Shadow proteins in thymus - Clues to how immune system works?
Findings could lead to new understanding of diabetes,
Crohns, and more
Researchers at Joslin Diabetes Center, Harvard Medical School, and other
institutions have identified the function of a protein, dubbed aire, that is
critical to helping immune cells learn to recognize--and avoid attacking--the
far-flung organs and tissues of the body. The protein appears to work by turning
on in the thymus, which lies beneath the breast bone, the production of a wide
array of proteins from the body's periphery. The discovery could shed light not
only on how the healthy immune system develops tolerance to its own proteins but
also how tolerance is lost, as it is in diabetes, rheumatoid arthritis, Crohn's
disease and other autoimmune illnesses.
"Our findings lead back to humans because they tell us about a very important
mechanism for controlling autoimmunity," said Diane Mathis, a Harvard Medical
School professor of medicine at Joslin. "At the same time, they may help us
understand why people develop autoimmune diseases." The findings are reported in
the Oct. 11 Science.
Until recently, immune cells, in particular T cells, were thought to learn
their most basic lesson--attack foreign proteins but spare those that are
native--in one of two places. Those with a broad mandate, namely to monitor
widely expressed cellular proteins or proteins circulating in the bloodstream,
were thought to be trained to distinguish self from foreign proteins while still
in the thymus. Cells that recognize proteins in organs and tissues in the
periphery, such as the pancreas, thyroid, and adrenals, were believed to learn
the self-vs.-nonself lesson once they left the thymus. This organ was thought
incapable of producing proteins made by distant organs such as the liver, brain,
and pancreas.
But it appears that T cells in training may be learning the lesson while
still in the thymus. Building on work of other groups, first author Mark
Anderson, a research fellow in medicine at Joslin; Emily Venanzi, a Harvard
Medical School graduate student in immunology; Christophe Benoist, a professor
of medicine at Joslin; Mathis, and colleagues, reported that a small network of
thymic cells, the medullary epithelial cells, expresses hundreds of genes
usually associated with organs such as the pancreas, brain, and liver.
"No one would think you would encounter your big toe protein in the thymus,
but in fact proteins from the eye, the liver, from all over the place are
specifically expressed in a small population of stromal cells in the thymus,"
said Benoist.
A majority of these expressed proteins are used by the peripheral organs to
tell T cells to stay away. Indeed, the researchers believe the proteins are used
in the thymus to foreshadow the very self-antigens that the T cells will
encounter once they travel out into the body. "There is a foretelling of these
proteins in the thymus, which is why we call it an immunological self-shadow,"
said Mathis.
In a critical step, the Joslin team discovered that the transcription factor
aire plays a critical role in producing these self-shadow proteins in the thymus
(hence its name, which is formed from two letters in each word of autoimmune
regulator). Mutant mice lacking aire exhibited in their thymus only a fraction
of the peripheral self-proteins found in the thymus of normal mice. And the
mutants exhibited widespread autoimmunity. In fact, their condition was
reminiscent of a condition found in humans carrying a defective AIRE gene,
autoimmune polyglandular syndrome.
It is not yet clear how the shadow proteins educate developing T cells inside
the thymus, though Benoist suspects the processes are similar to those used to
eliminate T cells that react to ubiquitous or circulating proteins. Nor is it
clear how aire controls the expression of so many shadow proteins. One
possibility is that it works by binding to other transcription factors. "It is
going to be interesting to figure out what the mechanism really is," she said.
While novel, the mechanism is probably only one of many that the immune
system uses to educate peripheral T cells about the self-vs.-foreign
distinction. "It is very dangerous for the immune system to have self-reactive T
cells," Anderson said. "It takes advantage of any mechanism to get rid of these
cells. So there is a whole net of mechanisms."
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Other main collaborators on this study were Ludger Klein from the DanaFarber
Cancer Institute and Roderick Bronson from Harvard Medical School.
Harvard Medical School has more than 5,000 full-time faculty working in eight
academic departments based at the School's Boston quadrangle or in one of 47
academic departments at 17 affiliated teaching hospitals and research
institutes. Those HMS affiliated institutions include Beth Israel Deaconess
Medical Center, Boston VA Medical Center, Brigham and Women's Hospital,
Cambridge Hospital, Center for Blood Research, Children's Hospital, Dana-Farber
Cancer Institute, Harvard Pilgrim Health Care, Joslin Diabetes Center, Judge
Baker Children's Center, Massachusetts Eye and Ear Infirmary, Massachusetts
General Hospital, Massachusetts Mental Health Center, McLean Hospital, Mount
Auburn Hospital, Schepens Eye Research Institute, Spaulding Rehabilitation
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