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Maléne Lindholm, PhD
dkNet webinar
March 8, 2024
The multi-omic response to exercise training
across rat tissues
Data dissemination through the MoTrPAC data hub
Physical inactivity is a major cause of chronic disease
• Regular exercise improves
metabolic health and reduces
risk of chronic disease1
• Exercise has positive effect on
treatment of at least 26 different
diseases2
• Physically active individuals tend
to live longer3
1
Booth FW, et al., Compr Physiol. 2012
2
Pedersen BK and Saltin B, Scand J Med Sci Sports 2015
3
Arem H, et al., JAMA Intern Med. 2015
Physical inactivity is a major cause of chronic disease
• Regular exercise improves
metabolic health and reduces
risk of chronic disease1
• Exercise has positive effect on
treatment of at least 26 different
diseases2
• Physically active individuals tend
to live longer3
1
Booth FW, et al., Compr Physiol. 2012
2
Pedersen BK and Saltin B, Scand J Med Sci Sports 2015
3
Arem H, et al., JAMA Intern Med. 2015
There is a limited understanding of the underlying molecular mechanisms by
which exercise promotes health and prevents disease
Study Species Exercise type
Sample
size
Number of
tissues
Genomics
Epigen-
omics
Transcript-
omics
Proteomics
Metabolomics/
Lipidomics
HERITAGE
Family Study
(1992-2013)
Human
Endurance training
(20 w)
~650 1-2 X Muscle (N=78) Targeted
Robbins,
2021 Nature
Metab.
Human
Endurance training
(20 w)
650
(HERITA
GE)
1 (plasma) X
Contrepois,
2020 Cell
Human Acute endurance 36
1 (blood/
plasma) X X X
Robinson,
2017 Cell
Metab.
Human
HIIT, resistance,
combined (12 w)
72 1 (muscle) X X X Targeted
Sato, 2022
Cell Metab.
Mouse Acute endurance
5-6 per
group
8 X
Existing exercise omics studies are limited
The Molecular Transducers of Physical Activity
Consortium (MoTrPAC)
Sanford, Nogiec, Lindholm et al., Cell 2020
The Molecular Transducers of Physical Activity
Consortium (MoTrPAC)
Sanford, Nogiec, Lindholm et al., Cell 2020
Study Species Exercise type
Sample
size
Number of
tissues
Genomics
Epigen-
omics
Transcript-
omics
Proteomics
Metabolomics/
Lipidomics
HERITAGE
Family Study
(1992-2013)
Human
Endurance training
(20 w)
~650 1-2 X Muscle (N=78) Targeted
Robbins,
2021 Nature
Metab.
Human
Endurance training
(20 w)
650
(HERITA
GE)
1 (plasma) X
Contrepois,
2020 Cell
Human Acute endurance 36
1 (blood/
plasma) X X X
Robinson,
2017 Cell
Metab.
Human
HIIT, resistance,
combined (12 w)
72 1 (muscle) X X X Targeted
Sato, 2022
Cell Metab.
Mouse Acute endurance
5-6 per
group
8 X
MoTrPAC
animal
studies
Rat
Endurance, acute
and training (8 w)
3-6 per
group 19 X X X X
MoTrPAC
human
studies
Human
Endurance or
resistance, acute
and training (12 w)
~2000 3 X X X X X
Existing exercise omics studies are limited
MoTrPAC preclinical endurance training study
• Progressive protocol
• Male and female 6mo
animals
• Time-series
• Multiple tissues
• Multiple -omes
Phenotypic changes
Differentially regulated analytes
Training time (weeks)
Analyte A in Tissue T
Abundance
0 (SED) 1 2 4 8
Males
Females
1. Is the analyte level changing
at any time in either sex?
Training time (weeks)
Analyte A in Tissue T (males)
Abundance
0 (SED) 1 2 4 8
2. What are the per-time and per-sex
effects relative to the control?
Sedentary
Trained
Training-regulated analytes across -omes
Training-regulated analytes across -omes
(null, up, down) (null, up, down)
Males Females
X
1
2
3
4
5
6
7
8
9
*node size = N
features
Up-regulated
(at least one sex)
Null in both sexes
Down-regulated
(at least one sex)
Opposite directions
9 possible states per time point
Clustering analysis to visualize timewise changes
Clustering analysis to visualize timewise changes
Temporal dynamics of the multi-omic response to
exercise
Common analytical
questions
• What analytes increase in
abundance across both
sexes at 8 weeks?
• What proteins decrease in
abundance at all
timepoints in females
only?
• What is the top trajectory
for a certain –ome in a
certain tissue?
Exploring the multi-omic response to exercise training
Whole-body
responses to
training
Sex differences
in the training
response
Metabolic
adaptations
Multi-tissue
molecular
responses to
training
Exploring the multi-omic response to exercise training
Whole-body
responses to
training
Sex differences
in the training
response
Metabolic
adaptations
Organism-wide metabolic changes in response to
training
Increases in metabolic protein abundance and
acetylation in the liver
Exploring the multi-omic response to exercise training
Whole-body
responses to
training
Sex differences
in the training
response
Metabolic
adaptations
Sex differences in immune pathway responses in
adipose tissue and small intestine
Sex differences in lung protein phosphorylation with
training
Data dissemination through the
https://motrpac-data.org
Summary
• 19 tissues, 9 omes, 90 datasets
35,000 analytes regulated over the
training time course
• Substantial regulation of transcripts,
proteins, PTMs, metabolites
Unparalleled exercise biology molecular resource
• Pipelines for robust
statistical analysis and data
integration
• Analytical methods for
graphical representation of
temporal dynamics
Molecular dynamics in response to training
• Pathway analysis aid in biological
interpretation
• Computational and visualization
tools facilitate data access
R package
MoTrPAC Data Hub
Tools for exploration and interpretation
• Whole body responses
• Molecular hubs through interaction
networks
• Sex differences in exercise adaptation
• Metabolic adaptations
Mechanisms explaining health benefits of exercise
Acknowledgements
Joshua N. Adkins
Jose J. Almagro Armenteros
Mary Anne S. Amper
Julian Avila-Pacheco
Ali Tugrul Balci
Nasim Bararpour
Charles Burant
Steven Carr
Clarisa Chavez
Maria Chikina
Roxanne Chiu
Clary Clish
Surendra Dasari
Courtney Dennis
Charles R. Evans
Facundo M. Fernández
David Gaul
Nicole R. Gay‡
Yongchao Ge
Robert Gerszten
Marina A. Gritsenko
Kristy Guevara
Joshua R. Hansen
Krista M. Hennig
Zhenxin Hou
Chia-Jui Hung
Chelsea Hutchinson-Bunch
Olga Ilkayeva
Anna A. Ivanova
Pierre M. Jean Beltran‡
Christopher A. Jin
Maureen T. Kachman
Hasmik Keshishian
Ian R. Lanza
Jun Li
Marcas Bamman
Bryan Bergman
Daniel Bessesen
Thomas W. Buford
Toby L. Chambers
Paul M. Coen
Dan Cooper
Gary Cutter
Kishore Gadde
Bret H. Goodpaster
Fadia Haddad
Melissa Harris
Kim M. Huffman
Catherine Jankowski
Neil M. Johannsen
Wendy M. Kohrt
William E. Kraus
David Amar‡
Euan Ashley
Brian Bouverat
Elaine Cornell
Karen P. Dalton
Nicole Gagne
Trevor Hastie
Steven G. Hershman
Fang-Chi Hsu
David Jimenez-Morales
Christiaan Leeuwenburgh
Malene E. Lindholm
Ching-ju Lu
Shruti Marwaha
Sandy May
Michael E. Miller
Archana Natarajan Raja
Barbara Nicklas
Marco Pahor
W. Jack Rejeski
Jessica L. Rooney
Scott Rushing
Mihir Samdarshi
Cynthia L. Stowe
Christopher Teng
Rob Tibshirani
Russell Tracy
Michael P. Walkup
Matthew T. Wheeler
John Williams
Ashley Xia
Jimmy Zhen
Xueyun Liu
Kristal M. Maner-Smith
DR Mani
Gina M. Many
Nada Marjanovic
Matthew E. Monroe
Stephen B. Montgomery
Samuel Moore
Ronald J. Moore
Michael J. Muehlbauer
Charlie Mundorff
Daniel Nachun
Venugopalan D. Nair
K. Sreekumaran Nair
Michael D. Nestor
Christopher Newgard
German Nudelman
Eric A. Ortlund
Cadence Pearce
Vladislav A. Petyuk
Paul D. Piehowski
Hanna Pincas
Wei-Jun Qian
Irene Ramos
Alexander (Sasha) Raskind
Stas Rirak
Jeremy M. Robbins
Aliza B. Rubenstein
Frederique Ruf-Zamojski
Tyler J. Sagendorf
James A. Sanford
Evan Savage
Stuart C. Sealfon
Nitish Seenarine
Gregory R. Smith
Kevin S. Smith
Michael P. Snyder
Tanu Soni
Alec Steep
Yifei Sun
Karan Uppal
Sindhu Vangeti
Mital Vasoya
Nikolai G. Vetr
Alexandria Vornholt
Martin J. Walsh
Si Wu
Xuechen Yu
Elena Zaslavsky
Navid Zebarjadi
Tiantian Zhang
Bingqing Zhao
Bridget Lester
Edward Melanson
Kerrie L. Moreau
Nicolas Musi
Robert L. Newton Jr.
Shlomit Radom-Aizik
Megan E. Ramaker
Tuomo Rankinen
Blake B. Rasmussen
Eric Ravussin
Irene E. Schauer
Robert Schwartz
Lauren M. Sparks
Anna Thalacker-Mercer
Scott Trappe
Todd A. Trappe
Elena Volpi
Brent G. Albertson
Dam Bae
Elisabeth R. Barton
Sue C. Bodine
Frank Booth
Tiziana Caputo
Michael Cicha
Luis Gustavo Oliveria De Sousa
Karyn Esser
Roger Farrar
Laurie J. Goodyear
Andrea Hevener
Michael F. Hirshman
Bailey E. Jackson
Benjamin G. Ke
Kyle S. Kramer
Sarah J. Lessard
Ana C. Lira
Nathan S. Makarewicz
Andrea Marshall
Pasquale Nigro
Scott Powers
David M. Presby
Krithika Ramachandran
R. Scott Rector
Collyn Richards
Simon Schenk
John Thyfault
Zhen Yan
Chongzhi Zang
MoTrPAC is supported by the National Institutes of
Health (NIH) Common Fund through cooperative
agreements managed by the National Institute of
Diabetes and Digestive and Kidney Diseases (NIDDK),
National Institute of Arthritis and Musculoskeletal
Diseases (NIAMS), and National Institute on Aging
(NIA).
Coordinating
Centers
Preclinical Animal
Study Sites
Clinical Sites
‡ Lead Analysts Primary authors
Chemical Analysis Sites

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dkNET Webinar "The Multi-Omic Response to Exercise Training Across Rat Tissues: Data Dissemination Through the MoTrPAC Data Hub" 03/08/2024

  • 1. Maléne Lindholm, PhD dkNet webinar March 8, 2024 The multi-omic response to exercise training across rat tissues Data dissemination through the MoTrPAC data hub
  • 2. Physical inactivity is a major cause of chronic disease • Regular exercise improves metabolic health and reduces risk of chronic disease1 • Exercise has positive effect on treatment of at least 26 different diseases2 • Physically active individuals tend to live longer3 1 Booth FW, et al., Compr Physiol. 2012 2 Pedersen BK and Saltin B, Scand J Med Sci Sports 2015 3 Arem H, et al., JAMA Intern Med. 2015
  • 3. Physical inactivity is a major cause of chronic disease • Regular exercise improves metabolic health and reduces risk of chronic disease1 • Exercise has positive effect on treatment of at least 26 different diseases2 • Physically active individuals tend to live longer3 1 Booth FW, et al., Compr Physiol. 2012 2 Pedersen BK and Saltin B, Scand J Med Sci Sports 2015 3 Arem H, et al., JAMA Intern Med. 2015 There is a limited understanding of the underlying molecular mechanisms by which exercise promotes health and prevents disease
  • 4. Study Species Exercise type Sample size Number of tissues Genomics Epigen- omics Transcript- omics Proteomics Metabolomics/ Lipidomics HERITAGE Family Study (1992-2013) Human Endurance training (20 w) ~650 1-2 X Muscle (N=78) Targeted Robbins, 2021 Nature Metab. Human Endurance training (20 w) 650 (HERITA GE) 1 (plasma) X Contrepois, 2020 Cell Human Acute endurance 36 1 (blood/ plasma) X X X Robinson, 2017 Cell Metab. Human HIIT, resistance, combined (12 w) 72 1 (muscle) X X X Targeted Sato, 2022 Cell Metab. Mouse Acute endurance 5-6 per group 8 X Existing exercise omics studies are limited
  • 5. The Molecular Transducers of Physical Activity Consortium (MoTrPAC) Sanford, Nogiec, Lindholm et al., Cell 2020
  • 6. The Molecular Transducers of Physical Activity Consortium (MoTrPAC) Sanford, Nogiec, Lindholm et al., Cell 2020
  • 7. Study Species Exercise type Sample size Number of tissues Genomics Epigen- omics Transcript- omics Proteomics Metabolomics/ Lipidomics HERITAGE Family Study (1992-2013) Human Endurance training (20 w) ~650 1-2 X Muscle (N=78) Targeted Robbins, 2021 Nature Metab. Human Endurance training (20 w) 650 (HERITA GE) 1 (plasma) X Contrepois, 2020 Cell Human Acute endurance 36 1 (blood/ plasma) X X X Robinson, 2017 Cell Metab. Human HIIT, resistance, combined (12 w) 72 1 (muscle) X X X Targeted Sato, 2022 Cell Metab. Mouse Acute endurance 5-6 per group 8 X MoTrPAC animal studies Rat Endurance, acute and training (8 w) 3-6 per group 19 X X X X MoTrPAC human studies Human Endurance or resistance, acute and training (12 w) ~2000 3 X X X X X Existing exercise omics studies are limited
  • 8. MoTrPAC preclinical endurance training study • Progressive protocol • Male and female 6mo animals • Time-series • Multiple tissues • Multiple -omes
  • 10. Differentially regulated analytes Training time (weeks) Analyte A in Tissue T Abundance 0 (SED) 1 2 4 8 Males Females 1. Is the analyte level changing at any time in either sex? Training time (weeks) Analyte A in Tissue T (males) Abundance 0 (SED) 1 2 4 8 2. What are the per-time and per-sex effects relative to the control? Sedentary Trained
  • 13. (null, up, down) (null, up, down) Males Females X 1 2 3 4 5 6 7 8 9 *node size = N features Up-regulated (at least one sex) Null in both sexes Down-regulated (at least one sex) Opposite directions 9 possible states per time point Clustering analysis to visualize timewise changes
  • 14. Clustering analysis to visualize timewise changes
  • 15. Temporal dynamics of the multi-omic response to exercise Common analytical questions • What analytes increase in abundance across both sexes at 8 weeks? • What proteins decrease in abundance at all timepoints in females only? • What is the top trajectory for a certain –ome in a certain tissue?
  • 16. Exploring the multi-omic response to exercise training Whole-body responses to training Sex differences in the training response Metabolic adaptations
  • 18. Exploring the multi-omic response to exercise training Whole-body responses to training Sex differences in the training response Metabolic adaptations
  • 19. Organism-wide metabolic changes in response to training
  • 20. Increases in metabolic protein abundance and acetylation in the liver
  • 21. Exploring the multi-omic response to exercise training Whole-body responses to training Sex differences in the training response Metabolic adaptations
  • 22. Sex differences in immune pathway responses in adipose tissue and small intestine
  • 23. Sex differences in lung protein phosphorylation with training
  • 26. Summary • 19 tissues, 9 omes, 90 datasets 35,000 analytes regulated over the training time course • Substantial regulation of transcripts, proteins, PTMs, metabolites Unparalleled exercise biology molecular resource • Pipelines for robust statistical analysis and data integration • Analytical methods for graphical representation of temporal dynamics Molecular dynamics in response to training • Pathway analysis aid in biological interpretation • Computational and visualization tools facilitate data access R package MoTrPAC Data Hub Tools for exploration and interpretation • Whole body responses • Molecular hubs through interaction networks • Sex differences in exercise adaptation • Metabolic adaptations Mechanisms explaining health benefits of exercise
  • 27. Acknowledgements Joshua N. Adkins Jose J. Almagro Armenteros Mary Anne S. Amper Julian Avila-Pacheco Ali Tugrul Balci Nasim Bararpour Charles Burant Steven Carr Clarisa Chavez Maria Chikina Roxanne Chiu Clary Clish Surendra Dasari Courtney Dennis Charles R. Evans Facundo M. Fernández David Gaul Nicole R. Gay‡ Yongchao Ge Robert Gerszten Marina A. Gritsenko Kristy Guevara Joshua R. Hansen Krista M. Hennig Zhenxin Hou Chia-Jui Hung Chelsea Hutchinson-Bunch Olga Ilkayeva Anna A. Ivanova Pierre M. Jean Beltran‡ Christopher A. Jin Maureen T. Kachman Hasmik Keshishian Ian R. Lanza Jun Li Marcas Bamman Bryan Bergman Daniel Bessesen Thomas W. Buford Toby L. Chambers Paul M. Coen Dan Cooper Gary Cutter Kishore Gadde Bret H. Goodpaster Fadia Haddad Melissa Harris Kim M. Huffman Catherine Jankowski Neil M. Johannsen Wendy M. Kohrt William E. Kraus David Amar‡ Euan Ashley Brian Bouverat Elaine Cornell Karen P. Dalton Nicole Gagne Trevor Hastie Steven G. Hershman Fang-Chi Hsu David Jimenez-Morales Christiaan Leeuwenburgh Malene E. Lindholm Ching-ju Lu Shruti Marwaha Sandy May Michael E. Miller Archana Natarajan Raja Barbara Nicklas Marco Pahor W. Jack Rejeski Jessica L. Rooney Scott Rushing Mihir Samdarshi Cynthia L. Stowe Christopher Teng Rob Tibshirani Russell Tracy Michael P. Walkup Matthew T. Wheeler John Williams Ashley Xia Jimmy Zhen Xueyun Liu Kristal M. Maner-Smith DR Mani Gina M. Many Nada Marjanovic Matthew E. Monroe Stephen B. Montgomery Samuel Moore Ronald J. Moore Michael J. Muehlbauer Charlie Mundorff Daniel Nachun Venugopalan D. Nair K. Sreekumaran Nair Michael D. Nestor Christopher Newgard German Nudelman Eric A. Ortlund Cadence Pearce Vladislav A. Petyuk Paul D. Piehowski Hanna Pincas Wei-Jun Qian Irene Ramos Alexander (Sasha) Raskind Stas Rirak Jeremy M. Robbins Aliza B. Rubenstein Frederique Ruf-Zamojski Tyler J. Sagendorf James A. Sanford Evan Savage Stuart C. Sealfon Nitish Seenarine Gregory R. Smith Kevin S. Smith Michael P. Snyder Tanu Soni Alec Steep Yifei Sun Karan Uppal Sindhu Vangeti Mital Vasoya Nikolai G. Vetr Alexandria Vornholt Martin J. Walsh Si Wu Xuechen Yu Elena Zaslavsky Navid Zebarjadi Tiantian Zhang Bingqing Zhao Bridget Lester Edward Melanson Kerrie L. Moreau Nicolas Musi Robert L. Newton Jr. Shlomit Radom-Aizik Megan E. Ramaker Tuomo Rankinen Blake B. Rasmussen Eric Ravussin Irene E. Schauer Robert Schwartz Lauren M. Sparks Anna Thalacker-Mercer Scott Trappe Todd A. Trappe Elena Volpi Brent G. Albertson Dam Bae Elisabeth R. Barton Sue C. Bodine Frank Booth Tiziana Caputo Michael Cicha Luis Gustavo Oliveria De Sousa Karyn Esser Roger Farrar Laurie J. Goodyear Andrea Hevener Michael F. Hirshman Bailey E. Jackson Benjamin G. Ke Kyle S. Kramer Sarah J. Lessard Ana C. Lira Nathan S. Makarewicz Andrea Marshall Pasquale Nigro Scott Powers David M. Presby Krithika Ramachandran R. Scott Rector Collyn Richards Simon Schenk John Thyfault Zhen Yan Chongzhi Zang MoTrPAC is supported by the National Institutes of Health (NIH) Common Fund through cooperative agreements managed by the National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK), National Institute of Arthritis and Musculoskeletal Diseases (NIAMS), and National Institute on Aging (NIA). Coordinating Centers Preclinical Animal Study Sites Clinical Sites ‡ Lead Analysts Primary authors Chemical Analysis Sites