Events Calendar

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30 Mar
2020-03-30 - 2020-03-31    
All Day
This Cardio Diabetes 2020 includes Speaker talks, Keynote & Poster presentations, Exhibition, Symposia, and Workshops. This International Conference will help in interacting and meeting with diabetes and [...]
Trending Topics In Internal Medicine 2020
2020-04-02 - 2020-04-04    
All Day
Trending Topics in Internal Medicine is a CME course that will tackle the latest information trending in healthcare today.   This course will help you discuss options [...]
2020 Summit On National & Global Cancer Health Disparities
2020-04-03 - 2020-04-04    
All Day
The 2020 Summit on National & Global Cancer Health Disparities is planned with the goal of creating a momentum to minimize the disparities in cancer [...]
2020 Primary Care Kauai- Caring For The Active And Athletic Patient
2020-04-06 - 2020-04-10    
All Day
CMX Travel and Meetings programs meetings and group conferences for physicians and medical professionals throughout the United States. CMX Travel and Meetings programs meetings and [...]
ISER- 787th International Conference On Science, Health And Medicine ICSHM
2020-04-07 - 2020-04-08    
All Day
ISER- 787th International Conference on Science, Health and Medicine (ICSHM) is a prestigious event organized with a motivation to provide an excellent international platform for the academicians, [...]
RW- 801st International Conference On Medical And Biosciences ICMBS
2020-04-08 - 2020-04-09    
All Day
About the EventConference : RW- 801st International Conference on Medical and Biosciences ICMBS is a prestigious event organized with a motivation to provide an excellent [...]
Palliative Care 2020
2020-04-08 - 2020-04-09    
All Day
ABOUT PALLIATIVE CARE 2020 Palliative Care 2020 welcomes attendees, presenters, and exhibitors from all over the world to Dubai, UAE. We are glad to invite [...]
The 4th Annual Dubai International Paediatric Neurology Congress
2020-04-09 - 2020-04-11    
All Day
Based on the sound success of previous Dubai International paediatric Neurology congresses the 4th Annual Dubai International paediatric Neurology Conference expects to attract over 400 delegates devoted [...]
13 Apr
2020-04-13 - 2020-04-14    
All Day
IASTEM - 814th International Conference on Medical, Biological and Pharmaceutical Sciences (ICMBPS) will be held on 13th - 14th April, 2020 at Dammam, Saudi Arabia . ICMBPS is to bring together [...]
Patient Engagement USA At Eyeforpharma Philadelphia
2020-04-14 - 2020-04-15    
All Day
As we enter election year in 2020, the pressure has never been higher on our industry to justify what we add to the cost of [...]
28th International Conference On Clinical Pediatrics
2020-04-15 - 2020-04-16    
All Day
It is our great pleasure to invite you to participate in the 28th International Conference on Clinical Pediatrics Clinical Pediatrics 2020 which will take place [...]
5th World Congress On Public Health And Health Care Management
2020-04-16 - 2020-04-17    
All Day
We would like to invite you all people to take part in our Public Health and Health Care Management-2020 Conference in Miami, USA during 16-17 [...]
Topics In Emergency Medicine, Pain Management, And Palliative Care CME Cruise
2020-04-18 - 2020-04-25    
All Day
These set of lectures is designed to provide important updates in emergency medicine with a focus on anticoagulation and the management of venous thromboembolism as [...]
RW- 809th International Conference On Medical And Biosciences ICMBS
2020-04-19 - 2020-04-20    
All Day
RW- 809th International Conference on Medical and Biosciences (ICMBS) is a prestigious event organized with a motivation to provide an excellent international platform for the academicians, researchers, [...]
RF - 627th International Conference On Medical & Health Science - ICMHS 2020
2020-04-20 - 2020-04-21    
All Day
Welcome to the Official Website of the  627th International Conference on Medical & Health Science - ICMHS 2020. It will be held during 20th-21st April, 2020 at San [...]
30th Annual Art And Science Of Health Promotion Conference
2020-04-20 - 2020-04-24    
All Day
Integrating Health Promotion into the Organization’s and Community’s Core Values A common element of virtually every successful health promotion program in workplace, clinical and community [...]
ISER- 796th International Conference On Science, Health And Medicine ICSHM
2020-04-21 - 2020-04-22    
All Day
ISER- 796th International Conference on Science, Health and Medicine ICSHM is a prestigious event organized with a motivation to provide an excellent international platform for [...]
Biomolecular Condensates Summit
2020-04-21 - 2020-04-23    
All Day
An ever-increasing amount of evidence points towards the importance of Biomolecular Condensates function to health and disease. However, with many of the fundamental questions behind [...]
The Middle East Pharma Cold Chain Congress
2020-04-22 - 2020-04-23    
All Day
The pharma sector in the MENA region has witnessed rapid development, which has been largely fueled by high population growth, increased life expectancy coupled with [...]
45th Annual Regional Anesthesiology And Acute Pain Medicine Meeting
2020-04-23 - 2020-04-25    
All Day
ASRA was officially "re-founded" in 1975, led by Alon P. Winnie, MD, who had a dream of a society devoted to teaching regional anesthesia. (An [...]
25th International Conference on Dermatology & Skin Care
2020-04-27 - 2020-04-28    
All Day
About Conference Derma 2020 Derma 2020 welcomes all the attendees, lecturers, patrons and other research expertise from all over the world to 25th International Conference on Dermatology & [...]
Events on 2020-03-30
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Latest News

Scientists identify reversible molecular defect underlying rheumatoid arthritis

rheumatoid arthritis

In rheumatoid arthritis, immune cells called helper T cells behave differently from their counterparts in healthy cells and in other autoimmune diseases. Stanford scientists have learned why.

Stanford University School of Medicine investigators succeeded in countering inflammation and tissue damage caused by rheumatoid arthritis in mice engrafted with human joint-lining tissue and a human immune system.

The researchers accomplished this by shutting down a faulty molecular mechanism that they identified in humans with the disease.

lining tissue and a human immune system.

The researchers accomplished this by shutting down a faulty molecular mechanism that they identified in humans with the disease.

In addition, they found that a novel drug, which is not yet commercially available, helped protect both human cells in a dish and the humanized mice from rheumatoid arthritis. Clinical trials of the drug or a closely related compound could begin in the near future.

The findings were published online Feb. 4 in Nature ImmunologyCornelia Weyand, MD, PhD, professor and chief of immunology and rheumatology, is the senior author. The lead author is postdoctoral scholar Zhenke Wen, MD, PhD.

Rheumatoid arthritis is one of the most common autoimmune diseases, affecting about 1 percent of the population. It involves destruction of synovia, soft tissue that lubricates joints to prevent bones from scraping together. Whereas osteoarthritis is attributable to age-related wear and tear, rheumatoid arthritis results from a chronic attack on the synovia by cells of the body’s immune system. The inflammatory character of rheumatoid arthritis also causes systemic problems. For example, it doubles the risk of heart disease.

Existing rheumatoid-arthritis medications relieve symptoms but don’t actually eradicate  the disease by rectifying the behavior of the immune cells causing it, Weyand said. Why those cells go on the attack to begin with has been mysterious.

But Weyand’s team has clues. “We’ve learned that rheumatoid arthritis is, at root, a problem of faulty cell metabolism and, in particular, of one type of immune cell’s inappropriate diversion of resources from generating energy to the production of an army of inflammatory offspring,” she said. This cellular army exits the lymph nodes, makes its way to synovial tissues, takes up residence there and instigates the inflammatory damage that’s the hallmark of rheumatoid arthritis.

“We know how these immune cells fuel their bad behavior,” Weyand said. “And now we’ve shown we can reverse this behavior and make these cells behave as they should.”

Errant helper T cells

The errant cells are helper T cells. After infiltrating synovial tissue, they send out signals that call in other super-aggressive immune cells and cause ordinary synovial cells to become inflamed and destructive.

In prior work, Weyand’s group noticed telling differences between the helper T cells of patients with rheumatoid arthritis and those of healthy people. The former, for instance, have low reserves of a molecule called ATP, which serves as cell’s internal energy currency, accepted by all of a cell’s myriad metabolic enterprises. Yet instead of directing their primary energy source, glucose, toward ATP production, these cells divert their glucose supplies toward fashioning various materials — proteins, nucleic acids, membranes and the like — used to build new T cells that will contribute to further damage.

That shouldn’t happen. Like all cells, T cells contain AMPK, a regulatory molecule that senses ratios of ATP and its two main breakdown products. If it finds ATP too outnumbered by these breakdown products, AMPK clamps down on the T cell’s cell-building program and, instead, sends glucose off to the cell’s ATP-generating apparatus.

“When your house is cold, you need to throw your logs into your fireplace, not use them to build a new house in your backyard,” Weyand said.

The new study provides an answer to the question of why AMPK fails to perform its energy-monitoring function in the faulty helper T cells of patients with rheumatoid arthritis.

We know how these immune cells fuel their bad behavior. And now we’ve shown we can reverse this behavior and make these cells behave as they should.

To redirect glucose traffic from biosynthesis to internal energy production, AMPK must first be activated. This happens when a small chemical group gets tacked onto AMPK, starting it up like the ignition of a car. That, in turn, can occur only on the outer surface of vesicles called lysosomes.

Lysosomes have a reputation as cells’ garbage disposals because they’re full of cellular debris in the act of being recycled. But they’re more than that. Their membrane surfaces are dotted with all manner of receptors, channels, enzymes and other proteins. Only when AMPK perches on the lysosomal surface and seats itself in a large protein supercomplex there does it get activated and poised to shut down an ATP-deficient helper T cell’s biosynthetic materials-building apparatus and redirect glucose back to ATP production.

Weyand’s team obtained blood samples from 155 rheumatoid arthritis patients, an equivalent number of healthy subjects and a smaller number of patients with other autoimmune disorders. They extracted helper T cells from these samples and, analyzing them, found several striking differences.

Rheumatoid arthritis patients’ T cells had just as much AMPK as cells from healthy subjects or patients with other autoimmune diseases did. But their AMPK molecules weren’t getting activated. Nor were they as likely to turn up on lysosomal surfaces. AMPK molecules in these cells were also much less likely to feature molecules of a substance called myristic acid affixed to their back ends.

Rheumatoid-arthritis helper T cells also had much-reduced levels of the enzyme NMT1, whose job is to staple myristic acid “tails” to proteins’ back ends. These tails, Weyand and her colleagues found, act as anchors pinning AMPK to the lysosomal surface. Laboratory techniques that increased NMT1 levels in rheumatoid-arthritis helper T cells caused the cells’ secretions of inflammatory chemicals to drop. When injected into mice with human synovial tissue, unmodified helper T cells from rheumatoid arthritis patients caused severe damage to the human synovial tissue. But those with lab-enhanced levels of NMT1 produced far less inflammation or tissue damage.

An exploratory compound, A769662, that causes AMPK to become activated even when it’s just floating around in a cell’s cytoplasm rather than anchored to a lysosome reversed rheumatoid-arthritis helper T cells’ inflammatory output and their propensity to infiltrate and damage human synovial tissue in the mice, the study found.

Weyand said she expects to test the efficacy of the compound, or a derivative, among rheumatoid arthritis patients in a clinical trial, hopefully in the near future.

Weyand is a member of Stanford Bio-X, of the Stanford Institute for Immunity, Transplantation and Infection and of the Stanford Cardiovascular Institute.

Other Stanford-affiliated co-authors of the study are Stanford Shoor, MD, professor of immunology and rheumatology; Niall Roche, MD, a rheumatology specialist at Stanford Health Care-Valley Care; postdoctoral scholars Ke Jin, PhD, Yi Shen, PhD, Yinyin Li, PhD, and Bowen Wu, PhD; research associate Zhen Yang, PhD; Lu Tian, ScD, associate professor of biomedical data science; and Jorg Goronzy, MD, PhD, professor of immunology and rheumatology.

The work was funded by the National Institutes of Health (grants AR042547, AI108906, HL117913, HL129941, AI108891, AG045779, AI057266 and BX001669).

Stanford’s Department of Medicine also supported the work.

Source