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Daily Archives: April 7, 2014
Ridgewood Savings Bank Selects DNA from Fiserv to Accelerate Growth
Posted: April 7, 2014 at 9:47 pm
Largest mutual savings bank in New York selects DNA from Fiserv to attract and deepen customer relationships
Unified design and open architecture of DNA will help Ridgewood Savings Bank increase efficiency
Bank leaders cite the platform's person-centric design, business intelligence tools and ability to introduce new products quickly as key factors in their decision
Brookfield, Wis., Fiserv, Inc. (NASDAQ: FISV), a leading global provider of financial services technology solutions, today announced that Ridgewood Savings Bank, based in Ridgewood, N.Y., has selected the DNA account processing platform and several complementary Fiserv solutions to accelerate its growth. The $5.1 billion asset bank will use the integrated Fiserv solution to attract new customers, deepen existing relationships and enhance its already excellent reputation for customer service.
As the largest mutual savings bank in New York State, Ridgewood Savings Bank required a unified enterprise platform that would drive efficiency across its 34 branches from the back office through to its customers. DNA will enable the bank to streamline operations and roll-out new, highly-relevant products more quickly and easily than ever before.
"DNA is a key component of our strategy to make Ridgewood Savings Bank more visible and competitive in the marketplace," said Peter M. Boger, chairman, president CEO of Ridgewood Savings Bank. "The platform's business intelligence tools will help us add relationships and expand existing ones while delivering on our commitment to superior service. We'll offer new services and boost efficiency with a state-of-the-art platform that we can build on for years to come."
Ridgewood Savings Bank selected DNA for its open architecture and person-centric design - factors that will allow the bank to easily integrate complementary solutions while maintaining a 360-degree view of its retail and small business relationships. Developed using modern, standards-based components, DNA provides Ridgewood Savings Bank with 24/7 real-time processing, virtually unlimited scalability and robust retail, mortgage and commercial banking capabilities.
With DNA, Ridgewood Savings Bank will also have the ability to add new functionality with integrated core extensions, called DNAapps, which are available through the DNAappstore - the first collaborative online marketplace for custom core applications.
"While Ridgewood Savings Bank is new to DNA, this leading community bank has been a valued partner with Fiserv for over 20 years," said Steve Cameron, president, Open Solutions Division, Fiserv. "Ridgewood Savings Bank's selection of DNA reflects the success of our longstanding relationship and provides us with an even greater opportunity to help the bank grow with a vast array of integrated Fiserv solutions."
In addition to its hosted deployment of DNA, Ridgewood Savings Bank will implement Nautilus for electronic content management, WireXchange for wire exchanges, tMagic for DNA integrated teller capture, the CRM and Business Intelligence suite for DNA and card production services. The bank will integrate its existing Fiserv solutions into DNA, including ATM & Debit Solutions, Fraud Risk Solutions for Cards, Voice Response and the Financial Accounting suite for DNA. Annual Best Practice Reviews will help Ridgewood Savings Bank get the most out of its Fiserv investment.
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Ridgewood Savings Bank Selects DNA from Fiserv to Accelerate Growth
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DNA test is latest to confirm ID of American WWII soldier buried in Germany
Posted: at 9:47 pm
By Karen Herzog
Milwaukee Journal Sentinel
Published: April 7, 2014
MILWAUKEE An American forensic lab announced Monday it has independently confirmed through DNA testing that the remains recovered from a German ossuary in France are indeed U.S. Army Pfc. Lawrence S. Gordon, who was mistakenly buried with the enemy after World War II.
DNA was extracted from bones by the national crime lab in France after Wisconsin filmmaker Jed Henry's dogged research through military records led to a crypt of an unknown soldier identified as a German.
The French crime lab announced in February that it had a mitochondrial DNA match, meaning the results matched DNA from maternal relatives of Gordon's. Samples then were sent to a DNA testing facility at University of Wisconsin-Madison and to Bode Technology Group in Lorton, Va., for independent confirmation.
Bode not only confirmed the French crime lab's results on Monday, but announced that it did a more specific nuclear DNA profile for further proof of identification all within eight days of receiving the DNA samples from France.
The DNA facility at University of Wisconsin-Madison will begin its testing this week. In addition to confirming the Virginia lab's results, the UW-Madison lab is working on refining techniques for recovering DNA from bones and teeth that are 70 years old and older.
Henry became interested in the Gordon case because his grandfather, Staff Sgt. David L. Henry of Viroqua, served in the same reconnaissance company, and Gordon was the only member of the company who died and was not identified for a proper burial.
The U.S. military accounting community refused to help confirm the remains in the German crypt were Gordon's, but French and German officials agreed to allow DNA to be extracted and tested in hopes of identifying the soldier.
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3-D structure for malaria parasite genome constructed
Posted: at 9:46 pm
A research team led by a cell biologist at the University of California, Riverside has generated a 3D model of the human malaria parasite genome at three different stages in the parasite's life cycle -- the first time such 3D architecture has been generated during the progression of the life cycle of a parasite.
The parasite that causes malaria in humans is Plasmodium falciparum. The female Anopheles mosquito transmits P. falciparum from an infected human to healthy individuals, spreading malaria in the process. According to the World Health Organization, an estimated 207 million people were infected with malaria in 2012, leading to 627,000 deaths.
"Understanding the spatial organization of chromosomes is essential to comprehend the regulation of gene expression in any eukaryotic cell," said Karine Le Roch, an associate professor of cell biology and neuroscience, who led the study.
Her research team also found that those genes that need to be highly expressed in the malaria parasite -- for example, genes involved in translation -- tend to cluster in the same area of the cell nucleus, while genes that need to be tightly repressed -- for example, genes involved in virulence -- are found elsewhere in the 3D structure in a "repression center." The 3D structure for the malaria parasite genome revealed one major repression center.
Virulence genes in the malaria parasite are a large family of genes that are responsible for the parasite's survival inside humans. Le Roch's team found that these genes, all organized into one repression center in a distinct area in the nucleus, seem to drive the full genome organization of the parasite.
Study results appeared online last week in Genome Research, an international, peer-reviewed journal that features outstanding original research providing novel insights into the genome biology of all organisms. The research paper will appear in print in the June issue of the journal.
"We successfully mapped all physical interactions between genetic elements in the parasite nucleus," Le Roch said. "To do so, we used a 'chromosome conformation capture method,' followed by high throughput sequencing technology -- a recently developed methodology to analyze the organization of chromosomes in the natural state of the cell. We then used the maps of all physical interactions to generate a 3D model of the genome for each stage of the parasite life cycle analyzed."
To understand the biology of an organism or any cell type, scientists need to understand not only the information encoded in the genome sequence but also how the sequence is compacted and physically organized in each cell/tissue, and how changes in the 3D genome architecture can play a critical role in regulating gene expression, chromosome morphogenesis and genome stability. In human cells, changes in chromosome organization and compaction can lead to diseases such as cancer.
"If we understand how the malaria parasite genome is organized in the nucleus and which components control this organization, we may be able to disrupt this architecture and disrupt, too, the parasite development," Le Roch said. "We know that the genome architecture is critical in regulating gene expression and, more important, in regulating genes that are critical for parasite virulence. Now we can more carefully search for components or drugs that can disrupt this organization, helping in the identification of new anti-malaria strategies."
Le Roch's lab is now looking at other stages of the malaria life cycle in order to identify components responsible for the 3D genome architecture.
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Can genome sequencing be used outsmart foodborne diseases?
Posted: at 9:46 pm
WASHINGTON - Chances are you've heard of mapping genes to diagnose rare diseases, predict your risk of cancer and tell your ancestry. But to uncover food poisonings?
The nation's disease detectives are beginning a program to try to outsmart outbreaks by routinely decoding the DNA of potentially deadly bacteria and viruses.
The initial target is listeria, the third-leading cause of death from food poisoning and bacteria that are especially dangerous to pregnant women. Already, the government credits the technology with helping to solve a listeria outbreak that killed one person in California and sickened seven others in Maryland.
"This really is a new way to find and fight infections," said Dr. Tom Frieden, director of the Centers for Disease Control and Prevention. "One way to think of it is, is it identifying a suspect by a lineup or by a fingerprint?"
Whole genome sequencing, or mapping all of an organism's DNA, has become a staple of medical research. But in public health, it has been used more selectively, to investigate particularly vexing outbreaks or emerging pathogens, such as a worrisome new strain of bird flu.
For day-to-day outbreak detection, officials rely instead on decades-old tests that use pieces of DNA and aren't as precise.
Now, with genome sequencing becoming faster and cheaper, the CDC is armed with $30 million from Congress to broaden its use with a program called advanced molecular detection. The hope is to solve outbreaks faster, foodborne and other types, and maybe prevent infections, too, by better understanding how they spread.
"Frankly, in public health, we have some catching up to do," said the CDC's Dr. Christopher Braden, who is helping to lead the work.
As a first step, federal and state officials are rapidly decoding the DNA of all the listeria infections diagnosed in the U.S. this year, along with samples found in tainted foods or factories.
It's the first time the technology has been used for routine disease surveillance, looking for people with matching strains who may have gotten sick from the same source.
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How to Treat Eczema on the Skin – Tired of Medications? Treat Yourself at Home & Clear You – Video
Posted: at 9:46 pm
How to Treat Eczema on the Skin - Tired of Medications? Treat Yourself at Home amp; Clear You
Eczema is a painful and irritating skin disease that can be cured if treated correctly (especially when natural eczema remedies a. Click Here: | Eczema Treatment. How to Get Rid of Eczema...
By: Healthy Cure
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Childhood eczema may last into adulthood, study says
Posted: at 9:46 pm
Despite a widespread belief that childhood eczema clears up by adolescence, a new study suggests the condition often lasts into adulthood.
Researchers followed kids with eczema over time and found that at least 80 percent of those surveyed at every age had the condition, up to age 26.
"This is a pretty persistent disease," Dr. David Margolis told Reuters Health. "Probably a lot of the adults that have dermatitis had it as children."
Margolis is the study's senior author from the Perelman School of Medicine at the University of Pennsylvania in Philadelphia.
Eczema is a common skin disorder, especially among children, marked by itchy, red skin. Between 10 and 20 percent of children experience symptoms of the condition, according to the National Institutes of Health.
"If you look at dermatologic textbooks over the past 20 years . . . it's pretty much assumed that by the time they're 10 or 12, the majority of them won't have symptoms anymore," Margolis said.
For the new study, he and his colleagues used data from a registry of eczema patients that have been followed since 2004, when they were between the ages of two and 17.
After they were enrolled in the trial, the children and teens received surveys through the mail every six months. Each survey asked if they'd had eczema symptoms within the last six months.
The study is funded by a grant from Valeant Pharmaceuticals, a company that makes a drug used to treat eczema.
The researchers found that at every age throughout the study - from two to 26 years - more than 80 percent of the participants reported eczema symptoms or were still using medications to treat the condition.
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Stress during pregnancy linked to increased asthma risk in children
Posted: at 9:46 pm
Stress during pregnancy brought on by events like divorce, job loss or death of a loved one appears to be linked to an increased risk of asthma and eczema among children.
These findings, Dr. Petra Arck told Reuters Health in an email, could "allow clinicians to evaluate future asthma risk in unborn children using a simple life event assessment questionnaire."
Arck, of University Medical Center Hamburg-Eppendorf in Germany, and her colleagues note that although there are strong genetic components to asthma and related conditions, these alone do not help explain the unprecedented increase in such diseases in recent years.
Over the same period as that increase, they add, stress levels have been on the rise. But there hasn't been much evidence to connect stress in pregnancy to asthma and eczema.
To investigate further, the researchers examined data from 1,587 children and their mothers who took part in an Australian pregnancy study. The original purpose of the study was to determine the effects of intensive fetal monitoring on pregnancy outcomes.
Mothers-to-be were asked about recent stressful life events halfway through their pregnancy and again toward the end of pregnancy. Their children were evaluated for asthma, eczema and other allergy-related conditions at age six and 14.
Complete data were available for 994 children and their mothers.
The researchers calculated that the likelihood of having asthma or eczema as a teenager was substantially higher among children of mothers who experienced stressful life events during the second half of their pregnancies.
Specifically, kids were about twice as likely to have asthma as 14-year-olds if their mothers had been through a single stressful life event, once other factors known to influence asthma were taken into account. Risks were similar when mothers had experienced multiple life stressors.
When the researchers looked closer, they found that pattern only held among children whose mothers did not have asthma themselves.
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Stress during pregnancy linked to increased asthma risk in children
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Patient with Psoriasis & GERD from Hyderabad Sharing Experience at Life Force – Video
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Patient with Psoriasis GERD from Hyderabad Sharing Experience at Life Force
Patient suffering with Psoriasis since 4 years, started treatment at Life Force and within a year got 80% treated. His wife was suffering with GERD and she t...
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Patient with Psoriasis & GERD from Hyderabad Sharing Experience at Life Force - Video
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Gene, immune therapy help cancer war
Posted: at 9:45 pm
Stanford University researcher Irving Weissman explains how the drug Rituxan, generically called rituximab, improves the cancer-killing effect of a new antibody that renders cancer cells vulnerable to immune attack. He spoke Monday, April 7, at the American Association for Cancer Research meeting in San Diego.
The war on cancer is getting some potent reinforcements, including a potentially broad-spectrum new weapon and genetically engineered immune cells with improved cancer-fighting abilities, speakers said at a major cancer research conference held this week in San Diego.
The American Association for Cancer Research, attended by an estimated 18,000 participants, is being held at the San Diego Convention Center through Wednesday. While it is covering the gamut of research, cancer immunotherapy is a major focus. The field began more than 100 years ago, and has lately scored impressive advances by using gene therapy to its tool kit.
The weapon is an antibody that makes a wide range of cancer cells vulnerable to immune attack. It's close to entering human clinical trials, said Irving L. Weissman, a Stanford University professor leading that project. The antibody neutralizes a chemical signal many cancers exude to decoy the immune system, Weissman said in a Monday morning plenary session.
The antibody is being tested first in acute myeloid leukemia patients, backed by $20 million from the California Institute for Regenerative Medicine, Weissman said. The institute is interested because the target cells are cancer stem cells, the cells that proliferate to spread cancer.
Moreover, research indicates the method can be used against many solid tumors that emit the signal, a protein called CD47. These include breast, ovarian, bladder, pancreatic and colon cancer.
"Every human cancer that we've seen has CD47," Weissman said.
Animal studies show that anti-CD47 antibodies inhibit growth of transplanted patient tumors, he said. And when used against non-Hodgkin's lymphoma along with an existing antibody drug called Rituxan, the result is a potent cancer-killing effect. Immune cells called macrophages actually engulf and destroy the cancer cells.
The CD47 molecule is normally present on young cells, serving as a "don't eat me" signal to immune system cells that might otherwise attack them, Weissman said. Cancer cells have chanced on mutations that cause the protein to be made in exceptionally high amounts. So even when they might be abnormal enough to merit immune system attack, they escape surveillance.
Another approach already in the clinic is to genetically engineer immune cells called T cells to be better at fighting cancer. Carl June, a University of Pennsylvania researcher behind one of the studies, said results continue to be encouraging. This approach targets another protein abnormally made by cancer cells, CD19. Novartis is testing the therapy.
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Well-known cancer gene NRAS produces 5 variants, study finds
Posted: at 9:45 pm
A new study shows that a gene discovered 30 years ago and now known to play a fundamental role in cancer development produces five different gene variants (called isoforms), rather than just the one original form, as thought.
The study of the NRAS gene by researchers at The Ohio State University Comprehensive Cancer Center -- Arthur G. James Cancer Hospital and Richard J. Solove Research Institute (OSUCCC -- James) identified four previously unknown variants that the NRAS gene produces.
The finding might help improve drugs for cancers in which aberrant activation of NRAS plays a crucial role. It also suggests that NRAS might affect additional target molecules in cells, the researchers say.
The isoforms show striking differences in size, abundance and effects. For example, the historically known protein (isoform 1) is 189 amino-acids long, while one of the newly discovered variants, isoform 5, is only 20 amino-acids long.
The study is published in the Proceedings of the National Academy of Sciences.
"We believe that the existence of these isoforms may be one reason why NRAS inhibitors have so far been unsuccessful," says corresponding author Albert de la Chapelle, MD, PhD, professor of Medicine and the Leonard J. Immke Jr. and Charlotte L. Immke Chair in Cancer Research.
Co-senior author Clara D. Bloomfield, MD, Distinguished University Professor and Ohio State University Cancer Scholar, notes that one of the newly discovered isoforms might play a greater role in the development of some cancers than the known protein itself.
"Targeting the NRAS pathway may have been unsuccessful in the past because we were unaware of the existence of additional targets of these novel isoforms," says Bloomfield, who is also senior adviser to the OSUCCC -- James and holds the William Greenville Pace III Endowed Chair in Cancer Research.
"The discovery of these isoforms might open a new chapter in the study of NRAS," says first author Ann-Kathrin Eisfeld, MD, a postdoctoral fellow in the laboratories of de la Chapelle and of Bloomfield. "Knowing that these isoforms exist may lead to the development of drugs that specifically decrease or increase the expression of one of them and provide more effective treatment for cancer patients."
For this study, de la Chapelle, Eisfeld and their colleagues analyzed expression of the NRAS isoforms in a variety of normal and matched tumor samples. Key technical findings include:
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