Urinary peptides in heart failure: a link to molecular pathophysiology

Tianlin He; Michaela Mischak; Andrew L Clark; Ross T. Campbell; Christian Delles; Javier Díez; Gerasimos Filippatos; Alexandre Mebazaa; John J V McMurray; Arantxa González; Julia Raad; Rafael Stroggilos; Helle S. Bosselmann; Archie Campbell; Shona M Kerr; Colette E Jackson; Jane A. Cannon; Morten Schou; Nicolas Girerd; Patrick Rossignol; Alex McConnachie; Kasper Rossing; Joost P Schanstra; Faiez Zannad; Antonia Vlahou; William Mullen; Vera Jankowski; Harald Mischak; Zhenyu Zhang; Jan A. Staessen; Agnieszka Latosinska

doi:10.1002/ejhf.2195

Urinary peptides in heart failure: a link to molecular pathophysiology

Tianlin He, Michaela Mischak, Andrew L Clark, Ross T. Campbell, Christian Delles, Javier Díez, Gerasimos Filippatos, Alexandre Mebazaa, John J V McMurray, Arantxa González, Julia Raad, Rafael Stroggilos, Helle S. Bosselmann, Archie Campbell, Shona M Kerr, Colette E Jackson, Jane A. Cannon, Morten Schou, Nicolas Girerd, Patrick RossignolAlex McConnachie, Kasper Rossing, Joost P Schanstra, Faiez Zannad, Antonia Vlahou, William Mullen, Vera Jankowski, Harald Mischak, Zhenyu Zhang, Jan A. Staessen, Agnieszka Latosinska^*

^*Corresponding author af dette arbejde

Publikation: Bidrag til tidsskrift › Tidsskriftartikel › Forskning › peer review

38 Citationer (Scopus)

16 Downloads (Pure)

Abstract

Aims: Heart failure (HF) is a major public health concern worldwide. The diversity of HF makes it challenging to decipher the underlying complex pathological processes using single biomarkers. We examined the association between urinary peptides and HF with reduced (HFrEF), mid-range (HFmrEF) and preserved (HFpEF) ejection fraction, defined based on the European Society of Cardiology guidelines, and the links between these peptide biomarkers and molecular pathophysiology. Methods and results: Analysable data from 5608 participants were available in the Human Urinary Proteome database. The urinary peptide profiles from participants diagnosed with HFrEF, HFmrEF, HFpEF and controls matched for sex, age, estimated glomerular filtration rate, systolic and diastolic blood pressure, diabetes and hypertension were compared applying the Mann–Whitney test, followed by correction for multiple testing. Unsupervised learning algorithms were applied to investigate groups of similar urinary profiles. A total of 577 urinary peptides significantly associated with HF were sequenced, 447 of which (77%) were collagen fragments. In silico analysis suggested that urinary biomarker abnormalities in HF principally reflect changes in collagen turnover and immune response, both associated with fibrosis. Unsupervised clustering separated study participants into two clusters, with 83% of non-HF controls allocated to cluster 1, while 65% of patients with HF were allocated to cluster 2 (P < 0.0001). No separation based on HF subtype was detectable. Conclusions: Heart failure, irrespective of ejection fraction subtype, was associated with differences in abundance of urinary peptides reflecting collagen turnover and inflammation. These peptides should be studied as tools in early detection, prognostication, and prediction of therapeutic response.

Originalsprog	Engelsk
Tidsskrift	European Journal of Heart Failure
Vol/bind	23
Udgave nummer	11
Sider (fra-til)	1875-1887
Antal sider	13
ISSN	1388-9842
DOI	https://doi.org/10.1002/ejhf.2195
Status	Udgivet - 2021

Bibliografisk note

Funding Information:
AC, CD, JD, AG, AM, JR, NG, PR, FZ, HM, ZZ, JS, AL are supported by the EU Commission via the HOMAGE (HEALTH-FP7?305507 HOMAGE) project. CD, FZ, HM, JD and JS were previously supported by the EU-MASCARA (HEALTH-FP7?278249) project, and CD and JM receive support from the British Heart Foundation (RE/18/6/34217). TH is supported by the EU Commission via the CaReSyAn Project (MSCA-ITN-2017-Project ID: 764474). VJ is supported by the Deutsche Forschungsgemeinschaft' (DFG, German Research Foundation) by the Transregional Collaborative Research Centre (TRR 219; Project-ID 322900939) (subproject S-03). PR, NG, FZ are supported by the RHU Fight-HF, a public grant overseen by the French National Research Agency (ANR) as part of the second ?Investissements d'Avenir? program (reference: ANR-15-RHUS-0004), and by the French PIA project ?Lorraine Universit? d'Excellence?(reference: ANR-15-IDEX-04-LUE). The Stanislas Cohort is sponsored by Nancy CHRU (France); its biobanking is managed by Biological Resource Center Lorrain BB-0033-00035. Generation Scotland received core support from the Chief Scientist Office of the Scottish Government Health Directorates [CZD/16/6] and the Scottish Funding Council [HR03006] and is currently supported by the Wellcome Trust [216767/Z/19/Z]. The non-profit Research Institute Alliance for the Promotion of Preventive Medicine received a non-binding grant from OMRON Healthcare Co., Inc., Kyoto, Japan. Conflict of interest: HM, AV, JS and VJ are members of the European Uraemic Toxin Working Group (EUTox). HM is cofounder and co-owner of Mosaiques Diagnostics. TH, MM, JR, JS and AL are employees of Mosaiques Diagnostics GmbH. PR reports personal fees (consulting) for Idorsia,G3P, KBP, and Sanofi, honoraria from AstraZeneca, Bayer, Boehringer Ingelheim, CVRx, Fresenius, Grunenthal, Novartis, NovoNordisk, Sequana medical, Servier, Stealth Peptides, Ablative Solutions, Corvidia, Relypsa and Vifor Fresenius Medical Care Renal Pharma, outside the submitted work, PR is the cofounder of CardioRenal. NG reports personal fees from Novartis, AstraZeneca, Bayer, Boehringer, Vifor, outside the submitted work. FZ reports personal fees from Janssen, Bayer, Amgen, CVRx, Boehringer, AstraZeneca, Cardior, Cereno pharmacuetical, Applied Therapeutics, Merck, Novartis, NovoNordisk, Myokardia, Actelion, Owkin, Cellprothera, other from CVCT and Cardiorenal, outside the submitted work. AM reports personal fees from Orion, Servier, Otsuka, Philips, Sanofi, Adrenomed, Epygon and Fire 1 and grants and personal fees from 4TEEN4, Abbott, Roche and Sphyngotec. JM reported other support from AstraZeneca; non-financial support from Cytokinetics, Bayer, Theracos, Oxford University, Dalcor, Merck, GlaxoSmithKline, Bristol Myers Squibb, Vifor-Fresenius, Kidney Research UK, Alnylam, Abbvie, Cyclerion, Cardurion; and personal fees from Amgen, and personal fees from Abbott, Hickma, Sun Pharmaceuticals, Servier lecture fees outside the submitted work.

Funding Information:
AC, CD, JD, AG, AM, JR, NG, PR, FZ, HM, ZZ, JS, AL are supported by the EU Commission via the HOMAGE (HEALTH‐FP7–305507 HOMAGE) project. CD, FZ, HM, JD and JS were previously supported by the EU‐MASCARA (HEALTH‐FP7–278249) project, and CD and JM receive support from the British Heart Foundation (RE/18/6/34217). TH is supported by the EU Commission via the CaReSyAn Project (MSCA‐ITN‐2017‐Project ID: 764474). VJ is supported by the Deutsche Forschungsgemeinschaft' (DFG, German Research Foundation) by the Transregional Collaborative Research Centre (TRR 219; Project‐ID 322900939) (subproject S‐03). PR, NG, FZ are supported by the RHU Fight‐HF, a public grant overseen by the French National Research Agency (ANR) as part of the second ‘Investissements d'Avenir’ program (reference: ANR‐15‐RHUS‐0004), and by the French PIA project ‘Lorraine Université d'Excellence’(reference: ANR‐15‐IDEX‐04‐LUE). The Stanislas Cohort is sponsored by Nancy CHRU (France); its biobanking is managed by Biological Resource Center Lorrain BB‐0033‐00035. Generation Scotland received core support from the Chief Scientist Office of the Scottish Government Health Directorates [CZD/16/6] and the Scottish Funding Council [HR03006] and is currently supported by the Wellcome Trust [216767/Z/19/Z]. The non‐profit Research Institute Alliance for the Promotion of Preventive Medicine received a non‐binding grant from OMRON Healthcare Co., Inc., Kyoto, Japan.

Publisher Copyright:
© 2021 The Authors. European Journal of Heart Failure published by John Wiley & Sons Ltd on behalf of European Society of Cardiology.

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10.1002/ejhf.2195Licens: CC BY

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Citationsformater

He, T., Mischak, M., Clark, A. L., Campbell, R. T., Delles, C., Díez, J., Filippatos, G., Mebazaa, A., McMurray, J. J. V., González, A., Raad, J., Stroggilos, R., Bosselmann, H. S., Campbell, A., Kerr, S. M., Jackson, C. E., Cannon, J. A., Schou, M., Girerd, N., ... Latosinska, A. (2021). Urinary peptides in heart failure: a link to molecular pathophysiology. European Journal of Heart Failure, 23(11), 1875-1887. https://doi.org/10.1002/ejhf.2195

He, T, Mischak, M, Clark, AL, Campbell, RT, Delles, C, Díez, J, Filippatos, G, Mebazaa, A, McMurray, JJV, González, A, Raad, J, Stroggilos, R, Bosselmann, HS, Campbell, A, Kerr, SM, Jackson, CE, Cannon, JA, Schou, M, Girerd, N, Rossignol, P, McConnachie, A, Rossing, K, Schanstra, JP, Zannad, F, Vlahou, A, Mullen, W, Jankowski, V, Mischak, H, Zhang, Z, Staessen, JA & Latosinska, A 2021, 'Urinary peptides in heart failure: a link to molecular pathophysiology', European Journal of Heart Failure, bind 23, nr. 11, s. 1875-1887. https://doi.org/10.1002/ejhf.2195

@article{27470569fd3a4244a640224f294db59f,

title = "Urinary peptides in heart failure: a link to molecular pathophysiology",

abstract = "Aims: Heart failure (HF) is a major public health concern worldwide. The diversity of HF makes it challenging to decipher the underlying complex pathological processes using single biomarkers. We examined the association between urinary peptides and HF with reduced (HFrEF), mid-range (HFmrEF) and preserved (HFpEF) ejection fraction, defined based on the European Society of Cardiology guidelines, and the links between these peptide biomarkers and molecular pathophysiology. Methods and results: Analysable data from 5608 participants were available in the Human Urinary Proteome database. The urinary peptide profiles from participants diagnosed with HFrEF, HFmrEF, HFpEF and controls matched for sex, age, estimated glomerular filtration rate, systolic and diastolic blood pressure, diabetes and hypertension were compared applying the Mann–Whitney test, followed by correction for multiple testing. Unsupervised learning algorithms were applied to investigate groups of similar urinary profiles. A total of 577 urinary peptides significantly associated with HF were sequenced, 447 of which (77%) were collagen fragments. In silico analysis suggested that urinary biomarker abnormalities in HF principally reflect changes in collagen turnover and immune response, both associated with fibrosis. Unsupervised clustering separated study participants into two clusters, with 83% of non-HF controls allocated to cluster 1, while 65% of patients with HF were allocated to cluster 2 (P < 0.0001). No separation based on HF subtype was detectable. Conclusions: Heart failure, irrespective of ejection fraction subtype, was associated with differences in abundance of urinary peptides reflecting collagen turnover and inflammation. These peptides should be studied as tools in early detection, prognostication, and prediction of therapeutic response.",

keywords = "Biomarker, Collagen, Fibrosis, Heart failure, Proteome, Urine",

author = "Tianlin He and Michaela Mischak and Clark, {Andrew L} and Campbell, {Ross T.} and Christian Delles and Javier D{\'i}ez and Gerasimos Filippatos and Alexandre Mebazaa and McMurray, {John J V} and Arantxa Gonz{\'a}lez and Julia Raad and Rafael Stroggilos and Bosselmann, {Helle S.} and Archie Campbell and Kerr, {Shona M} and Jackson, {Colette E} and Cannon, {Jane A.} and Morten Schou and Nicolas Girerd and Patrick Rossignol and Alex McConnachie and Kasper Rossing and Schanstra, {Joost P} and Faiez Zannad and Antonia Vlahou and William Mullen and Vera Jankowski and Harald Mischak and Zhenyu Zhang and Staessen, {Jan A.} and Agnieszka Latosinska",

note = "Publisher Copyright: {\textcopyright} 2021 The Authors. European Journal of Heart Failure published by John Wiley & Sons Ltd on behalf of European Society of Cardiology.",

year = "2021",

doi = "10.1002/ejhf.2195",

language = "English",

volume = "23",

pages = "1875--1887",

journal = "European Journal of Heart Failure",

issn = "1388-9842",

publisher = "JohnWiley & Sons Ltd",

number = "11",

}

TY - JOUR

T1 - Urinary peptides in heart failure

T2 - a link to molecular pathophysiology

AU - He, Tianlin

AU - Mischak, Michaela

AU - Clark, Andrew L

AU - Campbell, Ross T.

AU - Delles, Christian

AU - Díez, Javier

AU - Filippatos, Gerasimos

AU - Mebazaa, Alexandre

AU - McMurray, John J V

AU - González, Arantxa

AU - Raad, Julia

AU - Stroggilos, Rafael

AU - Bosselmann, Helle S.

AU - Campbell, Archie

AU - Kerr, Shona M

AU - Jackson, Colette E

AU - Cannon, Jane A.

AU - Schou, Morten

AU - Girerd, Nicolas

AU - Rossignol, Patrick

AU - McConnachie, Alex

AU - Rossing, Kasper

AU - Schanstra, Joost P

AU - Zannad, Faiez

AU - Vlahou, Antonia

AU - Mullen, William

AU - Jankowski, Vera

AU - Mischak, Harald

AU - Zhang, Zhenyu

AU - Staessen, Jan A.

AU - Latosinska, Agnieszka

PY - 2021

Y1 - 2021

N2 - Aims: Heart failure (HF) is a major public health concern worldwide. The diversity of HF makes it challenging to decipher the underlying complex pathological processes using single biomarkers. We examined the association between urinary peptides and HF with reduced (HFrEF), mid-range (HFmrEF) and preserved (HFpEF) ejection fraction, defined based on the European Society of Cardiology guidelines, and the links between these peptide biomarkers and molecular pathophysiology. Methods and results: Analysable data from 5608 participants were available in the Human Urinary Proteome database. The urinary peptide profiles from participants diagnosed with HFrEF, HFmrEF, HFpEF and controls matched for sex, age, estimated glomerular filtration rate, systolic and diastolic blood pressure, diabetes and hypertension were compared applying the Mann–Whitney test, followed by correction for multiple testing. Unsupervised learning algorithms were applied to investigate groups of similar urinary profiles. A total of 577 urinary peptides significantly associated with HF were sequenced, 447 of which (77%) were collagen fragments. In silico analysis suggested that urinary biomarker abnormalities in HF principally reflect changes in collagen turnover and immune response, both associated with fibrosis. Unsupervised clustering separated study participants into two clusters, with 83% of non-HF controls allocated to cluster 1, while 65% of patients with HF were allocated to cluster 2 (P < 0.0001). No separation based on HF subtype was detectable. Conclusions: Heart failure, irrespective of ejection fraction subtype, was associated with differences in abundance of urinary peptides reflecting collagen turnover and inflammation. These peptides should be studied as tools in early detection, prognostication, and prediction of therapeutic response.

AB - Aims: Heart failure (HF) is a major public health concern worldwide. The diversity of HF makes it challenging to decipher the underlying complex pathological processes using single biomarkers. We examined the association between urinary peptides and HF with reduced (HFrEF), mid-range (HFmrEF) and preserved (HFpEF) ejection fraction, defined based on the European Society of Cardiology guidelines, and the links between these peptide biomarkers and molecular pathophysiology. Methods and results: Analysable data from 5608 participants were available in the Human Urinary Proteome database. The urinary peptide profiles from participants diagnosed with HFrEF, HFmrEF, HFpEF and controls matched for sex, age, estimated glomerular filtration rate, systolic and diastolic blood pressure, diabetes and hypertension were compared applying the Mann–Whitney test, followed by correction for multiple testing. Unsupervised learning algorithms were applied to investigate groups of similar urinary profiles. A total of 577 urinary peptides significantly associated with HF were sequenced, 447 of which (77%) were collagen fragments. In silico analysis suggested that urinary biomarker abnormalities in HF principally reflect changes in collagen turnover and immune response, both associated with fibrosis. Unsupervised clustering separated study participants into two clusters, with 83% of non-HF controls allocated to cluster 1, while 65% of patients with HF were allocated to cluster 2 (P < 0.0001). No separation based on HF subtype was detectable. Conclusions: Heart failure, irrespective of ejection fraction subtype, was associated with differences in abundance of urinary peptides reflecting collagen turnover and inflammation. These peptides should be studied as tools in early detection, prognostication, and prediction of therapeutic response.

KW - Biomarker

KW - Collagen

KW - Fibrosis

KW - Heart failure

KW - Proteome

KW - Urine

U2 - 10.1002/ejhf.2195

DO - 10.1002/ejhf.2195

M3 - Journal article

C2 - 33881206

AN - SCOPUS:85105230999

SN - 1388-9842

VL - 23

SP - 1875

EP - 1887

JO - European Journal of Heart Failure

JF - European Journal of Heart Failure

IS - 11

ER -