PLCG1 is required for AML1-ETO leukemia stem cell self-renewal

Tina M. Schnoeder,Adrian Schwarzer,Ashok Kumar Jayavelu,Chen-Jen Hsu,Joanna Kirkpatrick,Konstanze Döhner,Florian Perner,Theresa Eifert,Nicolas Huber,Patricia Arreba-Tutusaus,Anna Dolnik,Salam A. Assi,Monica Nafria,Lu Jiang,Yuting Dai,Zhu Chen,Sai Juan Chen,Sophie G. Kellaway,Anetta Ptasinska,Elizabeth Ng,Edouard G. Stanley,Andrew G. Elefanty,Marcus Buschbeck,Holger Bierhoff,Steffen Brodt,Georg Matziolis,Klaus-Dieter Fischer,Andreas Hochhaus,Chun-Wei Chen,Olaf Heidenreich,Matthias Mann,Steven W. Lane,Lars Bullinger,Alessandro Ori,Björn von Eyss,Constanze Bonifer,Florian H. Heidel

PLCG1 is required for AML1-ETO leukemia stem cell self-renewal

2021

In an effort to identify novel drugs targeting fusion-oncogene induced acute myeloid leukemia (AML), we performed high-resolution proteomic analysis. In AML1-ETO (AE) driven AML we uncovered a de-regulation of phospholipase C (PLC) signaling. We identified PLCgamma 1 (PLCG1) as a specific target of the AE fusion protein which is induced after AE binding to intergenic regulatory DNA elements. Genetic inactivation of PLCG1 in murine and human AML inhibited AML1-ETO dependent self-renewal programs, leukemic proliferation, and leukemia maintenance in vivo. In contrast, PLCG1 was dispensable for normal hematopoietic stem- and progenitor cell function. These findings are extended to and confirmed by pharmacologic perturbation of Ca++-signaling in AML1-ETO AML cells, indicating that the PLCG1 pathway poses an important therapeutic target for AML1-ETO positive leukemic stem cells.

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