Lipopolysaccharide Adsorption at Septic Shock

Not Applicable

Completed

• Conditions: Septic Shock
• Interventions: Device: Efferon LPS hemoperfusion

• Registration Number: NCT04827407
• Lead Sponsor: Efferon JSC

Brief Summary

Sepsis is a global healthcare burden sepsis, it reaches 20-30 million cases annually (WHO data). Numerous studies have shown that extracorporeal hemoperfusion therapies that eliminate endotoxin and\\or excess of cytokines improve treatment outcomes in patients with septic shock. The main purpose of the study is to obtain new data on the efficacy and safety of the Efferon LPS device in extracorporeal therapy in patients with abdominal sepsis complicated by septic shock.

Detailed Description

Sepsis is a global healthcare burden sepsis, it reaches 20-30 million cases annually (WHO data). A two-stage trial by Rudnov et al. using one-day data from 62 centres in 29 subjects of the Russian Federation showed that one third of the patients admitted to the ICU were patients with infection, one fifth of them developed septic shock, the proportion of hospital sepsis was 46.6%, and fatal outcome occurred in 30.4% of patients with infection. Despite apparent advances in intensive care, the prognosis of patients with endotoxaemia and septic shock remains poor.

Extracorporeal removal of toxic substances from the bloodstream by adsorbing them onto a porous material may provide clear clinical benefits. Extracorporeal blood adsorption method can be a good complement or substitute for the classical methods of haemofiltration and haemodialysis if the diffusion or convection of toxic substances through the membrane is not efficient enough. Since the method was first proposed by Muirhead and Reid in 1948, it has developed considerably.

Endotoxin (lipopolysaccharide), one of the most potent mediators of sepsis, is found in high concentrations in about 50% of patients with septic shock. The use of extracorporeal sorption techniques that eliminate endotoxin has been shown in numerous trials to improve outcomes in patients with septic shock.

Efferon LPS (Efferon JSC, Moscow, Russia) is a single-use therapeutic device for extracorporeal blood purification using direct hemoperfusion. Detoxification is carried out by selective adsorption of lipopolysaccharides (bacterial endotoxins) and non-selective removal of cytokines by internal porous structure. It is a cylindrical polycarbonate casing filled with spherical granules of LPS-selective polymeric adsorbent mesoporous beads and isotonic sodium chloride solution. The device is registered in Russia as a medical device RZN 2019/8886.

Study Timeline

• Study Start: 2021-03-23
• Study First Submitted: 2021-03-30
• Study First Submitted QC: 2021-03-30
• Study First Posted: 2021-04-01
• Primary Completion: 2022-03-30
• Study Completion: 2022-08-30
• Status Verified: 2024-06
• Last Update Submitted: 2024-06-24
• Last Update Posted: 2024-06-25

Recruitment & Eligibility

• Status: COMPLETED
• Sex: All
• Target Recruitment: 58

Inclusion Criteria

• Age ≥18 years

• Established diagnosis of Gram-negative septic shock according to SEPSIS-3 criteria

• The immediate post-operative period (no more than 24 hours after surgery)

• Hypotension requiring vasopressor support: the need for at least one of the vasopressors listed below at the dose listed below for at least 2 hours continuously and not more than 12 hours.

  • Norepinephrine> 0.05 µg/kg/min
  • Dopamine> 10 µg/kg/min
  • Phenylephrine> 0.4 µg/kg/min
  • Adrenaline > 0.05 µg/kg/min
  • Vasopressin> 0.03 units/min Vasopressin (any dose) in combination with another vasopressor listed above

• The patient must have received intravenous infusion therapy of at least 30 ml/kg administered within 24 hours of inclusion.

• The patient's condition allows therapy with the Efferon LPS device for at least 4 hours.

Exclusion Criteria

Lack of adequate antimicrobial chemotherapy

• Identifying the criteria for non-inclusion;
• A patient may voluntarily withdraw from a trial at any time after giving informed consent and before the trial is completed. The investigator may also withdraw a participant from the trial at any time at his or her discretion and for any of the following reasons:
• Reasons for a participant's withdrawal from the trial will be recorded and may include, amongst others, the following
• Withdrawal of consent to participate in the trial by the participant.
• The development of an adverse event, including a serious one; individual intolerance to the investigational product, hypersensitivity to the components of the product due to which further participation in the trial is not possible.
• Continued participation in the trial is not, in the researcher's opinion, in the participant's health interests.
• The presence of deviations from the plan which, in the opinion of the Sponsor and Investigator, require the withdrawal of the participant from the trial.
• A positive pregnancy test result at any time during the test.
• When any participant withdraws from a trial, the reason for the withdrawal should be documented.

Study & Design

• Study Type: INTERVENTIONAL
• Study Design: PARALLEL

Arm && Interventions

Group	Intervention	Description
Basic therapy + Efferon LPS	Efferon LPS hemoperfusion	Basic therapy is the institution's routine practice for treating patients with septic shock against a background of abdominal sepsis plus extracorporeal hemoperfusion therapy (Efferon LPS)

Primary Outcome Measures

Name	Time	Method
Effect of the Efferon LPS hemoperfusion in extracorporeal therapy in patients with abdominal sepsis complicated by septic shock	1-14 days	The time (number of days) from randomisation to the earliest time that the 'resolution of septic shock' event is achieved. Event criteria: 1) end of vasopressor support (persistence of effect - for 4 hours) and 2) investigator/trained staff rating the trial as 'resolved' when assessed from baseline to day 14 or hospital discharge (if discharge occurs earlier than day 14).

Secondary Outcome Measures

Name	Time	Method
Effect of the Efferon LPS hemoperfusion on systemic haemodynamic parameters after the start of use in patients with abdominal sepsis complicated by septic shock	1-72 hours	Sats every 6 hours ± 1 hour from the start of hemoperfusion (hour 0) to 72 hours. The time (number of days) from randomisation to the end of vasopressor support within 72 x hours or hospital discharge (if earlier than 72 hours). Maximum dose of vasopressors within 24 hours and 72 hours of the start of hemoperfusion.
Effect of the Efferon LPS hemoperfusion on pulmonary oxygen metabolism function in patients with abdominal sepsis complicated by septic shock	1-72 hours	Value of oxygenation index (Pa02 / Fi02 (Pa) every 24 hours ± 1 hour from the start of hemoperfusion (hour 0) to 72 hours
Effect of the Efferon LPS hemoperfusion on the length of stay in the ICU of patients with abdominal sepsis complicated by septic shock	1-14 days	The time (number of days) from randomisation to transfer from the ORIT within 14 days or hospital discharge or transfer from the ORIT (if occurring earlier than day 14).

Trial Locations

Locations (4)

N.I. Pirogov City Clinical Hospital No. 1; 🇷🇺 Moscow, Russian Federation

S.S. Yudin City Clinical Hospital; 🇷🇺 Moscow, Russian Federation

N.V. Sklifosovsky Moscow Research Institute of Emergency; 🇷🇺 Moscow, Russian Federation

V.P. Demikhov City Clinical Hospital No. 68; 🇷🇺 Moscow, Russian Federation