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Evidencebased criteria for celiac disease diagnosis

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Title: Evidencebased criteria for celiac disease diagnosis

1
Evidence-based criteria for celiac disease
diagnosis

Steffen Husby
Hans Christian Andersen Childrens Hospital
Odense University Hospital
Denmark

2
ESPGHAN Working GroupCeliac Disease Diagnosis

David Branski
Carlo Catassi
Steffen Husby
Sibylle Koletzko
Ilma Korbonai-Zsabo
Markku Maki
Luisa Mearin

Carmen Ribes
Luca Ronfani
Raanan Shamir
Riccardo Troncone
Peter Zimmer
Alessandro Ventura

3
Outline

Celiac disease diagnosis
Definition of celiac disease
Current practices in Europe
Evidence-based Medicine, principles
Already-existing data
Addition 2004-8
Literature search

4
Celiac disease as a multiorgan autoimmune disease
CNS Ataxia, seizures
Depression Heart Carditis Skin
mucosa Dermatitis herpetiformis Aphtous
stomatitis Hair loss Reproductive
system Miscarriage Infertility
General Puberty growth delay
Malignancies Anemia GI system
Diarrhea, vomiting Distension, pain
Malnutrition, weight loss Hepatitis,
cholangitis Bone Osteoporosis,
fractures Arthritis Dental
anomalies
Modified from Rewers, Gastroenterology 2005
5
Towards a new definition of Celiac Disease

A permanent gluten-sensitive enteropathy
Ferguson, 1995
Celiac spectrum (disease?) is an immune-mediated
systemic disorder elicited by gluten and related
prolamines in genetically (mainly HLA)
susceptible
individuals, characterized by anti-tissue
transglutaminase antibodies and/or gluten
dependent
clinical manifestations and/or enteropathy
Troncone/
ESPGHAN 2008

6
Celiac disease
7
Histology Marsh criteria
ORIGINAL
MODIFIED

0 pre-infiltrative, normal
I infiltrative
Normal mucosa and villous architecture, IELs
II hyperplastic
enlarged crypts, increased turnover
III Destructive lesion
VA, lymphocytre infiltration, hyperplastic crypts
IV Hypoplastic
total VA, normal IELs
Does it exist?

0 pre-infiltrative, normal
I infiltrative
as original
II hyperplastic
as original
III Destructive lesion
A. partial VA
B. sub-total VA
C. total VA
IV Hypoplastic
as original

Marsh Gastro. 1982 102 330
Rostami Am.J.Gastro. 1989 94 888
8
Interlaken ESPGHAN criteria

1. biopsy Pathological small intestinal biopsy
villous atrophy
Gluten free diet for 1-2 years
2. biopsy Normalised
3. biopsy Again pathology after re-introduction
of gluten - villous atrophy

McNeish et al. Arch. Dis. Childh. 1979 54 783
9
Revised ESPGHAN criteria 1990

1. biopsy Pathological small intestinal biopsy
villous atrophy
Clinical and serological improvement after 2-3
months
No further biopsy
Provided age gt 2 years

Walker-Smith et al. Archs. Dis. Child. 1990 65
99
10
COELIAC DISEASE DIAGNOSIS ESPGHAN 1990
Criteria or need for a change? QUESTIONNAIRE

85 of those who are compliant to the 1990
criteria want them to be changed
challenge policy 100
HLA should be included for DX 80

C.Ribes, unpublished 2008
11
Evidence-based criteria for clinical decisions
12
Origin of Clinical Questions

Diagnosis how to select and interpret diagnostic
tests
Prognosis how to anticipate the patients likely
course
Therapy how to select treatments that do more
good
than harm
Prevention how to screen and reduce the risk for
disease

13
Steps in EBM

Formulate an answerable question
Track down the best evidence
Critically appraise the evidence for
Validity
Impact (size of the benefit)
Applicability
Integrate with clinical expertise and patient
values
Evaluate our effectiveness and efficiency
keep a record improve the process

14
Step 1- Framing the Question (Q)

Clear, unambiguous, structured question
Questions formulated re PPICO
Populations of interest
Prior test(s) (if appropriate)
Intervention
Comparisons (if appropriate)
Outcomes

15
Step 2 Identifying relevant publications (F)

Wide search of medical/scientific databases
Medline, EMBASE
Cochrane Reviews
Ovid
Relevance to focused question PPICO
Population
Prior test
Intervention
Comparator
Outcome

16
Publication and reporting biases
All studies conducted
All studies published

Positive Results Bias
Grey Literature Bias
Time-Lag Bias
Language and Country Bias
Multiple Publication Bias
Selective Citation Bias
Database Indexing Bias
Selective Outcome
Reporting B.

Grey literature
Studies reviewed
Health Technology Assessment, 2000 4(10)1-115
17
Quality of the evidence

clinical aspects
patient characteristics
comparator
duration of follow-up
relevance of endpoints
(outcomes)
relevance of effect sizes

Methodological aspects
Randomisation
Concealement of allocation
Blinding
intention-to-treat
subgroup analyses
.........

18
Oxford Centre for Evidence-based Medicine Levels
of Evidence (May 2001)
19
Grading the quality of evidence

Give the confidence of the recommendation.
Can the reader be sure that the recommendation
reflects the evidence
Is coded into 4 grades
NOT Strength of recommendation

20
Grades of quality of Evidence
for the Statements

High Further research is unlikely to change our
confidence in the estimate of effect
Moderate Further research is likely to have an
important impact on our confidence in the
estimate of effect and may change the estimate
Low Further research is very likely to have an
important impact on our confidence in the
estimate of effect and may change the estimate
Very low Any estimate of effect is uncertain

GRADE working group BMJ20043281490-4
21
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22
From evidence to recommendations
Quality of evidence
Strength of recommendation
do / dont do we recommend
1 high
probably do/dont do we suggest
2 - moderate
3 - low
Uncertain can be considered we do not know
4 - very low
considered judgment a group decision
DM-CPG programme method report
(www.versorgungsleitlinien.de/english/methods) Eur
opean Council, Recommendation (2001) 13 GRADE
2004 (www.gradeworkinggroup.org)
23
Step 4 Summarising the Evidence (S)

Extracting data from trials
Combining data Meta analysis
Does it make sense to combine?

Oxford Centre for Evidence-based Medicine, 2001
24
Diagnostic Test Accuracymeasurements

Sensitivity is the probability of a positive test
in a diseased person
Specificity is the probability of a negative test
in a non-diseased person.

25
Can a test rule-in or rule-out?

SpPln
Specific test, Positive rules Ine.g. Rovsing's
sign, ST elevation gt 2mm
SnNout
Sensitive test, Negative rules Oute.g. Erect
abdominal film for obstruction, Elevated WCC in
CSF (gt5/mm )

26
organisational framework names and jobs
coordinator, secretary
consensus-panel
steering group
Working Group 1
Working group 2
27
Vote Rules for identifying agreement and dissent
28
Why we need formal methods of consensus
development

Safety in numbers several people are less
likely to arrive at a wrong decision than a
single individual.
Authority a selected group of individuals is
more likely to lend some authority of the
decision produced.
Rationality decisions are improved by reasoned
arguments in which assumptions are challenged and
members forced to justify their views.
Controlled process by providing a structured
process formal methods can eliminate negative
aspects of group decision-making.
Scientific credibility formal consensus methods
meet the requirements of scientific methods.

Murphy, Black et al. Consensus development
methods and their use in clinical guideline
development a review. HTA 1998
29
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30
USA AHRQ report 2004 Main issues

(1) sensitivity, specificity of serological tests
(2) prevalence and incidence of CD
(3) CD associated lymphoma
(4) consequences of testing for CD
(5) interventions for adherence to a gluten-
free diet.

Rostom A, et al.. Celiac Disease.
EvidenceReport/Technology Assessment No. 104.
AHRQ Publication No. 04-E029-2, 2004
31
USA AHRQ report 2004. Conclusions.

The sensitivity and specificity of EMA and tTG
are quite high
CD is a very common disorder with a prevalence in
the general population that is likely close to
1100 (1)
No specific interventions have been identified
that promote adherence to a GFD, but education
and participation in local celiac societies has
been shown to improve compliance.

Rostom A, et al.. Celiac Disease.
EvidenceReport/Technology Assessment No. 104.
AHRQ Publication No. 04-E029-2, 2004
32
NASPGHAN guidelines 2005

PubMed, DARE, Cochrane
317 articles
Evaluation by two committee members
Consensus Nominal Group Technique
Quality of evidence

Hill ID et al. JPGN 2005 40 1-19
33
NASPGHAN 2005 Algorithms for diagnosis
34
ESPGHAN EBM and Celiac disease
35
Celiac disease 2008 ESPGHAN diagnostic
questions

Clinical presentation
What are the symptoms of CD?
What sub-clinical signs are present in CD?
What are the risks for developing sequelae in
asymptomatic CD?
Serology
What are convincing CD-antibody tests (type,
level, quality, number)?
HLA
How many with pos. EMA/TTG are positive for HLA
DQ2/DQ8?
Do we need both HLA and serology in asymptomatic
risk groups?
Biopsy
Does the pathology from intestinal biopsy qualify
for the gold standard?
Is intestinal biopsy necessary in patients with
symptomatic CD and convincing CD-antibodies?

36
Task ESPGHAN criteria for celiac disease
To try to answer our questions update the AHRQ
systematic review (from 2004 to 2008) - update
the literature - select the papers (3 levels
screening) - evaluate the methodological quality
- synthesize the evidence
Rostom A, et al. Celiac disease. Agency for
Healthcare Research and Quality (AHRQ) 2004)
37
3 levels of screening for papers selection

Level 1 (broad screening).
Inclusion any article reporting
sensitivity/specificity of AGA, EMA, tTG, HLA
DQ2/DQ8, or biopsy. Exclusion clearly unrelated
citation
Level 2 (refined screening).
Inclusion for serology/HLA articles where
sensitivity and specificity could be extracted
for biopsy articles where some measure of
diagnostic utility could be obtained.
Level 3 (final screening) ? see below