Necrotizing Soft Tissue Infection Clinical Trial
Official title:
Immunoglobulin for Necrotizing Soft Tissue Infections: a Randomised Controlled Trial
The purpose of this study is to estimate the effect of intravenous polyspecific immunoglobulin G (IVIG) compared with placebo (saline) on the patient-reported outcome measure Physical Component Summary Score (PCS) of the SF-36 in patients with necrotizing soft tissue infections (NSTI).
Patients with necrotizing soft tissue infections (NSTI) receive intravenous polyspecific
immunoglobulin G (IVIG) as part of the standard treatment at Rigshospitalet. The current
evidence available does not support neither the use of IVIG, nor omitting it, as adjuvant
treatment of NSTI. With this trial the investigators will estimate the effects of IVIG on a
patient-reported outcome and other important outcomes in patients with NSTI
Design A randomized, double-blinded, clinical trial where patients are randomly assigned 1:1
to receive either IVIG or an equal volume of 0.9% saline.
Location A single centre trial conducted at Dept. of Intensive Care 4131, Copenhagen
University Hospital, Rigshospitalet.
Randomisation Randomisation will be stratified according to primary presentation of NSTI on
the extremities/head/neck (yes/no) as streptococci mainly affect these anatomical sites. Two
randomisation lists, with varying block size, are generated. Two separate boxes contain
sequentially numbered, opaque, sealed envelopes (SNOSE). Two people independent of the trial
will generate the envelopes following the randomisation lists and will document that the
envelopes are concordant with the randomisation lists. Staff at trial site will have access
to the boxes around the clock, and will draw an envelope containing a patient randomisation-
and medicine log document assigned either "Privigen" or "Saline" from one of the two boxes.
Intervention Trial medicine is given when the patient arrives at the ICU and the following
two consecutive days. Alternatively, the first dose of trial medicine will be given in the
operating theatre.The trial medicine will consist of either IVIG 25 g/day (250 ml)
(Privigen, CSL Behring) or an equal volume of 0.9% saline. The dosage of IVIG is 25g/day for
three consecutive days for all patients, which is according to the clinical protocol at
Rigshospitalet. The treatment will be given according to the clinical protocol for Privigen
at Rigshospitalet. The treating clinicians will decide all other interventions.
Blinding The trial medicine will be prepared in the ICU at the time of arrival of the
patient and the following two consecutive days by an ICU nurse not otherwise involved in the
care of the trial patient and is supervised by another staff member who as well is not
involved in the care of the patient. Privigen has a slight yellowish appearance whereas
saline is clear. Furthermore, Privigen is produced in bottles of 50 and 100 ml,
respectively. A bottle of Privigen will be packed with a bag of saline, containing a
corresponding number of millilitres, in a black plastic bag and sealed with a plastic strip.
An orange, transparent infusion set (B. Braun, ref. 8700127SP) is inserted into either the
Privigen bottle or the bag containing saline, dependent on whether the patient has been
allocated to active treatment or placebo. The orange colour masks the fluid colour while
allowing air bubbles to be seen. A piece of non-transparent tape will mask the drip chamber
making it impossible to see the frothing of Privigen. For each of the three dosages of trial
medicine, three bags are prepared, containing 100 ml, 100 ml and 50 ml respectively. The bag
will be marked with an etiquette containing the patient number. If unblinding is necessary,
this is easily done by looking in the envelope with the same patient number.
Medicine score The trial medicine batch number will be noted on the patient randomisation-
and medicine log document by the ICU nurse preparing the trial medicine. The attending
physician will prescribe "trial medicine" in the electronic medication file (CIS 3.9.1,
Daintel).
Subgroup Analysis Presumed Streptococcal Infection A subgroup analysis will be performed on
patients with primary presentation of NSTI on the extremities, neck or head as these are
more likely to be streptococcal infections, in which the effects of IVIG may be different.
Data Registration Data will be entered into the electronically, web-based case report form
(eCRF) from patient notes by trial personnel. The eCRF is specifically designed for this
purpose.
Safety
Patients will be withdrawn from the trial protocol if the following occurs:
- SARs or SUSARs Patients withdrawn from the trial for the above mentioned reasons will
receive the standard protocol treatment for NSTI with the exception of IVIG.
During the trial, Sponsor will send yearly reports on the occurrence of SARs to the Danish
Health and Medicines Authority and Regional Ethics Committee.
Suspected Unexpected Serious Adverse Reactions Suspected unexpected serious adverse
reactions (SUSARs) will be defined as serious adverse reactions not described in the summary
of product characteristics (SPC) for Privigen (no serious adverse reactions are described
for 0.9% saline). Sponsor will report any SUSARs within 7 days to the Danish Health and
Medicines Authority via Eudravigilance Clinical Trials Module, to the Regional Ethics
Committee and to CSL Behring. During the trial, investigator will send yearly reports on the
occurrence of SUSARs to the Danish Health and Medicines Authority and the Regional Ethics
Committees.
Adverse Events and Serious Adverse Events Adverse events (AEs) and serious adverse events
(SAEs) will not be recorded as an entity because the majority of ICU patients will
experience several SAEs during their critical illness. In addition, most SAEs will be
captured in the secondary outcome measures (SOFA scores and bleeding).
Termination of Trial The trial will be terminated prematurely in the case that new, definite
information regarding the use of IVIG in patients with NSTI arises.
Sample Size Estimation 50 subjects in each group are needed to detect a difference of 7
points in PCS of SF-36 based on an expected score of 42 (SD 11) in the control group (data
from our own follow-up studies), for a power of 80% and a two-tailed significance level of
0.05, and an expected 1-year mortality rate of 20%.
Statistical Methods Analysis will be by intention-to-treat comparing PCS of SF-36 in the two
groups after six months by chi-squared test and multiple logistic regression analysis using
unadjusted analyses and analyses adjusted for patient variables (SAPS II and SOFA score in
the 24 h prior to randomisation).
Patients Included In Final Statistical Analysis Patients who are withdrawn from the trial
protocol will be followed up and analysed as the remaining patients. Patients who are
transferred to another ICU will be followed up for the primary outcome measure. Patients who
are withdrawn will not be replaced by new patients, with the exception of the specific case,
where the patient demands deletion of all registered data.
Accountability Procedure for Missing Data Imputation will be used if missingness >5%.
Interim Analysis An interim analysis will not be performed as analyses of a sample size
below the planned 100 patients are less meaningful for those outcomes that are of relevance
(mortality and SARs).
Monitoring
We will perform Good Clinical Practice (GCP)-monitoring according to a predefined monitoring
plan including the following issues:
- Initiation visit
- For all patients: Documented informed consent
- Inclusion and exclusion criteria
- Documented delivery or non-delivery in the eCRF of the intervention according to the
protocol compared with source data being patients' hospital records
- Termination visit: Primary outcome
Data Handling and Record Keeping Data will be handled according to the National Data
Protection Agency, and is protected by the national law "Loven om behandling af
personoplysninger" and "Sundhedsloven". All original records (incl. consent forms, eCRFs,
and relevant correspondences) will be archived at trial site for 15 years. The clean
electronic trial database file will be delivered to the Danish Data Archive and maintained
for 15 years and anonymised if requested by the authorities.
Quality Control and Quality Assurance The subinvestigator will be responsible for preparing
the research nurses and other trial site personnel before the initiation of the trial. This
education will be continuously documented.
Monitoring of the Intervention Groups Day-to-day monitoring of the eCRF will be done by
persons delegated to this specific task.
Ethics The trial will adhere to the Helsinki Declaration and Danish law. Inclusion will
start after approval by the Regional Ethics Committee, the Danish Health and Medicines
Authority and the National Data Protection Agency (via the Joint Notification System of The
Capital Region of Denmark - Region Hovedstaden) and trial registration at
www.clinicaltrials.gov.
;
Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Caregiver, Investigator, Outcomes Assessor), Primary Purpose: Treatment
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