Rate, Rhythm or Risk Control for New-onset Supraventricular Arrhythmia During Septic Shock: a Randomized Controlled Trial

Not Applicable

• Conditions: Supraventricular Arrhythmia; Septic Shock
• Interventions: Procedure: Risk control strategy

• Registration Number: NCT04844801
• Lead Sponsor: Assistance Publique - Hôpitaux de Paris

Brief Summary

New-onset supraventricular arrhythmia (NOSVA) is reported in 40 % of patients with septic shock and is associated with hemodynamic alterations and mortality. The lack of consensus regarding best practices for the management of NOSVA in this setting has led to major variations in practice patterns. Observational studies reported three usual strategies: (i) heart rate control (hereafter rate control) with the use of antiarrhythmic drugs, essentially based on low dose of amiodarone, (ii) rhythm control with the use of antiarrhythmic drugs, essentially based on high dose of amiodarone, and electrical cardioversionand (iii) modifiable NOSVA risk factors control (hereafter risk control) without using antiarrhythmic drugs.

Risk control would minimize adverse events of antiarrhythmic drugs. Rhythm control would rapidly improve haemodynamics via restoring diastole and decreasing cardiac metabolic demand, while minimizing exposure to anticoagulation. Rate control, would limit potential adverse events of high dose of amiodarone and of electrical cardioversion (only in patients intubated on mechanical ventilation), while controlling haemodynamics. Therefore, it seems important to compare these three strategies.

Our hypothesis is dual: first, that rate control and rhythm control each improve hemodynamics with in fine a decreased mortality, as compared to a risk control; second, that rhythm control outperforms rate control in this setting.

This is a multicenter, parallel-group, open-label, randomized controlled superiority trial to compare the effectiveness and safety of these three strategies (risk control, rate control and rhythm control) for NOSVA during septic shock.

Detailed Description

All consecutive adult patients admitted to the intensive care unit with NOSVA during septic shock will be included in the presence of inclusion criteria and in the absence of exclusion criteria.

Randomization, performed immediately after the inclusion (Day-1), in 1:1:1 ratio will be stratified on center. Then the patient will receive the randomized strategy: risk control, rate control or rhythm control.

Before inclusion, the informed consent will be proposed to the patient. If the patient is unable to give his/her consent, the informed consent of the next-of-kin will be sought by study investigator. In the case the next-of-kins are unidentified and/or unreachable, an emergency procedure will be applied. Patient consent will be sought as soon as their state of health allows it.

According to clinical guidelines, patients in all groups will receive therapeutic anticoagulation if NOSVA \> 48 hours and in the absence of contraindication. In all groups, recommendations for the management of septic shock will be followed.

After day-7 (or hospital discharge if before J7), NOSVA treatment will be left at the discretion of attending physicians.

Evaluation criteria will be collected at day-2, day-3, day-7 (or at hospital discharge if before day-7), at the day of ICU discharge and at Day-28. If the patient has been discharged before Day-28, the vital status may be obtained by phone call at Day-28.

Study Timeline

• Study First Submitted: 2021-02-26
• Study First Submitted QC: 2021-04-13
• Study First Posted: 2021-04-14
• Study Start: 2021-11-09
• Status Verified: 2022-08
• Last Update Submitted: 2022-08-22
• Last Update Posted: 2022-08-25
• Primary Completion: 2023-12
• Study Completion: 2023-12

Recruitment & Eligibility

• Status: UNKNOWN
• Sex: All
• Target Recruitment: 240

Inclusion Criteria

1. Age >= 18 years

2. Septic shock, defined by the association of the following criteria:

   • Documented or suspected infection, with initiation of antibiotic therapy
   • Initiation of vasopressors (norepinephrine, epinephrine) for at least 1 hour to maintain the MAP > 65 mmHg

3. NOSVA with heart rate ≥ 110 bpm lasting 5 minutes or more

4. Written informed consent (patient, next of skin or emergency situation)

5. Affiliation to a social security system

Exclusion Criteria :

1. Refractory shock defined by a dose of noradrenaline BASE or adrenaline BASE > 1.2 µg/kg/min
2. Cardiac surgery or cardiac transplant in the previous month
3. Aortic or mitral mechanical prosthesis, significant mitral stenosis (mitral surface < 1.5 cm2)
4. Congenital heart disease other than bicuspid aortic valve, atrial defect or patent foramen ovale.
5. History of supraventricular arrhythmia before septic shock
6. NOSVA lasting at most 36 hrs (or 24 hrs with vasopressors)
7. Electrical cardioversion or use of amiodarone, other antiarrhythmic, or drug inducing bradycardia (beta-blockers, bradycardic calcium channel blocker, digitalis, flécaïnamide) in the previous 6 hours before inclusion
8. Contraindication to amiodarone: history of serious adverse event related to amiodarone, history of lung disease related to amiodarone, history of hyperthyroidism related to amiodarone, PR interval > 240 ms, severe sinus node dysfunction with no pacemaker, 2°/ 3° atrioventricular block with no pacemaker, QTc>480 ms, known or treated hyperthyroidism, hypersensitivity to iodine, amiodarone or to any of the excipients, severe hepatocellular insufficiency (prothrombin rate <20%), diffuse Interstitial Lung Disease.
9. Kalemia < 3 mmol/L
10. Pregnant or breast feeding women
11. Moribund patient or death expected from underlying disease during the current admission; Patient deprived of liberty and persons subject to institutional psychiatric care
12. Participation to another interventional trial on septic shock and/or arrhythmic disease

Exclusion Criteria

Not provided

Study & Design

• Study Type: INTERVENTIONAL
• Study Design: PARALLEL

Arm && Interventions

Group	Intervention	Description
Risk control strategy	Risk control strategy	Magnesium sulfate + control of the modifiable NOSVA risk factors

Primary Outcome Measures

Name	Time	Method
all-cause mortality (a hierarchical criterion)	28 days	The duration of septic shock is defined as the time (number of days) from randomization to successful weaning of vasopressors; The Finkelstein-Schoenfeld method is based on the principle that each patient in the clinical trial is compared with every other patient within each stratum in a pairwise manner. The pairwise comparison proceeds in hierarchical fashion, using all-cause mortality, followed by the duration of septic shock when patients cannot be differentiated on the basis of mortality. This method gives a higher importance to all-cause mortality.
the duration of septic shock according to the Finkelstein-Schoenfeld method (a hierarchical criterion).	28 days	The duration of septic shock is defined as the time (number of days) from randomization to successful weaning of vasopressors; The Finkelstein-Schoenfeld method is based on the principle that each patient in the clinical trial is compared with every other patient within each stratum in a pairwise manner. The pairwise comparison proceeds in hierarchical fashion, using all-cause mortality, followed by the duration of septic shock when patients cannot be differentiated on the basis of mortality. This method gives a higher importance to all-cause mortality.

Secondary Outcome Measures

Name	Time	Method
Rhythm efficacy at day-7 (or at discharge or death if before day-7)	up to 7 days	1. Number of patients with sinus rhythm; 2. Number of days alive with sinus rhythm; 3. Number of days alive with NOSVA and heart rate \< 110 bpm; 4. Proportion of patients receiving therapeutic anticoagulation after randomisation
Morbimortality	Day 28	1. Duration of septic shock and Length of stay in intensive care unit and in hospital at day-28; 2. Proportion of patients alive free from vasopressors at day-7 (or at discharge or death if before day-7); 3. Arterial lactate clearance at day-3 defined as the percentage of arterial lactate decrease between lactate at randomisation (day-1) and at day-3.; 4. Proportion of patients alive free from organ dysfunction at day-7 (or at discharge or death if before day-7); 5. All-cause deaths at day-28.
Tolerance at day-7 and day-28	Day 7 and day 28	1. Proportion of patients with at least one arterial thrombotic event including ischemic stroke and non-cerebrovascular arterial thrombotic event; 2. Proportion of patients with at least one major bleeding event according to the International Society of Thrombosis and Haemostasis definition at Day-28; 3. Proportion of patients with at least one serious adverse event related to amiodarone or to magnesium sulfate; and proportion of each type of event; 4. Proportion of patients presenting at least one serious adverse event associated with electrical cardioversion (for patients receiving electrical cardioversion).

Trial Locations

Locations (1)

Service de Médecine Intensive Réanimation-Hôpital Tenon; 🇫🇷 Paris, France