Sepsis Clinical Trial
Official title:
The Effect of the Alpha-7 Nicotinic AChR Agonist GTS-21 on Inflammation and End-organ Dysfunction During Human Endotoxemia
Rationale: The vagus nerve exerts an anti-inflammatory effect in in vitro and animal
experiments. This 'vagal anti-inflammatory pathway' is mediated by the nicotinergic α7nACh
receptor that can be selectively stimulated by GTS-21. Activation of the cholinergic
anti-inflammatory pathway via vagus nerve stimulation or α7nAChR agonists improves outcome
in animal models of endotoxemia, sepsis and experimental arthritis. Up to now, the
anti-inflammatory effects of oral administration of GTS-21 in humans in vivo has not been
investigated.
Objective: Primary aim: to investigate the anti-inflammatory effects of oral administration
of GTS-21 on the inflammatory response in the human endotoxemia model and the subsequent
inflammation-induced subclinical organ dysfunction. Secondary aim: to measure the effect of
LPS administration in the absence or presence of GTS-21 in human volunteers on vagal nerve
activity measured by heart rate variability analysis.
Study design: Double-blind placebo-controlled randomized cross-over intervention study in
healthy human volunteers during experimental endotoxemia.
Study population: Non-smoking healthy male volunteers, age 18-35 yrs Intervention: Subjects
will be tested in a cross-over design in 2 separate sequential sessions, 2-4 weeks apart. A
total of 12 subjects will be randomly assigned to one of two dosing groups in a 1:1 ratio:
GTS-21 followed by Placebo n=6, Placebo followed by GTS-21 n=6. Subjects will receive 150mg
GTS-21 or placebo orally tid 3 days before LPS injection and an oral dose of 150 mg GTS-21
or placebo the morning of the day of LPS administration (07:00 AM). Subjects will then
receive an oral dose of 150 mg GTS-21 or placebo at 08:00 AM and another oral dose of 150 mg
GTS-21 or placebo at 1 hour before LPS administration (t=0). Before LPS injection,
prehydration will be performed by infusion of 1.5 L 2.5% glucose/0.45% saline solution in 1
hour. One hour after the last dose of GTS-21 or placebo, LPS derived from E coli O:113 will
be injected (2 ng/kg iv in 1 minute). There will be a 14 day washout period for patients in
all groups. The last group of subjects will be subjected to an identical dose of LPS and
placebo at two different moments 2-4 weeks apart to obtain time controls.
Main study parameters/endpoints: Main study endpoint is the concentration of circulating
cytokines after LPS in the absence and presence of GTS-21.
Nature and extent of the burden and risks associated with participation, benefit and group
relatedness: A medical interview and physical examination is part of this study.
Approximately 350 ml blood will be withdrawn and urine will be collected. There will be mild
discomfort associated with participation in this study, as LPS induces flu-like symptoms for
approximately 4 hrs. GTS-21 was found to be well tolerated at a dose of 150 mg three times
daily (450 mg/day).
INTRODUCTION AND RATIONALE: The innate immune response is the first line of defense against
invading pathogens(1). This tightly regulated system consists of a wide variety of
chemokines, cytokines, cell associated receptors and other mediators orchestrating the
initial response to infection. Experimental evidence in the past several years has
demonstrated that activation of the efferent vagus nerve has an inhibitory effect on the
innate immune response (the cholinergic anti-inflammatory pathway, reviewed in (2,3,4)). The
anti-inflammatory effect of the vagal nerve is mediated by the α7 nicotinic acetylcholine
receptor (α7nAChR) expressed on macrophages and other cytokine-producing cells (9).
Activation of the cholinergic anti-inflammatory pathway with vagus nerve stimulation or
α7nAChR agonists improves outcome in animal models of endotoxemia, sepsis and experimental
arthritis. This cholinergic anti-inflammatory pathway is the efferent arm of a reflex
mechanism that is activated by inflammatory mediators in peripheral tissues signaling
through the afferent vagus nerve. Thus, the vagus nerve can relay inflammation signals to
the central nervous system and activate an opposing efferent response to inhibit excessive
inflammation.
GTS-21 (E-3-(2,4)-dimethoxybenzylidene anabaseine) is a highly specific α7nAchR agonist,
that has been developed for the treatment of Alzheimer's disease that has been studied in a
few inflammation-related models. In a murine pancreatitis model pre-treatment of the animals
with GTS-21 decreased pancreatitis severity and was associated with reduced IL-6 levels and
decreased pancreatic neutrophil accumulation (11). Pre-treatment of mice with GTS-21
attenuated systemic TNF concentrations after injection with LPS and increases survival
(12,13). Similarly, GTS-21 inhibited blood levels of the inflammatory mediator High Mobility
Group Box 1 (HMGB1) and improved survival of mice after cecal ligation and puncture.(13).
Recently, we have shown that stimulation of the α7nAChR by the highly selective agonist
GTS-21 leads to a dramatic dose-dependent inhibition of pro-inflammatory cytokine release
induced by stimulation of various Toll-like receptors (TLR) in human whole blood (Kox et al,
submitted). This inhibitory effect of GTS-21 was not specific for the TLR-agonist used and
GTS-21 inhibited pro-inflammatory cytokine production stronger than nicotine at equimolar
concentrations. Moreover, the production of the anti-inflammatory cytokine IL-10 was not
inhibited, but even significantly stimulated. Therefore, stimulation of the α7nAChR by
GTS-21 results in a profound anti-inflammatory shift of the pro-/anti-inflammatory balance.
So far, no data are available on the anti-inflammatory effects of GTS-21 in humans in vivo.
The human endotoxemia model is widely used to study inflammation in humans in vivo. Systemic
inflammation is induced by low-dose infusion of Escherichia coli lipopolysaccharide (LPS) in
healthy volunteers, resulting in flu-like symptoms, increased production of C-reactive
protein and increased concentrations of pro- and anti-inflammatory cytokines. The "human
endotoxemia model" permits elucidation of key players in this proinflammatory response in
humans in vivo and it serves as a useful tool to investigate potential novel therapeutic
strategies in a standardized setting.
GTS-21 was developed as a novel agent in the treatment of Alzheimer's disease. Until date,
87 healthy male volunteers were enrolled in four Phase I studies that assessed the safety,
tolerability, pharmacokinetics, and effects on cognitive function of oral administration of
GTS-21 of which 77 subjects received GTS-21 and 10 subjects received placebo. GTS-21 was
found to be well tolerated up to a dose of 150 mg three times daily (450 mg/day) in healthy
male subjects. The most common adverse event was headache, which occurred in 27% of subjects
in the GTS-21 group compared to 21% of subjects in the placebo group. There were no serious
adverse events, or severe adverse events reported during these studies. In one patient in
the GTS-21 group transient mild elevation of liver enzymes was detected, without signs of
hepatic dysfunction.
PRIMARY AIM: Primary aim of the present study is to investigate the putative
anti-inflammatory effects of oral administration of GTS-21 on the inflammatory response and
subsequent subclinical organ dysfunction in the human endotoxemia model. Secondary aim is to
measure the effect of LPS administration in the absence and presence of GTS-21 in human
volunteers on vagal nerve activity.
;
Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Crossover Assignment, Masking: Double Blind (Subject, Investigator), Primary Purpose: Treatment
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