Calunduloside E inhibits HepG2 cell proliferation and migration via p38/JNK-HMGB1 signalling axis

Calunduloside E inhibits HepG2 cell proliferation and migration via p38/JNK-HMGB1 signalling axis

High-mobility group box 1 (HMGB1), a highly conserved chromosome protein, is considered as a potential therapeutic target and novel biomarker because of its regulation in the proliferation and metastasis of Hepatocellular carcinoma (HCC). Calenduloside E (CE), a natural active product, has been repo...

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Main Authors: Shengnan Wang, Xuelei Chen, Jin Cheng, Tianyu Cai, Xiaoming Wu, Zhenyu Cheng, Shimei Qi, Zhilin Qi
Format: Article
Language:English
Published: Elsevier 2021-09-01
Series:Journal of Pharmacological Sciences
Subjects:
Calunduloside E
HepG2 cells
HMGB1
Proliferation
Migration
Online Access:http://www.sciencedirect.com/science/article/pii/S1347861321000475
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spelling doaj-e0a2ff28f0364c5b89c9126eb7d72ea42021-07-21T04:10:31ZengElsevierJournal of Pharmacological Sciences1347-86132021-09-0114711826Calunduloside E inhibits HepG2 cell proliferation and migration via p38/JNK-HMGB1 signalling axisShengnan Wang0Xuelei Chen1Jin Cheng2Tianyu Cai3Xiaoming Wu4Zhenyu Cheng5Shimei Qi6Zhilin Qi7Department of Biochemistry and Molecular Biology, PR China; Anhui Province Key Laboratory of Active Biological Macro-molecules, PR ChinaDepartment of Biochemistry and Molecular Biology, PR China; Anhui Province Key Laboratory of Active Biological Macro-molecules, PR ChinaAnhui Province Key Laboratory of Active Biological Macro-molecules, PR China; School of Clinical Medicine, Wannan Medical College, Wuhu, Anhui 241002, PR ChinaAnhui Province Key Laboratory of Active Biological Macro-molecules, PR China; School of Clinical Medicine, Wannan Medical College, Wuhu, Anhui 241002, PR ChinaAnhui Province Key Laboratory of Active Biological Macro-molecules, PR China; School of Clinical Medicine, Wannan Medical College, Wuhu, Anhui 241002, PR ChinaAnhui Province Key Laboratory of Active Biological Macro-molecules, PR China; School of Clinical Medicine, Wannan Medical College, Wuhu, Anhui 241002, PR ChinaDepartment of Biochemistry and Molecular Biology, PR China; Anhui Province Key Laboratory of Active Biological Macro-molecules, PR China; Corresponding author. Department of Biochemistry and Molecular biology, Wannan Medical College, No.22 Wenchang West Road, Wuhu, Anhui 241002, PR China.Department of Biochemistry and Molecular Biology, PR China; Anhui Province Key Laboratory of Active Biological Macro-molecules, PR China; Corresponding author. Department of Biochemistry and Molecular biology, Wannan Medical College, No.22 Wenchang West Road, Wuhu, Anhui 241002, PR China.High-mobility group box 1 (HMGB1), a highly conserved chromosome protein, is considered as a potential therapeutic target and novel biomarker because of its regulation in the proliferation and metastasis of Hepatocellular carcinoma (HCC). Calenduloside E (CE), a natural active product, has been reported to anti-cancer effect. However, the role and underlying molecular mechanism of CE in HCC is still unclear. The purpose of this study is to investigate the effects of CE on the proliferation and migration of HCC, and then explore the possible underlying molecular mechanism. HepG2 cells were treated with CE or transfected with HMGB1 shRNA plasmids, EdU and colony formation assays were used to detect cell proliferation ability. Wound healing and transwell assays were used to determine the role of CE in cell migration. The expression of Cyclins, PCNA, MMPs, HMGB1, N-cadherin, E-cadherin and phosphorylation of p38, ERK and JNK were all detected using Western blotting. Our results showed that CE inhibited HepG2 cells proliferation and migration in a dose dependent manner; reduced the expression levels of Cycins, PCNA, HMGB1, MMPs and N-cadherin; up-regulated E-cadherin expression; enhanced the phosphorylation of p38 and JNK signalling pathways. Blocking the activation of p38 and JNK obviously reversed CE-mediated inhibitory effects on HepG2 cell proliferation and migration; reversed CE-induced down-regulation of Cyclins, PCNA, MMPs, N-cadherin and HMGB1, as well as E-cadherin up-regulation. In conclusion, our study suggested that CE reduces the expression levels of Cyclins, MMPs and epithelial-mesenchymal transformation (EMT) through p38/JNK-HMGB1 signaling axis and then inhibits HepG2 cells proliferation and migration in HepG2 cells. This study provides a new perspective for the anti-tumour molecular mechanism of CE in HCC.http://www.sciencedirect.com/science/article/pii/S1347861321000475Calunduloside EHepG2 cellsHMGB1ProliferationMigration
collection DOAJ
language English
format Article
sources DOAJ
author Shengnan Wang
Xuelei Chen
Jin Cheng
Tianyu Cai
Xiaoming Wu
Zhenyu Cheng
Shimei Qi
Zhilin Qi
spellingShingle Shengnan Wang
Xuelei Chen
Jin Cheng
Tianyu Cai
Xiaoming Wu
Zhenyu Cheng
Shimei Qi
Zhilin Qi
Calunduloside E inhibits HepG2 cell proliferation and migration via p38/JNK-HMGB1 signalling axis
Journal of Pharmacological Sciences
Calunduloside E
HepG2 cells
HMGB1
Proliferation
Migration
author_facet Shengnan Wang
Xuelei Chen
Jin Cheng
Tianyu Cai
Xiaoming Wu
Zhenyu Cheng
Shimei Qi
Zhilin Qi
author_sort Shengnan Wang
title Calunduloside E inhibits HepG2 cell proliferation and migration via p38/JNK-HMGB1 signalling axis
title_short Calunduloside E inhibits HepG2 cell proliferation and migration via p38/JNK-HMGB1 signalling axis
title_full Calunduloside E inhibits HepG2 cell proliferation and migration via p38/JNK-HMGB1 signalling axis
title_fullStr Calunduloside E inhibits HepG2 cell proliferation and migration via p38/JNK-HMGB1 signalling axis
title_full_unstemmed Calunduloside E inhibits HepG2 cell proliferation and migration via p38/JNK-HMGB1 signalling axis
title_sort calunduloside e inhibits hepg2 cell proliferation and migration via p38/jnk-hmgb1 signalling axis
publisher Elsevier
series Journal of Pharmacological Sciences
issn 1347-8613
publishDate 2021-09-01
description High-mobility group box 1 (HMGB1), a highly conserved chromosome protein, is considered as a potential therapeutic target and novel biomarker because of its regulation in the proliferation and metastasis of Hepatocellular carcinoma (HCC). Calenduloside E (CE), a natural active product, has been reported to anti-cancer effect. However, the role and underlying molecular mechanism of CE in HCC is still unclear. The purpose of this study is to investigate the effects of CE on the proliferation and migration of HCC, and then explore the possible underlying molecular mechanism. HepG2 cells were treated with CE or transfected with HMGB1 shRNA plasmids, EdU and colony formation assays were used to detect cell proliferation ability. Wound healing and transwell assays were used to determine the role of CE in cell migration. The expression of Cyclins, PCNA, MMPs, HMGB1, N-cadherin, E-cadherin and phosphorylation of p38, ERK and JNK were all detected using Western blotting. Our results showed that CE inhibited HepG2 cells proliferation and migration in a dose dependent manner; reduced the expression levels of Cycins, PCNA, HMGB1, MMPs and N-cadherin; up-regulated E-cadherin expression; enhanced the phosphorylation of p38 and JNK signalling pathways. Blocking the activation of p38 and JNK obviously reversed CE-mediated inhibitory effects on HepG2 cell proliferation and migration; reversed CE-induced down-regulation of Cyclins, PCNA, MMPs, N-cadherin and HMGB1, as well as E-cadherin up-regulation. In conclusion, our study suggested that CE reduces the expression levels of Cyclins, MMPs and epithelial-mesenchymal transformation (EMT) through p38/JNK-HMGB1 signaling axis and then inhibits HepG2 cells proliferation and migration in HepG2 cells. This study provides a new perspective for the anti-tumour molecular mechanism of CE in HCC.
topic Calunduloside E
HepG2 cells
HMGB1
Proliferation
Migration
url http://www.sciencedirect.com/science/article/pii/S1347861321000475
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AT jincheng calundulosideeinhibitshepg2cellproliferationandmigrationviap38jnkhmgb1signallingaxis
AT tianyucai calundulosideeinhibitshepg2cellproliferationandmigrationviap38jnkhmgb1signallingaxis
AT xiaomingwu calundulosideeinhibitshepg2cellproliferationandmigrationviap38jnkhmgb1signallingaxis
AT zhenyucheng calundulosideeinhibitshepg2cellproliferationandmigrationviap38jnkhmgb1signallingaxis
AT shimeiqi calundulosideeinhibitshepg2cellproliferationandmigrationviap38jnkhmgb1signallingaxis
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