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Aggressor cells, which have the potential to cause
autoimmunity, are targeted by treatment, causing conversion of these cells to
protector cells. Gene expression changes gradually at each stage of treatment,
as illustrated by the color changes in this series of heat maps.
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Scientists have made an important breakthrough in the fight against debilitating autoimmune diseases such as multiple sclerosis by revealing how to stop cells attacking healthy body tissue.
Rather than the body's immune system destroying its own
tissue by mistake, researchers at the University of Bristol have discovered how
cells convert from being aggressive to actually protecting against disease.
The study, funded by the Wellcome Trust, is published in
Nature Communications.
It's hoped this latest insight will lead to the widespread
use of antigen-specific immunotherapy as a treatment for many autoimmune
disorders, including multiple sclerosis (MS), type 1 diabetes, Graves' disease
and systemic lupus erythematosus (SLE).
MS alone affects around 100,000 people in the UK and 2.5
million people worldwide.
Scientists were able to selectively target the cells that
cause autoimmune disease by dampening down their aggression against the body's
own tissues while converting them into cells capable of protecting against
disease.
This type of conversion has been previously applied to
allergies, known as 'allergic desensitisation', but its application to
autoimmune diseases has only been appreciated recently.
The Bristol group has now revealed how the administration of
fragments of the proteins that are normally the target for attack leads to
correction of the autoimmune response.
Most importantly, their work reveals that effective
treatment is achieved by gradually increasing the dose of antigenic fragment
injected.
In order to figure out how this type of immunotherapy works,
the scientists delved inside the immune cells themselves to see which genes and
proteins were turned on or off by the treatment.
They found changes in gene expression that help explain how
effective treatment leads to conversion of aggressor into protector cells. The
outcome is to reinstate self-tolerance whereby an individual's immune system
ignores its own tissues while remaining fully armed to protect against
infection.
By specifically targeting the cells at fault, this
immunotherapeutic approach avoids the need for the immune suppressive drugs
associated with unacceptable side effects such as infections, development of
tumours and disruption of natural regulatory mechanisms.
Professor David Wraith, who led the research, said:
"Insight into the molecular basis of antigen-specific immunotherapy opens
up exciting new opportunities to enhance the selectivity of the approach while
providing valuable markers with which to measure effective treatment. These
findings have important implications for the many patients suffering from
autoimmune conditions that are currently difficult to treat."
This treatment approach, which could improve the lives of
millions of people worldwide, is currently undergoing clinical development
through biotechnology company Apitope, a spin-out from the University of
Bristol.
Story Source:
The above post is reprinted from materials provided by
University of Bristol. Note: Materials may be edited for content and length.
Journal Reference:
Bronwen R. Burton, Graham J. Britton, Hai Fang, Johan
Verhagen, Ben Smithers, Catherine A. Sabatos-Peyton, Laura J. Carney, Julian
Gough, Stephan Strobel, David C. Wraith. Sequential transcriptional changes
dictate safe and effective antigen-specific immunotherapy. Nature
Communications..
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