N-terminal pro-brain natriuretic peptide in patients with acute pulmonary embolism

doi:10.1183/09031936.03.00023303

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N-terminal pro-brain natriuretic peptide in patients with acute pulmonary embolism

P. Pruszczyk¹, M. Kostrubiec¹, A. Bochowicz¹, G. Styczy $n$ ski¹, M. Szulc¹, M. Kurzyna², A. Fija $l$ kowska², A. Kuch-Wocial¹, I. Chlewicka¹ and A. Torbicki²

¹ Dept of Internal Medicine and Hypertension, Medical University of Warsaw, and ² Dept of Chest Medicine, Institute of Lung Diseases and Tuberculosis, Warsaw, Poland

CORRESPONDENCE: P. Pruszczyk, Dept of Internal Medicine and Hypertension, Medical University of Warsaw, Banacha 1a, 02-097, Warsaw, Poland. Fax: 48 226593373. E-mail: piotr.pruszczyk@amwaw.edu.pl

Keywords: brain natriuretic peptide, echocardiography, mortality, pulmonary embolism, right ventricle

Received: March 2, 2003
Accepted May 14, 2003

Abstract

TOP
Abstract
Materials and methods
Results
Discussion
References

Plasma brain natriuretic peptide (BNP), released from myocytesof ventricles upon stretch, has been reported to differentiatepulmonary from cardiac dyspnoea. Limited data have shown elevatedplasma BNP levels in acute pulmonary embolism (APE), frequentlyaccompanied by dyspnoea and right ventricular (RV) dysfunction.The aim of this study was to assess plasma N-terminal proBNP(NT-proBNP) in APE, and to establish whether it reflects theseverity of RV overload and if it can be used to predict adverseclinical outcome.

On admission, NT-proBNP and echocardiography for RV overloadwere performed in 79 APE patients (29 males), aged 63±16 yrs.

Plasma NT-proBNP was elevated in 66 patients (83.5%) and washigher in patients with (median 4,650 pg·mL^–1(range 61–60,958)) than without RV strain (363 pg·mL^–1(16–16,329)). RV-to-left ventricular ratio and inferiorvena cava dimension correlated with NT-proBNP. All 15 in-hospitaldeaths and 24 serious adverse events occurred in the group withelevated NT-proBNP, while all 13 (16.5%) patients with normalvalues had an uncomplicated clinical course. Plasma NT-proBNPpredicted in-hospital mortality.

Plasma N-terminal pro-brain natriuretic peptide is elevatedin the majority of cases of pulmonary embolism resulting inright ventricular overload. Plasma levels reflect the degreeof right ventricular overload and may help to predict short-termoutcome. Acute pulmonary embolism should be considered in thedifferential diagnosis of patients with dyspnoea and abnormallevels of brain natriuretic peptide.

Elevated plasma levels of brain natriuretic peptide (BNP) releasedfrom myocytes of ventricles upon stretch have been found inpatients with congestive heart failure and even in those withasymptomatic left ventricular (LV) systolic dysfunction 1. Moreover,elevated plasma BNP was found in patients with primary pulmonaryhypertension and chronic thromboembolic pulmonary hypertension3. Interestingly, elevated plasma BNP was reported to help differentiatepulmonary from cardiac aetiologies of acute dyspnoea 5. PlasmaN-terminal proBNP (NT-proBNP) is also increased incongestiveheart failure patients 6 and it may help to stratify their prognosis7. However, limited data suggest that plasma BNP may be elevatedin patients with acute pulmonary embolism (APE), frequentlyaccompanied by acute dyspnoea and right ventricular (RV) dysfunction9–11. Therefore, the aim of this study was to assess plasmalevels of NT-proBNP in patients with APE, and to establish whetherthe levels reflect the severity of RV overload and whether theycan be used to predict adverse clinical outcome.

Materials and methods

TOP
Abstract
Materials and methods
Results
Discussion
References

Clinical data
The study analysed consecutive patients with symptomatic APE.APE was confirmed by contrast-enhanced spiral computed tomographyor by high-probability lung scintigraphy according to PIOPED(Prospective Investigation of Pulmonary Embolism Diagnosis)criteria 12. On admission, systemic blood pressure (BP) andcardiac frequency (fc) were measured, 12-lead electrocardiogram(ECG) and transcutaneous pulsoximetry (S_p,O₂) were also recorded.

Echocardiographic data
In order to assess the degree of RV overload on admission, transthoracicechocardiography (TTE) was performed with Hewlett Packard SONOS4500 (Hewlett Packard, Andover, MA, USA) or Acuson Sequoia systems(Acuson, Mountain View, CA, USA). The data were stored and off-linecalculations were carried out for the assessment of RV pressureoverload. Examinations were performed in the left supine position.The end-diastolic transverse dimensions of the RV and LV weremeasured in the apical four-chamber view at the onset of theR wave of the ECG tracing. Subsequently, the RV:LV end-diastolicratio was calculated. Quantitatively, thesystolic function ofRV was assessed, specifically for hypokinesis of the RV freewall, as described previously 13. After measuring the peak velocityof tricuspid valve regurgitation with continuous Doppler, thetricuspid valve pressure gradient (TVPG) was calculated accordingto the simplified Bernoulli's formula. The acceleration timeof pulmonary ejection was measured with pulsed Doppler in theRV outflow tract. Dimensions of inferior vena cava (IVC) weremeasured during expiration using the subcostal approach.

RV pressure overload was diagnosed when echocardiography showedRV:LV >0.6 with RV hypokinesis and/or elevated TVPG >30 mmHgwith shortened acceleration time of pulmonary ejection <80 ms.

Severity of acute pulmonary embolism
According to the systemic systolic BP (BPs) measured on admissionand the result of the echocardiographic examination, three subgroupsof APE patients were defined: massive APE with BPs $≤$ 90 mmHg;nonmassive APE with BPs >90 mmHg without echocardiographicsigns of RV overload; and submassive APE in whom, despite preservedsystemic BPs (>90 mmHg), RV overload was present atTTE.

Biochemical assays
On admission, blood samples were collected from an antecubitalvein for routine assays and for plasma NT-proBNP. Samples fordetermination of NT-proBNP were centrifuged and plasma was frozenuntil the quantitative assay (electrochemiluminescence method;Roche Diagnostics GmbH, Mannheim, Germany) wasperformed. PlasmaNT-proBNP concentrations greater than age- and sex-specificvalues were regarded as abnormal (reference values accordingto the manufacturer: female <50 yrs, <153 pg·mL^–1;female $≥$ 50 yrs, <334 pg·mL^–1; males<50 yrs, <88 pg·mL^–1; males $≥$ 50 yrs,<227 pg·mL^–1). The protocol of this studywas approved by the local Institutional Bioethical Committee.All participating patients gave their informed consent.

Statistical analysis
Data characterised by normal distribution are expressed as mean±sd.Parameters not normally distributed are expressed as median(range). Unpaired, two-sided t-tests or the Mann-Whitney U-testwere used for two-group comparisons. Yate's corrected Chi-squaredtest was used to compare discrete variables. Receiver-operatingcharacteristic (ROC) analysis was performed in order to assessoptimal cut-off values for plasma NT-proBNP in the selectionof in-hospital deaths and serious adverse events (SAE) duringhospitalisation. Odds ratio (OR) analysis was used to assessthe influence of NT-proBNP on the in-hospital mortality andon SAE during hospitalisation, which included at least one ofthe following in-hospital adverse clinical events: death, cardiopulmonaryresuscitation, thrombolysis and need for i.v. catecholamineinfusion. In order to normalise the distribution of NT-proBNPvalues, their log was used for OR analysis. Multivariate logisticanalysis was used to assess factors influencing in-hospitaldeaths or SAE.

Results

TOP
Abstract
Materials and methods
Results
Discussion
References

Patients' characteristics and clinical course
The group of 79 APE patients who were investigated included29 males and 50 females, aged 63±17 yrs (table 1).In nine patients, massive APE was diagnosed. Nonmassive APEwas found in 18 patients, while the remaining 51 cases formedthe subgroup with submassive APE. TTE was not performed in onenormotensive patient. Echocardiography was not performed inthree patients with clinically massive APE. However, in theremaining six patients with massive APE, TTE showed significantRV overload. At least one coexisting disease (chronic obstructivepulmonary disease, neoplasm, renal insufficiency, congestiveheart failure) was present in 20 (25.3%) of the subjects studied.Initially, all investigated patients with submassive and nonmassiveAPE were anticoagulated with an i.v. infusion of unfractionatedheparins, with dose-activated partial thrombin time (APTT) adjustedto reach 1.5–2.0-times control APTT, or received subcutaneouslow molecular weight heparins in a body weight-adjusted dose.The decision to start thrombolysis was based on the clinicalassessment of each individual patient by thephysician in charge.The decrease in systemic BPs <90 mmHg, progressive accelerationof fc or respiratory insufficiency were considered as potentialindications for such aggressive treatment. Eventually, fivepatients with submassive APE received thrombolysis. Three ofnine patients with massive APE were thrombolised. The decisionto start aggressive therapy was influenced by co-existing conditionsincreasing the risk of bleeding. Altogether, eight (10%) patientsreceived thrombolysis with 1,500,000 U i.v. streptokinaseover 2 h. When control APTT decreased down to three-timescontrol, i.v. heparin was restarted.

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Table 1 Clinical and echocardiographic characteristics of patients with acute pulmonary embolism (APE)

Despite the implemented treatment, 15 of 79 patients died duringhospitalisation (in-hospital mortality 18.9%). This includedfour patients (44%) with massive APE, 10 (19.6%) with submassiveAPE and one patient with an initial BP of 160/100 mmHg.The latter patient had subarachnoideal bleeding 2 weeks beforethe radiologically massive APE and died shortly after admission,probably due to intracranial bleeding during heparin infusion,before echocardiographic examination could be performed. IrreversibleRV failure was diagnosed in 11 patients and in three othersrecurrent fatal APE was clinically suspected. Thrombolysis wasused with similar frequency in survivors and nonsurvivors (9and 13%, respectively). SAE occurred in 24 (30.4%) cases. Thisgroup comprised 15 deaths and an additional six patients withthrombolysis, which was accompanied by successful cardiopulmonaryresuscitation and i.v. use of vasopressor agents in one case.Successful cardiopulmonary resuscitation without thrombolysiswas performed in two others.

Plasma N-terminal pro-brain natriuretic peptide
On admission, plasma NT-proBNP levels were above the referenceage- and sex-specific values in 66 patients (83.5%). It waselevated in 10 (55.6%) cases with nonmassive APE, while it wassignificantly more frequent in submassive and massive APE (90.2and 100%, respectively, p<0.01). Plasma levels in massiveAPE were significantly higher than in submassive or nonmassiveAPE: massive 9,865.0 pg·mL^–1 (414.5–31,168.0),submassive 4,650.5 pg·mL^–1 (61.0–60,958.0)and nonmassive 363.6 pg·mL^–1 (16.3–16,329.0)(Kruskal-Wallis analysis of variance, p<0.0002; fig. 1).

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Fig. 1.— Plasma N-terminal pro-brain natriuretic peptide (NT-proBNP) levels in patients with acute pulmonary embolism, classified as nonmassive (n=18), submassive (n=51) or massive (n=9). Data are presented as median, 25–75% and min–max. p=0.0002.

Plasma N-terminal pro-brain natriuretic peptide and echocardiographic parameters
Transthroracic echocardiography was performed in 75 patients.Fifty-seven (76%) patients presented with RV overload (RV+),while the remaining 18 (24%) patients showed no alteration inRV morphology or function (RV–). When compared with age-and sex-specific reference values, plasma NT-proBNP levels wereabnormal in 52 (91%) patients from the RV+ group and 10 (56%)patients from the RV– group (p<0.002). Moreover, plasmaNT-proBNP was significantly lower in RV– than in RV+ (363.6 pg·mL^–1(16.3–16,329.0) versus 4,650.5 pg·mL^–1(61.0–60,958.0), p<0,00001). Interestingly, significantcorrelations between echocardiographic indices of RV overloadand NT-proBNP were found, specifically with the RV:LV ratio(r=0.53, p<0.001) and IVC (r=0.49, p<0.001; table 2

).However, plasma NT-proBNP correlated with systemic haemodynamicstatus to a lesser degree. TTE showed LV systolic dysfunction,defined by its ejection fraction <50%, in three (4.0%) ofall investigated patients. However, there were no differencesin plasma NT-proBNP between groups with preserved and diminishedLV systolic function (16,162.0 pg·mL^–1 (188.3–2,1494.0)versus 2,397.5 pg·mL^–1 (16.3–60958.0),p=0.39).

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Table 2 Correlations between haemodynamic data and plasma N-terminal pro-brain natriuretic peptide (NT-proBNP) levels in 79 patients with acute pulmonary embolism

Plasma N-terminal pro-brain natriuretic peptide and clinical course
All deaths and SAEs occurred in patients with elevated NT-proBNPlevels, while all 13 (16.5%) patients with normal values hadan uncomplicated clinical course. Nonelevated plasma NT-proBNPsignificantly differentiated patients with uncomplicated clinicalcourse form subjects with SAE during hospitalisation (p=0.01)and showed marked trends in distinguishing survivors from nonsurvivors(p=0.06). Thus, normal values of plasma NT-proBNP reached 100%negative predictive value (NPV) for in-hospital mortality orcomplicated clinical course. However, positive predictive value(PPV) of elevated NT-proBNP for death or SAE was only 22.7 and36.3%, respectively. Interestingly, plasma NT-proBNP levelswere significantly higher in nonsurvivors than in survivors(11,491.0 pg·mL^–1 (617.9–60,958.0) versusmedian 1,939.0 pg·mL^–1 (16.3–27,752.0),p=0.0005; fig. 2

). Levels were also higher in patientswith SAE during hospitalisation than in patients with uncomplicatedclinical course (9,678.5 pg·mL^–1 (414.5–60,958.0)versus 1,319.0 pg·mL^–1 (16.3–27,752.0),p=0.0002; fig. 3

). OR analysis revealed that log of plasmaNT-proBNP predicted in-hospital mortality (OR 2.15 (95% confidenceinterval (CI) 1.30–3.56)) and SAE (OR 1.88 (95% CI 1.29–2.74)).A plasma NT-proBNP cut-off value of 600 pg·mL^–1for SAE prediction was identified by ROC analysis (fig. 4

).Values of plasma NT-proBNP concentration >600 pg·mL^–1showed 96% sensitivity and 35% specificity in the predictionof SAE. The same plasma NT-proBNP level in the ROC analysisfor fatal in-hospital outcome reached 100% sensitivity and 33%specificity. Multivariate logistic analysis, including clinicaland echocardiographic parameters and plasma NT-proBNP levels,showed that in this model, only NT-proBNP and S_p,O₂ predictedin-hospital death and SAE (death: log NT-proBNP OR 1.89 (95%CI 1.12–3.20), S_p,O₂ OR 0.85 (95% CI 0.76–0.94);SAE: log NT-proBNP OR 1.70 (95%CI 1.12–2.58), SO₂ OR 0.84(95% CI 0.76–0.92)). Other variables, including age, BPs,RV:LV and TVPG, were nonsignificant in this analysis.

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Fig. 2.— Plasma N-terminal pro-brain natriuretic peptide (NT-proBNP) levels in patients with acute pulmonary embolism, survivors (n=64) and nonsurvivors (n=15). Data are presented as median, 25–75% and min–max. p=0.0005.

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Fig. 3.— Plasma N-terminal pro-brain natriuretic peptide (NT-proBNP) levels in patients with acute pulmonary embolism, group with event-free course (n=55) and group with serious adverse events (SAE; n=24). Data are presented as median, 25–75% and min–max. p=0.0002.

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Fig. 4.— Receiver-operating characteristic analysis (ROC curve) for plasma N-terminal pro-brain natriuretic peptide (NT-proBNP) in the selection of serious adverse events during hospitalisation. Arrow: NT-proBNP=600 pg·mL^–1. Area under curve=0.76.

	Discussion

TOP Abstract Materials and methods Results Discussion References

Plasma N-terminal pro-brain natriuretic peptide and haemodynamics of patients with acute pulmonary embolism
Elevated plasma levels of BNP were reported to differentiateacute dyspnoea due to congestive heart failure from itsothercauses 5. The current data show that 83% of patients with symptomaticAPE had elevated plasma NT-proBNP. These findings suggest thatAPE should be considered in the differential diagnosis of patientswith dyspnoea and elevated plasma NT-proBNP. Interestingly,plasma NT-proBNP was increased in almost all cases of clinicallymassive and submassive APE, which are accompanied by RV overloadand dyspnoea, while in patients without echocardiographic signsof RV dysfunction, NT-proBNP elevation was found in only 50%of patients. It may be that NT-proBNP, abiochemical marker ofmyocardial stretch, is more sensitive in the detection of RVoverload than echocardiography. However, this cannot be confirmedwithout direct haemodynamic evaluation, which was not performedon the patients in this study, but significant relationshipswere observed between RV:LV ratio, IVC and plasma NT-proBNP(r=0.53, p<0.001; and r=0.49, p<0.001, respectively).Since BNP is released by myocytes submitted to stretch, elevatedplasma NT-proBNP could be expected in patients with distendedRV and a higher RV:LV ratio. IVC noncollapsing at inspirationhas been shown to indicate elevated right atrial and RV end-diastolicpressures 15. The current authors also observed a positive correlationbetween TVPG and plasma NT-proBNP. Interestingly, similar correlationswere detected in patients before thombendartherectomy of chronicthromboembolic pulmonary hypertension 3 and also in subjectswith atrial septum defect complicated by pulmonary hypertension16.

Plasma N-terminal pro-brain natriuretic peptide and clinical course of acute pulmonary embolism
Plasma concentration of BNP is related to the severity of congestiveheart failure and it is an established independent risk factorof mortality in this population 8. Recently, elevated levelsof BNPs were also reported to affect the prognosis in patientsafter acute coronary syndromes 17 orprimary pulmonary hypertension4. In the present study, there were significant differencesin plasma NT-proBNP between patients with massive, submassiveand nonmassive APE. High mortality rates were observed (in-hospitalmortality 18.9%). However, it should be mentioned that mostfatalities occurred in patients with massive or submassive APE.In the current authors' opinion, this high mortality was causedby the coexisting diseases and individually assessed increasedrisk of bleeding limiting the frequency of thrombolysis. Atthe time of the study, surgical embolectomy or mechanical fragmentationof proximal clots were not available in participating centres.Moreover, one patient with APE and preserved systemic BP diedbecause of intracranial bleeding. Interestingly, all deathsand SAEs occurred in patients with elevated NT-proBNP, whileall 13 (16.5%) patients, including three subjects with RV overloadwith normal values, had uncomplicated clinical courses. Evenmore importantly, OR analysis revealed that log of plasma NT-proBNPpredicted in-hospital mortality (OR 2.15 (95% CI 1.30–3.56))and SAE (OR 1.88 (95% CI 1.29–2.74)). Multivariate analysis,including clinical and echocardiographic variables, showed thatonly increased plasma NT-proBNP and decreased S_p,O₂ influencedin-hospital deaths and SAE. Lack of haemodynamic and echocardiographicparameters in this analysis, most probably was due to the factthat NT-proBNP reflected the severity of RV overload and haemodynamiccompromise. Normal values of plasma NT-proBNP reached 100% NPVforin-hospital mortality or complicated clinical course. ROCanalysis of the data revealed that plasma NT-proBNP >600 pg·mL^–1showed 96% sensitivity and 35% specificity for the predictionof in-hospital SAE. Interestingly, this cut-off value is veryclose to the NT-proBNP level of 500 pg·mL^–1recently identified by Kucher et al. 11 These authors found,for NT-proBNP concentration >500 pg·mL^–1,sensitivity of 95% and specificity of 43% in the predictionof complicated clinical outcome. Although plasma NT-proBNP wassignificantly higher in nonsurvivors than in survivors, andalso higher in patients with SAE during hospitalisation thanin patients with uncomplicated clinical course, due to low PPVfor these events, plasma NT-proBNP cannot be helpful in theselection of high-risk APE patients. However, the current authorsdo think that normal plasma NT-proBNP may be useful in the identificationof low-risk patients. This observation corresponds to findingsby Kucher et al. 11 who also showed that low plasma NT-proBNPlevels predict benign clinical course in APE patients.

Conclusion
Plasma N-terminal pro-brain natriuretic peptide is elevatedin the majority of patients with acute pulmonary embolism resultingin right ventricular overload and reflects the degree of rightventricular overload. Therefore, pulmonary embolism should beconsidered in the differential diagnosis of patients with dyspnoeaand abnormal levels of brain natriuretic peptide. High levelsof plasma N-terminal pro-brain natriuretic peptide in patientswith acute pulmonary embolism are associated with serious adverseevents and poor prognosis. While normal plasma N-terminal pro-brainnatriuretic peptide levels found in a minority of acute pulmonaryembolism patients identify subjects with a favourable courseof the disease. Therefore, plasma N-terminal pro-brain natriureticpeptide may serve as an indicator of disease severity, whichmay complement conventional clinical variables.

References

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Chest, September 1, 2005; 128(3): 1836 - 1852.
[Abstract] [Full Text] [PDF]

L. B. Yap, D. Mukerjee, P. M. Timms, H. Ashrafian, and J. G. Coghlan
Natriuretic Peptides, Respiratory Disease, and the Right Heart
Chest, October 1, 2004; 126(4): 1330 - 1336.
[Abstract] [Full Text] [PDF]

P Pruszczyk, M Szulc, and M Kostrubiec
Potential clinical application of brain natriuretic peptides in acute pulmonary embolism
Eur. Heart J., April 1, 2004; 25(7): 621 - 621.
[Full Text] [PDF]

N. Kucher and S. Z. Goldhaber
Cardiac Biomarkers for Risk Stratification of Patients With Acute Pulmonary Embolism
Circulation, November 4, 2003; 108(18): 2191 - 2194.
[Full Text] [PDF]

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