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Rapid Recognition of Corticosteroid Resistant or Sensitive Sepsis

Not Applicable
Recruiting
Conditions
Sepsis
Interventions
Drug: Administration procedures
Registration Number
NCT04280497
Lead Sponsor
Assistance Publique - Hôpitaux de Paris
Brief Summary

Main objective and primary endpoint: To compare the effect hydrocortisone plus fludrocortisone vs. placebo on a composite of death or persistent organ dysfunction - defined as continued dependency on mechanical ventilation, new renal replacement therapy, or vasopressors - assessed at 90 days on intensive care unit (ICU) adults and having different biological profiles for immune responses and corticosteroids bioactivity.

Secondary objectives and endpoints:

* Mortality and health-related quality of life at 6 months;

* Daily organ function (SOFA score days 1, 2, 3, 4, 7, 10, 14, 28, and 90);

* Daily secondary infections (up to 90 days)

* Daily blood and urinary levels of glucose, sodium and potassium (up to 28 day)

* Daily gastroduodenal bleeding (up to 28 day)

* Daily cognitive function and muscles' strength (days 1 to 28, 90 and 180 days).

Detailed Description

The potential benefits of a lower dose ( ≤ 400 mg of hydrocortisone or equivalent per day), and a longer duration at full dose ( ≥ three days) of treatment, have been investigated in numerous randomized controlled trials over the past three decades. In the past two years, guidelines for clinical practices about corticosteroids use in sepsis have been released. All but one of the guidelines, recommended against the use of corticosteroids in sepsis, except in patients with septic shock and poorly responsive to fluid replacement and vasopressor therapy. Some guidelines suggested that corticosteroids should be given as a continuous infusion rather than intermittent boluses.

Corticosteroids survival benefit is not affected by age, gender, disease severity, type of infection, source of infection, or type of pathogens. There is currently no diagnostic test for CS sensitivity/resistance in sepsis. The scientific community is competing to identify markers delineating between patients who draw survival benefit from corticosteroids (CS-sensitive sepsis) and those who may be harmed (CS-resistant sepsis). In sepsis, the deregulated response may result in systemic inflammation and organs damage, or immune paresis and secondary infections. Obviously, patients with systemic inflammation may benefit from CS whereas those with immune paresis may deteriorate. The study team had have looked for an interaction between survival in response to corticosteroids and the presence of CIRCI according to the ACTH test results (cortisol increment of less than 9µg/dL). The benefits from corticosteroids were more important in patients with CIRCI in the Ger-Inf-05 trial but not in the APROCCHS trial. Thus, current sepsis guidelines suggest that the ACTH test may not reliably guide the use of corticosteroids. Indeed, this test provides information neither on corticosteroids bioactivity nor on patient's immune status, when this information should precede any corticotherapy. Recent studies suggested that a transcriptomic signature based on 100 genes may identify a subset of paediatric sepsis that had increased risk of death when exposed to corticosteroids. Another study found transcriptomic based sepsis response signatures (SRS) associated with immune paresis (SRS1) or with systemic inflammation (SRS 2). In this study, patients with a SRS 2 transcriptomic signature had significantly higher mortality when treated with hydrocortisone. Thus, we have started exploring the mechanisms of sensitivity/resistance to corticosteroids in sepsis, namely by investigating endocan, as a surrogate of patient's inflammatory status, and GILZ expression as a marker of corticosteroids bioactivity.

This is a new multicentre concealed-allocation multi-arms, parallel-group, adaptive blinded randomized controlled trial. The overall objective of the trial is to determine whether different signatures of immune status and/or corticosteroids biological activity influence the responses to hydrocortisone plus fludrocortisone of adults with sepsis. To remain pragmatic, this trial has broad eligibility criteria and includes all patients admitted to the ICU with a primary diagnosis of sepsis. Patients will be randomly assigned to hydrocortisone plus fludrocortisone or placebo for 7 days, targeting 1800 patients with full follow-up up to 6 months.

Recruitment & Eligibility

Status
RECRUITING
Sex
All
Target Recruitment
1800
Inclusion Criteria

  1. Patient ≥18 years old;

  2. Admitted to ICU with proven or suspected infection as the main diagnosis;

  3. Community acquired pneumonia related sepsis or vasopressors dependency (norepinephrine, epinephrine, vasopressin, dopamine, phenylephrine) or septic shock (vasopressor to maintain mean blood pressure of at least 65 mmHg and lactate levels above 2 mmol/l) or acute respiratory distress syndrome (ARDS: a- acute onset, i.e. within one week of an apparent clinical insult and with progression of respiratory syndrome, b- bilateral opacities on chest imaging not explained by other pulmonary pathologies, e.g. pleural effusion, atelectasis, nodules etc, c- no evidence for heart failure or volume overload, d- PaO2/FiO2 ≤ 300 mm Hg, - PEEP ≥ 5 cm H2O;

  4. Patients who have been tested for one or more RECORDS specific biomarkers:

    1. CIRCI
    2. Endocan
    3. GILZ
    4. DUSP-1
    5. MDW
    6. lymphopenia
    7. Transcriptomic SRS2
    8. Endotype B
    9. PCR COVID-19
    10. PCR Influenza
    11. PCR other respiratory virus
    12. Cutaneous vasoconstrictor response to glucocorticoids

  5. Patient who has signed an informed and written consent whevener he/she is able of consent, if not, if not ascent from his/her representant whenever he/she is present at time of screening for inclusion;

  6. Patient affiliated to a social security system or to an universal health coverage (Couverture Maladie Universelle (CMU) in France;

  7. Patient under guardianship or curatorship will be included;

  8. Patient in case of simple emergency (legal definition) will be included;

  9. Patients managed with covid 19 and having biological samples available.

Exclusion Criteria
  1. Pregnancy;
  2. Expected death or withdrawal of life-sustaining treatments within 48 hours;
  3. Previously enrolled in this study
  4. Formal indication for corticosteroids according to most recent international guidelines
  5. Vaccination with live virus within past 6 months
  6. Hypersensitivity to hydrocortisone or fludrocortisone or (microsined betamethasone dipropionate*) or any of their excipients (spc)
  7. Women of childbearing potential not using contraception
  8. Nursing women * For patients included in this stratum, if applicable, do not apply the cream to an infected or ulcerated area

Study & Design

Study Type
INTERVENTIONAL
Study Design
PARALLEL
Arm && Interventions
GroupInterventionDescription
Biomarker CIRCI neg: Corticosteroid armAdministration proceduresHydrocortisone plus fludrocortisone as treatment: hydrocortisone hemisuccinate and 9 alpha fludrocortisone as experimental treatment.
Biomarker CIRCI neg: Placebo armAdministration proceduresPlacebo: hydrocortisone placebo and 9 alpha fludrocortisone placebo as placebo treatment.
Biomarker endocan: Corticosteroid armAdministration proceduresHydrocortisone plus fludrocortisone as treatment: hydrocortisone hemisuccinate and 9 alpha fludrocortisone as experimental treatment.
Biomarker endocan: Placebo armAdministration proceduresPlacebo: hydrocortisone placebo and 9 alpha fludrocortisone placebo as placebo treatment.
Biomarker GILZ: Corticosteroid armAdministration proceduresHydrocortisone plus fludrocortisone as treatment: hydrocortisone hemisuccinate and 9 alpha fludrocortisone as experimental treatment.
Biomarker GILZ: Placebo armAdministration proceduresPlacebo: hydrocortisone placebo and 9 alpha fludrocortisone placebo as placebo treatment.
Biomarker CPD: Corticosteroid armAdministration proceduresHydrocortisone plus fludrocortisone as treatment: hydrocortisone hemisuccinate and 9 alpha fludrocortisone as experimental treatment.
Biomarker CPD: Placebo armAdministration proceduresPlacebo: hydrocortisone placebo and 9 alpha fludrocortisone placebo as placebo treatment.
Biomarker Transcriptomic SRS: Corticosteroid armAdministration proceduresHydrocortisone plus fludrocortisone as treatment: hydrocortisone hemisuccinate and 9 alpha fludrocortisone as experimental treatment.
Biomarker Transcriptomic SRS: Placebo armAdministration proceduresPlacebo: hydrocortisone placebo and 9 alpha fludrocortisone placebo as placebo treatment.
Biomarker Endotype B: Corticosteroid armAdministration proceduresHydrocortisone plus fludrocortisone as treatment: hydrocortisone hemisuccinate and 9 alpha fludrocortisone as experimental treatment.
Biomarker Endotype B: Placebo armAdministration proceduresPlacebo: hydrocortisone placebo and 9 alpha fludrocortisone placebo as placebo treatment.
Primary Outcome Measures
NameTimeMethod
3-month mortalityDaily up to 3 months

Patient's vital status.

Persistent organ dysfunctionAt baseline, 1 month and 3 months

Persistent organ dysfunction (defined as continued dependency on mechanical ventilation, renal replacement therapy, or vasopressors) and with SOFA score ≤6 up to 90 days.

Secondary Outcome Measures
NameTimeMethod
ICU and hospital length of staythrough study completion, an average of 6 month
Rate of re-admission to the ICU during the 180 days after randomizationthrough study completion, an average of 6 month
Vasopressor free daysthrough study completion, an average of 6 month

defined as the number of days with permanent hemodynamic stability in the absence of any vasopressor agent, norepinephrine, phenylephrine, epinephrine, dopamine, vasopressine or its analogs, and soever. When a patient will die on vasopressor therapy, the corresponding vasopressor free day will be 0.

HRQoL in 6-month survivors assessed by the EuroQol-5D (EQ-5D)at 1, 28, 90 day and 6 months

This questionnaire is a standardised measure of health status developed to provide a simple, generic measure of health for clinical and economic appraisal. It is made up for two components; health state description and evaluation. The health status is measured in terms of five dimensions; mobility, self-care, usual activities, pain/discomfort, and anxiety/depression. In evaluation part, the respondents evaluate their overall health status using the visual analogue scale.

Safety endpoints: proportion of patients affected by any serious adverse eventsup to 90 days

Serious adverse events associated with corticosteroids, among the following: hospital-acquired infections, hyperglycemia, hypernatremia, neurological disorders (coma, stroke or muscle weakness, as defined below) during the 90 days after randomization.

Comaup to 90 days

Coma will be defined as a Glasgow coma score \< 8

Number of episodes of hyperglycemiadaily during ICU stay or up to 90 days

Number of episodes of hyperglycemia (blood glucose levels \>150mg/dl) during ICU stay (or up to day 90, whichever occurs first)

Mechanical ventilation free daysthrough study completion, an average of 6 month

defined as the number of days with permanent appropriate oxygenation while the patients is extubated and breathing spontaneously, i.e. no need for non invasive ventilation, high flow oxygen or CPAP. Other uses of non-invasive ventilation (e.g., chronic night-time use for chronic obstructive pulmonary disease) are not counted. When a patient will die on mechanical ventilation or will be discharge home on mechanical ventilation, the corresponding mechanical ventilation free day will be 0.

Number of episodes of hypernatremiadaily during ICU stay or up to day 90

Number of episodes of hypernatremia (serum sodium \> 145 mmol/L) during ICU stay (or up to day 90, whichever occurs first)

Glasgow coma scale at ICU and hospital dischargeat ICU discharge and hospital discharge

Glasgow coma scale at ICU and hospital discharge

Number of patients with an episode of strokedaily during ICU stay or up to day 90

Number of patients with an episode of stroke (medical diagnosis as registered in the medical file) during ICU stay (or up to day 90, whichever occurs first)

Gastroduodenal bleedingdaily during ICU stay or up to day 90

Gastroduodenal bleeding requiring transfusion or hemostatic treatment during ICU stay (or up to day 90, whichever occurs first)

Adult cognitive function scoreat 1, 28, 90 day and 6 months

Neurological cognitive dysfunction defined as by low score on the PROMIS (Adult cognitive function score).

PROMIS (Patient-Reported Outcomes Measurement Information System): for assessment of fatigue, ability to partake in social activities, physical function, emotional distress, depression, anxiety and cognitive function.

Mortality at 7, 14, 28 day and 6 monthsat 7, 14, 28 day and 6 months

Patient's vital status.

Organ dysfunction free daysthrough study completion, an average of 6 month

Organ function (including renal function) will be assessed by the SOFA score (Vincent 1996). Organ dysfunction will be defined by a SOFA score of \> 6 (Annane 2018). Organ dysfunction free days are defined by the number of days with os total SOFA score of 6 or less. When a patient will die on vasopressor therapy, the corresponding vasopressor free day will be 0.

Proportion of patients with a decision to withhold and/or withdraw active treatmentsthrough study completion, an average of 6 month
Neurologic sequelaeup to 90 days

Neurologic sequelae will be assessed according to the score on the Muscular Disability Rating Scale (MDRS), with a score of 1 indicating no deficit, 2 minor deficit with no functional disability, 3 distal motor deficit, 4 mild-to-moderate proximal motor deficit, and 5 severe proximal motor deficit.

Proportion of patients affected by hospital-acquired infectionsup to 90 days

Proportion of patients affected by hospital-acquired infections (CTINILS. Définition des infections associées aux soins. 2007, (document in french)).

Trial Locations

Locations (1)

Department of medical and surgical Intensive Care Unit, Raymond Poincaré Hospital - APHP

🇫🇷

Garches, Hauts-de-Seine, France

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