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Scientists identify a key barrier to proliferation of insulin-producing … – Medical Xpress

Posted: March 10, 2017 at 12:42 pm

March 9, 2017 Rohit Kulkarni, M.D., Ph.D., Senior Investigator at Joslin Diabetes Center, and Professor of Medicine at Harvard Medical School. Credit: John Soares

If you become resistant to insulin, a condition that is a precursor to type 2 diabetes, your body tries to compensate by producing more of the "beta" cells in the pancreas that produce the critical hormone. Researchers have long sought to understand why these cells often fail to proliferate in people who go on to develop the disease. Studying both humans and mice, scientists at Joslin Diabetes Center now have pinpointed one key biological mechanism that can prevent the cells from dividing successfully.

Better understanding of the beta-cell proliferation process eventually may lead toward therapies for diabetes patients, whose supplies of these cells often shrink over time, says Rohit Kulkarni, M.D., Ph.D., a Joslin Senior Investigator and senior author on a paper about the work published in the journal Cell Metabolism.

Previous studies of beta cell proliferation generally have focused on mechanisms that kick off the cell cycle that leads to successful cell division. "Most adult mammalian beta cells are in a quiescent phase, and so if you want to push them into the cell cycle, you need to shake them out of their sleep," explains Kulkarni, who is also a Professor of Medicine at Harvard Medical School. Over the years, scientists have discovered a number of biological mechanisms that help to initiate the cell cycle.

"However, very often many of the beta cells that begin the cell cycle don't complete it, because the regulatory signals aren't appropriate," Kulkarni notes. "The cells choose to die because that's an easier route than completing the cell cycle."

Seeking to understand this failure to divide, his lab previously analyzed beta cells that were modified to lack an insulin receptor and didn't divide as easily as normal beta cells. Among their findings, the scientists saw that these cells generated significantly smaller amounts than normal beta cells of two proteins that partner to help separate the cell's chromosomes just before the cell divides.

In their latest research, the Joslin team performed many experiments to explore the actions of these two proteins, called centromere protein A (CENP-A) and polo-like kinase-1 (PLK1), in mice and in cells from humans and mice.

Among their experiments, the researchers studied beta cell signaling in mice that were modified to lack expression of the proteins and experienced insulin resistance by being placed on a high-fat diet, or aging, or becoming pregnant. "We showed that mice that lacked the CENP-A protein could not compensate for insulin resistance by making more insulin-secreting cells," Kulkarni says.

Additionally, his team examined human beta cells and found lower levels of CENP-A and PLK-1 proteins in cells from donors with diabetes compared to cells from healthy donors.

To better understand how insulin signaling affects beta-cell growth, the Joslin scientists next studied a pathway involving a protein called FOXM1. This protein acts as a "transcription factor" that regulates genes by binding to their DNA regions. FOXM1 helps to drive cell proliferation, and it can promote the expression of CENP-A and PLK-1.

"We found that insulin signaling can initiate the binding of this transcription factor with PLK-1 and CENP-A, in both mouse and human beta cells," Kulkarni says. "This binding is lost in beta cells lacking the insulin receptor, and the loss of binding leads to cell death rather than division."

"We also discovered that this type of regulation is, interestingly, specific to beta cells, and not seen in other metabolic cell types such as liver and fat cells," he says.

Given this new insight into how beta cells divide or fail to divide, "our next step will be to begin to ask whether we can target FOXM1 or other proteins in the pathway to enable a better progression through the cell cycle and to generate more beta cells," Kulkarni says.

The research may hold the eventual promise of treatments not only for type 2 diabetes but for type 1 diabetes, in which beta cells are wiped out by autoimmune attack, he adds.

Joslin's Jun Shirakawa was first author on the paper. Other contributors, all from Joslin, included Megan Fernandez, Tomozumi Takatani, Abdelfattah El Ouaamari, Prapaporn Jungtrakoon, Erin Okawa, Wei Zhang, Peng Yi and Alessandro Doria. The National Institutes of Health provided lead funding for the study.

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Interval training exercise could be a fountain of youth – CNN

Posted: March 10, 2017 at 12:42 pm

"Any exercise is better than being sedentary," said Dr. Sreekumaran Nair, senior author of the study and a diabetes researcher at the Mayo Clinic in Rochester, Minnesota. However, Nair noted that high-intensity interval training (HIIT), in particular, is "highly efficient" when it comes to reversing many age-related changes.

High intensity interval training involves short bursts of intense aerobic activity within a stretch of more moderate exercise: intermittently sprinting for 30 seconds, for example, in the middle of a moderate-pace jog.

For the National Institutes of Health-funded study, Nair and his colleagues enlisted the help of both men and women from two age groups: The "young" volunteers ranged in age from 18 to 30; "older" volunteers ranged in age between 65 and 80. Next, the researchers divided these participants into three mixed-age groups and assigned each a different supervised exercise training program lasting three months.

The high-intensity interval training training group did three days a week of cycling, with high-intensity bouts sandwiched between low-intensity pedaling, and two days a week of moderately difficult treadmill walking. The strength training group performed repetitions targeting both lower and upper body muscles just two days each week. Finally, the combined training group cycled (less strenuously than the first group) and lifted weights (fewer repetitions than the second group) for a total of five days a week.

There were clear differences, then, in the amount of time different participants spent in the gym.

Before and after each training session, the researchers assessed various aspects of each volunteer's physiology, including body mass index, quantity of lean muscle mass and insulin sensitivity, one indication of diabetes. The researchers also did routine biopsies of each volunteer's thigh muscles and performed a biochemical analysis in order to establish a comprehensive fingerprint of the muscle.

Analyzing the gathered data, Nair and his colleagues found that all forms of exercise improved overall fitness, as measured by cardiorespiration, and increased insulin sensitivity, which translates into a lower likelihood of developing diabetes. Although all exercise helped with musculature, strength training was most effective for building muscle mass and for improving strength, which typically declines with age.

Meanwhile, at the cellular level, high-intensity interval training yielded the biggest benefits.

Specifically, in the HIIT group, younger participants saw a 49% increase in mitochondrial capacity, while older participants saw a 69% increase. Most cells in our bodies contain infrastructure known as mitochondria. These "organelles" -- a mini-version of an organ within a cell -- perform as tiny batteries do, producing much-needed energy.

Interval training also improved volunteers' insulin sensitivity more than other forms of exercise. Drilling down deeper, Nair and his colleagues compared the protein-level data gathered from participants to understand why exercise provided these benefits.

If we think of the cell as a corporate hierarchy, genes (DNA) are the executives issuing orders to their middle managers: messenger RNA. Tasked with transcribing this order, the RNA turns to ribosomes, which perform a supervisory role by linking amino acids in order to assemble protein molecules. Finally, the proteins, cellular work horses, carry out the task originally dictated by the gene.

"Proteins sustain environmental damage and the damaged proteins have to be ... replaced with newly synthesized (produced) proteins," explained Nair in an email. "With aging in sedentary people, production of many protein molecules decline. ... Gradually the quantity of these protein molecules decrease causing functional decline."

Analyzing the muscle biopsies, the researchers discovered that exercise boosts cellular production of mitochondrial proteins and the proteins responsible for muscle growth.

"Exercise training, especially high intensity interval training, enhanced the machinery (ribosomes) to produce proteins, increased the production of proteins and enhanced protein abundance in muscle," Nair said. He said the results also showed that "the substantial increase in mitochondrial function that occurred, especially in the older people, is due to increase in protein abundance of muscle."

In some cases, the high-intensity regimen actually seemed to reverse the age-related decline in both mitochondrial function and muscle-building proteins.

Exercise's ability to transform mitochondria could explain why it benefits our health in so many different ways, according to the authors. Muscle cells, like brain and heart cells, are unusual in that they divide only rarely compared with most cells in the body. Because muscle, brain and heart cells do wear out yet are not easily replaced, the function of all three of these tissues are known to decline with age, noted Nair.

If exercise restores or prevents deterioration of mitochondria and ribosomes in muscle cells, exercise possibly performs the same magic in other tissues, too. And, although it is important simply to understand how exercise impacts the mechanics of cells, these insights may also allow researchers "to develop targeted drugs to achieve some of the benefits that we derive from the exercise in people who cannot exercise," Nair said.

"We cannot have enough studies surrounding this information because of how impactful it is for health," said Trilk, who was not involved in the research. She explained that if younger people boost mitochondrial function when they're young, they would be preventing disease, while for an older population, they would also be preventing disease while maintaining skeletal muscle, which wanes in older age.

"Mitochondrial function is important to almost every cell in the human body," Trilk said. "So when you don't have mitochondrial function or when you have mitochondrial dysfunction, you have dysfunction of cells, so from a molecular standpoint, you start seeing cellular dysfunction years before you start seeing the global effect, which ends up coming out as symptoms of diseases: diabetes, cancers and cardiovascular disease."

"A strength is that they studied males and females," Zierath said, though she noted that the number of participants in each group was "quite small." Still, this is a minor flaw.

"It teases out some of the training regimes that might be leading to greater effects on what they call mitochondrial fitness," she said. Compared with the other two exercise programs, interval training "really had a more robust effect" on the machinery of cells, she said.

"It boosted the proteins that are important for mitochondrial function -- the oxygen powerhouse of the cells," Zierath said. "It reversed many of what we call age-related differences in mitochondrial function and oxidative metabolism."

"Part of what happens with HIIT is, you disturb homeostasis, you exercise at a really high level, and the body needs to cope with that," she explained.

Even though one program had superior effects, "every single exercise protocol they tested had positive effects," said Zierath, who is looking forward to future research in this vein.

"We need to understand even more about how the human body adapts to different exercise regimes and how this can be important for mitigating what we see as sort of aging-related changes that occur in the functionality of muscle and the ability of the muscle to metabolize fuel, sugar and fat," she said.

"Exercise is almost a medicine in some respects," Zierath said. "It's never too late to start exercising."

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Partnership Formed to Advance Bioelectronic Medicine and Cell Therapy – Pharmaceutical Processing

Posted: March 10, 2017 at 12:41 pm

Northwell Health and United Therapeutics announce strategic partnership.

Northwell Health's Feinstein Institute for Medical Research and United Therapeutics Corporation announced today a strategic partnership focused on the application of bioelectronic medicine and cell therapy to cardiology, hypertension and post-transplant tolerance induction.

"We are truly honored to work with the pioneers of these next generation medical technologies," said Martine Rothblatt, PhD, United Therapeutics' Chairman and Chief Executive Officer. "We expect a great fit with our clinical development pipeline in heart failure, pulmonary disease and transplantation."

"Collaboration is the indispensable factor in successful medical research," said Kevin J. Tracey, MD, President and CEO of the Feinstein Institute. "With great partners, you can accomplish great things for science and for patients. United Therapeutics is such a partner, we share their aims and their values, and we could not be more pleased than to join with them in this effort.

Under the strategic partnership, United Therapeutics will fund Northwell's efforts in four research and development tracks, while United Therapeutics will bring the results into clinical development. The two organizations are working toward the goal of initial regulatory approvals within five years.

Two of the research projects will be conducted by the Feinstein Institute's Center for Bioelectronic Medicine (CBEM). The Feinstein Institute is a worldwide leader for the advancement of scientific knowledge and intellectual property for the rapidly emerging field of bioelectronic medicine.

Bioelectronic medicine represents the convergence of three well-established scientific fields: neuroscience, molecular and cell biology, and bioengineering. The Feinstein Institute team, led by Dr. Tracey, a neurosurgeon who pioneered the field, has been working in this area since 1998, and Northwell Health has already invested $75 million in support of the underlying research. As bioelectronic solutions are successfully identified, tested and refined, CBEM will foster the creation of new companies to bring life-changing solutions to market.

United Therapeutics Corporation is a biotechnology company focused on the development and commercialization of products to address the unmet medical needs of patients with chronic and life-threatening conditions.Northwell Health is New York State's largest health care provider with 21 hospitals and over 550 outpatient facilities.The Feinstein Institute for Medical Research is the research arm of Northwell Health.

(Source: EurekAlert!)

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Gluten-Free Diets Actually Increase Risks of Type 2 Diabetes – Newsweek

Posted: March 10, 2017 at 12:40 pm

This article was originally published on The Conversation. Read the original article.

Its hard not to notice that the range of gluten-free foods available in supermarkets has increased massively in recent years. This is partly because the rise in the number of people diagnosed with coeliac disease and gluten sensitivity, and partly because celebrities, such as Gwyneth Paltrow, Miley Cyrus and Victoria Beckham,have praised gluten-free diets. What used to be prescription-only food is now a global health fad. But for how much longer? New research from Harvard University has found a link between gluten-free diets and an increased risk of developing type 2 diabetes.

Gluten is a protein found in cereals such as wheat, rye and barley. It is particularly useful in food production. For example, it gives elasticity to dough, helping it to rise and keep its shape, and providing a chewy texture. Many types of foods may contain gluten, including less obvious ones such as salad dressing, soup and beer.

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Loaves of bread are seen at a Metro cash and carry store in Kiev, Ukraine, August 17, 2016. Gluten-free versions are not healthier than traditional bread. Valentyn Ogirenko/REUTERS

The same protein that is so useful in food production is a nightmare for people with coeliac disease. Coeliac disease is an autoimmune disorder in which the body mistakenly reacts to gluten as if it were a threat to the body. The condition is quite common, affecting one in 100 people, but only a quarter of those who have the disease have been diagnosed.

There is evidence that the popularity of gluten-free diets has surged, even though the incidence of coeliac disease has remained stable. This is potentially due to increasing numbers of people with non-coeliac gluten sensitivity. In these cases, people exhibit some of the symptoms of coelaic disease but without having an immune response. In either case, avoiding gluten in foods is the only reliable way to control symptoms, that may include diarrhoea, abdominal pain and bloating.

Without any evidence for beneficial effects, many people without coeliac disease or gluten sensitivity are now turning to gluten-free diets as a healthy alternative to a normal diet. Supermarkets have reacted to meet this need by stocking ever growing free from ranges. The findings of this recent study, however, suggest that there could be a significant drawback to adopting a gluten-free diet that was not previously known.

What the Harvard group behind this study have reported is that there is an inverse association between gluten intake and type 2 diabetes risk. This means that the less gluten found in a diet, the higher the risk of developing type 2 diabetes.

The data for this exciting finding comes from three separate, large studies thatcollectively included almost 200,000 people. Of those 200,000 people, 15,947 cases of type 2 diabetes were confirmed during the follow-up period. Analysis showed that those who had the highest intake of gluten had an 80 percentlower chance of developing type 2 diabetes compared to those who had the lowest levels of gluten intake.

This study has important implications for those who either have to avoid or choose to avoid gluten in their diet. Type 2 diabetes is a serious condition that affects more than 400m people worldwidea number which is certain to increase for many years to come.

Collectively, diabetes is responsible for around 10 percentof the entire NHS budget and drugs to treat diabetes alone cost almost 1 billion annually. There is no cure for type 2 diabetes and remission is extremely rare. This means that once diagnosed with type 2 diabetes, it is almost impossible to revert back to being healthy.

It is important to note that the data for this study was retrospectively gathered. This allows for very large numbers to be included but relies on food-frequency questionnaires collected every two to four years and the honesty of those recruited to the study. This type of study design is rarely as good as a prospective study where you follow groups of people randomly assigned to either have low- or high-gluten diets over many years. However, prospective studies are expensive to run and its difficult to find enough people willing to take part in them.

While there is some evidence for a link between coeliac disease and type 1 diabetes, this is the first study to show a link between gluten consumption and the risk of type 2 diabetes. This is an important finding. For those who choose a gluten-free diet because they believe it to be healthy, it may be time to reconsider your food choices.

James Brown, Lecturer in Biology and Biomedical Science, Aston University

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Research may provide solutions for the future treatment of diabetes – Science Daily

Posted: March 10, 2017 at 12:40 pm


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Research may provide solutions for the future treatment of diabetes
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In a new study published in the journal Diabetes, researchers at the U of A examined the impact of resveratrol on the community of bacteria, or microbiome, in the gut of obese mice. The team found that feeding resveratrol to obese mice over a period of ...

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Diabetes education program on tap – Holmes County Times Advertiser

Posted: March 10, 2017 at 12:40 pm

Special to The Times

Diabetes self-management is important. People living with a diabetes diagnosis must learn to balance the food they eat, exercise and and have an understanding of the medicines they are prescribed. By managing their diabetes, people can prevent or delay diabetic complications such as blindness and amputations. People managing their diabetes can live long and healthful lives.

The Etowah County Extension Office will offer a Diabetes Empowerment Education Program from 1 p.m. to 2:30 p.m. March 21 through April 25 at the Etowah County Annex Building, 3200-A W. Meighan Blvd.

DEEP sessions include providing information about risk factors for diabetes, complications because of diabetes, health literacy, issues with food (selection, portion sizes, label reading) and living with the diagnosis.

Donna Shanklin, Regional Extension Agent for human nutrition, diet and health, will facilitate the class.

Early registration is advised, as the class size is limited. People do not have to have diabetes to attend.

For more information, call 256-547-7936.

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Sickle Cell Trait May Distort Diabetes Test Results – Northwestern University NewsCenter

Posted: March 10, 2017 at 12:40 pm

Mercedes Carnethon, PhD, associate professor of Preventive Medicine in the Division of Epidemiology, was a co-author of the study, which examined associations between the sickle cell trait and hemoglobin A1C.

A study has found that levels of hemoglobin A1C a biomarker frequently used to diagnose and manage diabetes are significantly lower in African-Americans with sickle cell trait, compared to those without.

The findings suggest the common blood sugar test may be missing diabetes diagnoses in patients with the trait, which affects up to 10 percent of African-Americans. People with sickle cell trait have inherited just one copy of the mutated sickle cell gene, and generally live normal lives without any symptoms of sickle cell disease.

The study, published in the Journal of the American Medical Association, was co-authored by Mercedes Carnethon, PhD, associate professor of Preventive Medicine in the Division of Epidemiology, and Robert Liem, MD, associate professor of Pediatrics in the Division of Hematology, Oncology and Stem Cell Transplantation.

The hemoglobin A1C (HbA1c) test provides a patients average blood glucose over the past three months, based on the amount of glucose that has bonded to hemoglobin in red blood cells. Although the test is commonly used, results can vary for some individuals, especially in those with hemoglobin variants such as sickle cell trait.

In the current, retrospective study of 4,620 African-Americans from two established cohorts, investigators compared HbA1c results between patients with and without sickle cell trait. They discovered that among those with the trait, the mean HbA1c was 5.7 percent, compared to 6.0 in those without even though the two groups showed similar blood glucose levels through other tests.

The test may be underestimating long-term glucose levels in patients with sickle cell trait, the authors noted, and lead to missed opportunities for diabetes diagnosis and intervention.

Robert Liem, MD, associate professor of Pediatrics in the Division of Hematology, Oncology and Stem Cell Transplantation, was also a co-author of the JAMA study.

Clinicians need to be aware that among individuals with sickle cell trait, the use of HbA1c to screen for diabetes or pre-diabetes may be inaccurate, said Liem, also director of the Comprehensive Sickle Cell Program at the Ann & Robert H. Lurie Childrens Hospital of Chicago. These data emphasize another reason why African-Americans need to know their sickle cell trait status.

While the investigators arent certain exactly why HbA1c appears to be less accurate in African-Americans with sickle cell trait, one theory is that red blood cells in those with the trait have a shorter life-span, thus giving glucose less time to build up on hemoglobin molecules.

The CARDIA trial was supported by National Heart, Lung, and Blood Institute (NHLBI) contracts HHSN268201300025C, HHSN268201300026C, HHSN268201300027C, HHSN268201300028C, HHSN268201300029C, and HHSN26820090004; the Intramural Research Program of the National Institute on Aging (NIA), and an intra-agency agreement between NIA and NHLBI (AG0005). The Jackson Heart Study was supported by contracts HHSN268201300046C, HHSN268201300047C, HHSN268201300048C, HHSN268201300049C, and HHSN268201300050C from the NHLBI and the National Institute on Minority Health and Health Disparities (NIMHD). The research was also supported by F31DK105791; Center of Innovation in Long-Term Services and Support, Providence VA Medical Center; K01DK095928; the intramural program of the National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK) and NIMHD; the Intramural Research Program of the National Institutes of Health (NIH); NHLBI grant K08HL125100; R01HL107816.

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Early first menstruation tied to pregnancy diabetes risk – Reuters

Posted: March 10, 2017 at 12:40 pm

(Reuters Health) - Women who got their first period at age 11 or earlier are at higher risk of developing diabetes during pregnancy, a recent Australian study suggests.

Being overweight is known to be a factor in early periods and also in whats known as gestational diabetes, but it did not fully explain the link between the two conditions, the researchers write in the American Journal of Epidemiology.

Diabetes develops in as many as 9 percent of pregnant women in the United States and can carry serious health risks, according to the Centers for Disease Control and Prevention.

Mothers with gestational diabetes are more likely to have high blood pressure and go into premature labor, said lead study author Danielle Schoenaker, a research officer at The University of Queensland.

There are also consequences for the baby, which is more likely to grow faster and be larger at birth, Schoenaker told Reuters Health by email. In the longer term, both mothers and their children are at higher risk of developing type 2 diabetes later in life.

To explore the link between womens age at first menstruation, known as menarche, and their risk of developing gestational diabetes, the study team analyzed data on nearly 5,000 women participating in the larger Australian Longitudinal Study on Womens Health between 2000 and 2012.

The women included in the analysis all reported a live birth during the study and had completed a questionnaire every three to four years, answering questions about when they had their first period and whether they were diagnosed or treated for diabetes during pregnancy. None had type 2 diabetes or a previous history of gestational diabetes at the start of the study.

The average age at which women got their first period was just under 13 years, researchers found.

Women who had their first period at or before age 11 were more likely to have been overweight in childhood, to engage in little physical activity as adults and to currently be overweight or obese.

Overall, 357 women, or about 7.5 percent of the participants, reported being diagnosed with gestational diabetes. These women were also more likely to be overweight or obese and to have a sedentary lifestyle at the beginning of the study.

Women who got their first period before age 11 were 51 percent more likely to develop gestational diabetes, compared with those who started menstruating at age 13.

This was true even after the researchers took into account things that might influence age at menarche or risk for gestational diabetes, including mothers education level, physical activity, previous children, a hormonal condition known as polycystic ovary syndrome and body mass index (BMI), a measure of body fat based on height and weight.

Chronic disease risk, such as risk of type 2 or gestational diabetes may be programmed much earlier in life by exposures occurring during developmentally sensitive periods such as puberty, infancy or even intrauterine life, said Dr. Dana Dabelea, a professor at the University of Colorado Denver who studies gestational diabetes but was not involved in this research.

Interventions to address these health issues may need to start earlier to address the risk of diseases like diabetes, Dabelea said by email.

Women with early menarche are at increased risk of diabetes later in life so they should take additional precautions, especially active lifestyles and maintaining a healthy body weight, to mitigate this increased risk, Dabelea said.

Supporting healthy environments and behaviors from early in life are important strategies, and promoting healthy eating and physical activity should be a priority for young mothers and schools, and for all women throughout their lives, Schoenaker said.

SOURCE: bit.ly/2n66XQ5 American Journal of Epidemiology, online March 5, 2017.

(Reuters Health) - - Pain and other symptoms of chronic sinus problems might cause sufferers to miss work or school but depression is their biggest source of lost productivity, a small study suggests.

Days may get a lot longer for some doctors in training after the group that oversees medical education in the United States rolled back controversial rules limiting the number of hours first-year residents may work.

NFL teams violated federal laws governing prescription drugs, according to a Washington Post story based on sealed court documents contained in a federal lawsuit filed by former players against the league and reviewed by the newspaper.

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Diabetes Education Expert and Registered Dietitian Hope Warshaw Joins WellDoc as Consultant – GlobeNewswire (press release)

Posted: March 10, 2017 at 12:40 pm

March 10, 2017 09:00 ET | Source: WellDoc Inc.

COLUMBIA, Md., March 10, 2017 (GLOBE NEWSWIRE) -- Digital health technology leader, WellDoc, announced today that Hope Warshaw, MMSc, RD, CDE, BC-ADM, a well-known and respected spokesperson who is passionate about improving the clinical and cost effectiveness of diabetes care and education, will join the Company in a consultative role. In this role, she will advise on further engagement with the expanding BlueStar user base, industry advocacy groups and business partners. Additionally, she will provide social media consultation and strategy, utilizing her long-term adoption and engagement with this medium with the diabetes community. BlueStar is WellDocs FDA-cleared, proven digital therapeutic, which provides real-time and timely individualized coaching and support, as well as diabetes educational tools that are actionable and personal.

Ms. Warshaw also recognizes the value novel devices and technologies bring to the evolution of healthcare delivery. She has been an involved member of the diabetes community for nearly four decades, and has been a strong advocate for diabetes educators and education, as well as for individuals living with diabetes.

Hope is a leader and advocate in the field of diabetes education, and we are excited that she is joining us as a consultant. She brings invaluable insight and counsel to our team, which already encompasses individuals who are passionate about providing solutions to improve diabetes care and self-management, said Kevin McRaith, CEO of WellDoc. Like many of us at WellDoc, Hope is focused on advocating for people with diabetes. Her participation alongside the WellDoc team will help ensure our users needs are consistently top-of-mind as we further enhance BlueStar and work to make it broadly available in the marketplace.

Ms. Warshaw is an accomplished author, having written books and articles for publications that are centered around nutrition and diabetes. She is also the Immediate Past President of the American Association of Diabetes Educators (AADE)joining already highly recognized diabetes educators at WellDoc including Malinda Peeples (AADE Past President) and Janice MacLeod (Former AADE Regional Chapter President).

Its an exciting time at WellDoc as the Company focuses on rolling out BlueStar broadly, and there are many opportunities in the area of diabetes management, community building and advocacy, said Ms. Warshaw. WellDoc is leading the charge in digital health to tackle type 2 diabetes by arming individuals with a robust tool to help them manage their condition to achieve significant health outcomes.

About WellDoc WellDoc is the leading digital health company revolutionizing chronic disease management to help transform lives. Our groundbreaking digital health technology is guiding individuals through the complicated journey of living with chronic diseases, with a goal of improving their health and helping them to be more balanced. We are the first digital health company based on a life science business model, and our foundation is built on randomized clinical trials that demonstrate significant clinical outcomes. We have mastered diabetes management by taking an aggressive and innovative approach that utilizes sophisticated logic and precise algorithms, and integrates the most advanced mobile technology, behavioral insight, and diabetes education for those living with type 2 diabetes. Our FDA-cleared, proven digital therapeutic, BlueStar, provides real-time and timely individualized coaching and support, as well as diabetes educational tools that are actionable and personal. Our clinical evidence shows a 1.7 to 2.0 point A1C reduction for adults living with type 2 diabetes who used BlueStar. For more information, visit http://www.WellDoc.com and http://www.BlueStarDiabetes.com.

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R. William Funk Lands New Leader for University of Arizona – Hunt Scanlon Media (press release)

Posted: March 9, 2017 at 6:47 am

March 8, 2017 Just as Elon University gets its president search off the ground with the help of a recruiting boutique, the University of Arizona has selected its 22ndpresident with assistance fromR. William Funk & Associates.

The firm recently presented two finalist candidates: Dr. Robert Robbins, CEO of Texas Medical Center, and Sethuraman Panchanathan, Arizona State Universitys VP of research. Yesterday, the school announced it selected Dr. Robbins to fill its top leadership post. He replaces Ann Weaver Hart, who decided not to seek an extension to her current contract as president.

Recruiting firm founder and president R. William Funk led the assignment. His firm has recruited more presidents to AAU land-grant universities than any other search firm. He expertise extends to recruiting leaders to universities with major health science and medical centers.

Dr. Robbins joined the Texas Medical Center, as president and CEO, in 2012. Since then, he has significantly enhanced its commitment to collaboration, introducing five cross-institutional research initiatives centered on innovation, genomics, regenerative medicine, health policy and clinical research.

Recruitment of Academia Presidents RisingReduced state funding, rising tuition costs, soaring student debt and decreased federal research funding have all contributed to a dramatic rise in the role search firms are playing in the recruitment of university presidents and chancellors.

An internationally recognized cardiac surgeon, Dr. Robbins has focused his clinical efforts on acquired cardiac diseases with a special expertise in the surgical treatment of congestive heart failure and cardiothoracic transplantation. His research work includes the investigation of stem cells for cardiac regeneration, cardiac transplant allograft vasculopathy, bioengineered blood vessels and automated vascular anastomotic devices.

Prior to joining the Texas Medical Center, Dr. Robbins served as professor and chairman of the department of cardiothoracic surgery at Stanford University School of Medicine, founding director of the Stanford Cardiovascular Institute, president of the International Society of Heart and Lung Transplantation, president of the Western Thoracic Surgical Association, president of the American Heart Association Western States Affiliate, president of the Bay Area Society of Thoracic Surgeons, and chair of the American Heart Association Cardiovascular Surgery and Anesthesia Council, among other roles.

He was also elected to the Houston branch of the Dallas Federal Reserve board in 2015; to the board of directors of the Welch Foundation in 2014, where he currently serves as treasurer; and as the president of the American Heart Association Southwest Affiliate in 2016.

Dr. Robbins comprehensive experience as both a visionary leader and highly-respected physician, as well as his evident talent for advancing research, innovation, entrepreneurship and economic development, will serve the University of Arizona and our state well, said Eileen Klein, president of the Arizona board of regents. I look forward to the possibility of collaborating with Dr. Robbins to advance the University of Arizona and achieve aggressive goals for the state of Arizona.

Founded in 1885, the University of Arizona was the first university in theArizona Territory. It includes theBanner University Medical Center Tucson, which operates a separate four-year M.D. collegein downtownPhoenix.Total enrollment is more than 42,100 students, with the largest freshmen class in its history at 8,100 students in 2015. The school offers 334 fields of study leading to bachelors, masters, doctoral, and professional degrees.

Emergence of Physician Leaders

The emergence of physician leaders is part of a trend centered on the unpredictability that both physicians, health systems and academic centers now face. In response, these organizations are taking steps to revise criteria for who they want to lead them forward and what the qualifications incoming leaders should have .. Heres some further reading from Hunt Scanlon Media.

Why Physician Leaders are Now Trending Due to uncertainty and volatility in the U.S. healthcare sector, physician leaders are better positioned to relate, communicate and navigate changes on the horizon. To executive recruiters specializing in the sector, these professionals are the new standard-bearers who bring vision and new ways of thinking.

R. William Funk & Associates is an executive search firm specializing in higher education executive recruitment. The firm, located in Dallas, TX, has conducted more than 400 searches for university and college presidents and chancellors over the last 35 years.

Among the nearly 70 currently sitting presidents Mr. Funk has helped recruit, many are seated at some of the nations most respected universities. Heres a sampling: Michael V. Drake, president of Ohio State University; Max Nikias, president of the University of Southern California; Carol Folt, chancellor of the University of North Carolina-Chapel Hill; Teresa Sullivan, president of the University of Virginia; Bernadette Gray-Little, chancellor of the University of Kansas; Robert Barchi, president of Rutgers University; Mitch Daniels, president of Purdue University; James Clements, president of Clemson University; and G.P. Peterson, president of Georgia Tech.

Academic Search Roundup

A number of institutions of higher education have been replacing top leaders over the past year.Heres a roundup of recent recruiting activity in the education and academic sector, taken from theHunt Scanlon Media newswire archives:

Contributed by Dale M. Zupsansky, Managing Editor, Hunt Scanlon Media

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R. William Funk Lands New Leader for University of Arizona - Hunt Scanlon Media (press release)

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