There’s quite a competition these days for the best minds in the field of adaptive immune responses, and GlaxoSmithKline has provided Tempero Pharmaceuticals with some of the hottest recruits to be found in this emerging class of new drugs. As Xconomy’s Ryan McBride reports, GSK launched Tempero just a little more than a year ago to establish a leading position in this section of the immunology field, and it quickly focused on the top academics.

“There was a realization that a lot of the basic science in this space was driven by academic thought leaders,” Tempero CEO Spiros Jamas told Xconomy. “And a lot of them were being pursued by venture capital groups or other companies, so there was a competition. In order to attract the academic experts, and build a group quickly, the decision was made that this was a ripe opportunity to set this up as an independent company with a biotech model.”

Harvard’s Christophe Benoist, Vijay Kuchroo and Diane Mathis provided the scientific brain trust needed by the developer. And leading biotech figures like Rich Aldrich and Alnylam’s John Maraganore are offering guidance on the board. Currently, the developer is engaged in preclinical work identifying new therapies for MS, psoriasis and diabetes.

Source: FierceBiotech

Popularity: 1% [?]

An experimental breast cancer drug made from sea sponges added months to the lives of breast cancer patients whose cancer had come back despite several rounds of chemotherapy, doctors reported Sunday.

Eisai’s eribulin added an average of two and a half months to the lives of patients dying of breast cancer, which is a big improvement in such seriously ill cancer patients, the international team of researchers said.

The results of the Phase III trial, presented to a meeting of the American Society of Clinical Oncology in Chicago, have been anticipated after Eisai was given priority review June 1 for U.S. Food and Drug Administration approval of the drug.

“This is potentially practice changing,” ASCO president Dr. Douglas Blayney said in a telephone interview.

Dr. Christopher Twelves of St. James Hospital in Leeds in Britain and an international team studied 762 breast cancer patients with different types of tumor.

All had cancer that had spread and been through at least two rounds of chemotherapy. Two-thirds got two doses of eribulin while getting standard treatment, usually with one other chemotherapy drug but occasionally with just supportive care to treat pain and other symptoms.

The other third got either a third round of chemotherapy or supportive care. “Once this treatment fails, the patient often died,” Blayney said.

The patients given eribulin did considerably better, the researchers told the meeting. The eribulin patients lived a median of 13 months, compared to just under 11 months for patients who did not get eribulin.

LONGER LIVES

Most cancer trials look for what is called progression-free survival, meaning the doctors are looking to see if the tumors start growing back, or sometimes just response rate, to see if the tumors shrink at all.

This one looked to see how long the patients actually lived.

“This study is the first to compare overall survival with this new chemotherapeutic agent to real-life choices in heavily pretreated patients with metastatic breast cancer,” Twelves and colleagues said in their written presentation.

The drug works on the same principle, but with a slightly different mechanism, as older cancer drugs called taxanes and is infused intravenously.

Other experts said eribulin could be one of the last new chemotherapy drugs, which typically target fast-growing cells that include tumors but also healthy cells.

“This is the era of targeted therapy. It’s not an era of chemotherapy,” said Dr. Eric Winer of Harvard’s Dana-Farber Cancer Institute in Boston, who was not involved in the study.

“I don’t know that there are going to be many more chemotherapy agents approved for women with breast cancer. That said, this may be one of the last, and potentially provide women with an additional option and maybe an option to be used in combination with targeted therapies in the future.”

Three other studies presented to the meeting showed eribulin was effective and tolerated in a different group of patients with breast cancer, as well as colon cancer and urinary cancer patients.

Eisai has filed in Japan, the United States and Europe for approval of eribulin. The company hopes it will become a blockbuster, with global earnings of $1 billion a year.

“I think there is a reasonable chance that this drug will actually get approved,” Winer said. “There aren’t many drugs that show a survival advantage in this setting.”

Source: Reuters

Popularity: 2% [?]

US researchers say they are a step closer to understanding why some people have natural protection against HIV.

They believe rare individuals who progress very slowly to Aids when infected make white blood cells that are better at fighting the virus.

The findings, published in Nature, may help international efforts to design an effective Aids vaccine.

But the research team at MIT and Harvard says any such vaccine is at least a decade away.

The findings relate to so-called “elite controllers” – a small number of people who, when exposed to HIV, progress very slowly to Aids or never develop it at all.

In the late 1990s it was discovered that these individuals – about one in 200 of those infected with HIV – carry a specific gene, known as HLA B57.

The research team, led by MIT Professor Arup Chakraborty and Harvard Professor Bruce Walker, found this gene causes the body to make more potent killer T cells – a type of white blood cell that fights infections.

This helps them to keep the HIV virus at bay, but also makes them more susceptible to autoimmune diseases, where the body’s immune system turns on itself.

The work is based on computer modelling of how immune cells develop in a specialised organ of the immune system known as the thymus.

Vaccine puzzle

The researchers say the study has implications for designing an effective vaccine.

It could help them develop vaccines that provoke the same response to HIV that individuals with “natural immunity” can do on their own.

But they say even if they knew exactly what vaccine they wanted to make, it would take at least a decade to reach the hands of a healthcare worker.

Prof Bruce Walker told the BBC: “Some people are able to control HIV on their own and it’s really critical for us to understand how this happens. This study takes us a step forward in understanding that.”

Prof Chakraborty added: “It shows another piece in the puzzle of what we want a vaccine to do.”

Genetic defences

Commenting on the study, Jason Warriner, clinical director at the Terrence Higgins Trust, said: “Anything that gives us greater insight into genetic defences related to HIV is useful in searching for a vaccine and, one day, a cure for this complex virus.

“However, these elite controllers are a tiny proportion of people and they are not immune from HIV-related illnesses.

“HIV remains the UK’s fastest-growing serious health condition, with 83,000 people affected, so it is vital that people continue to use condoms to protect themselves.”

The study is published online in the journal Nature.

Source: BBC NEWS

Popularity: 2% [?]

Francis Collins, who helped map the human genome, did not get around to having his own genes analyzed until last summer. And he was surprised by what he learned.

Collins has a predisposition for type-2 diabetes, something he had never suspected. The lanky, former director of the National Human Genome Research Institute (NHGRI) discovered this through tests offered by Navigenics, 23andMe and DecodeMe — companies that charge customers a few hundred dollars for a peek at their genetic makeup.

“I signed up for all three because I wanted to see if they gave the same answer,” he said. “They all agreed my diabetes risk is higher.”

Armed with that information, he eventually lost 25 pounds. But as a rule, he doesn’t consider such tests especially useful — at least not yet. “Admittedly, right now your family history may be your best bet and it doesn’t cost anything,” he said.

And so it goes in the fledgling genome field.

Some experts say the world is on the cusp of a “golden age” of genomics, when a look at the DNA code will reveal your risk of cancer, diabetes or heart disease, and predict which drugs will work for you. Yet the $3 billion international Human Genome Project, whose first phase was completed a decade ago, has not led to a single blockbuster diagnosis or product.

To be sure, there have been some tantalizing glimpses:

– A personalized blood test can tell whether a patient’s cancer has spread or come back. Dr. Bert Vogelstein of Johns Hopkins University in Baltimore and colleagues found stretches of DNA in colon and breast tumors with extra DNA copies, or fused-together chromosomes.

– A gene-based test called Oncotype DX made by Genomic Health Inc helps identify breast cancer patients who are not likely to benefit at all from chemotherapy.

– Dr. James Lupski of the Baylor College of Medicine in Houston studied his own entire DNA map and sequenced the genomes of family members — including his deceased grandfather — to diagnose the mutation causing his rare genetic nerve disease, called Charcot-Marie-Tooth syndrome.

– Genetic tests are now able to pick out poor responders to Plavix, or clopidogrel, a common life-saving anticlotting drug made by Sanofi-Aventis SA and Bristol-Myers Squibb Co.

Still, Collins describes this as low-hanging fruit. He says the hard work is only just beginning.

In a sense, the field is a victim of its own success. Companies are beating down the price of genetic sequencing, competing to make the machine that every biotech lab will have as standard equipment to sequence a person’s entire genome on the spot. But all this genome sequencing is creating what current NHGRI director Dr. Eric Green calls a “tsunami of information” that is overloading the brains of scientists and the capacity of computers.

Paradoxically, this reflects the fact that people have relatively few actual genes, the stretches of DNA that instruct a cell to make a protein, or what Green refers to as “bricks and mortar.” Humans have just 20,500 of them, compared with up to 30,000 for mice and 50,000 in rice. That was one of the big surprises from the Human Genome Project.

As a result, much of the most important information lies in what used to be called “junk DNA,” which makes up two-thirds of the human genetic code.

“There is this dark matter of the genome that is lurking out there, waiting to be uncovered,” says Collins.

PUT IT IN THE BIOBANK

One part of the hunt starts in a nondescript building in west London, where volunteers line up to reveal their innermost secrets. While many have given blood before, this time they are donating their DNA and medical records, both past and future, to a vast experiment that will track them to the grave.

It sounds Orwellian. Yet volunteers checking into UK Biobank — backed by the government and the Wellcome Trust — are keen to participate in something that might help their children or grandchildren.

This age group, 40 to 69 years, has been chosen because the volunteers won’t keep researchers waiting too long before developing interesting conditions such as cancer, arthritis, diabetes, heart disease and dementia.

So far some 450,000 Britons have signed up, consenting to have their DNA sequenced and their health tracked, anonymously, through the National Health Service.

The target of 500,000 should be reached around July, by which time the project’s giant freezer facility in northern England will have the equivalent of two road tankers worth of frozen blood samples.

Principal investigator Dr. Rory Collins says it is only by doing such large-scale sampling that scientists can uncover how lifestyle factors interact with a long list of rare genetic variants to cause common diseases.

“If you are looking for the effect of lots and lots of different genetic variants that are producing modest effects and they’re interacting with a lot of non-genetic factors, then you need to be able to do studies that are very, very big,” he said. “It’s only just now that the technology allows those experiments to be done.”

China, Sweden and other countries have also set up biobanks but the British one is the most comprehensive in terms of the number of factors studied. Organizers hope it will go beyond what earlier biobanks produced — like one in Iceland that helped create gene-hunting firm Decode Genetics.

Working out of a glass-and-steel building on the outskirts of Reykjavik, Decode’s scientists have peppered the scientific literature with reports on common DNA variants linked to schizophrenia, cancer and other diseases by trawling the country’s genetic heritage, which has changed little since the Vikings arrived more than 1,000 years ago.

Understanding a few of the pieces of the gene puzzle, however, was not enough to shore up Decode’s ailing business and the former Nasdaq-listed company filed for bankruptcy protection last November. It re-emerged as a private business in January.

Decode was one of a number of biotech start-ups that rode the first wave of genomics, offering the technological tools needed to understand the links between genes and diseases. Many fell by the wayside after just a couple of years — but not all.

Human Genome Sciences Inc is one that finally looks set for prime time. Its shares have skyrocketed since last year, when it reported unexpectedly strong data from a trial of its experimental lupus drug Benlysta.

Last March the company was trading as low as 45 cents; now its shares hover around $30. If approved, the drug, which is being developed in partnership with GlaxoSmithKline Plc, would be the first new treatment for lupus, a serious immune system disease, in more than 50 years.

But such winners are rare and investors remain wary of biotech drug developers over-selling the promise of genomics, given the fact that new medicines face a risky, 10 to 15-year path to market.

In fact, the past decade has turned out to be the worst in the history of the drugs industry, with a dearth of new medicines and an unprecedented cliff of patent expiries.

“There is no question that people have felt that they got their fingers burned and the enthusiasm has decreased a great deal,” said Glaxo’s head of genetics Lon Cardon.

The problem for drug developers and investors is that greater knowledge has brought with it greater complexity, frustrating early hopes for relatively simple fixes to complex diseases.

Yet Cardon, too, now sees a turning point, driven by cheaper, faster sequencing and clear advances in one key disease area — cancer.

GENES AND CANCER

For many cancer patients, a major fear is that their surgeon missed something and their cancer will grow back. The only way to tell now is to wait until tumors are big enough to be spotted by imaging machines.

That could soon change. A gene-based test that can search a patient’s blood for tiny bits of DNA shed from tumors may soon give doctors an early warning that they may have missed something.

“That’s only become possible through the advent of so-called next-generation sequencing technology,” said Dr. Bert Vogelstein of Johns Hopkins University in Baltimore and the Howard Hughes Medical Institute, who is developing the blood test.

The test takes advantage of rapid advances in the technology to sequence whole genomes. The latest machines from companies like Illumina Inc and Life Technologies Corp can map out a patient’s whole DNA code in just a few weeks for as little as $5,000, a far cry from 13 years and $3 billion it took Collins and his international collaborators to get the first human genome.

Vogelstein said the rapidly falling cost of genome sequencing means the blood test could be affordable enough to be on the market within two years. Before long, all cancer patients could have their tumors sequenced routinely to find the genetic defects that cause them to grow.

“Cancer is maybe the best disease to cut our teeth on,” said Yale Medical School geneticist Richard Lifton. “The reason for that is we know that cancer is largely a disease in changes of DNA sequence.”

Matthew Meyerson of the Dana-Farber Cancer Institute and the Broad Institute of Harvard and the Massachusetts Institute of Technology said he is impressed by the pace of change. “The first cancer gene sequence was reported in 2008. There were probably 100 done last year. Maybe there will be many hundreds or even 1,000 this year,” he said.

Lifton predicts that within the next two years, scientists will have the genetic sequence of every major human cancer. “Many of these will identify new genes that we had not previously known about with a role in cancer,” he said. “Some of these will turn out to be incredibly important new drug targets.”

Or new tests, as Collins suggests. “If you’ve just discovered the molecular basis of a rare disease, you can turn it into a (test),” he said.

A new industry is just emerging to help them get there — and its smart kit is bowling over scientists.

SHRINKING TECHNOLOGY

Dr. Eric Green had never seen anything like it. At a meeting of what he calls “sequencing geeks” at Marco Island, Florida in February a small start-up called Ion Torrent was demonstrating its new DNA sequencer.

“It’s the size of a computer printer,” he said. “They were sequencing in a hotel room.”

It was a shock to researchers who had used rooms the size of a football field full of sequencers for the original human genome.

Green said his institute has directed some funding to Guilford, Connecticut, and San Francisco based Ion Torrent for its $50,000 sequencer.

“This may completely crash and burn,” he acknowledged. But he and others were intrigued at the company’s compact system to detect individual molecules of hydrogen as a way to sequence the A, C, T, G code of DNA.

In another room was Pacific Biosystems’ $750,000 sequencer the size of a conference table.

“It is the Wild West,” Green said. “It is emblematic of what is going on in the field now, with not one, not two, not three, not four but multiple technologies.”

They are doing what the companies and the researchers want, and prices are plummeting. “There is a mix of science and business here,” said Green. “It’s breathtaking, what is happening.”

If human genome sequencing is to transform medicine, it will have to be quick and easy to do. “One could imagine that acquiring a complete genome sequence of an individual might become the standard of care one day,” Green said.

“What these companies are doing is giving us a taste of the future of medicine.”

Dr. Richard Gibbs, who directs the Human Genome Sequencing Center at Baylor College of Medicine in Houston, said there are about 20 to 30 different sequencing companies out there that are trying new things.

He said scientists had expected to have to wait for these machines to produce real breakthroughs, but the ones by Illumina and Life Technologies are cranking out so much data and the price is falling so quickly that they are likely to be the ones that transform medicine.

“The current things are performing so damn well they are blowing out of the water the pie-in-the-sky numbers that were pushed around by the next next-generation companies,” Gibbs said.

Illumina’s Chief Executive Jay Flatley said storing and analyzing the trillions of bits of data generated by their machines will likely be the biggest future stumbling block for sequencing companies.

Collins is confident they can do it. “We are not going to hit any limits any time soon,” he said. “No laws of physics need to be broken … We’ll have the $1,000 genome in a few years. It will (eventually) be possible for people to make a $100 genome.”

The high expense is not stopping China, which is making a big push into genomics. The Beijing Genomics Institute just bought 128 Illumina machines and is employing 1,000 researchers to focus on illnesses that are specific to Asian populations. They may also find new markets for drugs.

AstraZeneca Plc’s lung cancer pill Iressa, or gefitinib, was found to work far better than chemotherapy in people from East Asia whose tumors had specific mutations in genes for the epidermal growth factor receptor or EGFR. The discovery saved the drug, which only works in about 10 to 15 percent of lung cancer patients in Europe and which was headed for the trash bin.

“Most genomics research has been done on Caucasians based in Europe or the United States and we are only just starting to understand about how applicable these findings are to worldwide or Asian populations,” said Martin Hibberd of the Genome Institute of Singapore.

ANALYZE THIS

None of this means people should rush out to have their DNA tested by companies such as 23andMe and DecodeMe.

“I’d hesitate to call them a scam,” said Frances Flinter, a member of Britain’s Human Genetics Commission which is coordinating a global working group on the new guidelines. “Some of the companies offering these tests are trying very hard to develop something that has some scientific validity. But at the moment the scientific knowledge doesn’t exist to demonstrate they are useful.”

The Human Genetics Commission’s working group — which also includes members from Iceland’s Decode and California’s Navigenics — say firms should ensure buyers understand what they are doing, and what the outcome of the actions might be.

The draft guidelines, due to be revised by the end of the year, also suggest firms should only offer tests for incurable conditions like Huntington’s or Parkinson’s disease with “before and after” counseling, and on other tests, “make clear the limitations … and the relative roles of genetic makeup and lifestyle.”

“For the vast majority of people, decisions on lifestyle will probably have far more impact on health,” said Flinter, a consultant in clinical genetics.

Collins agrees. After all, the leading causes of death in the developed world — cancer, heart disease, stroke, diabetes — all can be prevented to a large degree with exercise, by avoiding tobacco and by eating less fat and sugar and more fruits and vegetables.

Then again, he had no family history of diabetes.

“Everybody in my family is lean and athletic so perhaps they were fighting off their genetic risks by their individual behavior choices,” he said.

“I wasn’t looking that lean and athletic when I got these test results last summer, and it caused me to pay attention to something I should have paid attention to all along.”

Source: Reuters

Popularity: 6% [?]

Genentech chairman and CEO Art Levinson and his executive team got a wintry day in Manhattan to make their case to investors that Roche is lowballing the company with its $86.50 hostile tender for the shares of the company it doesn’t already own.

Despite projections of a near-doubling of revenues to $17 billion by 2015 and descriptions of some 25 new drugs being tested in patients, the team’s reception from traders was as chilly as the weather. Genentech shares fell nearly $4, to finish almost $5 off the offering price.

[ad]

But it’s hard to put a value on much of what Levinson said in a 40-minute talk that included a mini-lecture on the biology of allergies and a proud recitation of the fruits of Genentech’s culture. Those include a first-place ranking in the number of biotech patents issued in 2007, easily topping the University of California and the U.S. Government, and a best employer for scientists from Science Magazine in six of the last seven years.

Genentech more than most any company encourages its researchers to publish findings in top peer-reviewed journals — leading to another recent first: the most citations in papers by other researchers in the field molecular biology and genetics. Genentech trumped Harvard, UCSF and Stanford among others in this category.

That’s a reflection “of the quailty of the science that we do,” Levinson said.

Pranks are another part of Genentech culture and to the Health Blog’s eye, Levinson pulled one on Roche in his closing remarks. Arguing that Roche’s offer failed to adequately account for the value of Genentech’s drugs to Roche, he displayed a bar graph showing how the percentage of Roche drug sales based on Genentech-derived products increased from 21% in 2000 to 66% in 2008.

What would the picture look like without those drugs, he asked? The next slide provided the answer: Animated flames consumed the Genentech portion, leaving a charred vision of Roche’s remaining sales.

Source: The Wall Street Journal

Popularity: 3% [?]

Virginia Commonwealth University researchers have identified a gene that plays a key role in regulating liver cancer progression, a discovery that could one day lead to new targeted therapeutic strategies to fight the highly aggressive disease.

Hepatocellular carcinoma, HCC, or liver cancer, is the fifth most common cancer and the third leading cause of cancer deaths in the world. Treatment options for HCC include chemotherapy, chemoembolization, ablation and proton-beam therapy. Liver transplantation offers the best chance for a cure in patients with small tumors and significant associated liver disease.

[ad]

In the study, published online in the February issue of the Journal of Clinical Investigation, researchers reported that the astrocyte elevated gene-1, AEG-1, plays a key role in regulating HCC in series of cellular models. By examining human liver tumor cells of patients with HCC, the team found that the expression of AEG-1 gradually increases as the tumor becomes more and more aggressive. Using microarray technology, they analyzed cDNA from the tumor cells and determined that AEG-1 modulates expression of genes relevant to the progression of HCC, including invasion, metastasis, resistance to chemotherapy, the formation of new blood vessels, and senescence. cDNAs are complementary DNAs that are generated from mRNAs to analyze gene expression profiles.

“AEG-1 also activates multiple intracellular signaling pathways that are known to be involved in HCC progression. So, strategies to inhibit AEG-1 that could lead to the shutdown of these pathways, either by small molecules or by siRNAs, might be an important therapeutic modality for HCC patients,” said principal investigator Devanand Sarkar, Ph.D., MBBS, assistant professor in the Department of Human and Molecular Genetics in the VCU School of Medicine, and Harrison Endowed Scholar in Cancer Research at the VCU Massey Cancer Center.

siRNAs are small inhibitory RNAs that can specifically inhibit targeted mRNA and protein production. siRNAs may be used in the future for targeted inhibition of AEG-1 in patients, Sarkar said.

According to Sarkar, the team found a significantly higher expression of AEG-1 protein in more than 90 percent of tumor samples from HCC patients compared to normal human liver cells.

“The expression of AEG-1 protein gradually increases as the disease becomes more aggressive. No other genes have been shown to be upregulated in such a high percentage of HCC patients,” said Sarkar.

Further, he said that findings from a separate pool of 132 HCC patients revealed significant overexpression of AEG-1 mRNA compared to normal liver. In a subset of these patients, the team detected an increased number of copies of the AEG-1 gene.

“We observed an increase in AEG-1 DNA, mRNA and protein in HCC patients, which indicates a significant involvement of AEG-1 in HCC progression. Stable overexpression of AEG-1 converts non-tumorigenic human HCC cells into highly aggressive vascular tumors and inhibition of AEG-1 abrogates tumorigenesis by aggressive HCC cells,” he said.

Previous studies suggest that the expression of AEG-1 is very low in normal cells or tissues such as breast, prostate and brain. However, in cancers of the same organs, expression of AEG-1 is significantly increased.

The team will conduct studies to further understand the molecular mechanisms by which AEG-1 works and identify other proteins with which it interacts.

This work was supported by grants from The Goldhirsh Foundation, the National Institutes of Health, the Spanish National Health Institute, and the Samuel Waxman Cancer Research Foundation.

Sarkar worked with a team that included VCU School of Medicine researchers, Byoung Kwon Yoo, Ph.D., Zao-zhong Su, Ph.D., Nitai D. Mukhopadhyay, Ph.D., Alan Scott Mills, M.D., Robert A. Fisher, M.D., and Paul B. Fisher, M.Ph., Ph.D.; Luni Emdad Ph.D., Augusto Villanueva, Ph.D., Samuel Waxman, M.D., Josep M. Llovet, M.D., all from the Mount Sinai School of Medicine in New York; and Derek Y Chiang, Ph.D., with the Broad Institute of Harvard and MIT. Sarkar and Paul B. Fisher are the founding members of the VCU Institute of Molecular Medicine, which also provided support in conducting these studies.

About VCU and the VCU Medical Center:
Virginia Commonwealth University is the largest university in Virginia and ranks among the top 100 universities in the country in sponsored research. Located on two downtown campuses in Richmond, VCU enrolls 32,000 students in 205 certificate and degree programs in the arts, sciences and humanities. Sixty-five of the programs are unique in Virginia, many of them crossing the disciplines of VCU’s 15 schools and one college. MCV Hospitals and the health sciences schools of Virginia Commonwealth University compose the VCU Medical, one of the nation’s leading academic medical centers. For more, see www.vcu.edu.

Source: Virginia Commonwealth University

Popularity: 6% [?]

Get ready for results from a cholesterol-drug study of jovian proportions.

After the storm from studies of Merck and Schering-Plough’s Vytorin, though, you may be surprised to know this one on AstraZeneca’s Crestor looks pretty good.

[ad]

The 18,000-patient trial, known as Jupiter, was halted last spring, much earlier than expected, after a planned interim check found substantial reductions in deaths, heart attacks and other serious events in patients taking the drug compared with placebo, the WSJ explains this morning. So we know the results are good, but just how good will be revealed in a few days.

A big reason the study is garnering so much interest is the type of patients in it. They had normal level of bad cholesterol — below 130 — and no evidence of disease. So they wouldn’t qualify for statin therapy under current guidelines. They did have heightened levels of a marker for inflammation called C-reactive protein that’s been the subject of debate among cardiologists.

Considering the study’s results, which will be described in detail at the American Heart Association’s upcoming annual scientific meeting, this may open up a new market in a much broader group of patients.

“This will take the world by storm,” Christopher Cannon, a cardiologist at Harvard and Brigham and Women’s Hospital, predicted in an interview with the WSJ.

Source: The Wall Street Journal

Popularity: 4% [?]