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. 2023 Sep;37(9):1802-1811.
doi: 10.1038/s41375-023-01970-5. Epub 2023 Jul 18.

SETBP1 is dispensable for normal and malignant hematopoiesis

Atsushi Tanaka  1   2   3 Koutarou Nishimura  1 Wataru Saika  1   4 Ayana Kon  5 Yui Koike  1 Hiromi Tatsumi  6 June Takeda  5 Masaki Nomura  1   7 Weijia Zang  1   3 Manabu Nakayama  8 Masashi Matsuda  6 Hiromi Yamazaki  1 Miki Fukumoto  1 Hiromi Ito  1 Yasutaka Hayashi  1 Toshio Kitamura  1 Hiroshi Kawamoto  2 Akifumi Takaori-Kondo  3 Haruhiko Koseki  6 Seishi Ogawa  5   9   10 Daichi Inoue  11   12
Affiliations

SETBP1 is dispensable for normal and malignant hematopoiesis

Atsushi Tanaka et al. Leukemia. 2023 Sep.

Abstract

SETBP1 is a potential epigenetic regulator whose hotspot mutations preventing proteasomal degradation are recurrently detected in myeloid malignancies with poor prognosis. It is believed that the mutant SETBP1 exerts amplified effects of wild-type SETBP1 rather than neomorphic functions. This indicates that dysregulated quantitative control of SETBP1 would result in the transformation of hematopoietic cells. However, little is known about the roles of endogenous SETBP1 in malignant and normal hematopoiesis. Thus, we integrated the analyses of primary AML and healthy samples, cancer cell lines, and a newly generated murine model, Vav1-iCre;Setbp1fl/fl. Despite the expression in long-term hematopoietic stem cells, SETBP1 depletion in normal hematopoiesis minimally alters self-renewal, differentiation, or reconstitution in vivo. Indeed, its loss does not profoundly alter transcription or chromatin accessibilities. Furthermore, although AML with high SETBP1 mRNA is associated with genetic and clinical characteristics for dismal outcomes, SETBP1 is dispensable for the development or maintenance of AML. Contrary to the evidence that SETBP1 mutations are restricted to myeloid malignancies, dependency on SETBP1 mRNA expression is not observed in AML. These unexpected results shed light on the unrecognized idea that a physiologically nonessential gene can act as an oncogene when the machinery of protein degradation is damaged.

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