Plasma proteomic approach in patients with heart failure: insights into pathogenesis of disease progression and potential novel treatment targets

T. H. Cao; D. J. L. Jones; A. A. Voors; P. A. Quinn; J. K. Sandhu; D. C. S. Chan; H. M. Parry; M. Mohan; I. R. Mordi; I. E. Sama; S. D. Anker; J. G. Cleland; K. Dickstein; G. Filippatos; H. L. Hillege; M. Metra; P. Ponikowski; N. J. Samani; D. J. Van Veldhuisen; F. Zannad; C. C. Lang; L. L. Ng

doi:10.1002/ejhf.1608

Plasma proteomic approach in patients with heart failure: insights into pathogenesis of disease progression and potential novel treatment targets

T. H. Cao, D. J. L. Jones, A. A. Voors, P. A. Quinn, J. K. Sandhu, D. C. S. Chan, H. M. Parry, M. Mohan, I. R. Mordi, I. E. Sama, S. D. Anker, J. G. Cleland, K. Dickstein, G. Filippatos, H. L. Hillege, M. Metra, P. Ponikowski, N. J. Samani, D. J. Van Veldhuisen, F. ZannadC. C. Lang, L. L. Ng

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Abstract

To provide insights into pathogenesis of disease progression and potential novel treatment targets for patients with heart failure by investigation of the plasma proteome using network analysis.|The plasma proteome of 50 patients with heart failure who died or were rehospitalised were compared with 50 patients with heart failure, matched for age and sex, who did not have an event. Peptides were analysed on two-dimensional liquid chromatography coupled to tandem mass spectrometry (2D LC ESI-MS/MS) in high definition mode (HDMSE). We identified and quantified 3001 proteins, of which 51 were significantly up-regulated and 46 down-regulated with more than two-fold expression changes in those who experienced death or rehospitalisation. Gene ontology enrichment analysis and protein-protein interaction networks of significant differentially expressed proteins discovered the central role of metabolic processes in clinical outcomes of patients with heart failure. The findings revealed that a cluster of proteins related to glutathione metabolism, arginine and proline metabolism, and pyruvate metabolism in the pathogenesis of poor outcome in patients with heart failure who died or were rehospitalised.|Our findings show that in patients with heart failure who died or were rehospitalised, the glutathione, arginine and proline, and pyruvate pathways were activated. These pathways might be potential targets for therapies to improve poor outcomes in patients with heart failure.

Original language	English
Pages (from-to)	70-80
Number of pages	11
Journal	EUROPEAN JOURNAL OF HEART FAILURE
Volume	22
Issue number	1
DOIs	https://doi.org/10.1002/ejhf.1608
Publication status	Published - 2020

Keywords

Aged Aged, 80 and over Angiotensin Receptor Antagonists Angiotensin-Converting Enzyme Inhibitors Disease Progression Female Heart Failure Humans Male Percutaneous Coronary Intervention Plasma Proteome Proteomics Stroke Volume Tandem Mass Spectrometry Ventricular Function, Left Heart failure Mass spectrometry Metabolism Pathogenesis Proteomics Treatment target

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10.1002/ejhf.1608

https://www.ncbi.nlm.nih.gov/pubmed/31692186

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Cao, T. H., Jones, D. J. L., Voors, A. A., Quinn, P. A., Sandhu, J. K., Chan, D. C. S., Parry, H. M., Mohan, M., Mordi, I. R., Sama, I. E., Anker, S. D., Cleland, J. G., Dickstein, K., Filippatos, G., Hillege, H. L., Metra, M., Ponikowski, P., Samani, N. J., Van Veldhuisen, D. J., ... Ng, L. L. (2020). Plasma proteomic approach in patients with heart failure: insights into pathogenesis of disease progression and potential novel treatment targets. EUROPEAN JOURNAL OF HEART FAILURE, 22(1), 70-80. https://doi.org/10.1002/ejhf.1608

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title = "Plasma proteomic approach in patients with heart failure: insights into pathogenesis of disease progression and potential novel treatment targets",

abstract = "To provide insights into pathogenesis of disease progression and potential novel treatment targets for patients with heart failure by investigation of the plasma proteome using network analysis.|The plasma proteome of 50 patients with heart failure who died or were rehospitalised were compared with 50 patients with heart failure, matched for age and sex, who did not have an event. Peptides were analysed on two-dimensional liquid chromatography coupled to tandem mass spectrometry (2D LC ESI-MS/MS) in high definition mode (HDMSE). We identified and quantified 3001 proteins, of which 51 were significantly up-regulated and 46 down-regulated with more than two-fold expression changes in those who experienced death or rehospitalisation. Gene ontology enrichment analysis and protein-protein interaction networks of significant differentially expressed proteins discovered the central role of metabolic processes in clinical outcomes of patients with heart failure. The findings revealed that a cluster of proteins related to glutathione metabolism, arginine and proline metabolism, and pyruvate metabolism in the pathogenesis of poor outcome in patients with heart failure who died or were rehospitalised.|Our findings show that in patients with heart failure who died or were rehospitalised, the glutathione, arginine and proline, and pyruvate pathways were activated. These pathways might be potential targets for therapies to improve poor outcomes in patients with heart failure.",

keywords = "Aged Aged, 80 and over Angiotensin Receptor Antagonists Angiotensin-Converting Enzyme Inhibitors Disease Progression Female Heart Failure Humans Male Percutaneous Coronary Intervention Plasma Proteome Proteomics Stroke Volume Tandem Mass Spectrometry Ventricular Function, Left Heart failure Mass spectrometry Metabolism Pathogenesis Proteomics Treatment target",

author = "Cao, {T. H.} and Jones, {D. J. L.} and Voors, {A. A.} and Quinn, {P. A.} and Sandhu, {J. K.} and Chan, {D. C. S.} and Parry, {H. M.} and M. Mohan and Mordi, {I. R.} and Sama, {I. E.} and Anker, {S. D.} and Cleland, {J. G.} and K. Dickstein and G. Filippatos and Hillege, {H. L.} and M. Metra and P. Ponikowski and Samani, {N. J.} and {Van Veldhuisen}, {D. J.} and F. Zannad and Lang, {C. C.} and Ng, {L. L.}",

note = "Cao, Thong H Jones, Donald J L Voors, Adriaan A Quinn, Paulene A Sandhu, Jatinderpal K Chan, Daniel C S Parry, Helen M Mohan, Mohapradeep Mordi, Ify R Sama, Iziah E Anker, Stefan D Cleland, John G Dickstein, Kenneth Filippatos, Gerasimos Hillege, Hans L Metra, Marco Ponikowski, Piotr Samani, Nilesh J Van Veldhuisen, Dirk J Zannad, Faiez Lang, Chim C Ng, Leong L 2019/11/7",

year = "2020",

doi = "10.1002/ejhf.1608",

language = "English",

volume = "22",

pages = "70--80",

journal = "EUROPEAN JOURNAL OF HEART FAILURE",

issn = "1879-0844",

publisher = "John Wiley & Sons, Ltd",

number = "1",

}

Cao, TH, Jones, DJL, Voors, AA, Quinn, PA, Sandhu, JK, Chan, DCS, Parry, HM, Mohan, M, Mordi, IR, Sama, IE, Anker, SD, Cleland, JG, Dickstein, K, Filippatos, G, Hillege, HL, Metra, M, Ponikowski, P, Samani, NJ, Van Veldhuisen, DJ, Zannad, F, Lang, CC & Ng, LL 2020, 'Plasma proteomic approach in patients with heart failure: insights into pathogenesis of disease progression and potential novel treatment targets', EUROPEAN JOURNAL OF HEART FAILURE, vol. 22, no. 1, pp. 70-80. https://doi.org/10.1002/ejhf.1608

TY - JOUR

T1 - Plasma proteomic approach in patients with heart failure: insights into pathogenesis of disease progression and potential novel treatment targets

AU - Cao, T. H.

AU - Jones, D. J. L.

AU - Voors, A. A.

AU - Quinn, P. A.

AU - Sandhu, J. K.

AU - Chan, D. C. S.

AU - Parry, H. M.

AU - Mohan, M.

AU - Mordi, I. R.

AU - Sama, I. E.

AU - Anker, S. D.

AU - Cleland, J. G.

AU - Dickstein, K.

AU - Filippatos, G.

AU - Hillege, H. L.

AU - Metra, M.

AU - Ponikowski, P.

AU - Samani, N. J.

AU - Van Veldhuisen, D. J.

AU - Zannad, F.

AU - Lang, C. C.

AU - Ng, L. L.

N1 - Cao, Thong H Jones, Donald J L Voors, Adriaan A Quinn, Paulene A Sandhu, Jatinderpal K Chan, Daniel C S Parry, Helen M Mohan, Mohapradeep Mordi, Ify R Sama, Iziah E Anker, Stefan D Cleland, John G Dickstein, Kenneth Filippatos, Gerasimos Hillege, Hans L Metra, Marco Ponikowski, Piotr Samani, Nilesh J Van Veldhuisen, Dirk J Zannad, Faiez Lang, Chim C Ng, Leong L 2019/11/7

PY - 2020

Y1 - 2020

N2 - To provide insights into pathogenesis of disease progression and potential novel treatment targets for patients with heart failure by investigation of the plasma proteome using network analysis.|The plasma proteome of 50 patients with heart failure who died or were rehospitalised were compared with 50 patients with heart failure, matched for age and sex, who did not have an event. Peptides were analysed on two-dimensional liquid chromatography coupled to tandem mass spectrometry (2D LC ESI-MS/MS) in high definition mode (HDMSE). We identified and quantified 3001 proteins, of which 51 were significantly up-regulated and 46 down-regulated with more than two-fold expression changes in those who experienced death or rehospitalisation. Gene ontology enrichment analysis and protein-protein interaction networks of significant differentially expressed proteins discovered the central role of metabolic processes in clinical outcomes of patients with heart failure. The findings revealed that a cluster of proteins related to glutathione metabolism, arginine and proline metabolism, and pyruvate metabolism in the pathogenesis of poor outcome in patients with heart failure who died or were rehospitalised.|Our findings show that in patients with heart failure who died or were rehospitalised, the glutathione, arginine and proline, and pyruvate pathways were activated. These pathways might be potential targets for therapies to improve poor outcomes in patients with heart failure.

AB - To provide insights into pathogenesis of disease progression and potential novel treatment targets for patients with heart failure by investigation of the plasma proteome using network analysis.|The plasma proteome of 50 patients with heart failure who died or were rehospitalised were compared with 50 patients with heart failure, matched for age and sex, who did not have an event. Peptides were analysed on two-dimensional liquid chromatography coupled to tandem mass spectrometry (2D LC ESI-MS/MS) in high definition mode (HDMSE). We identified and quantified 3001 proteins, of which 51 were significantly up-regulated and 46 down-regulated with more than two-fold expression changes in those who experienced death or rehospitalisation. Gene ontology enrichment analysis and protein-protein interaction networks of significant differentially expressed proteins discovered the central role of metabolic processes in clinical outcomes of patients with heart failure. The findings revealed that a cluster of proteins related to glutathione metabolism, arginine and proline metabolism, and pyruvate metabolism in the pathogenesis of poor outcome in patients with heart failure who died or were rehospitalised.|Our findings show that in patients with heart failure who died or were rehospitalised, the glutathione, arginine and proline, and pyruvate pathways were activated. These pathways might be potential targets for therapies to improve poor outcomes in patients with heart failure.

KW - Aged Aged, 80 and over Angiotensin Receptor Antagonists Angiotensin-Converting Enzyme Inhibitors Disease Progression Female Heart Failure Humans Male Percutaneous Coronary Intervention Plasma Proteome Proteomics Stroke Volume Tandem Mass Spectrometry Vent

U2 - 10.1002/ejhf.1608

DO - 10.1002/ejhf.1608

M3 - Article

SN - 1879-0844

VL - 22

SP - 70

EP - 80

JO - EUROPEAN JOURNAL OF HEART FAILURE

JF - EUROPEAN JOURNAL OF HEART FAILURE

IS - 1

ER -

Plasma proteomic approach in patients with heart failure: insights into pathogenesis of disease progression and potential novel treatment targets

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Keywords

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