Systemic Inflammatory Response Syndrome Clinical Trial
Official title:
Autonomic Nervous Activity During the Systemic Inflammatory Response in Trained and Untrained Healthy Volunteers
Critical illness, severe infection, extensive trauma or tissue damage cause an inflammatory
(irritative) reaction in the body. This reaction affects the whole body and causes malaise,
circulatory and cardiac changes, fever, increases the number of white blood cells in the
blood stream and prompts release of signaling proteins. This reaction contributes to the
development of considerable organ damage and possibly organ failure. These are serious
complications in critical illness which are associated with a high mortality. This
inflammatory reaction is affected by the autonomic nervous system. This is the part of the
nervous system, which is beyond the control of the free will, and the part that regulates
circulation, breathing and digestive functions. The autonomic nervous system works via
so-called sympathetic signals, which set the body in a state of alertness to overcome
immediate challenges, and parasympathetic (vagal) signals, which are especially active
during restitution and rest. It is known, that the balanced activity in the autonomic
nervous system affects the body's inflammatory response in critical illness. A study in mice
has shown that if parasympathetic (vagal) signals are blocked mortality in critical illness
is increased. Reversely, when the autonomic nervous system is medically stimulated towards
parasympathetic signaling, the magnitude of the inflammatory response is decreased. Nicotine
exerts this stimulatory effect.
Also, we know that individuals in good physical shape have increased parasympathetic tone
compared to less trained individuals. However, studies have never addressed whether this
shifted balance in the autonomic nervous system affects the inflammatory response related to
critical illness.
Over the last 30 years an experimental model mimicking the inflammatory response has been
used in studies. Inflammation may be simulated by injecting the drug E.Coli LPS, which
induces a controlled, fully reversible, harmless reaction the duration of which is a few
hours. Influenza-like symptoms occur and changes in circulatory parameters and
concentrations of signaling proteins can be measured.
Using this experimental model, the investigators wish to study whether this shifted balance
in the autonomic nervous system in individuals in good physical shape affects the body's
reaction to critical illness. Investigators also want to determine how nicotine (using a
nicotine patch) affects this reaction.
| Status | Completed |
| Enrollment | 23 |
| Est. completion date | December 2015 |
| Est. primary completion date | January 2013 |
| Accepts healthy volunteers | Accepts Healthy Volunteers |
| Gender | Male |
| Age group | 18 Years to 35 Years |
| Eligibility |
Inclusion Criteria: - Male - Age 18-35 years - BMI < 30 kg/m2 - Healthy - Well-trained (N = 12): VO2max > 60 ml/kg/min - Untrained (N = 12): VO2max < 47 ml/kg/min Exclusion Criteria: - Daily medicine intake (excl. antihistamines during pollen season) - Smoking or use of nicotine substitutes - Previous allergic reaction to nicotine pads - Previous splenectomy |
Allocation: Randomized, Intervention Model: Crossover Assignment, Masking: Open Label, Primary Purpose: Basic Science
| Country | Name | City | State |
|---|---|---|---|
| Denmark | Center for Inflammation and Metabolism, Rigshospitalet | Copenhagen | Copenhagen OE |
| Lead Sponsor | Collaborator |
|---|---|
| Rigshospitalet, Denmark | Bispebjerg Hospital |
Denmark,
| Type | Measure | Description | Time frame | Safety issue |
|---|---|---|---|---|
| Other | Pain Pressure Threshold (PPT) | Pressure algometry performed by a hand-held device with a tip area of 1 cm2 applied perpendicularly on the non-dominant lateral vastus muscle with a gradual increase in pressure until participant indicates painful stimuli. | Baseline, 2 hours, 6 hours | No |
| Other | Heat Pain Perception | A sequence of 4 tonic heat stimuli (45, 46, 47 and 48°C) delivered by a thermos with a duration of 5 s each and separated by an interstimulus interval of 30 s. Participants rated pain sensation using a visual analog scale (VAS). | Baseline, 2 hours, 6 hours | No |
| Primary | Cytokines | Cytokines are released into the bloodstream as part of the systemic inflammatory response and allow quantification of the severity of the systemic inflammatory response. Cytokines are measured multiple times to record changes from baseline during the intervention. |
up to 8 hours | No |
| Secondary | Heart Rate Variability (HRV) | HRV is the variation in the interval between heart beats over a given time period. A higher variability is considered an indirectly marker of increasing vagal acitivity. Low variability contrarily indicates decreasing vagal activity and increased sympathetic activity. HRV is calculated from continous, non-invasive monitoring of heart rhytm. Recordings are made at multiple fixed times to track changes from baseline during intervention. |
up to 8 hours | No |
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