Sunday, January 01, 2006

prostaglandins choreograph perturbations

Study fishes out new role for prostaglandins - Prostaglandins – the fat-derived compounds linked to pain, inflammation, reproduction and cancer – can add another biological function to their extensive catalog.

A new study by Vanderbilt researchers reveals that prostaglandins help choreograph the intricate cell movements during early embryonic development in zebrafish, highlighting how perturbations in this pathway might influence human development and the spread of cancer. The results also may point to new molecular targets for cancer prevention therapies.

The findings, published January 1 in the journal Genes and Development, result from a cross-campus collaboration between the labs of Raymond DuBois, M.D., Ph.D., director of the Vanderbilt-Ingram Cancer Center and B.F. Byrd Jr. Professor of Molecular Oncology, and Lilianna Solnica-Krezel, Ph.D., professor of Biological Sciences.

Early in development, vertebrate embryos consist of one layer of cells. These simple embryos must go through a complex reorganization called gastrulation to establish the three primitive layers from which all adult tissues develop – the innermost layer (endoderm), which forms the gut and associated digestive organs; the middle layer (mesoderm), which develops into muscle, bone and cardiovascular organs, and the outer layer (ectoderm), which becomes the skin and nervous system.

"The body is a tube in a tube in a shell," Solnica-Krezel explained. "Before gastrulation, all of these prospective tubes are at the surface of the embryo. Gastrulation puts these different tissue precursors inside the embryo and gives them a proper shape."

But little is known about the chemical signals that cause these cells to move. Previous studies in mice and zebrafish suggested that prostaglandins were important in development. Mice lacking an enzyme that synthesizes prostaglandin had numerous developmental defects, but the true effects of prostaglandins on the embryo were likely obscured by maternal prostaglandin production.

Because they develop outside the mother and are transparent, zebrafish embryos provide a unique model in which to examine prostaglandin's role in development.

Yong Cha, a graduate student in DuBois' lab and first author on the study, established a collaboration with zebrafish researcher Solnica-Krezel to study this process.

The researchers inhibited the production of a specific type of prostaglandin, PGE2, in zebrafish embryos and examined their development.

In embryos treated with the inhibitor, gastrulation was arrested or slowed down significantly. The resulting embryo was also shorter than an untreated embryo.

"What is spectacular," said Solnica-Krezel, "is that…if you just put some prostaglandin back in the culture medium, you rescue the phenotype."

In another set of embryos, the researchers blocked prostaglandin receptors, EP2 and EP4. Blocking the EP4 receptor caused defects similar to those associated with blocking PGE2 synthesis. When the researchers analyzed cell movement, they found that the shapes and trajectories of embryonic cells were normal – they simply moved much slower. This suggested that signaling through the EP4 receptor regulates the speed of cell movements during gastrulation.

The sluggish cell movements could have profound implications for development.

"Timing (in development) is really important," DuBois explains. "If you are traveling and have to get to the train station at a particular time, if you are too slow, you are going to miss the train. If you don't get on that part of the trip, that disturbs the whole agenda."

"Development synchronizes or orchestrates a myriad of events in the proper sequence (lots of trains)," said Solnica-Krezel, "and sometimes one train wreck can halt the entire process."

While 'bad timing' during development can spell the end for an embryo, finding ways to exploit this pathway could have beneficial effects in cancer cells.

"The pathways important for regulating development are also dysregulated in cancer," said DuBois, who studies prostaglandin signaling in colon cancer. Knowing how prostaglandins regulate cell movement in development can help cancer researchers determine how cancer cells spread throughout the body, or metastasize – and how to stop the process. DuBois previously found that adding PGE2 to cultured cancer cells causes them to move much more rapidly.

"We've been able to show that some genes in this pathway are really important for cancer cells to spread to the liver," he said. "Eventually, we may be able to find a way to attack this pathway and prevent metastatic spread of colon cancer."

Scientists have known that people who take aspirin, a drug that inhibits prostaglandin synthesis, have about a 50 percent reduction in their risk of getting colon cancer, DuBois explained.

"We've been on a quest for the last 10 years to understand why such a simple drug leads to such a significant reduction in cancer risk," he said. "There are several parts to that puzzle. This (finding) may be one piece."

Zebrafish models may seem like a step back from the more traditional mouse models used to study cancer. But zebrafish, which develop quickly, are inexpensive and easy to manipulate, could actually aid in the discovery of new cancer drugs.

"If you could use the zebrafish intelligently to screen for these drugs, it might really speed up the drug discovery process and give us some early clues about the effects we may see in humans," DuBois said. ###

Other authors on the study were Seok-Hyung Kim and Diane Sepich in the Solnica-Krezel group, and F. Gregory Buchanan in the DuBois group. The research was supported by grants from the National Institutes of Health, the T.J. Martell Foundation, the National Colorectal Cancer Research Alliance and the Zebrafish Initiative funded by the Vanderbilt University Academic Venture Capital Fund.

Contact: Heather Hall
heather.l.hall@vanderbilt.edu 615-936-7245 Vanderbilt University Medical Center

more at
or and or and or or and or

Related: Keyword Agriculture Sunday, December 25, 2005
Why Christmas trees are not extinct, Sunday, May 08, 2005 Laser Shows if Fruit's Beauty is Only Skin Deep, Saturday, May 28, 2005 5th World Bonsai Convention, Sunday, May 29, 2005 regarding over-fortified corn soy blend, Monday, June 06, 2005 From a Few Wild Ancestors, a Citrus Cornucopia, Sunday, July 03, 2005 Grafting Watermelon Makes Firmer, Healthier Fruit, Sunday, July 24, 2005 Prehistoric Native Americans maize cultivation, Sunday, August 28, 2005 Coffee is number one source of antioxidants, Sunday, November 27, 2005 Give thanks for the cranberry, say dental researchers,

Saturday, December 31, 2005

Presidential Message: New Year's Day, 2006

Presidential Message: New Year's Day, 2006

The New Year is a time of hope as we reflect on the past and prepare for the future.

The great strength of our Nation lies in the hearts and souls of the American people. This past year, Americans responded with an outpouring of compassion to help the people of the Gulf Coast region recover from one of the most devastating natural disasters in our Nation's history. We remember the victims of the past year's hurricanes and give thanks for the millions of people who opened their hearts, homes, and communities to those in need.

In the past year, we continued our work to spread freedom and peace. In 2005, Iraqis three times exercised their right to vote in free elections, and the Afghan people conducted successful parliamentary elections. In the coming year, America will continue to stand beside these young democracies and lay the foundation of peace for our children and grandchildren.

We appreciate the brave men and women in uniform who protect our country and advance freedom around the world. We are grateful to their families for their support and sacrifice, and we pray for all those who have lost loved ones in freedom's cause. Our Nation will always remember the heroes who have given their lives to protect us all.

As we celebrate the New Year, we give thanks to God for His blessings and ask for His guidance. We look with hope to the year ahead and the many new opportunities the future will bring.

Laura and I send our best wishes for a happy New Year. May God bless you, and may God continue to bless America.

GEORGE W. BUSH

# # # For Immediate Release, Office of the Press Secretary, December 30, 2005

Related: Keyword Presidential Message, Saturday, January 22, 2005
Presidential Message: Eid Al-Adha, Thursday, March 17, 2005 Nowruz, new year and celebration of life, Monday, July 11, 2005 10th Anniversary of the Massacre in Srebrenica, Saturday, October 01, 2005 Rosh Hashanah, 5766, Tuesday, October 04, 2005 Presidential Message: Ramadan,

more at
and or and , or and , or , and ,