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Microbiome Medicine: Scientists Harness the Body’s ‘Bugs’ to Treat Asthma, MS, and More – UCSF News Services

Plenty of probiotic yogurts, pickles, and kombuchas claim to boost our digestive health with armies of microbes, but some scientists have more ambitious therapeutic plans for the bugs that colonize us. They hope to leverage these microbes as living therapeuticsfor a range of health conditions, including ulcerative colitis, multiple sclerosis, eczema, and asthma.

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Our guts, skin, and other regions of the body harbor trillions of microbes, as many as we have cells of our own. Each of these microbes bacteria, viruses, microscopic fungi, and others that make up the human microbiome brings with it a unique genome.

The composition of our microbiome and its microbial pan-genome is shaped by diet and environment, which in turn affect its important influences on human physiology, from digestion to brain health to immune function.

One real advantage of the microbiome is that its a dynamic system, said Susan Lynch, PhD, professor of gastroenterology and director of the UCSF Benioff Center for Microbiome Medicine. What were thinking about is how we can leverage microbes in engineering that system to improve health or prevent disease.

Much of the clinical research on the microbiome revolves around its connection with autoimmune disorders, such as rheumatoid arthritis, Crohns disease, and multiple sclerosis (MS), which altogether affect 24 million Americans. While genetics factor into why some people develop autoimmune disorders, environmental triggers likely contribute, said Sergio Baranzini, PhD, a neurology professor at the UCSF Weill Institute for Neurosciences, who studies the genetics and immunology of MS.

This is where we turn to the microbiome, he said. Because it is so influenced by food and other environmental factors, its a proxy for the environment.

A decade ago, when rapid DNA sequencing techniques made it cost-effective to identify bacteria, Baranzini began studying the relationship between the gut microbiome and MS, an autoimmune disorder in which the immune system attacks the nervous system. He had been intrigued by reports of other autoimmune conditions in which patients and controls were found to have different gut microbes.

In fact, most of our immune cells reside in our gut, and they depend on short-chain fatty acids produced when gut bacteria digest dietary fiber.

Baranzini compared stool and blood samples from people with MS to those from a member of the same household without MS. He found that the two populations of gut bacteria indeed differed, and that the blood from the person with MS had considerably fewer regulatory T cells, which normally tamp down the bodys immune response.

The deficiency of these T cells, Baranzini hypothesizes, is likely tied to the microbiome and impairs the bodys ability to control inflammation. He launched the International MS Microbiome Study to seek a comprehensive picture of gut microbiota in people with MS.

B cells (green), dendritic cells (blue) and T cells (red) are immune cells that help maintain the delicate relationship between the gut microbiome and the host. Image byLauren Rodda

Weve started discovering how diverse our microbiota are and how intimately they are in contact with our own immune systems, he said. And we now know that theres a lot of back-and-forth between the immune system and cells in the intestine that were only beginning to understand.

Microbial therapies for autoimmune disorders already exist in the form of fecal microbial transplants, or FMT, which involves taking stool samples from healthy individuals, isolating the gut microbes, and giving them to patients via a pill or enema.

This past April, Najwa El-Nachef, MD, an associate professor of medicine, wrapped up a clinical trial for ulcerative colitis and found that some patients respond much better to FMT than others, with a few reporting improvements in inflammatory skin and joint conditions as well. Her next step is to identify the best patients for microbiota-based therapy and to develop more targeted treatments.

For a subset of ulcerative colitis patients, manipulating the microbiome may provide a way to treat their autoimmune disease without suppressing their immune system, she said.

Our microbiome begins to take shape early, so interventions at the start of life can set the stage for future health. Lynch has focused some of her research on the gut microbiota during a babys first months of development. Its a critical time when the composition of the babys microbiome, influenced by the mother and the environment, can affect the development of the immune system and immune memory, with lasting consequences.

Susan Lynch, PhD, is the director of the UCSF Benioff Center for Microbiome Medicine. Photo by Barbara Ries

Najwa El-Nachef, MD, is studying the role of the microbiome in treatingulcerative colitis. Photo by Barbara Ries

Weve found that the gut microbiome at one month of age really predicts the risk of developing asthma and airway disease later in childhood, she said. Lynch and her team have identified specific microbial products that drive the dysfunction of regulatory T cells, which is associated with subsequent disease.

Weve considered that engineering the gut microbiome during this key window of immune training could have a long-term beneficial impact on the health status of high-risk children, she said

Lynch has developed a live microbial intervention administered at birth to babies at high-risk for asthma, comprised of bacteria that can modulate immune response. Their bacterial genomes encode a range of functions consistently absent from high-risk infant gut microbiomes.

The idea is to shape the developing gut microbiome by providing bacteria that can train the immune system early in life with their microbial products and metabolites, ultimately influencing the microbiomes function in the long term.

Our skin harbors its own set of microbes that interact with immune cells and protect the skin from infection.

Clinical trials using skin microbiota are already showing promise for patients with eczema, an autoimmune condition that can flare up when staph bacteria proliferate, said Tiffany Scharschmidt, MD, an associate professor of dermatology. The trials involve supplementing the bacteria that ordinarily keep the staph population under control.

Tiffany Scharschmidt, MD, is studying using skin microbiota arefor patients with eczema.Photo by Barbara Ries

Sergio Baranzini, PhD, is studying he genetics and immunology of multiple sclerosis.Photo bySteve Babuljak

As we gain more understanding of the interaction between the skin microbiome and its immune system, well see other microbial-based treatments emerging, she said. In the future, therapeutic skin microbes could even be genetically engineered to produce needed compounds.

The gut microbiome is, of course, intimately tied with digestion, producing diet-derived compounds that program immune cells and produce nutrients critical for the growth of the cells that line our intestines. The basic digestive and immune functions in our gut depend on colonization by specific bacteria, said Peter Turnbaugh, PhD, an associate professor of microbiology and immunology. Our intestinal cells have evolved receptors just lying in wait to sense the chemicals produced by the gut microbiome.

Turnbaugh has found that our inner critters also play a role in metabolizing medication. A better understanding of that role, he said, could increase drug efficacy.

We think the microbiome might be second only to the liver in determining how drugs are metabolized in the body, affecting how a patient responds to an existing therapy, he said.

Some antibiotics, for example, are activated by enzymes produced by the gut microbiota. Our microbial tenants may even influence how substances move around the body or change a drugs mechanism of action, but much remains unexplored in this area, said Turnbaugh.

Deeper knowledge of how our gut microbiome interacts with drugs might enable physicians to prescribe treatments that align with or supplement our individual microbiome, a new form of precision medicine.

Lynch believes that the therapeutic advances we can make through understanding the microbiome will rival those that came with understanding the human genome, particularly on autoimmune disorders.

Though the human microbiome field is still relatively young, it has already provided exceptional insights into the dependence of human physiology on our dynamic microbial inhabitants and offers a new set of tools to elicit better health, said Lynch. Translating these early observations into new live biotherapeutics represents the next step in realizing the potential of this field.

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Microbiome Medicine: Scientists Harness the Body's 'Bugs' to Treat Asthma, MS, and More - UCSF News Services

Novartis says it overpaid Roche’s Genentech nearly $210M in a licensing dealand it wants its money back – FiercePharma

For years, Novartis said it dutifully shelled out tens of millions to Genentech as part of a patent licensing deal that dated back to 2005. Later, the Swiss pharma discovered it accidentally overpaid by nearly $210 million.

Those are the central arguments in a lawsuit filed by Novartis against its Swiss pharma counterpart seeking $209.5 million.In the suit, whichrecently made its way to California federal court, Novartis says Genentech isn't coughing up the dough.

Novartis claims Genentech was aware, or at least shouldve known, that the company was overpaying the entire time.

The paymentsstemmed from a 2005 licensing agreement Genentech struck with then Chiron Corporation related to its antibody patents. Novartis picked up Chiron a year later and developed several commercial antibody products from the pact, notablyimmunology meds Ilaris and Cosentyx, the suit says.

RELATED:Novartis hits setback in bid to block Regeneron's Eylea prefilled syringe as dual lawsuits drag on

Instead of alerting Novartis of the overpayments, Genentech continued to seek, accept, and retain the funds driven by Ilaris and Cosentyx sales, even though they werent entitled to them, Novartis argued in the filing.

While terms of the initial licensing deal weren't disclosed, Novartis maintains itperformed all or substantially all of its obligations under the deal and later learned of the overpayments after it expired.

Meanwhile, lawyers representing Genentech dismissed Novartis claims in a filing seeking to move the case from state to federal court, arguing the claims fall under federal patent law.

The companies werent immediately available for comment.

RELATED:Novartis' closely watched canakinumab hits a snag in lung cancer. What's next for the anti-inflammatory drug?

Cosentyx, which first launched in 2015, directly inhibits interleukin-17A (IL-17A), an important cytokine involved in the inflammation of psoriatic arthritis, moderate to severe plaque psoriasis, ankylosing spondylitis and non-radiographic axial spondyloarthritis.

The treatment has become Novartis largest brand, driving $3.9 billion in sales last year, up 13% compared with the year prior.

Meanwhile, sales of IL-1beta inhibitor Ilaris came in at roughly $873 million, up 30%. Despite efforts to push the medicine, also known ascanakinumab,into fields outside immunology, Novartis has run intomultiple setbacks, including in heart disease, COVID-19 and, most recently, non-small cell lung cancer.

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Novartis says it overpaid Roche's Genentech nearly $210M in a licensing dealand it wants its money back - FiercePharma

Study paves the way for development of new therapeutics for C. difficile infection – News-Medical.Net

A new study paves the way for the development of next generation therapeutics for the prevention and treatment of Clostridioides difficile infection (CDI), the most frequent cause of healthcare-acquired gastrointestinal infections and death in developed countries.

Published today in Nature Communications, the study reveals the first 3D structure of the Clostridioides difficile toxin B (TcdB) in complex with chondroitin sulfate proteoglycan 4 (CSPG4), a human receptor. The study was co-led by senior author Rongsheng Jin, PhD, a professor in the Department of Physiology & Biophysics at the University of California, Irvine, School of Medicine, and Min Dong, PhD, an associate professor at Harvard Medical School.

TcdB is one of two homologous C. difficile exotoxins, which are major virulence factors responsible for the spread of C. difficile infections. TcdB alone is capable of causing the full-spectrum of diseases associated with CDI in humans."

Rongsheng Jin, PhD, Professor, Department of Physiology & Biophysics, University of California, Irvine, School of Medicine

Previous studies had identified CSPG4 as a potential receptor for TcdB, however the pathophysiological relevance and molecular details were unknown. Results from this new study reveal a unique binding site involving TcdB and CSPG4, and also show that CSPG4-binding residues are highly conserved across most TcdB variants known to date.

CDI has become the most common cause of antibiotic-associated diarrhea and gastroenteritis-associated death in developed countries, accounting for approximately 223,900 infections, 12,800 deaths, and $1 billion in healthcare costs in the United States in 2017. It is classified as one of the top five "urgent threats" by CDC. There is also growing global concern surrounding the emergence of rapidly spreading hypervirulent C. difficile strains, reminiscent of the current COVID pandemic.

"What these new findings tell us is that a rationally designed CSPG4-mimicking decoy could neutralize major TcdB variants, providing a unique therapeutic avenue for combating some of the hypervirulent C. difficile strains," said Jin. In contrast, researchers also revealed that the therapeutic mechanism for bezlotoxumab, the only FDA approved anti-TcdB antibody, is sensitive to escaping mutations in some bacterial strains.

The current standard of care for CDI involves treatments using broad spectrum antibiotics, which often lead to frequent disease recurrence. While bezlotoxumab could reduce the recurrence rate of CDI in some patients, results from this and some earlier studies indicate it has weaker potency against some TcdB variants.

"We have designed a CSPG4-mimicking decoy based on the 3D structure we observed, which could neutralize major TcdB variants and is superior to bezlotoxumab on a major TcdB variant from a hypervirulent strain (TcdB2) in our studies. As a highly conserved cellular receptor of TcdB, a CSPG4 decoy molecule would be difficult for TcdB to escape, since any mutations that disrupt toxin binding to the decoy would also disrupt binding to its native receptors," said Jin.

The team of researchers has also developed a family of recombinant protein therapeutics based on these new findings, as well as on an earlier discovery on how TcdB recognizes another human receptor Frizzled (FZD).

"We are now examining the therapeutic features of these novel antitoxin molecules, and we believe they could provide broad-spectrum protection and neutralization against most known TcdB variants, thus improving existing antibody therapeutics for CDI," said Jin, whose team has filed a patent on these neutralizing molecules.

Source:

Journal reference:

Chen, P., et al. (2021) Structural basis for CSPG4 as a receptor for TcdB and a therapeutic target in Clostridioides difficile infection. Nature Communications. doi.org/10.1038/s41467-021-23878-3.

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Study paves the way for development of new therapeutics for C. difficile infection - News-Medical.Net

Switching from face-to-face to an online teaching strategy: how anatomy and physiology teaching transformed post-COVID-19 for a university…

This article was originally published here

Adv Physiol Educ. 2021 Sep 1;45(3):481-485. doi: 10.1152/advan.00233.2020.

ABSTRACT

The College of Science and Health Professions offers a university preprofessional program. Like most medical schools in Saudi Arabia, the teaching delivery strategy in the university preprofessional program is on campus and face-to-face. During the month of March 2020, teaching activities of the spring semester were proceeding as normal; however, the sudden emergence of COVID-19 disturbed routine activities and compelled authorities to switch all teaching activities from face-to-face to online. Training sessions and workshops for all stakeholders on online delivery methods were arranged. Blackboard and other online facilities were utilized. All teaching materials, including newly made video clips for anatomy and physiology practicals, were uploaded on Blackboard and discussed online with students. Students anxiety related to the exam was reassured by giving them the option of open book quizzes during summative continuous assessment. All scheduled teaching sessions, lectures, and practicals were conducted proficiently. Revision sessions and assessment quizzes were conducted with students satisfaction. At the end of the semester, a final exam was conducted online as an open book exam. Students with technical issues while attempting the exam were given an opportunity to make up for it. After a successful final exam, the cumulative block grades showed students secured higher grades in the open book exam. Following that, the King Saud bin Abdulaziz University for Health Sciences has managed to conduct on-campus close book exams that abide by self-distancing and standard operating procedure policies.

PMID:34142877 | DOI:10.1152/advan.00233.2020

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Switching from face-to-face to an online teaching strategy: how anatomy and physiology teaching transformed post-COVID-19 for a university...

Plans revealed to build world’s deepest pool, Blue Abyss, in the UK | spabusiness.com news – Spa Business

The 150m project would see an aquatic centre housing a 164ft (50m) deep pool

Primarily designed for sea and space research, the project is led by a privately-funded company, Blue Abyss

The pool will hold more than 42,000 cubic metres of water

Blue Abyss has been designed by British architect Robin Partington

The 150m project would see an aquatic centre, housing a 164ft (50m) deep pool built at the Aerohub Enterprise Zone at Cornwall Airport.

The project is led by a privately-funded company, Blue Abyss, which is now in the process of applying for planning permission.

The centrepiece of Blue Abyss will be an aquatic centre featuring a 50m by 40m stepped pool with a 50m deep shaft. The pool will hold more than 42,000 cubic metres of water the equivalent of 17 Olympic size swimming pools making it the largest and deepest indoor pool in the world.

A sliding roof and 30-tonne crane will allow large objects to be lowered into the pool, from simulated sections of the International Space Station to underwater film sets and even cave systems to test remote operated vehicles or train deep-sea divers.

With the facility, Blue Abyss wants to "revolutionise extreme environment research and training in Europe".

The centre will offer state-of-the-art whole system human physiology and human-robotic interface R&D capabilities, serving the human spaceflight, sports science and terrestrial healthcare communities.

The on-site Kuehnegger Human Performance Centre will look to cater particularly for the professional sports sector as well as healthcare with an emphasis on rehabilitation from physical deconditioning.

Blue Abyss will look to form academic partnership with national and international universities, drawing on its resources to execute R&D projects, providing a mix of expertise and facilities.

In all, the 10-acre site is set to house the pool, an astronaut training centre, the Kuehnegger Human Performance Centre, hypobaric and hyperbaric chambers, microgravity suite, training centre with six classrooms, workshops, onsite catering and accommodation facilities.

There will also be a visitor and educational centre.

Blue Abyss has been designed by British architect Robin Partington, who led the design team for The Gherkin in London.

Once open, the facility is expected to generate 8m annually for the local economy.

Blue Abyss CEO, for British Army diving instructor, John Vickers, said: "We're planning a globally unique facility with a wide range of potential uses that tap into so many of the industries that Cornwall and the South West are known for.

"Blue Abyss will be a huge research asset for aerospace, offshore energy, underwater robotics, human physiology, defence, leisure and marine industries and a fantastic education centre for children."

Other deep pools in the world include Y-40, The Deep Joy a thermal pool in Italy.

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Plans revealed to build world's deepest pool, Blue Abyss, in the UK | spabusiness.com news - Spa Business

Bring the ‘dad jokes,’ we need ’em. (Warning: This story contains actual dad jokes) – KSL.com

Dad jokes are known to reduce tension and strengthen connections as a meta-analysis from 2017 in the journal Advances in Physiology Education examined the health benefits of humor and backs those findings. (CNN)

ATLANTA (CNN) In September 2019, just ahead of the COVID-19 pandemic so roughly before-anyone-can-remember ago Merriam-Webster added the term "dad joke" to the dictionary, to little fanfare.

As it turns out, the official addition to our vocabulary was just in time to remind us of the value of instantly available humor, especially among freaked-out family members enduring lockdowns together.

If you tell dad jokes, you already know their usefulness in reducing tension and strengthening connections. A meta-analysis from 2017 in the journal Advances in Physiology Education examined the health benefits of humor and backs those findings. Humor, the analysis found, also promotes increased learning and stress reduction. That's no joke.

"We value humor because it teaches communication, humility and happiness," articulated my brother, Matthew Henneberger, an aficionado of the dad joke. What he loves about the genre is that dad jokes introduce these great lessons to kids at a very young age.

One of my favorites I got from him: "Where does George Washington keep his armies? In his sleevies."

Dad jokes are also easy to come by, one of the low-hanging fruits of comedy. They require no setup, context or segue. They are prt--porter. You can just drop a bad pun, say something goofy or blurt out the question and punchline answer together and immediately cash in on those eyerolls and smiles.

Try this one to anyone within earshot right now: "I was going to tell a time-traveling joke, but you didn't like it."

It's that combination of groan and chuckle that defines a dad joke and also explains their appeal.

They are not all "dumb" though, even if that label is the response you get. Or maybe they are a little dumb. Smart-dumb. More Marx Brothers than Three Stooges. They are populated by puns ("Clones are people two"), one-liners ("It takes guts to be an organ donor") and malapropisms ("What does a baby computer call his father? Data.")

They are often simple and easy to grasp, but the best ones are clever, too. "What rhymes with orange? No, it doesn't."

But do you know when a joke really becomes a dad joke? When it's apparent.

And they don't have to be just for kids, despite the name. But they must be G-rated. Dad jokes don't do blue or offensive. You can always safely tell a dad joke in front of kids, but depending on their age, you may need to explain why it's funny (in a very dadlike fashion).

Take this Zen koanlike gem: "What did Buddha say to the hot dog vendor? Make me one with everything." A worldly 10-year-old may get that one along with most adults, less so little kids.

And given their liberal use of homonyms, these jokes are often better delivered in person, like this one: "Did you hear about the circus fire? It was intense (in tents)."

My CNN colleague Alberto Mier likes to misuse his kids' slang or purposely bungle the names of things they like ("The Tickity Tock," for example).

"My 16-year-old, in particular hates it, so I do it even more," he added. "Stupid, but it drives her nuts, and that's what it's all about."

Basically, dad jokes are just fun. And we need more fun. It's also why we invited the mushroom to the party because they are the fungi!

So, collect them, memorize them, and start dropping them on others. I have a Google doc of favorites I've stumbled across or were told to me by fellow dads (and moms), like this winner from fellow dad and friend Sam Younis: "Why did the old man fall in the well? He couldn't see that well."

During the pandemic, Younis bought a book of dad jokes ("The Little Book of Dad Jokes: So Bad They're Good"). He keeps it handy in the kitchen just to lighten the mood.

"Now my kids read the jokes to me and shake their heads when they see me laugh," he said.

When you hear or read them, curate your favorites. I picked up this science dad joke from a CNN interview with Neil deGrasse Tyson: "Why can't you trust an atom? Because they make up everything."

So, curate your list (in a "dad-a-base!") and start busting them out. Fill the awkward wait at the start of a meeting, make your kid and their friends crack up (or enjoy their bonding over shared eye-rolling), and do it maybe the chief reason to delight yourself.

All right, ready for more jokes? CNN's Dad Joke Generator has your fix.

Time for me to make like a tree and leaf.

The-CNN-Wire & 2021 Cable News Network, Inc., a Time Warner Company. All rights reserved.

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Bring the 'dad jokes,' we need 'em. (Warning: This story contains actual dad jokes) - KSL.com

Ohio University announces spring 2021 graduates – The Times

From Staff Reports| Beaver County Times

ATHENS, OH More than 4,800 students graduated with bachelor's, master's or doctorate degrees from Ohio University for spring semester 2021.

* Michelle Behana, of Freedom, PA, graduated with a Bachelor of Science in Nursing (Baccalaureate Nursing) from the College of Health Sciences and Professions;

* Patrick Boff, of Freedom, PA, graduated with a Master of Engineering Management from the Russ College of Engineering and Technology;

* Madeline Brown of Beaver, PA, graduated with a Bachelor of Arts majoring in anthropology and linguistics from the College of Arts and Sciences;

* Chad Cable of Aliquippa, PA, graduated with a Bachelor of Science majoring in psychology from the College of Arts and Sciences;

* Meredith Camp, of Beaver Falls, PA, graduated with a Bachelor of Science in Physiology of Exercise majoring in exercise physiology - pre-physical therapy from the College of Health Sciences and Professions;

* Devin Daley, of Conway, PA, graduated with a Bachelor of Business Administration majoring in business analytics, management information systems, and marketing from the College of Business;

* Christian Petti, of Beaver Falls, PA, graduated with a Bachelor of Business Administration majoring in marketing from the College of Business;

* Derek Weber, of Georgetown, PA, graduated with a Bachelor of Science in Engineering Technology and Management from the Russ College of Engineering and Technology.

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Ohio University announces spring 2021 graduates - The Times

PET/CT Effective Measures NSCLC Biomarker, Predicts Therapy Response – Diagnostic Imaging

PET/CT images can non-invasively measure levels of a non-small cell lung cancer (NSCLC) biomarker, eliminating the need for biopsy and predicting the patients response to therapy.

Checkpoint inhibitors that target the PD1/PD-L1 signaling pathway are an effective treatment for NSCLC, but it only works in roughly half of patients. Investigators from Moffitt Cancer Center demonstrated, in a study published this week in the Journal for ImmunoTherapy of Cancer, that PET/CT can effectively assess the patients PD-L1 level, helping patients and providers to side-step the risks that come with invasive biopsy.

This study is important, as it is the single largest multi-institutional radiomic study population of NSCLC patients to date treated with immunotherapy to predict PD-L1 status and subsequent treatment response using PET/CT scans, said Robert Gillies, Ph.D., chair of Moffitts cancer physiology department. Because images are routinely obtained and are not subject to sampling bias per se, we propose that the individualized risk assessment information provided by these analyses may be useful as a future clinical decision support tool pending larger prospective trials.

For their study, the team examined PET/CT scans for nearly 700 patients who had NSCLC who were treated in three institutions. They assessed shape, size, pixel intensity, and textures to train a deep learning tool to accurately measure PD-L1 expression. Using the data, they developed a deep learning score that could predict PD-L1 expression which, after validation, could predict checkpoint inhibitor outcomes in these patients.

Their results point to the usefulness of using images as a replacement for biopsy, said Matthew Schabath, Ph.D., associate member of the cancer epidemiology department.

These data demonstrate the feasibility of using an alternative non-invasive approach to predict expression of PD-L1, he said. This approach could help physicians determine optimum treatment strategies for their patients, especially when tissue samples are not available or when common testing approaches for PD-L1 fail.

For more coverage based on industry expert insights and research, subscribe to the Diagnostic Imaging e-Newsletterhere.

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PET/CT Effective Measures NSCLC Biomarker, Predicts Therapy Response - Diagnostic Imaging

Study Explored Benefits of Yoga in Chronic Low Back Pain – India Education Diary

Most of the yoga-based studies so far have relied on patients experience and rating of pain and disability as an indicator of recovery and better quality of life. Researchers who measured pain, pain tolerance and body flexibility have found that yoga leads to pain relief, increases tolerance of pain and improves flexibility in patients of chronic low back pain.

Dr Renu Bhatia, Additional Professor, Department of Physiology, AIIMS, New Delhi conducted research to measure the impact of yoga on Chronic Low Back Pain (CLBP) along with Dr Raj Kumar Yadav (Professor, Department of Physiology, AIIMS, New Delhi), Dr Sri Kumar V (Associate Professor, Department of Physical Medicine & Rehabilitation, AIIMS, New Delhi).

The study conducted on 100 Chronic Low Back Pain (CLBP) patients of 50 years with 3 years of history of the disease. After systematic Yogic intervention of 4 weeks, Quantitative sensory testing (QST) showed increase in thresholds for cold pain and cold pain tolerance. Corticomotor excitability and flexibility improved significantly in the patients.

They recorded objective measures for pain (electrophysiology), sensory perception (quantitative computerized sensory testing) and cortical excitability parameters. (using Transcranial Magnetic Stimulation of motor cortex).They found significant changes between all the parameters in CLBP patients compared to healthy controls at baseline. Significant improvement in all parameters was found after yoga.

This research supported by the Science and Technology of Yoga and Meditation (SATYAM) funded by the Department of Science and Technology, GoI has been recently published in theJournal of Medical Science and Clinical Research.

Assessment of pain and corticomotor excitability parameters shall help in establishing strong ground with scientific evidence for yoga to be prescribed as therapeutic intervention for chronic low back pain relief with or without standard therapy depending on the pathology. Also these parameters can be used for prognosis and follow-up of patients during recovery phase.

The team also developed yoga protocol for CLBP patients and for fibromyalgia patientsin Pain Research and TMS laboratory, AIIMS, New Delhi.

In patients with Chronic Low Back Pain, 4 weeks of yoga intervention improved pain status and pain-related functional disability, increased spinal flexibility and corticomotor excitability significantly more than standard care.

The study suggests that in long term Yoga can be performed at home, and hence is an inexpensive therapeutic intervention. It not only relieves pain but also improves overall quality of life and bestows other health benefits.

Dr. Renu Bhatia

Publication link:https://dx.doi.org/10.18535/jmscr/v9i3.30

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Study Explored Benefits of Yoga in Chronic Low Back Pain - India Education Diary

Ocean warming could hit shark survival – The University of Manchester

Infant sharks that live in the familiar mermaids purses found on most beaches in the UK and throughout the world are more vulnerable to predation because of ocean warming, new research suggests.

According to Daniel Ripley from The University of Manchester, higher temperatures reduce freeze response times which the animals employ to avoid being eaten by predators.

The study by the ecophysiologist is funded by the Biotechnology and Biological Sciences Research Council and The University of Manchesters Knowledge and Innovation hub for Environmental stability

It is published in the Journal of Conservation Physiology today (17 June).

If an embryo employs a freeze response, it stops moving so that predators - including large fish and other sharks - wont detect them.

That explains why being able to elicit a freeze response is key to surviving predation during embryonic development and the longer an embryo can freeze, the better chance it has of not being detected by predators.

In the lab Ripley compared the freeze response time of small spotted catshark embryos - which are 7 to 8cm long - at a water temperature of 15C and a water temperature of 20C.

The 5C temperature rise resulted in a 7-fold decrease in the time the animals froze following a predator simuli, mimicked by gently flicking the egg case

And that could have major consequences for embryonic sharks in a warming world. Being able to freeze is key to avoiding predators and if warming means infant sharks will not be able to freeze as long, it could reduce the number of sharks surviving to adulthood.

Around 45% of shark and ray species lay eggs which grow inside a mermaids purse, which can last for around a year before they hatch

The purses come in various colours, shapes and textures, depending on the species of shark.

Beachcombers often spot the empty shell cases on the beach, though the live egg cases often lie tangled up with sea weed in shallow waters and rockpools.

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Ocean warming could hit shark survival - The University of Manchester