Trials / Active Not Recruiting
Active Not RecruitingNCT04695119
Sepsis in the ICU-II
Sepsis in the Intensive Care Unit-II
- Status
- Active Not Recruiting
- Phase
- —
- Study type
- Observational
- Enrollment
- 379 (actual)
- Sponsor
- Linkoeping University · Other Government
- Sex
- All
- Age
- 18 Years
- Healthy volunteers
- Not accepted
Summary
Sepsis-induced cardiac dysfunction (SIMD) is a well-known phenomenon yet its diagnosis remains elusive with no accepted definition, or defining pathophysiological mechanism associated with this disease. Systolic dysfunction occurs in 20-70% of patients, and may be severe, yet does not appear to have any prognostic value for mortality. Diastolic function has also been variably described and seems to be related to short-term mortality. However, the contribution of left ventricular systolic and diastolic dysfunction to mortality in sepsis are still far from clear, with uncertain contribution from previous cardiovascular disease, vasopressor and inotropic drugs and mechanical ventilation. Another poorly investigated area is right ventricular dysfunction. Cor pulmonale occurs in up to 25% of patients with septic shock, and is invariably related to pulmonary haemodynamics and mechanical ventilation, yet very little is known about how this affects prognosis. Finally, although the outcome of disease is a function of multiple parameters, septic cardiomyopathy is most frequently characterized based on individual echocardiographic parameters, without considering their interactions or placing them in the context of biomarkers and clinically available haemodynamic data. Available relevant studies are often monocentric, and many fail to consider the various confounders that influence the clinical outcome in sepsis. Therefore, the diagnostic and prognostic value of combinations of clinical, biochemical and haemodynamic variables remains to be established. Accordingly, the purpose of this study is to identify biomarkers and echocardiographic and haemodynamic signatures characteristic of specific outcomes in SIMD to support the diagnosis and prognosis in SIMD. Specific aims are: 1. To determine the association between left ventricular systolic and diastolic dysfunction, and adverse outcome in SIMD; 2. To determine the association between right ventricular systolic and diastolic dysfunction, and adverse outcome in SIMD; 3. To determine the association between novel biomarkers and adverse outcome in SIMD; 4. To determine the combined value of biomarker, echocardiographic, and haemodynamic variables for predicting adverse outcomes in SIMD; 5. To explore if there are different phenotypes of SIMD using unsupervised machine learning algorithms, and whether they are associated with adverse outcomes. 50 patients will be enrolled in a feasibility study to evaluate the logistical setup for acute echocardiography and biobanking facilities. A further 280 patients will be enrolled with inclusion from peripheral centers once feasibility is confirmed. Note 15 Mar 2026: typing mistake noted in prior text, the sample size was originally for 330 patients (i.e. 50 + 280), not 350 (50 + 300) patients.
Detailed description
UPDATE 26 Feb 2022: A pilot project was completedafter recruitment of 50 patients confirming the feasibility of data collection, study logistics, biomarker assay set-up and frequency of outcomes. Cancellation of non-COVID related research in 2020\&2021 has caused significant delays. Recruitment of patients will continue during 2022\&2023. At the time of writing 70 patients have been recruited across 4 centres. UPDATE 15 Mar 2026: At the steering committee meeting on 12 August 2024, the principal investigator presented population characteristics of the first 49 patients in the feasibility phase and compared them with the subsequent 231 recruited patients. The two cohorts were similar in age and sex, but the later cohort had higher median SAPS II scores, greater use of organ support, and higher ICU and 30-day mortality. Discussions with recruiting sites indicated that the COVID-19 pandemic had substantially changed the case-mix of ICU admissions; nursing staff shortages and bed closures led to admission of more severely ill patients, particularly at the major recruiting site. The steering committee concluded that there was no need to deviate from the original protocol but recommended recruitment of an additional 49 patients to reduce potential heterogeneity in the underlying population. The total target sample size was therefore set at 379 patients. The expanded sample size was approved by the Swedish Ethical Review Authority on 7 Feb 2025.
Conditions
Interventions
| Type | Name | Description |
|---|---|---|
| OTHER | Exposure is septic shock (defined according to Sepsis-III) and standard treatment according to departmental protocols. | Collection of data, biomarker and echocardiography analysis will be centralized and blinded. Assessment of endpoints will be blinded. |
Timeline
- Start date
- 2018-09-17
- Primary completion
- 2026-02-11
- Completion
- 2027-12-31
- First posted
- 2021-01-05
- Last updated
- 2026-03-17
Locations
4 sites across 2 countries: France, Sweden
Source: ClinicalTrials.gov record NCT04695119. Inclusion in this directory is not an endorsement.