Abstract
Celiac disease (CeD) affects about 1% of most world populations. It presents a wide spectrum of clinical manifestations, ranging from minor symptoms to mild or severe malabsorption, and it may be associated with a wide variety of autoimmune diseases. CeD is triggered and maintained by the ingestion of gluten proteins from wheat and related grains. Gluten peptides that resist gastrointestinal digestion are antigenically presented to gluten specific T cells in the intestinal mucosa via HLA-DQ2 or HLA-DQ8, the necessary genetic predisposition for CeD. To date, there is no effective or approved treatment for CeD other than a strict adherence to a gluten-free diet, which is difficult to maintain in professional or social environments. Moreover, many patients with CeD have active disease despite diet adherence due to a high sensitivity to traces of gluten. Therefore, safe pharmacological treatments that complement the gluten-free diet are urgently needed. Oral enzyme therapy, employing gluten-degrading enzymes, is a promising therapeutic approach. A prerequisite is that such enzymes are active under gastro-duodenal conditions, quickly neutralize the T cell activating gluten peptides and are safe for human consumption. Several enzymes including prolyl endopeptidases, cysteine proteases and subtilisins can cleave the human digestion-resistant gluten peptides in vitro and in vivo. Examples are several prolyl endopeptidases from bacterial sources, subtilisins from Rothia bacteria that are natural oral colonizers and synthetic enzymes with optimized gluten-degrading activities. Without exception, these enzymes must cleave the otherwise unusual glutamine and proline-rich domains characteristic of antigenic gluten peptides. Moreover, they should be stable and active in both the acidic environment of the stomach and under near neutral pH in the duodenum. This review focuses on those enzymes that have been characterized and evaluated for the treatment of CeD, discussing their origin and activities, their clinical evaluation and challenges for therapeutic application. Novel developments include strategies like enteric coating and genetic modification to increase enzyme stability in the digestive tract.
Highlights
Celiac Disease (CeD) is the most common food-induced heritable and life-long inflammatory disease in humans
Celiac disease (CeD) is triggered upon ingestion of wheat gluten or similar proteins found in other cereals such as barley and rye
CeD and the associated autoimmune diseases are linked to common and necessary genetic predisposition, human lymphocyte antigen
Summary
Celiac Disease (CeD) is the most common food-induced heritable and life-long inflammatory disease in humans. CeD is characterized by flattening of the proximal intestinal villi and crypt hyperplasia resulting in a loss of resorptive surface area This frequently causes malabsorption of nutrients, vitamins and minerals and increases the risk of anemia, osteoporosis, infertility, otherwise rare small intestinal cancers and a wide spectrum of autoimmune diseases. CeD and the associated autoimmune diseases are linked to common and necessary genetic predisposition, human lymphocyte antigen This drives an inflammatory T helper 1 (Th1) cell response resulting in villous atrophy and usually in clinical disease.
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