Literature DB >> 23100144

Immune system dysregulation occurs during short duration spaceflight on board the space shuttle.

Brian Crucian1, Raymond Stowe, Satish Mehta, Peter Uchakin, Heather Quiriarte, Duane Pierson, Clarence Sams.   

Abstract

BACKGROUND: Post-flight data suggests immunity is dysregulated immediately following spaceflight, however this data may be influenced by the stress effects of high-G entry and readaptation to terrestrial gravity. It is unknown if immunity is altered during spaceflight.
METHODS: Blood samples were collected from 19 US Astronauts onboard the Space Shuttle ~24 h prior to landing and returned for terrestrial analysis. Assays consisted of leukocyte distribution, T cell blastogenesis and cytokine production profiles.
RESULTS: Most bulk leukocyte subsets (WBC, differential, lymphocyte subsets) were unaltered during spaceflight, but were altered following landing. CD8+ T cell subsets, including cytotoxic, central memory and senescent were altered during spaceflight. T cell early blastogenesis varied by culture mitogen. Functional responses to staphylococcal enterotoxin were reduced during and following spaceflight, whereas response to anti-CD3/28 antibodies was elevated post-flight. The level of virus specific T cells were generally unaltered, however virus specific T cell function was depressed both during and following flight. Plasma levels of IFNα, IFNγ, IL-1β, IL-4, IL-10, IL-12, and TNFα were significantly elevated in-flight, while IL-6 was significantly elevated at R + 0. Cytokine production profiles following mitogenic stimulation were significantly altered both during, and following spaceflight. Specifically, production of IFNγ, IL-17 and IL-10 were reduced, but production of TNFα and IL-8 were elevated during spaceflight.
CONCLUSIONS: This study indicates that specific parameters among leukocyte distribution, T cell function and cytokine production profiles are altered during flight. These findings distinguish in-flight dysregulation from stress-related alterations observed immediately following landing.

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Year:  2012        PMID: 23100144     DOI: 10.1007/s10875-012-9824-7

Source DB:  PubMed          Journal:  J Clin Immunol        ISSN: 0271-9142            Impact factor:   8.317


  32 in total

1.  Leukocyte subsets and neutrophil function after short-term spaceflight.

Authors:  R P Stowe; C F Sams; S K Mehta; I Kaur; M L Jones; D L Feeback; D L Pierson
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2.  The natural cytotoxicity in cosmonauts on board space stations.

Authors:  D Meshkov; M Rykova
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3.  Effects of mission duration on neuroimmune responses in astronauts.

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4.  Immune status, latent viral reactivation, and stress during long-duration head-down bed rest.

Authors:  Brian E Crucian; Raymond P Stowe; Satish K Mehta; Deborah L Yetman; Melanie J Leal; Heather D Quiriarte; Duane L Pierson; Clarence F Sams
Journal:  Aviat Space Environ Med       Date:  2009-05

5.  Immune system dysregulation during spaceflight: clinical risk for exploration-class missions.

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Journal:  J Leukoc Biol       Date:  2009-11       Impact factor: 4.962

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Review 7.  The role of cytokines in immune changes induced by spaceflight.

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9.  Effect of spaceflight on lymphocyte proliferation and interleukin-2 production.

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10.  Neuroendocrine and immune responses to 16-day bed rest with realistic launch and landing G profiles.

Authors:  Raymond P Stowe; Deborah L Yetman; William F Storm; Clarence F Sams; Duane L Pierson
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  43 in total

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5.  Plasma cytokine concentrations indicate that in vivo hormonal regulation of immunity is altered during long-duration spaceflight.

Authors:  Brian E Crucian; Sara R Zwart; Satish Mehta; Peter Uchakin; Heather D Quiriarte; Duane Pierson; Clarence F Sams; Scott M Smith
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6.  Effects of spaceflight on the immunoglobulin repertoire of unimmunized C57BL/6 mice.

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7.  Salivary antimicrobial proteins and stress biomarkers are elevated during a 6-month mission to the International Space Station.

Authors:  Nadia H Agha; Forrest L Baker; Hawley E Kunz; Guillaume Spielmann; Preteesh L Mylabathula; Bridgette V Rooney; Satish K Mehta; Duane L Pierson; Mitzi S Laughlin; Melissa M Markofski; Brian E Crucian; Richard J Simpson
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8.  Simultaneous exposure to chronic irradiation and simulated microgravity differentially alters immune cell phenotype in mouse thymus and spleen.

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9.  Human immune system adaptations to simulated microgravity revealed by single-cell mass cytometry.

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Review 10.  Immunological Aspects of Isolation and Confinement.

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