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Self-Enforcing Feedback Activation between BCL6 and Pre-B Cell Receptor Signaling Defines a Distinct Subtype of Acute Lymphoblastic Leukemia
- Geng, Huimin;
- Hurtz, Christian;
- Lenz, Kyle B;
- Chen, Zhengshan;
- Baumjohann, Dirk;
- Thompson, Sarah;
- Goloviznina, Natalya A;
- Chen, Wei-Yi;
- Huan, Jianya;
- LaTocha, Dorian;
- Ballabio, Erica;
- Xiao, Gang;
- Lee, Jae-Woong;
- Deucher, Anne;
- Qi, Zhongxia;
- Park, Eugene;
- Huang, Chuanxin;
- Nahar, Rahul;
- Kweon, Soo-Mi;
- Shojaee, Seyedmehdi;
- Chan, Lai N;
- Yu, Jingwei;
- Kornblau, Steven M;
- Bijl, Janetta J;
- Ye, B Hilda;
- Ansel, K Mark;
- Paietta, Elisabeth;
- Melnick, Ari;
- Hunger, Stephen P;
- Kurre, Peter;
- Tyner, Jeffrey W;
- Loh, Mignon L;
- Roeder, Robert G;
- Druker, Brian J;
- Burger, Jan A;
- Milne, Thomas A;
- Chang, Bill H;
- Müschen, Markus
- et al.
Published Web Location
https://doi.org/10.1016/j.ccell.2015.02.003Abstract
Studying 830 pre-B ALL cases from four clinical trials, we found that human ALL can be divided into two fundamentally distinct subtypes based on pre-BCR function. While absent in the majority of ALL cases, tonic pre-BCR signaling was found in 112 cases (13.5%). In these cases, tonic pre-BCR signaling induced activation of BCL6, which in turn increased pre-BCR signaling output at the transcriptional level. Interestingly, inhibition of pre-BCR-related tyrosine kinases reduced constitutive BCL6 expression and selectively killed patient-derived pre-BCR(+) ALL cells. These findings identify a genetically and phenotypically distinct subset of human ALL that critically depends on tonic pre-BCR signaling. In vivo treatment studies suggested that pre-BCR tyrosine kinase inhibitors are useful for the treatment of patients with pre-BCR(+) ALL.
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