Research Advances in Pancreas Cancer

From John Hopkins ...

At the Kimmel Cancer Center, state-of-the-art is just the starting point of what we provide patients with pancreas cancer.

Researcher Anirban Maitra created a
system that makes cancer therapies easier
to give to patients.

About 80 percent of patients diagnosed with pancreas cancer will need novel therapies. The goal of the Skip Viragh Center for Pancreas Cancer Clinical Research and Patient Care is to pursue clinical innovation and develop new treatments based on our laboratory discoveries. The transfer of research findings to clinical research has resulted in the development of a pancreas cancer vaccineand other promising therapies.

• Pancreas Cancer Vaccine
• Metabolic Pathways for Pancreas Cancer
  Johns Hopkins investigators test and develop drugs that target faulty enzymes that process glutamine, glucose and fatty acids in some pancreatic cancers. Researchers scan patients' DNA for genes that could benefit from glutamine- and glucose-blocking drugs.

This research was made possible by a $3.75 million grant and clinical trial funding fromStand Up to Cancer, established by the Entertainment Industry Foundation. Funds were raised during a simultaneous, primetime television broadcast on the ABC, CBS and NBC television networks in September 2008.

Team members on this project include Chi Dang, M.D., Ph.D., vice dean for research at the Johns Hopkins University School of Medicine, Manuel Hidalgo, M.D., Ph.D., director of the Centro Integral Oncológico Clara Campal (CIOCC) in Madrid, Spain, Ralph Hruban, M.D.,Kenneth Kinzler, Ph.D., Daniel Laheru, M.D., Anirban Maitra, M.D., Martin Pomper, M.D., Ph.D., Victor Velculescu, M.D., Ph.D., from the Sol Goldman Pancreatic Cancer Research Center at Johns Hopkins, and David L. Vander Jagt, Ph.D. of the University of New Mexico.

• The National Familial Pancreas Tumor Registry
   
• Rapid Autopsy Program
  
  A selfless act by terminal cancer patients is helping Christine Iacobuzio-Donahue, M.D., Ph.D., and Daniel Laheru, M.D. decipher how pancreas cancer originates and spreads as well as identify potential new ways to treat the disease.
• Iacobuzio-Donahue directs the Johns Hopkins Gastrointestinal Cancer Rapid Medical Donation Program, a unique program in which patients who lose their battle with cancer volunteer to have a rapid autopsy so that investigators can study their tumors, cells, and genes to find answers that may save the lives of future patients. She has performed more than 150 autopsies to identify the genetic differences in pancreas cancer that underlie its progression and spread to other organs.
  This research, funded by the Skip Viragh Center for Pancreas Cancer Clinical Research and Patient Care, allowed Iacobuzio-Donahue, Laheru, and colleagues to link a gene discovered by another Johns Hopkins investigator to pancreas cancer metastasis.
  "This work was considered way 'outside of the box' thinking, and no one would fund it," says Laheru. "We were the only cancer center in the country doing this kind of research."
  Their findings have been key to research projects aimed at identifying new drugs to specifically target late-stage cancers.

Identifying a window for cancer prevention

• More recently, Iacobuzio-Donahue developed a mathematical model that allows clinicians, for the first time, to quantify the development of pancreas cancer and how best to treat it. Their work was transformative, disproving common scientific thought that this type of cancer progresses to a deadly stage very early in its development. To the contrary, she calculated that it takes an average of 11 years before a cancer cell arises from a precancerous pancreas lesion. Still another seven years may pass as that cancer grows to form a tumor, giving at least one cell the potential to break away and spread the cancer outside of the pancreas in a process known as metastasis.
  "This spread represents a lethal turning point in the progression of the cancer. Once it occurs, these patients die, on average, two and half years later," says Laheru. "This was a revolutionary idea that a disease this clinically aggressive could be have such potential opportunity for intervention early on while it is still curable. It moves us closer to the ultimate prize-prevention."
  To make the calculations, Iacobuzio-Donahue and team studied tissue collected at autopsy from seven patients who died of metastatic pancreas cancer. The research team identified and classified the genetic alterations in each patient's pancreas tumor and the sites to which it spread.
  In all of the patients, the investigators found similar mutations in both the originating tumor and the body sites where it spread, genetically linking the metastatic lesions to the original pancreas tumor from which it arose. They classified mutations that occurred prior to metastasis and those that happened after the cancer began to spread. Then, they applied their findings to mathematical models and created a timeline of progression from precancerous lesion to deadly, metastatic disease.
  In search of a screening tool
  Although the research reveals a large window of time before a pancreas cancer turns deadly, currently, "pretty much everybody is diagnosed after that window has closed," says Iacobuzio-Donahue. "New, early diagnostic tests to detect these cancers during this 11- to 18-year window, would provide an opportunity to intervene, and potentially cure these cancers, with surgery."
  The discovery has led to the development of technology that rapidly picks out proteins and other biomarkers that help predict and diagnose pancreas cancer.
  Iacobuzio-Donahue's goal is to create a screening method, similar to those used to screen for breast and colon cancers, to detect very early pancreas cancers, long before they cause symptoms. She suggests that just as colonoscopies are used to look inside the colon for precancerous lesions called polyps, physicians could use a similar technique called endoscopy, which uses an endoscope inserted through the mouth, to examine the pancreas for precancerous lesions.

• Mouse Models
  
  Investigator James Eshleman, M.D., Ph.D., has developed a mouse that grows pancreas cancer cells providing some of the groundwork for a massive exploration of the pancreas cancer genome. Ralph Hruban, M.D., and Eshleman are working with Bert Vogelstein, M.D., in the sequencing of 24,000 known genes and then validating them in some 96,000 pancreas cancers.

• Preventing Pancreas Cancer

Endoscopy

Our endoscopy specialists help people with a family history of pancreas cancer learn if they have precancerous lesions that could develop into cancer. Early precancerous lesions can be surgically removed and the pancreas saved. Some patients may choose prophylactic removal of the pancreas to stave off cancer.

Nanopill

Johns Hopkins scientists combined nanoscience with the Indian spice curcumin to develop a novel pancreas cancer prevention strategy. Curcumin has the ability to activate cancer detoxifying enzymes, but is not absorbed well by cells when eaten. To overcome the absorption problem, the investigators created a nanoparticle carrier for the curcumin. The engineered nanocurcumin can be given intravenously or orally.

Recruiting Genes to Kill Cancer

The Johns Hopkins Kimmel Cancer Center team who discovered the pivotal genes abundant in pancreas cancer patients also is investigating the potential for gene therapy. Studies suggest that a tumor suppressor gene, DCP4, is either missing or inactivated in more than half of all patients with pancreas cancer. Losing the function of both copies of this gene is like losing the brakes on a car. When left unchecked, these cells begin to multiply. Studies are under way to see whether bystander genes can be activated to replace the lost tumor suppressor function and put the brakes on cancer cells.

• Pancreas Cancer Stem Cells
  
  Cancer stem cells are small in number, almost undetectable, but they can be the fuel that promotes certain cancers to grow and spread. Recent research has brought these cells into focus. Johns Hopkins scientists have developed a method to identify cells marked with the proteins CD44 and CD24 and those with high levels of the enzyme aldehyde dehydrogenase, believed to be characteristics of pancreas cancer stem cells.
  
  The investigators found that pancreas cancer stem cells marked with aldehyde dehydrogenase indicated decreased survival. Researchers are working to further define pancreas cancer stem cell populations and decipher the processes that control them. Using drugs to target cancer stem cells has provided new therapeutic strategies for other cancers, and these advances could be applied to pancreatic cancer.
• 
  
• The Pancreatic Cancer Action Network and the American Association for Cancer Research have awarded Zeshaan A. Rasheed, M.D., Ph.D., of the Johns Hopkins Kimmel Cancer Center, the 2010 Pancreatic Cancer Action Network-AACR Pathway to Leadership Grant. This grant, totaling $600,000 over five years, will support Rasheed's efforts to examine the relevance of cancer stem cells in pancreatic adenocarcinoma.
  
  Cancer stem cells are a subset of cells hypothesized to mediate the growth and spread of cancer. Rasheed earned his medical degree and doctorate in cellular and molecular pharmacology from the University of Medicine and Dentistry of New Jersey - Robert Wood Johnson Medical School and Graduate School of Biomedical Sciences. Currently, he is a medical oncology fellow at The Sidney Kimmel Comprehensive Cancer Center of Johns Hopkins. . His research focuses on how different populations of pancreatic cancer stem cells are related to one another and which factors regulate cancer stem cell growth and spread throughout the body. By making these determinations, Rasheed will then investigate how cancer stem cell inhibition is possible, which may lead to the development of novel cancer stem cell-targeting therapies. The grant will be formally awarded at the AACR Annual Meeting on April 20, 2010. The term for the grant begins on July 1, 2010.

• Targeting Genes That Make Therapies Work Better
  
  Three genes, BRCA2, FANCC, and FANCG, have long been linked to a rare, inherited disease known as Fanconi's Anemia (FA) and appear to play a role in 10 percent or more of pancreas cancers. People affected are born with only a single, normal copy of one or more of the genes. Though they do not develop FA, these people often develop pancreas cancer, usually in their 40s and 50s, about a decade earlier than the average person who develops the disease.
  
  Investigators believe these gene mutations may be the tumor's Achilles' heel of the tumor and make these particular cancers more responsive to treatment. The presence of these three genes appear to make pancreas cancer cells highly susceptible to treatment with two FDA-approved cancer drugs, mitomycin C and cisplatin.

• Calculating Cancer Risk
  
  A novel computer software tool, called PancPRO, helps identify people at risk of developing pancreas cancer because they have inherited gene alterations linked to the cancer. The program's calculator computes the likelihood that a person carries a pancreas cancer-related gene and the person's lifetime risk of developing this disease. Physicians and genetic counselors use the tool to identify people who may benefit from pancreas cancer screening.
• Misdirected Cell Pathway
  
  Johns Hopkins researchers have uncovered a genetic defect that may be triggering the development of pancreas cancer. A growth signal that should be turned off in adult tissues is mistakenly turned back on. The growth signal appears to be activated in response to injury to, or inflammation of the pancreas. Investigators suspect that reactivation could be a first step in the initiation of pancreas cancer, occurring even before gene alterations.
• Cells at the Root of Pancreatic Cancer

In the laboratory at Johns Hopkins Kimmel Cancer Center in Baltimore, Hopkins researchers are working diligently to figure out how to interfere with pancreas cancer-initiating cells.

A select group of researchers have shown that pancreas cancer, like many types of cancer, contains colonies of cancer-promoting cells. These cells, while small in number, appear to be a major force in cell growth by evading anticancer drugs and perpetually giving rise to the larger number of cancer cells that make up the bulk of tumors. Maitra is working with Viragh Scholars Ana De Jesus-Acosta, M.D., and Zeshaan Rasheed, M.D., Ph.D., to determine if targeting these cells with new therapies could help combat pancreas cancer.

Maitra has shown that a chemical pathway called Hedgehog is more active in pancreas cancer- initiating cells and tested agents that inhibit it. In animal models, he found that blocking Hedgehog activity increased survival. De Jesus-Acosta and Daniel Laheru, M.D., co-director of the Skip Viragh Center for Pancreas Cancer Clinical Research and Patient Care, are now translating this laboratory research into a clinical trial for patients with advanced pancreas cancer to determine whether giving patients a Hedgehog inhibitor in combination with standard drug therapy extends survival.

De Jesus-Acosta has started another clinical study for earlier stage pancreas cancer, focusing on patients whose tumors could not be treated with surgery but have not yet spread outside the pancreas. Her goal is to achieve enough regression of the tumor with the Hedgehog inhibitor/chemotherapy combination to get patients to surgery.

In the laboratory, Rasheed is using biopsy and blood samples from patients to develop technologies to isolate pancreas cancer-initiating cells and measure the effect of the inhibitor on these cells. Because biopsy is an invasive procedure that requires local anesthesia, he is working to develop a first-of-its-kind method to collect the elusive cells from circulating blood.

While researchers at other institutions are studying Hedgehog inhibitors in pancreas cancer, the Kimmel Cancer Center team was the only group who collected biopsy and blood samples. As a result, our research continues as investigators conduct one-of-a-kind studies of Hedgehog pathway regulation in cancer-initiating cells. In the first trial, the inhibitor did not thwart pancreas cancer cell growth as it did in animal models, but the blood and biopsy samples are allowing Maitra and Rasheed to go back into the laboratory, figure out why, and make necessary adjustments.

By comparing the molecular composition of tumors from patients whose cancers did not respond to treatment with those that did, our scientists may be able to create a profile of specific characteristics, such as a defined level of Hedgehog activity, to help identify those patients whose cancers are most likely to benefit. This work is part of expanded efforts at the Skip Viragh Center to sequence the genome of each patient's tumor cells and improve treatment outcomes through personalized treatment approaches tailored to the unique molecular fingerprint of an individual's tumor.

Former President Jimmy Carter Has Advanced Cancer

 AUG 14 2015, 11:18 AM ET

Watch the video at: http://www.nbcnews.com/health/health-news/former-u-s-president-jimmy-carter-has-advanced-cancer-n408751

Former President Jimmy Carter says he has cancer that has spread, although it's not yet clear what kind of cancer he has.

Carter, 90, had a mass removed from his liver on Aug. 3.

"Recent liver surgery revealed that I have cancer that now is in other parts of my body. I will be rearranging my schedule as necessary so I can undergo treatment by physicians at Emory Healthcare. A more complete public statement will be made when facts are known, possibly next week," Carter said in a statement.

James Earl Carter Jr. was 39th president of the United States, from 1977 to 1981. He's kept active despite his age, working with groups such as Habitat for Humanity, winning the Nobel Peace Prize in 2002 and founding the nonprofit Carter Center in his home state of Georgia.

"RECENT LIVER SURGERY REVEALED THAT I HAVE CANCER THAT NOW IS IN OTHER PARTS OF MY BODY."

Carter's family has a history of pancreatic cancer. His father, both his sisters and his brother died of pancreatic cancer, and his mother had pancreatic cancer as well.

In 2007, Carter told The New York Times that he had CT scans twice a year and later MRI (magnetic resonance imaging) to look for tumors in his pancreas.

In May, Carter left Guyana early from a stint monitoring elections there, saying he was feeling unwell.

Pancreatic cancer can spread to other organs, including the liver, and cancer can also originate in the liver and spread elsewhere. Carter did not give details of what type of cancer he has or how far it has spread.

However, when cancer spreads from one organ to elsewhere in the body, it is considered Stage IV cancer -- the most advanced stage. Stage IV cancer is generally incurable, although it can be treated, depending on the type.

Dr. Robert Mayer, a gastrointestinal cancer specialist at the Dana Farber Cancer Institute, says that at age 90, Jimmy Carter is unlikely to tolerate much treatment.

There are many different possible cancers that Carter could have, Mayer said.

"THIS IS A 90 YEAR OLD GENTLEMEN WITH APPARENT WIDESPREAD DISEASE. THE GOALS OF TREATMENT WOULD BE HIS COMFORT."

"I really don't know from paucity of information which of these would be the situation for President Carter. I don't know what his symptoms were. I don't know what led to surgery on his liver," Mayer told NBC News.

"This is a 90-year-old gentleman with apparent widespread disease. The goals of treatment would be his comfort. If chemo is considered it would need to take into account his age."

Mayer says a 90-year-old patient cannot tolerate the same treatment that could buy years of life for cancer patients in their 60s or 70s.

Statements of support poured in, including from President Barack Obama.

"Our thoughts and prayers are with Rosalynn and the entire Carter family as they face this challenge with the same grace and determination that they have shown so many times before," Obama's statement read.

"Jimmy, you're as resilient as they come, and along with the rest of America, we are rooting for you."

What’s new in pancreatic cancer research and treatment?

Research into the causes, diagnosis, and treatment of pancreatic cancer is under way in many medical centers throughout the world.

Genetics and early detection

Scientists are learning more about some of the changes in DNA that cause cells in the pancreas to become cancerous. Inherited changes in genes such as BRCA2, p16, and the genes responsible for hereditary non-polyposis colorectal cancer (HNPCC) can increase a person’s risk of developing pancreatic cancer.

Researchers are now looking at how these and other genes may be altered in pancreatic cancers that do not seem to be inherited. They have discovered that pancreatic cancer does not form suddenly. It develops over many years in a series of steps known as pancreatic intraepithelial neoplasia or PanIN. In the early steps, such as PanIN 1, there are changes in a small number of genes, and the duct cells of the pancreas do not look very abnormal. In later steps such as PanIN 2 and PanIN 3, there are abnormalities in several genes and the duct cells look more abnormal.

Researchers are using this information to develop tests for detecting acquired (not inherited) gene changes in pancreatic cancer pre-cancerous conditions. One of the most common DNA changes in these conditions affects theKRAS oncogene, which affects regulation of cell growth. New diagnostic tests are often able to recognize this change in samples of pancreatic juice collected during an ERCP (endoscopic retrograde cholangiopancreatography).

For now, imaging tests like endoscopic ultrasound (EUS), ERCP, and genetic tests for changes in certain genes (such as KRAS) are options for people with a strong family history of pancreatic cancer. But these tests are not recommended for widespread testing of people at average risk who do not have any symptoms.

Treatment

The major focus of much research is on finding better treatments for pancreatic cancer. Improving surgery and radiation therapy are major goals, as is determining the best combination of treatments for people with certain stages of cancer.

Surgery

Surgery to remove pancreatic cancer (most often a Whipple procedure) is a long and complex operation that can be hard both for the surgeon and the patient. It often requires a hospital stay of a week or more, at least in part because of the long incision made in the belly.

A newer approach now used at some major medical centers is to do the operation laparoscopically. For this approach, the surgeon makes several small incisions in the belly instead of one large one. Long, thin surgical instruments and a tiny video camera are then inserted through these cuts to do the operation. One advantage of this surgery is that people often recover from it more quickly. But this is still a difficult operation. Surgeons are looking to see how it compares to the standard operation and which patients might be helped the most by it.

Radiation therapy

Some current studies are looking at different ways to give radiation to treat exocrine pancreas cancer. These include intraoperative radiation therapy (in which a single large dose of radiation is given to the pancreas in the operating room at the time of surgery) and proton beam radiation (which uses a special type of radiation that might do less damage to nearby normal cells).

Chemotherapy

Many clinical trials are testing new combinations of chemotherapy drugs for pancreatic cancer. Studies have looked to see if combining gemcitabine with other drugs would help patients live longer. For example, adding capecitabine (Xeloda) to gemcitabine seems to help some patients. The combination of gemcitabine, irinotecan, and celecoxib (an arthritis drug) also shows promise.

Other studies are testing the best ways to combine chemotherapy with radiation therapy or newer targeted therapies.

Targeted therapies

As researchers have learned more about what makes pancreatic cancer cells different from normal cells, they have developed newer drugs that should be able exploit these differences by attacking only specific targets. These targeted therapies may provide another option for treating pancreatic cancer. They may prove to be useful along with, or instead of, current treatments. In general, they seem to have fewer side effects than traditional chemo drugs. Looking for new targets to attack on cancers is an active area of research.

Growth factor inhibitors: Many types of cancer cells, including pancreatic cancer cells, have certain molecules on their surface that help them grow. These molecules are called growth factor receptors. One example is epidermal growth factor receptor (EGFR). Several drugs that target EGFR are now being studied. One, known as erlotinib (Tarceva), is already approved for use along with gemcitabine.

Anti-angiogenesis factors: All cancers depend on new blood vessels to nourish their growth. To block the growth of these vessels and thereby starve the tumor, scientists have developed anti-angiogenesis drugs. These are being studied in clinical trials for patients with pancreatic cancer.

Drugs that target the tumor stroma (supporting tissue): Pancreatic cancer does not always respond well to chemotherapy. This is partly because of the cancer cells themselves, but another reason might be the dense surrounding supportive tissue (stroma) in the tumor. The stroma seems to form a barrier that helps protect the cancer cells from the effects of chemo drugs. Researchers are now looking at drugs that attack the stroma directly to help break it down. This might allow chemo or other drugs to be more effective. Some of these types of drugs are now inclinical trials.

Other targeted therapies: Many drugs targeting other aspects of cancer cells are now being studied for use in pancreatic cancer. Some of these drugs, such as sunitinib (Sutent), have several different targets.

Immune therapy

Immune therapies attempt to boost a person’s immune system or give them ready-made components of an immune system to attack cancer cells. Some studies of these treatments have shown promising results.

Monoclonal antibodies: One form of immune therapy uses injections of man-made monoclonal antibodies. These immune system proteins are made to home in on a specific molecule, such as carcinoembryonic antigen (CEA), which is sometimes found on the surface of pancreatic cancer cells. Toxins or radioactive atoms can be attached to these antibodies, which bring them directly to the tumor cells. The hope is that they will affect cancer cells while leaving normal cells alone. For use in pancreatic cancer, these types of treatments are available only in clinical trials at this time.

Cancer vaccines: Several types of vaccines for boosting the body’s immune response to pancreatic cancer cells are being tested in clinical trials. Unlike vaccines against infections like measles or mumps, these vaccines are designed to help treat, not prevent, pancreatic cancer. One possible advantage of these types of treatments is that they seem to have very limited side effects. At this time, vaccines are available only in clinical trials.

Drugs that target immune system checkpoints: The immune system normally keeps itself from attacking other normal cells in the body by using “checkpoints” – molecules on immune cells that need to be activated (or inactivated) to start an immune response. Cancer cells sometimes find ways to use these checkpoints to avoid being attacked by the immune system. Newer drugs that target these checkpoints have shown a lot of promise in treating some types of cancer, and are now being studied for use in pancreatic cancer.

Individualization of therapy

Some drugs seem to work better if certain types of mutations can be found in the patient’s tumor. For example, erlotinib may work better in patients whose tumors have a particular change in the EGFR gene. This concept is an area of intense study. There might also be some gene alterations that affect how well gemcitabine will work in a particular patient. Identifying markers that may predict how well a drug will work before it is given is an important area of research in many types of cancer.

New treatments for pancreatic neuroendocrine tumors (NETs)

Many pancreatic NETs have receptors for somatostatin on their cells. These tumors can be treated with octreotide and other drugs like it. Newer drugs that use a radioactive form of octreotide have been shown to shrink some tumors and keep others from growing in early studies.

Last Medical Review: 06/11/2014
Last Revised: 01/09/2015

Carter: 'All of my family died with pancreatic cancer'

Learn more about President Jimmy Carter's family history with Pancreatic Cancer during his 2012 interview on CNN.

http://www.cnn.com/videos/us/2015/08/12/larry-king-live-jimmy-carter-pancreatic-cancer-in-his-family.cnn/video/playlists/jimmy-carters-legacy/

​Family history of cancer eyed in Jimmy Carter diagnosis

NEW YORK -- Former President Jimmy Carter announced Wednesday that he has cancer and that it has spread. The 90-year-old said he will be getting treatment at Emory Healthcare in Atlanta.

President Carter announced on August 3 that he had a procedure "to remove a small mass in his liver." In a statement released Tuesday, Carter said the surgery revealed the cancer.

Play VIDEO

Former President Jimmy Carter looks back at his legacy

The statement did not say what type of cancer the former president has and whether it began in the liver or spread there from another part of the body.

Mr. Carter has a strong family history of pancreatic cancer. His three siblings and father died from it.

Family history is important to consider because it increases his chance of getting it himself. In fact, one study found that people with three or more close relatives with pancreatic cancer had a 57 times increased chance of getting it themselves.

http://www.cbsnews.com/news/family-history-of-cancer-eyed-in-jimmy-carter-diagnosis/

Researchers find reason pancreatic cancer resists chemotherapy drug

By Amy Ellis Nutt January 30

Researchers have identified one reason pancreatic cancer is so resistant to chemotherapy treatment: vitamin D.

Only about 5 percent of pancreatic-cancer patients survive beyond five years even with the most aggressive treatment, according to the National Cancer Institute. One big reason is that chemotherapy — including the standard drug, gemcitabine — isn’t very effective at preventing pancreatic cancer cells from replicating.

To understand why, Timothy J. Yen, a professor at Temple University’s Fox Chase Cancer Center in Philadelphia, removed each of the 24,000 genes, one by one, in pancreatic cancer cells and then doused them with gemcitabine.

When some of these genes were “knocked out,” the gemcitabine was effective. One in particular surprised the researchers.

“When we knocked out the gene for a protein that binds to vitamin D, almost all of (the cancer cells) died,” said Yen, the leader of the research team.

Although vitamin D is important for health, especially for bone health, normal cells do not need vitamin D to survive, said Yen. Apparently, though, pancreatic cancer cells do.

That means if scientists can figure out a way to inactivate the vitamin D receptor in pancreatic cancer cells, the main drug used to treat patients would be more effective.

“My excitement about making vitamin D receptors a priority is because it is a ‘druggable’ target,” Yen said. “There are compounds out there that drug companies already make to affect vitamin D,” so the apparatus and knowledge already exist.

The researchers at Fox Chase Cancer Center, which is part of the Temple University Health System, published their findings in the journal Cell Cycle on Jan. 3. Their study took nearly four years to complete, and the initial findings were so unexpected, Yen said, that many more-sophisticated experiments were performed to convince the team that their findings were correct.

“I didn’t believe the results at first,” he said, “because the literature on vitamin D — what does it have to do with cancer? But this wasn’t just a fluke.”

Yen admits that he and his team are novices when it comes to vitamin D, but they did know that it aids functioning in nearly every tissue and organ of the human body, not just the bones. What was so unusual in their genetic experiments was to find that while normal cells do not require vitamin D to survive, pancreatic cancer cells need it to repair the damage caused by chemotherapy.

“This in-vitro study was quite elegant and suggested that targeting VDR (vitamin D receptors) may show synergistic effect with gemcitabine in pancreatic cancer patients,” said Haoqiang Ying, an expert in molecular and cellular oncology at the University of Texas MD Anderson Cancer Center in Houston. “Much more detailed studies are needed.”

Many researchers have examined how tumor cells hijack genes, according to Yen.

“Why they hijack certain genes we don’t know,” he said. “But they do re-purpose other genes to help the cancer to survive. In the case of pancreatic cancer, it’s the (gene for the) vitamin D receptor.”

Another reason pancreatic cancer is so stubborn to treat is that the malignancy creates a kind of moat around itself, making it difficult for chemo drugs to reach the primary tumor.

“The possibility is, if we can design something to inhibit vitamin D, we can enhance the sensitivity of the tumor to the limited amount of the drug that gets through,” Yen said. “I would love to see the day my research gets to the bedside, but there are so many things to overcome. This is just another light switch we’ve turned on. We just hope to keep it on as long as we can.”

Pulitzer Prize-winning reporter Amy Ellis Nutt covers health and science for The Washington Post.

Click here to learn more.

Comments are closed.

• All Comments
• • Newest First
• Pause live updates

FutureTense

2/1/2015 5:18 PM MST

but then there is this:
http://www.newsmaxhealth.com/Health-News/vitamin-d...

which gives all the BENEFITS of Vitamin D
what is a person supposed to do? Take it or not? Guess it depends on your family health history

LikeShare

nitrat

2/1/2015 3:59 PM MST [Edited]

How fascinating!
Good work, guys!

Is this research applicable to other genes and other cancers/diseases and other unknown vitamin D type factors?
You can no doubt tell how ignorant I am.
 

LikeShare

Jan Poehlmann

2/1/2015 1:44 PM MST

Ok, so if I had pancreatic cancer and my vitamin D levels are pretty much non-existent, is that a good thing? My doctor has been giving me mega doses of vitamin d, trying to get my numbers up. Should I stop taking it since it actually HELPS pancreatic cancer cells grow?

LikeShare

nitrat

2/1/2015 4:06 PM MST

Pancreatic cancer is pretty rare, right? Why stop something you must need on the slim chance you might develop pancreatic cancer? Particularly, without showing this to your doctor.

Like

AsperGirl

1/31/2015 3:54 PM MST

Excellent article. Thank you.

LikeShare

1

jean5050

1/30/2015 12:29 PM MST

Thank you for this article. My family is cursed with this horrid disease. We are grateful to see any progress and sincerely hope that with this breakthrough, the researchers will continue so that the survival rate will increase. Thank you!

LikeShare

3

satxusa

1/30/2015 10:36 AM MST

A blessing on the researchers working in unseen labs who strive to find solutions for this terrible cancer.

LikeShare

5

wadejg

1/30/2015 11:33 AM MST

Especially for a cancer like pancreatic that is so hard to treat or survive.

Like

2

Get Today's Headlines

Daily updates delivered just for you.