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ISSN (On-line): 1678-9741
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Volume 32 Number 4, July - August, 2017


DOI: http://dx.doi.org/10.21470/1678-9741-2017-0031

Risk Factors for Delayed Extubation after Ventricular Septal Defect Closure: a Prospective Observational Study

Divyakant ParmarI, MD; Ketav LakhiaII, M.Ch; Pankaj GargII, M.Ch; Kartik PatelII, M.Ch; Ritesh ShahI, MD; Jigar SurtiI, MD; Jigar PanchalI, MD; Himani PandyaIII, MSc

IDepartment of Cardiac Anesthesia of the U. N. Mehta Institute of Cardiology and Research Center (affiliated to BJ Medical College, Ahmedabad), Gujarat, India
IIDepartment of Cardiovascular and Thoracic Surgery of the U. N. Mehta Institute of Cardiology and Research Center (affiliated to BJ Medical College, Ahmedabad), Gujarat, India
IIIDepartment of Research of the U. N. Mehta Institute of Cardiology and Research Center (affiliated to BJ Medical College, Ahmedabad), Gujarat, India

This study was carried out at the U. N. Mehta Institute of Cardiology and Research Center (affiliated to BJ Medical College, Ahmedabad), Gujarat, India.

Correspondence To:
Pankaj Garg
Department of Cardiovascular and Thoracic Surgery
U. N. Mehta Institute of Cardiology and Research Center, Civil Hospital Campus,
Asarwa, Ahmedabad-380016, Gujarat, India
Email: pnkjgarg@yahoo.co.in


Objective: The objective of our study was to determine the feasibility of early extubation and to identify the risk factors for delayed extubation in pediatric patients operated for ventricular septal defect closure.
Methods: A prospective, observational study was carried out at our Institute. This study involved consecutive 135 patients undergoing ventricular septal defect closure. Patients were extubated if feasible within six hours after surgery. Based on duration of extubation, patients were divided two groups: Group 1= extubation time ≤ 6 hours, Group 2= extubation time >6 hours.
Results: A total of 99 patients were in Group 1 and 36 patients in Group 2. Duration of ventilation was 4.4±0.9 hours in Group 1 and 25.9±24.9 hours in Group 2 (P<0.001). Univariate analysis showed that young age, low weight, low partial pressure of oxygen, trisomy 21, multiple ventricular septal defect, high vasoactive inotropic score, transient heart block and low cardiac output syndrome were associated with delayed extubation. However, regression analysis revealed that only trisomy 21 (OR: 0.248; 95%CI: 0.176-0.701; P=0.001), low cardiac output syndrome (OR: 0.291; 95%CI: 0.267-0.979; P=0.001), multiple ventricular septal defect (OR: 0.243; 95%CI: 0.147-0.606; P=0.002) and vasoactive inotropic score (OR: 0.174 95%CI: 0.002-0.062; P=0.039) are strongest predictors for delayed extubation.
Conclusion: Trisomy 21, low cardiac output syndrome, multiple ventricular septal defect and high vasoactive inotropic score are significant risk factors for delay in extubation. Age, weight, pulmonary artery hypertension, size of ventricular septal defect, aortic cross-clamp and cardiopulmonary bypass time did not affect early extubation.

Keywords Heart Septal Defects. Ventricular. Cardiac Output. Low. Vasoactive Inotropic Score


ABG = Arterial blood gases

ACC = Aortic cross-clamp

ACT = Activated clotting time

ASD = Atrial septal defect

CPAP = Continuous positive airway pressure

CPB = Cardiopulmonary bypass

ETCO2 = End-tidal CO2

FiO2 = Fraction of inspired oxygen

ICU = Intensive care unit

IS = Inotropic score

LCOS = Low cardiac output syndrome

MAP = Mean arterial pressure

PaCO2 = Partial pressure of carbon dioxide

PAH = Pulmonary arterial hypertension

PDA = Patent ductus arteriosus

PEEP = Peek end expiratory pressure

PH = Pulmonary hypertension

PO2 = Partial pressure of oxygen

PTFE = Polytetrafluroethylene

RHC = Right heart catheterization

VIS = Vasoactive inotropic score

VSD = Ventricular septal defect


In the inceptual era of pediatric cardiac surgery, prolonged mechanical ventilation was a norm in the postoperative care, which significantly contributed to morbidity and mortality. Early extubation (within 6-8 hours after surgery)[1] following pediatric cardiac surgery was initially conceptualized in the 1980s[2]. This gradually received wide acceptance due to increasing number of patients and limited resources.

In the modern era, where chance of error tends to zero in terms of results, early extubation has improved results tremendously in appropriate cases by reducing potential complications of prolonged mechanical ventilation. This strategy reduces intensive care unit (ICU) and hospital stay, henceforth reduces overall treatment cost and utilization of resources.

In the literature, there have been relatively few articles addressing this useful strategy [3-10]. But, despite of its advantages, it cannot be applied in all cases, as various factors decide whether early extubation is feasible or not. Therefore, we have performed a prospective observational study to identify the predictive factors for early extubation after ventricular septal defect (VSD) closure.


All consecutive patients operated for VSD closure between March 2015 and February 2016 in the Department of Cardiothoracic Surgery, U.N. Mehta Institute of Cardiology & Research Center, were enrolled in this prospective observational study. The study was approved by our institutional ethics committee and informed and written consent was obtained from the parents of all the patients. Inclusion criteria were presence of isolated or multiple VSDs, with or without atrial septal defect (ASD), and/or patent ductus arteriosus (PDA). Patients with associated complex congenital cardiac disease other than ASD and PDA and patients on ventilator preoperatively were excluded. Size of VSD was categorized echocardiographically as small, moderate or large. A large defect has a diameter of 75% or greater of the aortic annulus and ≤ 1 m/s of velocity flow by Doppler. A small defect has diameter < 33% of aortic annulus and a flow velocity ≥ 4 m/s[11].

Premedication and Anesthetic Management

Intravenous midazolam was used as premedication at dose 0.1 mg/kg, 15-20 minutes before induction of anesthesia. Patients were induced with intravenous fentanyl (5-10 µg/kg) and vacuronium (0.2 mg/kg). Inhalational induction with sevoflurane 8% in 100% oxygen was done in patients with no intravenous line. Maintenance anesthesia consisted of low concentration sevoflurane, intravenous fentanyl (1 µg/kg) and vacuronium 0.1 mg/kg hourly and whenever required.

Invasive blood pressure monitoring was performed through right radial or right femoral artery catheterization. Central venous pressure monitoring was performed through internal jugular vein catheterization. Other monitoring included electrocardiogram, oxygen saturation, end-tidal CO2 (ETCO2), nasopharyngeal temperature and urine output. Arterial blood gases (ABG), with haemoglobin, electrolytes, blood sugar, and activated clotting time (ACT) were also monitored. Monitoring during cardiopulmonary bypass (CPB) time included mean arterial pressure (MAP), urine output and systemic venous oxygen saturation. ABG and ACT were done half hourly while the patient was on pump.

Surgery and Cardiopulmonary Bypass

All the patients were operated through midline sternotomy, moderate hypothermic cardiopulmonary bypass (temperature 32oC) and blood cardioplegic arrest. VSD was closed with polytetrafluroethylene (PTFE) patch using continuous sutures or primarily using pledgeted sutures. Milrinone (50 µg/kg loading dose followed by 0.5 µg/kg/min infusion) and epinephrine (0.05 µg/kg/min) were used as a choice of inotropes while weaning from CPB and continued in the postoperative period. Inotropes were titrated depending upon hemodynamics. Milrinone was continued in the postoperative period at least 24 hours postextubation and gradually tapered thereafter. Before extubation, effect of muscle relaxant was reversed with glycopyrrolate (10 µg/kg) and neostigmine (0.05 mg/kg) intravenously. Postoperatively, all patients were given fentanyl infusion (1-2 µg/kg/hour) and intravenous paracetamol 15 mg/kg/dose 8 hourly for pain relief. Fentanyl infusion was continued until the patient was extubated and/or drains were removed.

Criteria for Early Extubation

Patients were considered for extubation since they regained consciousness with adequate airway protective reflexes without the use of accessory respiratory muscle and if they met the following criteria: stable hemodynamics, adequate urine output, no significant mediastinal bleeding, adequate oxygenation at fraction of inspired oxygen (FiO2) 50% or less (pO2/FiO2 > 200), pH 7.35 or greater, partial pressure of carbon dioxide (PaCO2) in arterial blood ≤ 45 mmHg or less at peek end expiratory pressure (PEEP) 5 cmH2O on continuous positive airway pressure (CPAP) with pressure support ≤ 8 cmH2O. Intensivist, anesthesiologist and surgeon jointly decide on early or delayed extubation.

To identify the risk factors for early extubation, patients were divided into two groups based on duration of mechanical ventilation: Group 1 (≤ 6 hours) and Group 2 (> 6 hours). Both groups were compared for age, sex, weight, nutritional status, genetic disorders (e.g. Down syndrome), severity of pulmonary arterial hypertension (PAH), vasoactive inotropic score (VIS)[12], type and number of VSDs, aortic cross-clamp (ACC) and CPB time, postoperative complications[13], ICU stay, hospital stay and mortality. Definitive diagnosis of pulmonary hypertension (PH) requires an elevated mean pulmonary arterial pressure (Ppa) of ≥ 25 mmHg at rest, measured by right heart catheterization (RHC).

Low cardiac output syndrome (LCOS) was defined as clinical signs or symptoms (tachycardia, oliguria, poor perfusion, cold extremities, hypotension, lowered level of consciousness, cardiac arrest) with or without a widened arterial-mixed venous oxygen saturation difference or metabolic acidosis [14,15]. A stroke is any confirmed neurological deficit of abrupt onset caused by a disturbance in blood flow to the brain, when the neurologic deficit does not resolve within 24 hours. Significant bleeding (12 ml/kg/h in 1st hour or 10 ml/kg/h in 2nd hour or 8 ml/kg/h in the 3rd hour) affecting the hemodynamics or requiring re-exploration [16]. Hematologic dysfunction was defined as platelet count < 80,000/mm[14] or a decline of 50% in the platelet count from the highest value recorded over the last 48 hours[17]. Hepatic dysfunction was defined as alanine transaminase level 2 times upper limit of normal. Prolonged ventilatory requirement was defined as need for invasive ventilation for more than 48 hours[17].

Statistical Analysis

Statistical analysis was carried out using SPSS version 20.0 software (SPSS Inc., USA). Quantitative data was expressed as mean ± SD whereas qualitative data was expressed as percentage. The P value less than 0.05 was considered to be significant. Univariate analysis of the continuous data using Student's t-test, whereas chi-square test was used for the categorical data. The variables following non-normal distribution were assessed using Mann-Whitney U test.


Study included total 135 patients operated for VSD closure with or without ASD and/or PDA. Group 1 included 99 (73.3%) patients while Group 2 included 36 (26.7%). Demographic details of the patients are shown in Table 1. Mean age was 26.7 months (range 2 months to 12 years) and mean weight was 7.46 kg (range 3.4 to 25 kg). Trisomy 21 (Down syndrome) was present in 9 (6.6%) patients. One hundred and twenty (88.8%) patients had chronic malnutrition. However, mean age (26.37 months in Group 1 and 18.5 months in Group 2, P=0.019) was significantly more in Group 1 while incidence of trisomy 21 was significantly less (P=0.015) in Group 1 compared to Group 2. There was no significant difference between the two groups with regards to sex, type and size of VSD, severity of PAH and associated cardiac lesions. Incidence of multiple VSD was significantly more in Group 2 (P=0.019).

Table 1 - Demographic details.
  Group 1 ≤ 6 hrs (n=99) Group 2 > 6 hrs (n=36) Pvalue
Age (months) 26.37 ± 30.89 18.5 ± 26.2 0.019
Sex (male) (56.56%) (50%) 0.7869
Weight (kg) 7.85 ± 4.14 6.38 ± 3.68 0.005
Malnutrition 88 (87.8%) 32 (91.6%) 0.808
Trisomy 21 (n, %) 2 (3%) 7 (16.6%) 0.015
Type of VSD      
    Perimembranous (n, %) 68 (68.6%) 20 (55.5%) 0.225
    Subaortic (n, %) 19 (19.1%) 10 (27.7%) 0.402
    Muscular (n, %) 12 (12.1%) 6 (16.6%) 0.688
Size of VSD      
    Small VSD (n, %) 24 (25.2%) 7 (16.6%) 0.802
    Moderate VSD (n, %) 4 (4.04%) __ 0.533
    Large VSD (n, %) 72 (70.7%) 28 (83.3%) 0.480
    Mild PAH (n, %) 20 (21.21%) 3 (5.5%) 0.198
    Moderate PAH (n, %) 10 (10.10%) 3 (8.3%) 0.931
    Severe PAH (n, %) 70 (68.68%) 29 (86.1%) 0.208
    Single VSD (n, %) 80 (79.79%) 23 (66.6%) 0.139
    Multiple VSD (n, %) 5 (5.05%) 7 (19.4%) 0.019
    VSD+PDA (n, %) 3 (3.03%) 1 (2.7%) 0.618
    VSD+ASD (n, %) 12 (12.12%) 4 (11.1%) 0.888

VSD=ventricular septal defect; ASD=atrial septal defect; PAH=pulmonary arterial hypertension; PDA=patent ductus arteriosus

Table 1 - Demographic details.

In intraoperative data, ACC time (P=0.443) and CPB time (P=0.522) were comparable in both groups (Table 2). Postoperatively, VIS was significantly higher in Group 2 (P=0.001). Arterial blood gas data was comparable in both groups, except arterial partial pressure of oxygen (PO2), which was significantly higher in Group 1 (P=0.034). Mean duration of mechanical ventilation (4.4±0.9 hours vs. 25.9±24.9 hours, P<0.001), ICU stay (3.1±1.3 days vs. 5.6±2.9 days, P<0.001), and hospital stay (7.8±2.4 days vs. 11.2±4.9 days, P<0.001) were significantly lower in Group 1 compared to Group 2.

Table 2 - Intraoperative and postoperative data.
  Group 1≤ 6 hrs (n=99) Group 2> 6 hrs (n=36) P value
ACC time (min) 28.45±11.18 31.30±14.91 0.443
CPB time (min) 46.75±13.84 50.91±19.53 0.522
VIS 9.01±2.05 10.65±2.94 0.001
Arterial blood gas      
    pH 7.38±0.04 7.38±0.07 0.937
    PCO2 (mmHg) 38.29±5.78 38.20±7.9 0.978
    PO2 (mmHg) 246.57±79.28 207.98±82.52 0.034
    Hematocrit (%) 39.26±5.94 37.08±6.86 0.057
    Bicarbonate (mEq/L) 26.24±24.82 22.85±3.12 0.893
MVT (hours) 4.4±0.9 25.9±24.9 <0.001
ICU stay (days) 3.1±1.3 5.6±2.9 <0.001
Hospital stay (days) 7.8±2.4 11.2±4.9 <0.001

ACC=aortic cross-clamp; CPB=cardiopulmonary bypass; VIS=vasoactive inotropic score; PCO2=partial pressure of carbon dioxide; PO2=partial pressure of oxygen; MVT=mechanical ventilation time; ICU=intensive care unit

Table 2 - Intraoperative and postoperative data.

Reintubation was required in 6 patients, of which 2 patients were in Group 1. Incidence of reintubation and postoperative complications, including transient heart block, LCOS, sepsis, significant bleeding and neurological events was greater in Group 2. However, the difference was not statistically significant except for LCOS (Table 3). Incidence of LCOS was significantly higher in Group 2 (P<0.001). There was one death in Group 2 due to LCOS and no deaths in Group 1, however the difference was not statistically significant (P=0.596). Regression analysis is shown in Table 4. Regression analysis found independent association of trisomy 21 (OR: 0.248; 95% CI: 0.176-0.701; P=0.001), multiple VSD (OR: 0.243; 95% CI: 0.147-0.606; P=0.002), VIS score (OR: 0.174; 95% CI: 0.002-0.062; P=0.039) and LCOS (OR: 0.291; 95% CI: 0.267-0.979; P=0.001) with late extubation. LCOS and trisomy 21 were the strongest predictor of late extubation, closely followed by multiple VSD and the least was VIS (Table 4).

Table 3 - Postoperative complications and mortality.
  Group 1≤ 6 hrs (n=99) Group 2>6 hrs (n=36) Pvalue
Reintubation 2 (2%) 4 (11.1%) 0.072
LCOS 0 6 (16.6%) <0.001
Heart block      
    Transient __ 3  
    Permanent __ __  
Renal dysfunction __ __  
Hepatic dysfunction __ __  
Respiratory failure __ __  
Haematological complication __ __  
Prolonged mechanical ventilation __ __  
Sepsis 6 (6%) 2 (5.5%) 0.762
Bleeding __ 1 (2.7%) 0.596
Neurological event __ 1 (2.7%) 0.596
Mortality __ 1 (2.7%) 0.596

LCOS=low cardiac output syndrome

Table 3 - Postoperative complications and mortality.
Table 4 - Regression analysis.
  Unstandardized coefficients Standardized coefficients   95% Confidence Interval for B
B Std. Error Beta t Sig. Lower bound Upper bound
(Constant) 0.199 0.193   1.030 0.305 -0.184 0.582
Age (month) 0.003 0.003 0.200 1.164 0.247 -0.002 0.008
Weight -0.028 0.019 -0.261 -1.526 0.130 -0.065 0.008
PO2 -0.001 0.000 -0.144 -1.915 0.058 -0.002 0.000
Trisomy 21 0.438 0.133 0.248 3.303 0.001 0.176 0.701
Multiple VSD 0.376 0.116 0.243 3.240 0.002 0.147 0.606
VIS 0.032 0.015 0.174 2.090 0.039 0.002 0.062
Transient HB 0.211 0.267 0.071 0.790 0.431 -0.318 0.740
LCOS 0.623 0.180 0.291 3.462 0.001 0.267 0.979

VSD=ventricular septal defect; PO2=partial pressure of oxygen; VIS=vasoactive inotropic score; HB=heart block; LCOS=low cardiac output syndrome

Table 4 - Regression analysis.


Advances in surgical and anaesthetic techniques have facilitated early extubation following paediatric cardiac surgery. Early extubation has led to decreased cardiac and respiratory morbidity, lower rate of nosocomial pneumonia, reduction in overall length of hospital stay and decreased cost of patient care[8,18-20]. Reintubation rate following early extubation is also reported to be very low (< 2-3%)[21].

In our study, 74.1% patients were successfully extubated within 6 hours of surgery and mean duration of mechanical ventilation was 4.4±0.9 hours, while only 2% patients require reintubation after early extubation. These results are consistent with various studies. In the studies by Mittnacht et al.[20] and Akhtar et al.[17], 76% patients operated for VSD closure were successfully extubated early. Our results along with results of their studies show that with appropriate perioperative management, about 75% patients can be extubated early after VSD closure without significant increase in risk of reintubation.

In our study, on univariate analysis, age, weight, trisomy 21, multiple VSDs, high VIS, low PO2 and low cardiac output after surgery were significant risk factors for delayed extubation. However, on multivariate analysis, trisomy 21, multiple VSD, VIS score and LCOS after surgery were found to be independently associated with delayed extubation.

Patients who are operated for multiple, VSDs have higher risk of residual defect and ventricular dysfunction postoperatively, leading to increased mortality and morbidity[22]. Therefore, these patients are at higher risk for prolonged ventilation as seen in our study. Mean ventilation duration in these patients was significantly higher (13.7±8.5 hours vs. 4.4±0.9 hours) compared to patients with single VSD, despite having zero percent incidence of postoperative residual defect or ventricular dysfunction. However, we were able to extubate early 5 (41.6%) of the 12 patients with multiple VSDs. We feel that, although presence of multiple VSDs increases the risk of prolonged ventilation, it should not be taken as a contraindication to early extubation. Carefully selected patients with multiple VSDs can still be extubated early.

In our study, 9 (6.7%) patients had trisomy 21. Seven out of 9 patients had delayed extubation, however ACC and CPB time were comparable in patients with or without trisomy 21 (29.3±12.4 vs. 29.2±12.3, P=0.98 and 48±15.7 vs. 47.9±15.6, P=0.98 respectively). Of these 9 patients, none developed LCOS postoperatively. Our results are in congruence with Mittnacht et al.[20]. Studies have found that patients with trisomy 21 are at high risk for atelectasis and pneumonia[20,21]. We could not find any reason for prolonged intubation in these patients in our study.

LCOS was another significant risk factor for delayed extubation in our study. Shi et al.[7], in their retrospective review of 172 infants operated for cardiac surgery, found that LCOS is an independent risk factor for prolonged ventilation and increased mortality. In our study, patients with LCOS had significantly increased duration of ventilation (45.5±57.0 hrs) as compared to patients without LCOS (8.15±7.91 hrs). Studies have also found that positive pressure ventilation is helpful in patients with LCOS by decreasing work of breathing, improving systemic oxygen delivery and by improving cardiac performance. Thus, positive pressure ventilation act as an important hemodynamic support in postoperative systolic ventricular dysfunction[20,23]. Studies have also shown that greater inotropic score (IS) and VIS are significantly associated with delayed extubation and extubation failure[1,18,21,23,24] due to associated hemodynamic instability[16]. Our results are comparable to studies in literature.

Various studies have found age, ACC time and CPB time as independent risk factors for delayed extubation[1,8,26]; however, in our study, age, weight, sex, ACC time, CPB time, size of VSD, preoperative pulmonary hypertension and presence of malnutrition were not significant risk factor for delayed extubation. The possible mechanism given for these were mainly respiratory complications leading to delayed extubation. Literature has shown that CPB time > 150 minutes has been found to be a significant risk factor for delayed extubation[1], but in our study maximum CPB time was only 98 minutes, so the chances of pump related respiratory complications were lower. In their study, age < 6 months was strongly associated with delayed extubation, which was not the case in our study[1].

Many studies have also found young age as an independent risk factor for delayed extubation after paediatric cardiac surgery[18,19]. The reasons cited for this are poor fatigue resistance and endurance of respiratory muscles and immature respiratory centre with poor response to hypoxia and hypercarbia[18,19]. Many other factors responsible for delayed extubation are low body weight, malnutrition, frequent infections and depressed immunity[10,20,25,26]. However, most of recent studies, including ours, have failed to find age related risk factors significant for delayed extubation[2,27]. Mittnacht et al.[20] in their study extubated patients as young as 2 months. The authors found that other risk factors, in association with young age, increased the risk of delayed extubation rather than age alone. Moreover, authors commented that it is the resistance of anaesthetist and intensivist rather than age of the patient, which is responsible for delay in extubation in young patients.

Earlier, preoperative PAH was considered a major limiting factor for early extubation[8,21,28] due to risk of pulmonary hypertensive crisis. However, recent studies have found early extubation to be helpful in these patients by reduced airway irritation and ventilator-associated complications, such as laryngotracheal trauma, pulmonary hypertensive crisis during endotracheal tube suctioning, mucous plugging of endotracheal tubes, barotrauma secondary to positive airway pressure ventilation, ventilator-associated pulmonary infections and atelectasis[29-31]. Herein, we also did not find preoperative PAH as a risk factor for delayed extubation, comparable to study by Vida et al.[29].

We found that early extubation translates into significantly reduced ICU stay and hospital stay without increasing the risk of reintubation or mortality, similar to results of various studies [3-10]. This not only helps in early mobilisation of the patient and reduces parental anxiety, but also reduces the cost of patient care and provides better utilisation of limited hospital resources.

We believe that the most important determinant for successful early extubation is the approach to all the patients as potential candidates for early extubation and then to optimize the perioperative events to achieve this goal. When treated in this manner, even neonates and young infants operated for VSD closure can be successfully extubated early.


Every child with VSD closure is a potential candidate of early extubation. Early extubation after VSD closure is successful in the majority of infants and small children without increasing the risk of reintubation or mortality. The strongest independent risk factors delayed extubation are trisomy 21, LCOS, multiple VSDs and high VIS.


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Article received on february 14, 2017.

Article accepted on april 26, 2017.

No financial support.
No conflict of interest.

Authors' roles & responsibilities

DP Substantial contributions to the conception or design of the work; acquisition, analysis, or interpretation of data for the work; final approval of the version to be published

KL Revising the work critically for important intellectual content; final approval of the version to be published

PG Substantial contributions to the conception or design of the work; acquisition, analysis, or interpretation of data for the work; drafting the work or revising it critically for important intellectual content; final approval of the version to be published

KP Acquisition, analysis, or interpretation of data for the work; drafting the work or revising it critically for important intellectual content; final approval of the version to be published

RS Substantial contributions to the conception or design of the work; final approval of the version to be publisheda

JS Revising the work critically for important intellectual content; final approval of the version to be published

JP Analysis, or interpretation of data for the work; final approval of the version to be published

HP Interpretation of data for the work; final approval of the version to be published

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