Abstract
Endothelial dysfunction and increased platelet reactivity in acute coronary syndrome with unknown/undiagnosed COPD http://ow.ly/SVEg30eExbK
To the Editor:
Unknown/undiagnosed chronic obstructive pulmonary disease (UCOPD) frequently coexists and negatively impacts in the short- and long-term prognosis of patients with coronary artery disease (CAD) treated with percutaneous coronary intervention (PCI) [1]. In the Screening for COPD in Acute coronary syndromes Patients (SCAP) trial [2], we recently showed that COPD is frequently undiagnosed in ccute coronary syndrome (ACS) patients with smoking history. Furthermore, we found that a simple screening procedure including peak expiratory flow measurement and respiratory health status questionnaire (RHSQ) might be administered before hospital discharge to discriminate those at risk of UCOPD. In the SCAP study, it was pre-specified that an ancillary analysis aimed to clarify if UCOPD was related to abnormalities in platelet reactivity and endothelial function.
Inclusion and exclusion criteria of the SCAP trial have been previously reported [2]. Briefly, current or former smoking (≥10 pack-years) patients admitted to hospital with a diagnosis of ACS were enrolled. ACS diagnosis was based according to the criteria of current guidelines [3], as well as cardiovascular management and pharmacological therapy [3, 4]. Exclusion criteria were as follows: previous diagnosis of COPD and/or asthma, known pulmonary disease other than COPD, ongoing pneumonia, ongoing heart failure, documented or suspicion of malignant disease, life expectancy <1 year, and recent thoracic trauma. The P2Y12 inhibitor (ticagrelor versus clopidogrel versus prasugrel) was selected according to the physician's discretion. After 2 months from the time of discharge, patients underwent spirometry. COPD was defined by the presence of irreversible airflow obstruction (forced expiratory volume in 1 s/forced vital capacity <70% post-bronchodilator) [4]. The work was approved by the institutional ethics committee, and informed written consent was obtained from each subject. This study is registered at ClinicalTrials.gov (number: NCT02324660). A venous blood sample was collected from all patients at the time of the enrolment, which occurred at hospital discharge. Of note, the blood sample was collected when the diagnosis of COPD was still unknown. All patients underwent blood sampling early morning (08:00–10:00 h), after at least 30 min of rest and 2 h of fasting. Blood sample was obtained from an antecubital vein using a 21-gauge needle. The specific analyses for the present study were: 1) endothelial dysfunction assay, assessed by the rate of apoptosis in human umbilical vein endothelial cells (HUVECs) after 48-h incubation with 20% serum from patients, as previously reported [5, 6]; 2) on-treatment platelet reactivity measured with light transmittance aggregometry after arachidonic acid and adenosine diphosphate stimulus [7]. Continuous data were tested for normal distribution with the Kolmogorov–Smirnov test. Normally distributed values were presented as mean±sd and compared by t-test and one-way ANOVA. Otherwise, median (interquartile range), Mann–Whitney U- and Kruskal–Wallis tests were used. Categorical variables were summarised in terms of number and percentages and were compared by using two-sided Fisher's exact test. The association between all variables are listed in table 1. UCOPD and the rate of apoptosis was assessed by logistic regression models. Variables with a probability value <0.1 in the univariate analysis (age, diabetes, UCOPD, ticagrelor) and potential confounding factors (sex, clinical presentation, current smoking) were then entered into a multivariable analysis to identify the independent predictors of the rate of apoptosis. A two-sided value of p<0.05 was considered significant. All analyses were performed with STATISTICA 8 (Statsoft Inc, Tulsa, OK, USA).
The study population included 137 patients [2]. At the 2-month spirometry, we found UCOPD in 39 (29%) patients. A detailed description of all spirometric parameters has been previously reported [2]. Airflow limitation was mild in 23 (59%) patients, moderate in 15 (38%) patients and severe in one (3%). Baseline characteristics of patients are summarised in table 1. Patients with UCOPD showed a significantly higher rate of apoptosis in HUVECs than those without COPD (13.2±3% versus 9.2±4%; p<0.001). At multivariate analysis, UCOPD emerged as the independent predictor of the rate of apoptosis (HR 1.54, 95% CI 1.3–1.8; p<0.001). In addition, we found a significant trend between the values of the rate of apoptosis and airflow limitation severity (mild 12.3±3 versus moderate 14.3±2 versus severe 18.7; p=0.03). On-treatment platelet reactivity was significantly higher in patients with UCOPD than others, both after ADP stimulus (42±17% versus 32±14%; p<0.001) and arachidonic acid stimulus (22±20% versus 14±21%; p<0.001). We did not find any relation between on-treatment platelet reactivity and airflow limitation severity. Additionally, we analysed the effect of different P2Y12 inhibitors on endothelial dysfunction and platelet reactivity. Overall, ticagrelor was administered in 75 (55%) patients (20, 52% with UCOPD and 55, 56% without COPD). In patients treated with ticagrelor, the rate of apoptosis was lower than other P2Y12 inhibitors both in patients with UCOPD (12.2±2% versus 14.2±3%; p=0.03) and in those without COPD (7.7±3% versus 11.1±5%; p<0.001). In addition, in patients with UCOPD, ticagrelor ensured ADP-induced platelet reactivity values similar to those observed in patients without COPD, (UCOPD 28±9% versus no COPD 24±11%; p=0.3), while other P2Y12 inhibitors did not (UCOPD 57±7% versus no COPD 41±11%; p<0.001).
The main aim of the SCAP trial was to validate a simple screening procedure to identify ACS patients with smoking history and at a risk of UCOPD. In the SCAP trial, according to current guidelines, spirometry was systematically applied to overpassing misdiagnosis and under diagnosis [8, 9]. This sub-analysis highlighted that UCOPD is already associated with significant changes in endothelial function and on-treatment platelet reactivity. These physio-pathological elements may contribute to explain why UCOPD is related to poor prognosis in patients with ischaemic heart disease. We may speculate that these changes are reversible and an early identification of UCOPD may allow a timely cardiac and respiratory treatment with potentially beneficial prognosis.
For instance, we found that ticagrelor improved endothelial dysfunction, regardless of pulmonary function. We found that both COPD and UCOPD patients benefit from ticagrelor. A previous study on ACS patients showed that treatment with ticagrelor was able to improve endothelial function (tested with peripheral arterial tonometry) [10]. This was confirmed in a randomised clinical trial of COPD patients with stable coronary artery disease [6]. The present analysis confirms, in the subset of patients with UCOPD and ACS, this pleiotropic effect of ticagrelor on endothelial dysfunction, similarly for the relationship between ticagrelor and on-treatment platelet reactivity in UCOPD patients. It is well established that on-treatment platelet reactivity is heightened in COPD patients either with or without ischaemic heart disease [11]. This sub-study expands the observation showing that on-treatment platelet reactivity is heightened also in those with UCOPD. Ticagrelor modulates on-treatment platelet reactivity in ACS patients, regardless of the presence of UCOPD. This is not observed with other P2Y12 inhibitors. In the PLATelet inhibition and clinical Outcome (PLATO) trial, COPD patients showed greater benefit from ticagrelor treatment [12]. The combined effect of ticagrelor on endothelial function and on-treatment platelet reactivity helps to explain the mechanisms behind this observation. Similarly, we could extend, based on our findings, this potential benefit to UCOPD patients receiving ticagrelor.
In conclusion, to our best knowledge, this is the first study to show that patients with ACS and concomitant UCOPD have increased endothelial dysfunction and on-treatment platelet reactivity. Moreover, we showed that ticagrelor may contribute to improve both parameters. Accordingly, any further effort for early identification and treatment of patients with UCOPD should be encouraged.
Acknowledgements
Author contributions are as follows. R. Pavasini is the guarantor of the content of the manuscript, including the data and analysis. R. Pavasini, G. Campo, F. Vieceli dalla Sega: conception, design, analysis and interpretation of data. R. Pavasini, G. Campo, M. Contoli, A. Papi: data analysis and interpretation. All authors: drafting of the manuscript and revising it critically for important intellectual content. All authors: final approval of the manuscript submitted.
Footnotes
This study is registered at ClinicalTrials.gov (number: NCT02324660).
Conflict of interest: None declared.
- Received June 14, 2017.
- Accepted July 4, 2017.
- Copyright ©ERS 2017