Sepsis Clinical Trial
Official title:
Clinical Protocol Validation to Identify Prognostic Markers for Critical Care Pediatric Patients
The purpose of this study is to monitor the respiratory, metabolic and nutritional status of critically ill pediatric patients undergoing mechanical ventilation and to correlate the clinical and physiopathological findings with inflammatory activity measurements in order to identify prognostic biomarkers.
Background: Acute Respiratory Distress Syndrome (ARDS) is a frequent cause of respiratory
failure in the pediatric intensive care unit (ICU). Bedside respiratory and metabolic
monitoring has reduced both morbidity and mortality of children with ARDS in the ICU, and
allowed precise evaluation of the gravity of ARDS in individual patients. Recent advances
indicate that some ARDS patients present specific, genetically determined profiles of
cytokine production, but it is unclear how these relate to systemic inflammation and the
gravity of ARDS. It is necessary to define the correlation between genotype, systemic
inflammation and prognosis in this group of patients, ir order to define whether they should
be targeted for more aggressive anti-inflammatory and immunomodulatory therapy.
Objectives: 1) To evaluate metabolic expenditure,bioelectrical impedance (BIA) and
respiratory function in critically ill children undergoing mechanical ventilation. 2) To
correlate the metabolic and respiratory parameters with duration of mechanical ventilation,
weaning, nutritional status,Phase angle (PA) of BIA, PRISMI and PIM 2 scores in the same
children.3) To determine the presence of polymorphisms in the genes for TNF-alfa (- 308 and
-863), IL-1ra, IL-6, MIF, LTalfa, il-10 and CD14 in the same children. 4) To define
functional parameters of systemic inflammation, including plasma levels of TNF-alfa, IL-1ra,
IL-6 and translocation of NF-kappa B in the same children. 5) To correlate genomic and
immunological data with PRISM I and PIM 2 scores, PA and mortality.
Methodology: 1) Study Design: A cohort of patients undergoing mechanical ventilation will be
submitted to metabolic and respiratory monitoring, and to monitoring of systemic
inflammation by measurement of plasma cytokines and NF-kB translocation in peripheral blood
leukocytes; a cross-sectional study of cytokine gene polymorphisms will be carried out int
hte same population. 2)Subjects: 1000 children, aged 1 mo to 17 yr. Group A: 200 children
with ARDS; Group B: 400 children with respiratory failure unrelated to ARDS; Group C
(controls): 400 children undergoing preoperatory exams at surgical ward for elective
surgery. 3) Methods: Metabolic monitoring: determination of VCO2, VO2, RQ, EEM through
indirect calorimetry. Bioelectrical impedance: determination of resistance, reactance and
phase angle. Respiratory monitoring: determination of respiratory parameters through
capnography, pulse oxymetry, and assessment of respiratory mechanics. Genomic analysis:
restriction site mapping and allele-specific amplification by PCR. Immunological evaluation:
measurement of plasma cytokines by luminex multiple essays and analysis of NF-kB activation.
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Observational Model: Cohort, Time Perspective: Prospective
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