Clinical Trial Details
— Status: Completed
Administrative data
| NCT number |
NCT04021199 |
| Other study ID # |
GENEPEDIAB |
| Secondary ID |
|
| Status |
Completed |
| Phase |
N/A
|
| First received |
|
| Last updated |
|
| Start date |
October 22, 2018 |
| Est. completion date |
June 22, 2022 |
Study information
| Verified date |
July 2022 |
| Source |
Université Catholique de Louvain |
| Contact |
n/a |
| Is FDA regulated |
No |
| Health authority |
|
| Study type |
Interventional
|
Clinical Trial Summary
Background/Aims: Diabetes, which affects 420 million people worldwide with a continuously
rising incidence, is defined by a state of chronic hyperglycemia; a criterion referring to a
heterogeneous group of diseases with various etiologies and distinct therapeutic options.
Besides the two main forms of diabetes (i.e., type 1 (T1D) and type 2 (T2D)), there are rare
subtypes of the disease called monogenic diabetes (or formerly MODY) that are hardly
diagnosed because of their resemblance to T1D or T2D. Since these monogenic diabetes may
appear early in life, a consortium of expert pediatric clinical centers was created under a
clinical research initiative (the GENEPEDIAB study) to develop tools for accurate diagnosis
of rare diabetes and to propose appropriate care to these children and adolescents wrongly
assigned to T1D or T2D cohorts. The GENEPEDIAB study was initiated in the context of a
broader collaborative project (DiaType) with the objective to develop personalized diabetes
medicine and better patient care.
Methods: For discrimination of patients with monogenic diabetes from those with classical
forms of diabetes using the MODY probability calculator, patients enrolled in the GENEPEDIAB
study are phenotyped and genotyped for T1D risk (anti-islet antibodies and HLA). Patients
fulfilling sufficient criteria are then genotyped using the routine MODY panel, before being
proposed a thorough gene analysis. More comprehensive genetic tests will be conducted in
patients without anomalies found after the MODY gene-sequencing test.
Perspective: the GENEPEDIAB study will enable the investigators to adapt treatment to
diabetes etiology and help to provide genetic counseling to patients and their family
members. The investigators anticipate that its broad genetic analyses will provide them with
important information about the genetic susceptibility of these subgroups of patients with
atypical diabetes.
Description:
BACKGROUND:
Diabetes currently affects 420 million people worldwide, a number that is expected to
increase to 642 million in 2040. This disease is responsible for a high morbidity rate and an
overall mortality equivalent to 5 million deaths per year. In Belgium, the prevalence of
diabetes is estimated at 8% in adults over 35 years of age, the risk of diabetes being 3 to 5
times higher in populations with high consanguinity, mainly due to the susceptibility to
generate recessive genetic variants, which are characteristic of atypical forms of diabetes.
Although diabetes is linearly defined by a state of chronic hyperglycaemia, this criterion
refers to a heterogeneous group of diseases of various aetiologies and distinct therapeutic
options. Ten to 15% of diabetic patients have insulin-dependent type 1 diabetes (T1D),
attributed to autoimmune destruction of insulin-producing beta cells, while 80% of patients
have type 2 diabetes (T2DM), treated - inter alia - with oral antidiabetic drugs. Despite the
diagnosis of T1D is confirmed by the determination of specific antibodies, DT1 and T2D are
clinically characterized by the phenotypic type and evolution of the patient, without
recourse to specific etiological and/or pathognomonic criteria. Recently, subtypes of T1D and
T2D have been categorized to help the clinician choose the best therapeutic interventions for
the patient (i.e., dietary approach, physical activity, oral antidiabetic drugs, insulin,
combined therapies).
Monogenic causes of diabetes are less common (up to 5% of all cases) and of recent discovery,
their molecular basis having been established in the 1990s, under the name "maturity onset
diabetes of the young" (MODY). The diagnosis of a genetic origin of diabetes has multiple
consequences, primarily at therapeutic level. Despite the implications of a monogenic
diabetes diagnosis, this form remains largely underdiagnosed, and it is accepted that 2 to 3%
of active patients within diabetes conventions of care suffer from undetected genetic forms.
AIM:
Screening, using routinely diagnostic tools, of monogenic forms of diabetes in cohorts of
paediatric patients with atypical forms of diabetes, who are followed in conventions of care
for diabetic patients. After diagnosis of monogenic forms of diabetes, screened patients will
be monitored and treated according to international recommendations applied to specifically
recognized forms of diabetes.
The aim of GENEPEDIAB study is to improve the diagnosis of atypical forms of diabetes in
children and adolescents, and not to evaluate the effects of treatment modification following
genetic screening.
INTERVENTION:
1. Retrospective analysis of data from active and historical diabetic patients within
diabetes care conventions of paediatric endocrinology services; screening of patients
with atypical diabetes; use of clinical routine tests to allow genetic diagnosis of the
condition.
2. Prospective analysis of the evolution of new diabetic patients followed in paediatric
diabetes care conventions; screening of patients with atypical diabetes; use of clinical
routine tests to allow genetic diagnosis of the condition.
3. Screening of patients with atypical diabetes:
- The monogenic diabetes probability will initially be assessed using the MODY
probability calculator (old terminology for monogenic diabetes), which identifies
at risk patients based on clinical history (age, sex, body mass index, HbA1C, type
of therapy, presence of diabetes in the family). This calculator is available on
Internet at www.diabetesgenes.org.
- In addition, other clinical criteria will be used to improve the sensitivity and
specificity of screening for monogenic diabetes.
4. Genetic diagnosis of the condition:
- The diagnosis of T1D will first be completed based on factors currently recognized
by the International Society for Paediatric and Adolescent Diabetes (ISPAD): anti
islet antibodies and at risk HLA genotype. Residual insulin secretion will be also
evaluated.
- Subjects that are detected using criteria described above will be screened using
the routine MODY gene sequencing test, which includes GCK, HNF1A, HNF4A, HNF1B,
KCNJ11, ABCC8, and INS gene sequencing.
- More comprehensive genetic tests will be conducted in patients without anomalies
found after the MODY gene-sequencing test.
PARTICIPATING SITES:
GENEPEDIAB is a multicentre study that include various diabetes care conventions of
paediatric endocrinology services in Belgium.
- Main site: Cliniques universitaires Saint-Luc (UCLouvain), Brussel (Belgium)
- Principal investigator : Dr. Philippe Lysy, Paediatric Endocrinology Unit
- Co-investigators : PhD student Sophie Welsch, PhD Caroline Daems, Paediatric
Endocrinology Unit
- Clinical Research Coordinator : Paola Gallo, Paediatric Endocrinology Unit
- Other sites:
- CHU ND-des Bruyeres (ULg), Liege (Belgium) - Prof. Marie-Christine Lebrethon;
- CHU UCL Namur site Mont-Godinne & CHU UCL Namur site Sainte-Elisabeth (UCLouvain),
Namur (Belgium) - Dr. Dominique Beckers & Dr. Thierry Mouraux;
- CHC, Liege (Belgium) - Dr. Nicole Seret;
- Grand Hopital de Charleroi site Notre Dame (GHdC), Charleroi (Belgium) - Dr.
Jacques Louis.
