First-Line Immune Checkpoint Inhibitor-Based Sequential Therapies for Advanced Hepatocellular Carcinoma: Rationale for Future Trials

Giuseppe Cabibbo; Maria Reig; Ciro Celsa; Ferran Torres; Salvatore Battaglia; Marco Enea; Giacomo Emanuele Maria Rizzo; Salvatore Petta; Vincenza Calvaruso; Vito Di Marco; Antonio Craxì; Amit G. Singal; Jordi Bruix; Calogero Cammà

doi:10.1159/000520278

First-Line Immune Checkpoint Inhibitor-Based Sequential Therapies for Advanced Hepatocellular Carcinoma: Rationale for Future Trials

Giuseppe Cabibbo, Maria Reig, Ciro Celsa, Ferran Torres, Salvatore Battaglia, Marco Enea, Giacomo Emanuele Maria Rizzo, Salvatore Petta, Vincenza Calvaruso, Vito Di Marco, Antonio Craxì, Amit G. Singal, Jordi Bruix, Calogero Cammà

Research output: Contribution to journal › Article › peer-review

13 Scopus citations

Abstract

Atezolizumab (ATEZO) plus bevacizumab (BEVA) represents the new standard of care for the treatment of advanced hepatocellular carcinoma (HCC). However, the choice of the second-line treatment after the failure of immunotherapy-based first-line remains elusive. Taking into account the weaknesses of the available evidence, we developed a simulation model based on available phase III randomized clinical trials (RCTs) to identify optimal risk/benefit sequential strategies. Methods: A Markov model was built to estimate the overall survival (OS) of sequential first- and second-line systemic treatments. Sequences starting with first-line ATEZO plus BEVA followed by 5 second-line treatments (sorafenib [SORA], lenvatinib [LENVA], regorafenib, cabozantinib, and ramucirumab) were compared. The probability of transition between states (initial treatment, cancer progression, and death) was derived from RCTs. Life-year gained (LYG) was the main outcome. Rates of severe adverse events (SAEs) (≥ grade 3) were calculated. The incremental safety-effectiveness ratio (ISER) was calculated as the difference in probability of SAEs divided by LYG between the 2 most effective sequences. Results: ATEZO plus BEVA followed by LENVA (median OS, 24 months) or SORA (median OS, 23 months) was the most effective sequence, producing a LYG of 0.50 and 0.42 year, respectively. ATEZO plus BEVA followed by SORA was the safest sequence (SAEs 63%). At a willingness-to-risk threshold of 10% of SAEs for LYG, ATEZO plus BEVA followed by second-line SORA was favored in 72% of cases, while at a threshold of 30% of SAEs for LYG, ATEZO plus BEVA followed by second-line LENVA was favored in 69% of cases. Conclusion: Our simulation model provides a strong rationale to support ongoing trials evaluating second-line tyrosine-kinase inhibitors after first-line ATEZO plus BEVA. Future evidence from ongoing RCTs and prospective real-world studies are needed to prove the net health benefit of sequential treatment options for advanced HCC.

Original language	English (US)
Pages (from-to)	75-84
Number of pages	10
Journal	Liver Cancer
Volume	11
Issue number	1
DOIs	https://doi.org/10.1159/000520278
State	Published - Jan 23 2022

ASJC Scopus subject areas

Hepatology
Oncology

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10.1159/000520278

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Cabibbo, G., Reig, M., Celsa, C., Torres, F., Battaglia, S., Enea, M., Rizzo, G. E. M., Petta, S., Calvaruso, V., Di Marco, V., Craxì, A., Singal, A. G., Bruix, J., & Cammà, C. (2022). First-Line Immune Checkpoint Inhibitor-Based Sequential Therapies for Advanced Hepatocellular Carcinoma: Rationale for Future Trials. Liver Cancer, 11(1), 75-84. https://doi.org/10.1159/000520278

Cabibbo, G, Reig, M, Celsa, C, Torres, F, Battaglia, S, Enea, M, Rizzo, GEM, Petta, S, Calvaruso, V, Di Marco, V, Craxì, A, Singal, AG, Bruix, J & Cammà, C 2022, 'First-Line Immune Checkpoint Inhibitor-Based Sequential Therapies for Advanced Hepatocellular Carcinoma: Rationale for Future Trials', Liver Cancer, vol. 11, no. 1, pp. 75-84. https://doi.org/10.1159/000520278

@article{f35a50da72214d38b902f574e5a27b05,

title = "First-Line Immune Checkpoint Inhibitor-Based Sequential Therapies for Advanced Hepatocellular Carcinoma: Rationale for Future Trials",

abstract = "Atezolizumab (ATEZO) plus bevacizumab (BEVA) represents the new standard of care for the treatment of advanced hepatocellular carcinoma (HCC). However, the choice of the second-line treatment after the failure of immunotherapy-based first-line remains elusive. Taking into account the weaknesses of the available evidence, we developed a simulation model based on available phase III randomized clinical trials (RCTs) to identify optimal risk/benefit sequential strategies. Methods: A Markov model was built to estimate the overall survival (OS) of sequential first- and second-line systemic treatments. Sequences starting with first-line ATEZO plus BEVA followed by 5 second-line treatments (sorafenib [SORA], lenvatinib [LENVA], regorafenib, cabozantinib, and ramucirumab) were compared. The probability of transition between states (initial treatment, cancer progression, and death) was derived from RCTs. Life-year gained (LYG) was the main outcome. Rates of severe adverse events (SAEs) (≥ grade 3) were calculated. The incremental safety-effectiveness ratio (ISER) was calculated as the difference in probability of SAEs divided by LYG between the 2 most effective sequences. Results: ATEZO plus BEVA followed by LENVA (median OS, 24 months) or SORA (median OS, 23 months) was the most effective sequence, producing a LYG of 0.50 and 0.42 year, respectively. ATEZO plus BEVA followed by SORA was the safest sequence (SAEs 63%). At a willingness-to-risk threshold of 10% of SAEs for LYG, ATEZO plus BEVA followed by second-line SORA was favored in 72% of cases, while at a threshold of 30% of SAEs for LYG, ATEZO plus BEVA followed by second-line LENVA was favored in 69% of cases. Conclusion: Our simulation model provides a strong rationale to support ongoing trials evaluating second-line tyrosine-kinase inhibitors after first-line ATEZO plus BEVA. Future evidence from ongoing RCTs and prospective real-world studies are needed to prove the net health benefit of sequential treatment options for advanced HCC.",

author = "Giuseppe Cabibbo and Maria Reig and Ciro Celsa and Ferran Torres and Salvatore Battaglia and Marco Enea and Rizzo, {Giacomo Emanuele Maria} and Salvatore Petta and Vincenza Calvaruso and {Di Marco}, Vito and Antonio Crax{\`i} and Singal, {Amit G.} and Jordi Bruix and Calogero Camm{\`a}",

note = "Funding Information: A.G.S. received Grant support from the National Institute of Health (NIH) R01 MD12565. J.B. received Grant support from Instituto de Salud Carlos III (PI18/00768), AECC (PI044031), and WCR (AICR) 16-0026. CIBERehd is funded by the Instituto de Salud Carlos III. Funding Information: Giuseppe Cabibbo participated in advisory board for Bayer, Eisai, and Ipsen. Maria Reig is a consultant at Bayer-Shering Pharma, BMS, Roche, Ipsen, AstraZeneca, Lilly, and BTG; attended paid conferences at Bayer-Shering Pharma, BMS, Gilead, and Lilly; received research grants from Bayer-Shering Pharma and Ipsen. Ciro Celsa received speaker fees from Eisai. Amit Singal served on advisory boards or as consultant for Genentech, Bayer, Eisai, Exelixis, Bristol Myers Squibb, and AstraZeneca. Jordi Bruix is a consultant at AbbVie, Adaptimmune, Arqule, Astra-Medimmune, Basilea, Bayer-Shering Pharma, Bio-Alliance, BMS, BTG-Biocompatibles, Eisai, Gilead, Incyte, Ipsen, Kowa, Lilly, MSD, Nerviano, Novartis, Polaris, Quirem, Roche, Sirtex, Sanofi, and Terumo; received research grants from Bayer and BTG; received educational grants from Bayer and BTG; attended paid conferences at Bayer, BTG, Astra-Zeneca, and Ipsen; gave paid talks at Bayer-Shering Pharma, BTG-Biocompatibles, Eisai, Terumo, Sirtex, and Ipsen. Calogero Camm{\`a} participated in the advisory board for Bayer, MSD/Merck, Ipsen, and Eisai. The other authors have no disclosure to declare. Publisher Copyright: {\textcopyright} 2021 ",

year = "2022",

month = jan,

day = "23",

doi = "10.1159/000520278",

language = "English (US)",

volume = "11",

pages = "75--84",

journal = "Liver Cancer",

issn = "2235-1795",

publisher = "S. Karger AG",

number = "1",

}

TY - JOUR

T1 - First-Line Immune Checkpoint Inhibitor-Based Sequential Therapies for Advanced Hepatocellular Carcinoma

T2 - Rationale for Future Trials

AU - Cabibbo, Giuseppe

AU - Reig, Maria

AU - Celsa, Ciro

AU - Torres, Ferran

AU - Battaglia, Salvatore

AU - Enea, Marco

AU - Rizzo, Giacomo Emanuele Maria

AU - Petta, Salvatore

AU - Calvaruso, Vincenza

AU - Di Marco, Vito

AU - Craxì, Antonio

AU - Singal, Amit G.

AU - Bruix, Jordi

AU - Cammà, Calogero

N1 - Funding Information: A.G.S. received Grant support from the National Institute of Health (NIH) R01 MD12565. J.B. received Grant support from Instituto de Salud Carlos III (PI18/00768), AECC (PI044031), and WCR (AICR) 16-0026. CIBERehd is funded by the Instituto de Salud Carlos III. Funding Information: Giuseppe Cabibbo participated in advisory board for Bayer, Eisai, and Ipsen. Maria Reig is a consultant at Bayer-Shering Pharma, BMS, Roche, Ipsen, AstraZeneca, Lilly, and BTG; attended paid conferences at Bayer-Shering Pharma, BMS, Gilead, and Lilly; received research grants from Bayer-Shering Pharma and Ipsen. Ciro Celsa received speaker fees from Eisai. Amit Singal served on advisory boards or as consultant for Genentech, Bayer, Eisai, Exelixis, Bristol Myers Squibb, and AstraZeneca. Jordi Bruix is a consultant at AbbVie, Adaptimmune, Arqule, Astra-Medimmune, Basilea, Bayer-Shering Pharma, Bio-Alliance, BMS, BTG-Biocompatibles, Eisai, Gilead, Incyte, Ipsen, Kowa, Lilly, MSD, Nerviano, Novartis, Polaris, Quirem, Roche, Sirtex, Sanofi, and Terumo; received research grants from Bayer and BTG; received educational grants from Bayer and BTG; attended paid conferences at Bayer, BTG, Astra-Zeneca, and Ipsen; gave paid talks at Bayer-Shering Pharma, BTG-Biocompatibles, Eisai, Terumo, Sirtex, and Ipsen. Calogero Cammà participated in the advisory board for Bayer, MSD/Merck, Ipsen, and Eisai. The other authors have no disclosure to declare. Publisher Copyright: © 2021

PY - 2022/1/23

Y1 - 2022/1/23

N2 - Atezolizumab (ATEZO) plus bevacizumab (BEVA) represents the new standard of care for the treatment of advanced hepatocellular carcinoma (HCC). However, the choice of the second-line treatment after the failure of immunotherapy-based first-line remains elusive. Taking into account the weaknesses of the available evidence, we developed a simulation model based on available phase III randomized clinical trials (RCTs) to identify optimal risk/benefit sequential strategies. Methods: A Markov model was built to estimate the overall survival (OS) of sequential first- and second-line systemic treatments. Sequences starting with first-line ATEZO plus BEVA followed by 5 second-line treatments (sorafenib [SORA], lenvatinib [LENVA], regorafenib, cabozantinib, and ramucirumab) were compared. The probability of transition between states (initial treatment, cancer progression, and death) was derived from RCTs. Life-year gained (LYG) was the main outcome. Rates of severe adverse events (SAEs) (≥ grade 3) were calculated. The incremental safety-effectiveness ratio (ISER) was calculated as the difference in probability of SAEs divided by LYG between the 2 most effective sequences. Results: ATEZO plus BEVA followed by LENVA (median OS, 24 months) or SORA (median OS, 23 months) was the most effective sequence, producing a LYG of 0.50 and 0.42 year, respectively. ATEZO plus BEVA followed by SORA was the safest sequence (SAEs 63%). At a willingness-to-risk threshold of 10% of SAEs for LYG, ATEZO plus BEVA followed by second-line SORA was favored in 72% of cases, while at a threshold of 30% of SAEs for LYG, ATEZO plus BEVA followed by second-line LENVA was favored in 69% of cases. Conclusion: Our simulation model provides a strong rationale to support ongoing trials evaluating second-line tyrosine-kinase inhibitors after first-line ATEZO plus BEVA. Future evidence from ongoing RCTs and prospective real-world studies are needed to prove the net health benefit of sequential treatment options for advanced HCC.

AB - Atezolizumab (ATEZO) plus bevacizumab (BEVA) represents the new standard of care for the treatment of advanced hepatocellular carcinoma (HCC). However, the choice of the second-line treatment after the failure of immunotherapy-based first-line remains elusive. Taking into account the weaknesses of the available evidence, we developed a simulation model based on available phase III randomized clinical trials (RCTs) to identify optimal risk/benefit sequential strategies. Methods: A Markov model was built to estimate the overall survival (OS) of sequential first- and second-line systemic treatments. Sequences starting with first-line ATEZO plus BEVA followed by 5 second-line treatments (sorafenib [SORA], lenvatinib [LENVA], regorafenib, cabozantinib, and ramucirumab) were compared. The probability of transition between states (initial treatment, cancer progression, and death) was derived from RCTs. Life-year gained (LYG) was the main outcome. Rates of severe adverse events (SAEs) (≥ grade 3) were calculated. The incremental safety-effectiveness ratio (ISER) was calculated as the difference in probability of SAEs divided by LYG between the 2 most effective sequences. Results: ATEZO plus BEVA followed by LENVA (median OS, 24 months) or SORA (median OS, 23 months) was the most effective sequence, producing a LYG of 0.50 and 0.42 year, respectively. ATEZO plus BEVA followed by SORA was the safest sequence (SAEs 63%). At a willingness-to-risk threshold of 10% of SAEs for LYG, ATEZO plus BEVA followed by second-line SORA was favored in 72% of cases, while at a threshold of 30% of SAEs for LYG, ATEZO plus BEVA followed by second-line LENVA was favored in 69% of cases. Conclusion: Our simulation model provides a strong rationale to support ongoing trials evaluating second-line tyrosine-kinase inhibitors after first-line ATEZO plus BEVA. Future evidence from ongoing RCTs and prospective real-world studies are needed to prove the net health benefit of sequential treatment options for advanced HCC.

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ER -

First-Line Immune Checkpoint Inhibitor-Based Sequential Therapies for Advanced Hepatocellular Carcinoma: Rationale for Future Trials

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