Abstract

Non-steroidal anti-inflammatory drugs (NSAIDs) are used for the treatment of inflammatory diseases. Recently, NSAIDs have been reported to have a chemopreventive effect on the development of human colorectal cancer. However, some reports indicate that the chemopreventive effect on colon cancer may, in part, be independent of prostaglandin inhibition. In preliminary experiments, NSAIDs (indomethacin & aspirin) treatment of human colon cancer cells as well as breast and lung cancer cells causes the up-regulation of novel gene (name as nrg-1) which we have characterized as member of the TGF-Beta superfamily gene. Although they used different names (PTGFB, MIC-1, PDF, PLAB, and novel TGF-Beta gene), the sequence analysis revealed that the five genes are almost identical to each other and belong to the new TGF-Beta superfamily with unknown biological function. We have now sequenced the entire gene induced by Indo in HCT-116 cells and the sequence is identical to sequences reported. Indo induces nrg-1 gene expression with time and concentration dependent manner with highest expression at 48 hrs and 100mM indo. Indo also induced an increase in expression of nrg-1 in other cell lines, breast cell, prostate, and macrophage. In addition, we tested several inactive precursors or metabolites of NSAIDs, which are devoid of the ability to inhibit Cox-1/2. These inactive chemicals do not induce nrg-1 expression. Since the concentration of NSAID required to induce nrg-1 expression is higher than the concentration required to inhibit Cox-1/2, we suspected that the expression was not related to Cox-1/2 inhibition. Previous reports indicate NSAIDS at the concentrations used in our experiments to be ligands for PPARg. We measured the activation of PPARgamma by a luciferase assay using a system. It appears there is a relationship between activation of PPARg and increased expression of nrg-1. We tested several PPARgamma activators (BRL-troglitazone) and these chemicals were very potent inducers of nrg-1 expression. Moreover, nrg-1 expression in response to PPARg activators was very rapid compared to the NSAID response. Since both NSAIDs and troglitazone reduce several cancers in animals, one could hypothesize a common mechanism via the increased expression of nrg-1. Preliminary studies with cells in culture indicate NSAIDs and troglitazone are inducing apoptosis and some data suggests that nrg-1 may play an important role preventing tumor growth. - Prostaglandin H synhase, TGFBeta, NSAIDs, apoptosis, PPAR, colorectal cancer

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Environmental Health Sciences (NIEHS)
Type
Intramural Research (Z01)
Project #
1Z01ES010016-01
Application #
6227934
Study Section
Special Emphasis Panel (LMC)
Project Start
Project End
Budget Start
Budget End
Support Year
1
Fiscal Year
1999
Total Cost
Indirect Cost

  Institution

Name
National Institute of Environmental Health Sciences
Department
Type
DUNS #
City
State
Country
United States
Zip Code

  Publications

Binder, April K; Kosak, Justin P; Janardhan, Kyathanahalli S et al. (2016) Expression of Human NSAID Activated Gene 1 in Mice Leads to Altered Mammary Gland Differentiation and Impaired Lactation. PLoS One 11:e0146518
Ge, C; Zhao, G; Li, Y et al. (2016) Role of Runx2 phosphorylation in prostate cancer and association with metastatic disease. Oncogene 35:366-76
Min, K-W; Liggett, J L; Silva, G et al. (2016) NAG-1/GDF15 accumulates in the nucleus and modulates transcriptional regulation of the Smad pathway. Oncogene 35:377-88
Wang, Xingya; Chrysovergis, Kali; Kosak, Justin et al. (2014) Lower NLRP3 inflammasome activity in NAG-1 transgenic mice is linked to a resistance to obesity and increased insulin sensitivity. Obesity (Silver Spring) 22:1256-63
Chrysovergis, K; Wang, X; Kosak, J et al. (2014) NAG-1/GDF-15 prevents obesity by increasing thermogenesis, lipolysis and oxidative metabolism. Int J Obes (Lond) 38:1555-64
Wang, Xingya; Chrysovergis, Kali; Kosak, Justin et al. (2014) hNAG-1 increases lifespan by regulating energy metabolism and insulin/IGF-1/mTOR signaling. Aging (Albany NY) 6:690-704
Kim, J M; Kosak, J P; Kim, J K et al. (2013) NAG-1/GDF15 transgenic mouse has less white adipose tissue and a reduced inflammatory response. Mediators Inflamm 2013:641851
Wang, Xingya; Baek, Seung Joon; Eling, Thomas E (2013) The diverse roles of nonsteroidal anti-inflammatory drug activated gene (NAG-1/GDF15) in cancer. Biochem Pharmacol 85:597-606
Kambe, Atsushi; Yoshioka, Hiroki; Kamitani, Hideki et al. (2009) The cyclooxygenase inhibitor sulindac sulfide inhibits EP4 expression and suppresses the growth of glioblastoma cells. Cancer Prev Res (Phila) 2:1088-99
Moon, Yuseok; Kim, Jeung Il; Yang, Hyun et al. (2008) Growth compensatory role of sulindac sulfide-induced thrombospondin-1 linked with ERK1/2 and RhoA GTPase signaling pathways. Life Sci 82:591-9

Showing the most recent 10 out of 41 publications