Celiac Disease Clinical Trial
— WHETMITOfficial title:
Wheat Flour Subjected to Microbial Transglutaminase Enzymatic Treatment in the Presence of Lysine Ethyl Ester for Alimentary Use in the Treatment of Celiac Disease.
Celiac disease is one of the most common forms of food intolerance (prevalence 1/200). The
disease occurs in genetically predisposed individuals after ingestion of foods containing
gluten. Celiac patients can suffer from severe malabsorption syndrome, mainly characterized
by diarrhea and weight loss. The only therapeutic approach currently recognized is a
life-long gluten-free diet.
Specific regions of gluten molecule become recognizable by lymphocytes and activate them,
due to changes made by tissue transglutaminase. These changes consist in the conversion of
specific residues of glutamine into glutamic acid. The consequence is an increased binding
affinity between gluten and histocompatibility molecule (HLA-DQ2), localized on the surface
of the "antigen presenting cells" (APC); the exposure of the fragments of modified gluten on
the surface of APC is a phenomenon that eventually activates T lymphocytes.
Recent studies on modified gluten confirmed the hypothesis that it is possible to block the
presentation of gluten to lymphocytes by means of lysine ethyl ester binding exclusively to
those gluten regions responsible for lymphocyte activation.
The enzymatic treatment is performed directly on flour instead of extracted gluten,
maintaining the same anti-inflammatory effectiveness.
The procedure uses a food-grade enzyme, the microbial transglutaminase (mTGasi) isolated
from Streptoverticillium mobarensis, able to catalyze the formation of intermolecular
"cross-links" that modify the functional properties of the products.
Objective of the study is to validate the ability of the enzyme treatment of wheat flour
with mTGasi and lysine ethyl ester to block the toxic effect of gluten in celiac patients.
| Status | Recruiting |
| Enrollment | 20 |
| Est. completion date | August 2015 |
| Est. primary completion date | August 2015 |
| Accepts healthy volunteers | No |
| Gender | Both |
| Age group | 18 Years to 65 Years |
| Eligibility |
Inclusion Criteria: INCLUSION CRITERIA - diagnosis of celiac disease according to ESPGHAN criteria: class III according to Marsh-Oberhuber classification, clear response to gluten-free diet, serological antiendomysium and antitransglutaminase antibodies positive results before GFD; - HLA DQ2-DQ8 positive results; - gluten-free diet from at least one year; - negative serology from at least 1 year; EXCLUSION CRITERIA - inflammatory bowel diseases; - tumors; - infectious liver disease; - renal impairment. |
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Caregiver, Investigator), Primary Purpose: Treatment
| Country | Name | City | State |
|---|---|---|---|
| Italy | Sapienza University - Policlinico Umberto I | Rome |
| Lead Sponsor | Collaborator |
|---|---|
| University of Roma La Sapienza |
Italy,
Branski D, Fasano A, Troncone R. Latest developments in the pathogenesis and treatment of celiac disease. J Pediatr. 2006 Sep;149(3):295-300. Review. — View Citation
Catassi C, Fabiani E, Iacono G, D'Agate C, Francavilla R, Biagi F, Volta U, Accomando S, Picarelli A, De Vitis I, Pianelli G, Gesuita R, Carle F, Mandolesi A, Bearzi I, Fasano A. A prospective, double-blind, placebo-controlled trial to establish a safe gluten threshold for patients with celiac disease. Am J Clin Nutr. 2007 Jan;85(1):160-6. — View Citation
Fink ML, Chung SI, Folk JE. gamma-Glutamylamine cyclotransferase: specificity toward epsilon-(L-gamma-glutamyl)-L-lysine and related compounds. Proc Natl Acad Sci U S A. 1980 Aug;77(8):4564-8. — View Citation
Gianfrani C, Siciliano RA, Facchiano AM, Camarca A, Mazzeo MF, Costantini S, Salvati VM, Maurano F, Mazzarella G, Iaquinto G, Bergamo P, Rossi M. Transamidation of wheat flour inhibits the response to gliadin of intestinal T cells in celiac disease. Gastroenterology. 2007 Sep;133(3):780-9. Epub 2007 Jun 20. — View Citation
Molberg O, Mcadam SN, Körner R, Quarsten H, Kristiansen C, Madsen L, Fugger L, Scott H, Norén O, Roepstorff P, Lundin KE, Sjöström H, Sollid LM. Tissue transglutaminase selectively modifies gliadin peptides that are recognized by gut-derived T cells in celiac disease. Nat Med. 1998 Jun;4(6):713-7. Erratum in: Nat Med 1998 Aug;4(8):974. — View Citation
Nilsen EM, Jahnsen FL, Lundin KE, Johansen FE, Fausa O, Sollid LM, Jahnsen J, Scott H, Brandtzaeg P. Gluten induces an intestinal cytokine response strongly dominated by interferon gamma in patients with celiac disease. Gastroenterology. 1998 Sep;115(3):551-63. — View Citation
Picarelli A, Di Tola M, Sabbatella L, Anania MC, Calabrò A, Renzi D, Bai JC, Sugai E, Carroccio A, Di Prima L, Bardella MT, Barisani D, Ribes-Koninckx C, Aliaga ED, Gasparin M, Bravi E; Multicentre Organ Culture System Study Group. Usefulness of the organ culture system in the in vitro diagnosis of coeliac disease: a multicentre study. Scand J Gastroenterol. 2006 Feb;41(2):186-90. — View Citation
Picarelli A, Maiuri L, Frate A, Greco M, Auricchio S, Londei M. Production of antiendomysial antibodies after in-vitro gliadin challenge of small intestine biopsy samples from patients with coeliac disease. Lancet. 1996 Oct 19;348(9034):1065-7. — View Citation
Yokoyama K, Nio N, Kikuchi Y. Properties and applications of microbial transglutaminase. Appl Microbiol Biotechnol. 2004 May;64(4):447-54. Epub 2004 Jan 22. Review. — View Citation
| Type | Measure | Description | Time frame | Safety issue |
|---|---|---|---|---|
| Primary | Change from baseline in IgA anti-tissue transglutaminase (anti-tTG) antibodies at 30 days | Proof of any positivization of specific serological antibodies for celiac disease. Results quantified by an ELISA reader at 450 nm (A450nm) is expressed in U/mL and the antibody level 10 U/mL was used as a cutoff value to identify anti-tTG positive results. | After 1 month | No |
| Primary | Change from baseline in IgA anti-tissue transglutaminase (anti-tTG) antibodies at 60 days | Proof of any positivization of specific serological antibodies for celiac disease. Results quantified by an ELISA reader at 450 nm (A450nm) is expressed in U/mL and the antibody level 10 U/mL was used as a cutoff value to identify anti-tTG positive results. | After 2 months | No |
| Primary | Change from baseline in IgA anti-tissue transglutaminase (anti-tTG) antibodies at 90 days | Proof of any positivization of specific serological antibodies for celiac disease. Results quantified by an ELISA reader at 450 nm (A450nm) is expressed in U/mL and the antibody level 10 U/mL was used as a cutoff value to identify anti-tTG positive results. | After 3 months | No |
| Primary | Change from baseline in IgA anti-endomysium antibodies (EMA) at 30 days | Test used to confirm serological activation of celiac disease. IgA EMA were searched in sera diluted 1:5 by indirect immunofluorescence analysis on cryostat sections of monkey esophagus. The results are expressed as ''positive/negative''. | After 1 month | No |
| Primary | Change from baseline in IgA anti-endomysium antibodies (EMA) at 60 days | Test used to confirm serological activation of celiac disease. IgA EMA were searched in sera diluted 1:5 by indirect immunofluorescence analysis on cryostat sections of monkey esophagus. The results are expressed as ''positive/negative''. | After 2 months | No |
| Primary | Change from baseline in IgA anti-endomysium antibodies (EMA) at 90 days | Test used to confirm serological activation of celiac disease. IgA EMA were searched in sera diluted 1:5 by indirect immunofluorescence analysis on cryostat sections of monkey esophagus. The results are expressed as ''positive/negative''. | After 3 months | No |
| Primary | Pathologic variations in histologic analysis from baseline | Proof of duodenal mucosa histological alterations induced by celiac disease, consisting in altered (<3:1) villous height/crypt depth ratio and increased (>25) intraepithelial lymphocytes per 100 intestinal epithelial cells, according to Marsh-Oberhuber classification. | After 3 months, or in case of serum anti-tTG IgA/EMA IgA positive results | No |
| Secondary | Presence of bloating at baseline | Evaluation of bloating intensity is reported according to the Visual Analog or Analogue Scale (VAS), with a range of 0-10. | At baseline | No |
| Secondary | Presence of abdominal pain at baseline | Evaluation of abdominal pain intensity is reported according to the Visual Analog or Analogue Scale (VAS), with a range of 0-10. | At baseline | No |
| Secondary | Presence of diarrhea at baseline | Evaluation of diarrhea intensity is reported according to the Visual Analog or Analogue Scale (VAS), with a range of 0-10. | At baseline | No |
| Secondary | Presence of asthenia at baseline | Evaluation of asthenia intensity is reported according to the Visual Analog or Analogue Scale (VAS), with a range of 0-10. | At baseline | No |
| Secondary | Variation of bloating from baseline at 30 days | Evaluation of bloating intensity is reported according to the Visual Analog or Analogue Scale (VAS), with a range of 0-10. | After 1 month | No |
| Secondary | Variation of abdominal pain from baseline at 30 days | Evaluation of abdominal pain intensity is reported according to the Visual Analog or Analogue Scale (VAS), with a range of 0-10. | After 1 month | No |
| Secondary | Variation of diarrhea from baseline at 30 days | Evaluation of diarrhea intensity is reported according to the Visual Analog or Analogue Scale (VAS), with a range of 0-10. | After 1 month | No |
| Secondary | Variation of asthenia from baseline at 30 days | Evaluation of asthenia intensity is reported according to the Visual Analog or Analogue Scale (VAS), with a range of 0-10. | After 1 month | No |
| Secondary | Variation of bloating from baseline at 60 days | Evaluation of bloating intensity is reported according to the Visual Analog or Analogue Scale (VAS), with a range of 0-10. | After 2 months | No |
| Secondary | Variation of abdominal pain from baseline at 60 days | Evaluation of abdominal pain intensity is reported according to the Visual Analog or Analogue Scale (VAS), with a range of 0-10. | After 2 months | No |
| Secondary | Variation of diarrhea from baseline at 60 days | Evaluation of diarrhea intensity is reported according to the Visual Analog or Analogue Scale (VAS), with a range of 0-10. | After 2 months | No |
| Secondary | Variation of asthenia from baseline at 60 days | Evaluation of asthenia intensity is reported according to the Visual Analog or Analogue Scale (VAS), with a range of 0-10. | After 2 months | No |
| Secondary | Variation of bloating from baseline at 90 days | Evaluation of bloating intensity is reported according to the Visual Analog or Analogue Scale (VAS), with a range of 0-10. | After 3 months | No |
| Secondary | Variation of abdominal pain from baseline at 90 days | Evaluation of abdominal pain intensity is reported according to the Visual Analog or Analogue Scale (VAS), with a range of 0-10. | After 3 months | No |
| Secondary | Variation of diarrhea from baseline at 90 days | Evaluation of diarrhea intensity is reported according to the Visual Analog or Analogue Scale (VAS), with a range of 0-10. | After 3 months | No |
| Secondary | Variation of asthenia from baseline at 90 days | Evaluation of asthenia intensity is reported according to the Visual Analog or Analogue Scale (VAS), with a range of 0-10. | After 3 months | No |
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