Tuesday, April 22, 2008

How Dietary Restriction Slows Down Aging


ScienceDaily (Apr. 21, 2008) — University of Washington scientists have uncovered details about the mechanisms through which dietary restriction slows the aging process. Working in yeast cells, the researchers have linked ribosomes, the protein-making factories in living cells, and Gcn4, a specialized protein that aids in the expression of genetic information, to the pathways related to dietary response and aging. The study, which was led by UW faculty members Brian Kennedy and Matt Kaeberlein, appears in the April 18 issue of the journal Cell.

Previous research has shown that the lifespan-extending properties of dietary restriction are mediated in part by reduced signaling through TOR, an enzyme involved in many vital operations in a cell. When an organism has less TOR signaling in response to dietary restriction, one side effect is that the organism also decreases the rate at which it makes new proteins, a process called translation.

In this project, the UW researchers studied many different strains of yeast cells that had lower protein production. They found that mutations to the ribosome, the cell's protein factory, sometimes led to increased life span. Ribosomes are made up of two parts -- the large and small subunits -- and the researchers tried to isolate the life-span-related mutation to one of those parts.

"What we noticed right away was that the long-lived strains always had mutations in the large ribosomal subunit and never in the small subunit," said the study's lead author, Kristan Steffen, a graduate student in the UW Department of Biochemistry.

The researchers also tested a drug called diazaborine, which specifically interferes with synthesis of the ribosomes' large subunits, but not small subunits, and found that treating cells with the drug made them live about 50 percent longer than untreated cells. Using a series of genetic tests, the scientists then showed that depletion of the ribosomes' large subunits was likely to be increasing life span by a mechanism related to dietary restriction -- the TOR signaling pathway.

"We knew that dietary restriction decreased TOR signaling, and that decreased TOR signaling reduced translation or protein production, but this was the first direct evidence that all three were acting in the same genetic pathway," said Kennedy, an associate professor of biochemistry.

"The big question then became what's happening in these translation-deficient cells to slow aging," added Kaeberlein, an assistant professor of pathology. "That's when Vivian MacKay, a co-author on the study, had the idea to look at Gcn4."

Gcn4 is a specialized protein called a transcription factor, which helps transfer genetic information during cell growth. The protein is activated when a cell is starving for amino acids. What made Gcn4 interesting to the UW team was its unique mode of regulation.

"When ribosomes aren't working at 100 percent capacity, most proteins are made less efficiently, but Gcn4 is different," explained Dr. MacKay, a research professor of biochemistry. "Sometimes, you actually get more Gcn4 produced even when everything else is going down. That's precisely what we found in the longer-lived yeast strains with mutations in the large subunit of the ribosome."

To make the link between Gcn4 and longevity, the scientists then asked whether preventing the increase of Gcn4 would block life span extension. In every case, cells lacking Gcn4 did not respond as strongly as Gcn4-positive cells.

"The increased production of Gcn4 in long-lived yeast strains, combined with the requirement of Gcn4 for full life-span extension, makes a compelling case for Gcn4 as an important downstream factor in this longevity pathway," Kaeberlein said.

Although scientists don't yet know whether Gcn4 plays a similar role in organisms other than yeast, Kennedy points out that worms, flies, mice and humans all have Gcn4-like proteins that appear to be regulated in a similar way.

"The role of TOR and translation in aging is known to be conserved across many different species, so it's plausible that this function of Gcn4 is conserved as well," Kennedy said. Future research will be aimed at testing this hypothesis.

"Clearly TOR signaling is one component, and perhaps the major component, of the beneficial health effects associated with dietary restriction," said Kaeberlein. "The difficulty with TOR as a therapeutic target, however, is the potential for negative side effects. As we learn more of the mechanistic details behind how TOR regulates aging, we will hopefully be able to identify even better targets for treating age-associated diseases in people."

Adapted from materials provided by University of Washington.

Chemotherapy Causes Delayed Severe Neural Damage, Study Shows
April 22, 2008 — Cancer treatment with chemotherapeutic agents is often associated with delayed adverse neurological consequences -- an occurrence often referred to as "chemobrain" -- that may compromise the quality ... > full story

Thursday, April 3, 2008

Overweight Kids Have Fewer Cavities, New Study Shows

ScienceDaily (Apr. 3, 2008) — Contrary to conventional wisdom, overweight children have fewer cavities and healthier teeth compared to their normal weight peers, according to a study published in this month's issue of Community Dentistry & Oral Epidemiology.

Surprised researchers at the Eastman Dental Center, part of the University of Rochester Medical Center, conducted a secondary analysis of nearly 18,000 children who participated in two separate National Health and Nutrition Examination Surveys (NHANES III and NHANES 99-02).

The study found no differences in rates of caries (tooth decay) among children ages 2-5 in all weight ranges, while children ages 6-18 who were considered overweight and at risk for becoming overweight showed a decreased risk of caries compared to their normal weight peers.

"We expected to find more oral disease in overweight children of all ages, given the similar causal factors that are generally associated with obesity and caries," said Eastman Dental Center's Dorota Kopycka-Kedzierawski, DDS, MPH, the lead author. "Our findings raise more questions than answers. For example, are overweight children eating foods higher in fat rather than cavity-causing sugars? Are their diets similar to normal weight peers but lead more sedentary lifestyles? Research to analyze both diet and lifestyle is needed to better understand the results."

The study defined overweight children as being at the 95th or higher percentile for their age and sex; children at the 85th or higher percentile and less than 95th percentile for their age and sex were defined as at risk for becoming overweight.

Adapted from materials provided by University of Rochester Medical Center, via EurekAlert!, a service of AAAS

Monday, March 10, 2008

First Step Taken To Create Cystic Fibrosis Model Using Pig
March 10, 2008 — The median lifespan for those with cystic fibrosis is 36 years, and lung disease is the major cause of mortality. For years, scientists have studied cystic fibrosis using mice in which the cystic ... > full story

Sunday, February 24, 2008

Novel Link Between Excessive Nutrient Levels And Insulin Resistance Uncovered
February 24, 2008 — For quite some time now, scientists suspected the so-called hexosamine pathway -- a small side business of the main sugar processing enterprise inside a cell -- to be involved in the development of ... > full story

Wednesday, February 20, 2008

Study Of 'Ouzo Effect' May Lead To Design Of Improved Drugs, Cosmetics
February 20, 2008 — Scientists studying the cloudy emulsions produced by anise-flavored liquors such as Ouzo have discovered new molecular insights into their formation, findings that could lead to the design of better ... > full story

Monday, February 11, 2008

Sex, Drugs And Alcohol: Parents Still Influence College Kids' Risky Behavior, Study Shows


ScienceDaily (Feb. 11, 2008) — New research shows that parents influence their child’s likelihood of involvement with drugs, alcohol and risky sexual activity even after their child leaves for college.

In an upcoming issue of the Journal of Youth and Adolescence, Brigham Young University family scientist Laura Walker’s study found that parents’ knowledge or awareness of what’s going on in their child’s life at college is associated with fewer risky behaviors.

Specifically, students who said their fathers were in the loop had a lower likelihood of doing drugs or engaging in risky sexual behaviors. When mothers were in the know, students were less likely to drink alcohol.

The protective effect of mothers’ awareness was more pronounced when the students also felt close to their mom. Under those circumstances, the researchers found that students were less likely to be involved in any of the three risk behavior categories studied: drugs, alcohol and risky sexual activity.

“For parents, the fact that closeness plays a strong role is a message to not be overbearing,” Walker said. “Having a close relationship promotes the child wanting to open up and share what’s going on rather than the parent having to intrusively solicit the information from the child.”

Walker and her colleagues agree that delaying adulthood results in an extension of parents’ period of service to their children. The study’s findings show that the relationships between parents and children continue to be important during the transition to adulthood.

The study involved 200 undergraduate students ages 18 to 25 from two mid-Atlantic colleges, a Midwestern university and a West Coast university. The title of the paper is “The Role of Perceived Parental Knowledge on Emerging Adults’ Risk Behaviors.” Professor Larry Nelson, also from BYU’s School of Family Life, is a co-author on the study.

Delaying adulthood to find identity has bright side

Similar research by Walker and her colleagues finds that delaying the transition to adulthood involves experimentation of a positive nature, indicating this life stage is not simply a period of risk-taking and delinquency.

In an upcoming issue of the Journal of Adolescence, Walker compared the altruism and positive values of two types of emerging adults: those who were already committed to an identity and those still in the process of exploring their identity.

The research found the two groups had few differences when it came to outward behaviors like helping other people and inward personal values such as honesty, kindness and fairness.

“The assumption too often is that delaying adulthood is automatically a negative thing, dominated by exploration with risky drinking, drug use, and sex,” Walker said. “However, these findings suggest that young people are also exploring positive behaviors and participate in society to the same degree as those who have already established their identity.”

The study involved 491 students ages 18 to 25 from two private colleges in the mid-Atlantic, two public universities in the Midwest, and a public university on the West Coast. Each student took a questionnaire about exploration and commitment to an identity. Forty-three percent scored high on commitment to an identity. Another 23 percent scored low on commitment but high on identity exploration. The researchers compared these two groups and found few differences when it came to helping other people, ideas of fairness and honesty and the role of faith in their lives.

The title of the paper is “Looking on the Bright Side: The Role of Identity Status and Gender on Positive Orientations during Emerging Adulthood.” Nelson is also a co-author on this study along with Professor Jason Carroll of BYU’s School of Family Life.

Adapted from materials provided by Brigham Young University.

Changing Our Clocks: New Research Explores How Our Bodies Keep Time
February 11, 2008 — Our alarm clocks may spring forward on March 9, but our biological clocks may take longer to adjust. That's because our internal clocks are so tightly wound to many physiological and behavioral ... > full story

Saturday, February 2, 2008

Diabetes Makes It Hard For Blood Vessels To Relax


ScienceDaily (Feb. 1, 2008) — One way diabetes is bad for your blood vessels is by creating too much competition for an amino acid that helps blood vessels relax, researchers say.

That amino acid, L-arginine, is broken down by the enzyme arginase to urea, which helps the body eliminate toxins resulting from the proteins we eat. Diabetics have a lot of arginase activity, which means they use a lot more L-arginine, says Dr. Maritza Romero, postdoctoral fellow at the Medical College of Georgia and lead author of the paper published in the current issue of Circulation Research.

It also means too little L-arginine is available to help nitric oxide synthase make nitric oxide, the powerful vasodilator that helps blood vessels relax, says Dr. Romero, who works in the lab of Dr. R. William Caldwell, chair of the MCG Department of Pharmacology and Toxicology and the study's corresponding author.

Researchers also found the amino acid, L-citrulline, as well as statins, compounds known to lower cholesterol, prevent elevation of arginase activity, restoring normal dilation abilities in animal models of type 1 diabetes. In fact, L-citrulline can be recycled into L-arginine.

Now they want to know specific factors and pathways involved in arginase activation and develop pharmaceutical agents to combat excessive arginase activity in diabetes. They also suggest clinical trials of L-citrulline as a supplemental therapy for diabetics with vascular problems.

Their findings also help explain why L-arginine supplement, marketed to treat hypertension, chest pain, heart failure and more, may not work long term. In the January 4, 2006 issue of the Journal of the American Medical Association, Johns Hopkins researchers reported that a clinical trial of patients taking an L-arginine supplement following a heart attack didn't improve in their vascular tone or their hearts' ability to pump. In fact, more patients died who were taking L-arginine than placebo and the study was closed with the recommendation the supplement not be used by heart attack patients. The supplement still is widely marketed.

"The findings of increased arginase I activity in diabetes may limit other therapeutic approaches proposed for early endothelial dysfunction such as oral L-arginine supplementation," Drs. Thomas L. Luscher and Jan Steffel, of the University of Zurich Cardiovascular Research Institute write in an accompanying editorial. "Although dietary L-arginine supplementation has been shown to exert vascular protective effects in certain clinical settings, this approach is unlikely to be effective in diabetes, if the results of this study can be confirmed by patients in vivo. In fact, the findings of Romera et al may provide a possible explanation for the unexpected neutral or even adverse effects of oral L-arginine in some clinical studies, in particular patients with coronary artery disease and infarction."

A short intravenous course of L-arginine may provide short-term improvement in blood vessel tone, Dr. Romero notes. However most of L-arginine ingested goes directly to the liver to be broken down, not the bloodstream where it can promote relaxation of blood vessels, Dr. Romero says.

Arginase also is associated with vascular problems related to aging, hypertension, sickle cell disease, atherosclerosis and erectile dysfunction, Dr. Romero says. L-citrulline already is taken by some sickle cell patients to reduce breath-taking fibrosis in their lungs. In addition to helping the body turn toxins into urea that can be safely eliminated from the body, arginase also helps in collagen formation and cell proliferation, but too much can be bad. In fact, Drs. Caldwell and Romero are pursuing studies of how increased arginase activity may harden blood vessel walls.

Adapted from materials provided by Medical College of Georgia.

Taking More Than One Anti-inflammatory Drug May Lead To Complications
February 2, 2008 — A new study found that taking two NSAIDs was associated with lower scores on a health-related quality of life assessment. Nonsteroidal anti-inflammatory drugs (NSAIDs) are used to treat arthritis, ... > full story

Tuesday, January 22, 2008

Genes Linked To Lupus In Women Identified


ScienceDaily (Jan. 21, 2008) — An international consortium of scientists has identified multiple genes that are linked to systemic lupus erythematosus, a devastating autoimmune disease that affects between 1 million and 2 million Americans. Reporting in Nature Genetics, the scientists also confirmed earlier findings linking lupus to several other genes -- highlighting the role that genetics plays in the disease.

These findings underscore that numerous genes, which are often immune-function related, contribute to the risk of developing lupus," said Carl D. Langefeld, Ph.D., senior author from Wake Forest University School of Medicine and co-director of the International Consortium for Systemic Lupus Erythematosus Genetics.

"These results suggest biologic pathways that help us understand the condition better and suggest additional genetic and non-genetic triggers," said Langefeld. "In addition, they help delineate the genetic distinctions between rheumatoid arthritis, lupus and other autoimmune diseases, which could lead to earlier, more accurate diagnoses."

Systemic lupus can involve the joints, kidneys, heart, lungs, brain and blood. The disease occurs in about 31 out of every 100,000 people and affects women nine times more frequently than men. Scientists believe that lupus is caused by genetic variants that interact with each other and the environment.

The current study was made possible because of advances in technology that allow researchers to take a more systematic approach to looking at the entire genome.

The researchers studied the DNA of 720 women of European descent with lupus and 2,337 women without lupus. They scanned the entire genome for more than 317,000 single nucleotide polymorphisms (SNPs), which are locations on chromosomes where a single unit of DNA, or genetic material, may vary from one person to the next. The goal was to identify SNPs linked to lupus. They confirmed these results in another independent set of 1,846 women with lupus and 1,825 women without lupus.

The scientists found evidence of an association with multiple SNPs in three genes: ITGAM, KIAA1542 and PXK, and also at SNP rs10798269, which is not within any known gene. ITGAM is important for both the adherence of immune cells and for cleaning up pathogens. KIAA1542 is important for translating the DNA code into proteins. PXK encodes a molecule that transmits signals and controls complex processes in cells. These scientists also found association in genes previously associated with lupus and other autoimmune diseases.

The scientists are now focusing their attention on specific pathways and genes identified in this study, trying to dissect the precise molecular mechanisms by which these genes contribute to the risk for lupus. Genetic factors likely predict specific complications or patterns of complications. If so, it might be possible to intervene earlier in the process to delay or prevent their onset.

"This initial, important discovery will prove invaluable to all those affected by lupus," said Barbara Boyts, president of the Alliance for Lupus Research, which supported the study and continues to support SLEGEN's efforts to uncover genetic information about lupus. "We are hopeful that this information will lead to new and better treatment possibilities and, eventually, a cure for lupus."

"Lupus is a decimating illness," said John Harley, M.D., Ph.D., lead author and SLEGEN director, from the Oklahoma Medical Research Foundation. "As researchers, our goal is to reduce the burden of suffering caused by this disease. These findings have opened many new doors, and we're excited to investigate what's inside each of them."

Other researchers in SLEGEN include: Marta E. Alarcon-Riquelme, M.D., Ph.D., the University of Uppsala in Sweden, Lindsey A. Criswell, M.D., MPH, the University of California at San Francisco, Chaim O. Jacob, M.D., Ph.D., the University of Southern California, Betty P. Tsao, Ph.D., the University of California at Los Angeles, Robert P. Kimberly, M.D., the University of Alabama at Birmingham, Kathy L. Moser, Ph.D., the Oklahoma Medical Research Foundation, and Timothy J. Vyse, M.D., Ph.D., the Imperial College in London.

This research was supported by the Alliance for Lupus Research and the National Institutes of Health.

Adapted from materials provided by Wake Forest University Baptist Medicl Center.

Saline Nasal Wash Helps Improve Children's Cold Symptoms
January 22, 2008 — A saline nasal wash solution made from processed seawater appears to improve nasal symptoms and may help prevent the recurrence of respiratory infections when used by children with the common cold, ... > full story

Sunday, January 20, 2008

Stem Cell Research Aims To Tackle Parkinson's Disease
January 20, 2008 — Scientists are developing new ways to grow brain cells in the laboratory that could one day be used to treat patients with Parkinson's disease. Stem cell therapy hold the promise of treating disease ... > full story

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