4.3 Article

Data-independent acquisition mass spectrometry in severe rheumatic heart disease (RHD) identifies a proteomic signature showing ongoing inflammation and effectively classifying RHD cases

Journal

CLINICAL PROTEOMICS
Volume 19, Issue 1, Pages -

Publisher

BMC
DOI: 10.1186/s12014-022-09345-1

Keywords

Rheumatic heart disease; Biomarker; Inflammatory response; Adiponectin; Complement component C7; Fibulin-1

Funding

  1. Wellcome Trust [099313/B/12/A.]
  2. South African National Research Foundation (NRF) [116287]
  3. American Heart Association, United States [NW17SFRN33630027]
  4. British Heart Foundation [CH/13/2/30154, RG/15/12/31616]
  5. UKRI ESRC via the Newton Fund [ES/N01393X/1]
  6. UKRI Medical Research Council [MR/P025463]
  7. Global Challenge Research Fund
  8. Wellcome Trust [099313/B/12/A] Funding Source: Wellcome Trust
  9. ESRC [ES/N01393X/1] Funding Source: UKRI

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By using SWATH-MS, this study identified several biomarkers that showed significant changes in protein expression levels in patients with RHD, indicating a persistent inflammatory response. These biomarkers have the potential to be used as tools for recognizing different degrees of ongoing inflammation in RHD patients.
Background Rheumatic heart disease (RHD) remains a major source of morbidity and mortality in developing countries. A deeper insight into the pathogenetic mechanisms underlying RHD could provide opportunities for drug repurposing, guide recommendations for secondary penicillin prophylaxis, and/or inform development of near-patient diagnostics. Methods We performed quantitative proteomics using Sequential Windowed Acquisition of All Theoretical Fragment Ion Mass Spectrometry (SWATH-MS) to screen protein expression in 215 African patients with severe RHD, and 230 controls. We applied a machine learning (ML) approach to feature selection among the 366 proteins quantifiable in at least 40% of samples, using the Boruta wrapper algorithm. The case-control differences and contribution to Area Under the Receiver Operating Curve (AUC) for each of the 56 proteins identified by the Boruta algorithm were calculated by Logistic Regression adjusted for age, sex and BMI. Biological pathways and functions enriched for proteins were identified using ClueGo pathway analyses. Results Adiponectin, complement component C7 and fibulin-1, a component of heart valve matrix, were significantly higher in cases when compared with controls. Ficolin-3, a protein with calcium-independent lectin activity that activates the complement pathway, was lower in cases than controls. The top six biomarkers from the Boruta analyses conferred an AUC of 0.90 indicating excellent discriminatory capacity between RHD cases and controls. Conclusions These results support the presence of an ongoing inflammatory response in RHD, at a time when severe valve disease has developed, and distant from previous episodes of acute rheumatic fever. This biomarker signature could have potential utility in recognizing different degrees of ongoing inflammation in RHD patients, which may, in turn, be related to prognostic severity.

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