Disruption of the ZFP574–THAP12 complex suppresses B cell malignancies in mice

Xue Zhong; James J. Moresco; Jeffrey A. SoRelle; Ran Song; Yiao Jiang; Mylinh T. Nguyen; Jianhui Wang; Chun Hui Bu; Eva Marie Y. Moresco; Bruce Beutler; Jin Huk Choi

doi:10.1073/pnas.2409232121

Disruption of the ZFP574–THAP12 complex suppresses B cell malignancies in mice

Xue Zhong, James J. Moresco, Jeffrey A. SoRelle, Ran Song, Yiao Jiang, Mylinh T. Nguyen, Jianhui Wang, Chun Hui Bu, Eva Marie Y. Moresco, Bruce Beutler, Jin Huk Choi

Research output: Contribution to journal › Article › peer-review

Abstract

Despite the availability of life-extending treatments for B cell leukemias and lymphomas, many of these cancers remain incurable. Thus, the development of new molecular targets and therapeutics is needed to expand treatment options. To identify new molecular targets, we used a forward genetic screen in mice to identify genes required for development or survival of lymphocytes. Here, we describe Zfp574, an essential gene encoding a zinc finger protein necessary for normal and malignant lymphocyte survival. We show that ZFP574 interacts with zinc finger protein THAP12 and promotes the G1-to-S-phase transition during cell cycle progression. Mutation of ZFP574 impairs nuclear localization of the ZFP574–THAP12 complex. ZFP574 or THAP12 deficiency results in cell cycle arrest and impaired lymphoproliferation. Germline mutation, acute gene deletion, or targeted degradation of ZFP574 suppressed Myc-driven B cell leukemia in mice, but normal B cells were largely spared, permitting long-term survival, whereas complete lethality was observed in control animals. Our findings support the identification of drugs targeting ZFP574–THAP12 as a unique strategy to treat B cell malignancies.

Original language	English (US)
Article number	e2409232121
Journal	Proceedings of the National Academy of Sciences of the United States of America
Volume	121
Issue number	31
DOIs	https://doi.org/10.1073/pnas.2409232121
State	Published - Jul 30 2024

Keywords

B cell malignancies
ENU
THAP12
ZFP574
cell cycle

ASJC Scopus subject areas

General

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10.1073/pnas.2409232121

Cite this

Zhong, X., Moresco, J. J., SoRelle, J. A., Song, R., Jiang, Y., Nguyen, M. T., Wang, J., Bu, C. H., Moresco, E. M. Y., Beutler, B., & Choi, J. H. (2024). Disruption of the ZFP574–THAP12 complex suppresses B cell malignancies in mice. Proceedings of the National Academy of Sciences of the United States of America, 121(31), Article e2409232121. https://doi.org/10.1073/pnas.2409232121

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abstract = "Despite the availability of life-extending treatments for B cell leukemias and lymphomas, many of these cancers remain incurable. Thus, the development of new molecular targets and therapeutics is needed to expand treatment options. To identify new molecular targets, we used a forward genetic screen in mice to identify genes required for development or survival of lymphocytes. Here, we describe Zfp574, an essential gene encoding a zinc finger protein necessary for normal and malignant lymphocyte survival. We show that ZFP574 interacts with zinc finger protein THAP12 and promotes the G1-to-S-phase transition during cell cycle progression. Mutation of ZFP574 impairs nuclear localization of the ZFP574–THAP12 complex. ZFP574 or THAP12 deficiency results in cell cycle arrest and impaired lymphoproliferation. Germline mutation, acute gene deletion, or targeted degradation of ZFP574 suppressed Myc-driven B cell leukemia in mice, but normal B cells were largely spared, permitting long-term survival, whereas complete lethality was observed in control animals. Our findings support the identification of drugs targeting ZFP574–THAP12 as a unique strategy to treat B cell malignancies.",

keywords = "B cell malignancies, ENU, THAP12, ZFP574, cell cycle",

author = "Xue Zhong and Moresco, {James J.} and SoRelle, {Jeffrey A.} and Ran Song and Yiao Jiang and Nguyen, {Mylinh T.} and Jianhui Wang and Bu, {Chun Hui} and Moresco, {Eva Marie Y.} and Bruce Beutler and Choi, {Jin Huk}",

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AU - Zhong, Xue

AU - Moresco, James J.

AU - SoRelle, Jeffrey A.

AU - Song, Ran

AU - Jiang, Yiao

AU - Nguyen, Mylinh T.

AU - Wang, Jianhui

AU - Bu, Chun Hui

AU - Moresco, Eva Marie Y.

AU - Beutler, Bruce

AU - Choi, Jin Huk

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N2 - Despite the availability of life-extending treatments for B cell leukemias and lymphomas, many of these cancers remain incurable. Thus, the development of new molecular targets and therapeutics is needed to expand treatment options. To identify new molecular targets, we used a forward genetic screen in mice to identify genes required for development or survival of lymphocytes. Here, we describe Zfp574, an essential gene encoding a zinc finger protein necessary for normal and malignant lymphocyte survival. We show that ZFP574 interacts with zinc finger protein THAP12 and promotes the G1-to-S-phase transition during cell cycle progression. Mutation of ZFP574 impairs nuclear localization of the ZFP574–THAP12 complex. ZFP574 or THAP12 deficiency results in cell cycle arrest and impaired lymphoproliferation. Germline mutation, acute gene deletion, or targeted degradation of ZFP574 suppressed Myc-driven B cell leukemia in mice, but normal B cells were largely spared, permitting long-term survival, whereas complete lethality was observed in control animals. Our findings support the identification of drugs targeting ZFP574–THAP12 as a unique strategy to treat B cell malignancies.

AB - Despite the availability of life-extending treatments for B cell leukemias and lymphomas, many of these cancers remain incurable. Thus, the development of new molecular targets and therapeutics is needed to expand treatment options. To identify new molecular targets, we used a forward genetic screen in mice to identify genes required for development or survival of lymphocytes. Here, we describe Zfp574, an essential gene encoding a zinc finger protein necessary for normal and malignant lymphocyte survival. We show that ZFP574 interacts with zinc finger protein THAP12 and promotes the G1-to-S-phase transition during cell cycle progression. Mutation of ZFP574 impairs nuclear localization of the ZFP574–THAP12 complex. ZFP574 or THAP12 deficiency results in cell cycle arrest and impaired lymphoproliferation. Germline mutation, acute gene deletion, or targeted degradation of ZFP574 suppressed Myc-driven B cell leukemia in mice, but normal B cells were largely spared, permitting long-term survival, whereas complete lethality was observed in control animals. Our findings support the identification of drugs targeting ZFP574–THAP12 as a unique strategy to treat B cell malignancies.

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Disruption of the ZFP574–THAP12 complex suppresses B cell malignancies in mice

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