The molecular basis of T cell acute lymphoblastic leukemia

Pieter Van Vlierberghe(Columbia University Irving Medical Center), Adolfo A. Ferrando(Columbia University Irving Medical Center)
Journal of Clinical Investigation
October 1, 2012
10.1172/jci61269
Cited by 484Open Access
Full Text

Abstract

T cell acute lymphoblastic leukemias (T-ALLs) arise from the malignant transformation of hematopoietic progenitors primed toward T cell development, as result of a multistep oncogenic process involving constitutive activation of NOTCH signaling and genetic alterations in transcription factors, signaling oncogenes, and tumor suppressors. Notably, these genetic alterations define distinct molecular groups of T-ALL with specific gene expression signatures and clinicobiological features. This review summarizes recent advances in our understanding of the molecular genetics of T-ALL.

Related Papers

ARF Promotes MDM2 Degradation and Stabilizes p53: ARF-INK4a Locus Deletion Impairs Both the Rb and p53 Tumor Suppression Pathways
Yanping Zhang, Yue Xiong, Wendell G. Yarbrough|Cell|1998|1.6k
γ-secretase inhibitors reverse glucocorticoid resistance in T cell acute lymphoblastic leukemia
Pedro J. Real, Valeria Tosello, Teresa Palomero et al.|Nature Medicine|2008|440
lyl-1, a novel gene altered by chromosomal translocation in T cell leukemia, codes for a protein with a helix-loop-helix DNA binding motif
Julia D. Mellentin, Stephen D. Smith, Michael L. Cleary|Cell|1989|358
The tal gene undergoes chromosome translocation in T cell leukemia and potentially encodes a helix‐loop‐helix protein.
Q. Chen, Jiin‐Tsuey Cheng, L.H. Tasi et al.|The EMBO Journal|1990|343
Candidate tumor-suppressor genes MTS1 (p16INK4A) and MTS2 (p15INK4B) display frequent homozygous deletions in primary cells from T- but not from B-cell lineage acute lymphoblastic leukemias [see comments]
J Hebert, JM Cayuela, Jennifer L. Berkeley et al.|Blood|1994|297