9 7 3 1 8
论文已发表
注册即可获取德孚的最新动态
IF 收录期刊
- 3.3 Breast Cancer (Dove Med Press)
- 3.4 Clin Epidemiol
- 2.5 Cancer Manag Res
- 2.9 Infect Drug Resist
- 3.5 Clin Interv Aging
- 4.7 Drug Des Dev Ther
- 2.7 Int J Chronic Obstr
- 6.6 Int J Nanomed
- 2.5 Int J Women's Health
- 2.5 Neuropsych Dis Treat
- 2.7 OncoTargets Ther
- 2.0 Patient Prefer Adher
- 2.3 Ther Clin Risk Manag
- 2.5 J Pain Res
- 2.8 Diabet Metab Synd Ob
- 2.8 Psychol Res Behav Ma
- 3.0 Nat Sci Sleep
- 1.8 Pharmgenomics Pers Med
- 2.7 Risk Manag Healthc Policy
- 4.2 J Inflamm Res
- 2.1 Int J Gen Med
- 4.2 J Hepatocell Carcinoma
- 3.7 J Asthma Allergy
- 1.9 Clin Cosmet Investig Dermatol
- 2.7 J Multidiscip Healthc
DcR3 的下调使肝癌细胞对 TRAIL 诱导凋亡敏感
Authors Liang CJ, Xu YC, Li GM, Zhao TJ, Xia F, Li GQ, Zhang D, Wu JX
Received 10 November 2016
Accepted for publication 5 December 2016
Published 18 January 2017 Volume 2017:10 Pages 417—428
DOI https://doi.org/10.2147/OTT.S127202
Checked for plagiarism Yes
Review by Single-blind
Peer reviewers approved by Dr Amy Norman
Peer reviewer comments 2
Editor who approved publication: Dr William Cho
Abstract: Decoy receptor 3 (DcR3) has been recently described as an antiapoptosis
and prometastasis factor since it can competitively bind to FasL, TL1A, and
LIGHT, and it is highly expressed in many malignant tumors. Downregulation of
DcR3 can promote tumor cell apoptosis and inhibit metastasis. A previous study
demonstrated that reduction of DcR3 could induce tumor necrosis factor-related
apoptosis-inducing ligand (TRAIL)-mediated apoptosis in pancreatic cancer
cells. However, whether such an effect is seen in hepatocellular carcinoma
(HCC) remains to be explored. This study was designed to investigate the
sensitivity of HCC cells to TRAIL after silencing DcR3, and this was done by
evaluating the expression of DcR3 in HCC cells and the effect on TRAIL-mediated
apoptosis after downregulation of DcR3. Our data showed that DcR3 was highly
expressed in HepG2, BEL-7402, Hep3B, Huh-7, MHCC97H, and SMCC7721 cell lines
compared with normal liver cell line LO-2. Both HepG2 and BEL-7402 were
tolerant to TRAIL-mediated apoptosis, and the tolerance was negatively
correlated to the expression of DcR3. Silencing of DcR3 with shRNA and
treatment with TRAIL induced obvious apoptosis in HepG2 and BEL-7402, with more
cancer cells found in the G1 phase. SiDcR3 combined with TRAIL could induce
activation of caspases-3, -8, and -9, raise the expression of the apoptotic
protein Bax, and reduce the expression of antiapoptotic proteins (Bcl-2, Mcl-1,
Bcl-XL, IAP-2, and survivin). Caspase-8 inhibitor Ac-IETD-CHO significantly
decreased the activation of caspase cascade, indicating that the extrinsic
pathway may have a vital role in the apoptotic events induced by SiDcR3/TRAIL.
Furthermore, our results showed that the TRAIL death receptor 5 (DR5) was
upregulated and that DR5 neutralizing antibody abrogated the effect of SiDcR3.
Our results demonstrated that downregulation of DcR3 could enhance
TRAIL-mediated apoptosis in HCC through the death receptor pathway. In the
future, this might be useful as a clinical treatment method of liver cancer.
Keywords: apoptosis, DcR3, TRAIL, HCC, DR5,
caspase-8
