Septic Shock Clinical Trial
Official title:
Effects on Sublingual Microcirculation of IgGAM Immunoglobulins (Pentaglobin®) in Severe Septic/Septic Shock Patients: a Randomized Controller Trial.
IgM-enriched immunoglobulins (IgGAM; Pentaglobin ® ) are new therapy for sepsis and septic
shock since they support immune system especially in case of " immunoparalysis" . However
IgGAM isn't commonly prescribed, few centres use it as routine in severe infections and there
aren't any guidelines to determine how and when to use them.
Microcirculatory dysfunction is a crucial aspect in the pathogenesis of sepsis-induced organ
dysfunction, resulting in hypoperfusion and tissue hypoxia. Unpublished clinical data suggest
a beneficial effect of IgGAM at microvascular level proved with near infrared spectroscopy
and Vascular occlusion test (VOT).
This study is a double blind phase II prospective randomised controlled trial that will
include patients admitted to the Intensive Care Unit of the University Hospital "Ospedali
Riuniti" of Ancona, after no more than 24 hours from development of severe sepsis or septic
shoc.
Patients will be randomized into two groups (treaties and controls): patients in group of the
treaties will be submitted to infusion of IgGAM conjugate (Pentaglobin ®) at dosage of 250
mg/kg IV (5 mL/kg) per day (rate of 0.4 mL/kg/h), for 72 hours. The controls will receive
equal amount of physiological NaCl solution (0.9%) as placebo. Neither the patient nor the
staff nurses and MD will be aware of the group and of the treatment applied. IgGAM solutions
or NaCl 0.9% will be provided by the hospital pharmacy in similar bags. The remaining
treatments will not be changed in any way and will be at the discretion of the doctor who's
in charge of the patient. All patients of the two groups will receive the optimal therapy for
their conditions, according to good medical clinical practice (GMP), with appropriate
antibiotic therapy, vasoactive and infusional therapy
Sepsis is a complex set of signs and symptoms caused by Systemic Inflammatory Response
Syndrome (SIRS) to an infection. Sepsis-related mortality is directly proportional to the
severity of organ dysfunction, and can be up to 80% in the case of septic shock.
Due to the pro-inflammatory response to this insult, tissues can be damaged far away from the
primary site of infection. Concurrently with pro-inflammatory cytokines, the immune system
produces anti-inflammatory mediators such as IL-10, which exert a compensatory antagonist
response. The imbalance toward the anti-inflammatory one can conduce to "immuno-paralysis"
that undermines the defense of the organism against infection.
Antibodies play a crucial role in fighting infections; low levels of protective antibodies
are directly related to worst outcome. In consideration to that, polyvalent immunoglobulins
(Ig) represent a potential therapeutic support for modulation of immune response and of
inflammation in sepsis and septic shock.
They contain a broad spectrum of antibodies direct against a wide variety of bacterial
antigens (all three classes normally found in human plasma - IgG and IgM and IgGAM
conjugate).
In addition to antibody activity and antigen neutralization, benefits of Ig may include:
inactivation of bacterial toxins (endotoxin and exotoxins); increased clearance of
lipopolysaccharide; stimulation of leukocytes and their bactericidal activity through
mechanism of opsonization; reduction in the activity of the classical pathway of the
complement; modulation of cytokine production by blood mononuclear cells; synergistic
activity with antibiotics.
Meta-analysis of main studies produced so far have shown that the Ig support, in particular
the IgM-enriched ones, are associated with improved survival of patient with severe sepsis;
these are promising results but the quality of the studies doesn't allow yet to have strong
evidence in favour of their use.
The IgM-enriched immunoglobulins (IgGAM) proved to be most effective and are currently in the
formulary and usable in case of severe infections (Pentaglobin ®). However, they are not
commonly prescribed, and there aren't any guidelines to determine how and when to use them.
Unpublished clinical data suggest a beneficial effect even at microvascular level by
application of the method of near infrared spectroscopy with vascular occlusion tests on
level of tenar eminence of the hand.
Microcirculatory dysfunction (endothelial damage and glycocalyx, increased permeability and
tissue edema, leukocyte adhesion, pro-coagulating agent, reduction of deformability of red
blood cells) is a crucial aspect in the pathogenesis of sepsis-induced organ dysfunction,
resulting in hypoperfusion and tissue hypoxia. Persistent microvascular perfusion
abnormalities have been associated with an unfavorable outcome in patients with septic shock.
In consideration to that, a therapy that can prove to act on the microcirculation by
restoring tissue perfusion would represent a promising pathophysiological approach to the
patient in septic shock.
Material and Methods This is a double blind phase II prospective randomised controlled trial.
It will include patients admitted to the Intensive Care Unit of the University Hospital
"Ospedali Riuniti" of Ancona, after no more than 24 hours from development of severe sepsis
or septic shock (diagnosis according to the criteria established by the Consensus Conference
of 2001).
Patients younger than 18 years old, pregnant women, patients with severe sepsis/septic shock
for more than 24 hours, chronic renal failure, terminal state with a life expectancy of less
than 24 hours, contraindications to treatment with IgGAM, lack of informed consent will be
excluded.
When inclusion criteria present and there aren't any exclusion criteria for this trials
written informed consent will be taken by patient.
Demographic and clinical data will be collected by the investigator (age, weight, sex, acute
and chronic diseases present at inclusion, GCS, APACHE II, SAPS II, arterial blood gases,
SOFA score, lab data such as Hb, WBC, hepatic and renal function, blood sugar, Procalcitonin
) Patients will be randomized into two groups (treaties and controls): patients in Group of
the treaties will be submitted to infusion of IgGAM conjugate (Pentaglobin ®) at dosage of
250 mg/kg IV (5 mL/kg) per day (rate of 0.4 mL/kg/h), for 72 hours. The controls will receive
equal amount of physiological NaCl solution (0.9%) as placebo. Neither the patient nor the
staff nurses and MD will be aware of the group and of the treatment applied (double blind
trial). IgGAM solutions or NaCl 0.9% are provided by the hospital pharmacy in similar bags.
All patients of the two groups will receive the optimal therapy for their conditions,
according to good medical clinical practice (GMP), with appropriate antibiotic therapy,
vasoactive and infusional therapy.All treatments except from Pentaglobin/placebo will not be
changed and will be at the discretion of the doctor who's in charge of the patient.At the
time of inclusion, the following data will be collected: gender, age, anthropometric
parameters, ICU admission diagnosis, known or suspected infection, results of microbiological
tests. Prior to initiating therapy (T0), after 24 hours (T24) and at the end of therapy with
IgGAM conjugate sublingual microcirculation will be evaluated by "Incident Dark Field Imaging
(Medical imaging, Cytocam, IDF Braedius, Amsterdam, The Netherlands) and tissue oxygenation
by using "Near Infrared Spectroscopy technique " (NIRS, InSpectra ™ Model 650; Hutchinson
Technology Inc., Hutchinson, MN, USA). Both techniques are commonly used in our clinical
practice and include CE mark.
At the same time points temperature and hemodynamic parameters (mean arterial pressure and
heart rate; cardiac index, global end-diastolic volume, extravascular Lung water when
monitored) will be collected, together with arterial and venous blood gas and lab data,
diuresis and water balance, GCS. Concomitant treatments are noted. Data regarding the
duration of hospital stay in intensive care and the outcome will be recorded.
The sample size has been assessed on the basis of the primary objective of the study, based
on a significantly higher PVD in the Group of patients treated with IgGAM compared with
controls at 72 hours after starting treatment. Assuming an average difference between the two
groups at 72hrs of 4 mm/mm2 with a SD of 3, nine patients per group would be sufficient with
an α error of 0.05 and a power of 80%. In total 20 patients will be included (10 per group
All data will be collected anonymously, attributing to each selected patient only an
alpha-numeric code, into an electronic database (password protected), respecting privacy and
confidentiality of the data.
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