Nrf2 alleviates spaceflight-induced immunosuppression and thrombotic microangiopathy in mice

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作者
Ritsuko Shimizu
Ikuo Hirano
Atsushi Hasegawa
Mikiko Suzuki
Akihito Otsuki
Keiko Taguchi
Fumiki Katsuoka
Akira Uruno
Norio Suzuki
Akane Yumoto
Risa Okada
Masaki Shirakawa
Dai Shiba
Satoru Takahashi
Takafumi Suzuki
Masayuki Yamamoto
机构
[1] Tohoku University,Tohoku Medical Megabank Organization
[2] Tohoku University Graduate School of Medicine,Department of Molecular Hematology
[3] The Advanced Research Center for Innovations in Next-Generation Medicine (INGEM) Tohoku University,Division of Oxygen Biology, New Industry Creation hatchery Center (NICHe)
[4] Tohoku University,Japanese Experiment Module (JEM) Utilization Center, Human Spaceflight Technology Directorate
[5] Japan Aerospace Exploration Agency (JAXA),Department of Anatomy and Embryology and Laboratory Animal Resource Center in Transborder Medical Research Center, Institute of Medicine
[6] University of Tsukuba,undefined
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摘要
Spaceflight-related stresses impact health via various body systems, including the haematopoietic and immune systems, with effects ranging from moderate alterations of homoeostasis to serious illness. Oxidative stress appears to be involved in these changes, and the transcription factor Nrf2, which regulates expression of a set of cytoprotective and antioxidative stress response genes, has been implicated in the response to spaceflight-induced stresses. Here, we show through analyses of mice from the MHU-3 project, in which Nrf2-knockout mice travelled in space for 31 days, that mice lacking Nrf2 suffer more seriously from spaceflight-induced immunosuppression than wild-type mice. We discovered that a one-month spaceflight-triggered the expression of tissue inflammatory marker genes in wild-type mice, an effect that was even more pronounced in the absence of Nrf2. Concomitant with induction of inflammatory conditions, the consumption of coagulation-fibrinolytic factors and platelets was elevated by spaceflight and further accelerated by Nrf2 deficiency. These results highlight that Nrf2 mitigates spaceflight-induced inflammation, subsequent immunosuppression, and thrombotic microangiopathy. These observations reveal a new strategy to relieve health problems encountered during spaceflight.
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