Advisory: Give yourself extra time when travelling by car to Toronto General Hospital, Princess Margaret Cancer Centre, or Toronto Rehab University Centre. City of Toronto construction on University Ave. may cause delays.
At UHN, we strive to deliver Compassionate Care & Caring. Learn more about the services and supports that are available to you throughout your journey.
Our UHN programs and services are among the most advanced in the world. We have grouped our physicians,
staff, services and resources into 10 medical programs to meet the needs of our patients and help us make
the most of our resources.
At the heart of everything we do at UHN are our Healthcare Professionals. Refer a patient to one of our 12 medical programs. Learn more about the resources and opportunities available for professional growth.
University Health Network has grown to be one of the largest research and teaching hospital networks in Canada - pioneers in improving the lives of patients. Our long history of health professions education at Toronto General, Toronto Western, Princess Margaret and Toronto Rehab hospitals has consistently advanced the science of education.
University Health Network is a health care and medical research organization in
Toronto, Ontario, Canada. The scope of research and complexity of cases at UHN has made us a national and international
source for discovery, education and patient care.
Being touched by illness affects us in different ways. Many people want to give back to the community
and help others. At UHN, we welcome your contribution and offer different ways you can help so you can find one that suits you.
The Newsroom is the source for media looking for information about UHN or trying to connect with one
of our experts for an interview. It's also the place to find UHN media policies and catch up on our news stories, videos, media releases,
podcasts and more.
Toronto (Oct. 20, 2021) – In a paper published today in the journal
Science Translational Medicine, researchers at the Schroeder Arthritis Institute, part of University Health Network (UHN) in Toronto, have made a discovery that could lead to new treatments for axial spondyloarthritis (SpA), a painful and debilitating form of arthritis which affects one per cent to two per cent of Canadians and causes inflammation in the spine, joints, eyes, gut and skin.
"We currently have very few therapeutic options for the majority of patients living with SpA and this is a devastating disease that directly impacts quality of life," says Dr. Nigil Haroon, a rheumatologist, co-Director of the Spondylitis Program and senior author on the paper.
"Although several treatments including biologic drugs have been approved for SpA, 40 per cent to 50 per cent of patients do not respond to any treatments and develop severe pain and abnormal new bone formation," says Dr. Akihiro Nakamura, first author on the paper and a spondylitis fellow and PhD candidate in Dr. Haroon's lab. "So, there is a desperate need to find new treatments that are effective and cover all of the clinical symptoms of SpA."
The study focuses on the role of the Macrophage migration inhibitory factor (MIF), which functions as a protein that induces an inflammatory or immune response in the body. Until now, the role that MIF plays in the disease progression of SpA was unknown.
In this study, researchers observed that the expression of MIF and its receptor CD74, is increased in the blood and tissues of pre-clinical models. They also found that human neutrophils (a type of white blood cell that induces the immune system's response) from SpA patients secreted higher concentrations of MIF, compared to healthy individuals. This, in turn, drives other cells to cause more inflammation.
"What this means is that if the body has been exposed to a trigger, too much MIF could be produced in susceptible individuals that could then lead to a diagnosis of SpA later in life. If we can block the excess production of MIF early, we may be able to induce disease remission and prevent disability and mortality linked to SpA," explains Dr. Haroon.
In a 2017 paper, the researchers found that the concentration or expression of MIF is substantially increased in the blood, joint fluids and gut tissues of SpA patients, compared to those of a different type of arthritis patients or healthy volunteers. In the same paper, they also demonstrated that MIF might be involved in promoting the development of new bone formation. These recent findings have helped to solidify those results and further our understanding of the role of MIF in SpA.
The specific blocker of MIF, called MIF098, successfully prevented and restricted the disease onset and development of SpA in the pre-clinical model. The team will focus now on testing the potential of other therapies targeting MIF, which could lead to finding a novel treatment in SpA.
"Patients with SpA experience inflammation, pain, stiffness and over time, this can lead to spinal fusion and loss of mobility. But it's not just the disease itself that these patients have to worry about," says Dr. Haroon. "Compared to the general population, there is also a 60 per cent increased chance of stroke and a 30 per cent increase that they may experience a cardiovascular event or a mental illness."
For Dr. Nakamura, a clinician from Japan who came to the Schroeder Arthritis Institute to become a leading researcher in the area of inflammatory arthritis, these new findings are nothing short of "exciting."
"In research, once we make a new discovery, that has the potential to help many more patients than I could in my clinic back in Japan," says Dr. Nakamura. "So that motivates me a lot."
Researchers are next hoping to test the efficacy of MIF blockers in patients with SpA through clinical trials, where they would look to determine the optimal concentration and administration frequency of MIF-targeted drugs for humans, as well as study potential side effects, to ensure safety.
"The drugs we have currently don't work for half of all SpA patients," says Dr. Haroon. "At the same time, rates of arthritis are going up worldwide. We believe this treatment could be effective for a good proportion of SpA patients, including those who don't respond to other currently available treatments."
This work is supported by the Canadian Institute of Health Research, Arthritis Society, Krembil Foundation, UHN Foundation, American College of Rheumatology (ACR) Research Fund, National Institutes of Health (NIH), Natural Sciences Research Council, Canada Foundation for Innovation (CFI), Ontario Research Fund, IBM, Ian Lawson van Toch Fund, Medicine by Design Program, MiTACS Accelerate Fellowship, Spondyloarthritis Research and Treatment Network (SPARTAN), and Spondyloarthritis Research Consortium of Canada (SPARCC).
Dr. Nigil Haroon acts as a consultant for Abbvie, Eli Lilly, Janssen, Novartis and UCB, none of whom have funded this study.
The Schroeder Arthritis Institute is the largest multidisciplinary arthritis hub in Canada, integrating medical, surgical and basic science aspects of Hand, Orthopaedics, Osteoporosis and Rheumatology, with a goal of making a global impact in discovery, learning and patient care. The Institute comprises 51 scientists and clinician-scientists, 113 trainees and 200 staff. The Schroeder Arthritis Institute is headquartered at Toronto Western Hospital, in downtown Toronto. For more information, visit: www.uhn.ca/arthritis
University Health Network consists of Toronto General and Toronto Western Hospitals, the Princess Margaret Cancer Centre, Toronto Rehabilitation Institute, and The Michener Institute of Education at UHN. The scope of research and complexity of cases at University Health Network has made it a national and international source for discovery, education and patient care. It has the largest hospital-based research program in Canada, with major research in arthritis, cardiology, transplantation, neurosciences, oncology, surgical innovation, infectious diseases, genomic medicine and rehabilitation medicine. University Health Network is a research hospital affiliated with the University of Toronto.
Phone: 416 340 4636