Celiac Disease Clinical Trial
Official title:
Lymphocytic Enteritis and Suspected Coeliac Disease: Double-blind Gluten vs Placebo Rechallenge
Patients with lymphocytic enteritis (LE), HLA-DQ2/8+, negative celiac serology and clinical
and histological response to a gluten-free diet (GFD) do not fulfil the diagnostic criteria
of coeliac disease (CoD). At present it remains unclear whether they suffer from coeliac
gluten sensitivity (CGS) or non-coeliac gluten sensitivity (NCGS). There are specific tissue
markers of CoD such as anti-transglutaminase deposits (tTG) and intraepithelial lymphocytes
expressing T-cell receptor (TCR) gamma/delta+.
Aim: To demonstrate the existence of CGS in these patients despite having negative celiac
serology.
Methods: Double-blind randomized clinical trial of gluten vs placebo rechallenge for 6
months in patients with LE on a GFD. Inclusion criteria: >18 years, initial presentation
with GI symptoms, HLA-DQ2/8+, negative celiac serology, good clinical and histological
response to GFD. Patients were randomised to gluten (20 g/day) and placebo (maltrodextrin)
(identical powder sachets mixed with meals). Clinical symptoms were analysed using visual
analogue scales. Quality of life (GIQLI), adherence to diet, serology, and histological
changes including gamma/delta+ IEL and tTG deposits were evaluated.
Duodenal intraepithelial lymphocytosis (lymphocytic enteritis, LE) is defined by normal
villous architecture and intraepithelial lymphocytes (IEL) >25/100 enterocytes. It is a
frequent finding present in 2% to 5,4% of duodenal biopsies.
LE is secondary to coeliac disease (CoD) in only a minority of patients, since it may be a
response to other inflammatory processes in the gut. Other possible aetiologies of LE
include infections (Helicobacter Pylori), drugs (nonsteroidal anti-inflammatory or
acetylsalicylic acid) and autoimmune disease. Observational studies have established CoD to
account for 10% to 43% of cases with LD and positive HLA-DQ2/8 after undertaking an
exhaustive diagnostic work-up. These 'minor' forms of CoD may have similar clinical
manifestations to those with villous atrophy.
However, these patients with 'minor' CoD have often negative celiac serology, and then do
not fulfil the present criteria to diagnose CoD. In fact, using the present diagnostic
criteria they should be included in the definition of non-celiac gluten sensitivity (NCGS).
For diagnosing NCGS it is necessary to rule out CoD by means of negative serology
-endomysial and tissue transglutaminase IgA antibodies- and a duodenal biopsy with absence
of villous atrophy on a gluten-containing diet. As such it is accepted that NCGS patients
might have LE. A recent systematic review on NCGS revealed that 44% of patients presented
HLA-DQ2/8 haplotypes, suggesting that a subgroup of patients with NCGS may actually belong
in the spectrum of CoD, which some authors have so-called 'coeliac lite' disease.
The gold-standard assay for confirming NCGS requires dietary elimination, followed by
double-blind, randomized, placebo-controlled food challenge. This procedure is difficult to
adopt routinely in clinical practice. To date two double-blind placebo-controlled dietary
interventions in patients with presumptive NCGS have been published. The first gluten vs
placebo rechallenge trial showed that patients who received gluten had significantly more
abdominal symptoms than those on placebo (68% vs 40%). The second study that investigated
the specific effects of gluten after dietary reduction of fermentable, poorly absorbed,
short-chain carbohydrates (FODMAPs) in subjects believed to have NCGS, showed no symptomatic
worsening after gluten challenge as compared to placebo. Thus, there was no evidence of
specific or dose dependent effect of gluten on NCGS patients placed on a diet low in
FODMAPs. It is worth mentioning that patients included in these trials were HLA-DQ2/8
negative, and if positive they had a normal duodenal biopsy (Marsh 0) while on a gluten
containing diet. Besides, a GFD has been shown to be more effective in IBS-D patients with
negative CoD serology but HLA-DQ2/8+ than in those with a negative genetic study.
The recent ESPGHAN guidelines for CoD diagnosis suggest that in cases with low-grade
enteropathy (including LE) both a high γδ IEL count and the presence of Ig A anti-tissue
transglutaminase (anti-TG2) deposits in the mucosa increase the likelihood of CoD. In
contrast to CoD, there is stated that in NCGS there is not an increase of T-cell receptor γδ
IELs. However, these parameters have only been scarcely used to rule out CoD in patients
with NCGS in literature.
The aim of study was demonstrate the existence of gluten sensitivity in patients with
HLA-DQ2/8+, LE and negative celiac serology, who had presented a clinical and histological
response to a gluten-free diet (GFD), using a gluten vs placebo-controlled challenge. In
addition, to assess the presence of tissue markers of CoD before and after gluten challenge,
thus confirming the existence of a 'coeliac-lite' disease.
;
Allocation: Randomized, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Caregiver, Investigator, Outcomes Assessor), Primary Purpose: Treatment
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