Translational Activation of ATF4 through Mitochondrial Anaplerotic Metabolic Pathways Is Required for DLBCL Growth and Survival

Meng Li; Matthew R. Teater; Jun Young Hong; Noel R. Park; Cihangir Duy; Hao Shen; Ling Wang; Zhengming Chen; Leandro Cerchietti; Shawn M. Davidson; Hening Lin; Ari Melnick

doi:10.1158/2643-3230.BCD-20-0183

Translational Activation of ATF4 through Mitochondrial Anaplerotic Metabolic Pathways Is Required for DLBCL Growth and Survival

Meng Li, Matthew R. Teater, Jun Young Hong, Noel R. Park, Cihangir Duy, Hao Shen, Ling Wang, Zhengming Chen, Leandro Cerchietti, Shawn M. Davidson, Hening Lin, Ari Melnick

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

15 Scopus citations

Abstract

Diffuse large B-cell lymphomas (DLBCL) are broadly dependent on anaplerotic metabolism regulated by mitochondrial SIRT3. Herein we find that translational upregulation of ATF4 is coupled with anaplerotic metabolism in DLBCLs due to nutrient deprivation caused by SIRT3 driving rapid flux of glutamine into the tricarboxylic acid (TCA) cycle. SIRT3 depletion led to ATF4 downregulation and cell death, which was rescued by ectopic ATF4 expression. Mechanistically, ATF4 translation is inhibited in SIRT3-deficient cells due to the increased pools of amino acids derived from compensatory autophagy and decreased glutamine consumption by the TCA cycle. Absence of ATF4 further aggravates this state through downregulation of its target genes, including genes for amino acid biosynthesis and import. Collectively, we identify a SIRT3–ATF4 axis required to maintain survival of DLBCL cells by enabling them to optimize amino acid uptake and utilization. Targeting ATF4 translation can potentiate the cytotoxic effect of SIRT3 inhibitor to DLBCL cells.

Original language	English
Pages (from-to)	50-65
Number of pages	16
Journal	Blood cancer discovery
Volume	3
Issue number	1
DOIs	https://doi.org/10.1158/2643-3230.BCD-20-0183
State	Published - Jan 1 2022

Keywords

Activating Transcription Factor 4/genetics
Amino Acids/metabolism
Citric Acid Cycle
Glutamine/metabolism
Humans
Lymphoma, Large B-Cell, Diffuse/genetics
Mitochondria/metabolism
Sirtuin 3/genetics

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10.1158/2643-3230.BCD-20-0183

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title = "Translational Activation of ATF4 through Mitochondrial Anaplerotic Metabolic Pathways Is Required for DLBCL Growth and Survival",

abstract = "Diffuse large B-cell lymphomas (DLBCL) are broadly dependent on anaplerotic metabolism regulated by mitochondrial SIRT3. Herein we find that translational upregulation of ATF4 is coupled with anaplerotic metabolism in DLBCLs due to nutrient deprivation caused by SIRT3 driving rapid flux of glutamine into the tricarboxylic acid (TCA) cycle. SIRT3 depletion led to ATF4 downregulation and cell death, which was rescued by ectopic ATF4 expression. Mechanistically, ATF4 translation is inhibited in SIRT3-deficient cells due to the increased pools of amino acids derived from compensatory autophagy and decreased glutamine consumption by the TCA cycle. Absence of ATF4 further aggravates this state through downregulation of its target genes, including genes for amino acid biosynthesis and import. Collectively, we identify a SIRT3–ATF4 axis required to maintain survival of DLBCL cells by enabling them to optimize amino acid uptake and utilization. Targeting ATF4 translation can potentiate the cytotoxic effect of SIRT3 inhibitor to DLBCL cells.",

keywords = "Activating Transcription Factor 4/genetics, Amino Acids/metabolism, Citric Acid Cycle, Glutamine/metabolism, Humans, Lymphoma, Large B-Cell, Diffuse/genetics, Mitochondria/metabolism, Sirtuin 3/genetics",

author = "Meng Li and Teater, {Matthew R.} and Hong, {Jun Young} and Park, {Noel R.} and Cihangir Duy and Hao Shen and Ling Wang and Zhengming Chen and Leandro Cerchietti and Davidson, {Shawn M.} and Hening Lin and Ari Melnick",

note = "Publisher Copyright: {\textcopyright}2021 The Authors; Published by the American Association for Cancer Research.",

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doi = "10.1158/2643-3230.BCD-20-0183",

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T1 - Translational Activation of ATF4 through Mitochondrial Anaplerotic Metabolic Pathways Is Required for DLBCL Growth and Survival

AU - Li, Meng

AU - Teater, Matthew R.

AU - Hong, Jun Young

AU - Park, Noel R.

AU - Duy, Cihangir

AU - Shen, Hao

AU - Wang, Ling

AU - Chen, Zhengming

AU - Cerchietti, Leandro

AU - Davidson, Shawn M.

AU - Lin, Hening

AU - Melnick, Ari

PY - 2022/1/1

Y1 - 2022/1/1

N2 - Diffuse large B-cell lymphomas (DLBCL) are broadly dependent on anaplerotic metabolism regulated by mitochondrial SIRT3. Herein we find that translational upregulation of ATF4 is coupled with anaplerotic metabolism in DLBCLs due to nutrient deprivation caused by SIRT3 driving rapid flux of glutamine into the tricarboxylic acid (TCA) cycle. SIRT3 depletion led to ATF4 downregulation and cell death, which was rescued by ectopic ATF4 expression. Mechanistically, ATF4 translation is inhibited in SIRT3-deficient cells due to the increased pools of amino acids derived from compensatory autophagy and decreased glutamine consumption by the TCA cycle. Absence of ATF4 further aggravates this state through downregulation of its target genes, including genes for amino acid biosynthesis and import. Collectively, we identify a SIRT3–ATF4 axis required to maintain survival of DLBCL cells by enabling them to optimize amino acid uptake and utilization. Targeting ATF4 translation can potentiate the cytotoxic effect of SIRT3 inhibitor to DLBCL cells.

AB - Diffuse large B-cell lymphomas (DLBCL) are broadly dependent on anaplerotic metabolism regulated by mitochondrial SIRT3. Herein we find that translational upregulation of ATF4 is coupled with anaplerotic metabolism in DLBCLs due to nutrient deprivation caused by SIRT3 driving rapid flux of glutamine into the tricarboxylic acid (TCA) cycle. SIRT3 depletion led to ATF4 downregulation and cell death, which was rescued by ectopic ATF4 expression. Mechanistically, ATF4 translation is inhibited in SIRT3-deficient cells due to the increased pools of amino acids derived from compensatory autophagy and decreased glutamine consumption by the TCA cycle. Absence of ATF4 further aggravates this state through downregulation of its target genes, including genes for amino acid biosynthesis and import. Collectively, we identify a SIRT3–ATF4 axis required to maintain survival of DLBCL cells by enabling them to optimize amino acid uptake and utilization. Targeting ATF4 translation can potentiate the cytotoxic effect of SIRT3 inhibitor to DLBCL cells.

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KW - Glutamine/metabolism

KW - Humans

KW - Lymphoma, Large B-Cell, Diffuse/genetics

KW - Mitochondria/metabolism

KW - Sirtuin 3/genetics

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JO - Blood cancer discovery

JF - Blood cancer discovery

IS - 1

ER -

Translational Activation of ATF4 through Mitochondrial Anaplerotic Metabolic Pathways Is Required for DLBCL Growth and Survival

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