Molecular Markers of Response to Anti-PD1 Therapy in Advanced Hepatocellular Carcinoma

Philipp K. Haber; Florian Castet; Miguel Torres-Martin; Carmen Andreu-Oller; Marc Puigvehí; Maeda Miho; Pompilia Radu; Jean Francois Dufour; Chris Verslype; Carolin Zimpel; Jens U. Marquardt; Peter R. Galle; Arndt Vogel; Melanie Bathon; Tim Meyer; Ismail Labgaa; Antonia Digklia; Lewis R. Roberts; Mohamed A. Mohamed Ali; Beatriz Mínguez; Davide Citterio; Vincenzo Mazzaferro; Fabian Finkelmeier; Jörg Trojan; Burcin Özdirik; Tobias Müller; Moritz Schmelzle; Anthony Bejjani; Max W. Sung; Myron E. Schwartz; Richard S. Finn; Swan Thung; Augusto Villanueva; Daniela Sia; Josep M. Llovet

doi:10.1053/j.gastro.2022.09.005

Molecular Markers of Response to Anti-PD1 Therapy in Advanced Hepatocellular Carcinoma

Philipp K. Haber, Florian Castet, Miguel Torres-Martin, Carmen Andreu-Oller, Marc Puigvehí, Maeda Miho, Pompilia Radu, Jean Francois Dufour, Chris Verslype, Carolin Zimpel, Jens U. Marquardt, Peter R. Galle, Arndt Vogel, Melanie Bathon, Tim Meyer, Ismail Labgaa, Antonia Digklia, Lewis R. Roberts, Mohamed A. Mohamed Ali, Beatriz MínguezDavide Citterio, Vincenzo Mazzaferro, Fabian Finkelmeier, Jörg Trojan, Burcin Özdirik, Tobias Müller, Moritz Schmelzle, Anthony Bejjani, Max W. Sung, Myron E. Schwartz, Richard S. Finn, Swan Thung, Augusto Villanueva, Daniela Sia, Josep M. Llovet^*

^*Korrespondierende/r Autor/-in für diese Arbeit

Medizinische Klinik I

114 Zitate (Scopus)

Abstract

Background & Aims: Single-agent anti-PD1 checkpoint inhibitors convey outstanding clinical benefits in a small fraction (∼20%) of patients with advanced hepatocellular carcinoma (aHCC) but the molecular mechanisms determining response are unknown. To fill this gap, we herein analyze the molecular and immune traits of aHCC in patients treated with anti-PD1. Methods: Overall, 111 tumor samples from patients with aHCC were obtained from 13 centers before systemic therapies. We performed molecular analysis and immune deconvolution using whole-genome expression data (n = 83), mutational analysis (n = 72), and histologic evaluation with an endpoint of objective response. Results: Among 83 patients with transcriptomic data, 28 were treated in frontline, whereas 55 patients were treated after tyrosine kinase inhibitors (TKI) either in second or third line. Responders treated in frontline showed upregulated interferon-γ signaling and major histocompatibility complex II–related antigen presentation. We generated an 11-gene signature (IFNAP), capturing these molecular features, which predicts response and survival in patients treated with anti-PD1 in frontline. The signature was validated in a separate cohort of aHCC and >240 patients with other solid cancer types where it also predicted response and survival. Of note, the same signature was unable to predict response in archival tissue of patients treated with frontline TKIs, highlighting the need for fresh biopsies before immunotherapy. Conclusion: Interferon signaling and major histocompatibility complex–related genes are key molecular features of HCCs responding to anti-PD1. A novel 11-gene signature predicts response in frontline aHCC, but not in patients pretreated with TKIs. These results must be confirmed in prospective studies and highlights the need for biopsies before immunotherapy to identify biomarkers of response.

Originalsprache	Englisch
Zeitschrift	Gastroenterology
Jahrgang	164
Ausgabenummer	1
Seiten (von - bis)	72-88.e18
ISSN	0016-5085
DOIs	https://doi.org/10.1053/j.gastro.2022.09.005
Publikationsstatus	Veröffentlicht - 01.2023

Fördermittel

Funding This study was supported by a research grant from Bayer Pharmaceuticals to Josep M. Llovet. Philipp K. Haber is supported by the fellowship grant of the German Research Foundation (DFG, HA 8754/1–1). Florian Castet is supported by an AECC Clínico Junior grant, ID code (CLJUN20007CAST). Carmen Andreu-Oller is supported by a Fulbright fellowship. Marc Puigvehí received a "Juan Rodés" scholarship grant from Asociación Española para el Estudio del Hígado (AEEH). Jens U. Marquardt is supported by grants from the German Research Foundation (MA 4443/2–2; SFB1292) and the Volkswagen Foundation (Lichtenberg program). Arndt Vogel is funded by the DFG (SFB/TRR 209 - 314905040, and Vo959/9–1). Tim Meyer is funded by the NIHR UCH Biomedical Research Centre and Accelerator Award (HUNTER, Ref. C9380/A26813, partnership between the CRUK, AECC, and AIRC). Lewis R. Roberts and Mohamed A. Mohamed Ali are supported by the Mayo Clinic Hepatobiliary SPORE (P50 CA210964). Moritz Schmelzle acknowledges a research grant from the DFG (SCHM2661/3–2). The work of Daniela Sia is supported by the Tisch Cancer Institute and the PhD Scientist Innovative Research Award. Josep M. Llovet is supported by National Cancer Institute (P30-CA196521), National Institute of Diabetes and Digestive and Kidney Diseases (R01 DK128289), US Department of Defense (CA150272P3), European Commission / Horizon 2020 Program (HEPCAR, Ref. 667273–2), Accelerator Award (CRUK, AECC, AIRC) (HUNTER, Ref. C9380/A26813), Samuel Waxman Cancer Research Foundation, Centro de Investigación Biomédica en Red (CIBER) – ISCIII, Spanish National Health Institute (SAF2016–76390), Generalitat de Catalunya/AGAUR (SGR-1358), and the Acadèmia de Ciències Mèdiques i de la Salut de Catalunya i de Balears.

UN SDGs

Dieser Output leistet einen Beitrag zu folgendem(n) Ziel(en) für nachhaltige Entwicklung

SDG 3 – Gesundheit und Wohlergehen

Strategische Forschungsbereiche und Zentren

Zentren: Universitäres Cancer Center Schleswig-Holstein (UCCSH)

Dokumente

10.1053/j.gastro.2022.09.005

Weitere Links

Link to publication in Scopus

Zitieren

Haber, P. K., Castet, F., Torres-Martin, M., Andreu-Oller, C., Puigvehí, M., Miho, M., Radu, P., Dufour, J. F., Verslype, C., Zimpel, C., Marquardt, J. U., Galle, P. R., Vogel, A., Bathon, M., Meyer, T., Labgaa, I., Digklia, A., Roberts, L. R., Mohamed Ali, M. A., ... Llovet, J. M. (2023). Molecular Markers of Response to Anti-PD1 Therapy in Advanced Hepatocellular Carcinoma. Gastroenterology, 164(1), 72-88.e18. https://doi.org/10.1053/j.gastro.2022.09.005

@article{5800d4493c1b4566af8f30df5c233ec1,

title = "Molecular Markers of Response to Anti-PD1 Therapy in Advanced Hepatocellular Carcinoma",

abstract = "Background \& Aims: Single-agent anti-PD1 checkpoint inhibitors convey outstanding clinical benefits in a small fraction (∼20\%) of patients with advanced hepatocellular carcinoma (aHCC) but the molecular mechanisms determining response are unknown. To fill this gap, we herein analyze the molecular and immune traits of aHCC in patients treated with anti-PD1. Methods: Overall, 111 tumor samples from patients with aHCC were obtained from 13 centers before systemic therapies. We performed molecular analysis and immune deconvolution using whole-genome expression data (n = 83), mutational analysis (n = 72), and histologic evaluation with an endpoint of objective response. Results: Among 83 patients with transcriptomic data, 28 were treated in frontline, whereas 55 patients were treated after tyrosine kinase inhibitors (TKI) either in second or third line. Responders treated in frontline showed upregulated interferon-γ signaling and major histocompatibility complex II–related antigen presentation. We generated an 11-gene signature (IFNAP), capturing these molecular features, which predicts response and survival in patients treated with anti-PD1 in frontline. The signature was validated in a separate cohort of aHCC and >240 patients with other solid cancer types where it also predicted response and survival. Of note, the same signature was unable to predict response in archival tissue of patients treated with frontline TKIs, highlighting the need for fresh biopsies before immunotherapy. Conclusion: Interferon signaling and major histocompatibility complex–related genes are key molecular features of HCCs responding to anti-PD1. A novel 11-gene signature predicts response in frontline aHCC, but not in patients pretreated with TKIs. These results must be confirmed in prospective studies and highlights the need for biopsies before immunotherapy to identify biomarkers of response.",

author = "Haber, \{Philipp K.\} and Florian Castet and Miguel Torres-Martin and Carmen Andreu-Oller and Marc Puigveh{\'i} and Maeda Miho and Pompilia Radu and Dufour, \{Jean Francois\} and Chris Verslype and Carolin Zimpel and Marquardt, \{Jens U.\} and Galle, \{Peter R.\} and Arndt Vogel and Melanie Bathon and Tim Meyer and Ismail Labgaa and Antonia Digklia and Roberts, \{Lewis R.\} and \{Mohamed Ali\}, \{Mohamed A.\} and Beatriz M{\'i}nguez and Davide Citterio and Vincenzo Mazzaferro and Fabian Finkelmeier and J{\"o}rg Trojan and Burcin {\"O}zdirik and Tobias M{\"u}ller and Moritz Schmelzle and Anthony Bejjani and Sung, \{Max W.\} and Schwartz, \{Myron E.\} and Finn, \{Richard S.\} and Swan Thung and Augusto Villanueva and Daniela Sia and Llovet, \{Josep M.\}",

note = "Publisher Copyright: {\textcopyright} 2023 AGA Institute",

year = "2023",

month = jan,

doi = "10.1053/j.gastro.2022.09.005",

language = "English",

volume = "164",

pages = "72--88.e18",

journal = "Gastroenterology",

issn = "0016-5085",

publisher = "W.B. Saunders",

number = "1",

}

Haber, PK, Castet, F, Torres-Martin, M, Andreu-Oller, C, Puigvehí, M, Miho, M, Radu, P, Dufour, JF, Verslype, C, Zimpel, C , Marquardt, JU, Galle, PR, Vogel, A, Bathon, M, Meyer, T, Labgaa, I, Digklia, A, Roberts, LR, Mohamed Ali, MA, Mínguez, B, Citterio, D, Mazzaferro, V, Finkelmeier, F, Trojan, J, Özdirik, B, Müller, T, Schmelzle, M, Bejjani, A, Sung, MW, Schwartz, ME, Finn, RS, Thung, S, Villanueva, A, Sia, D & Llovet, JM 2023, 'Molecular Markers of Response to Anti-PD1 Therapy in Advanced Hepatocellular Carcinoma', Gastroenterology, Jg. 164, Nr. 1, S. 72-88.e18. https://doi.org/10.1053/j.gastro.2022.09.005

TY - JOUR

T1 - Molecular Markers of Response to Anti-PD1 Therapy in Advanced Hepatocellular Carcinoma

AU - Haber, Philipp K.

AU - Castet, Florian

AU - Torres-Martin, Miguel

AU - Andreu-Oller, Carmen

AU - Puigvehí, Marc

AU - Miho, Maeda

AU - Radu, Pompilia

AU - Dufour, Jean Francois

AU - Verslype, Chris

AU - Zimpel, Carolin

AU - Marquardt, Jens U.

AU - Galle, Peter R.

AU - Vogel, Arndt

AU - Bathon, Melanie

AU - Meyer, Tim

AU - Labgaa, Ismail

AU - Digklia, Antonia

AU - Roberts, Lewis R.

AU - Mohamed Ali, Mohamed A.

AU - Mínguez, Beatriz

AU - Citterio, Davide

AU - Mazzaferro, Vincenzo

AU - Finkelmeier, Fabian

AU - Trojan, Jörg

AU - Özdirik, Burcin

AU - Müller, Tobias

AU - Schmelzle, Moritz

AU - Bejjani, Anthony

AU - Sung, Max W.

AU - Schwartz, Myron E.

AU - Finn, Richard S.

AU - Thung, Swan

AU - Villanueva, Augusto

AU - Sia, Daniela

AU - Llovet, Josep M.

PY - 2023/1

Y1 - 2023/1

N2 - Background & Aims: Single-agent anti-PD1 checkpoint inhibitors convey outstanding clinical benefits in a small fraction (∼20%) of patients with advanced hepatocellular carcinoma (aHCC) but the molecular mechanisms determining response are unknown. To fill this gap, we herein analyze the molecular and immune traits of aHCC in patients treated with anti-PD1. Methods: Overall, 111 tumor samples from patients with aHCC were obtained from 13 centers before systemic therapies. We performed molecular analysis and immune deconvolution using whole-genome expression data (n = 83), mutational analysis (n = 72), and histologic evaluation with an endpoint of objective response. Results: Among 83 patients with transcriptomic data, 28 were treated in frontline, whereas 55 patients were treated after tyrosine kinase inhibitors (TKI) either in second or third line. Responders treated in frontline showed upregulated interferon-γ signaling and major histocompatibility complex II–related antigen presentation. We generated an 11-gene signature (IFNAP), capturing these molecular features, which predicts response and survival in patients treated with anti-PD1 in frontline. The signature was validated in a separate cohort of aHCC and >240 patients with other solid cancer types where it also predicted response and survival. Of note, the same signature was unable to predict response in archival tissue of patients treated with frontline TKIs, highlighting the need for fresh biopsies before immunotherapy. Conclusion: Interferon signaling and major histocompatibility complex–related genes are key molecular features of HCCs responding to anti-PD1. A novel 11-gene signature predicts response in frontline aHCC, but not in patients pretreated with TKIs. These results must be confirmed in prospective studies and highlights the need for biopsies before immunotherapy to identify biomarkers of response.

AB - Background & Aims: Single-agent anti-PD1 checkpoint inhibitors convey outstanding clinical benefits in a small fraction (∼20%) of patients with advanced hepatocellular carcinoma (aHCC) but the molecular mechanisms determining response are unknown. To fill this gap, we herein analyze the molecular and immune traits of aHCC in patients treated with anti-PD1. Methods: Overall, 111 tumor samples from patients with aHCC were obtained from 13 centers before systemic therapies. We performed molecular analysis and immune deconvolution using whole-genome expression data (n = 83), mutational analysis (n = 72), and histologic evaluation with an endpoint of objective response. Results: Among 83 patients with transcriptomic data, 28 were treated in frontline, whereas 55 patients were treated after tyrosine kinase inhibitors (TKI) either in second or third line. Responders treated in frontline showed upregulated interferon-γ signaling and major histocompatibility complex II–related antigen presentation. We generated an 11-gene signature (IFNAP), capturing these molecular features, which predicts response and survival in patients treated with anti-PD1 in frontline. The signature was validated in a separate cohort of aHCC and >240 patients with other solid cancer types where it also predicted response and survival. Of note, the same signature was unable to predict response in archival tissue of patients treated with frontline TKIs, highlighting the need for fresh biopsies before immunotherapy. Conclusion: Interferon signaling and major histocompatibility complex–related genes are key molecular features of HCCs responding to anti-PD1. A novel 11-gene signature predicts response in frontline aHCC, but not in patients pretreated with TKIs. These results must be confirmed in prospective studies and highlights the need for biopsies before immunotherapy to identify biomarkers of response.

UR - https://www.scopus.com/pages/publications/85142162479

U2 - 10.1053/j.gastro.2022.09.005

DO - 10.1053/j.gastro.2022.09.005

M3 - Journal articles

C2 - 36108710

AN - SCOPUS:85142162479

SN - 0016-5085

VL - 164

SP - 72-88.e18

JO - Gastroenterology

JF - Gastroenterology

IS - 1

ER -

Molecular Markers of Response to Anti-PD1 Therapy in Advanced Hepatocellular Carcinoma

Abstract

Fördermittel

UN SDGs

Strategische Forschungsbereiche und Zentren

Dokumente

Weitere Links

Fingerprint

Zitieren