Critically Ill Clinical Trial
Official title:
Randomized Directed Immuno Nutrition by L-arginine for Critically Ill Patients
The main objective of this proof-of-concept study is to demonstrate that the only administration of L-arginine, based on a suspected deficit monitored by nasal nitric oxide measurement, can improve immune functions in critically ill patients at high risk of nosocomial infection.
Background : A meta-analysis has demonstrated the beneficial effect of immuno nutrition in
surgical patients, leading to half reduction of incidence of nosocomial infections (HEYLAND
DK, JAMA ; 2001). This beneficial effect seems to be related to L-arginine content of
formula. In medical intensive care, such an improvement has not been shown, in spite of
similar impairment of immune response, which could be due to a more heterogenous population.
Our hypothesis is that this beneficial effect could be observed in selected patients of
medical intensive care units. L-arginine is a semi-essential amino acid that is the
precursor of nitric oxide (NO) synthesis. NO is involved in immune response regulation and
has antimicrobial properties, notably into airways where it can be measured in exhaled gas.
A decrease in exhaled and nasal NO has been demonstrated in critically ill patients, which
may suggest an impairment of its production.
Objectives : The aim of this study is to evaluate the immune effects of enteral L-arginine
administration in non surgical critically ill patients. These patients will be selected
based on the decrease in nasal NO: directed immuno nutrition. The main objective is to
demonstrate that L-arginine administration, as compared to placebo administration, increases
nasal NO and enhances immune functions (increase in HLA-DR expression on monocytes,
modification of circulating Myeloid-Derived Suppressor Cells (MDSC), decrease in IL-6, IL-17
plasmatic concentrations): stimulation of immune response. The secondary objective is to
demonstrate the safety of L-arginine administration on organ failure and on the incidence of
nosocomial infections.
This is a monocentric therapeutic trial, randomized and double blind: standard enteral
nutrition plus L-arginine (200 mg/kg/d for 5 days from the admission in ICU) versus standard
enteral nutrition plus placebo.
Methods-Patients: Non surgical patients admitted in a single medical intensive care unit,
under mechanical ventilation for an expected duration > 2 days, with decreased
concentrations of nasal NO (< 60 ppb), without severe sepsis or septic shock, will be
enrolled. On admission (before treatment), the severity will be evaluated (SAPS II and SOFA
score) together with an assessment of plasmatic L-arginine, cytokines (IL-6, IL-17), MDSC,
and expression of HLA-DR by monocytes. The same evaluation will be repeated on day 4 (during
treatment) and on day 7 (after treatment). The enrolment of 50 patients is statistically
enough to demonstrate an increased expression of HLA-DR in the L-arginine group as compared
to the placebo group on day 4.
Expected results and perspectives: The aim of this study is to demonstrate the validity of
the concept of directed immune stimulation by the sole L-arginine in medical intensive care
unit, the patients being selected based on their decrease in exhaled and nasal NO
concentrations. This pathophysiological study is the necessary first step before conducting
a large clinical trial aimed at demonstrating a reduction of nosocomial infection incidence
by L-arginine.
;
Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Investigator), Primary Purpose: Treatment
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