Please use this identifier to cite or link to this item: https://scholarbank.nus.edu.sg/handle/10635/246650
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dc.titleMultiomics analyses reveal dynamic bioenergetic pathways and functional remodeling of the heart during intermittent fasting
dc.contributor.authorArumugam, TV
dc.contributor.authorAlli-Shaik, A
dc.contributor.authorLiehn, EA
dc.contributor.authorSelvaraji, S
dc.contributor.authorPoh, L
dc.contributor.authorRajeev, V
dc.contributor.authorCho, Y
dc.contributor.authorCho, Y
dc.contributor.authorKim, J
dc.contributor.authorKim, J
dc.contributor.authorSwa, HLF
dc.contributor.authorHao, DTZ
dc.contributor.authorRattanasopa, C
dc.contributor.authorFann, DYW
dc.contributor.authorMayan, DC
dc.contributor.authorNg, GYQ
dc.contributor.authorBaik, SH
dc.contributor.authorMallilankaraman, K
dc.contributor.authorGelderblom, M
dc.contributor.authorDrummond, GR
dc.contributor.authorSobey, CG
dc.contributor.authorKennedy, BK
dc.contributor.authorSingaraja, RR
dc.contributor.authorMattson, MP
dc.contributor.authorJo, DG
dc.contributor.authorGunaratne, J
dc.date.accessioned2024-01-08T01:49:44Z
dc.date.available2024-01-08T01:49:44Z
dc.date.issued2023-09-01
dc.identifier.citationArumugam, TV, Alli-Shaik, A, Liehn, EA, Selvaraji, S, Poh, L, Rajeev, V, Cho, Y, Cho, Y, Kim, J, Kim, J, Swa, HLF, Hao, DTZ, Rattanasopa, C, Fann, DYW, Mayan, DC, Ng, GYQ, Baik, SH, Mallilankaraman, K, Gelderblom, M, Drummond, GR, Sobey, CG, Kennedy, BK, Singaraja, RR, Mattson, MP, Jo, DG, Gunaratne, J (2023-09-01). Multiomics analyses reveal dynamic bioenergetic pathways and functional remodeling of the heart during intermittent fasting. eLife 12 : RP89214-. ScholarBank@NUS Repository.
dc.identifier.issn2050-084X
dc.identifier.urihttps://scholarbank.nus.edu.sg/handle/10635/246650
dc.description.abstractIntermittent fasting (IF) has been shown to reduce cardiovascular risk factors in both animals and humans, and can protect the heart against ischemic injury in models of myocardial infarction. However, the underlying molecular mechanisms behind these effects remain unclear. To shed light on the molecular and cellular adaptations of the heart to IF, we conducted comprehensive system-wide analyses of the proteome, phosphoproteome, and transcriptome, followed by functional analysis. Using advanced mass spectrometry, we profiled the proteome and phosphopro-teome of heart tissues obtained from mice that were maintained on daily 12-or 16 hr fasting, every-other-day fasting, or ad libitum control feeding regimens for 6 months. We also performed RNA sequencing to evaluate whether the observed molecular responses to IF occur at the transcriptional or post-transcriptional levels. Our analyses revealed that IF significantly affected pathways that regulate cyclic GMP signaling, lipid and amino acid metabolism, cell adhesion, cell death, and inflammation. Furthermore, we found that the impact of IF on different metabolic processes varied depending on the length of the fasting regimen. Short IF regimens showed a higher correlation of pathway alteration, while longer IF regimens had an inverse correlation of metabolic processes such as fatty acid oxidation and immune processes. Additionally, functional echocardiographic analyses demonstrated that IF enhances stress-induced cardiac performance. Our systematic multi-omics study provides a molecular framework for understanding how IF impacts the heart’s function and its vulnerability to injury and disease.
dc.publishereLife Sciences Publications, Ltd
dc.sourceElements
dc.subjectRNA sequencing
dc.subjectheart
dc.subjectintermittent fasting
dc.subjectmedicine
dc.subjectmetabolism
dc.subjectmouse
dc.subjectphosphoproteomics
dc.subjectproteomics
dc.subjectregenerative medicine
dc.subjectstem cells
dc.subjectHumans
dc.subjectMice
dc.subjectAnimals
dc.subjectIntermittent Fasting
dc.subjectMultiomics
dc.subjectProteome
dc.subjectFasting
dc.subjectEnergy Metabolism
dc.typeArticle
dc.date.updated2024-01-04T02:05:09Z
dc.contributor.departmentPHYSIOLOGY
dc.contributor.departmentMECHANOBIOLOGY INSTITUTE
dc.contributor.departmentPHARMACOLOGY
dc.contributor.departmentDUKE-NUS MEDICAL SCHOOL
dc.contributor.departmentMEDICINE
dc.contributor.departmentPHYSIOLOGY
dc.contributor.departmentBIOCHEMISTRY
dc.contributor.departmentCANCER SCIENCE INSTITUTE OF SINGAPORE
dc.description.sourcetitleeLife
dc.description.volume12
dc.description.pageRP89214-
dc.published.statePublished
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