Islamabad, Dec 18: A new study provides fascinating insight into the underlying
pathology associated with the autoimmune disease, systemic lupus erythematosus
(SLE).
The research, published by Cell Press in the journal Immunity,
reveals an unexpected role for a key type of immune cell and provides a
potential new therapeutic strategy for SLE and, potentially, other autoimmune
diseases.
SLE is a chronic systemic disease that can affect many regions
of the body and, as a result, presents with diverse clinical symptoms. As is
characteristic of other autoimmune disease, in SLE the immune system attacks and
damages the body's own cells and tissues. Previous research had shown that SLE
is associated with activation of the two main parts of the adaptive immune
system, B cells and T cells.
"We were interested in examining the
contribution of another type of immune cell, the dendritic cell (DC), to SLE
pathology," explains senior study author Dr. Mark J. Shlomchik from Yale
University School of Medicine in New Haven, Connecticut. "DCs initiate and
control the adaptive immune response to infection and have the potential to
influence SLE in many different ways."
Dr. Shlomchik and colleagues
deleted DCs in a mouse model of SLE and observed that although DCs contributed
to the expansion and differentiation of T cells, they were surprisingly not
required for the initial activation of T cells. These findings were unexpected
because it is well established that DC cells initiate the T and B cell immune
response to pathogens. Alternatively, DCs were very important for the invasion
of target organs by inflammatory cells, including T cells. SLE-prone mice
lacking DCs had markedly reduced kidney and skin disease. DCs also markedly
affected the quantity and quality of the classic autoantibody response
associated with lupus.
Taken together, the observations indicate that the
way DC cells function in autoimmune disease is quite different from their role
in the immune response to pathogens. "Our findings reveal that DCs operate not
to initiate but rather to amplify disease in a mouse model of lupus which is in
contrast to how they are thought to work in response to infection," concludes
Dr. Shlomchik.
"Although there is much more work to do in defining the
roles of DCs in autoimmunity our current data validate DCs as a potential new
therapeutic target in autoimmunity as well as point to future studies to
determine how DCs promote local tissue inflammation and to test if depleting DCs
will be therapeutic during disease."
Ends
SA/EN
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Immune cell plays unexpected role in autoimmune disease
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