Inhibition of SIRT7 overcomes sorafenib acquired resistance by suppressing ERK1/2 phosphorylation via the DDX3X-mediated NLRP3 inflammasome in hepatocellular carcinoma.

Kim, Yuna; Jung, Kwan-Young; Kim, Yun Hak; Xu, Pan; Kang, Baeki E; Jo, Yunju; Pandit, Navin; Kwon, Jeongho; Gariani, Karim; Gariani, Joanna; Lee, Junguee; Verbeek, Jef; Nam, Seungyoon; Bae, Sung-Jin; Ha, Ki-Tae; Yi, Hyon-Seung; Shong, Minho; Kim, Kyun-Hwan; Kim, Doyoun; Jung, Hee Jung; Lee, Chang-Woo; Kim, Kwang Rok; Schoonjans, Kristina; Auwerx, Johan; Ryu, Dongryeol

Kim, Yuna; Jung, Kwan-Young; Kim, Yun Hak; Xu, Pan; Kang, Baeki E; Jo, Yunju; Pandit, Navin; Kwon, Jeongho; Gariani, Karim; Gariani, Joanna; Lee, Junguee; Verbeek, Jef; Nam, Seungyoon; Bae, Sung-Jin; Ha, Ki-Tae; Yi, Hyon-Seung; Shong, Minho; Kim, Kyun-Hwan; Kim, Doyoun; Jung, Hee Jung; Lee, Chang-Woo; Kim, Kwang Rok; Schoonjans, Kristina; Auwerx, Johan; Ryu, Dongryeol.

Affiliation

Kim Y; Department of Molecular Cell Biology, Sungkyunkwan University School of Medicine, Suwon, Republic of Korea. Electronic address: yuna716@skku.edu.
Jung KY; Therapeutics & Biotechnology Division, Korea Research Institute of Chemical Technology, Daejeon, Republic of Korea.
Kim YH; Department of Anatomy, School of Medicine, Pusan National University, Yangsan, Republic of Korea; Department of Biomedical Informatics, School of Medicine, Pusan National University, Yangsan, Republic of Korea.
Xu P; Laboratory of Integrative Systems Physiology, Institute of Bioengineering, Ecole Polytechnique Federale de Lausanne, Lausanne, Switzerland.
Kang BE; Department of Molecular Cell Biology, Sungkyunkwan University School of Medicine, Suwon, Republic of Korea.
Jo Y; Department of Biomedical Science and Engineering, Gwangju Institute of Science and Technology, Gwangju, Republic of Korea.
Pandit N; Therapeutics & Biotechnology Division, Korea Research Institute of Chemical Technology, Daejeon, Republic of Korea.
Kwon J; Department of Molecular Cell Biology, Sungkyunkwan University School of Medicine, Suwon, Republic of Korea.
Gariani K; Service of Endocrinology, Diabetes, Nutrition and Therapeutic Patient Education, Geneva University Hospitals, Geneva, Switzerland.
Gariani J; Department of radiology, Hirslanden Grangettes Clinic, Geneva, Switzerland.
Lee J; Department of Pathology, Daejeon St. Mary's Hospital, College of Medicine, The Catholic University of Korea, Daejeon, Republic of Korea.
Verbeek J; Laboratory of Hepatology, Department of Chronic Diseases and Metabolism (CHROMETA), KU Leuven, Belgium; Department of Gastroenterology and Hepatology, University Hospitals KU Leuven, Leuven, Belgium.
Nam S; Department of Genome Medicine and Science, AI Convergence Center for Medical Science, Gachon Institute of Genome Medicine and Science, Gachon University Gil Medical Center, Gachon University College of Medicine, Incheon, Republic of Korea; Department of Health Sciences and Technology, Gachon Advance
Bae SJ; Department of Molecular Biology and Immunology, Kosin University College of Medicine, Busan, Republic of Korea.
Ha KT; Department of Korean Medical Science, Pusan National University School of Korean Medicine, Yangsan, Republic of Korea.
Yi HS; Laboratory of Endocrinology and Immune System, Chungnam National University School of Medicine, Daejeon, Republic of Korea.
Shong M; Research Center for Endocrine and Metabolic Diseases, Chungnam National University School of Medicine, Daejeon, Republic of Korea.
Kim KH; Department of Molecular Cell Biology, Sungkyunkwan University School of Medicine, Suwon, Republic of Korea.
Kim D; Therapeutics & Biotechnology Division, Korea Research Institute of Chemical Technology, Daejeon, Republic of Korea.
Jung HJ; Therapeutics & Biotechnology Division, Korea Research Institute of Chemical Technology, Daejeon, Republic of Korea.
Lee CW; Department of Molecular Cell Biology, Sungkyunkwan University School of Medicine, Suwon, Republic of Korea.
Kim KR; Therapeutics & Biotechnology Division, Korea Research Institute of Chemical Technology, Daejeon, Republic of Korea. Electronic address: kkrok@krict.re.kr.
Schoonjans K; Laboratory of Integrative Systems Physiology, Institute of Bioengineering, Ecole Polytechnique Federale de Lausanne, Lausanne, Switzerland. Electronic address: kristina.schoonjans@epfl.ch.
Auwerx J; Laboratory of Integrative Systems Physiology, Institute of Bioengineering, Ecole Polytechnique Federale de Lausanne, Lausanne, Switzerland. Electronic address: admin.auwerx@epfl.ch.
Ryu D; Department of Molecular Cell Biology, Sungkyunkwan University School of Medicine, Suwon, Republic of Korea; Department of Biomedical Science and Engineering, Gwangju Institute of Science and Technology, Gwangju, Republic of Korea. Electronic address: dryu@gist.ac.kr.

Drug Resist Updat ; 73: 101054, 2024 Mar.

Article in En | MEDLINE | ID: mdl-38277756

ABSTRACT

ABSTRACT

AIMS:

Sirtuin 7 (SIRT7) plays an important role in tumor development, and has been characterized as a potent regulator of cellular stress. However, the effect of SIRT7 on sorafenib acquired resistance remains unclear and a possible anti-tumor mechanism beyond this process in HCC has not been clarified. We examined the therapeutic potential of SIRT7 and determined whether it functions synergistically with sorafenib to overcome chemoresistance.

METHODS:

Cancer Genome Atlas-liver HCC data and unbiased gene set enrichment analyses were used to identify SIRT7 as a potential effector molecule in sorafenib acquired resistance. Two types of SIRT7 chemical inhibitors were developed to evaluate its therapeutic properties when synergized with sorafenib. Mass spectrometry was performed to discover a direct target of SIRT7, DDX3X, and DDX3X deacetylation levels and protein stability were explored. Moreover, an in vivo xenograft model was used to confirm anti-tumor effect of SIRT7 and DDX3X chemical inhibitors combined with sorafenib.

RESULTS:

SIRT7 inhibition mediated DDX3X depletion can re-sensitize acquired sorafenib resistance by disrupting NLRP3 inflammasome assembly, finally suppressing hyperactive ERK1/2 signaling in response to NLRP3 inflammasome-mediated IL-1ß inhibition.

CONCLUSIONS:

SIRT7 is responsible for sorafenib acquired resistance, and its inhibition would be beneficial when combined with sorafenib by suppressing hyperactive pro-cell survival ERK1/2 signaling.

Subject(s)

Carcinoma, Hepatocellular; Liver Neoplasms; Sirtuins; Humans; Carcinoma, Hepatocellular/drug therapy; Carcinoma, Hepatocellular/genetics; Sorafenib/pharmacology; Sorafenib/therapeutic use; Liver Neoplasms/drug therapy; Liver Neoplasms/genetics; Inflammasomes/metabolism; Inflammasomes/pharmacology; Phosphorylation; NLR Family, Pyrin Domain-Containing 3 Protein/genetics; NLR Family, Pyrin Domain-Containing 3 Protein/metabolism; MAP Kinase Signaling System; Drug Resistance, Neoplasm/genetics; Cell Line, Tumor; Cell Proliferation; DEAD-box RNA Helicases/genetics; DEAD-box RNA Helicases/metabolism; DEAD-box RNA Helicases/pharmacology; Sirtuins/genetics; Sirtuins/metabolism; Sirtuins/pharmacology

Key words

DDX3X; ERK1/2 phosphorylation; Hepatocellular carcinoma; SIRT7 inhibitor; Sorafenib resistance

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Full text: 1 Collection: 01-internacional Database: MEDLINE Main subject: Carcinoma, Hepatocellular / Sirtuins / Liver Neoplasms Limits: Humans Language: En Journal: Drug Resist Updat Year: 2024 Document type: Article

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