Aging Clinical Trial
Official title:
The Role of the "Inflammatory/ Pathogen Burden" for Cardiac Ageing
In the elderly a chronic basal systemic inflammation prevails - which is evident by enhanced
CRP or IL-6 plasma concentrations - and by compromised defense mechanisms against invading
microbes. These alterations belong to the physiological ageing process of the immune system
(immunosenescence) and are regarded as an inflammatory response towards lifelong antigen
stress ("inflammatory/pathogen burden"). This lifelong antigen stress evokes an
age-dependent basal inflammatory activation of innate immunity as well as a wasting of
specific immunity: it is supposed that in the course of life-time due to a multitude of
infectious/inflammatory events ("multiple hits") an inflammatory stress prevails or
"inflammatory/pathogen burden" accumulates, which substantially contributes to an
enhancement of the inflammatory parameters of natural immune response. Such enhanced
inflammatory parameters characterize persons at increased risk of degenerative diseases like
atherosclerosis or coronary heart disease. The risk is the higher, the higher the "pathogen
burden". An impact of the inflammatory load on cardiac ageing has not yet been described.
"CARDIAC AGEING", REFLECTED BY A NARROWING OF HEART RATE VARIABILITY: The physiological
ageing process of the heart goes along with a narrowing of heart rate variability as shown
by various groups, including our own. Arguments in favour of a causal relationship between
inflammation and cardiac ageing come from an experimental study with healthy human
volunteers who had received a low dose of endotoxin: such a proinflammatory stimulus leads
to a reversible narrowing of heart rate variability (7). Also in senescence heart rate
variability steadily declines, paralleled by a steady increase of basal inflammatory
activity.
The reduction of heart rate variability also is regarded as a sensitive parameter of
autonomic dysfunction, which contributes to the compromise of cardiac reserve in old age.
Apart from typical morphological features and functional deterioration, e.g. diastolic
dysfunction, the senescent heart is typically characterized by a narrowed heart rate
variability. Efforts have been made to estimate the cardiac age of an individual by this
compromised heart rate variability, which may be divergent to the biological age. In recent
years diverse approaches were proposed to measure cardiac age on the basis of heart rate
variability. The published mathematical formulae were mostly validated with small patient
groups and have presently not entered clinical practice. Still heart rate variability is an
accepted surrogate parameter of cardiac ageing and is amenable by therapeutic measures, e.g.
beta-blockade.
The interaction between autonomic nervous system and inflammation is bilateral: thus vagal
stimulation can improve heart rate variability and at the same time evoke anti-inflammatory
action: this "cholinergic anti-inflammatory" reflex could make the basis for pharmacological
interventions to confine overwhelming inflammatory response syndromes. The afferent vagal
nerve, on the other hand, can be stimulated by inflammatory mediators and toxins (endotoxin,
Interleukin-1), thus activating the efferent vagus to release acetylcholine, which can bind
to a nicotinergic acetylcholine receptor on macrophages and thus interrupt cytokine release
and limit the rise in the blood levels of proinflammatory cytokines (TNF, IL-6). The
biological meaning of this reflex is to localise inflammatory reactions in the organism and
prevent a spill of cytokines to the circulation. A functioning autonomic nervous system is
thus mandatory to prevent overshooting of inflammatory response to infection and
non-infectious stimuli. The link between cardiac ageing and autonomic dysfunction gives
another argument in favour of the notion that autonomic dysfunction and
pathogen/inflammatory load could be factors promoting cardiac ageing. This, on the other
hand, implies the chance of slowing down the cardiac ageing process by successfully
modulating the extent of autonomic dysfunction and the scope of "pathogen/inflammatory
burden".
THE NEED FOR A TRIAL:
A possible causal relationship between basal inflammatory activation and cardiac ageing has
not been established. This is the issue of the project proposal. In this trial the
investigators strive to lower the "pathogen/ inflammatory load" by simple and safe measures.
The investigators therefore chose treatment with statins, standardised physical training
(both parameters of heart function and heart rate variability could thus be improved) and
vaccinations against influenza and pneumococci to prevent a further enhanced "pathogen/
inflammatory burden".
n/a
Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Prevention
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