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Synergism of FAK and tyrosine kinase inhibition in Ph+ B-ALL.


ABSTRACT: BCR-ABL1+ B progenitor acute lymphoblastic leukemia (Ph+ B-ALL) is an aggressive disease that frequently responds poorly to currently available therapies. Alterations in IKZF1, which encodes the lymphoid transcription factor Ikaros, are present in over 80% of Ph+ ALL and are associated with a stem cell-like phenotype, aberrant adhesion molecule expression and signaling, leukemic cell adhesion to the bone marrow stem cell niche, and poor outcome. Here, we show that FAK1 is upregulated in Ph+ B-ALL with further overexpression in IKZF1-altered cells and that the FAK inhibitor VS-4718 potently inhibits aberrant FAK signaling and leukemic cell adhesion, potentiating responsiveness to tyrosine kinase inhibitors, inducing cure in vivo. Thus, targeting FAK with VS-4718 is an attractive approach to overcome the deleterious effects of FAK overexpression in Ph+ B-ALL, particularly in abrogating the adhesive phenotype induced by Ikaros alterations, and warrants evaluation in clinical trials for Ph+ B-ALL, regardless of IKZF1 status.

SUBMITTER: Churchman ML 

PROVIDER: S-EPMC4844070 | biostudies-literature | 2016

REPOSITORIES: biostudies-literature

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BCR-ABL1<sup>+</sup> B progenitor acute lymphoblastic leukemia (Ph<sup>+</sup> B-ALL) is an aggressive disease that frequently responds poorly to currently available therapies. Alterations in <i>IKZF1</i>, which encodes the lymphoid transcription factor Ikaros, are present in over 80% of Ph<sup>+</sup> ALL and are associated with a stem cell-like phenotype, aberrant adhesion molecule expression and signaling, leukemic cell adhesion to the bone marrow stem cell niche, and poor outcome. Here, we s  ...[more]

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