Category Archives: Physiology

AIIMS Patna: Great opportunity to apply for these posts, know the age limit – News Track English

All India Institute of Medical Sciences, Patnais invitingeligible candidates for the vacant posts of Senior Resident (Physiology).28-1-2020 is the last date to apply. Application fee, selection process for the job, age limit for the job, details of the posts, the names of the posts, educational qualifications for the job, total number of posts and other details are mentioned below.

This is the age limit of the candidates for the job ...

The maximum age department of the candidates will be 45 years and age relaxation will be given to the reserved category.

the wages....

The candidates who will be selected for these posts will be given salary as per the rules of the department.

It is necessary academic qualification for the job ...

Candidates should have postgraduate degree and experience in Physiology from any recognized institute.

Eligible candidates will be selected for the job in this way ...

The candidate will be selected on the basis of interview.

Candidates can attend the interview on 28-1-2020. As per the date of the candidates, certified and original documents have to be brought with them at the time of interview.

All India Institute of Medical Sciences, Patnais invitingeligible candidates for the vacant posts of Senior Resident (Physiology).28-1-2020 is the last date to apply. Application fee, selection process for the job, age limit for the job, details of the posts, the names of the posts, educational qualifications for the job, total number of posts and other details are mentioned below.

Post Name - Senior Resident (Physiology)

Total post-1

Location- Patna

This is the age limit of the candidates for the job ...

The maximum age department of the candidates will be 45 years and age relaxation will be given to the reserved category.

the wages....

The candidates who will be selected for these posts will be given salary as per the rules of the department.

It is necessary academic qualification for the job ...

Candidates should have postgraduate degree and experience in Physiology from any recognized institute.

Eligible candidates will be selected for the job in this way ...

The candidate will be selected on the basis of interview.

How to apply

Candidates can attend the interview on 28-1-2020. As per the date of the candidates, certified and original documents have to be brought with them at the time of interview.

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AIIMS Patna: Great opportunity to apply for these posts, know the age limit - News Track English

Doubt Cast on the Use of Viagra for Fetal Therapy – Technology Networks

University of Manchester scientists investigating a possible treatment for fetal growth restriction (FGR), a condition in which babies grow poorly in the womb, have urged further caution on the use of Viagra.

The drug, commonly used to treat erectile dysfunction, as it enhances blood flow - has been undergoing trials as a potential treatment for FGR. However, in a recent study in mice, Viagra showed no improvement in fetal growth but did result in high blood pressure in the pups as they reached maturity.

Babies with Fetal Growth Restriction (FGR) are at increased risk of stillbirth and are more likely to suffer from developmental problems and other conditions such as heart disease and diabetes in adulthood.

FGR affects around 3 in every 100 pregnancies and most cases are caused by poor function of the placenta, affecting blood flow and thus nutrient transfer from mother to the baby.

No treatments are available for FGR and often the only option for obstetricians is to deliver the baby early so they can be cared for outside the womb.

The Manchester team are the first to report the long-term effects of the drug, on both male and female offspring, when given to mice during pregnancy and publish their results in theAmerican Journal of Physiology - Heart and Circulatory Physiology.

An international clinical trial of Viagra on severe cases of human FGR called STRIDER, and carried out at the same time as the Manchester study, also found the drug had no significant benefit on fetal growth or prolongation of pregnancy.

The Dutch arm of the STRIDER trial was halted after 11 babies of mothers using the medication died from lung complications, though this did not happen to babies in the New Zealand-Australia or the UK-Ireland trials.

In the Manchester study, over 90% of mice whose mothers were given Viagra during their pregnancy experienced a significant increase in their blood pressure. This increase was in the range of values equivalent to those used to diagnose high blood pressure in humans.

The effect was similar in both wild type (normally grown) and growth restricted mice and was consistent in both females and males.

Female mice also experienced a modest increased weight gain after birth and a minor reduction in glucose tolerance after 8 weeks.

The study was carried out by former PhD student Dr Lewis Renshall. He said "This, and other studies have shown Sildenafil - otherwise known as Viagra - may not be a suitable treatment for FGR unless life-saving benefits can be demonstrated."

"So there is still much work to do if we are to eventually find a treatment for this distressing condition."

Dr Mark Dilworth, who led the study, added: "The evidence from this study and others suggest that caution should be used for the use of Viagra in fetal Growth Restriction. Our study suggests there may be long-term risks associated with its use in mice and importantly, there is a lack of beneficial effect in recent human clinical trials."

"We do feel, however, that it is important to continue to conduct studies which look at longer term impacts of giving medication during pregnancy as there is surprisingly little research on this."

Reference: Renshall et al. (2020).Antenatal sildenafil citrate treatment increases offspring blood pressure in the placental-specific Igf2 knockout mouse model of FGR. American Journal of Physiology. DOI: https://doi.org/10.1152/ajpheart.00568.2019.

This article has been republished from the following materials. Note: material may have been edited for length and content. For further information, please contact the cited source.

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Doubt Cast on the Use of Viagra for Fetal Therapy - Technology Networks

Exercise can help in the fight against cancer, but how do we persuade patients to do it? – The Globe and Mail

When a major new set of international guidelines on exercise and cancer was released in October, most of the headlines understandably focused on two key promises: That appropriate levels of physical activity could enhance quality and possibly length of life in those with a cancer diagnosis; and that they might help others avoid developing cancer in the first place.

The evidence for these two claims was dissected in depth in a pair of papers published simultaneously in Medicine & Science in Sports & Exercise, the fruits of a lengthy roundtable process involving more than three-dozen researchers from 17 health organizations around the world, including the Canadian Society for Exercise Physiology.

Less heralded, however, was a third paper from the same group that addressed a knottier problem thats all too familiar to exercise researchers: How do you move from knowing that something is a good practice to getting people to actually do it? Establishing a regular exercise habit can be challenging for just about anybody, but there are extra hurdles for people with cancer.

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Theyre all in different types of treatment, theyve had different surgeries, says Kristin Campbell, the director of the University of British Columbias Clinical Exercise Physiology Lab and one of the authors of the new guidelines. As a result, cancer survivors themselves have a lot of questions, like Is this safe for me?

The answer, in most cases, is yes but with some adjustments. While a previous set of guidelines published in 2010 had suggested that those undergoing cancer treatment should aim for the same amount of exercise as everyone else, meaning at least 150 minutes of moderate to vigorous exercise for each week, the new guidelines revise that target down to three weekly sessions of 30 minutes each.

That adjustment, based on a wealth of new evidence published in the past decade, is a good change, says Margie McNeely, the director of the University of Albertas Cancer Rehabilitation Clinic, and a more realistic standard for a survivor undergoing or in the early stages of recovering from cancer treatment.

For reasons that arent fully understood theories include reduced inflammation and oxidative stress, better blood-sugar control and changed hormone levels exercise has powerful effects on cancer cells.

Theres now strong evidence that regular physical activity lowers your risk of at least seven different types of cancer, and moderate evidence that it raises your chances of survival if you do get diagnosed. For those undergoing cancer treatment, it staves off reductions in physical function and helps reduce anxiety, depression and cancer-related fatigue.

In other words, the pressing question isnt whether cancer survivors should exercise its how to give them the confidence and information they need to do it.

Oncologists and oncology nurses are not trained in exercise, Campbell points out. They dont really know how to screen people or what to prescribe for exercise, because its just not their wheelhouse.

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In the third roundtable paper, Campbell and her colleagues propose a three-step process for oncologists: Assess, advise and refer. Simply asking about a patients current exercise capacity assessing is a good way to raise awareness, and basic advice about the new exercise guidelines advising may be enough to send some people down the right path.

But many will need a referral for more detailed help from an exercise specialist. Thats where initiatives such as the Alberta Cancer Exercise program, a continuing study led by McNeely, come in. Over the last year, more than 1,500 people with cancer have taken part in the supervised 12-week program at sites across the province.

About a quarter of the participants have what McNeely calls chronic cancer. Theyre not cured, but are living with the disease and will likely live for a long time while cycling in and out of treatment. Prescribing exercise for these people is trickier, but the benefits quality of life, physical function and the fitness to withstand their treatments are even more significant.

Given these constraints, there will never be a single set of generic exercise guidelines that applies to all cancer survivors. But the most essential message, now backed by solid science, is the simplest: Avoid inactivity, Campbell urges. Get out there and start doing whatever youre able to do.

Alex Hutchinson is the author of Endure: Mind, Body, and the Curiously Elastic Limits of Human Performance. Follow him on Twitter @sweatscience.

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Exercise can help in the fight against cancer, but how do we persuade patients to do it? - The Globe and Mail

VIVIT the Live autopsy experience is returning to Bangor – The Bangor Aye

VIVIT, the worlds only travelling live post mortem experience, is returning to Bangor this April.

The live human body dissection experience offers front row seats to the hidden world of all things post mortem, where you get to play the pathologist.

This once in a lifetime experience gives you access to nationally acclaimed clinical experts, doctors and PhD researchers at the cutting edge of anatomy and physiology. Live at VIVIT events the skin will be peeled back and using real specimens youll embark on solving the mystery behind the mortality.

VIVITs team of award winning experts undertake hundreds of cadaveric dissections every year and really are international experts in technical dissection showcasing the best of human anatomy and physiology

The VIVIT Experience is a nationally award winning academic experience offering you the chance to participate in a recreated post mortem experience conducted on VIVIT the worlds only semi-synthetic human cadaver.

During this special 5 hour experience you will be taken on a scientifically accurate recreated human body dissection learning in-depth anatomy and physiology relevant to your academic studies.

The course is designed to support students studying in the biosciences, health, sports or associated degree pathways that require an understanding of advanced anatomy and physiology or indeed the associated clinical pathologies.

The procedure will be lead by highly skilled and internationally accliamed human anatomists who will first set out the basics of anatomical dissection before systematically working their way through the anatomical cavities comparing normal specimens with various states of pathology.

You will also be taught a variety of important clinical skills including interpreting X-rays and linking symptoms to clinical diagnosis. There will be the opportunity to ask questions and at the same time handle the anatomical samples and even the chance to undertake some dissection for yourself.

In 2018, VIVIT appeared on Dragons Den and successfully secured investment from Peter Jones and Deborah Meaden after almost three hours of intense negotiation.

CEO, Sam Piri, 31, walked away with the investment and expertise he wanted. Peter and Deborahs team have been working very closely with VIVIT over the last year allowing us to expand the ITAE Group.

VIVIT events are more prominent than ever before whether youre a teenager, undergraduate, healthcare professional or member of the general public you can engage with the experience.

How long does the VIVIT dissection last?The post mortem experience is 5 hours long, split into 2 parts.

How many people can participate in one VIVIT dissection?There is 150 tickets available for each session. This is a comfortable number that can engage with the experience given the AV equipment installed.

Is the anatomy human?No. The anatomy is of swine origin. Identical in size and structure -once harvested the samples are moved into VIVIT. VIVIT is a life size synthetic cadaver which is dissected for the audience to teach the structure and function of the human body.

Want to get involved in the dissection? The event will take place on 19 April 2020 at Bangor University, Prichard Jones Hall, 56 College Rd, Bangor, LL57 2AP

STUDENT TICKET 35.00 This ticket is for students at any university in the UK. Student ID will be required. The price includes the booking fee.

STANDARD TICKET 45.00 This ticket is for non-students, academics and healthcare staff wishing to attend as a refresher. The basket price includes the booking fee.

https://www.thevivitexperience.co.uk/tickets

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VIVIT the Live autopsy experience is returning to Bangor - The Bangor Aye

Dr Javed Butler on Importance of Diabetes Can Break Your Heart Initiative for American Heart Month – AJMC.com Managed Markets Network

Diabetes Can Break Your Heart is an important initiative that highlights the vital need for heightened education on the link between diabetes and heart failure, especially with American Heart Month looming, said Javed Butler, MD, MPH, MBA, professor of physiology and chairman for the Department of Medicine at the University of Mississippi.

Diabetes Can Break Your Heart is an important initiative that highlights the vital need for heightened education on the link between diabetes and heart failure, especially with American Heart Month looming, said Javed Butler, MD, MPH, MBA, professor of physiology and chairman for the Department of Medicine at the University of Mississippi.

Transcript

What makes Diabetes Can Break Your Heart a unique awareness initiative as were approaching February 2020, Heart Awareness Month?

The reason why I am very excited about this initiative is because of its importance, and the reason why this initiative is very important is because 1, diabetes is common, risk for heart failure is commonwe can do a lot to prevent the risk of heart failure; but the bigger issue is that there have been a lot of attempts over the years to educate people about the risk of heart attack and what we can do. So, the medical community is engaged in this dialogue.

Right now, almost the entire medical community is not particularly engaged or knowledgeable about prevention of heart failure, and only the cardiology community is really engaged right now in the treatment of heart failure; but the problem is that most of these patients are in other settings. So, the reason why this initiative is really important is because we need to educate the primary care physicians, primary care nurses, nephrologists, endocrinologistsall of these patients that touch the lives of patients with diabetes. There is an interaction, along with the cardiology community also, for prevention as well.

Then, the timing of this initiative is beautiful. February is Heart Month, so that is great, we're just starting right about that time, so that we can perhaps link the 2 things together.

What stakeholder groups are taking part of Diabetes Can Break Your Heart, and how will these groups carry the message?

There are multiple stakeholders that we need to be engaged in this initiative. This is not 1 particular kind of doctor or nurse, sub specialist, or patientI think it's really pretty much all. So, number 1, to start with the patients themselves. So, patients who have diabetes, they need to know the message so that they can go and ask their clinicians the right questions, and not ignore their symptoms.

One thing is that if you have a heart attack and you have severe chest pain, you're not likely going to ignore it; but if you are a little bit short of breath, a little bit tired, a little bit more fatigued, a lot of the people for a very long time can ignore those symptoms saying: maybe it's my weight, maybe I'm getting olderthey change their expectations.

So, first is to go to the patients, families, and caregivers to realize these symptoms early and go and talk to the clinicians. The second is the medical community doctors, nurses, and other medical communitieslocal nonprofits that are involved in healthcare, local leaders in the community involved in healthcare, maybe local governments that are involved in healthcare. All of these, we need to sort of weave into this thing.

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Dr Javed Butler on Importance of Diabetes Can Break Your Heart Initiative for American Heart Month - AJMC.com Managed Markets Network

Blood Pressure Changes Appear To Progress Earlier And Faster In Women Than In Men: Study – DocWire News

An new analysis suggests, contrary to conventional thinking, that sex-specific changes in lifetime blood pressure trajectory may actually progress more rapidly and present differently in women compared to men.

The analysis, published in JAMA Cardiology, contrasted with the common belief that women lag behind men by one or two decades for the development of vascular disease. The authors said that this can create a scenario where women, whose blood pressure trajectories can differ relative to men, can present differently later on in life with cardiovascular disease.

If we assume that women and men exhibit variations of the same fundamental vascular physiology, then conventional analyses of subclinical measures would suggest that women catch up to men by midlife in the extent of potentially important vascular disease, the researchers wrote in their study. Alternatively, under the assumption that vascular physiology may fundamentally differ between women and men, a sex-specific analysis of existing data could offer new insights and augment our understanding of sex differences in cardiovascular diseases.

The authors conducted a sex-specific analysis of blood pressure measures over a period of 43 years (1971 to 2014) in four community-based studies in the United States. Over 32,000 participants were included in the sample, 17,733 of whom were women (54%). The study outcomes of interest included changes in primary blood pressure [systolic, diastolic, mean arterial pressure (MAP) and pulse pressure (PP)] compared to baseline, as well as new-onset cardiovascular events.

According to the study results, women exhibited steeper increases in blood pressure in the third decade, which the authors reported continued through life (likelihood ratio test 2=531 for systolic BP; 2=123 for diastolic BP; 2=325 for MAP; and 2=572 for P; P<0.001 for all measures). These differences persisted between sexes even after adjusting for multiple cardiovascular disease (likelihood ratio test 2=314 for systolic BP; 2=31 for diastolic BP; 2=129 for MAP; and 2=485 for PP; P<0.001 for all measures).

In contrast with the notion that important vascular disease processes in women lag behind men by 10 to 20 years, sex-specific analyses indicate that blood pressure measures actually progress more rapidly in women than in men, beginning early in life. This early-onset sexual dimorphism may set the stage for later-life cardiovascular diseases that tend to present differently, not simply later, in women compared with men.

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Blood Pressure Changes Appear To Progress Earlier And Faster In Women Than In Men: Study - DocWire News

Looking for answers in the circadian rhythm – The Week Magazine

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Long before Apple watches, grandfather clocks or even sundials, nature provided living things with a way to tell time.

Life evolved on a rotating world that delivered alternating light and darkness on a 24-hour cycle. Over time, cellular chemistry tuned itself to that rhythm. Today, circadian rhythms governed by a master timekeeper in the brain guide sleeping schedules and mealtimes and influence everything from diet to depression to the risk of cancer. While an Apple watch can monitor a few vital functions such as your heart rate, your body's natural clock controls or affects nearly all of them.

"Circadian rhythms impact almost every aspect of biology," says neuroscientist Joseph Takahashi of the University of Texas Southwestern Medical Center.

Lately, research by Takahashi and others has suggested strategies for manipulating the body's clock to correct circadian-controlled chemistry when it goes awry. Such circadian interventions could lead to relief for shift workers, antidotes for jet lag, and novel treatments for mood disorders and obesity, not to mention the prospect of counteracting aging.

Prime weapons for the assault on clock-related maladies, Takahashi believes, can be recruited from an arsenal of small molecules, including some existing medical drugs.

"Researchers are increasingly interested in developing small molecules to target the circadian system directly for therapeutic gains," Takahashi and coauthors Zheng Chen and Seung-Hee Yoo wrote in the 2018 Annual Review of Pharmacology and Toxicology.

In sophisticated life-forms (such as mammals), central control of the body's clock resides in a small cluster of nerve cells within the brain's hypothalamus. That cluster, called the suprachiasmatic nucleus SCN for short is tuned to the day-night signal by light transmitted via the eyes and the optic nerve.

But the SCN does not do the job alone. It's the master clock, for sure, but satellite timekeepers operate in all kinds of cells and body tissues.

"There isn't just an SCN clock in the brain," Takahashi said at a recent meeting of the Society for Neuroscience. "There are clocks throughout the entire body. Every major organ system has its own intrinsic clock."

The proliferation of clocks throughout the body makes circadian chemistry relevant to various behaviors and physiological processes, such as metabolism and blood flow. Maintaining healthy physiology requires all the body's various clocks to be synchronized by signals (in the form of hormones and nerve impulses) from the SCN. SCN signals govern the timing of genetic activity responsible for the production of numerous clock-related proteins. Studies mainly in mice have shown how those proteins participate in complex chemical feedback loops, perpetuating rhythmic genetic activity in which proteins are first produced and then degraded to drive circadian cycles. Similar chemistry operates in humans.

Key molecular players in keeping the body's clocks ticking are the proteins known as CLOCK and BMAL1. Studies of liver cells in mice show that CLOCK partners with BMAL1 to regulate gene activity, driving all the important circadian chemical reactions. "Generally in many cells you see a similar kind of picture, in the brain or other tissues," Takahashi said.

The CLOCK-BMAL1 tandem activates genes that produce several forms of the circadian proteins period and cryptochrome. In mice, that process starts work in daytime, leading to a substantial buildup of period (PER) and cryptochrome (CRY) by evening. At night, PER and CRY migrate into the cell's nucleus and block the action of CLOCK-BMAL1, thereby halting production of PER and CRY themselves. PER and CRY amounts then diminish as other molecules degrade them. By morning, PER and CRY levels drop so low that CLOCK and BMAL1 are no longer disabled and can begin producing PER and CRY anew.

Many other molecules participate in circadian chemistry; the exact molecular participants differ from tissue type to tissue type. In the (mouse) liver alone, the activity of thousands of genes fluctuates on a circadian schedule.

An hourglass uses the flow of sand to mark time. The body uses the build-up and flow of proteins to keep its rhythms. Although there are numerous different players in the bodys many clocks, the workings of the circadian proteins period (PER) and cryptochrome (CRY) (and their counterparts CLOCK and BMAL1) exemplify the kind of feedback loop that keeps the body in sync with the day-night cycle.

While signals from the SCN set the daily schedule for circadian chemistry, various small molecules, such as many medicinal drugs, can disrupt cellular timing. (That's one reason certain drugs such as blood thinners and chemotherapy treatments are more or less effective depending on the time of day that they are administered.) Researchers have identified dozens of small molecules that can influence circadian processes.

Some such molecules change the length of the circadian period. Some alter the precise timing of specific processes during the cycle. Others help maintain robust signals for synchronizing the body's clocks. Circadian signaling weakens with age, possibly contributing to many age-related disorders such as impaired metabolism or sleep problems.

Among the common drugs that exert effects on the circadian system are opsinamides, sulfur-containing compounds that suppress the amount of light input into the SCN. Nobiletin, found in the peels of citrus fruits, manipulates circadian rhythms to improve metabolism in obese mice. (Nobiletin also counters tumors and inflammation.) Resveratrol is a well-known compound that alters the activity of certain clock genes, with some possible human health benefits.

Scientists have discovered a long list of existing medicines and small molecules now under investigation that act on or influence the bodys circadian system.

Today's challenge, Takahashi and coauthors say, is to identify the precise targets where small molecules exert their influence. Knowing the targets should help researchers find ways to repair defects in the circadian system or alleviate temporary inconveniences such as jet lag.

Jet lag occurs when sudden changes in time zone generate a mismatch between the body clock's expectations and the actual day-night cycle (not to mention timing of meals and social activities). While it is usually just an annoyance for travelers, shift workers face long-term consequences for working when the body clock advises sleep. Shift workers, Chen, Yoo, and Takahashi point out, are at risk for sleep problems, gastrointestinal disorders, obesity, cardiovascular disease, cancer and mood disorders. Molecules tested in mice have shown promise for reconciling expectations with reality, getting the clock back in phase with the body's environment.

Clock malfunction also affects the body's disease-fighting immune system, and certain clock components have been identified as potential targets for alleviating autoimmune disease and excessive inflammation. Other recent studies have shown that molecular intervention with clock components can aid proper functioning of mitochondria, the cellular structures responsible for energy production.

While most of the details about circadian chemistry come from studies in mice, studies of human sleep disorders indicate that the basic circadian story is similar in people. A mutation in the human gene responsible for making one of the period proteins has been linked, for example, to familial advanced sleep phase disorder. (In people with that mutation, the normal sleep-wake cycles shift by several hours.) Other research has shown that a variant version of the human gene for cryptochrome protein increases the risk of diabetes.

An especially intriguing possibility is that body clock management could provide strategies for slowing down aging.

Many studies have shown that aging in some animals can be slowed by restricting food intake. Fewer calories can lead to longer lives. But work by Takahashi and others has found that (in mice, at least) timing of ingesting the calories can be almost as important as the quantity.

Mice allowed to eat a normal amount of calories, but only within restricted hours, have lived about 15 percent longer than usual, Takahashi reported at the neuroscience meeting. In humans, that would correspond to a life span increase from 80 years to 92.

"We're super excited about these results, because these are the first experiments to show that you can extend life span by restriction of time of nutrient intake only without a reduction of calories," Takahashi said.

"For us it's much easier to restrict the time that we eat than the amount that we eat. Now if you can do both, that's even better. I think that this, I hope, could have benefit for human health and longevity in the future."

This article originally appeared in Knowable Magazine, an independent journalistic endeavor from Annual Reviews. Sign up for the newsletter.

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Looking for answers in the circadian rhythm - The Week Magazine

Exercise Training and Fasting: Current Insights | OAJSM – Dove Medical Press

Hassane Zouhal, 1 Ayoub Saeidi, 2,* Amal Salhi, 3,* Huige Li, 4 M Faadiel Essop, 5 Ismail Laher, 6 Fatma Rhibi, 1 Sadegh Amani-Shalamzari, 2 Abderraouf Ben Abderrahman 7

1M2S (Laboratoire Mouvement, Sport, Sant), University of Rennes, Rennes F-35000, France; 2Department of Exercise Physiology, Faculty of Physical Education & Sports Science, Kharazmi University, Tehran, Iran; 3Department of Medicine Physical and Functional Rehabilitation of the National Institute of Orthopedics M.T. Kassab, Tunis, Tunisia; 4Department of Pharmacology, Johannes Gutenberg University Medical Center, Mainz, Germany; 5Cardio-Metabolic Research Group (CMRG), Department of Physiological Sciences, Stellenbosch University, Stellenbosch 7600, South Africa; 6Department of Anesthesiology, Pharmacology & Therapeutics, Faculty of Medicine, The University of British Columbia, Vancouver, Canada; 7Higher Institute of Sport and Physical Education, Ksar-Said, University of Manouba, Manouba, Tunisia

*These authors contributed equally to this work

Correspondence: Hassane ZouhalM2S (LaboratoireMouvement, Sport, Sant), University of Rennes, EA 1274, Rennes F-35000, FranceEmail hassane.zouhal@univ-rennes2.fr

Abstract: Fasting is defined as the abstinence from consuming food and/or beverages for different periods of time. Both traditional and modern healthcare systems recommend fasting as a therapeutic intervention for the management of several chronic, non-infectious diseases. Exercising during a fasting state increases lipolysis in adipose tissue while also stimulating peripheral fat oxidation, resulting in increased fat utilization and weight loss. A key focus of this review is to assess whether endurance training performed while fasting induces specific training adaptations, where increased fat oxidation improves long-term endurance levels. Fasting decreases body weight, lean body and fat content in both trained and untrained individuals. Several studies indicate a broader impact of fasting on metabolism, with effects on protein and glucose metabolism in sedentary and untrained subjects. However, there are conflicting data regarding the effects of fasting on glucose metabolism in highly trained athletes. The effects of fasting on physical performance indicators also remain unclear, with some reporting a decreased performance, while others found no significant effects. Differences in experimental design, severity of calorie restriction, duration, and participant characteristics could, at least in part, explain such discordant findings. Our review of the literature suggests that there is little evidence to support the notion of endurance training and fasting-mediated increases in fat oxidation, and we recommend that endurance athletes should avoid high intensity training while fasting.

Keywords: fasting state, calorie restriction, metabolic adaptation fat oxidation, glucose metabolism, endurance performance, Ramadan

This work is published and licensed by Dove Medical Press Limited. The full terms of this license are available at https://www.dovepress.com/terms.php and incorporate the Creative Commons Attribution - Non Commercial (unported, v3.0) License.By accessing the work you hereby accept the Terms. Non-commercial uses of the work are permitted without any further permission from Dove Medical Press Limited, provided the work is properly attributed. For permission for commercial use of this work, please see paragraphs 4.2 and 5 of our Terms.

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Has the Average Human Body Temperature Always Been the Same? – Livescience.com

98.6. Why does that number ring a bell?

For years, the figure has held an important place in hospital rooms and physiology textbooks: 98.6 degrees Fahrenheit (37 degrees Celsius) is widely considered to be the "normal" average human body temperature.

But is this temperature still accurate? New research suggests the average American body temperature has dropped, and researchers think they know why.

Related: Why Does Being in the Heat Make Us Feel Tired?

A German physician named Carl Reinhold August Wunderlich was the first to crunch the 98.6 degrees number in 1851 after collecting millions of temperatures from about 2,500 patients in the city of Leipzig. "He took temperatures of everybody he could find, whether they were healthy sick, and he wrote a large book on temperature variation with illness," said study senior researcher Dr. Julie Parsonnet, a professor of medicine and of health research and policy at Stanford University. Wunderlich's work also highlighted temperature variations between people of different sexes, ages, weights and heights.

"Almost everything he said was correct," Parsonnet told Live Science. "He must have been sitting there with a pen, paper and pencil for an awful long time with all those temperatures."

Since Wunderlich's pioneering efforts, doctors still use body temperature as a key vital sign to help determine a person's health status. We now know that body temperature fluctuates as much as 0.5 F (0.2 C) throughout the day; that young people generally stay warmer than elderly people; and that women tend to maintain a higher temperature than men, depending on where they are in their menstrual cycles, according to a 2019 report in the journal Open Forum Infectious Diseases. Our body temperature also varies with the weather, our level of physical activity and whether we've eaten recently.

But why is it that, in general, the human body tends to hover around 98.6 degrees?

Evidence suggests that the body maintains a relatively stable temperature in order to keep its many organs and chemical reactions running smoothly, and potentially keep fungal infections at bay. But, according to the new study, published Jan. 7 in the journal eLife, the ideal body temperature may no longer be 98.6 F.

Rather, the average body temperature among Americans has dropped about 0.05 F (0.02 C) every decade since the early 1800s, the researchers found. American men born in the 2000s measure an average 1.06 F (0.58 C) cooler than men born in the early 1800s. Women born in the 2000s measure about 0.58 F (0.32 C) cooler than women born in the 1890s. The big question is, why?

As an infectious disease researcher, Parsonnet has spent many years studying a bacterial disease caused by the microorganism Helicobacter. The bug causes open sores called ulcers in the esophagus, stomach and small intestine and raises affected people's risk of developing gastric cancers. Over the years, though, Helicobacter infections have become less common in the U.S.

"I became aware, because I worked on it for 30 years, that that organism is disappearing from populations in the United States," Parsonnet said. The change reflects a larger trend; compared with our 19-century relatives, modern humans catch far fewer infectious diseases. People who lived through the 1800s were plagued with recurrent malaria, chronic wounds, tuberculosis, never-ending dental disease and bouts of dysentery, Parsonnet said.

Related: Why Is Humidity So Uncomfortable?

Today, we don't have all these bugs swimming through our bodies and revving our immune systems into overdrive. Parsonnet wondered how the loss of these microorganisms has altered human physiology through time.

To find out, Parsonnet and her co-authors dug through the data, including data sets from the American Civil War, the 1970s and the early 2000s. With these data sets combined, the researchers accrued more than 677,000 temperature measurements to examine.

The team spotted a steady drop in average human body temperature through the years. To rule out the possibility that improved thermometer technology had skewed the data, the researchers also looked for trends within each individual data set. Sure enough, the cooling trend appeared in each, regardless of the thermometer used by each historical group.

"We as human beings have evolved over time physiologically changed," Parsonnet said. "We've changed from who we were in the 19th century, and who we were in the 1960s, to a different human today that's colder."

The findings echo the results of a 2017 study conducted in England that analyzed about 250,000 temperature measurements from more than 35,000 patients. The average temperature among the British patients measured about 97.88 F (36.6 C), down a significant fraction from the "normal" average temperature of 98.6 F (37 C). Although humankind seems to be growing cooler by the decade, what does this actually mean for our physiology?

It's still a mystery, Parsonnet said. "We don't really understand what this cooling means in humans, what it means to our health, what it means to our longevity," she said.

Perhaps our decreased body temperature likely reflects the historical decline in infectious disease rates a trend that reduced excess inflammation in the human body to a significant degree, the researchers wrote in the study. Inflammation produces proteins called cytokines that ramp up the body's metabolic rate, thus generating heat.

Related: Why Do I Sweat So Much?

Additionally, unlike our ancestors, many people now live in a largely temperature-controlled world. "We don't have to work very hard to maintain our body temperature; it's always 70 F (21.1 C) in our houses," Parsonnet said.

Of course, it may be that people living in regions beyond the U.K. and the U.S. maintain entirely different body temperatures. For example, a 2008 study determined that the average body temperature in Pakistan still hovers around 98.6 F. However, these slight temperature differences between populations likely don't alter how our bodies function, physiologically, Parsonnet said.

"It might affect how microbes function, [but] I don't think we know the answers to those questions at all," she said. On the level of individuals, only extreme temperature changes signal worrisome health issues, such as fever or hypothermia. On a grand scale, though, average body temperatures may continue to fall as medicine advances and life expectancy increases, Parsonnet added.

Body temperature is "a marker of inflammatory state. And if you can take the temperature of a population, you might be able to predict their life expectancy," she noted. Parsonnet added that, someday, both life expectancy and body temperature will likely level off and remain consistent into the future.

Originally published on Live Science.

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Has the Average Human Body Temperature Always Been the Same? - Livescience.com

Who is Ivan Pavlov and What Did He Do for the Field of Psychology? – The Good Men Project

Ivan Pavlov was a Russian physiologist who discovered classical conditioning. He did a large amount of research on dogs and how they reacted to stimuli. He noticed that when he rang a bell, and there was food available, the dog would salivate. This is known as classical conditioning. Classical conditioning is something that many psychology students study, and its revolutionized the field of psychology. In psychology programs all around and outside of the United States, students learn about Ivan Pavlovs famous experiments in class.

Pavlov won the 1904 Nobel prize in physiology. He coined classical conditioning and researched digestion and physiology. At the beginning of his career, he studied religion, and then he moved to Science. In 1870, he started studying natural sciences while attending St. Petersburg University. Pavlov was primarily interested in physiology and natural science. He was instrumental in founding the department of physiology at the Institute of Experimental Medicine. Pavlov went on to oversee that department for 45 years.

When Pavlov was researching dog digestion, he found that a dog would salivate right before they got food. There were many stimuli presented to the dog. Pavlov determined that before he rang a bell after affiliating its sound with the presentation of food over some time, theyd notably salivate when they heard the bell, which meant that they were conditioned to affiliate the sound with food over time. This became a primary example of classical conditioning. He was awarded for this work, and in 1901, he was appointed to the Russian Academy of Sciences, three years before he won the Nobel Prize in Physiology.

Pavlov was not a psychologist, and in fact, he disliked psychology, but his work had a supreme impact on the field. His work influenced behaviorism. One of the earliest published works by Pavlov was the work of the digestive glands, and that was centered around his physiology research with dogs. He didnt intend to influence the world of psychology, but with his work regarding classical conditioning, great strides were made in the field.

In Pavlovs famous experiment when the dogs found the association between hearing the bell sound and the food, he called the bell conditioned stimulus because the signal served as a stimulation for behavior and he called the salivation a conditioned response because the salivated was the dogs response to the sound of the bell. It was determined that not only do dogs respond to stimuli in this way, but humans do, too. Pavlovs discovery of conditioned stimulus conditioned response, and spontaneous recovery taught us a lot about how our brains affiliate things with one another and how we can train our minds using this knowledge about how conditioning works. One common example of how we can implement this in our daily lives is in reward-punishment systems used by both children and adults. For instance, if a parent provides a child with a toy or sticker when they behave well, the child will be conditioned to affiliate good behavior with receiving a reward.

Therapy is a great place to learn about the modern applications of classical conditioning. Individuals frequently go to therapy to work on behavior or thought processes, and while the field has developed substantially since Pavlovs time, he had a significant influence on what we know and use in counseling today. Whether you see an online therapist or someone in your local area, you can gain insight in therapy thatll help you learn more about yourself and others.

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Who is Ivan Pavlov and What Did He Do for the Field of Psychology? - The Good Men Project