4.2 Article

CLIC1 Promotes the Progression of Gastric Cancer by Regulating the MAPK/AKT Pathways

CELLULAR PHYSIOLOGY AND BIOCHEMISTRY (2018)

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Journal

CELLULAR PHYSIOLOGY AND BIOCHEMISTRY
Volume 46, Issue 3, Pages 907-924

Publisher

KARGER
DOI: 10.1159/000488822

Keywords

Chloride intracellular channel 1; Gastric cancer; Integrins; MAPKs; AKT

Categories

Cell Biology Physiology

Funding

  1. National Natural Science Foundation of China [81360370]
  2. Scientific Research and Technology-development Program of Guangxi [1598011-4]
  3. Scientific Research Project of Guangxi Zhuang Autonomous Region People's Government [2014396]
  4. Natural Science Foundation of Guangxi [2016GXNSFAA380180]
  5. Research Project of Guangxi Health and Family Planning Commission [Z2015526]
  6. Science Foundation for Young Scientists of Guangxi Medical University [GXMUYSF201502]

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Background/Aims: Chloride intracellular channel 1 (CLIC1), which is a member of the chloride channel protein family, is associated with various human tumors. Recent studies have shown that CLIC1 is involved in the occurrence and development of gastric cancer (GC). However, the exact mechanism remains unclear in GC. Methods: Effects of CLIC1 on the progression of GC in vivo and in vitro and the potential underlying mechanisms have been investigated by analysing 54 patients with GC, as well as human gastric cell lines SGC-7901 and MGC-803, utilizing proteomics, RT-PCR, Western blotting, flow cytometry, Cell invasion and migration assays and xenograft tumor models. Results: Our study shows that CLIC1 knockdown by targeted-siRNA markedly inhibits GC cell invasion and migration and induces apoptosis in vitro. In total, 54 differentially expressed proteins were identified in GC cells SGC-7901 after CLIC1 silencing by isobaric tags for relative isotope labeled and absolute quantitation (iTRAQ) technology, including integrin alpha 1 (ITG alpha 1) and ITG alpha 3. The expression levels of ITG alpha 3, ITG alpha v, ITG beta 1 and Bcl-2 mRNA and protein were decreased significantly in GC cells after CLIC1 knockdown; ITGa1 and Fas were upregulated, but the level of survivin was not significantly different. GC growth and metabolism were decreased in vivo after CLIC1 silencing, but apoptosis was markedly increased. Further study showed that the expression levels of ITG alpha 3, ITG alpha v and ITG beta 1, as well as AKT-phosphorylation, ERK-phosphorylation and p38-phosphorylation, were reduced in vivo after CLIC1 knockdown, while ITG alpha 1 was upregulated. Conclusions: We speculate that CLIC1 may play an important role in the progression of GC, and its mechanism may be related to the regulation of integrin family proteins, which leads to the sequential regulation of the PI3K/AKT, MAPK/ERK and MAPK/p38 pathways. (C) 2018 The Author(s) Published by S. Karger AG, Basel

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