EWOG-MDS 2006
Author: Dipl.-Inform. MPH Peter Nöllke, Prof. Dr. med. Charlotte Niemeyer, erstellt 2003/07/24,
Last modification: 2019/09/17
EWOG-MDS 2006 |
Prospective non–randomized multi-center study for epidemiology and characterization of Myelodysplastic Syndromes (MDS) and Juvenile Myelomonocytic Leukemia (JMML) in childhood |
Disease |
Myelodysplastic Syndrome (MDS) and Juvenile Myelomonocytic Leukemia (JMML) in childhood |
Type |
Trial aiming at the standardization of diagosis and therapy |
Problem / Objectives |
The aim of the study is to improve the accuracy of diagnosis for children and adolescents with MDS by a standardized review of morphology and standardized cytogenetic and molecular analyses.
Primary objectives
- To evaluate the frequency of the different subtypes of MDS in childhood and adolescence by a standardized diagnostic approach
- To evaluate the frequency of cytogenetic and molecular abnormalities: -Specifically using array-CGH to evaluate the frequency of subtle chromosomal imbalances, i.e.gains and losses of defined chromosomal regions, and amplifications.-Specifically using mFISH to identify unknown chromosomal aberrations, particularly subtle translocations involving new candidate genes, and to better define chromosomal breakpoints.
Secondary objectives
- To assess survival for children and adolescents with MDS and JMML
- To evaluate relapse rate, morbidity and mortality in children with MDS and JMML treated by HSCT
|
Inclusion Criteria |
- Confirmed diagnosis of MDS or JMML (morphology, cytogenetics)
- Myeloid leukemia of Down syndrome (patients aged > 6 years).
- Age: age less than 18 years
|
Exclusion Criteria |
- Denied informed consent and/or assent by caretakers/patient.
- Fanconi anemia (diagnosed by chromosomal breakage, G2 cell cycle arrest, Western blot or mutational analysis) or other congenital bone marrow failure disorders (diagnosed clinically or by disease specific germ line mutations) without secondary MDS. Secondary MDS in congenital bone marrow failure is defined by a consistent acquired bone marrow abnormality as a) increase in blasts, b) acquired consistent, hromosomal abnormality, c) increasing bone marrow cellularity in the presence of blood pancytopenia
- Shwachman syndrome or Fanconi anemia with a single aberration not typical of MDS.
- Translocation characteristic for de novo AML like t(8;21)(q22;q22) [AML1/ETO fusion gene], t(15,17)(q22;q12) [PML/RARα rearrangement], inv(16)(p13q22) [CBFβ/MYH11rearrangement]
- Myeloid leukemia of Down syndrome (patients aged < 6 years).
- Participation in another interventional study within the last 4 weeks (except for therapy optimizing
- studies in cancer or bone marrow failure, diagnostic protocols).
|
Recruitment |
260 |
Status |
Start 01/01/2007; end of recruitment: 01/04/2013 |
Principal Investigator |
Prof. Dr. med. Charlotte Niemeyer |
E-Mail |
ewog-mds@uniklinik-freiburg.de
|
URL |
http://www.ewog-mds.org/
|
Contact |
Investigator
Prof. Dr.
Charlotte Niemeyer
Universitätsklinikum Freiburg, ZKJ
Klinik IV: Pädiatrische Hämatologie und Onkologie
Mathildenstraße 1
79106
Freiburg i. Brsg.
Telefon +49 761 270 46170
Fax +49 (761) 270 45180
ewog-mds-saa@uniklinik-freiburg.de
Statistics
Peter Noellke
Univ. Klinikum Freiburg
Zentrum für Kinderheilkunde und Jugendmedizin, Abt. f. Päd. Hämatologie und Onkologie
Breisacher Str. 62
79106
Freiburg
Telefon +49 (761) 270 43453
Fax +49 (0)761 270 9646200
peter.noellke@uniklinik-freiburg.de
|
Sponsoring |
Carreras-Stiftung, Förderverein für krebskranke Kinder e.V., Freiburg i. Br. |