Cardiovascular Responses to Simulated Spaceflight: Molecular Signatures and Surrogate Outputs to Measure CVD Risk
During extended space missions beyond low Earth orbit, astronauts will encounter prolonged periods of weightlessness and low dose space radiation. Previous studies have shown that exposure to small doses of high LET radiation (< 50 cGy) can lead to both short-term and long-term alterations in hea...
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| creator | Tahimic, Candice Ronca, April Alwood, Joshua Shirazi-Fard, Yasaman Puukila, Stephanie Mhatre, Siddhita Iyer, Janani Ruiz, Steffy Tabares Lowe, Moniece Paul, Amber Goukassian, David Christenson, Lane Rubinstein, Linda Delp, Michael Brekker, Adaline Semel, Maya Korostenskij, Ivan Kelly, Kaelyn Santos, Julia Krikourian, Osanna Palatsidis, Yanni Bommarito, Kennedy |
| description | During extended space missions beyond low Earth orbit, astronauts will encounter prolonged periods of weightlessness and low dose space radiation. Previous studies have shown that exposure to small doses of high LET radiation (< 50 cGy) can lead to both short-term and long-term alterations in heart function, structure and underlying molecular mechanisms. In this study, we aim to identify the molecular signature associated with the cardiovascular response to simulated galactic cosmic radiation (5-ion GCR) alone or in combination with simulated weightlessness at time intervals relevant to mission length and recovery. Additionally, we aim to determine whether sex impacts cardiovascular responses to these spaceflight factors. Our overarching goal is to enhance our understanding of the cardiovascular risks associated with extended space missions and the clinical endpoints they suggest. We hypothesize that exposure to simulated space radiation leads to enduring alterations in the transcriptome, redox signaling and cytokine environment of cardiovascular tissue, some which have known links with reduced cardiovascular performance, aging, and increased risk of cardiovascular disease (CVD). Furthermore, we posit that simulated space radiation exposure in combination with simulated microgravity exacerbates cardiovascular deficits compared to single factor exposure. Female and male C57BL/6J mice, aged 23-24 weeks, were exposed to a single dose of 5, 15, or 50 cGy of 5-ion GCR, or sham-treated (0 cGy). Euthanasia was performed at 14 days and ~4 months post-irradiation. Hearts, aorta and blood plasma were collected shortly thereafter. RNA-sequencing of left ventricles at ~4 months post-GCR exposure revealed sex differences in the heart transcriptome with a few genes showing radiation-dependent changes in expression levels. Notably, some of the differentially expressed genes in 15 and 50 cGy GCR groups are known to play roles in the development of CVD. Analysis of protein levels of a subset of inflammatory cytokines in the heart indicated sex differences but no differences between sham and 50 cGy groups. Results also showed correlations among differentially expressed genes and a subset of inflammatory cytokines, with some correlations altered by GCR exposure. These findings suggest that GCR exposure can modify protein and gene networks linked to inflammation and CVD progression. In the aorta, telomere lengths were comparable across treatment groups sexes. Mitochondrial co |
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Previous studies have shown that exposure to small doses of high LET radiation (< 50 cGy) can lead to both short-term and long-term alterations in heart function, structure and underlying molecular mechanisms. In this study, we aim to identify the molecular signature associated with the cardiovascular response to simulated galactic cosmic radiation (5-ion GCR) alone or in combination with simulated weightlessness at time intervals relevant to mission length and recovery. Additionally, we aim to determine whether sex impacts cardiovascular responses to these spaceflight factors. Our overarching goal is to enhance our understanding of the cardiovascular risks associated with extended space missions and the clinical endpoints they suggest. We hypothesize that exposure to simulated space radiation leads to enduring alterations in the transcriptome, redox signaling and cytokine environment of cardiovascular tissue, some which have known links with reduced cardiovascular performance, aging, and increased risk of cardiovascular disease (CVD). Furthermore, we posit that simulated space radiation exposure in combination with simulated microgravity exacerbates cardiovascular deficits compared to single factor exposure. Female and male C57BL/6J mice, aged 23-24 weeks, were exposed to a single dose of 5, 15, or 50 cGy of 5-ion GCR, or sham-treated (0 cGy). Euthanasia was performed at 14 days and ~4 months post-irradiation. Hearts, aorta and blood plasma were collected shortly thereafter. RNA-sequencing of left ventricles at ~4 months post-GCR exposure revealed sex differences in the heart transcriptome with a few genes showing radiation-dependent changes in expression levels. Notably, some of the differentially expressed genes in 15 and 50 cGy GCR groups are known to play roles in the development of CVD. Analysis of protein levels of a subset of inflammatory cytokines in the heart indicated sex differences but no differences between sham and 50 cGy groups. Results also showed correlations among differentially expressed genes and a subset of inflammatory cytokines, with some correlations altered by GCR exposure. These findings suggest that GCR exposure can modify protein and gene networks linked to inflammation and CVD progression. In the aorta, telomere lengths were comparable across treatment groups sexes. Mitochondrial copy number is a biomarker for mitochondrial function with decreased copy numbers associated with cardiometabolic disease traits. Mitochondrial copy numbers of aorta also showed no sex nor dose differences. In a second study, mice underwent one week of simulated microgravity by hindlimb unloading (HU) and then exposed to a single dose of 15 cGy of 5-ion GCR. HU was conducted for an additional two weeks following GCR exposure. Single factor exposure groups (HU or GCR only) also were included in the study. Euthanasia was then performed and the same tissues were collected. Protein levels of select inflammatory cytokines in the heart showed sex-dependent differences in expression. In the aorta, telomere lengths and mitochondrial copy number also showed sex differences. In summary, our results indicate differences between sexes in biomarkers related to cardiovascular health. Exposure to 5-ion GCR or HU, alone or in combination, did not result in changes in most of the cardiovascular biomarkers that were examined. However, in the heart, simulated space radiation at doses of 15 and 50 cGy led to long-term alterations in the expression levels of a small group of genes known to be associated with the progression of CVD. The long-term transcriptomic changes resulting from exposure to simulated space radiation should be carefully investigated to mitigate adverse cardiovascular events during and after deep space missions. Our results also highlight the importance of sex-specific strategies in monitoring and maintaining cardiovascular health during and after deep space missions.</description><language>eng</language><publisher>Ames Research Center</publisher><subject>Aerospace Medicine</subject><rights>Copyright Determination: MAY_INCLUDE_COPYRIGHT_MATERIAL</rights><oa>free_for_read</oa><woscitedreferencessubscribed>false</woscitedreferencessubscribed><orcidid>0000-0001-8161-8512</orcidid></display><links><openurl>$$Topenurl_article</openurl><openurlfulltext>$$Topenurlfull_article</openurlfulltext><thumbnail>$$Tsyndetics_thumb_exl</thumbnail><link.rule.ids>780,800</link.rule.ids><linktorsrc>$$Uhttps://ntrs.nasa.gov/citations/20230014752$$EView_record_in_NASA$$FView_record_in_$$GNASA$$Hfree_for_read</linktorsrc></links><search><creatorcontrib>Tahimic, Candice</creatorcontrib><creatorcontrib>Ronca, April</creatorcontrib><creatorcontrib>Alwood, Joshua</creatorcontrib><creatorcontrib>Shirazi-Fard, Yasaman</creatorcontrib><creatorcontrib>Puukila, Stephanie</creatorcontrib><creatorcontrib>Mhatre, Siddhita</creatorcontrib><creatorcontrib>Iyer, Janani</creatorcontrib><creatorcontrib>Ruiz, Steffy Tabares</creatorcontrib><creatorcontrib>Lowe, Moniece</creatorcontrib><creatorcontrib>Paul, Amber</creatorcontrib><creatorcontrib>Goukassian, David</creatorcontrib><creatorcontrib>Christenson, Lane</creatorcontrib><creatorcontrib>Rubinstein, Linda</creatorcontrib><creatorcontrib>Delp, Michael</creatorcontrib><creatorcontrib>Brekker, Adaline</creatorcontrib><creatorcontrib>Semel, Maya</creatorcontrib><creatorcontrib>Korostenskij, Ivan</creatorcontrib><creatorcontrib>Kelly, Kaelyn</creatorcontrib><creatorcontrib>Santos, Julia</creatorcontrib><creatorcontrib>Krikourian, Osanna</creatorcontrib><creatorcontrib>Palatsidis, Yanni</creatorcontrib><creatorcontrib>Bommarito, Kennedy</creatorcontrib><title>Cardiovascular Responses to Simulated Spaceflight: Molecular Signatures and Surrogate Outputs to Measure CVD Risk</title><description>During extended space missions beyond low Earth orbit, astronauts will encounter prolonged periods of weightlessness and low dose space radiation. Previous studies have shown that exposure to small doses of high LET radiation (< 50 cGy) can lead to both short-term and long-term alterations in heart function, structure and underlying molecular mechanisms. In this study, we aim to identify the molecular signature associated with the cardiovascular response to simulated galactic cosmic radiation (5-ion GCR) alone or in combination with simulated weightlessness at time intervals relevant to mission length and recovery. Additionally, we aim to determine whether sex impacts cardiovascular responses to these spaceflight factors. Our overarching goal is to enhance our understanding of the cardiovascular risks associated with extended space missions and the clinical endpoints they suggest. We hypothesize that exposure to simulated space radiation leads to enduring alterations in the transcriptome, redox signaling and cytokine environment of cardiovascular tissue, some which have known links with reduced cardiovascular performance, aging, and increased risk of cardiovascular disease (CVD). Furthermore, we posit that simulated space radiation exposure in combination with simulated microgravity exacerbates cardiovascular deficits compared to single factor exposure. Female and male C57BL/6J mice, aged 23-24 weeks, were exposed to a single dose of 5, 15, or 50 cGy of 5-ion GCR, or sham-treated (0 cGy). Euthanasia was performed at 14 days and ~4 months post-irradiation. Hearts, aorta and blood plasma were collected shortly thereafter. RNA-sequencing of left ventricles at ~4 months post-GCR exposure revealed sex differences in the heart transcriptome with a few genes showing radiation-dependent changes in expression levels. Notably, some of the differentially expressed genes in 15 and 50 cGy GCR groups are known to play roles in the development of CVD. Analysis of protein levels of a subset of inflammatory cytokines in the heart indicated sex differences but no differences between sham and 50 cGy groups. Results also showed correlations among differentially expressed genes and a subset of inflammatory cytokines, with some correlations altered by GCR exposure. These findings suggest that GCR exposure can modify protein and gene networks linked to inflammation and CVD progression. In the aorta, telomere lengths were comparable across treatment groups sexes. Mitochondrial copy number is a biomarker for mitochondrial function with decreased copy numbers associated with cardiometabolic disease traits. Mitochondrial copy numbers of aorta also showed no sex nor dose differences. In a second study, mice underwent one week of simulated microgravity by hindlimb unloading (HU) and then exposed to a single dose of 15 cGy of 5-ion GCR. HU was conducted for an additional two weeks following GCR exposure. Single factor exposure groups (HU or GCR only) also were included in the study. Euthanasia was then performed and the same tissues were collected. Protein levels of select inflammatory cytokines in the heart showed sex-dependent differences in expression. In the aorta, telomere lengths and mitochondrial copy number also showed sex differences. In summary, our results indicate differences between sexes in biomarkers related to cardiovascular health. Exposure to 5-ion GCR or HU, alone or in combination, did not result in changes in most of the cardiovascular biomarkers that were examined. However, in the heart, simulated space radiation at doses of 15 and 50 cGy led to long-term alterations in the expression levels of a small group of genes known to be associated with the progression of CVD. The long-term transcriptomic changes resulting from exposure to simulated space radiation should be carefully investigated to mitigate adverse cardiovascular events during and after deep space missions. Our results also highlight the importance of sex-specific strategies in monitoring and maintaining cardiovascular health during and after deep space missions.</description><subject>Aerospace Medicine</subject><fulltext>true</fulltext><rsrctype>other</rsrctype><recordtype>other</recordtype><sourceid>CYI</sourceid><recordid>eNqFzLEKwjAQBuAuDqK-gcO9gFBbpeBaFZcitOJajvZagzGJuYvPb1B3p4P___6bJs8Sfa_sC7kLGj3UxM4aJgax0KhHDIV6aBx2NGg13mQHldX01Y0aDUrwkaOJKnhvxziAcxAX5POkIuQooLzuoVZ8nyeTATXT4ndnyfJ4uJSnlUHG1ojnNkuzPE3Xm2Kb5X_qN_JuP2U</recordid><creator>Tahimic, Candice</creator><creator>Ronca, April</creator><creator>Alwood, Joshua</creator><creator>Shirazi-Fard, Yasaman</creator><creator>Puukila, Stephanie</creator><creator>Mhatre, Siddhita</creator><creator>Iyer, Janani</creator><creator>Ruiz, Steffy Tabares</creator><creator>Lowe, Moniece</creator><creator>Paul, Amber</creator><creator>Goukassian, David</creator><creator>Christenson, Lane</creator><creator>Rubinstein, Linda</creator><creator>Delp, Michael</creator><creator>Brekker, Adaline</creator><creator>Semel, Maya</creator><creator>Korostenskij, Ivan</creator><creator>Kelly, Kaelyn</creator><creator>Santos, Julia</creator><creator>Krikourian, Osanna</creator><creator>Palatsidis, Yanni</creator><creator>Bommarito, Kennedy</creator><scope>CYE</scope><scope>CYI</scope><orcidid>https://orcid.org/0000-0001-8161-8512</orcidid></search><sort><title>Cardiovascular Responses to Simulated Spaceflight: Molecular Signatures and Surrogate Outputs to Measure CVD Risk</title><author>Tahimic, Candice ; Ronca, April ; Alwood, Joshua ; Shirazi-Fard, Yasaman ; Puukila, Stephanie ; Mhatre, Siddhita ; Iyer, Janani ; Ruiz, Steffy Tabares ; Lowe, Moniece ; Paul, Amber ; Goukassian, David ; Christenson, Lane ; Rubinstein, Linda ; Delp, Michael ; Brekker, Adaline ; Semel, Maya ; Korostenskij, Ivan ; Kelly, Kaelyn ; Santos, Julia ; Krikourian, Osanna ; Palatsidis, Yanni ; Bommarito, Kennedy</author></sort><facets><frbrtype>5</frbrtype><frbrgroupid>cdi_FETCH-nasa_ntrs_202300147523</frbrgroupid><rsrctype>other</rsrctype><prefilter>other</prefilter><language>eng</language><topic>Aerospace Medicine</topic><toplevel>online_resources</toplevel><creatorcontrib>Tahimic, Candice</creatorcontrib><creatorcontrib>Ronca, April</creatorcontrib><creatorcontrib>Alwood, Joshua</creatorcontrib><creatorcontrib>Shirazi-Fard, Yasaman</creatorcontrib><creatorcontrib>Puukila, Stephanie</creatorcontrib><creatorcontrib>Mhatre, Siddhita</creatorcontrib><creatorcontrib>Iyer, Janani</creatorcontrib><creatorcontrib>Ruiz, Steffy Tabares</creatorcontrib><creatorcontrib>Lowe, Moniece</creatorcontrib><creatorcontrib>Paul, Amber</creatorcontrib><creatorcontrib>Goukassian, David</creatorcontrib><creatorcontrib>Christenson, Lane</creatorcontrib><creatorcontrib>Rubinstein, Linda</creatorcontrib><creatorcontrib>Delp, Michael</creatorcontrib><creatorcontrib>Brekker, Adaline</creatorcontrib><creatorcontrib>Semel, Maya</creatorcontrib><creatorcontrib>Korostenskij, Ivan</creatorcontrib><creatorcontrib>Kelly, Kaelyn</creatorcontrib><creatorcontrib>Santos, Julia</creatorcontrib><creatorcontrib>Krikourian, Osanna</creatorcontrib><creatorcontrib>Palatsidis, Yanni</creatorcontrib><creatorcontrib>Bommarito, Kennedy</creatorcontrib><collection>NASA Scientific and Technical Information</collection><collection>NASA Technical Reports Server</collection></facets><delivery><delcategory>Remote Search Resource</delcategory><fulltext>fulltext_linktorsrc</fulltext></delivery><addata><au>Tahimic, Candice</au><au>Ronca, April</au><au>Alwood, Joshua</au><au>Shirazi-Fard, Yasaman</au><au>Puukila, Stephanie</au><au>Mhatre, Siddhita</au><au>Iyer, Janani</au><au>Ruiz, Steffy Tabares</au><au>Lowe, Moniece</au><au>Paul, Amber</au><au>Goukassian, David</au><au>Christenson, Lane</au><au>Rubinstein, Linda</au><au>Delp, Michael</au><au>Brekker, Adaline</au><au>Semel, Maya</au><au>Korostenskij, Ivan</au><au>Kelly, Kaelyn</au><au>Santos, Julia</au><au>Krikourian, Osanna</au><au>Palatsidis, Yanni</au><au>Bommarito, Kennedy</au><format>book</format><genre>document</genre><ristype>GEN</ristype><title>Cardiovascular Responses to Simulated Spaceflight: Molecular Signatures and Surrogate Outputs to Measure CVD Risk</title><abstract>During extended space missions beyond low Earth orbit, astronauts will encounter prolonged periods of weightlessness and low dose space radiation. Previous studies have shown that exposure to small doses of high LET radiation (< 50 cGy) can lead to both short-term and long-term alterations in heart function, structure and underlying molecular mechanisms. In this study, we aim to identify the molecular signature associated with the cardiovascular response to simulated galactic cosmic radiation (5-ion GCR) alone or in combination with simulated weightlessness at time intervals relevant to mission length and recovery. Additionally, we aim to determine whether sex impacts cardiovascular responses to these spaceflight factors. Our overarching goal is to enhance our understanding of the cardiovascular risks associated with extended space missions and the clinical endpoints they suggest. We hypothesize that exposure to simulated space radiation leads to enduring alterations in the transcriptome, redox signaling and cytokine environment of cardiovascular tissue, some which have known links with reduced cardiovascular performance, aging, and increased risk of cardiovascular disease (CVD). Furthermore, we posit that simulated space radiation exposure in combination with simulated microgravity exacerbates cardiovascular deficits compared to single factor exposure. Female and male C57BL/6J mice, aged 23-24 weeks, were exposed to a single dose of 5, 15, or 50 cGy of 5-ion GCR, or sham-treated (0 cGy). Euthanasia was performed at 14 days and ~4 months post-irradiation. Hearts, aorta and blood plasma were collected shortly thereafter. RNA-sequencing of left ventricles at ~4 months post-GCR exposure revealed sex differences in the heart transcriptome with a few genes showing radiation-dependent changes in expression levels. Notably, some of the differentially expressed genes in 15 and 50 cGy GCR groups are known to play roles in the development of CVD. Analysis of protein levels of a subset of inflammatory cytokines in the heart indicated sex differences but no differences between sham and 50 cGy groups. Results also showed correlations among differentially expressed genes and a subset of inflammatory cytokines, with some correlations altered by GCR exposure. These findings suggest that GCR exposure can modify protein and gene networks linked to inflammation and CVD progression. In the aorta, telomere lengths were comparable across treatment groups sexes. Mitochondrial copy number is a biomarker for mitochondrial function with decreased copy numbers associated with cardiometabolic disease traits. Mitochondrial copy numbers of aorta also showed no sex nor dose differences. In a second study, mice underwent one week of simulated microgravity by hindlimb unloading (HU) and then exposed to a single dose of 15 cGy of 5-ion GCR. HU was conducted for an additional two weeks following GCR exposure. Single factor exposure groups (HU or GCR only) also were included in the study. Euthanasia was then performed and the same tissues were collected. Protein levels of select inflammatory cytokines in the heart showed sex-dependent differences in expression. In the aorta, telomere lengths and mitochondrial copy number also showed sex differences. In summary, our results indicate differences between sexes in biomarkers related to cardiovascular health. Exposure to 5-ion GCR or HU, alone or in combination, did not result in changes in most of the cardiovascular biomarkers that were examined. However, in the heart, simulated space radiation at doses of 15 and 50 cGy led to long-term alterations in the expression levels of a small group of genes known to be associated with the progression of CVD. The long-term transcriptomic changes resulting from exposure to simulated space radiation should be carefully investigated to mitigate adverse cardiovascular events during and after deep space missions. Our results also highlight the importance of sex-specific strategies in monitoring and maintaining cardiovascular health during and after deep space missions.</abstract><cop>Ames Research Center</cop><orcidid>https://orcid.org/0000-0001-8161-8512</orcidid><oa>free_for_read</oa></addata></record> |
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| title | Cardiovascular Responses to Simulated Spaceflight: Molecular Signatures and Surrogate Outputs to Measure CVD Risk |
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