A genome-scale in vivo loss-of-function screen identifies phf6 as a lineage-specific regulator of leukemia cell growth

Corbin E. Meacham; Lee N. Lawton; Yadira M. Soto-Feliciano; Justin R. Pritchard; Brian A. Joughin; Tobias Ehrenberger; Nina Fenouille; Johannes Zuber; Richard T. Williams; Richard A. Young; Michael T. Hemann

doi:10.1101/gad.254151.114

A genome-scale in vivo loss-of-function screen identifies phf6 as a lineage-specific regulator of leukemia cell growth

Corbin E. Meacham, Lee N. Lawton, Yadira M. Soto-Feliciano, Justin R. Pritchard, Brian A. Joughin, Tobias Ehrenberger, Nina Fenouille, Johannes Zuber, Richard T. Williams, Richard A. Young, Michael T. Hemann

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37 Scopus citations

Abstract

We performed a genome-scale shRNA screen for modulators of B-cell leukemia progression in vivo. Results from this work revealed dramatic distinctions between the relative effects of shRNAs on the growth of tumor cells in culture versus in their native microenvironment. Specifically, we identified many ‘‘context-specific’’ regulators of leukemia development. These included the gene encoding the zinc finger protein Phf6. While inactivating mutations in PHF6 are commonly observed in human myeloid and T-cell malignancies, we found that Phf6 suppression in B-cell malignancies impairs tumor progression. Thus, Phf6 is a ‘‘lineage-specific’’ cancer gene that plays opposing roles in developmentally distinct hematopoietic malignancies.

Original language	English (US)
Pages (from-to)	483-488
Number of pages	6
Journal	Genes and Development
Volume	29
Issue number	5
DOIs	https://doi.org/10.1101/gad.254151.114
State	Published - 2015
Externally published	Yes

Keywords

Context dependency
In vivo screen
Leukemia
Phf6

ASJC Scopus subject areas

Genetics
Developmental Biology

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10.1101/gad.254151.114

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Meacham, C. E., Lawton, L. N., Soto-Feliciano, Y. M., Pritchard, J. R., Joughin, B. A., Ehrenberger, T., Fenouille, N., Zuber, J., Williams, R. T., Young, R. A., & Hemann, M. T. (2015). A genome-scale in vivo loss-of-function screen identifies phf6 as a lineage-specific regulator of leukemia cell growth. Genes and Development, 29(5), 483-488. https://doi.org/10.1101/gad.254151.114

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abstract = "We performed a genome-scale shRNA screen for modulators of B-cell leukemia progression in vivo. Results from this work revealed dramatic distinctions between the relative effects of shRNAs on the growth of tumor cells in culture versus in their native microenvironment. Specifically, we identified many {\textquoteleft}{\textquoteleft}context-specific{\textquoteright}{\textquoteright} regulators of leukemia development. These included the gene encoding the zinc finger protein Phf6. While inactivating mutations in PHF6 are commonly observed in human myeloid and T-cell malignancies, we found that Phf6 suppression in B-cell malignancies impairs tumor progression. Thus, Phf6 is a {\textquoteleft}{\textquoteleft}lineage-specific{\textquoteright}{\textquoteright} cancer gene that plays opposing roles in developmentally distinct hematopoietic malignancies.",

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year = "2015",

doi = "10.1101/gad.254151.114",

language = "English (US)",

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AU - Meacham, Corbin E.

AU - Lawton, Lee N.

AU - Soto-Feliciano, Yadira M.

AU - Pritchard, Justin R.

AU - Joughin, Brian A.

AU - Ehrenberger, Tobias

AU - Fenouille, Nina

AU - Zuber, Johannes

AU - Williams, Richard T.

AU - Young, Richard A.

AU - Hemann, Michael T.

N1 - Publisher Copyright: ã 2015 Meacham et al.

PY - 2015

Y1 - 2015

N2 - We performed a genome-scale shRNA screen for modulators of B-cell leukemia progression in vivo. Results from this work revealed dramatic distinctions between the relative effects of shRNAs on the growth of tumor cells in culture versus in their native microenvironment. Specifically, we identified many ‘‘context-specific’’ regulators of leukemia development. These included the gene encoding the zinc finger protein Phf6. While inactivating mutations in PHF6 are commonly observed in human myeloid and T-cell malignancies, we found that Phf6 suppression in B-cell malignancies impairs tumor progression. Thus, Phf6 is a ‘‘lineage-specific’’ cancer gene that plays opposing roles in developmentally distinct hematopoietic malignancies.

AB - We performed a genome-scale shRNA screen for modulators of B-cell leukemia progression in vivo. Results from this work revealed dramatic distinctions between the relative effects of shRNAs on the growth of tumor cells in culture versus in their native microenvironment. Specifically, we identified many ‘‘context-specific’’ regulators of leukemia development. These included the gene encoding the zinc finger protein Phf6. While inactivating mutations in PHF6 are commonly observed in human myeloid and T-cell malignancies, we found that Phf6 suppression in B-cell malignancies impairs tumor progression. Thus, Phf6 is a ‘‘lineage-specific’’ cancer gene that plays opposing roles in developmentally distinct hematopoietic malignancies.

KW - Context dependency

KW - In vivo screen

KW - Leukemia

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A genome-scale in vivo loss-of-function screen identifies phf6 as a lineage-specific regulator of leukemia cell growth

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Keywords

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