silvia Camera and Bernardo Stefanini and Mario Scartozzi and Stefano Cascinu and Andrea Casadei-Gardini and Margherita Rimini",

note = "Publisher Copyright: {\textcopyright} 2024 The Author(s). Published by S. Karger AG, Basel.",

year = "2024",

month = apr,

day = "10",

doi = "10.1159/000537915",

language = "英語",

volume = "13",

pages = "522--536",

journal = "Liver Cancer",

issn = "2235-1795",

publisher = "S. Karger AG",

number = "5",

}

Rossari, F, Tada, T, Suda, G, Shimose, S, Kudo, M, Yoo, C, Cheon, J, Finkelmeier, F, Lim, HY, Presa, J, Masi, G, Bergamo, F, Amadeo, E, Vitiello, F, Kumada, T, Sakamoto, N, Iwamoto, H, Aoki, T, Chon, HJ, Himmelsbach, V, Iavarone, M, Cabibbo, G, Montes, M, Foschi, FG, Vivaldi, C, Soldà, C, Sho, T, Niizeki, T, Nishida, N, Steup, C, Hirooka, M, Kariyama, K, Tani, J, Atsukawa, M, Takaguchi, K, Itobayashi, E, Fukunishi, S, Tsuji, K, Ishikawa, T, Tajiri, K, Ochi, H, Yasuda, S, Toyoda, H, Ogawa, C, Nishimura, T, Hatanaka, T, Kakizaki, S, Shimada, N, Kawata, K, Hiraoka, A, Tada, F, Ohama, H, Nouso, K, Morishita, A, Tsutsui, A, Nagano, T, Itokawa, N, Okubo, T, Imai, M, Kosaka, H, Naganuma, A, Koizumi, Y, Nakamura, S, Kaibori, M, Iijima, H, Hiasa, Y, Persano, M, Foti, S, Camera, S, Stefanini, B, Scartozzi, M, Cascinu, S, Casadei-Gardini, A & Rimini, M 2024, 'Disease Etiology Impact on Outcomes of Hepatocellular Carcinoma Patients Treated with Atezolizumab plus Bevacizumab: A Real-World, Multicenter Study', Liver Cancer, vol. 13, no. 5, pp. 522-536. https://doi.org/10.1159/000537915

TY - JOUR

T1 - Disease Etiology Impact on Outcomes of Hepatocellular Carcinoma Patients Treated with Atezolizumab plus Bevacizumab

T2 - A Real-World, Multicenter Study

AU - Rossari, Federico

AU - Tada, Toshifumi

AU - Suda, Goki

AU - Shimose, Shigeo

AU - Kudo, Masatoshi

AU - Yoo, Changhoon

AU - Cheon, Jaekyung

AU - Finkelmeier, Fabian

AU - Lim, Ho Yeong

AU - Presa, José

AU - Masi, Gianluca

AU - Bergamo, Francesca

AU - Amadeo, Elisabeth

AU - Vitiello, Francesco

AU - Kumada, Takashi

AU - Sakamoto, Naoya

AU - Iwamoto, Hideki

AU - Aoki, Tomoko

AU - Chon, Hong Jae

AU - Himmelsbach, Vera

AU - Iavarone, Massimo

AU - Cabibbo, Giuseppe

AU - Montes, Margarida

AU - Foschi, Francesco Giuseppe

AU - Vivaldi, Caterina

AU - Soldà, Caterina

AU - Sho, Takuya

AU - Niizeki, Takashi

AU - Nishida, Naoshi

AU - Steup, Christoph

AU - Hirooka, Masashi

AU - Kariyama, Kazuya

AU - Tani, Joji

AU - Atsukawa, Masanori

AU - Takaguchi, Koichi

AU - Itobayashi, Ei

AU - Fukunishi, Shinya

AU - Tsuji, Kunihiko

AU - Ishikawa, Toru

AU - Tajiri, Kazuto

AU - Ochi, Hironori

AU - Yasuda, Satoshi

AU - Toyoda, Hidenori

AU - Ogawa, Chikara

AU - Nishimura, Takashi

AU - Hatanaka, Takeshi

AU - Kakizaki, Satoru

AU - Shimada, Noritomo

AU - Kawata, Kazuhito

AU - Hiraoka, Atsushi

AU - Tada, Fujimasa

AU - Ohama, Hideko

AU - Nouso, Kazuhiro

AU - Morishita, Asahiro

AU - Tsutsui, Akemi

AU - Nagano, Takuya

AU - Itokawa, Norio

AU - Okubo, Tomomi

AU - Imai, Michitaka

AU - Kosaka, Hisashi

AU - Naganuma, Atsushi

AU - Koizumi, Yohei

AU - Nakamura, Shinichiro

AU - Kaibori, Masaaki

AU - Iijima, Hiroko

AU - Hiasa, Yoichi

AU - Persano, Mara

AU - Foti, Silvia

AU - Camera, Silvia

AU - Stefanini, Bernardo

AU - Scartozzi, Mario

AU - Cascinu, Stefano

AU - Casadei-Gardini, Andrea

AU - Rimini, Margherita

PY - 2024/4/10

Y1 - 2024/4/10

N2 - 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 (A + B) is equally effective in viral and nonviral patients. Methods: We retrospectively analyzed 885 HCC patients treated with the first-line A + B from multiple centers from Eastern and Western countries, 53.9% having viral and 46.1% nonviral etiology. Baseline clinical and laboratory characteristics were analyzed with uni- and multivariate models to explore potential differences on overall survival (OS), time-to-progression (TTP), disease control rates (DCRs) based on etiology and to identify putative prognostic factors in etiology subgroups. Treatment toxicities and access to the second-line treatments and outcomes were also reported and compared between etiologies. Results: Overall, no statistically significant differences were found in median OS (mOS: viral 15.9 months; nonviral 16.3 months), TTP (mTTP: viral 8.3 months; nonviral 7.2 months), and DCRs (viral 78.1%; nonviral 80.8%) based on etiology. Prognostic factors of survival and progression were mainly shared between viral and nonviral 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 the 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 nonviral 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.

AB - 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 (A + B) is equally effective in viral and nonviral patients. Methods: We retrospectively analyzed 885 HCC patients treated with the first-line A + B from multiple centers from Eastern and Western countries, 53.9% having viral and 46.1% nonviral etiology. Baseline clinical and laboratory characteristics were analyzed with uni- and multivariate models to explore potential differences on overall survival (OS), time-to-progression (TTP), disease control rates (DCRs) based on etiology and to identify putative prognostic factors in etiology subgroups. Treatment toxicities and access to the second-line treatments and outcomes were also reported and compared between etiologies. Results: Overall, no statistically significant differences were found in median OS (mOS: viral 15.9 months; nonviral 16.3 months), TTP (mTTP: viral 8.3 months; nonviral 7.2 months), and DCRs (viral 78.1%; nonviral 80.8%) based on etiology. Prognostic factors of survival and progression were mainly shared between viral and nonviral 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 the 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 nonviral 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.

KW - Atezolizumab

KW - Bevacizumab

KW - Etiology

KW - Hepatocellular carcinoma

KW - Immunotherapy

KW - Non-alcoholic steatohepatitis

KW - Viral hepatitis

UR - http://www.scopus.com/inward/record.url?scp=85196725470&partnerID=8YFLogxK

U2 - 10.1159/000537915

DO - 10.1159/000537915

M3 - 学術論文

C2 - 39296620

AN - SCOPUS:85196725470

SN - 2235-1795

VL - 13

SP - 522

EP - 536

JO - Liver Cancer

JF - Liver Cancer

IS - 5

ER -