Specific elastin degradation products are associated with poor outcome in the ECLIPSE COPD cohort

Rønnow, Sarah; Langholm, Lasse; Sand, J.M.B.; Thorlacius-Ussing, Jeppe; Leeming, Diana Julie; Manon‐Jensen, Tina; Tal‐Singer, Ruth; Miller, Bruce E.; Karsdal, Morten A.; Vestbo, Jørgen

doi:10.1038/s41598-019-40785-2

Cited by 21 publications

(23 citation statements)

References 38 publications

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“…The fibrinogen footprint of PR3 activity is also likely to be an indirect marker of elastin degradation considered central to the pathophysiology of emphysema. Since our results were generated, a recent article using a similar methodology to measure a PR3-specific elastin cleavage product in healthy controls and a COPD cohort indicates similar increased PR3 compared with an NE cleavage product to that seen here [23]. Direct comparison of both assays should, however, be undertaken in a single α 1 -AT-deficient cohort for final confirmation.…”

Section: Discussionsupporting

confidence: 55%

A specific proteinase 3 activity footprint in α₁-antitrypsin deficiency

et al. 2019

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α1-Antitrypsin (α1-AT) deficiency is a risk factor for emphysema due to tissue damage by serine proteases. Neutrophil elastase (NE) has long been considered the enzyme responsible. However, proteinase 3 (PR3) also produces the pathological features of chronic obstructive pulmonary disease (COPD), is present in the same granules in the neutrophil and is inhibited after NE. We developed a specific footprint assay for PR3 activity and assessed its relationship to an NE footprint in α1-AT deficiency.An ELISA was developed for the specific PR3 fibrinogen cleavage site Aα-Val541. Levels were measured in plasma from 239 PiZZ patients, 94 PiSZ patients, 53 nondeficient healthy smokers and 78 individuals with usual COPD. Subjects underwent extensive demographic characterisation including full lung function and lung computed tomography scanning.Aα-Val541 was greater than the NE footprint in all cohorts, consistent with differential activity. Values were highest in the PiZZ α1-AT-deficient patients and correlated with the NE marker Aα-Val360, but were ∼17 times higher than for the NE footprint, consistent with a greater potential contribution to lung damage. Aα-Val541 was related cross-sectionally to the severity of lung disease (forced expiratory volume in 1 s % pred: rs= −0.284; p<0.001) and was sensitive to augmentation therapy, falling from 287.2 to 48.6 nM (p<0.001).An in vivo plasma footprint of PR3 activity is present in greater quantities than an NE footprint in patients with α1-AT deficiency, is sensitive to augmentation therapy and represents a likely biomarker for dose-ranging studies.

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Section: Discussionsupporting

confidence: 55%

A specific proteinase 3 activity footprint in α₁-antitrypsin deficiency

et al. 2019

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“…ECM remodeling, including both formation and degradation of the lung tissue, has been shown to be increased in patients with COPD [22][23][24][25]. Furthermore, an accelerated rate of remodeling was associated with acute exacerbations of COPD and an elevated risk of mortality [18,[22][23][24][25][26]. Abdillahi et al showed that type VI collagen mRNA and protein are increased in the lungs of COPD patients when compared to controls [27].…”

Section: Discussionmentioning

confidence: 99%

Endotrophin, an extracellular hormone, in combination with neoepitope markers of von Willebrand factor improves prediction of mortality in the ECLIPSE COPD cohort

et al. 2020

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Background: Lung epithelial damage, activation of the wound healing cascade, and remodeling of the extracellular matrix (ECM) play a major role in chronic obstructive pulmonary disease (COPD). The pro-peptide of type VI collagen has been identified as the hormone endotrophin. Endotrophin has been shown to promote fibrosis and inflammation, whereas von Willebrand factor (VWF) is a crucial part of wound healing initiation. Here, we assessed the released and activated form of VWF and endotrophin, the pro-peptide of type VI collagen, serologically to investigate their association with mortality in COPD subjects alone or in combination. Methods: One thousand COPD patients with 3 years of clinical follow-up from the Evaluation of COPD Longitudinally to Identify Predictive Surrogate Endpoints (ECLIPSE) cohort were included. Serum and heparin plasma were collected at 6 months and 1 year, respectively. Competitive ELISA utilizing specific monoclonal antibodies assessed endotrophin/ type VI collagen formation (PRO-C6), VWF release (VWF-N), and activated VWF (VWF-A). Biomarker levels were dichotomized into high and low as defined by receiver operating characteristic (ROC) curves based on mortality data. Kaplan-Meier analysis was used to determine hazard ratios for all-cause mortality for biomarkers alone or in combination. Results: High levels of PRO-C6, VWF-A, and VWF-N have previously been shown to be individually associated with a higher risk of mortality with hazard ratios of 5.6 (95% CI 2.4-13.1), 3.7 (1.8-7.6), and 4.6 (2.2-9.6), respectively. The hazard ratios increased when combining the biomarkers: PRO-C6*VWFA 8.8 (2.8-27.7) and PRO-C6*VWFN 13.3 (5.6-32.0). Notably, PRO-C6*VWF-N increased more than 2-fold.

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“…Another limitation of the data was the lack of adjudication of the cause of death, as performed in several prospective interventional trials [39][40][41]. A limited number of serum and blood biomarkers were evaluated and did not include recently described markers such as collagen and elastin turnover biomarkers [42], which could be of use in assessing different components of COPD disease activity. Finally, the ECLIPSE population was recruited by specialists, often at academic centres with expertise in clinical trials, and does not represents a population-based sample.…”

Section: Strengths and Limitationsmentioning

confidence: 99%

Markers of disease activity in COPD: an 8-year mortality study in the ECLIPSE cohort

et al. 2020

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RationaleThere are no validated measures of disease activity in chronic obstructive pulmonary disease (COPD). Since “active” disease is expected to have worse outcomes (e.g. mortality), we explored potential markers of disease activity in patients enrolled in the ECLIPSE cohort in relation to 8-year all-cause mortality.MethodsWe investigated: (1) how changes in relevant clinical variables over time (1 or 3 years) relate to 8-year mortality; (2) whether these variables inter-relate; and (3) if any clinical, imaging, and/or biological marker measured cross-sectionally at baseline relates to any activity component.ResultsResults showed that: (1) After 1 year, hospitalisation for COPD, exacerbation frequency, worsening of body mass index, airflow obstruction, dyspnoea, and exercise (BODE) index or health status (St. George's Respiratory Questionnaire [SGRQ]), and persistence of systemic inflammation were significantly associated with 8-year mortality; (2) At 3 years, the same markers, plus forced expiratory volume in 1 s (FEV1) decline and to a lesser degree computed tomography (CT) emphysema, showed association, thus qualifying as markers of disease activity; (3) Changes in FEV1, inflammatory cytokines and CT emphysema were not inter-related, while the multidimensional indices (BODE and SGRQ) showed modest correlations; and, (4) Changes in these markers could not be predicted by any baseline cross-sectional measure.ConclusionsIn COPD, 1- and 3-year changes in exacerbation frequency, systemic inflammation, BODE and SGRQ scores, and FEV1 decline are independent markers of disease activity associated with 8-year all-cause mortality. These disease activity markers are generally independent and not predictable from baseline measurements.

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Specific elastin degradation products are associated with poor outcome in the ECLIPSE COPD cohort

Cited by 21 publications

References 38 publications

A specific proteinase 3 activity footprint in α₁-antitrypsin deficiency

A specific proteinase 3 activity footprint in α₁-antitrypsin deficiency

Endotrophin, an extracellular hormone, in combination with neoepitope markers of von Willebrand factor improves prediction of mortality in the ECLIPSE COPD cohort

Markers of disease activity in COPD: an 8-year mortality study in the ECLIPSE cohort

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Specific elastin degradation products are associated with poor outcome in the ECLIPSE COPD cohort

Cited by 21 publications

References 38 publications

A specific proteinase 3 activity footprint in α1-antitrypsin deficiency

A specific proteinase 3 activity footprint in α1-antitrypsin deficiency

Endotrophin, an extracellular hormone, in combination with neoepitope markers of von Willebrand factor improves prediction of mortality in the ECLIPSE COPD cohort

Markers of disease activity in COPD: an 8-year mortality study in the ECLIPSE cohort

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A specific proteinase 3 activity footprint in α₁-antitrypsin deficiency

A specific proteinase 3 activity footprint in α₁-antitrypsin deficiency