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Mar 10
New class of antibiotics discovered
In a breakthrough, scientists have discovered a new class of antibiotics to fight deadly bacteria such as methicillin-resistant Staphylococcus aureus and other drug-resistant bacteria that threaten public health.

The new class, called oxadiazoles, was discovered by University of Notre Dame researchers led by Mayland Chang and Shahriar Mobashery in silico (by computer) screening and has shown promise in the treatment of MRSA in mouse models of infection.

Researchers who screened 1.2 million compounds found that the oxadiazole inhibits a penicillin-binding protein, PBP2a, and the biosynthesis of the cell wall that enables MRSA to resist other drugs.

The oxadiazoles are also effective when taken orally. This is an important feature as there is only one marketed antibiotic for MRSA that can be taken orally, researchers said.

MRSA has become a global public-health problem since the 1960s because of its resistance to antibiotics.

In the US alone, 278,000 people are hospitalised and 19,000 die each year from infections caused by MRSA, said researchers.

Only three drugs currently are effective treatments, and resistance to each of those drugs already exists.

The researchers have been seeking a solution to MRSA for years.

"Professor Mobashery has been working on the mechanisms of resistance in MRSA for a very long time," Chang said.

"As we understand what the mechanisms are, we can devise strategies to develop compounds against MRSA," said Chang.

"Mayland Chang and Shahriar Mobashery's discovery of a class of compounds that combat drug resistant bacteria such as MRSA could save thousands of lives around the world. We are grateful for their leadership and persistence in fighting drug resistance," said Greg Crawford, dean of the College of Science at the University of Notre Dame.

The research is published in the Journal of the American Chemical Society.

Mar 10
Blood test can predict Alzheimer's: Study
Researchers in the United States say they have developed a prototype blood test that can tell with 90 percent accuracy whether a healthy person will develop Alzheimer`s disease within three years.

The test looks for 10 signatures of fatty proteins called lipids, according to a study published on Sunday in the journal Nature Medicine.

It could help families of people developing the cognitive disorder make early decisions on how best to care for them and may also aid the search for treatment, the authors said.

Several years of clinical trials are likely to be needed to assess the prototype technique, the first blood "biomarker" to predict the tragic degenerative disease.

Alzheimer`s, caused by toxic proteins that destroy brain cells, is a currently incurable and fatal degenerative disease.

Around 35 million people have the disease, a tally that is expected to reach 115 million people by 2050, according to the World Health Organization.

"Our novel blood test offers the potential to identify people at risk for progressive cognitive decline and can change how patients, their families and treating physicians plan for and manage the disorder," said Howard Federoff, a professor of neurology at Georgetown University Medical Center in Washington.

It could also help efforts to treat the disease, he said in a press release.

Attempts to develop drugs for Alzheimer`s have failed possibly because they are tested when the disease has progressed too far, Federoff said.

These treatments may have a better chance of braking or reversing the disease if they are trialled at a much earlier stage, he said.

The researchers started by taking blood samples from 525 healthy volunteers aged 70 and older.

Three years later, they looked at a group of 53 volunteers who had developed symptoms of early Alzheimer`s or a memory-affecting condition known as amnestic mild cognitive impairment (aMCI).

The blood samples from this group were compared against the samples from 53 otherwise healthy volunteers to see what the difference was.

From this, the scientists spotted the 10 telltale lipid proteins, which appear to be metabolised residues of brain cell membranes.

Mar 07
Low fat diets do not curb heart disease, warns US expert
In a setback to those who have switched to low-saturated fat diets for better heart health, a leading US cardiovascular research scientist has claimed diets low in saturated fat or based on Omega 6 fats do not curb heart disease risk or help you live longer.

"Current dietary advice to replace saturated fats with carbohydrates or omega 6-rich polyunsaturated fats is based on flawed and incomplete data from the 1950s," declared James DiNicolantonio in the medical journal Open Heart.

The best diet to boost and maintain heart health is one low in refined carbohydrates, sugars and processed foods, he recommended.

Anyone who has had a heart attack should not be thinking of replacing saturated fats with refined carbs or omega 6 fatty acids -- particularly those found in processed vegetable oils containing large amounts of corn or safflower oil, he added.

"Dietary guidelines should be urgently reviewed and the vilification of saturated fats stopped to save lives," he insisted.

DiNicolantonio said the idea that fat causes heart disease was based on a flawed 1950s study which used data from six countries but excluded data from another 16.

This study "seemingly led us down the wrong 'dietary road' for decades to follow", he said.

There is now a strong argument in favour of the consumption of refined carbohydrates as the causative dietary factor behind the surge in obesity and diabetes in the US.

While a low fat diet may lower 'bad' (LDL) cholesterol, there are two types of LDL cholesterol.

"Switching to carbs may increase pattern B (small dense) LDL which is more harmful to heart health than pattern A (large buoyant) LDL, as well as creating a more unfavourable overall lipid profile," DiNicolantonio noted.

In the race to cut saturated fat intake, several dietary guidelines recommend upping polyunsaturated fat intake.

However, a recent data shows that replacing saturated fats and trans fatty acids with omega 6 fatty acids, without a corresponding rise in omega 3 fatty acids, seems to increase the risk of death from coronary heart and cardiovascular diseases.

"We need a public health campaign as strong as the one we had in the 70s and 80s demonising saturated fats, to say that we got it wrong," urged DiNicolantonio.

"Eating a Mediterranean-style diet rich in fruit, veg, pulses and fish would help lower cholesterol and reduce the risk of coronary heart disease," he suggested.

Mar 07
Restless legs syndrome linked to bigger underlying health problems
A new study has revealed that Restless Legs Syndrome (RLS) may be a possible biomarker for other underlying disease.

The study done by a nationally-recognized sleep expert found that patients with RLS have a higher mortality rate and are prone to cardiovascular diseases and hypertension.

Boston Medical Center neurologist Sanford H. Auerbach said that men with RLS were more likely to be diagnosed with lung disease, endocrine disease, diseases of nutrition and metabolism and immune system problems.

The study was published in Neurology the medical journal of the American Academy of Neurology.

Mar 06
How scientists are rewriting the code of life
Scientists have stumbled upon a novel and path-breaking way to edit our DNAs which may lead to future therapies.

A sophisticated immune system that bacteria use to fight viruses has been unlocked which may provide scientists with unprecedented power to rewrite the code of life, a new research shows.

"It allows customising the genome of any cell or any species at will," Charles Gersbach, assistant professor of biomedical engineering at the Duke University, US, was quoted as saying in a New York Times report.

The molecular system, known as Crispr, is being used to make genetically engineered laboratory animals more easily than before - with changes in multiple genes.

Scientists hope Crispr might also be used for genomic surgery to correct errant genes that cause diseases, said the report.

Agricultural companies might use Crispr to change existing genes in crops to create new traits.

Crispr or 'clustered regularly interspaced short palindromic repeats' is part of an adaptive immune system - one that remembers a pathogen so it is ready the next time the same invader appears.

"The Crispr region is like a tape recording of exposure to prior invaders," said Erik J. Sontheimer, a professor at the Northwestern University.

Cheese and yogurt firms can examine Crispr regions to see if their bacterial cultures are immunised against particular viruses that could slow production.

Some questions, however, have been raised over this method.

For instance, Crispr can sometimes change genes other than the intended ones. That could lead to unwanted side effects, added the report.

Scientists are trying to figure out how to make Crispr more specific.

Mar 06
Tests to start on vaginal ring to prevent pregnancy, HIV
Clinical trials are to begin soon on a new vaginal ring that promises to provide months of protection against pregnancy, HIV and herpes, US researchers said Wednesday.

The device, which is similar to birth control rings already on the market, delivers both an antiretroviral drug and a contraceptive which are slowly released over 90 days.

A report on the ring and how it was developed by scientists at Northwestern University is published in the peer-reviewed journal PLOS ONE.

The ring could offer women an alternative that eliminates the anxiety of missed pills and requires a lower dose of an antiretroviral drug aimed at preventing HIV since it is delivered at the point of transmission.

Scientists and AIDS prevention advocates have been trying to develop a ring like this for a long time, said Rowena Johnston, vice president and director of research at amfAR, the Foundation for AIDS Research.

"If you have something that is long acting that people don`t have to think about every time they have sex but something that is in place, that is thought to be a boon," she said.

While the ring is only designed to protect against transmission during vaginal sex, it could be a valuable tool for some women, she said.

"And it is probably not easily detected by the male partner, if that is important to you," Johnston added.

Both drugs released by the ring -- levonorgestrel and tenofovir -- are already used to prevent pregnancy and the spread of HIV.

Tenofovir -- which inhibits HIV and herpes replication in susceptible cells -- is taken orally by 3.5 million HIV-infected people worldwide.

It has been found to help prevent HIV infection as well, but so far only with pills that must be taken daily.

A gel which delivers tenofovir has been found to be somewhat effective in clinical trials but the gel needs to be inserted into the vagina before and after sex.

Many of the women in the clinical trials did not use the gel every time they had sex.

"Products only work when they are used," said study co-author David Friend, product development director at CONRAD, which develops reproductive health technologies for low-income countries and is affiliated with Eastern Virginia Medical School.

"By having a ring that can remain in the body for up to 90 days, our hope is that this ring will offer a solution to increase adherence, and therefore provide greater protection against HIV while also preventing pregnancy," Friend said.

The differences between the two drugs presented a "huge" design challenge, said Northwestern University biomedical engineer Patrick Kiser, who holds the ring`s patent.

Tenofovir dissolves easily whereas the contraceptive drug levonorgestrel is highly insoluble. The drugs also had to be delivered in drastically different -- but consistent -- doses.

"A lot of engineering has gone into developing the ring," Kiser said.

The ring uses a new kind of polymer -- or chain of molecules -- that swells in the presence of bodily fluids and is capable of delivering up to 100 times more tenofovir than current intravaginal rings.

Mar 05
Yoga can help improve well being of women with breast cancer
Researchers suggest that breast cancer patients who practice yoga, experience better quality of life.

Researchers at The University of Texas MD Anderson Cancer Center conducted the study on 191 women with breast cancer. The sample was split into three groups: yoga, simple stretching and neither.

The results of the research depicted that women undergoing radiation therapy and who have also enrolled in yoga exercises like breathing, meditation and relaxation techniques, experienced improved ability to engage in their daily activities, less stress and fatigue, better regulation of stress hormone cortisol and overall wellbeing.

The study has been published in the Journal of Clinical Oncology.

Mar 05
Male hormones important for female fertility: Study
Researchers including and an Indian origin researcher has said that male hormones, also called androgens, help drive the development of follicles - structures that contain and ultimately release an egg that can be fertilized by a man's sperm.

The research also details how male hormones boost the production of follicles in mice. Authors believe the study provides potential biological targets to enhance fertility in women with diminished ovarian reserve, who produce few or no follicles in response to IVF drugs designed to boost follicle development.

Using multiple animal models and cell experiments, Stephen R. Hammes, M.D., Ph.D.,senior study author and professor of Endocrinology at the University of Rochester School of Medicine and Dentistry, and lead study author Aritro Sen , Ph.D., research assistant professor of Endocrinology at the medical school found that male hormones promote follicle development in two ways.

First, they prevent follicles from dying at an early stage. They do this by ramping up a molecule that stops cells from self destructing, a process called apoptosis. Hammes and Sen speculate that if a woman doesn't have enough androgens (male hormones), more of her follicles may be dying and fewer progressing to a mature stage when they produce and release an egg.

Second, androgens make ovarian cells more sensitive to follicle-stimulating hormone or FSH, which promotes follicle growth. They do this by creating more FSH receptors - molecules on the surface of ovarian cells that jumpstart the follicle making process in response to the hormone.

When the team administered small doses of androgens to mice that were taking the equivalent of medications given to women undergoing IVF therapy, they developed more mature, egg-containing follicles than mice that didn't receive androgens.

The androgen-treated female mice also released larger numbers of eggs with ovulation.

The study has been published in the Proceedings of the National Academy of Sciences.

Mar 03
Gene mutation behind type 2 diabetes identified
Researchers have identified mutations in a gene that can reduce the risk of developing type 2 diabetes, even in people who have risk factors such as obesity and old age.

The current study breaks new ground in type 2 diabetes research and guides future therapeutic development in this disease. In the new study, researchers describe the genetic analysis of 150,000 patients showing that rare mutations in a gene called SLC30A8 reduce risk of type 2 diabetes by 65 percent.

The results were seen in patients from multiple ethnic groups, suggesting that a drug that mimics the effect of these mutations might have broad utility around the globe.

The protein encoded by SLC30A8 had previously been shown to play an important role in the insulin-secreting beta cells of the pancreas, and a common variant in that gene was known to slightly influence the risk of type 2 diabetes.

However, it was previously unclear whether inhibiting or activating the protein would be the best strategy for reducing disease risk - and how large an effect could be expected.

The team set out to ask if the effects of SLC30A8 protective mutations were limited to the two mutations found in populations in Finland and Iceland. As part of the NIH-funded T2D-GENES Project, chaired by Mike Boehnke at the University of Michigan, the Broad Institute had performed sequencing of 13,000 samples drawn from multiple ethnicities.

The T2D-GENES Project joined the collaboration, found ten more mutations in the same gene, and again saw a protective effect. Combining all the results confirmed that inheriting one copy of a defective version of SLC30A8 led to a 65 percent reduction in risk of diabetes.

In laboratory experiments, members of Altshuler's team showed that the protective mutations disrupt the normal function of the protein encoded by SLC30A8, known as ZnT8. The ZnT8 protein transports zinc into insulin-producing beta cells, where zinc plays a key role in the crystallization of insulin. Exactly how the reduction in ZnT8 functions plays a protective role remains unknown.

THE study has been published in the journal Nature Genetics.

Mar 03
HIV vaccine comes closer to reality
A research team has found how the immune system makes a powerful antibody that blocks HIV infection of cells by targeting a site on the virus called V1V2.

Analyses of the results of a clinical trial of the only experimental HIV vaccine to date to have modest success in people suggest that antibodies to sites within V1V2 were protective.

The new findings point the way toward a potentially more effective vaccine that would generate V1V2-directed HIV neutralizing antibodies.

The study led by scientists from the National Institute of Allergy and Infectious Diseases (NIAID) began by identifying an HIV-infected volunteer in the CAPRISA cohort who naturally developed V1V2-directed HIV neutralizing antibodies, named CAP256-VRC26, after several months of infection.

Using techniques similar to those employed in an earlier study of HIV-antibody co-evolution, the researchers analyzed blood samples donated by the volunteer between 15 weeks and 4 years after becoming infected.

This enabled the scientists to determine the genetic make-up of the original form of the antibody; to identify and define the structures of a number of the intermediate forms taken as the antibody mutated toward its fullest breadth and potency; and to describe the interplay between virus and antibody that fostered the maturation of CAP256-VRC26 to its final, most powerful HIV-fighting form.

Notably, the study revealed that after relatively few mutations, even the early intermediates of CAP256-VRC26 can neutralize a significant proportion of known HIV strains.

This improves the chances that a V1V2-directed HIV vaccine developed based on the new findings would be effective, according to the scientists, who have begun work on a set of vaccine components designed to elicit V1V2 neutralizing antibodies and guide their maturation.

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