Misregulation of Drosophila Myc Disrupts Circadian Behavior and Metabolism

Annie L. Hsieh; Xiangzhong Zheng; Zhifeng Yue; Zachary E. Stine; Anthony Mancuso; Seth D. Rhoades; Rebekah Brooks; Aalim M. Weljie; Robert N. Eisenman; Amita Sehgal; Chi V. Dang

doi:10.1016/j.celrep.2019.10.022

Misregulation of Drosophila Myc Disrupts Circadian Behavior and Metabolism

Annie L. Hsieh, Xiangzhong Zheng, Zhifeng Yue, Zachary E. Stine, Anthony Mancuso, Seth D. Rhoades, Rebekah Brooks, Aalim M. Weljie, Robert N. Eisenman, Amita Sehgal, Chi V. Dang

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

Abstract

Drosophila Myc (dMyc) is highly conserved and functions as a transcription factor similar to mammalian Myc. We previously found that oncogenic Myc disrupts the molecular clock in cancer cells. Here, we demonstrate that misregulation of dMyc expression affects Drosophila circadian behavior. dMyc overexpression results in a high percentage of arrhythmic flies, concomitant with increases in the expression of clock genes cyc, tim, cry, and cwo. Conversely, flies with hypomorphic mutations in dMyc exhibit considerable arrhythmia, which can be rescued by loss of dMnt, a suppressor of dMyc activity. Metabolic profiling of fly heads revealed that loss of dMyc and its overexpression alter steady-state metabolite levels and have opposing effects on histidine, the histamine precursor, which is rescued in dMyc mutants by ablation of dMnt and could contribute to effects of dMyc on locomotor behavior. Our results demonstrate a role of dMyc in modulating Drosophila circadian clock, behavior, and metabolism.

Original language	English (US)
Pages (from-to)	1778-1788.e4
Journal	Cell Reports
Volume	29
Issue number	7
DOIs	https://doi.org/10.1016/j.celrep.2019.10.022
State	Published - Nov 12 2019
Externally published	Yes

ASJC Scopus subject areas

General Biochemistry, Genetics and Molecular Biology

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10.1016/j.celrep.2019.10.022

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title = "Misregulation of Drosophila Myc Disrupts Circadian Behavior and Metabolism",

abstract = "Drosophila Myc (dMyc) is highly conserved and functions as a transcription factor similar to mammalian Myc. We previously found that oncogenic Myc disrupts the molecular clock in cancer cells. Here, we demonstrate that misregulation of dMyc expression affects Drosophila circadian behavior. dMyc overexpression results in a high percentage of arrhythmic flies, concomitant with increases in the expression of clock genes cyc, tim, cry, and cwo. Conversely, flies with hypomorphic mutations in dMyc exhibit considerable arrhythmia, which can be rescued by loss of dMnt, a suppressor of dMyc activity. Metabolic profiling of fly heads revealed that loss of dMyc and its overexpression alter steady-state metabolite levels and have opposing effects on histidine, the histamine precursor, which is rescued in dMyc mutants by ablation of dMnt and could contribute to effects of dMyc on locomotor behavior. Our results demonstrate a role of dMyc in modulating Drosophila circadian clock, behavior, and metabolism.",

author = "Hsieh, {Annie L.} and Xiangzhong Zheng and Zhifeng Yue and Stine, {Zachary E.} and Anthony Mancuso and Rhoades, {Seth D.} and Rebekah Brooks and Weljie, {Aalim M.} and Eisenman, {Robert N.} and Amita Sehgal and Dang, {Chi V.}",

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doi = "10.1016/j.celrep.2019.10.022",

language = "English (US)",

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AU - Hsieh, Annie L.

AU - Zheng, Xiangzhong

AU - Yue, Zhifeng

AU - Stine, Zachary E.

AU - Mancuso, Anthony

AU - Rhoades, Seth D.

AU - Brooks, Rebekah

AU - Weljie, Aalim M.

AU - Eisenman, Robert N.

AU - Sehgal, Amita

AU - Dang, Chi V.

PY - 2019/11/12

Y1 - 2019/11/12

N2 - Drosophila Myc (dMyc) is highly conserved and functions as a transcription factor similar to mammalian Myc. We previously found that oncogenic Myc disrupts the molecular clock in cancer cells. Here, we demonstrate that misregulation of dMyc expression affects Drosophila circadian behavior. dMyc overexpression results in a high percentage of arrhythmic flies, concomitant with increases in the expression of clock genes cyc, tim, cry, and cwo. Conversely, flies with hypomorphic mutations in dMyc exhibit considerable arrhythmia, which can be rescued by loss of dMnt, a suppressor of dMyc activity. Metabolic profiling of fly heads revealed that loss of dMyc and its overexpression alter steady-state metabolite levels and have opposing effects on histidine, the histamine precursor, which is rescued in dMyc mutants by ablation of dMnt and could contribute to effects of dMyc on locomotor behavior. Our results demonstrate a role of dMyc in modulating Drosophila circadian clock, behavior, and metabolism.

AB - Drosophila Myc (dMyc) is highly conserved and functions as a transcription factor similar to mammalian Myc. We previously found that oncogenic Myc disrupts the molecular clock in cancer cells. Here, we demonstrate that misregulation of dMyc expression affects Drosophila circadian behavior. dMyc overexpression results in a high percentage of arrhythmic flies, concomitant with increases in the expression of clock genes cyc, tim, cry, and cwo. Conversely, flies with hypomorphic mutations in dMyc exhibit considerable arrhythmia, which can be rescued by loss of dMnt, a suppressor of dMyc activity. Metabolic profiling of fly heads revealed that loss of dMyc and its overexpression alter steady-state metabolite levels and have opposing effects on histidine, the histamine precursor, which is rescued in dMyc mutants by ablation of dMnt and could contribute to effects of dMyc on locomotor behavior. Our results demonstrate a role of dMyc in modulating Drosophila circadian clock, behavior, and metabolism.

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Misregulation of Drosophila Myc Disrupts Circadian Behavior and Metabolism

Abstract

ASJC Scopus subject areas

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