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Sweden Launches Initiative to Establish Center for Cell and Gene Therapy Research – Genetic Engineering & Biotechnology News

Posted: June 22, 2017 at 11:44 am

Sweden aims to establish a new Center for Advanced Medical Products (CAMP) as part of a SEK 320-million ($36.6-million), 8-year Swedish government initiative to position the country as a leading biologics developer.

Swedish regenerative medicine firm Xintela has been appointed a partner in the 6-year project to establish the CAMP cell and gene therapy research center, with SEK 48 million ($5.5 million) in funding from the countrys innovation agency and research council, Vinnova and Vetenskapsrdet. Xintel said that as one of the CAMP initiative founders, it will work with Swedens universities, research institutes, and with firms including AstraZeneca, GE Healthcare and Pfizer. Xintela will initially act as an advisor for development of the center, but in the longer term expects to benefit from emerging R&D.

It is gratifying that the Swedish government, Vinnova and Vetenskapsrdet acknowledge the huge potential of cell and gene therapy and the strong position that Sweden has in this research field,commented Xintela CEO Evy Lundgren-kerlund. Xintela is one of the companies in Sweden with large development potential in cell therapy, which makes us a natural partner for this project.

In the short term CAMP aims to establish itself as an internationally recognised center for R&D, innovation and clinical practice, and to promote industrial growth and SMEs. Longer-term goals include attracting investment from the global pharmaceutical and biotech sectors.

Xintela is exploiting its XINMARK protein marker technology and XACT (Xintela assay for cell therapy) assay platform to develop an allogeneic mesenchymal stem cell-based therapy for repairing cartilage damage in osteoarthritis, and to progress a tumor-targeting antibody treatment for glioblastoma.

Last month the firm established a collaboration with Germany-based CO.DON, which develops autologous cell therapies for cartilage repair. The firms will work together on the development of Xintelas markers both for a next generation CO.DN cell therapy program and for Xintelas cartilage repair cell therapy product.

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Cell Medica boosts manufacturing capacity in cell therapy deal – BioPharma Dive

Posted: June 22, 2017 at 11:44 am

Dive Brief:

Even more than traditional drug development, manufacturing is a crucial step in the development of complex therapeutics like cell therapies. As the field evolves, it will likely be a difference maker between success and setback. Such focus on production and logistics can be see in the attention paid to the processes set up by the more advanced CAR-T developers like Kite Pharma, Novartis and Juno Therapeutics.

With this deal, Cell Medica has seized on an opportunity to gain access to an existing GMP facility, taking a short cut to support further development and potential commercialization of the WT1-TCR therapy. More cell therapy products might also be produced at the site in the future, Cell Medica said.

Catapult Therapy TCR was created by CGT Catapult, UCL Business and Imperial Innovations the technology transfer arms of University College London and Imperial College, London in order to develop the WT1-TCR cell therapy.

By acquiring Catapult Therapy TCR, Cell Medica can also integrate WT1-TCR cell therapy into its Dominant TCR platform technology. This has potential to improve efficacy, Cell Medica believes, and to expand use of the therapeutic from its existing focus on blood cancers to hard-to-treat solid tumors such as mesothelioma and ovarian cancer.

Cell Medica recently upped its financial firepower,closinga 60 million ($75.9 million) Series C investor round in March 2017 to further develop its cell-based cancer immunotherapies.

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Langer-backed Sigilon sets sail with $23M and new ‘living’ cell … – Endpoints News

Posted: June 22, 2017 at 11:44 am

While Flagship Pioneering was unwrapping a huge $120 million round for Rubius this morning, the busy venture group also launched a biotech on a mission to create a new type of encapsulated cell therapy.

Turning to two scientific founders MITs Daniel Anderson and the prolific Robert Langer the discovery group at Flagship has been working on permeable biomaterials that are designed to implant cells in tissue to deliver proteins in a sustained fashion, without triggering fibrosis.

Paul Wotton, CEO, Sigilon

Researchers have been refining this tech in Flagships VentureLabs for the past two years, and now they are pursuing it at Sigilon Therapeutics with a $23.5 million A round.

Imagine the potential of a living therapeutic that could be implanted in the body and manufacture and release therapeutic proteins at steady levels for long periods of time, avoiding the critical limitations of intermittent infusion required with current therapies, said CEO Paul Wotton.

Flagship has pulled together another veteran team for this new player.

Wotton ran Ocata until it was bought out by Astellas. This rest of the team includes chief technology officer David Peritt, a Pfizer vet, and chief strategyofficer and head of operations Devyn Smith, who was previously head of operations and strategy for the medicinal sciences division of worldwide R&D at Pfizer. James Watson, chief business officer of Sigilon Therapeutics, previously served as CBO at Alvine Pharmaceuticals.

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ImmunoCellular Therapeutics halts brain cancer cell therapy trial due to lack of cash – BioPharma-Reporter.com

Posted: June 22, 2017 at 11:44 am

ImmunoCellular Therapeutics Ltd has halted a Phase III trial of its brain cancer cell therapy ICT-107 due to a lack of funds and is looking for a buyer or partner for the programme.

The Los Angeles, US-based biotech announced the move on June 21, explaining it is unable at this time to secure sufficient additional financial resources to complete the phase III registration trial of ICT-107.

ImmunoCellular said it is looking for a partner or buyer for the programme adding that the suspension of the phase III registration trial of ICT-107 is expected to reduce the amount of cash used in the Companys operations.

ICT-107 is a dendritic cell (DC) vaccine designed to activate a patients immune system to target six different antigens associated with glioblastoma multiforme, a form of brain cancer.

ThePhase III trial is being conducted at sites in the US, Austria and Canada.

The halt comes weeks after ImmunoCellular Therapeutics signalled its intention to raise funds to allow it to continue the study.

R&D costs

According to a first quarter filing ,ImmunoCellular Therapeutics has cash reserves of $5.3m (4.68m), which is just under half of what it had in reserve this time last year.

The document also revealed the firm spent $5.4m in the quarter, the majority of which was used for R&D.

Supplies of ICT-107 for the trial were produced by Netherlands-based contractor PharmaCell, under an agreement announced in 2015 , andCaladrius subsidiary PCT under an deal signed the same year.

Financial details of the contracts have not been disclosed, althoughImmunoCellular Therapeutics does state in its Q1 filing that it is paying PharmaCell for "manufacturing services."

Similarly, while ImmunoCellular Therapeutics does not provide specifics about itsdeal withPCT, it does is say the contractoris providing manufacturing services for the Phase III ICT-107 trial and for a Phase 1 study of ICT-121, a second cell therapy candidate.

ImmunoCellular Therapeutics is alsopaying PCT monthly fees for the use of a controlled environment room and personnel performing the services.

PharmaCell was acquired by Swiss life sciences supplier Lonza last week .

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Birdseed Turned Superfood May Help Curb India’s Diabetes Scourge – Bloomberg

Posted: June 22, 2017 at 11:43 am

Podiatrist Vinaya A.S. has bumped across southern India in a bus-turned mobile clinic for 17 years, going village to village checking feet for the ulcer-causing effects of diabetes. These days, her key to staving off limb amputations comes down to one thing: food.

Millets, to be precise. The ancient grains were a staple in India for thousands of years, but largely spurned since a so-called Green Revolution last century led to cheaper, more abundant supplies of refined rice and wheat flour that can bolster blood-sugar. Now a surge in type-2 diabetes is pushing doctors and government officials to recommend a return towholegrains, like ragi or finger millet, that healthfully sustained previous generations.

Vinaya A.S. with patients at a mobile clinic on the outskirts of Bengaluru

Photographer: Dhiraj Singh/Bloomberg

Food is your medicine you need to eat right, Vinaya, 48, told a group of villagers inDoddaballapur, on the outskirts of Bangalore, last month. Bring the fiber-rich ragi back to your plates, along with fruits and vegetables.

Healthy food choices are becoming critical in India, where diabetes is ripping through the population with deadly consequences. The number of adults living with the disease has risen more than five fold since 1980, though more than half of sufferers arent aware they have it. Left uncontrolled, high blood-sugar levels can damage organs and tissues, including the nerves and blood vessels in the feet, making them susceptible to injuries that fail to heal and eventually turn gangrenous. When that happens, amputations can be life-saving.

Onset of diabetes occurs about a decade earlier in Indians than in North Americans and Europeans. About a third of Indians with the obesity-linked disease are thin, suggesting that too many calories isnt the only diet-related problem, saidK. Srinath Reddy, president of the Public Health Foundation of India.

Modern Indian meals lack fiber, which protects against diabetes, and are high in white rice and other refined carbohydrates, like wheat flour, used to make poori, or deep-fried bread, and samosas, a deep-fried, vegetable-containing pastry. Such energy-dense foods cause spikes in blood-sugar that weaken the bodys response to insulin and, when eaten regularly, can eventually lead to type-2 diabetes.

Traditional staples, like millets, have been replaced by polished rice and refined wheat flour even in rural areas, said Reddy, a cardiologist who is a past president of the World Heart Federation. Traditional Indian diets, not in vogue now, had a protective effect against diabetes.

There were 69.2 million adults living with diabetes in India in 2015, according to the International Diabetes Federation. Complications such as stroke, kidney failure and blood-poisoning from festering sores kill more than 1 million annually and the country will have 123.5 million diabetics by 2040 unless trends in overweight and obesity are curbed, the Brussels-based group predicts.

Health awareness is motivating Indias urban upper crust to seek out so-called superfoods, such as steel-cut oats and quinoa, a type of edible seed from South America, but millets an umbrella term for many small seeded grains have been slower to catch on, said Krishna Byregowda, the agriculture minister of Karnataka state.

Why are we forgetting our own superfoods while buying and adopting imported oats and quinoa? he asked a crowd at a three-day Organics and Millets National Trade Fair in the state capital, Bangalore, last month.

Customers at Vaathsalya Millet Cafe in Bengaluru.

Photographer: Dhiraj Singh/Bloomberg

Byregowda is spearheading a campaign involving chefs, nutritionists, doctors and food businesses to bolster demand for a grain he grew up eating as ragi mudde finger-millet flour cooked and shaped into soft mounds and served with leafy greens in a spiced gravy.

His farmer-ancestors grew it not just for its nutritional benefits: the crop needs a third of the rainfall of rice. Yet, millet and sorghum production have declined by a combined 51 percent in India and rice and wheat output has almost quadrupled since the 1960s, when a Green Revolution introduced modern seeds, chemicals and irrigation to boost harvests and stave off hunger.

Drought-induced crop failures in recent years in southern India have convinced the 44-year-old American University graduate of the need to return to growing millet.

In these times of climate change, it made sense to encourage farmers to switch to climate-smart crops rather than cultivate the water-intensive rice, Byregowda said in an interview. The post-Green Revolution planning left millet farmers, like my family, in the lurch.

The government of the neighboring southern state of Tamil Nadu has allocated 8 billion rupees ($124 million) to subsidize the cultivation of millets and pulses, and restaurants in the capital, Chennai, are catering for a growing appetite for millets. P. Sathiya Moorthi sells biscuits, biscotti and sweets from the grain to customers working at the local Hyundai Motor India Ltd. factory and Cognizant Technology Solutions Corp.s offices.

In Hyderabad in Telangana state, Narayana Peesapaty and his wife Pradnya Keskar have found another culinary use for the grain: edible spoons costing a few cents apiece.

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While millets have gained some international popularity thanks to pop starMadonna and chef Joanne Weir, they are only just gaining traction among health-conscious consumers in the U.S., according to Amrita Hazra. The India-born researcher is part of the Millet Project, a two-year-old University of California, Berkeley program thats working with Californian farmers, chefs and retailers to rediscover the traditions of cultivating and consuming millets.

Ancient grains are making a comeback in peoples diet, and very slowly into the fields, Hazra said.

A farmer cuts millet on the outskirt of Bengaluru.

Photographer: Dhiraj Singh/Bloomberg

A reviewin 2014 of sorghum and millets used as livestock fodder and birdseed in some countries found they contain health-enhancing properties, though more human clinical trials are needed to assess their direct dietary benefits. They contain more fiber, more micro-nutrients and probably have a smaller blood-sugar impact than refined carbohydrates, said Jennie Brand-Miller, professor of human nutrition at the University of Sydney.

As long as the millets are prepared and consumed in traditional ways, I think this is a good suggestion, said Brand-Miller, who is internationally recognized for her research on the bodys absorption of carbohydrates. To maximize the health benefits of millets, consumers need to resist the urge to grind and refine them.

For podiatrist Vinaya, they are much healthier alternative to the fast-foods, sweetened soda drinks and rice more of her patients are consuming. Of the 60 people who turned up for last months free clinicin which her team checks blood flow to the foot, nerve sensitivity and blood-glucose, 27 were found to have diabetes, she said.

Unchecked, that can lead to foot sores that ulcerate. Her hospital in Bangalore does 30 to 35 foot amputations a month because of diabetes. In at least three of these cases, an entire lower limb needs to be amputated to prevent gangrene causing lethal blood poisoning, or sepsis.

Checking for diabetes at a mobile clinic.

Photographer: Dhiraj Singh/Bloomberg

To London-trained Vinaya, who runs the diabetic foot clinic at Bhagwan Mahaveer Jain Hospital, the link between diet and lifestyle changes and the rising incidence of diabetes has strengthened based on data her team has gathered from 2.4 million people in 350,000 households across 1,700 villages the largest such diabetes study in the world.

Even physically active, slender farmers in their 30s and 40s are being afflicted with the disease in India. She tells them how to replace the rice in their favorite dosa pancakes and idli savory cakes with millets. On her repeat rounds to the rural camps, villagers gather round to titter, Doctor-madam has come to conduct cooking classes.

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Many diabetes patients produce some insulin – Medical Xpress

Posted: June 22, 2017 at 11:43 am

June 22, 2017 by Elin Bckstrm High-resolution model of six insulin molecules assembled in a hexamer. Credit: Isaac Yonemoto/Wikipedia

Some insulin is still produced in almost half of patients that have had type 1 diabetes for more than ten years. The study conducted by researchers at Uppsala University in Sweden has now been published online by the medical journal Diabetes Care.

Type 1 diabetes, a chronic disease mainly debuting during childhood or adolescence, has previously been considered to result in full loss of the patients' insulin production. However, by the use of sophisticated insulin assays that have been introduced in recent years, this has now been shown to not be true in all cases.

In a study from Uppsala University more than one hundred type 1 diabetes patients at Uppsala University Hospital have been investigated. Almost half of the adult patients that have had type 1 diabetes for at least ten years still produced some insulin.

The study showed striking differences in the immune system between patients with full loss of their insulin production and patients that still produced some insulin. Patients with remaining insulin production had much higher blood levels of interleukin-35, a recently discovered anti inflammatory signal protein of the immune system. They also had many more immune cells that produce interleukin-35 and dampen immune attacks.

It is still not known if the patients had higher levels of interleukin-35 already at the onset of their disease, or if those levels had increased over the years, stopping immune attacks towards the insulin producing cells as a result. A previous study by the same research group has shown that both patients newly diagnosed for type 1 diabetes and patients with long-standing disease on average have lower levels of interleukin-35 when compared to healthy individuals. The previous study also showed that diabetes development could be prevented, and that fully developed diabetes could be reversed, through interleukin-35 treatment in animal models with type 1 diabetes.

The results of the present study in Diabetes Care may increase the interest to develop interleukin-35 into a drug for the treatment of type 1 diabetes. The discovery that almost half of the patients with type 1 diabetes have some remaining insulin production also makes it attractive to let the patients test new treatments that can induce regeneration of their remaining insulin producing cells. Such a study has now been initiated at Uppsala University Hospital.

Explore further: Mislocalized calcium channel causes insulin secretion defect in diabetes

More information: Daniel Espes et al. Increased Interleukin-35 Levels in Patients With Type 1 Diabetes With Remaining C-Peptide, Diabetes Care (2017). DOI: 10.2337/dc16-2121

Journal reference: Diabetes Care

Provided by: Uppsala University

Researchers from Uppsala University have studied beta cells of type-2 diabetic donors, and find that a mislocalized calcium channel contributes to the failed insulin secretion associated with the disease.

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A plants-based cure for diabetes – Longview Daily News

Posted: June 22, 2017 at 11:43 am

TOLEDO As a former Type II diabetic, Norm Baird admits that he used to abuse dairy. For years, the retired engineer enjoyed eggs and loved yogurt. He used to cut off little pieces of cheese to nibble on as he passed through his kitchen. His diet resembled a typical Americans: high in sugar, processed foods, meat and scant on vegetables.

But the silver-haired Toledo resident and cancer survivor no longer looks like a dairy abuser, having shed about 65 pounds and his diabetes diagnosis after adopting a plants-based diet in February 2016.

The 72-year-old is one of a small but growing number of people who have opted to go vegan or near-vegan as a first-line treatment for chronic weight- and diet-related illnesses such diabetes.

With more than two-thirds of American adults considered to be overweight or obese, diabetes is one of the leading causes of death in the country. The number of people with Type II diabetes is expected to double by 2030, according to the Centers for Disease Control and Prevention. In Washington, Cowlitz County ranks 10th among the states 39 counties in prevalence of the disease. About 13 percent of Cowlitz residents are living with the condition, according to a chronic disease report by the Washington State Department of Health. Thats more than a third higher than the statewide average of 9 percent.

Things first started to change for Baird when he was diagnosed with cancer, and they snowballed from there.

As you get older it feels like doctors have two columns of health conditions, Baird said. Every year that passes it seems they move another one over from the list of possible conditions into the column of ones you have.

During his cancer treatment Baird started injecting himself with insulin to counteract a steroid he was taking that drove up his blood sugar.

After chemotherapy, Baird stopped taking his insulin until he was diagnosed with Type II diabetes. At a follow-up visit, Dr. Robert Ellis, an oncologist at the Kaiser Permanente Clinic in Longview, proposed the idea of adopting a vegetarian diet.

Ellis is a passionate champion of plants-based eating. In an interview, he noted that the top health conditions in the United States cancer, heart disease and obesity are all preventable and treatable through diet and nutrition.

One of the first things I go over with patients is their diet, he said. If you had a high-performance car and I told you that it needs high performance gas, would you really drive to Costco and put that crappy gas in your car?

In 2013 Kaiser issued a nutritional update for physicians urging health care providers to recommend plants-based diets to patients. Its now one of the most-cited scholarly journal articles ever published on the subject.

As one of the nations largest not-for-profit health plans and the largest managed care agency in the United States, with 10.2 million members, its in Kaisers interest to keep its patients healthy.

Ellis said he has serious discussions about diet with about 80 percent of his patients. Of that number, about 40 percent to 50 percent say theyre actually going to change the way they eat, he said. And the percentage that go full crazy on you and adopt a vegan diet like Bairds is around 10 percent to 20 percent, he said.

Were not hiding something, Ellis said. This isnt quantum physics.

A person can dramatically lower their blood sugar by eating plants and whole foods while avoiding meat and other animal products that are high in fat, he said.

Some of the biggest impediments to adopting this kind of diet are socioeconomic. Not having much money for food and living far away from grocery stores that sell quality produce can make it hard for people to commit, Ellis said.

But Baird is one of the few who has bought into the eating program. With a referral from his primary physician in hand, he next met with Andrea Ferreiro, a Portland-based Kaiser nutritionist who specializes in healthy eating plans.

Norm was kind of the ideal patient, Ferreiro said in an interview. Norms an engineer and hes pretty analytical, so we just kind of told him exactly what to do and how to do it and he implemented it precisely.

Baird proceeded to cut out all meat, dairy and other animal products from his meals. In a mere five weeks, his A1C score a measure of blood sugar dropped to 6.1, placing him below the 6.5 or above score used to classify a person as diabetic.

Baird was able to stop injecting himself with the insulin he had been using twice daily for two years. He also stopped taking an oral prescription medication for diabetes and went from monitoring his blood sugar four times a day to just two.

Its exceptional its a really big deal, Ferreiro said of Bairds progress.

Ellis said he had to revise Bairds medication regimen to compensate for the chemistry changes that can occur within the body after just a few days of vegetarian meals.

The rest of Bairds follow-up visits were conducted by phone by one of Ferrieros assistants, and he still receives a weekly call to review his numbers.

They call once a week to make sure nothings out of whack, he said.

Baird said he still fixes himself a plate with some meat on special occasions like Christmas and Thanksgiving but only one.

No seconds and no leftovers, he said.

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Regenexx: injections soon will replace orthopedic surgery – Broomfield Enterprise

Posted: June 21, 2017 at 10:46 am

Dr. John Schultz gives an injection of bone marrow derived stem cells into the knee of patient Steve Brink from Washington state at the Regenexx offices in Broomfield on Monday. Brink was in to have work done on a sports injury on his knee made worse by surgery. The company isolates platelets and stem cells to re inject them into patients to stimulate tissue healing in joints, ligaments and tendons. (Paul Aiken / Staff Photographer)

Eric Beck removes plasma from a centrifuge at the Regenexx processing lab at their offices in Broomfield on Monday. The company isolates platelets and stem cells to re inject them into patients to stimulate tissue healing in joints, ligaments and tendons. (Paul Aiken / Staff Photographer)

Broomfield physician Christopher Centeno has a bold prediction about one of the fastest-growing fields of medicine: Orthopedic surgery.

"Most of what we currently call orthopedic surgery will, in the next 10-20 years, be in the dust bin of history," he said. "Thirty years from now, cutting people open and drilling holes will be considered barbaric."

Like many men with big claims, Centeno isn't exactly unbiased. He is one-half of the Centeno-Schultz Clinic in Broomfield, and co-founder and owner of Regenexx, a company specializing in regenerative medicine through the use of biologics. Regenexx treatments include injection of patient's own stem cells and platelet-rich plasma (PRP) to encourage healing of tendons, joints and muscles.

Seventy percent of orthopedic issues currently treated with surgery could instead be handled using regenerative methods, Centeno said. Patients come to him from all over the country to repair torn ACL and rotator cuffs or find relief from osteoarthritis and sciatica.

Medical professionals are increasingly buying in to Centeno's ideals. Regenexx has licensed its technology to 48 clinics in the U.S. and abroad since 2012. And a classroom/lab at the Broomfield headquarters has instructed hundreds of doctors to administer the injections.

Even orthopedic surgeons who stand to lose out if scalpels can be replaced by syringes are increasingly seeing the benefits of non-invasive, regenerative therapies. The American Academy of Orthopaedic Surgeons in 2014 published an interview titled "Are Biologics the Future of Orthopaedics?"

Dr. Adam W. Anz provided the answer: "Biologics represent the next frontier in orthopaedics," he told AAOS. "I believe biologics will revolutionize the next 30 years."

There is certainly promise in stem cells and PRP, agreed ortho surgeon Eric McCarty, the chief of sports medicine and shoulder surgery for the University of Colorado School of Medicine's orthopedics department, and also director of sports medicine for CU athletics.

McCarty has used some biologic treatments on student athletes. He himself received an injection of PRP to ease the pain of his tennis elbow and prevent the need for surgery. But the treatments are usually preventive, or additive, to surgical options.

"In an active town (like) Boulder, people hurt themselves skiing or biking, and fixing an ACL or rotator cuff is not managed with biologics," he said. "What we're looking at now is how does that help speed up the process of healing or prevent osteoarthritis or the need for surgery."

McCarty cautions patients about clinics that promise healing. There are "a lot of claims about stem cells," he said, but not "much science to back it up."

"They have to understand what they're getting at this point and time. I caution people to be careful of how they spend their money."

The procedures are pricey. An ACL repair, for example, costs $6,000-$8,000 at Regenexx. A surgical procedure in a hospital would cost north of $10,000, McCarty said, but the procedure is covered by most insurers, unlike regenerative therapies.

Adoption among insurers has been slow, Centeno admits. But he disagrees with McCarty on the pace of change. The shift is happening now, he said.

"Twenty years ago, we were the only people in the country doing this. Then five years ago, 100 people were doing it. In the last 24 months, that has probably climbed to 1,000. It is spreading like wildfire as we speak."

Centeno doesn't concern himself with naysayers in the medical or insurance fields, instead keeping his focus on spreading the word and training ever more physicians in the ways of Regenexx.

"It's like anything in medicine," he said. "You've gotta push that rock uphill."

Shay Castle: 303-473-1626, castles@dailycamera.com or twitter.com/shayshinecastle

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What happens when scientists leave their labs to experiment with politics? – Los Angeles Times

Posted: June 21, 2017 at 10:46 am

June 15, 2017, 6:00 a.m.

Washington, D.C.

They have built careers isolating cells, designing integrated circuits and mastering computer languages. Now they are knocking on doors, being interviewed on TV and asking perfect strangers to give them money.

Across the country, scientists card-carrying members of an elite that prizes expertise are exiting their ivory towers to enter the political fray.Theres the cancer researcher from Mississippi, the integrated circuit designer from New York, the physician from Utah and the stem cell biologist from Southern California, among dozensof others.

Its a move that appears to defy the first principle of their profession: logic. Unlike a law degree, a Ph.D. does not provide a well-worn path to politics. And while 79% of Americans believe that science has made life easier, their esteem for the scientific enterprise has been on a steady decline, according to the Pew Research Center.

But even amidst signs that science is losing its power to persuade, a new crop of office-seekers is anything but discouraged. In districts blue and red, working scientists are putting two hypotheses to the test.

First: Their facility with facts and data will make them better policymakers than the politicians currently in office.

Second: Their professions reputation for pragmatism and problem-solving will mobilize and unify voters around them.

Our skill set works: We analyze complex information and make it understandable to people, said Dr. Kathie Allen, a family physician who is running for the Utah congressional seat soon to be vacatedby Republican firebrand Jason E. Chaffetz.

People are really tired of falsehoods, she added. With careers grounded in facts and evidence, she said, scientists offer a compelling alternative for voters fed up with career politicians.

That may sound like the wishful thinking of a political newbie, but some longtime campaign strategists agree.

Joe Trippi, who has worked with Ted Kennedy, John Edwards, Jerry Brown and Howard Dean, said scientists werea double threat in the current political moment.

For voters dismayed by the Trump administrations attacks on climate science and proposals to slash federal funding for biomedical research, a scientist-turned-office-seeker offers a direct antidote to the status quo. And for voters craving an alternative to politics as usual, these unconventional candidates feed into a compelling insurgent narrative.

If youre a scientist, your background is perfect for the time were in, Trippi said.

The ranks of scientists, engineers and medical professionals in Congress has grown from 24 two decades ago to 33 today. But those members are still dwarfed bypeople with backgrounds in law or business, who fill roughly three-quarters of the 535 seats in the House and Senate, according to the Congressional Research Service.

Theres no official tally of how many scientists have run for office. But anecdotal evidence for a surge in candidates is widespread.

Rush Holt, a plasma physicist who served eight terms in the U.S. House of Representatives before retiring in 2014, has seen it firsthand.People who were once wary of political participation have been pushed off the sidelines and into the public square by a sense that science is too relevant and important to be downgraded or ignored, he said.

Over the years, Holt has counseled a thin trickle of scientists pondering a run for public office. Now, he said, its a stampede.

Im getting more interest by far than Ive gotten in previous election cycles, said Holt, who is now president of the American Assn. for the Advancement of Science. He calls it a remarkable moment.

Like Allen and Holt, many of the scientists eyeing a run for office are Democrats, keen to challenge a president who has questioned the value of vaccines and dismissed global warming as a Chinese hoax.Whether they come from chemistry labs or radio astronomy observatories, they can channel the frustration and anger that prompted more than 1 million people to March for Science this spring.

But theyre quick to point out theyre not ideologues.

Is there a better way to create policy? asked Patricia Zornio, a biomedical researcher at Stanford University who is contemplating a 2020 challenge to Colorado Sen. Cory Gardner, a Republican. You take large amounts of information and distill it, and come up with a conclusion. It has nothing to do with partisanship.

If that faith in science sounds like it could easily veer toward sanctimonious bromides, the would-be candidates have been warned.

We are so naive as scientists, said South Miami Mayor Philip Stoddard, who also happens to be an expert on the evolution of animal communication on the faculty of Florida International University. We think the truth carries and that science always matters. The corrective, he told a group of prospective candidates recently, is to find a coach that knows more about the business than you do.

Since shortly after the inauguration of President Trump, training sessions and webinars have cropped up to coach Democratic office-seekers with a scientific bent. Among the most visible have been sessions organized by 314 Action (314 refers to the value of pi).

So far, the group has had inquiries from roughly 6,000 scientists and science advocates, from all 50 states. Close to 100 of them gathered in Washington, D.C., two days before the March for Science for the biggest training event to date.

There, would-be candidates learned how to craft a message (make science local), recruit and organize an army of volunteers (present it as an opportunity)and canvas voters (bring dog biscuits!). They learned what to wear, how to sit for a TV interview, and how to hit up potential donors.

Among the scientist dos: Introduce yourself as a different kind of politician. Mine data to find and target your districts voters. Change things up if your message isnt working. (Youre an experimentalist! Stoddardreminded them.)

Scientist donts included reading your curriculum vitae, using PowerPoint slidesand appending footnotes to position papers. (Footnotes! cried political communications specialist Chris Jahnke, who has coached Hillary Clinton and Michelle Obama. God bless you, please dont!)

Do scientists have an advantage in the current political environment, with the Democratic Party awash in volunteers eager to run against the GOP?

Absolutely, Democratic campaign strategist Martha McKennatold a 314 Action session. Voters think politicians talk and nothing gets done, she said. As scientists, you find solutions.

Its a message that resonates with Patrick Madden, a professor of computer science at Binghamton University in New York. In May, he announced a bid to challenge Rep. Claudia Tenney (R-N.Y.) in New Yorks 22ndCongressional District.

Madden holds up his cellphone, a device more powerful than the computer that sent men to the moon. His work on integrated circuits has helped make such devices faster, better and more fun to own.

Were not full of crap, he said. Things like this got better because we make stuff thats real. If we were a pack of liars, the jig would be up.

Madden calls himself a firm believer in the scientific method, the engineering mind-set.

These principles of being honest, being truthful and looking for solutions: its a radical idea, he said. But I think we ought to try it.

Originally posted here:
What happens when scientists leave their labs to experiment with politics? - Los Angeles Times

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Tackling hard-to-treat cancers from every angle – Medical Xpress

Posted: June 21, 2017 at 10:45 am

June 21, 2017

Improving the quality and quantity of research into cancers with the poorest survival rates remains a key priority across all aspects of our research activity from funding breakthroughs in biology, to growing a sustainable community of world-leading researchers.

In the three years since we pledged to increase research funding in cancers of unmet need, we have increased spend in our four identified priority cancers lung, pancreatic, oesophageal and brain. We invested 85.8m across these four disease types in 2016/17, more than doubling our spend since 2013/14.

But our ambitions in tackling these hard-to-treat diseases go far beyond funding research, as each of these intractable diseases has its own unique challenges.

We have been working closely with the community to determine the critical scientific questions or identify gaps in infrastructure standing in the way of progress, with a view to taking proactive, bespoke approaches to each disease type. Activities have ranged from specialist symposia and conferences bringing the research community in these fields together, to looking at ways to fund large-scale international research initiatives in partnership with others. A second symposium on oesophageal cancer took place in spring 2017, followed by a workshop with key members of the international research community to identify priority areas for research. And with the long-term view of building a sustainable community working on each disease, it is encouraging that this year we have seen an increase in the number of career development awards focused on the unmet need cancers, particularly in brain tumours.

In lung cancer, a notable highlight this year is a collaboration through our partnership with the US Cancer Moonshot Initiative which will see Professor Caroline Dive at our Manchester Institute and Professor Peter Kuhn's team at the University of Southern California apply their combined expertise and technology in circulating tumour cell analysis to study the blood of patients with early-stage lung (and bowel) cancer, to see if they can identify those who will relapse.

Here, we focus on two of the toughest cancers pancreatic and brain and share some of the exciting investments, initiatives and new research we're funding in the UK and internationally.

Tackling pancreatic cancer

Every year around 9,500 people are diagnosed with pancreatic cancer in the UK; only 1% survive their disease for 10 years or more. Surgery can significantly extend overall survival, but only 1015% of patients are diagnosed early enough for surgery to even be an option. Other treatments only prolong life by a matter of months. Now the 11th most common cancer in the UK, new approaches are urgently needed to combat this devastating disease.

A new era of precision

As for all cancers, molecular stratification of tumours is key to our basic understanding of pancreatic ductal adenocarcinoma (PDAC), and its prognosis and treatment. Professor Andrew Biankin, at the University of Glasgow, is a leader in molecular analysis and next generation sequencing of pancreatic cancers: besides confirming known mutations, his work has uncovered new genes and pathways mutated at lower frequencies, some of which are potential therapeutic targets. He is lead investigator on PRECISION-Panc, an ambitious programme of research that seeks to uncover the molecular profile of individual patients with pancreatic cancer, to learn more about the disease and to facilitate patients entering clinical trials for treatments that match their tumour biology. CRUK is investing 10m in this flagship initiative, to date our largest stand-alone investment in pancreatic cancer research. He also co-chairs Precision Promise, a sister programme to PRECISION-Panc, that will bring precision medicine to pancreatic cancer patients in the US.

Andrew's aim is to pull together a knowledge bank about PDAC, taking in information not just from the US and the UK, but from many other partners around the world. His hope is that, eventually, a newly-diagnosed patient's tumour characteristics can be run against the knowledge bank database, enabling the best treatment option to be offered as part of a clinical trial: "There'll be a day in the future, if we harmonise and align our methodology, that we can address specific issues through running international multicentre studies", he says, "but for that, we'll have to better integrate research with the clinic. We want a patient to know when experimental medicine is the best option for them, and make sure that they have trials to enter."

Targeting the molecular basis of pancreatic cancer

From the work of Andrew and others, we know that the KRAS oncogene is mutated in 80100% of PDACs, and has a frequent partner in crime: the MYC oncogene. Amplification of MYC in PDAC makes the tumours more aggressive, and, as in many other tumour types, MYC expression is critical for KRAS-driven tumour maintenance. Recently, it's been shown that MYC regulates so-called super-enhancers clusters of DNAprotein complexes that coordinate the expression of large banks of genes critical for specifying cell identity and behaviour. This may be how MYC can reprogramme cells at the flick of a switch. Because of its importance, MYC is one of the lead molecules being studied by the Pancreatic Cancer Dream Team, funded through a partnership between CRUK, Stand Up To Cancer (SU2C) and the US Lustgarten Foundation.

Led by Professor Gerard Evan at the University of Cambridge, Professor Daniel von Hoff at the Translational Genomics Research Institute in Arizona and Professor Ronald Evans at the Salk Institute for Biological Sciences in California, the Pancreatic Cancer Dream Team aims to map super-enhancer 'hotspots' in pancreatic cancers. They hope to understand how MYC 'hacks' into the normal regenerative programme of the pancreas, driving relentless proliferation and, eventually, pancreatic cancer. In particular, they are studying how MYC engages with the super-enhancers in pancreas cancer cells and how disabling that interaction triggers regression of pancreatic cancers. This knowledge will inform the use of super-enhancer-targeted drugs, some of which are already available, and has the potential to enhance responses to chemo- and immunotherapy.

One year in, Gerard has found the collaboration immensely rewarding: "The notion of looking at transcriptional changes would probably not have been something we'd have gone for in our own lab, as we didn't have the necessary expertise," he says, "so this was, and is, a game-changing opportunity for us and, we hope, for pancreatic cancer patients."

Targeting the microenvironment

One of the hallmarks of PDAC is extensive desmoplasia the formation of rigid fibrotic tissue or extracellular matrix, wrapped like a corset around the tumour. In some PDACs, as much as 90% of the tumour mass comprises non-tumour cells, and this stromal tissue shapes the tumour, both literally and metaphorically, toughening it up by starving it of oxygen and nutrients, and impeding treatment by reducing the access of drugs and immune cells.

These stromal and tumour cells talk extensively to each other. Dr Claus Jrgensen, at the CRUK Manchester Institute, made the crucial discovery last year that oncogenic KRAS ramps up tumour cell signalling by coercing the stroma into feeding paracrine signals back to the tumour. And this communication extends into 'mechanotransduction' too where cells sense their rigidity and that of their surroundings and convert that information into signals that control behaviours such as proliferation and invasion.

Building on this, Claus has set up a collaboration with Professor Martin Humphries at the University of Manchester, who has made fundamental discoveries about the basic mechanisms of cell adhesion, to determine how stromal rigidity drives proliferation. "Adhesion has evolved over hundreds of millions of years to control cell fate it's not simply a way of sticking cells together," says Martin. They will be studying how the adhesion nexus a cluster of receptors, extracellular matrix fibres and cytoskeletal polymers works as a sensor of stromal rigidity in PDAC, and hope to unpick exactly how desmoplasia forces proliferation under unfavourable circumstances, thereby accelerating tumour progression.

Tackling brain cancers

CRUK's spend on brain tumour research has more than doubled in the last five years. But growth since the launch of the Research Strategy in 2014 has been modest, suggesting more needs to be done. Brain cancer remains a challenging area in which there is limited research activity. To address this we held an international workshop in 2016 with a panel of expert leaders in the field. The meeting identified key research areas seen as crucial for the progress of brain tumour research and improving patient outcomes. We are now looking at ways to highlight these questions to the research community and to fund research to address them.

Like pancreatic cancer, glioblastoma, the most aggressive form of brain cancer, is intractable and rapidly lethal. Though thankfully rare, with around 2,300 cases in England each year, survival is low with less than 5% surviving for at least five years.

Clinician scientist Dr Paul Brennan, a recent Pioneer Award recipient, works on the frontline of glioblastoma, combining his work as a consultant neurosurgeon at Edinburgh's Western General Hospital with research at the CRUK Edinburgh Centre. When it comes to brain cancer, being a surgeon is peculiarly frustrating: "This is a disease that can't be cured surgically. In the brain, there's no natural containment barrier; glioblastomas spread quickly along the normal white matter tracts, so removing the mass isn't curative," he explains. "Eventually I'd hope only to offer surgery to people with no alternative. Frustratingly, at the moment, that's everyone."

Paul's Pioneer Award relies on a collaboration with two colleagues at the CRUK Edinburgh Centre Dr Dirk Sieger, who models brain cancer in zebrafish, and Dr Asier Unciti-Broceta, a medicinal chemist. Asier's work on palladium catalysts drives the project, and came to Paul's notice during a thesis committee meeting for one of Asier's students: "I remember thinking that although this is a pure chemistry PhD and I don't understand the aromatic chemistry, I do understand how this would be applicable to brain tumours", Paul says.

Glioblastomas tend to recur at their original site, implying that, post-surgery, residual cells remain. The Pioneer Award will be used to study the potential of implanting inert palladium beads at the time of surgery, and then treating patients with a prodrug that the palladium catalyst will activate. "We should be able to give people a higher concentration of the drug and avoid some of the side effects," Paul says. They hope to develop prodrugs that work in Dirk's zebrafish glioma model, providing proof-of-principle evidence needed to scale up the project and take it into pre-clinical development.

Developing research resources

Moving the brain cancer field forward will require the development of communal research resources to mine the knowledge gleaned from patient cell lines and samples, something that Dr Steve Pollard, also at the CRUK Edinburgh Centre, is passionate about. As well as having his own glioblastoma research programme, Steve is the principal investigator for the Glioma Cellular Genetics Resource (GCGR), funded by CRUK in 2016 through an Accelerator Award. The GCGR will be a centralised resource for the generation, cataloguing and curation of glioblastoma cell lines, accessed via an open source database. Genome editing tools and novel engineered patient-derived cellular models will also be on offer Steve's already receiving plenty of requests for the CRISPR tools he's developed in the last year for modifying target genes of interest.

There's a training and recruitment component too: a new generation of scientists will be nurtured via the PhD programme associated with the award, and the participation of the developmental neurobiologists at the Francis Crick Institute is a route for bringing some excellent basic scientists into the glioblastoma field: "We hope to tempt them in with the unique resources we can offer," he says, "Our cell lines, for example, contain a whole spectrum of glioblastoma mutations, many of which may have profound implications for normal neural development."

Taking a global view

International cooperation is vital for rare cancers, where national patient numbers are frequently too low to permit meaningful studies, and this is especially so in the challenging field of paediatric brain tumours. Professor Richard Gilbertson, at our Cambridge Centre, believes that the availability of big data means that the global community can now work together in a more purposeful way: "Next generation sequencing has allowed us to look into the biology of childhood cancer in a way we've never done before," he says. "It's like looking for keys in a dark room. What next generation sequencing has done is switched the light on so you can see the keys. You don't necessarily know what lock the keys fit but at least you've found them."

The tumour transcriptome has meant that paediatric brain cancers are now beginning to be stratified, but Richard says the challenge is to transfer this knowledge into the clinic: "We now know, for example, that in medulloblastoma there are four distinct subgroups, one of which does really well and should probably be spared radiotherapy. There are things we're armed with now that will make an impact, and I have a lot of hope for the next five years."

Major advances

In his own lab, Richard has had a long-standing preoccupation with the paradox that tissues grow faster during childhood than at any other time, and yet childhood cancers are so rare: "If you have a tissue with this massive mitotic process going on there has to be a mechanism in there to stop it becoming malignant," In what he believes is the most significant work of his career, CRUK-funded work from his lab published last year in Cell showed this to be true: stem cells that give rise to adult cancers are about seven-fold more sensitive to generating cancer than paediatric stem cells.

The results have profound implications: "Because we know precisely what those cells are, we can interrogate them at the molecular level in adults and neonates across all organs to find whether there is a particular biological cassette in a neonatal cell that is protecting it from cancer," Richard says. "And if you could pharmacologically activate that in adults, you'd have a system that was no longer susceptible to cancer."

Major discoveries draw people and resources into a field, and cause a build-up of momentum that pushes the field forward. Up until now, such advances have been few and far between in the cancers identified by CRUK as unmet needs. Now, though, thanks to the influx of new blood synergising with the expertise and dedication of long-term researchers, those discoveries are starting to come; and as some of the work profiled here shows, the consequences may be profound, not just for single cancers, but for the whole spectrum of disease.

Explore further: Improving radiotherapy for brain cancers

Journal reference: Cell

Provided by: Cancer Research UK

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Tackling hard-to-treat cancers from every angle - Medical Xpress

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