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DOI: 10.1055/s-0036-1582492
Pre-BCR expression predicts sensitivity to SYK inhibition in B-cell acute lymphoblastic leukemia
Introduction: Recent studies have suggested SYK as target for the treatment of pre-BCR+ B-ALL but whether pre-BCR status constitutes the only predictor for sensitivity to SYK inhibition in B-ALL is discussed controversially.
Methods: We employed a comparative approach of pre-BCR knockout and pharmacologic inhibition of pre-BCR signaling with SYK inhibitors to dissect the requirements for the SYK-dependent survival of B-ALL cells.
Results: Pre-BCR+ ALL requires constitutive signals from the pre-BCR and SYK for proliferation and survival. These signals involve the pre-BCR-dependent activation of SYK and PI3K, resulting in the inactivation of FOXO1 and the deregulation of MYC. Inhibition of pre-BCR signaling with SYK inhibitors reverses these effects and exhibits promising activity in several models of pre-BCR+ ALL.
Conclusion: Pre-BCR expression characterizes a subgroup of B-ALL selectively sensitive to SYK inhibition.