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Citations to this article

BETP degradation simultaneously targets acute myelogenous leukemic stem cells and the microenvironment
Sujan Piya, … , Michael Andreeff, Gautam Borthakur
Sujan Piya, … , Michael Andreeff, Gautam Borthakur
Published February 21, 2019
Citation Information: J Clin Invest. 2019;129(5):1878-1894. https://doi.org/10.1172/JCI120654.
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Research Article Cell biology Oncology Article has an altmetric score of 4

BETP degradation simultaneously targets acute myelogenous leukemic stem cells and the microenvironment

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Abstract

The antileukemic effect of inhibiting bromodomain and extra-terminal domain-containing (BET-containing) proteins (BETPs) such as BRD4 has largely been largely attributed to transcriptional downregulation of cellular anabolic and antiapoptotic processes, but its effect on the bone marrow microenvironment, a sanctuary favoring the persistence of leukemic stem/progenitor cells, is unexplored. Sustained degradation of BETP with the small-molecule BET proteolysis-targeting chimera (PROTAC) ARV-825 resulted in a marked downregulation of surface CXCR4 and CD44, key proteins in leukemia-microenvironment interactions, in acute myeloid leukemia (AML) cells. Abrogation of surface CXCR4 expression impaired SDF-1α–directed migration and was mediated through transcriptional downregulation of PIM1 kinase, which in turn phosphorylates CXCR4 and facilitates its surface localization. Downregulation of CD44, including isoforms CD44v8–10 impaired cystine uptake, lowered intracellular reduced glutathione, and increased oxidative stress. More important, BETP degradation markedly decreased the CD34+CD38–CD90–CD45RA+ leukemic stem cell population and, alone or in combination with cytarabine, prolonged survival in a mouse model of human leukemia that included AML patient-derived xenografts (AML-PDX). Gene expression profiling and single-cell proteomics confirmed a downregulation of the gene signatures associated with “stemness” in AML and Wnt/β-catenin and Myc pathways. Hence, BETP degradation by ARV-825 simultaneously targets cell-intrinsic signaling, stromal interactions, and metabolism in AML.

Authors

Sujan Piya, Hong Mu, Seemana Bhattacharya, Philip L. Lorenzi, R. Eric Davis, Teresa McQueen, Vivian Ruvolo, Natalia Baran, Zhiqiang Wang, Yimin Qian, Craig M. Crews, Marina Konopleva, Jo Ishizawa, M. James You, Hagop Kantarjian, Michael Andreeff, Gautam Borthakur

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Total citations by year

Year: 2025 2024 2023 2022 2021 2020 Total
Citations: 2 2 9 8 7 10 38
Citation information
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Citations to this article (38)

Title and authors Publication Year
CXCR Family and Hematologic Malignancies in the Bone Marrow Microenvironment
Liu Y, Tang H
Biomolecules 2025
Advances in the application of patient-derived xenograft models in acute leukemia resistance
Qin R, Liang Y, Zhou F
Cancer Drug Resistance 2025
The multi-CDK inhibitor dinaciclib reverses bromo- and extra-terminal domain (BET) inhibitor resistance in acute myeloid leukemia via inhibition of Wnt/β-catenin signaling
Marr AR, Halpin M, Corbin DL, Asemelash Y, Sher S, Gordon BK, Whipp EC, Mitchell S, Harrington BK, Orwick S, Benrashid S, Goettl VM, Yildiz V, Mitchell AD, Cahn O, Mims AS, Larkin KT, Long M, Blachly J, Woyach JA, Lapalombella R, Grieselhuber NR
Experimental Hematology and Oncology 2024
Divergent Processing of Cell Stress Signals as the Basis of Cancer Progression: Licensing NFκB on Chromatin
Vlahopoulos SA
International Journal of Molecular Sciences 2024
Unc51-like autophagy activating kinase 1 (ULK1) drives progression and drug-resistance in acute myelogenous leukemia
Seemana Bhattacharya, Sujan Piya, Huaxian Ma, Priyanka Sharma, Qi Zhang, Natalia Baran, Vivian Ruvolo, Teresa McQueen, R. Davis, Rasoul Pourebrahim, Marina Konopleva, Hagop Kantarjian, Nicholas Cosford, Michael Andreeff, Gautam Borthakur
Molecular cancer research : MCR 2023
Targeting IFN-γ by abemaciclib drives differentiation of acute myeloid leukemia stem cells
Xiaoling Xie, Wuju Zhang, Xuan Zhou, Binyan Xu, Jingyang Qiu, Hao Wang, Lijuan Zhou, Yingqi Qiu, Yuxing Hu, Shujie Hu, Mengyan Hou, Yating Pan, Le Hu, Sheng Zhang, Chenbo Zhao, Honghao Zhang, Xuefei Gao, Yuhua Li, Xiaochun Bai
Oncogene 2023
Optimization of PROTAC Ternary Complex Using DNA Encoded Library Approach
Chen Q, Liu C, Wang W, Meng X, Cheng X, Li X, Cai L, Luo L, He X, Qu H, Luo J, Wei H, Gao S, Liu G, Wan J, Israel DI, Li J, Dou D
ACS chemical biology 2023
Lethal activity of BRD4 PROTAC degrader QCA570 against bladder cancer cells
Wang Q, Li B, Zhang W, Li Z, Jiang B, Hou S, Ma S, Qin C
Frontiers in Chemistry 2023
Circular RNA PVT1 Regulates Cell Proliferation, Migration, and Apoptosis by Stabilizing c-Myc and Downstream Target CXCR4 Expression in Acute Myeloid Leukemia.
Sheng XF, Hong LL, Fan L, Zhang Y, Chen KL, Mu J, Shen SY, Zhuang HF
2023
CRISPR screening identifies synergy between BET and mTOR inhibitors in cholangiocarcinoma through impaired serine glycine one carbon metabolism
yan zhu, dengyong zhang, Sharmeen Chagani, Young-Ho Jung, Prit Benny Malgulwar, Medina Colic, Sarah Benjamin, Pooja Shukla, John Copland, Lin Tan, Philip Lorenzi, Milind Javle, Jason T. Huse, Jason Roszik, Traver Hart, Lawrence Kwong
JCI Insight 2023
Cytoprotective, Cytotoxic and Cytostatic Roles of Autophagy in Response to BET Inhibitors
Elshazly AM, Gewirtz DA
International journal of molecular sciences 2023
Enhanced TP53 reactivation disrupts MYC transcriptional program and overcomes venetoclax resistance in acute myeloid leukemias.
Nishida Y, Ishizawa J, Ayoub E, Montoya RH, Ostermann LB, Muftuoglu M, Ruvolo VR, Patsilevas T, Scruggs DA, Khazaei S, Mak PY, Tao W, Carter BZ, Boettcher S, Ebert BL, Daver NG, Konopleva M, Seki T, Kojima K, Andreeff M
Science Advances 2023
ARV-825 Showed Antitumor Activity against BRD4-NUT Fusion Protein by Targeting the BRD4.
Yang L, Jing Y, Xia X, Yin X
Journal of Oncology 2023
Targeting the NOTCH1-MYC-CD44 axis in leukemia-initiating cells in T-ALL
S Piya, Y Yang, S Bhattacharya, P Sharma, H Ma, H Mu, H He, V Ruvolo, N Baran, R Davis, A Jain, M Konopleava, H Kantarjian, M Andreeff, M You, G Borthakur
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EEF2K silencing inhibits tumour progression through repressing SPP1 and synergises with BET inhibitors in melanoma
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B Pardieu, J Pasanisi, F Ling, R Bello, J Penneroux, A Su, R Joudinaud, L Chat, H Wu, M Duchmann, G Sodaro, C Chauvel, F Castelli, L Vasseur, K Pacchiardi, Y Belloucif, M Laiguillon, E Meduri, C Vaganay, G Alexe, J Berrou, C Benaksas, A Forget, T Braun, C Gardin, E Raffoux, E Clappier, L Adès, H de Thé, F Fenaille, B Huntly, K Stegmaier, H Dombret, N Fenouille, C Lobry, A Puissant, R Itzykson
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