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DNA methylation signature of chronic low-grade inflammation and its role in cardio-respiratory diseases

Author: Bis Joshua C.
Bodinier Barbara
Brody Jennifer A.
Cardona Alexia
Chadeau-Hyam Marc
Chen Wei
Cugliari Giovanni
Deary Ian J.
Doerr Macus
Farlik Matthias
Fiorito Giovanni
Ghanbari Mohsen
Grabe Hans J.
Graf-Schindler Johanna
Gào Xin
Joehanes Roby
Järvelin Marjo-Riitta
Karhunen Ville
Koenig Wolfgang
Kuehnel Brigitte
Lehne Benjamin
Loh Marie
Mandaviya Pooja R.
Marioni Riccardo E.
Marouli Eirini
Miller Andrew H.
Mishra Pashupati P.
Mustafa Rima
Nauck Matthias
Palaniswamy Saranya
Peters Annette
Psaty Bruce M.
Rathmann Wolfgang
Robinson Oliver
Schlosser Pascal
Selvin Elizabeth
Smith Alicia K.
Sotoodehnia Nona
Teumer Alexander
Torres Mylin A.
Tsai Pei Chien
van der Harst Pim
van Meurs Joyce B.J.
Verweij Niek
Walton Esther
Weninger Wolfgang
Wielscher Matthias
Wilson Rory
Xia Yujing
Zhang Tao
Zhang Yan
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 03/05/2022
Field of study

We performed a multi-ethnic Epigenome Wide Association study on 22,774 individuals to describe the DNA methylation signature of chronic low-grade inflammation as measured by C-Reactive protein (CRP). We find 1,511 independent differentially methylated loci associated with CRP. These CpG sites show correlation structures across chromosomes, and are primarily situated in euchromatin, depleted in CpG islands. These genomic loci are predominantly situated in transcription factor binding sites and genomic enhancer regions. Mendelian randomization analysis suggests altered CpG methylation is a consequence of increased blood CRP levels. Mediation analysis reveals obesity and smoking as important underlying driving factors for changed CpG methylation. Finally, we find that an activated CpG signature significantly increases the risk for cardiometabolic diseases and COPD.publishedVersionPeer reviewe

Proceedings - University of Groningen

University of Groningen

ARTS repository - University of Groningen

EUR Research Repository

Trepo - Institutional Repository of Tampere University

Dissertations of the University of Groningen

DNA methylation signature of chronic low-grade inflammation and its role in cardio-respiratory diseases.

Author: Baccarelli Andrea A
Beekman Marian
Bell Jordana T
BIOS consortium
Bis Joshua C
Bodinier Barbara
Boerwinkle Eric
Brenner Hermann
Brody Jennifer A
Cardona Alexia
Chadeau-Hyam Marc
Chambers John C
Chen Wei
Colicino Elena
Conneely Karen N
Cugliari Giovanni
Deary Ian J
Dehghan Abbas
Deloukas Panos
Doerr Macus
Elliott Paul
Farlik Matthias
Fiorito Giovanni
Fisher Krista
Ghanbari Mohsen
Grabe Hans J
Graf-Schindler Johanna
Guan Weihua
Gào Xin
Heijmans Bastiaan T
Herzig Karl-Heinz
Hurme Mikko A
Iacoviello Licia
Joehanes Roby
Järvelin Marjo-Riitta
Karhunen Ville
Kasela Silva
Koenig Wolfgang
Kooner Jaspal S
Krogh Vittorio
Kuehnel Brigitte
Kähönen Mika
Köttgen Anna
Lehne Benjamin
Lehtimäki Terho
Levy Daniel
Li Shengxu
Loh Marie
Mandaviya Pooja R
Marioni Riccardo E
Marouli Eirini
Matullo Giuseppe
Milani Lili
Miller Andrew H
Mishra Pashupati P
Mustafa Rima
Nauck Matthias
Ong Ken K
Palaniswamy Saranya
Panico Salvatore
Peters Annette
Psaty Bruce M
Raitakari Olli T
Rathmann Wolfgang
Relton Caroline
Robinson Oliver
Sacerdote Carlotta
Schlosser Pascal
Selvin Elizabeth
Smith Alicia K
Sotoodehnia Nona
Tanaka Toshiko
Teumer Alexander
Torres Mylin A
Tsai Pei-Chien
Tumino Rosario
Tzala Evangelia
van der Harst Pim
van Meurs Joyce BJ
Verweij Niek
Vineis Paolo
Waite Lindsay L
Waldenberger Melanie
Walton Esther
Weninger Wolfgang
Wielscher Matthias
Wilson Rory
Xia Yujing
Zhang Tao
Zhang Yan
Publication venue: Nat Commun
Publication date: 01/01/2022
Field of study

LSHTM Research Online

PubMed Central

Edinburgh Research Explorer

Apollo (Cambridge)

Institutional Research Information System University of Turin

DNA methylation signature of chronic low-grade inflammation and its role in cardio-respiratory diseases

Author: Baccarelli A. A. (Andrea A.)
Beekman M. (Marian)
Bell J. T. (Jordana T.)
BIOS consortium
Bis J. C. (Joshua C.)
Bodinier B. (Barbara)
Boerwinkle E. (Eric)
Brenner H. (Hermann)
Brody J. A. (Jennifer A.)
Cardona A. (Alexia)
Chadeau-Hyam M. (Marc)
Chambers J. C. (John C.)
Chen W. (Wei)
Colicino E. (Elena)
Conneely K. N. (Karen N.)
Cugliari G. (Giovanni)
Deary I. J. (Ian J.)
Dehghan A. (Abbas)
Deloukas P. (Panos)
Doerr M. (Macus)
Elliott P. (Paul)
Farlik M. (Matthias)
Fiorito G. (Giovanni)
Fisher K. (Krista)
Gao X. (Xin)
Ghanbari M. (Mohsen)
Grabe H. J. (Hans J.)
Graf-Schindler J. (Johanna)
Guan W. (Weihua)
Heijmans B. T. (Bastiaan T.)
Herzig K.-H. (Karl-Heinz)
Hurme M. A. (Mikko A.)
Iacoviello L. (Licia)
Joehanes R. (Roby)
Järvelin M.-R. (Marjo-Riitta)
Kahonen M. (Mika)
Karhunen V. (Ville)
Kasela S. (Silva)
Koenig W. (Wolfgang)
Kooner J. S. (Jaspal S.)
Kottgen A. (Anna)
Krogh V. (Vittorio)
Kuehnel B. (Brigitte)
Lehne B. (Benjamin)
Lehtimaki T. (Terho)
Levy D. (Daniel)
Li S. (Shengxu)
Loh M. (Marie)
Mandaviya P. R. (Pooja R.)
Marioni R. E. (Riccardo E.)
Marouli E. (Eirini)
Matullo G. (Giuseppe)
Milani L. (Lili)
Miller A. H. (Andrew H.)
Mishra P. P. (Pashupati P.)
Mustafa R. (Rima)
Nauck M. (Matthias)
Ong K. K. (Ken K.)
Palaniswamy S. (Saranya)
Panico S. (Salvatore)
Peters A. (Annette)
Psaty B. M. (Bruce M.)
Raitakari O. T. (Olli T.)
Rathmann W. (Wolfgang)
Relton C. (Caroline)
Robinson O. (Oliver)
Sacerdote C. (Carlotta)
Schlosser P. (Pascal)
Selvin E. (Elizabeth)
Smith A. K. (Alicia K.)
Sotoodehnia N. (Nona)
Tanaka T. (Toshiko)
Teumer A. (Alexander)
Torres M. A. (Mylin A.)
Tsai P.-C. (Pei-Chien)
Tumino R. (Rosario)
Tzala E. (Evangelia)
van der Harst P. (Pim)
van Meurs J. B. (Joyce B. J.)
Verweij N. (Niek)
Vineis P. (Paolo)
Waite L. L. (Lindsay L.)
Waldenberger M. (Melanie)
Walton E. (Esther)
Weninger W. (Wolfgang)
Wielscher M. (Matthias)
Wilson R. (Rory)
Xia Y. (Yujing)
Zhang T. (Tao)
Zhang Y. (Yan)
Publication venue: Springer Nature
Publication date: 01/01/2022
Field of study

Abstract We performed a multi-ethnic Epigenome Wide Association study on 22,774 individuals to describe the DNA methylation signature of chronic low-grade inflammation as measured by C-Reactive protein (CRP). We find 1,511 independent differentially methylated loci associated with CRP. These CpG sites show correlation structures across chromosomes, and are primarily situated in euchromatin, depleted in CpG islands. These genomic loci are predominantly situated in transcription factor binding sites and genomic enhancer regions. Mendelian randomization analysis suggests altered CpG methylation is a consequence of increased blood CRP levels. Mediation analysis reveals obesity and smoking as important underlying driving factors for changed CpG methylation. Finally, we find that an activated CpG signature significantly increases the risk for cardiometabolic diseases and COPD

University of Oulu Repository - Jultika