Team:Washington/Celiacs

From 2011.igem.org

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This is where some stuff about Celiacs should go.
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Celiac disease is a genetic autoimmune disorder of the small intestine. For the 2 million people in the United States with celiac disease, the presence of gliadin and similar prolamines (parts of gluten) in the small intestine causes an inappropriate T cell-mediated response against ingested gluten. This results in intestinal damage, most notably inflammation, the loss of absorptive villi, and hyperplasia of the crypts. This damage to the small intestine causes malabsorption of nutrients due to the loss of villi. More visible symptoms could include diarrhea, fatigue, and weight loss. This autoimmune reaction is caused by a failure of the tight-junction system between the intestine and the immune system; a genetic defect could let undigested, immune-system-sensitive gluten proteins create a reinforcing immune response.
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Currently, the only known therapy for celiac disease is the complete avoidance of gluten-containing foods. However, research on this disorder has found enzymes capable of breaking apart gluten using prolyl endopeptidases (PEPs), which are able to cleave at internal proline residues in proteolytically resistant gluten epitopes. Unfortunately, such enzymes only produce catalytic activity at relatively neutral pH, like that of the small intestine; this would allow gluten to simultaneously react with the immune system, and could still trigger an inflammatory response. An optimal mutant PEP would be able to conduct its activity at low pH in the stomach to prevent the opportunity for inflammation.

Revision as of 05:34, 4 September 2011


Celiac disease is a genetic autoimmune disorder of the small intestine. For the 2 million people in the United States with celiac disease, the presence of gliadin and similar prolamines (parts of gluten) in the small intestine causes an inappropriate T cell-mediated response against ingested gluten. This results in intestinal damage, most notably inflammation, the loss of absorptive villi, and hyperplasia of the crypts. This damage to the small intestine causes malabsorption of nutrients due to the loss of villi. More visible symptoms could include diarrhea, fatigue, and weight loss. This autoimmune reaction is caused by a failure of the tight-junction system between the intestine and the immune system; a genetic defect could let undigested, immune-system-sensitive gluten proteins create a reinforcing immune response. Currently, the only known therapy for celiac disease is the complete avoidance of gluten-containing foods. However, research on this disorder has found enzymes capable of breaking apart gluten using prolyl endopeptidases (PEPs), which are able to cleave at internal proline residues in proteolytically resistant gluten epitopes. Unfortunately, such enzymes only produce catalytic activity at relatively neutral pH, like that of the small intestine; this would allow gluten to simultaneously react with the immune system, and could still trigger an inflammatory response. An optimal mutant PEP would be able to conduct its activity at low pH in the stomach to prevent the opportunity for inflammation.