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CHOICE - Directed Study: Consequences of longterm- Confinement and Hypobaric HypOxia on Immunity in the Antarctic Concordia EnvironmentConcerning ground-based space physiological research, the choice of analog must carefully match the system of interest. For spaceflight-associated immune dysregulation (SAID), Antarctica winter-over has emerged as potentially the best terrestrial analog. The prolonged mission durations, extreme/dangerous environment, station-based lifestyle, isolation from outside world, disrupted circadian rhythms, and other psychological aspects make this analog extremely high fidelity for exploration-class space missions (long duration lunar, Mars). NASA, ESA and RSA are currently investigating SAID, with NASA currently operating the Integrated Immune flight study. It is desirable to have a ground analog for SAID validated, so that potential countermeasures might be validated terrestrially prior to during flight. For this presentation, NASA data collected on the winterover 2009 crewmembers, baseline through early deployment will be presented. Through early deployment (approximately 2-3 weeks at Concordia), phenotypic alterations included increased levels of memory T cells, shifts among the CD8+ T cell compartment to a more mature phenotype, and increases in constitutively activated T cells. CD8+/IFNg+ T cell percentages, and T cell blastogenesis functional responses were depressed early deployment as compared to healthy controls. In four compatible subjects, secreted T cell Th1/Th2 cytokines were measured following culture stimulation, and a Th2 shift was observed as compared to controls. Post-winter over frozen sample return will be required to determine if this shift persisted during the winter over period. Additionally, circadian rhythms remained altered compared to baseline, as determined through 5x daily cortisol measurements. Latent viral reactivation will not be determined until frozen sample return occurs.
Document ID
20100003138
Acquisition Source
Johnson Space Center
Document Type
Conference Paper
Authors
Sams, Clarence
(NASA Johnson Space Center Houston, TX, United States)
Pierson, Duane
(NASA Johnson Space Center Houston, TX, United States)
Crucian, Brian
(Wyle Integrated Science and Engineering Group Houston, TX, United States)
Chouker, Alexander
Feurecker, matthias
(European Space Agency France)
Salem, Alexander
Stowe, Raymond
(JES Tech Houston, TX, United States)
Mehta, Satish
(Microgen, LLC Galveston, TX, United States)
Quiriarte, Heather
Pierson, Duane
Sams, Clarence
Date Acquired
August 25, 2013
Publication Date
February 3, 2010
Subject Category
Aerospace Medicine
Report/Patent Number
JSC-CN-19620
Meeting Information
Meeting: NASA Human Research Program Investigators Workshop
Location: Houston, TX
Country: United States
Start Date: February 3, 2010
End Date: February 5, 2010
Distribution Limits
Public
Copyright
Public Use Permitted.
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