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JNK1 activation predicts the prognostic outcome of the human hepatocellular carcinoma.

Authors

Chang-QS; Chen-JG; Beezhold-KJ; Castranova-V; Shi-XL; Chen-F

Source

Mol Cancer 2009 Aug; 8:64

Link

http://dx.doi.org/10.1186/1476-4598-8-64

NIOSHTIC No.

20035962

Abstract

Background: Hepatocellular carcinoma (HCC) is one of the most common cancers worldwide with an extremely poor prognosis. The classification of HCC based on the molecular signature is not well-established. Results: In the present study, we reported HCC signature genes based on the JNK1 activation status in 31 HCC specimens relative to the matched distal noncancerous liver tissue from 31 patients. The HCCs with high JNK1 (H-JNK1) and low JNK1 (L-JNK1) were sub-grouped. Two different signature gene sets for both H-JNK1 and L-JNK1 HCC were identified through gene expression profiling. A striking overlap of signature genes was observed between the H-JNK1 HCC and the hepatoblastoma or hepatoblastoma-type HCC. Many established biomarkers for hepatic progenitor cells were over-expressed in H-JNK1 HCC, including AFP, TACSTD1, KRT19, KRT7, THY1, and PROM1. In addition, the majority of the most up-regulated genes were those associated with metastasis and earlier recurrence, whereas the genes for normal liver function were substantially down-regulated in H-JNK1 HCC tissue. A Kaplan-Meier plot demonstrated that the survival of the patients with H-JNK1 HCC was severely impaired. Conclusion: Accordingly, we believe that the H-JNK1 HCC may originate from hepatic progenitor cells and is associated with poorer prognosis. The status of JNK1 activation in HCC tissue, thus, might be a new biomarker for HCC prognosis and therapeutic targeting.

Keywords

Biological-monitoring; Biomarkers; Cancer; Cell-biology; Cell-damage; Cell-growth; Cell-metabolism; Cell-morphology; Cellular-reactions; Genes; Genetic-factors; Hepatocytes; Liver-cancer; Liver-cells; Liver-disorders

Contact

Fei Chen, CDC, National Institute for Occupational Safety and Health, Pathology and Physiology Research Branch, The Health Effects Laboratory Division, Morgantown, WV 26505

CODEN

MCOACG

Publication Date

20090817

Document Type

Journal Article

Email Address

fchen@cdc.gov

Fiscal Year

2009

NTIS Accession No.

NTIS Price

ISSN

1476-4598

NIOSH Division

HELD

Priority Area

Manufacturing; Mining

Source Name

Molecular Cancer

State

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Page last reviewed:June 7, 2016
Page last updated:March 31, 2017
Content source:
- National Institute for Occupational Safety and Health
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