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Gepubliceerd in: Netherlands Heart Journal 11/2021

Open Access 15-09-2021 | Original Article

Contemporary management of patients with atrial fibrillation in the Netherlands and Belgium: a report from the EORP-AF long-term general registry

Auteurs: Ö. Erküner, M. van Eck, O. Xhaet, H. Verheij, J. Neefs, A. Duygun, R. Nijmeijer, S. A. M. Saïd, H. Uiterwaal, V. Hagens, R. Bhagwandien, T. Szili-Torok, N. Bijsterveld, G. Tjeerdsma, J. Vijgen, A. Friart, E. Hoffer, P. Evrard, M. Srynger, J. Meeder, J. R. de Groot, J. van Opstal, R. Gevers, G. Y. H. Lip, G. Boriani, H. J. G. M. Crijns, J. G. L. M. Luermans, G. H. Mairesse

Gepubliceerd in: Netherlands Heart Journal | Uitgave 11/2021

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Abstract

Background

Contemporary data regarding the characteristics, treatment and outcomes of patients with atrial fibrillation (AF) are needed. We aimed to assess these data and guideline adherence in the EURObservational Research Programme on Atrial Fibrillation (EORP-AF) long-term general registry.

Methods

We analysed 967 patients from the EORP-AF long-term general registry included in the Netherlands and Belgium from 2013 to 2016. Baseline and 1‑year follow-up data were gathered.

Results

At baseline, 887 patients (92%) received anticoagulant treatment. In 88 (10%) of these patients, no indication for chronic anticoagulant treatment was present. A rhythm intervention was performed or planned in 52 of these patients, meaning that the remaining 36 (41%) were anticoagulated without indication. Forty patients were not anticoagulated, even though they had an indication for chronic anticoagulation. Additionally, 63 of the 371 patients (17%) treated with a non-vitamin K antagonist oral anticoagulant (NOAC) were incorrectly dosed. In total, 50 patients (5%) were overtreated and 89 patients (9%) were undertreated. However, the occurrence of major adverse cardiac and cerebrovascular events (MACCE) was still low with 4.2% (37 patients).

Conclusions

Overtreatment and undertreatment with anticoagulants are still observable in 14% of this contemporary, West-European AF population. Still, MACCE occurred in only 4% of the patients after 1 year of follow-up.
What’s new?
  • The majority of patients with atrial fibrillation (AF) who are on anticoagulation are still on the ‘older’ vitamin K antagonists
  • Even though the Netherlands and Belgium are, in general, comparable countries, striking differences in the management of AF patients are observed
  • Overtreatment and undertreatment with anticoagulants are still observable in a considerable proportion of West-European AF patients

Introduction

Atrial fibrillation (AF) is the most common cardiac arrhythmia worldwide. In 2010, the prevalence of AF in the European Union was estimated at 8.8 million individuals. By 2060, this number will likely more than double to 17.9 million individuals [1]. In addition to this widespread occurrence of AF, the arrhythmia is associated with morbidities as well as with complications, the most important being ischaemic stroke, making it a major public health problem with inherent extensive economic burden [2].
Registries such as the one described in this paper, the EURObservational Research Programme on Atrial Fibrillation long-term general (EORP-AF LTG) registry, are important means to assess the characteristics, treatment, and outcomes of contemporary AF patients. Furthermore, guideline adherence can be checked and awareness raised to improve the treatment of AF patients. Therefore, we aimed to analyse these aspects in the patients from the EORP-AF LTG registry included in the Netherlands and Belgium, focusing on comorbidities at baseline, guideline adherence in treatment of AF, progression of AF, and occurrence of major adverse cardiac and cerebrovascular events (MACCE) after 1 year.

Methods

The EORP-AF LTG registry is initiated by the European Society of Cardiology, conducted in 27 countries, including a total of 11,096 patients from 2013 to 2016 across 250 centres and it is the successor of the EORP-AF Pilot General Registry [3, 4]. For this analysis, we included all patients from the Netherlands and Belgium included in the registry. The study was approved by the Institutional Review Boards of all including centres in Belgium and the Netherlands. All patients provided written informed consent. Patient baseline data were obtained and the patients were followed for two consecutive years. The exact methods have been published previously [3]. We describe the baseline characteristics and 1‑year follow-up data of the patients from the Netherlands and Belgium.
MACCE was defined as a composite of cardiovascular death, ischaemic stroke/transient ischaemic attack (TIA), systemic thromboembolism, myocardial infarction, and major bleeding (intracranial bleeding, bleeding requiring hospitalisation or lengthening of stay, causing a haemoglobin level drop of > 2 g/l, or requiring blood transfusion). AF progression was defined as paroxysmal AF at baseline becoming persistent/permanent AF at follow-up, whereas AF regression was defined as persistent/permanent AF at baseline becoming paroxysmal AF at follow-up. For this definition of AF progression, patients classified as first diagnosed AF at baseline were reclassified if possible, i.e. if patients had spontaneous or pharmacological conversion at baseline, they were reclassified as paroxysmal AF. Failed attempt of cardioversion was classified as persistent AF. All others were classified as unknown, including those with successful electrical cardioversion. The estimated glomerular filtration rate (eGFR) was calculated with the CKD-EPI (chronic kidney disease epidemiology) formula, using serum creatinine concentration, gender, age, and race [5].

Statistical analysis

Data were analysed with SPSS statistical software (version 23.0, SPSS Inc., IBM Corp., Armonk, NY, USA). Continuous variables are reported as mean ± standard deviation if normally distributed and as median and interquartile range if not. Normally distributed continuous variables were compared between groups using the independent samples t‑test, whereas not normally distributed continuous variables were compared using the Mann-Whitney U test. Categorical variables are reported as observed number of patients and percentage. Among-group comparisons were made using a χ2 test. Fisher’s exact test was used in case of any expected cell count < 5.

Results

In total, 967 consecutive patients were included across 23 centres, 648 (67%) from the Netherlands and 319 (33%) from Belgium (see supplemental material for participating centres and the number of included patients per centre). The majority of patients were included at the outpatient department (57.1%). A little over one third of patients were female (n = 345, 35.7%). Hypertension was the most frequently documented comorbidity with a prevalence of 49%. “Lone AF”, defined as the absence of any comorbidity in patients aged < 65 years, was present in 117 patients (12.1%).
Baseline characteristics of the total study population, with a comparison between the countries, are shown in Tab. 1. Noteworthy differences between the two countries, among others, are the higher prevalence of heart failure (21.4% vs 15.0%, p = 0.013), obstructive sleep apnoea (14.1% vs 4.1%, p < 0.001), type 2 diabetes mellitus (22.6% vs 15.5%, p = 0.007), and hyperlipidaemia (58.5% vs 36.8%, p < 0.001) in Belgian patients. Belgian patients also had a higher body mass index on average (29 ± 6 vs 28 ± 5, p < 0.001). In Belgium, more hospitalised patients were included in the registry (55.2% vs 36.9%, p < 0.001).
Table 1
Baseline characteristics of the study population with a comparison between the Netherlands and Belgium
Variable
NL & BE
N = 967
The Netherlands
N = 648
Belgium
N = 319
NL vs BE
N (%)
Missing
N (%)
Missing
N (%)
Missing
p-value
Female sex
345 (35.7)
231 (35.6)
114 (35.7)
  0.978
Age
 69.1 (±10.8)
 68.7 (±10.9)
 70.0 (±10.6)
  0.072
BMI
 28.3 (±5.3)
 45
 27.9 (±4.9)
 40
 29.2 (±5.9)
  5
<0.001
Inpatient
415 (42.9)
239 (36.9)
176 (55.2)
<0.001
Outpatient
552 (57.1)
 
409 (63.1)
 
143 (44.8)
  
Type of AF
 
  6
 
  3
 
  3
  0.001
– First classified
 92 (9.6)
 
 65 (10.1)
 
 27 (8.5)
  
– Paroxysmal
341 (35.5)
 
256 (39.7)
 
 85 (26.9)
  
– Persistent
324 (33.7)
 
196 (30.4)
 
128 (40.5)
  
– Long-standing pers
 23 (2.4)
 
 12 (1.9)
 
 11 (3.5)
  
– Permanent
181 (18.8)
 
116 (18.0)
 
 65 (20.6)
  
EHRA mean
  1.8 (±0.8)
  1
  1.7 (±0.8)
  1.8 (±0.8)
  1
  0.167
EHRA
      
  0.365
– 1
448 (46.4)
 
308 (47.5)
 
140 (44.0)
  
– 2
329 (34.1)
 
219 (33.8)
 
210 (34.6)
  
– 3
171 (17.7)
 
112 (17.3)
 
 59 (18.6)
  
– 4
 18 (1.9)
 
  9 (1.4)
 
  9 (2.8)
  
Previous PVI
107 (11.1)
 67 (10.3)
 40 (12.5)
  0.305
LVEF on echocardiogram
 54.4 (±12.0)
367
 53.8 (±11.6)
285
 55.4 (±12.5)
 82
  0.098
LA diameter on echocardiogram
 47.6 (±10.3)
414
 46.7 (±10.6)
283
 49.4 (±9.5)
131
  0.003
Lone AF
117 (12.1)
 75 (11.6)
 42 (13.2)
  0.475
Hypertension
470 (49.0)
  8
311 (48.6)
  8
159 (49.8)
  0.715
Coronary artery disease
218 (22.8)
 12
152 (23.8)
  9
 66 (20.9)
  3
  0.315
Heart failure
165 (17.1)
  1
 97 (15.0)
 68 (21.4)
  1
  0.013
– NYHA I
 51 (30.9)
 
 33 (34)
 
 18 (26.5)
  
– NYHA II
 72 (43.6)
 
 50 (51.5)
 
 22 (32.4)
  
– NYHA III
 37 (22.4)
 
 12 (12.4)
 
 25 (36.8)
  
– NYHA IV
  5 (3.0)
 
  2 (2.1)
 
  3 (4.4)
  
Valvular heart disease
382 (40.5)
 24
258 (41.3)
 24
124 (38.9)
  0.464
Dilated CMP
 43 (4.5)
 11
 17 (2.7)
 11
 26 (8.2)
<0.001
Congenital heart disease
 16 (1.7)
  9
 12 (1.9)
  9
  4 (1.3)
  0.478
Hypertrophic CMP
 33 (3.5)
 11
 10 (1.6)
 10
 23 (7.2)
  1
<0.001
Pulmonary art. hypertension
 41 (4.3)
 13
  3 (0.5)
  9
 38 (12.1)
  4
<0.001
OSAS
 67 (7.3)
 44
 26 (4.1)
 16
 41 (14.1)
 28
<0.001
Peripheral vascular disease
 77 (8.0)
  5
 47 (7.3)
  3
 30 (9.5)
  2
  0.242
T2DM
172 (17.9)
  4
100 (15.5)
  4
 72 (22.6)
  0.007
Lipid disorder
416 (44.1)
 24
231 (36.8)
 21
185 (58.5)
  3
<0.001
Hypothyroidism
 29 (3.2)
  8
  7 (1.1)
  4
 22 (7.5)
  4
<0.001
Hyperthyroidism
 11 (1.2)
  8
  6 (1.0)
  4
  5 (1.6)
  4
  0.548
Prior thromboembolic event
155 (16.0)
 99 (15.3)
 56 (17.6)
  0.364
Prior haemorrhagic event
 52 (5.4)
  1
 30 (4.6)
  1
 22 (6.9)
  0.143
LAA-occlusion
 11 (1.2)
 34
 10 (1.6)
  3
  1 (0.3)
 31
  0.188
CHA2DS2-VASc mean
  2.7 (±1.7)
  3
  2.6 (±1.7)
  2.9 (±1.7)
  3
  0.010
CHA2DS2-VASc
      
  0.265
– 0
 95 (9.9)
 
 70 (10.8)
 
 25 (7.9)
  
– 1
153 (15.9)
 
109 (16.8)
 
 44 (13.9)
  
– 2
199 (20.6)
 
135 (20.8)
 
 64 (20.3)
  
– 3
210 (21.8)
 
139 (21.5)
 
 71 (22.5)
  
– 4
177 (18.4)
 
117 (18.1)
 
 60 (19.0)
  
– 5
 70 (7.3)
 
 45 (6.9)
 
 25 (7.9)
  
– 6
 41 (4.3)
 
 22 (3.4)
 
 19 (6.0)
  
– 7
 13 (1.3)
 
  9 (1.4)
 
  4 (1.3)
  
– 8
  6 (0.6)
 
  2 (0.3)
 
  4 (1.3)
  
HAS-BLED mean
  1.5 (±1.0)
  1.4 (±1.0)
  1.6 (±1.0)
  0.003
HAS-BLED
      
  0.011
– 0
162 (16.8)
 
119 (18.4)
 
 43 (13.5)
  
– 1
357 (36.9)
 
252 (38.8)
 
105 (32.6)
  
– 2
300 (31.0)
 
187 (28.9)
 
113 (35.4)
  
– 3
123 (12.7)
 
 76 (11.7)
 
 47 (14.7)
  
– 4
 18 (1.9)
 
  8 (1.2)
 
 10 (3.1)
  
– 5
  7 (0.7)
 
  6 (0.9)
 
  1 (0.3)
  
Alcohol use
 
296
 
240
 
 56
  0.686
– None
250 (37.3)
 
143 (35.0)
 
107 (40.7)
  
– < 1 U/day
196 (29.2)
 
124 (30.4)
 
 72 (27.4)
  
– 1 U/day
 93 (13.9)
 
 59 (14.5)
 
 34 (12.9)
  
– 2–3 U/day
 99 (14.8)
 
 62 (15.2)
 
 37 (14.1)
  
– 4 or more
 33 (4.9)
 
 20 (4.9)
 
 13 (4.9)
  
Smoking
 
150
 
143
 
  7
  0.237
– No smoker
423 (51.8)
 
250 (49.5)
 
173 (55.4)
  
– Currently
103 (12.6)
 
 65 (12.9)
 
 38 (12.2)
  
– Former
291 (35.6)
 
190 (37.6)
 
101 (32.4)
  
AF atrial fibrillation, BE Belgium, BMI body mass index, CHA2DS2-VASc congestive heart failure, hypertension, age ≥ 75 years [doubled], diabetes mellitus, prior stroke [doubled], vascular disease, age 65–74, sex category, CMP cardiomyopathy, EHRA European Heart Rhythm Association, LA left atrial, LAA left atrial appendage, LVEF left ventricular ejection fraction, NL the Netherlands, NYHA New York Heart Association, OSAS obstructive sleep apnoea syndrome, T2DM type 2 diabetes mellitus
Baseline laboratory measurements are shown in Supplementary Table 1. Belgian patients had on average a lower total cholesterol level (4.3 ± 1.2 vs 4.7 ± 1.2, p = 0.002), corresponding with the higher prescription rate of statins (46.9% vs 40.2%, p = 0.049, Tab. 2). Furthermore, N‑terminal pro-brain natriuretic peptide (NT-proBNP) levels were higher in Belgian patients (1714 [IQR 636–2803] vs 448 [IQR 228–1081], p = 0.018), in line with the higher amount of patients with heart failure (21.4% vs. 15.0%, p = 0.013, Tab. 1), even though the number of NT-proBNP measurements were low in Belgium and disproportionate between the two countries, 10 (3%) versus 119 (18%) patients.
Table 2
Baseline medication of the study population with a comparison between the Netherlands and Belgium
Medication
NL & BE
N = 967
The Netherlands
N = 648
Belgium
N = 319
NL vs BE
N (%)
Missing
N (%)
Missing
N (%)
Missing
p-value
VKA
453 (46.9)
2
344 (53.2)
1
109 (34.3)
1
<0.001
Rivaroxaban
188 (19.5)
2
124 (19.1)
1
 64 (20.1)
1
  0.723
Dabigatran
 99 (10.3)
2
 63 (9.7)
1
 36 (11.3)
1
  0.446
Apixaban
130 (13.5)
2
 57 (8.8)
1
 73 (23.0)
1
<0.001
Edoxaban
  5 (0.5)
2
  5 (0.8)
1
1
  0.178
LMWH
 13 (1.3)
2
  1 (0.2)
1
 12 (3.8)
1
<0.001
Any anticoagulation drug
887 (91.9)
2
593 (91.7)
1
294 (92.5)
1
  0.669
ASA
101 (10.5)
2
 40 (6.2)
1
 61 (19.2)
1
<0.001
Clopidogrel
 29 (3.0)
2
 19 (2.9)
1
 10 (3.1)
1
  0.859
Ticagrelor
  4 (0.4)
2
  4 (0.6)
1
1
  0.309
Dipyridamole
  2 (0.2)
2
  1 (0.2)
1
  1 (0.3)
1
  0.551
Sotalol
141 (14.6)
2
111 (17.2)
1
 30 (9.4)
1
  0.001
– Mean ± SD dose per day in mg
155 ± 74
 
149 ± 73
 
176 ± 75
 
  0.056
Amiodaron
128 (13.3)
3
 38 (5.9)
2
 90 (28.3)
1
<0.001
– Mean ± SD dose per day in mg
232 ± 105
 
208 ± 78
 
241 ± 115
 
  0.052
Flecainide
 80 (8.3)
2
 53 (8.2)
1
 27 (8.5)
1
  0.874
– Mean ± SD dose per day in mg
151 ± 57
 
142 ± 54
 
169 ± 61
 
  0.078
Propafenone
  4 (0.4)
2
1
  4 (1.3)
1
  0.012
Disopyramide
  3 (0.3)
2
  2 (0.3)
1
  1 (0.3)
1
  0.999
Any anti-arrhythmic drug
354 (36.7)
2
203 (31.4)
1
151 (47.5)
1
<0.001
Beta blocker
541 (56.1)
3
367 (56.8)
2
174 (54.7)
1
  0.538
CCB
171 (17.7)
2
117 (18.1)
1
 54 (17.0)
1
  0.673
Digoxin
141 (14.6)
2
126 (19.5)
1
 15 (4.7)
1
<0.001
Any rate control drug
653 (67.7)
2
448 (69.2)
1
205 (64.5)
1
  0.136
ACE inhibitor
307 (31.8)
2
185 (28.6)
1
122 (38.4)
1
  0.002
Angiotensin receptor blocker
196 (20.3)
2
132 (20.4)
1
 64 (20.1)
1
  0.920
Aliskiren
  6 (0.6%)
2
1
  6 (1.9)
1
  0.001
Aldosterone blockers
 65 (6.7)
2
 35 (5.4)
1
 30 (9.4)
1
  0.019
Any RAAS inhibiting drug
529 (54.8)
2
327 (50.5)
1
202 (63.5)
1
<0.001
Diuretics
335 (34.7)
2
221 (34.2)
1
114 (35.8)
1
  0.604
Non-DHP CCB
 58 (6.0)
2
 46 (7.1)
1
 12 (3.8)
1
  0.040
Statin
409 (42.4)
2
260 (40.2)
1
149 (46.9)
1
  0.049
Oral anti-diabetics
133 (13.8)
2
 73 (11.3)
1
 60 (18.9)
1
  0.001
Insulin
 35 (3.6)
2
 24 (3.7)
1
 11 (3.5)
1
  0.845
Thyroid hormones
 64 (6.6)
2
 19 (2.9)
1
 45 (14.2)
1
<0.001
Thyroid-suppressing drugs
 10 (1.0)
2
  7 (1.1)
1
  3 (0.9)
1
  0.842
Proton pump inhibitors
275 (28.5)
2
201 (31.1)
1
 74 (23.3)
1
  0.012
ACE angiotensin-converting enzyme, ASA acetylsalicylic acid, CCB calcium channel blocker, DHP dihydropyridine, LMWH low molecular weight heparins, RAAS renin-angiotensin-aldosterone system, SD standard deviation, VKA vitamin K antagonist

Rate versus rhythm control therapy

At baseline, the majority of the patients were on a rhythm control strategy according to the treating physician (n = 565, 58.6%), whereas 326 patients (33.8%) were on a rate control strategy. For the remainder of the patients (n = 73, 7.6%), no decision regarding the treatment strategy had been made yet.
In total, 354 patients (36.7%) were prescribed an anti-arrhythmic drug (AAD) for daily use and 653 (67.7%) a rate control drug (Tab. 2). Belgian patients were more frequently on AAD therapy (47.5% vs 31.4%, p < 0.001) with significantly more amiodarone users compared with their Dutch counterparts (28.3% vs 5.9%, p < 0.001), whereas Dutch patients more often received sotalol (17.2% vs 9.4%, p = 0.001). The prescription rates for the other AADs were comparable (Tab. 2). For rate control drugs, only digoxin use was significantly different between the two countries, with more frequent prescription in the Netherlands (19.5% vs 4.7%, p < 0.001).
Of the 565 patients with rhythm control as treatment strategy, 313 patients (55.4%) were on daily AAD treatment. In the remainder of patients, 14 (5.6%) were planned for electrical cardioversion and 1 (0.4%) for surgical AF ablation, meaning that 237 patients (41.9%) were on a rhythm control strategy without daily AAD use or a planned rhythm intervention.
Of the 326 patients with rate control as treatment strategy, 280 patients (86.2%) were on rate control drugs, whereas 45 (13.8%) were not (for 1 patient medication was missing). Notably, 34 of the 326 patients with rate control as treatment strategy (10.4%) were on daily AAD treatment. In the remainder of patients, 4 (1.4%) were planned for electrical cardioversion, meaning that 38 patients (11.8%) were wrongfully classified as rate control and should in fact have been classified as rhythm control regarding the treatment strategy.

Anticoagulant therapy

At baseline, 887 patients (91.9%) received anticoagulant treatment, with a larger proportion of patients using a non-vitamin K antagonist oral anticoagulant (NOAC) in Belgium than in the Netherlands (54.4% vs 38.4%). Fig. 1 depicts the percentage of patients with and without anticoagulation for the different CHA2DS2-VASc (congestive heart failure, hypertension, age ≥ 75 years [doubled], diabetes mellitus, prior stroke [doubled], vascular disease, age 65–74, sex category) scores, also specifying the type of anticoagulant. For men with CHA2DS2-VASc 0 and for women with CHA2DS2-VASc 1, the anticoagulation rates were 71.6% (68/95 patients) and 66.7% (20/30 patients) respectively. In these patients with anticoagulation, a rhythm intervention was performed during the baseline assessment or planned for the near future in 45 men (66.2%) and 7 women (35%). The remaining 23 men (33.8%) and 13 women (65%) were on anticoagulant treatment without a clear indication (Fig. 2).
For patients with NOACs, over- and underdosing of NOACs were checked according to the dose reduction criteria for the respective drug [6]. In total, 14 patients were prescribed the full dose for a NOAC, whereas they should have received the reduced dose according to the Summary of Product Characteristics (SmPC). This was the case for 12/148 patients with rivaroxaban and 2/57 with dabigatran (“Overdosed NOAC” in Fig. 2). No overdosing was present for both apixaban (n = 70) and edoxaban (n = 5). Underdosing occurred in 49 patients (“Underdosed NOAC” in Fig. 2), i.e. 38/50 patients with apixaban, 8/24 with rivaroxaban, and 3/30 with dabigatran. Reduced dose of edoxaban was not prescribed. In total, 63 (16.7%) of 372 patients were not correctly dosed.

Follow-up

One year follow-up data was available in 882 (91.2%) of 967 patients. MACCE occurred in 37 (4.2%) of these patients. In total, 27 (3.1%) patients died within a year, 8 of whom from a cardiovascular cause (0.9%). Ischaemic stroke occurred in 7 patients (0.8%) and TIA in 3 (0.3%). Two patients (0.2%) had intracranial haemorrhage, one of whom died as a consequence, whereas 14 patients (1.6%) had a major extracranial bleeding. Myocardial infarction occurred in 5 patients (0.6%), one of these patients also had an ischaemic stroke.
Of the patients with ischaemic stroke/TIA, 7 out of 10 were on anticoagulant therapy at baseline. The remaining 3 patients were not, despite a CHA2DS2-VASc score of 2, 3 and 5 respectively. However, at follow-up all 3 patients were on anticoagulant therapy, but 1 of the other 7 patients with an ischaemic event had stopped using anticoagulant therapy. As for the 16 patients with a major bleeding event during follow-up, they all had anticoagulant therapy at baseline. At follow-up, 1 patient had stopped therapy (6.3%), 14 patients were still on anticoagulant therapy, and 1 had died as a consequence of the intracranial haemorrhage. Of the 37 patients with MACCE during follow-up, only 1 was underdosed (major extracranial bleeding event), totalling to 4 patients (10.8%) with undertreatment. No overtreatment was seen in these patients.
During follow-up, the most frequently established new diagnosis was heart failure (40 patients, 4.5%), followed by chronic kidney disease, defined as initiation of chronic dialysis, renal transplantation, or serum creatinine ≥ 200 μmol/l (2.26 mg/dl), in 23 patients (2.6%), and hypertension in 16 patients (1.8%). In addition, new-onset overt coronary artery disease was diagnosed in 15 patients (1.5%), diabetes mellitus in 8 (0.9%), and peripheral artery disease in 4 (0.5%) patients.

Rhythm follow-up and interventions

Rhythm follow-up was available in 839 patients (86.8%). AF progression and AF regression occurred at a similar rate, with 57 (17.3%) of 329 patients with paroxysmal AF at baseline progressing into persistent or permanent AF after one year of follow-up and 87 (17.6%) of 494 patients with persistent or permanent AF regressing into paroxysmal AF. Of the regressors, 38 patients (43.7%) were already on AAD treatment at baseline. A rhythm intervention was performed during follow-up in 20 (23.0%) of 87 patients showing regression, i.e. in 12 patients (13.8%) an AAD was initiated, in 9 patients (10.3%) a catheter ablation for AF was performed (1 of whom also started AAD therapy), and in 2 patients (2.3%) surgery for atrial fibrillation was performed (both of them started AAD therapy as well). The remaining 67 patients (77%) showed regression in type of AF without rhythm intervention.
In total, 233 (26.4%) of 882 patients had at least 1 rhythm intervention during follow-up, i.e. 155 patients (17.6%) underwent electrical cardioversion, 33 patients (3.7%) pharmacological cardioversion, and 77 patients (8.7%) catheter ablation for AF. Of the latter, 72 patients underwent a pulmonary vein isolation and 7 atrioventricular node ablation with pacemaker implantation. Furthermore, 14 patients (1.6%) underwent surgery for AF, 9 of which as stand-alone procedure and 5 concomitantly with another intervention, and 19 patients (2.2%) underwent an ablation for atrial flutter, 6 of which as stand-alone and 13 concomitantly with AF ablation.
Supplementary Fig. 1 shows the changes in treatment strategy for AF from baseline to follow-up. Relatively more patients changed from rate to rhythm control therapy than vice versa (24% vs 20%), although absolute numbers show the opposite (66 vs 99 patients). The majority of patients were on the same treatment strategy at baseline and at 1‑year follow-up, i.e. 610 of 775 patients (79%).

Discussion

In this analysis of the EORP-AF LTG registry, we provide a contemporary representation of the characteristics, treatment, and outcomes of AF patients in the Netherlands and Belgium, both inpatient and outpatient. Overall, hypertension was the most frequently documented comorbidity and present in almost half of all patients. “Lone AF” was present in 12% of the patients, which is comparable with the 10% seen in the Euro Heart Survey 15 years ago [7].
Strikingly, a large proportion of the patients without an indication for chronic anticoagulant treatment, i.e. men with a CHA2DS2-VASc score of 0 and women with a score of 1, are in fact anticoagulated at baseline (70%). A slim majority (59%) of these patients underwent a rhythm intervention at or shortly after baseline, resulting in overtreatment of patients with anticoagulant therapy in the remainder, which translates into 5% of the total population being overtreated (Fig. 2). Undertreatment of patients was even more prevalent, with 9% of the patients either receiving no anticoagulation at all in the presence of an indication based on the CHA2DS2-VASc score, or receiving the reduced dose of a NOAC without a reason for dose reduction. In total, 17% of the patients using a NOAC are incorrectly dosed. Previous reports have shown higher rates, with a Belgian single-centre study showing 25% and a Turkish single-centre study showing 37% of inappropriate dosing [8, 9].
MACCE occurred in 37 patients (4.2%) after 1 year of follow-up, which is relatively low. To put into perspective, 208 (5.3%) of 3890 patients in the Euro Heart Survey died of cardiovascular cause or developed ischaemic stroke/TIA after one year, not taking into account major bleeding events and myocardial infarction, which comprise half of the MACCE in this registry [10]. Given the rather low rate of ischaemic complications and major bleeding events after one year in this population, it is hard to draw any conclusions regarding the relationship between these endpoints and undertreatment or overtreatment. All patients with a major bleeding event were anticoagulated with correct dosing, whereas in the 10 patients with ischaemic stroke/TIA, 7 were correctly treated and 3 were incorrectly not anticoagulated. The rates of ischaemic stroke/TIA in patients with and without anticoagulants are in line with previous reports, i.e. 3.75% (3 of 80) in those without and 0.79% (7 of 887) in those with anticoagulants [11].
Rhythm control was the preferred treatment strategy at baseline in 59% of the analysed patients, whereas one third of the patients were on a rate control strategy. The majority of patients (80%) were on the same treatment strategy at baseline and at follow-up. Misclassification regarding treatment strategy was observed in 12% of patients. In these cases, rate control was the appointed treatment strategy, but patients were either receiving AAD treatment on a daily basis or were scheduled for electrical cardioversion. Therefore, more awareness regarding definitions and the correct use of terminology is warranted [6]. On a side note, in patients in whom rate control drugs do not sufficiently achieve adequate rate control physicians may feel the need to use AAD for rate control. Information regarding the reasoning behind the treatment strategy was not reported, so this could not be assessed in this population.
Both AF progression and regression occurred at a similar rate of 17% per year, keeping in mind that a misclassification in type of AF inherently leads to a misclassification in AF progression and regression. In a quarter of the regressors, AAD treatment was initiated or a rhythm intervention was performed during follow-up. The remainder of the patients regressed without a change in rhythm therapy, arising the question whether misclassification also plays a role in this high rate of regression after 1 year. The only way to solve this issue, is by increasing the monitoring duration, e.g. performing more 24-hour Holter recordings or making use of more rigorous modalities such as implantable loop recorders [12].
Some differences between the two countries are present at baseline, e.g. the higher prevalence of heart failure, type 2 diabetes, and sleep apnoea in Belgium. This is most likely caused by the higher proportion of hospitalised patients included in Belgium compared with the Netherlands (55% vs 37%). In addition to these differences in patient characteristics, distinct drug prescription patterns are discernible between the two countries, i.e. amiodarone is more frequently used in Belgium and sotalol more frequently in the Netherlands. No differences are seen in the use of flecainide, whereas propafenone is only prescribed in Belgium. In addition, digoxin use is more prevalent in the Netherlands for rate control. Regarding anticoagulant therapy, Belgian patients were more frequently on NOACs compared with their Dutch counterparts (54% vs 38%), showing the faster implementation and uptake of NOACs in Belgium, as shown previously [13].

Strengths and limitations

As in all registries, the strength of this registry is dependent upon the completeness of the data obtained by all participating centres, so clinical factors can be both over- and underrepresented. Furthermore, the reported data are observational. In order to reduce selection bias, participating centres were asked to include consecutive AF patients. Nonetheless, we believe the data presented in this article are comprehensive and provide a representative overview of AF patients in the Netherlands and Belgium and the treatment they receive.
Of note, patients were deemed underdosed for dabigatran only if both the regular and the lenient dose reduction criteria, i.e. age 75–80 years and eGFR 30–50 ml/min for which dose reduction can be considered, were not met. In addition, verapamil/diltiazem shared the same checkbox in the case report file, so it is unclear which of the two the patient is using, therefore we cannot be sure whether the dose reduction is adequate. Furthermore, treating physicians may have chosen to treat patients at increased risk of bleeding with the reduced dose of dabigatran, since the reduced dose is non-inferior to vitamin K antagonists (VKAs), this was not taken into account. For apixaban, the rate of underdosing is most likely to be overestimated, since in some patients not the daily dose of apixaban was filled in the case report file as requested, but rather the dose for a single gift. In patients with 10 mg and 2.5 mg of apixaban, it is clear whether the patient receives the reduced or full dose, for 5 mg however, this is not clear. These patients were assessed as having the reduced dose of apixaban, meaning that the rate of underdosing might be overestimated as these patients could in fact be on twice daily 5 mg of apixaban.

Conclusion

Overtreatment and undertreatment with anticoagulants are still observable in 14% of this contemporary, West-European AF population. Still, MACCE occurred in only 4% of the patients after 1 year of follow-up.

Acknowledgements

We are grateful to all participating centres, investigators, and data collection officers for performing the registry. Data collection was conducted by the EURObservational Research Programme department from the European Cardiac Society by Patti-Ann McNeill as project officer and by Viviane Missiamenou as data manager. Overall activities were coordinated by Dr Aldo P. Maggioni (EORP Scientific Coordinator).

Funding

We are very grateful to the alliance of Bristol-Myers Squibb and Pfizer for their financial support in performing the EORP-AF Long-Term General Registry in both the Netherlands and Belgium. The sponsor was not involved in the preparation or publication of this manuscript.
The EURObservational Research Programme is supported by the following companies: Abbott Vascular Int. (2011–2014), Amgen Cardiovascular (2009–2018), AstraZeneca (2014–2017), Bayer AG (2009–2018), Boehringer Ingelheim (2009–2019), Boston Scientific (2009–2012), The Bristol Myers Squibb and Pfizer Alliance (2011–2016), The Alliance Daiichi Sankyo Europe GmbH and Eli Lilly and Company (2011–2017), Edwards (2016–2019), Gedeon Richter Plc. (2014–2017), Menarini Int. Op. (2009–2012), MSD-Merck & Co. (2011–2014), Novartis Pharma AG (2014–2017), ResMed (2014–2016), Sanofi (2009–2011), and SERVIER (2009–2018).
This work was supported by the Netherlands Cardiovascular Research Initiative: an initiative with support of the Dutch Heart Foundation [CVON 2014‑9, RACE V: “Reappraisal of Atrial Fibrillation: interaction between hyperCoagulability, Electrical remodelling, and Vascular destabilisation in the progression of AF” to Ö.E., H.J.G.M.C., J.G.L.M.L].

Conflict of interest

Ö. Erküner, M. van Eck, O. Xhaet, H. Verheij, J. Neefs, A. Duygun, R. Nijmeijer, S.A.M. Saïd, H. Uiterwaal, V. Hagens, R. Bhagwandien, T. Szili-Torok, N. Bijsterveld, G. Tjeerdsma, J. Vijgen, A. Friart, E. Hoffer, P. Evrard, M. Srynger, J. Meeder, J.R. de Groot, J. van Opstal, R. Gevers, G.Y.H. Lip, G. Boriani, H.J.G.M. Crijns, J.G.L.M. Luermans and G.H. Mairesse declare that they have no competing interests.
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Metagegevens
Titel
Contemporary management of patients with atrial fibrillation in the Netherlands and Belgium: a report from the EORP-AF long-term general registry
Auteurs
Ö. Erküner
M. van Eck
O. Xhaet
H. Verheij
J. Neefs
A. Duygun
R. Nijmeijer
S. A. M. Saïd
H. Uiterwaal
V. Hagens
R. Bhagwandien
T. Szili-Torok
N. Bijsterveld
G. Tjeerdsma
J. Vijgen
A. Friart
E. Hoffer
P. Evrard
M. Srynger
J. Meeder
J. R. de Groot
J. van Opstal
R. Gevers
G. Y. H. Lip
G. Boriani
H. J. G. M. Crijns
J. G. L. M. Luermans
G. H. Mairesse
Publicatiedatum
15-09-2021
Uitgeverij
Bohn Stafleu van Loghum
Gepubliceerd in
Netherlands Heart Journal / Uitgave 11/2021
Print ISSN: 1568-5888
Elektronisch ISSN: 1876-6250
DOI
https://doi.org/10.1007/s12471-021-01634-y