BH3-only protein expression determines hepatocellular carcinoma response to sorafenib-based treatment

BH3-only protein expression determines hepatocellular carcinoma response to sorafenib-based treatment

Abstract Hepatocellular carcinoma (HCC) represents a global health challenge with limited therapeutic options. Anti-angiogenic immune checkpoint inhibitor-based combination therapy has been introduced for progressed HCC, but improves survival only in a subset of HCC patients. Tyrosine-kinase inhibit...

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Main Authors: Stephanie Busche, Katharina John, Franziska Wandrer, Florian W. R. Vondran, Ulrich Lehmann, Heiner Wedemeyer, Frank Essmann, Klaus Schulze-Osthoff, Heike Bantel
Format: Article
Language:English
Published: Nature Publishing Group 2021-07-01
Series:Cell Death and Disease
Online Access:https://doi.org/10.1038/s41419-021-04020-z
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spelling doaj-48fe77e844cc4ce08705c16637f512f72021-08-01T11:04:42ZengNature Publishing GroupCell Death and Disease2041-48892021-07-0112811110.1038/s41419-021-04020-zBH3-only protein expression determines hepatocellular carcinoma response to sorafenib-based treatmentStephanie Busche0Katharina John1Franziska Wandrer2Florian W. R. Vondran3Ulrich Lehmann4Heiner Wedemeyer5Frank Essmann6Klaus Schulze-Osthoff7Heike Bantel8Department of Gastroenterology, Hepatology and Endocrinology, Hannover Medical SchoolDepartment of Gastroenterology, Hepatology and Endocrinology, Hannover Medical SchoolDepartment of Gastroenterology, Hepatology and Endocrinology, Hannover Medical SchoolDepartment of Visceral and Transplantation Surgery, Hannover Medical SchoolDepartment of Pathology, Hannover Medical SchoolDepartment of Gastroenterology, Hepatology and Endocrinology, Hannover Medical SchoolDr. Margarete-Fischer-Bosch Institute of Clinical PharmacologyInterfaculty Institute of Biochemistry, University of TübingenDepartment of Gastroenterology, Hepatology and Endocrinology, Hannover Medical SchoolAbstract Hepatocellular carcinoma (HCC) represents a global health challenge with limited therapeutic options. Anti-angiogenic immune checkpoint inhibitor-based combination therapy has been introduced for progressed HCC, but improves survival only in a subset of HCC patients. Tyrosine-kinase inhibitors (TKI) such as sorafenib represent an alternative treatment option but have only modest efficacy. Using different HCC cell lines and HCC tissues from various patients reflecting HCC heterogeneity, we investigated whether the sorafenib response could be enhanced by combination with pro-apoptotic agents, such as TNF-related apoptosis-inducing ligand (TRAIL) or the BH3-mimetic ABT-737, which target the death receptor and mitochondrial pathway of apoptosis, respectively. We found that both agents could enhance sorafenib-induced cell death which was, however, dependent on specific BH3-only proteins. TRAIL augmented sorafenib-induced cell death only in NOXA-expressing HCC cells, whereas ABT-737 enhanced the sorafenib response also in NOXA-deficient cells. ABT-737, however, failed to augment sorafenib cytotoxicity in the absence of BIM, even when NOXA was strongly expressed. In the presence of NOXA, BIM-deficient HCC cells could be in turn strongly sensitized for cell death induction by the combination of sorafenib with TRAIL. Accordingly, HCC tissues sensitive to apoptosis induction by sorafenib and TRAIL revealed enhanced NOXA expression compared to HCC tissues resistant to this treatment combination. Thus, our results suggest that BH3-only protein expression determines the treatment response of HCC to different sorafenib-based drug combinations. Individual profiling of BH3-only protein expression might therefore assist patient stratification to certain TKI-based HCC therapies.https://doi.org/10.1038/s41419-021-04020-z
collection DOAJ
language English
format Article
sources DOAJ
author Stephanie Busche
Katharina John
Franziska Wandrer
Florian W. R. Vondran
Ulrich Lehmann
Heiner Wedemeyer
Frank Essmann
Klaus Schulze-Osthoff
Heike Bantel
spellingShingle Stephanie Busche
Katharina John
Franziska Wandrer
Florian W. R. Vondran
Ulrich Lehmann
Heiner Wedemeyer
Frank Essmann
Klaus Schulze-Osthoff
Heike Bantel
BH3-only protein expression determines hepatocellular carcinoma response to sorafenib-based treatment
Cell Death and Disease
author_facet Stephanie Busche
Katharina John
Franziska Wandrer
Florian W. R. Vondran
Ulrich Lehmann
Heiner Wedemeyer
Frank Essmann
Klaus Schulze-Osthoff
Heike Bantel
author_sort Stephanie Busche
title BH3-only protein expression determines hepatocellular carcinoma response to sorafenib-based treatment
title_short BH3-only protein expression determines hepatocellular carcinoma response to sorafenib-based treatment
title_full BH3-only protein expression determines hepatocellular carcinoma response to sorafenib-based treatment
title_fullStr BH3-only protein expression determines hepatocellular carcinoma response to sorafenib-based treatment
title_full_unstemmed BH3-only protein expression determines hepatocellular carcinoma response to sorafenib-based treatment
title_sort bh3-only protein expression determines hepatocellular carcinoma response to sorafenib-based treatment
publisher Nature Publishing Group
series Cell Death and Disease
issn 2041-4889
publishDate 2021-07-01
description Abstract Hepatocellular carcinoma (HCC) represents a global health challenge with limited therapeutic options. Anti-angiogenic immune checkpoint inhibitor-based combination therapy has been introduced for progressed HCC, but improves survival only in a subset of HCC patients. Tyrosine-kinase inhibitors (TKI) such as sorafenib represent an alternative treatment option but have only modest efficacy. Using different HCC cell lines and HCC tissues from various patients reflecting HCC heterogeneity, we investigated whether the sorafenib response could be enhanced by combination with pro-apoptotic agents, such as TNF-related apoptosis-inducing ligand (TRAIL) or the BH3-mimetic ABT-737, which target the death receptor and mitochondrial pathway of apoptosis, respectively. We found that both agents could enhance sorafenib-induced cell death which was, however, dependent on specific BH3-only proteins. TRAIL augmented sorafenib-induced cell death only in NOXA-expressing HCC cells, whereas ABT-737 enhanced the sorafenib response also in NOXA-deficient cells. ABT-737, however, failed to augment sorafenib cytotoxicity in the absence of BIM, even when NOXA was strongly expressed. In the presence of NOXA, BIM-deficient HCC cells could be in turn strongly sensitized for cell death induction by the combination of sorafenib with TRAIL. Accordingly, HCC tissues sensitive to apoptosis induction by sorafenib and TRAIL revealed enhanced NOXA expression compared to HCC tissues resistant to this treatment combination. Thus, our results suggest that BH3-only protein expression determines the treatment response of HCC to different sorafenib-based drug combinations. Individual profiling of BH3-only protein expression might therefore assist patient stratification to certain TKI-based HCC therapies.
url https://doi.org/10.1038/s41419-021-04020-z
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