Prostate lineage-specific metabolism governs luminal differentiation and response to antiandrogen treatment

Jenna M. Giafaglione; Preston D. Crowell; Amelie M.L. Delcourt; Takao Hashimoto; Sung Min Ha; Aishwarya Atmakuri; Nicholas M. Nunley; Rachel M.A. Dang; Mao Tian; Johnny A. Diaz; Elisavet Tika; Marie C. Payne; Deborah L. Burkhart; Dapei Li; Nora M. Navone; Eva Corey; Peter S. Nelson; Neil Y.C. Lin; Cedric Blanpain; Leigh Ellis; Paul C. Boutros; Andrew S. Goldstein

doi:10.1038/s41556-023-01274-x

Prostate lineage-specific metabolism governs luminal differentiation and response to antiandrogen treatment

Jenna M. Giafaglione
, Preston D. Crowell
, Amelie M.L. Delcourt
, Takao Hashimoto
, Sung Min Ha
, Aishwarya Atmakuri
, Nicholas M. Nunley
, Rachel M.A. Dang
, Mao Tian
, Johnny A. Diaz
, Elisavet Tika
, Marie C. Payne
, Deborah L. Burkhart
, Dapei Li
, Nora M. Navone
, Eva Corey
, Peter S. Nelson
, Neil Y.C. Lin
, Cedric Blanpain
, Leigh Ellis

Paul C. Boutros, Andrew S. Goldstein^*

^*Corresponding author for this work

Surgery

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

31 Scopus citations

Abstract

Lineage transitions are a central feature of prostate development, tumourigenesis and treatment resistance. While epigenetic changes are well known to drive prostate lineage transitions, it remains unclear how upstream metabolic signalling contributes to the regulation of prostate epithelial identity. To fill this gap, we developed an approach to perform metabolomics on primary prostate epithelial cells. Using this approach, we discovered that the basal and luminal cells of the prostate exhibit distinct metabolomes and nutrient utilization patterns. Furthermore, basal-to-luminal differentiation is accompanied by increased pyruvate oxidation. We establish the mitochondrial pyruvate carrier and subsequent lactate accumulation as regulators of prostate luminal identity. Inhibition of the mitochondrial pyruvate carrier or supplementation with exogenous lactate results in large-scale chromatin remodelling, influencing both lineage-specific transcription factors and response to antiandrogen treatment. These results establish reciprocal regulation of metabolism and prostate epithelial lineage identity.

Original language	English
Pages (from-to)	1821-1832
Number of pages	12
Journal	Nature Cell Biology
Volume	25
Issue number	12
DOIs	https://doi.org/10.1038/s41556-023-01274-x
State	Published - Dec 2023

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Giafaglione, J. M., Crowell, P. D., Delcourt, A. M. L., Hashimoto, T., Ha, S. M., Atmakuri, A., Nunley, N. M., Dang, R. M. A., Tian, M., Diaz, J. A., Tika, E., Payne, M. C., Burkhart, D. L., Li, D., Navone, N. M., Corey, E., Nelson, P. S., Lin, N. Y. C., Blanpain, C., ... Goldstein, A. S. (2023). Prostate lineage-specific metabolism governs luminal differentiation and response to antiandrogen treatment. Nature Cell Biology, 25(12), 1821-1832. https://doi.org/10.1038/s41556-023-01274-x

@article{3047a3601ef84721b60f7a285ff5c819,

title = "Prostate lineage-specific metabolism governs luminal differentiation and response to antiandrogen treatment",

abstract = "Lineage transitions are a central feature of prostate development, tumourigenesis and treatment resistance. While epigenetic changes are well known to drive prostate lineage transitions, it remains unclear how upstream metabolic signalling contributes to the regulation of prostate epithelial identity. To fill this gap, we developed an approach to perform metabolomics on primary prostate epithelial cells. Using this approach, we discovered that the basal and luminal cells of the prostate exhibit distinct metabolomes and nutrient utilization patterns. Furthermore, basal-to-luminal differentiation is accompanied by increased pyruvate oxidation. We establish the mitochondrial pyruvate carrier and subsequent lactate accumulation as regulators of prostate luminal identity. Inhibition of the mitochondrial pyruvate carrier or supplementation with exogenous lactate results in large-scale chromatin remodelling, influencing both lineage-specific transcription factors and response to antiandrogen treatment. These results establish reciprocal regulation of metabolism and prostate epithelial lineage identity.",

author = "Giafaglione, \{Jenna M.\} and Crowell, \{Preston D.\} and Delcourt, \{Amelie M.L.\} and Takao Hashimoto and Ha, \{Sung Min\} and Aishwarya Atmakuri and Nunley, \{Nicholas M.\} and Dang, \{Rachel M.A.\} and Mao Tian and Diaz, \{Johnny A.\} and Elisavet Tika and Payne, \{Marie C.\} and Burkhart, \{Deborah L.\} and Dapei Li and Navone, \{Nora M.\} and Eva Corey and Nelson, \{Peter S.\} and Lin, \{Neil Y.C.\} and Cedric Blanpain and Leigh Ellis and Boutros, \{Paul C.\} and Goldstein, \{Andrew S.\}",

note = "Publisher Copyright: {\textcopyright} 2023, The Author(s).",

year = "2023",

month = dec,

doi = "10.1038/s41556-023-01274-x",

language = "English",

volume = "25",

pages = "1821--1832",

journal = "Nature Cell Biology",

issn = "1465-7392",

publisher = "Nature Research",

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}

Giafaglione, JM, Crowell, PD, Delcourt, AML, Hashimoto, T, Ha, SM, Atmakuri, A, Nunley, NM, Dang, RMA, Tian, M, Diaz, JA, Tika, E, Payne, MC, Burkhart, DL, Li, D, Navone, NM, Corey, E, Nelson, PS, Lin, NYC, Blanpain, C, Ellis, L, Boutros, PC & Goldstein, AS 2023, 'Prostate lineage-specific metabolism governs luminal differentiation and response to antiandrogen treatment', Nature Cell Biology, vol. 25, no. 12, pp. 1821-1832. https://doi.org/10.1038/s41556-023-01274-x

TY - JOUR

T1 - Prostate lineage-specific metabolism governs luminal differentiation and response to antiandrogen treatment

AU - Giafaglione, Jenna M.

AU - Crowell, Preston D.

AU - Delcourt, Amelie M.L.

AU - Hashimoto, Takao

AU - Ha, Sung Min

AU - Atmakuri, Aishwarya

AU - Nunley, Nicholas M.

AU - Dang, Rachel M.A.

AU - Tian, Mao

AU - Diaz, Johnny A.

AU - Tika, Elisavet

AU - Payne, Marie C.

AU - Burkhart, Deborah L.

AU - Li, Dapei

AU - Navone, Nora M.

AU - Corey, Eva

AU - Nelson, Peter S.

AU - Lin, Neil Y.C.

AU - Blanpain, Cedric

AU - Ellis, Leigh

AU - Boutros, Paul C.

AU - Goldstein, Andrew S.

PY - 2023/12

Y1 - 2023/12

N2 - Lineage transitions are a central feature of prostate development, tumourigenesis and treatment resistance. While epigenetic changes are well known to drive prostate lineage transitions, it remains unclear how upstream metabolic signalling contributes to the regulation of prostate epithelial identity. To fill this gap, we developed an approach to perform metabolomics on primary prostate epithelial cells. Using this approach, we discovered that the basal and luminal cells of the prostate exhibit distinct metabolomes and nutrient utilization patterns. Furthermore, basal-to-luminal differentiation is accompanied by increased pyruvate oxidation. We establish the mitochondrial pyruvate carrier and subsequent lactate accumulation as regulators of prostate luminal identity. Inhibition of the mitochondrial pyruvate carrier or supplementation with exogenous lactate results in large-scale chromatin remodelling, influencing both lineage-specific transcription factors and response to antiandrogen treatment. These results establish reciprocal regulation of metabolism and prostate epithelial lineage identity.

AB - Lineage transitions are a central feature of prostate development, tumourigenesis and treatment resistance. While epigenetic changes are well known to drive prostate lineage transitions, it remains unclear how upstream metabolic signalling contributes to the regulation of prostate epithelial identity. To fill this gap, we developed an approach to perform metabolomics on primary prostate epithelial cells. Using this approach, we discovered that the basal and luminal cells of the prostate exhibit distinct metabolomes and nutrient utilization patterns. Furthermore, basal-to-luminal differentiation is accompanied by increased pyruvate oxidation. We establish the mitochondrial pyruvate carrier and subsequent lactate accumulation as regulators of prostate luminal identity. Inhibition of the mitochondrial pyruvate carrier or supplementation with exogenous lactate results in large-scale chromatin remodelling, influencing both lineage-specific transcription factors and response to antiandrogen treatment. These results establish reciprocal regulation of metabolism and prostate epithelial lineage identity.

UR - https://www.scopus.com/pages/publications/85178429295

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DO - 10.1038/s41556-023-01274-x

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AN - SCOPUS:85178429295

SN - 1465-7392

VL - 25

SP - 1821

EP - 1832

JO - Nature Cell Biology

JF - Nature Cell Biology

IS - 12

ER -

Prostate lineage-specific metabolism governs luminal differentiation and response to antiandrogen treatment

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