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  •   Ιδρυματικό Αποθετήριο Πανεπιστημίου Θεσσαλίας
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  •   Ιδρυματικό Αποθετήριο Πανεπιστημίου Θεσσαλίας
  • Επιστημονικές Δημοσιεύσεις Μελών ΠΘ (ΕΔΠΘ)
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Ιδρυματικό Αποθετήριο Πανεπιστημίου Θεσσαλίας
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ETV6/RUNX1-positive childhood acute lymphoblastic leukemia (ALL): The spectrum of clonal heterogeneity and its impact on prognosis

Thumbnail
Συγγραφέας
Ampatzidou Μ., Papadhimitriou S.I., Paterakis G., Pavlidis D., Tsitsikas Κ., Kostopoulos I.V., Papadakis V., Vassilopoulos G., Polychronopoulou S.
Ημερομηνία
2018
Γλώσσα
en
DOI
10.1016/j.cancergen.2018.03.001
Λέξη-κλειδί
transcription factor ETV6
transcription factor RUNX1
repressor protein
RUNX1 protein, human
transcription factor Ets
transcription factor ETV6
transcription factor RUNX1
acute lymphoblastic leukemia
adolescent
Article
cancer prognosis
child
chromosome 21q
chromosome 9p
clinical feature
cohort analysis
disease association
female
flow cytometry
follow up
genetic disorder
genetic heterogeneity
human
human cell
human tissue
long term care
major clinical study
male
minimal residual disease
priority journal
treatment outcome
treatment response
acute disease
acute lymphoblastic leukemia
clonal evolution
genetics
metabolism
pathology
preschool child
prognosis
retrospective study
Acute Disease
Child, Preschool
Clonal Evolution
Cohort Studies
Core Binding Factor Alpha 2 Subunit
Female
Humans
Male
Precursor Cell Lymphoblastic Leukemia-Lymphoma
Prognosis
Proto-Oncogene Proteins c-ets
Repressor Proteins
Retrospective Studies
Elsevier Inc.
Εμφάνιση Μεταδεδομένων
Επιτομή
The prognostic significance of the ETV6/RUNX1-fusion and of the accompanying aberrations is disputable; whether co-existing sub-clones are responsible for delayed MRD-clearance and thus, moderate outcome, remains to be clarified. We studied, in a paediatric cohort of 119 B-ALLs, the relation between the ETV6/RUNX1 aberration and the co-existing subclones with (a) presenting clinical/biological features, (b) early response to treatment(MRD) and (c) long-term outcome over a 12-year period. Patients were homogeneously treated according to BFM-based-protocols. 27/119 patients (22.7%) were ETV6/RUNX1-positive; 19/27 (70.4%) harbored additional genetic abnormalities while 9/19 (33.3%) presented with clonal heterogeneity. The most common abnormalities were del12p13 (37%), 3-6×21q22 (22.2%), del9p21 (18.5%) and 2-3xETV6/RUNX1 (18.5%). MRDd15-positivity (≥10−3) was detected in 44% of the cohort; the corresponding MRD among patients carrying subclones rises to 88.9%. Common features of all relapses were sub-clonal diversity, FCM-MRDd15-positivity and additional del(9p21) while there were no censored relapses among ETV6/RUNX1-positive patients with sole translocation and absence of additional aberrations, within a median follow-up time of 90 months. In our study, the presence of clonal heterogeneity and impaired FCM-MRD clearance among ETV6/RUNX1-positive patients, ultimately influenced prognosis. Longer follow-up is needed in order to further validate these initial results. © 2018 Elsevier Inc.
URI
http://hdl.handle.net/11615/81056
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  • Δημοσιεύσεις σε περιοδικά, συνέδρια, κεφάλαια βιβλίων κλπ. [19735]

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