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Metabolic Stress in Space: ROS-Induced Mutations in Mice Hint at A New Path to CancerLong-duration spaceflight beyond Earth's magnetosphere poses serious health risks, including muscle atrophy, bone loss, liver and kidney damage, and the Spaceflight-Associated Neuro-ocular Syndrome (SANS). RNA-seq of mice aboard the International Space Station (ISS) for 37 days revealed extraordinary hypermutation in tissue-specific genes, with guanine base conversion predominating, potentially contributing to spaceflight-associated health risks. Our results suggest that the genome-wide accelerated mutation that we measured, seemingly independent of radiation dose, was induced by oxidative damage from higher atmospheric carbon dioxide (CO2) levels and increased reactive oxygen species (ROS) on the ISS. This accelerated mutation, faster via RNA transcription than replication and more numerous than by radiation alone, unveils novel hotspots in the mammalian proteome. Notably, these hotspots correlate with commonly mutated genes across various human cancers, highlighting the ISS as a crucial platform for studying accelerated mutation, genome instability, and the induction of disease-causing mutations in model organisms. Our results suggest that metabolic processes can contribute to somatic mutation, and thus may play a role in the development of cancer. A metabolic link to genetic instability potentially has far-reaching implications for various diseases, with implications for human health on Earth and in space.
Document ID
20240015074
Acquisition Source
Ames Research Center
Document Type
Reprint (Version printed in journal)
Authors
Viktor Stolc
(Ames Research Center Mountain View, United States)
Miloslav Karhanek
(Wyle (United States) El Segundo, California, United States)
Friedemann Freund
(Search for Extraterrestrial Intelligence Mountain View, United States)
Yuri Griko
(Ames Research Center Mountain View, United States)
David J Loftus
(Ames Research Center Mountain View, United States)
Maurice M Ohayon
(Stanford University School of Medicine Stanford, United States)
Date Acquired
November 25, 2024
Publication Date
October 16, 2024
Publication Information
Publication: Redox Biology
Publisher: Elsevier Science
Volume: 78
Issue: 103398
Issue Publication Date: December 1, 2024
e-ISSN: 2213-2317
Subject Category
Behavioral Sciences
Funding Number(s)
WBS: 271118.01.01.10
Distribution Limits
Public
Copyright
Use by or on behalf of the US Gov. Permitted.
Technical Review
Single Expert
Keywords
mice
Carbon Dioxide
Cancer
International Space Station (ISS)
Reactive Oxygen Species (ROS)
Hypermutation
Metabolic stress
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