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Recent News and Articles on the Keywords: pancreatic cancer + cox-2 inhibitor + cancer  Related to the article below (Last Update: 5/12/2008)

Mouth test could predict lung cancer, study finds
Reuters - Apr 13, 2008
"Not only lung cancer, but pancreatic, bladder and head and neck cancers, which also are associated with tobacco use." Smoking is the leading cause of lung ...
Source: Google News

Cyclooxygenase-2 Expression Is Up-Regulated in Human Pancreatic Cancer 1 -
ON Tucker, AJ Dannenberg, EK Yang, F Zhang, L Teng … - Cancer Research, 1999 - AACR
... in pancreatic cancer. Our data show that levels of COX-2 are increased in
adenocarcinoma of the pancreas and raise the possibility that selective inhibitors ...

Blockade of cyclooxygenase-2 inhibits proliferation and induces apoptosis in human pancreatic cancer -
XZ Ding, WG Tong, TE Adrian - Anticancer Res, 2000 - ncbi.nlm.nih.gov
... or the specific COX-2 inhibitor, NS-398, on [3H]-thymidine incorporation and cell
number was investigated in these four pancreatic cancer cell lines. ...

Cyclooxygenase-2 expression in human colon cancer cells increases metastatic potential -
M Tsujii, S Kawano, RN DuBois - Proceedings of the National Academy of Sciences, 1997 - National Acad Sciences
... of MMP-2 can be modulated by COX-2 and treatment ... CJ Sweeney, and CM Schmidt Suppression
of pancreatic tumor growth ... Cancer Ther., June 1, 2007; 6(6): 1736 - 1744 ...

… -2 Inhibitor Nimesulide Induces Apoptosis in Pancreatic Cancer Cells Independent of COX-2. -
G Eibl, HA Reber, MN Wente, OJ Hines - Pancreas, 2003 - pancreasjournal.com
... Conclusion: The selective COX-2 inhibitor nimesulide is antimitogenic in pancreatic
cancer cells, which is independent of COX-2 expression. ...

… -2 Inhibitor Celecoxib Induces Apoptosis by Blocking Akt Activation in Human Prostate Cancer Cells … -
AL Hsu, TT Ching, DS Wang, X Song, VM Rangnekar, … - Journal of Biological Chemistry, 2000 - ASBMB
... shown). These data imply that the induction of apoptosis in prostate cancer
cells by NSAIDs is a COX-2 inhibitor-specific event. ...

Increased expression of cyclooxygenase-2 in human pancreatic neoplasms and potential for … -
A Kokawa, H Kondo, T Gotoda, H Ono, D Saito, S … - Cancer, 2001 - doi.wiley.com
... dependent inhibitory effects on four pancreatic cell lines. ... the IC 50 of etodolac,
a COX-2-specific inhibitor ... with previous findings in colon cancer cell lines. ...

Growth Stimulation of COX-2-Negative Pancreatic Cancer by a Selective COX-2 Inhibitor -
G Eibl, Y Takata, LG Boros, J Liu, Y Okada, HA … - Cancer Research, 2005 - AACR
... Experimental Therapeutics, Molecular Targets, and Chemical Biology. Growth Stimulation
of COX-2?Negative Pancreatic Cancer by a Selective COX-2 Inhibitor. ...

[PDF] COLORECTAL CANCER PREVENTION AND TREATMENT BY INHIBITION OF CYCLOOXYGENASE-2 -
RA Gupta, RN DuBois? - Nature Reviews Cancer, 2001 - nature.com
... evidence implicating a role for host COX-2 in carcinoma ... subcutaneously in the flank
of Cox2 ?/? mice than ... limited role in pro- moting cancer progression in ...

… by specific COX-2 activity and increases VEGF production in COX-2-expressing human pancreatic cancer -
G Eibl, D Bruemmer, Y Okada, JP Duffy, RE Law, HA … - Biochemical and Biophysical Research Communications, 2003 - Elsevier
... This pro-migratory effect was completely inhibited by pre-incubation of the pancreatic
cancer cells with a selective COX-2 inhibitor and an EP 1 /EP 2 receptor ...

… ) induces expression of cell cycle arrest genes and slows tumor growth in human pancreatic cancer -
WW Tseng, A Deganutti, MN Chen, RE Saxton, CD Liu - Journal of Gastrointestinal Surgery, 2002 - Springer
... 14 To the best of our knowledge, no previous studies have reported ther- apeutic
effects of a selective COX-2 inhibitor on hu- man pancreatic cancer growth in ...

Source: Google Scholar

COX-2 inhibitors delay pancreatic cancer precursors in mice

PHILADELPHIA-- Nimesulide, a cyclooxygenase-2 (COX-2) inhibitor, delays the progression of precancerous pancreatic lesions in mice, according to researchers at David Geffen School of Medicine at UCLA. While inflammation has been shown to be a factor in many forms of cancer, the researchers say this is the first study to demonstrate the effect of an anti-inflammatory COX-2 inhibitor on the development of pancreatic cancer.

The study, published in the August 1 issue of Cancer Research, a journal of the American Association for Cancer Research, suggests a potential role for COX-2 inhibitors in pancreatic cancer prevention among high-risk patients. Pancreatic cancer is one of the leading causes of cancer death in America – over 33,000 Americans will likely die from the disease in 2007, according to projections from the American Cancer Society.

“By inhibiting COX-2 in human patients, we may have an option to delay the progression of lesions,” said lead author Guido Eibl, M.D., scientific director of the Hirshberg Laboratory of Pancreatic Cancer Research and adjunct assistant professor at UCLA .

Researchers believe pancreatic cancer arises from abnormal tissues, or lesions in the pancreas, known as pancreatic intraepithelial neoplasias (PanINs). By stalling the growth of PanINs, researchers hope to slow the development of or prevent pancreatic cancer.

COX-2, an enzyme which causes inflammation, is no stranger to cancer researchers. Studies of breast, colon, and pancreatic cancers have led researchers to believe COX-2 plays a key role in the development and growth of tumors.

To study the effects of COX-2 on PanIN progression, Dr. Eibl and colleagues focused on the KrasG12D mouse, an animal model that mimics the early stages of pancreatic cancer. In the KrasG12D mouse, low-grade PanINs (stage I or II) begin to appear in the pancreas of mice at one month. Starting at six months, high-grade PanINs (stage III) can be found in the mouse pancreas. According to Dr. Eibl, most researchers agree that stage III PanINs are a direct precursor to pancreatic cancer in humans as well as mice. Between 12 and 15 months, Dr. Eibl says the majority of KrasG12D mice will develop pancreatic tumors.

The UCLA researchers divided the mice into two groups – one set received a nimesulide-enriched diet for 10 months; the other was offered only regular mouse chow. Their analyses revealed that the nimesulide diet greatly reduced the number of late-stage PanINs in KrasG12D (10 percent of pancreatic ducts had PanIN-2 or -3 in KrasG12D mice on nimesulide diet versus 40 percent of pancreatic ducts had PanIN-2 or -3 in KrasG12D mice on normal diet).

Because the pancreases of mice were analyzed at 10 months, before the typical appearance of pancreatic tumors, additional studies will be needed for researchers to conclude whether or not nimesulide can delay the onset of or prevent pancreatic cancer.

“With these results, I certainly wouldn’t say everyone should be taking COX-2 inhibitors to protect against cancer,” said Eibl. “However, with additional studies, we may find COX-2 inhibitors could help prevent pancreatic cancer in high risk populations.”

“Pancreatic cancer is so deadly because it often goes undetected until it’s too late,” said Dr. Eibl. “If a patient is at a high-risk for developing pancreatic cancer, a COX-2 inhibitor may offer some protection.”

In the future, Dr. Eibl and others plan to study the long-term effects of nimesulide and additional COX-2 inhibitors on the onset and progression of pancreatic cancer.

###

This study was funded by the National Institutes of Health, the Jonsson Cancer Center Foundation at UCLA, and the Hirshberg Foundation for Pancreatic Cancer Research.

The mission of the American Association for Cancer Research is to prevent and cure cancer. Founded in 1907, AACR is the world's oldest and largest professional organization dedicated to advancing cancer research. The membership includes nearly 26,000 basic, translational, and clinical researchers; health care professionals; and cancer survivors and advocates in the United States and more than 70 other countries.

AACR marshals the full spectrum of expertise from the cancer community to accelerate progress in the prevention, diagnosis and treatment of cancer through high-quality scientific and educational programs. It funds innovative, meritorious research grants. The AACR Annual Meeting attracts more than 17,000 participants who share the latest discoveries and developments in the field. Special Conferences throughout the year present novel data across a wide variety of topics in cancer research, treatment, and patient care.

AACR publishes five major peer-reviewed journals: Cancer Research; Clinical Cancer Research; Molecular Cancer Therapeutics; Molecular Cancer Research; and Cancer Epidemiology, Biomarkers & Prevention. Its most recent publication, CR, is a magazine for cancer survivors, patient advocates, their families, physicians, and scientists. It provides a forum for sharing essential, evidence-based information and perspectives on progress in cancer research, survivorship, and advocacy.

 
 
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