Effects of mission duration on neuroimmune responses in astronauts

RP Stowe, CF Sams, DL Pierson - Aviation, space, and …, 2003 - ingentaconnect.com
RP Stowe, CF Sams, DL Pierson
Aviation, space, and environmental medicine, 2003ingentaconnect.com
Stowe RP, Sams CF, Pierson DL. Effects of mission duration on neuroimmune responses in
astronauts. Aviat Space Environ Med 2003; 74: 1281–4. Background: Spaceflight poses a
unique stress to humans that can impair cellular immune responses and reactivate latent
herpes viruses. Notably, prior studies have suggested that mission length may be an
important factor in the variability of immune alterations observed after spaceflight. In this
study, adrenocortical responses and circulating leukocytes were compared between …
Stowe RP, Sams CF, Pierson DL.Effects of mission duration on neuroimmune responses in astronauts. Aviat Space Environ Med 2003; 74:1281–4.
Background
Spaceflight poses a unique stress to humans that can impair cellular immune responses and reactivate latent herpes viruses. Notably, prior studies have suggested that mission length may be an important factor in the variability of immune alterations observed after spaceflight. In this study, adrenocortical responses and circulating leukocytes were compared between astronauts who participated in either 9- or 16-d missions.
Hypothesis
Mission duration will differentially affect neuroimmune responses after spaceflight.
Methods
Blood and urine samples, collected from 28 crewmembers who flew on 5 Space Shuttle missions, were analyzed for levels of plasma and urinary cortisol, urinary catecholamines, leukocyte and lymphocyte subsets, and total IgE.
Results
After spaceflight, plasma cortisol was significantly decreased after the 9-d missions but increased after the 16-d missions. In contrast, urinary epinephrine and norepinephrine levels were greater after the 9-d missions than the 16-d missions. Total IgE was significantly increased after the 16-d missions and correlated with urinary cortisol. The number of white blood cells, polymorphonuclear leukocytes, and CD4+ T cells were significantly increased postflight. After the 9-d missions, monocytes were increased while natural killer cells were decreased. However, monocytes were decreased after the 16-d missions; no change occurred in natural killer cells.
Conclusions
These results suggest that sympathetic nervous system responses predominate after shorter spaceflights, while longer flights are characterized by glucocorticoid-mediated changes at landing that may result from the accumulative effects of microgravity (i.e., physiological deconditioning) over time.
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