Expression patterns of cardiac aging in Drosophila

Leah Cannon; Alexander C. Zambon; Anthony Cammarato; Zhi Zhang; Georg Vogler; Matthew Munoz; Erika Taylor; Jérôme Cartry; Sanford I. Bernstein; Simon Melov; Rolf Bodmer

doi:10.1111/acel.12559

Expression patterns of cardiac aging in Drosophila

Leah Cannon, Alexander C. Zambon, Anthony Cammarato, Zhi Zhang, Georg Vogler, Matthew Munoz, Erika Taylor, Jérôme Cartry, Sanford I. Bernstein, Simon Melov, Rolf Bodmer

School of Medicine

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

22 Scopus citations

Abstract

Aging causes cardiac dysfunction, often leading to heart failure and death. The molecular basis of age-associated changes in cardiac structure and function is largely unknown. The fruit fly, Drosophila melanogaster, is well-suited to investigate the genetics of cardiac aging. Flies age rapidly over the course of weeks, benefit from many tools to easily manipulate their genome, and their heart has significant genetic and phenotypic similarities to the human heart. Here, we performed a cardiac-specific gene expression study on aging Drosophila and carried out a comparative meta-analysis with published rodent data. Pathway level transcriptome comparisons suggest that age-related, extra-cellular matrix remodeling and alterations in mitochondrial metabolism, protein handling, and contractile functions are conserved between Drosophila and rodent hearts. However, expression of only a few individual genes similarly changed over time between and even within species. We also examined gene expression in single fly hearts and found significant variability as has been reported in rodents. We propose that individuals may arrive at similar cardiac aging phenotypes via dissimilar transcriptional changes, including those in transcription factors and micro-RNAs. Finally, our data suggest the transcription factor Odd-skipped, which is essential for normal heart development, is also a crucial regulator of cardiac aging.

Original language	English (US)
Pages (from-to)	82-92
Number of pages	11
Journal	Aging Cell
Volume	16
Issue number	1
DOIs	https://doi.org/10.1111/acel.12559
State	Published - Feb 1 2017

Keywords

LysX
MMP1
Odd-skipped
arrhythmia
cardiomyopathy
heart
nanofluidics
senescence

ASJC Scopus subject areas

Aging
Cell Biology

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10.1111/acel.12559

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title = "Expression patterns of cardiac aging in Drosophila",

abstract = "Aging causes cardiac dysfunction, often leading to heart failure and death. The molecular basis of age-associated changes in cardiac structure and function is largely unknown. The fruit fly, Drosophila melanogaster, is well-suited to investigate the genetics of cardiac aging. Flies age rapidly over the course of weeks, benefit from many tools to easily manipulate their genome, and their heart has significant genetic and phenotypic similarities to the human heart. Here, we performed a cardiac-specific gene expression study on aging Drosophila and carried out a comparative meta-analysis with published rodent data. Pathway level transcriptome comparisons suggest that age-related, extra-cellular matrix remodeling and alterations in mitochondrial metabolism, protein handling, and contractile functions are conserved between Drosophila and rodent hearts. However, expression of only a few individual genes similarly changed over time between and even within species. We also examined gene expression in single fly hearts and found significant variability as has been reported in rodents. We propose that individuals may arrive at similar cardiac aging phenotypes via dissimilar transcriptional changes, including those in transcription factors and micro-RNAs. Finally, our data suggest the transcription factor Odd-skipped, which is essential for normal heart development, is also a crucial regulator of cardiac aging.",

keywords = "LysX, MMP1, Odd-skipped, arrhythmia, cardiomyopathy, heart, nanofluidics, senescence",

author = "Leah Cannon and Zambon, {Alexander C.} and Anthony Cammarato and Zhi Zhang and Georg Vogler and Matthew Munoz and Erika Taylor and J{\'e}r{\^o}me Cartry and Bernstein, {Sanford I.} and Simon Melov and Rolf Bodmer",

note = "Funding Information: This work was funded by the following grants: American Heart Association grant 10SDG4180089 (to AC); AFAR Research Grant (to AC); CSUPERB (CSU Program for Education and Research in Biotechnology) Grant (to AC and SIB); American Heart Association grant 10SDG2630130 (to AZ); NIH R01 GM32443 (to SIB); Larry L. Hillblom Foundation 2009-A-001-CTR (to SM); NIH P01 AG033456; NIH P01 HL098053, NIH R01 HL54732 and a Senior Scholar Award from the Ellison Medical Foundation (to RB). The authors wish to thank Nakissa N. Alayari and Joan Choi (Sanford Burnham Prebys Medical Discovery Institute), and Meera Cozhimuttam Viswanathan (Johns Hopkins University) for technical assistance. Publisher Copyright: {\textcopyright} 2017 The Authors. Aging Cell published by the Anatomical Society and John Wiley & Sons Ltd.",

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doi = "10.1111/acel.12559",

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AU - Cannon, Leah

AU - Zambon, Alexander C.

AU - Cammarato, Anthony

AU - Zhang, Zhi

AU - Vogler, Georg

AU - Munoz, Matthew

AU - Taylor, Erika

AU - Cartry, Jérôme

AU - Bernstein, Sanford I.

AU - Melov, Simon

AU - Bodmer, Rolf

N1 - Funding Information: This work was funded by the following grants: American Heart Association grant 10SDG4180089 (to AC); AFAR Research Grant (to AC); CSUPERB (CSU Program for Education and Research in Biotechnology) Grant (to AC and SIB); American Heart Association grant 10SDG2630130 (to AZ); NIH R01 GM32443 (to SIB); Larry L. Hillblom Foundation 2009-A-001-CTR (to SM); NIH P01 AG033456; NIH P01 HL098053, NIH R01 HL54732 and a Senior Scholar Award from the Ellison Medical Foundation (to RB). The authors wish to thank Nakissa N. Alayari and Joan Choi (Sanford Burnham Prebys Medical Discovery Institute), and Meera Cozhimuttam Viswanathan (Johns Hopkins University) for technical assistance. Publisher Copyright: © 2017 The Authors. Aging Cell published by the Anatomical Society and John Wiley & Sons Ltd.

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AB - Aging causes cardiac dysfunction, often leading to heart failure and death. The molecular basis of age-associated changes in cardiac structure and function is largely unknown. The fruit fly, Drosophila melanogaster, is well-suited to investigate the genetics of cardiac aging. Flies age rapidly over the course of weeks, benefit from many tools to easily manipulate their genome, and their heart has significant genetic and phenotypic similarities to the human heart. Here, we performed a cardiac-specific gene expression study on aging Drosophila and carried out a comparative meta-analysis with published rodent data. Pathway level transcriptome comparisons suggest that age-related, extra-cellular matrix remodeling and alterations in mitochondrial metabolism, protein handling, and contractile functions are conserved between Drosophila and rodent hearts. However, expression of only a few individual genes similarly changed over time between and even within species. We also examined gene expression in single fly hearts and found significant variability as has been reported in rodents. We propose that individuals may arrive at similar cardiac aging phenotypes via dissimilar transcriptional changes, including those in transcription factors and micro-RNAs. Finally, our data suggest the transcription factor Odd-skipped, which is essential for normal heart development, is also a crucial regulator of cardiac aging.

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KW - cardiomyopathy

KW - heart

KW - nanofluidics

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Expression patterns of cardiac aging in Drosophila

Abstract

Keywords

ASJC Scopus subject areas

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