Plasma proteome analysis in patients with pulmonary arterial hypertension: an observational cohort study

Rhodes, Christopher J.; Wharton, John; Ghataorhe, Pavandeep; Watson, Geoffrey; Girerd, Barbara; Howard, Luke; Gibbs, J. Simon R.; Condliffe, Robin; Elliot, Charles; Kiely, David G.; Simonneau, Gérald; Montani, David; Sitbon, Olivier; Gall, Henning; Schermuly, Ralph Theo; Ghofrani, Hossein Ardeschir; Lawrie, Allan; Humbert, Marc; Wilkins, Martin R.

doi:10.1016/s2213-2600(17)30161-3

Cited by 119 publications

(113 citation statements)

References 31 publications

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“…CNDP1 was reduced by 43% after RYGB at the 3 month time point (FDR=1.6*10 -5 ) and remained lower in RYGB at 36 months ( Figure 5B). A previous study had been unable to validate SOMAscan CNDP1 measurements (38). ELISA-determined CNDP1 levels in our analysis showed little correlation with SOMAscan levels per time point, but changes within person over time showed stronger correlation (r=0.21, p=0.055).…”

Section: Proteomic and Metabolomic Integrative Pathway Analysiscontrasting

confidence: 80%

Novel mediation analysis of human plasma proteome and metabolome reveals mediators of improved glycemia after gastric bypass surgery

Dreyfuss

Yuchi

Hui

et al. 2019

Preprint

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Molecular mechanisms by which Roux-en-Y gastric bypass (RYGB) improves glycemic control and metabolism in type 2 diabetes (T2D) remain incompletely understood. In the SLIMM-T2D trial, participants with T2D were randomized to RYGB or nonsurgical management and their fasting plasma proteome and metabolome were analyzed for up to 3 years. To identify analytes that mediate improvement in outcomes, we developed a high-throughput mediation analysis method (Hitman), which is significantly more powerful than existing methods. Top-ranking analyte mediators of glycemia improvement were growth hormone receptor and prolylhydroxyproline, which were more significant than any clinical mediator, including BMI. Betaalanine and Histidine Metabolism (both including CNDP1) were top differentially regulated pathways, and Valine, Leucine and Isoleucine Degradation was also a top differentiallyregulated pathway and a top mediator of improvement in insulin resistance. The identified analytes may serve as novel targets for T2D therapy. More broadly, Hitman can identify analyte mediators of outcomes in randomized trials for which high-throughput data are available. Results ClinicalProteomic and metabolomic data at baseline, the 3 month time point, and 1 year were available from 35 of the 38 SLIMM-T2D participants. Metabolic characteristics of these 35 participants did not differ between groups at baseline ( Table S1). The HbA1c and BMI of those that had proteomics or metabolomics per time point also did not differ from the SLIMM-T2D participants within their group at any time point (Figure S1). After 3 years, no DWM participants achieved study-defined glycemic goals (HbA1c<6.5% and fasting plasma glucose<126 mg/dL), whereas eight RYGB participants did, and seven of these eight participants were not receiving any antidiabetes medications (Simonson et al., 2018). The number of participants taking each diabetes medication class per arm at each time point is tabulated in Table S1. ProteomeFasting proteomics were profiled at baseline, the 3 month time point, and years 1, 2 and 3 in RYGB and DWM. At baseline (pre-randomization), there were no statistically significant proteins as assessed by false discovery rate (FDR<0.15). For later, post-randomization time points, reduction in BMI was greater in RYGB, so groups were compared both with and without adjustment for each person's BMI change. Differences in the baseline-corrected proteome in RYGB vs. DWM (i.e. differences between groups in changes over time) emerged at the 3 month time point, with 14 significant proteins in the unadjusted analysis and 8 in the BMI-adjusted analysis. Proteins common to both analyses and downregulated in RYGB were: carnosine dipeptidase 1 (CNDP1, also known as Beta-Ala-His dipeptidase 1) and Fetuin-B (FETUB). Proteins in common upregulated in RYGB were: integrin-binding sialoprotein (IBSP), insulin-like growth factor binding protein (IGFBP2), endothelial cell-specific molecule 1 (ESM1), macrophage metalloelastase (MMP12), alpha-1-antichymotrypsin complex (SERPINA3), ...

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Section: Proteomic and Metabolomic Integrative Pathway Analysiscontrasting

confidence: 80%

Novel mediation analysis of human plasma proteome and metabolome reveals mediators of improved glycemia after gastric bypass surgery

Dreyfuss

Yuchi

Hui

et al. 2019

Preprint

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“…Evaluations of PH cohorts demonstrate a high frequency of ID and/or anaemia in PH patients, as approximately 40-60% of PH patients demonstrate ID and one-third of all PH patients suffer from anaemia [27,28]. Interestingly, both ID and anaemia significantly affect the morbidity and mortality of PH patients [27,29]. Current evidence suggests a significant role of iron handling in the pathogenesis and clinical outcome of both, pre-and post-capillary pulmonary hypertension [4,28,[30][31][32].…”

Section: Interconnection Of Pulmonary Hypertension Iron Homeostasismentioning

confidence: 99%

Anaemia, iron homeostasis and pulmonary hypertension: a review

et al. 2020

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Anaemia is a highly prevalent condition, which negatively impacts on patients' cardiovascular performance and quality of life. Anaemia is mainly caused by disturbances of iron homeostasis. While absolute iron deficiency mostly as a consequence of chronic blood loss or insufficient dietary iron absorption results in the emergence of iron deficiency anaemia, inflammation-driven iron retention in innate immune cells and blockade of iron absorption leads to the development of anaemia of chronic disease. Both, iron deficiency and anaemia have been linked to the clinical course of pulmonary hypertension. Various mechanistic links between iron homeostasis, anaemia, and pulmonary hypertension have been described and current treatment guidelines suggest regular iron status assessment and the implementation of iron supplementation strategies in these patients. The pathophysiology, diagnostic assessment as well as current and future treatment options concerning iron deficiency with or without anaemia in individuals suffering from pulmonary hypertension are discussed within this review.

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“…11,12 These studies and other reported molecular phenotyping efforts to date have inherent limitations, as analyses are anchored to specific clinical definitions and PAH subtypes that may not adequately reflect disease heterogeneity. [13][14][15][16][17] 'Unsupervised' phenotyping is a more agnostic strategy, where molecular profiles directly define phenotypes that are subsequently related to clinical characteristics. 18 These molecular phenotypes can be identified by machine learning, which is the inference of substructure in complex unlabeled data with computer algorithms.…”

Section: Introductionmentioning

confidence: 99%

Discovery of Distinct Immune Phenotypes Using Machine Learning in Pulmonary Arterial Hypertension

Sweatt

Hedlin

Balasubramanian

et al. 2019

Circulation Research

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153

116

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In December 2018, the average time from submission to first decision for all original research papers submitted to Circulation Research was 14.99 days. ABSTRACTRationale: Accumulating evidence implicates inflammation in pulmonary arterial hypertension (PAH) and therapies targeting immunity are under investigation, though it remains unknown if distinct immune phenotypes exist.Objective: Identify PAH immune phenotypes based on unsupervised analysis of blood proteomic profiles. Methods and Results:In a prospective observational study of Group 1 PAH patients evaluated at Stanford University (discovery cohort, n=281) and University of Sheffield (validation cohort, n=104) between 2008-2014, we measured a circulating proteomic panel of 48 cytokines, chemokines, and factors using multiplex immunoassay. Unsupervised machine learning (consensus clustering) was applied in both cohorts independently to classify patients into proteomic immune clusters, without guidance from clinical features. To identify central proteins in each cluster, we performed partial correlation network analysis. Clinical characteristics and outcomes were subsequently compared across clusters. Four PAH clusters with distinct proteomic immune profiles were identified in the discovery cohort. Cluster 2 (n=109) had low cytokine levels similar to controls. Other clusters had unique sets of upregulated proteins central to immune networks-cluster 1 (n=58)(TRAIL, CCL5, CCL7, CCL4, MIF), cluster 3 (n=77)(IL-12, IL-17, IL-10, IL-7, VEGF), and cluster 4 (n=37)(IL-8, IL-4, PDGF-, IL-6, CCL11). Demographics, PAH etiologies, comorbidities, and medications were similar across clusters. Non-invasive and hemodynamic surrogates of clinical risk identified cluster 1 as high-risk and cluster 3 as low-risk groups. Five-year transplant-free survival rates were unfavorable for cluster 1 (47.6%, CI 35.4-64.1%) and favorable for cluster 3 (82.4%, CI 72.0-94.3%)(across-cluster p<0.001). Findings were replicated in the validation cohort, where machine learning classified four immune clusters with comparable proteomic, clinical, and prognostic features.Conclusions: Blood cytokine profiles distinguish PAH immune phenotypes with differing clinical risk that are independent of World Health Organization Group 1 subtypes. These phenotypes could inform mechanistic studies of disease pathobiology and provide a framework to examine patient responses to emerging therapies targeting immunity. Nonstandard Abbreviations and Acronyms: CI confidence interval 95% EC pulmonary artery endothelial cell IQR interquartile range 25-75% K cluster number in unsupervised consensus clustering MFI median fluorescence intensity mPAP mean pulmonary arterial pressure NT-proBNP N-terminal pro b-type natriuretic peptide PAH pulmonary arterial hypertension PVDOMICS Pulmonary Vascular Disease Phenomics Program PVR pulmonary vascular resistance REVEAL Registry to Evaluate Early and Long-term PAH Disease Management SMC pulmonary artery smooth muscle cell SQL structured query language TAPSE tricuspid annular pla...

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Plasma proteome analysis in patients with pulmonary arterial hypertension: an observational cohort study

Cited by 119 publications

References 31 publications

Novel mediation analysis of human plasma proteome and metabolome reveals mediators of improved glycemia after gastric bypass surgery

Novel mediation analysis of human plasma proteome and metabolome reveals mediators of improved glycemia after gastric bypass surgery

Anaemia, iron homeostasis and pulmonary hypertension: a review

Discovery of Distinct Immune Phenotypes Using Machine Learning in Pulmonary Arterial Hypertension

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