Epigenome-wide analysis across the development span of pediatric acute lymphoblastic leukemia: backtracking to birth

Authors :: Akram Ghantous
Semira Gonseth Nusslé
Farah J. Nassar
Natalia Spitz
Alexei Novoloaca
Olga Krali
Eric Nickels
Vincent Cahais
Cyrille Cuenin
Ritu Roy
Shaobo Li
Maxime Caron
Dilys Lam
Peter Daniel Fransquet
John Casement
Gordon Strathdee
Mark S. Pearce
Helen M. Hansen
Hwi-Ho Lee
Yong Sun Lee
Adam J. de Smith
Daniel Sinnett
Siri Eldevik Håberg
Jill A. McKay
Jessica Nordlund
Per Magnus
Terence Dwyer
Richard Saffery
Joseph Leo Wiemels
Monica Cheng Munthe-Kaas
Zdenko Herceg
Source :: Molecular Cancer, Vol 23, Iss 1, Pp 1-8 (2024)
Publication Year :: 2024
Publisher :: BMC, 2024.
Abstract: Abstract Background Cancer is the leading cause of disease-related mortality in children. Causes of leukemia, the most common form, are largely unknown. Growing evidence points to an origin in-utero, when global redistribution of DNA methylation occurs driving tissue differentiation. Methods Epigenome-wide DNA methylation was profiled in surrogate (blood) and target (bone marrow) tissues at birth, diagnosis, remission and relapse of pediatric pre-B acute lymphoblastic leukemia (pre-B ALL) patients. Double-blinded analyses was performed between prospective cohorts extending from birth to diagnosis and retrospective studies backtracking from clinical disease to birth. Validation was carried out using independent technologies and populations. Results The imprinted and immuno-modulating VTRNA2-1 was hypermethylated (FDR

Subjects :: Pediatric leukemia
Epigenetics
DNA methylation
VTRNA2-1
Birth cohort
Neonatal blood spots
Neoplasms. Tumors. Oncology. Including cancer and carcinogens
RC254-282

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