Necrotizing Soft Tissue Infection Clinical Trial
Official title:
Biomarkers in Necrotizing Soft Tissue Infections - Aspects of the Innate Immune Response
The purpose of this study is to investigate the immune response in patients with necrotizing soft tissue infections (NSTI). The investigation will focus on inflammatory and vasoactive biomarkers as prognostic markers of severity and mortality at admission to Rigshospitalet and the following 3 days
Necrotizing soft tissue infection (NSTI) is a complex, multi-factorial disease with diverse
microbiological etiology and varying co-morbidities. The rapidly spreading infection may
cause extensive soft tissue damage, limb loss, and multiple organ failure. The incidence of
NSTIs has increased over the past years and the fatality rates are still high despite
increased focus on these patients (20-30%). The extensive inflammatory response is thought
to be a main course of death. However, it is unknown which biomarkers that are responsible
for the deleterious effects and how these molecular mediators are modulated during the
infection and treatment regimes. Thus, there is a need for novel insight into the immune
system disturbances in order to improve outcome of NSTIs.
Location: Copenhagen University Hospital, Rigshospitalet, Denmark.
Design: Observational cohort study.
Cohort: NSTI patients in Denmark.
Controls: 50-100 Patients undergoing elective, orthopedic surgery at Rigshospitalet.
Biomarkers: The investigators will focus on three major groups of biomarkers: Acute-phase
proteins, cytokines and vasoactive biomarkers.
Sample size calculations:
1. Acute-phase proteins: The investigators expect a mean PTX3-concentration at admission
at 120 nmol/L in patients without septic shock and a mean PTX3-concentration at 210
nmol/L in patients with septic shock. With an estimated standard deviation at 100
nmol/L, the inclusion of 52 patients will be able to detect a significant difference
with a statistical power of 90% at a 5% significance level. Since the groups are
unequal the investigators will need to include 82 patients (N'=52(1+4)^2/4*4).
2. Cytokines: In a pilot study with seven NSTI patients, the investigators found a minimal
clinically relevant difference in IL-6 concentration in NSTI patients with LRINEC < 6
and ≥ 6 to be 1050 pg/ml. With an estimated standard deviation at 2000 pg/ml, the
inclusion of 114 patients will be able to detect a significant difference with a
statistical power of 80% at a 5% significance level.
3. Vasoactive proteins: The investigators expect a mean NOx-concentration at admission at
90 μmol/L in patients without septic shock and a mean NOx-concentration at 145 μmol/Lin
patients with septic shock. With an estimated standard deviation at 70 μmol/L, the
inclusion of 70 patients will be able to detect a significant difference with a
statistical power of 90% at a 5% significance level. Since the groups are unequal the
investigators will need to include 110 patients (N'=70(1+4)^2/4*4).
Data: Data will be handled according to the National Data Protection Agency. All original
records (incl. consent forms and questionnaires) will be archived at trial site for 15
years. The National Data Protection Agency has approved the biobank (2007-58-0015, J. nr.
30-1282).
Ethics: The trial will adhere to the Helsinki Declaration and Danish law. The National
Ethics Committee and the Regional Ethics Committee have approved the inclusion of the NSTI
patients (CVK-1211709) and the control patients, including biomarker analyses
(H-2-2014-071).
Biomarker analyses, data extraction and interpretation will be performed once the recruiting
of participants has ended.
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Observational Model: Cohort, Time Perspective: Prospective
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