Antibody responses to bacteriophage φX-174 in human subjects exposed to the Antarctic winter-over model of spaceflight

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Abstract

Background: It has been proposed that exposure to long-term spaceflight conditions (stress, isolation, sleep disruption, containment, microbial contamination, and solar radiation) or to ground-based models of spaceflight will alter human immune responses, but specific antibody responses have not been fully evaluated. Objective: We sought to determine whether exposure to the 8-month Antarctic winter-over model of spaceflight would alter human antibody responses. Methods: During the 1999 Australian National Antarctic Research Expeditions, 11 adult study subjects at Casey, Antarctica, and 7 control subjects at Macquarie Island, sub-Antarctica, received primary and secondary immunizations with the T cell-dependent neoantigen bacteriophage φX-174. Periodic plasma samples were analyzed for specific antibody function. Results: All of the subjects from Casey, Antarctica, cleared bacteriophage φX-174 normally by 1 week after primary immunization, and all had normal primary and secondary antibody responses, including immunologic memory amplification and switch from IgM to IgG antibody production. One subject showed a high normal pattern, and one subject had a low normal pattern. The control subjects from Macquarie Island also had normal immune responses to bacteriophage φX-174. Conclusions: These data do not support the hypothesis that de novo specific antibody responses of subjects become defective during the conditions of the Antarctic winter-over. Because the Antarctic winter-over model of spaceflight lacks the important factors of microgravity and solar radiation, caution must be used in interpreting these data to anticipate normal antibody responses in long-term spaceflight.

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Shearer, W. T., Lugg, D. J., Rosenblatt, H. M., Nickolls, P. M., Sharp, R. M., Reuben, J. M., & Ochs, H. D. (2001). Antibody responses to bacteriophage φX-174 in human subjects exposed to the Antarctic winter-over model of spaceflight. Journal of Allergy and Clinical Immunology, 107(1), 160–164. https://doi.org/10.1067/mai.2001.112269

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