DNA damage and nuclear morphological changes in cardiac hypertrophy are mediated by SNRK through actin depolymerization

BACKGROUND: Proper nuclear organization is critical for cardiomyocyte (CM) function, as global structural remodeling of nuclear morphology and chromatin structure underpins the development and progression of cardiovascular disease. Previous reports have implicated a role for DNA damage in cardiac hy...

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Autores principales: Stanczyk, Paulina, Tatekoshi, Yuki, Shapiro, Jason S., Nayudu, Krithika, Chen, Yihan, Zilber, Zachary, Schipma, Matthew, De Jesus, Adam, Mahmoodzadeh, Amir, Akrami, Ashley, Chang, Hsiang-Chun, Ardehali, Hossein
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Cold Spring Harbor Laboratory 2023
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10370003/
https://www.ncbi.nlm.nih.gov/pubmed/37503243
http://dx.doi.org/10.1101/2023.07.14.549060
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author Stanczyk, Paulina
Tatekoshi, Yuki
Shapiro, Jason S.
Nayudu, Krithika
Chen, Yihan
Zilber, Zachary
Schipma, Matthew
De Jesus, Adam
Mahmoodzadeh, Amir
Akrami, Ashley
Chang, Hsiang-Chun
Ardehali, Hossein
author_facet Stanczyk, Paulina
Tatekoshi, Yuki
Shapiro, Jason S.
Nayudu, Krithika
Chen, Yihan
Zilber, Zachary
Schipma, Matthew
De Jesus, Adam
Mahmoodzadeh, Amir
Akrami, Ashley
Chang, Hsiang-Chun
Ardehali, Hossein
author_sort Stanczyk, Paulina
collection PubMed
description BACKGROUND: Proper nuclear organization is critical for cardiomyocyte (CM) function, as global structural remodeling of nuclear morphology and chromatin structure underpins the development and progression of cardiovascular disease. Previous reports have implicated a role for DNA damage in cardiac hypertrophy, however, the mechanism for this process is not well delineated. AMPK family of proteins regulate metabolism and DNA damage response (DDR). Here, we examine whether a member of this family, SNF1-related kinase (SNRK), which plays a role in cardiac metabolism, is also involved in hypertrophic remodeling through changes in DDR and structural properties of the nucleus. METHODS: We subjected cardiac specific (cs)-Snrk(−/−) mice to trans-aortic banding (TAC) to assess the effect on cardiac function and DDR. In parallel, we modulated SNRK in vitro and assessed its effects on DDR and nuclear parameters. We also used phospho-proteomics to identify novel proteins that are phosphorylated by SNRK. Finally, co-immunoprecipitation (co-IP) was used to verify Destrin (DSTN) as the binding partner of SNRK that modulates its effects on the nucleus and DDR. RESULTS: cs-Snrk(−/−) mice display worse cardiac function and cardiac hypertrophy in response to TAC, and an increase in DDR marker pH2AX in their hearts. Additionally, in vitro Snrk knockdown results in increased DNA damage and chromatin compaction, along with alterations in nuclear flatness and 3D volume. Phospho-proteomic studies identified a novel SNRK target, DSTN, a member of F-actin depolymerizing factor (ADF) proteins that directly binds to and depolymerize F-actin. SNRK binds to DSTN, and DSTN downregulation reverses excess DNA damage and changes in nuclear parameters, in addition to cellular hypertrophy, with SNRK knockdown. We also demonstrate that SNRK knockdown promotes excessive actin depolymerization, measured by the increased ratio of globular (G-) actin to F-actin. Finally, Jasplakinolide, a pharmacological stabilizer of F-actin, rescues the increased DNA damage and aberrant nuclear morphology in SNRK downregulated cells. CONCLUSIONS: These results indicate that SNRK is a key player in cardiac hypertrophy and DNA damage through its interaction with DSTN. This interaction fine-tunes actin polymerization to reduce DDR and maintain proper CM nuclear shape and morphology.
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spelling pubmed-103700032023-07-27 DNA damage and nuclear morphological changes in cardiac hypertrophy are mediated by SNRK through actin depolymerization Stanczyk, Paulina Tatekoshi, Yuki Shapiro, Jason S. Nayudu, Krithika Chen, Yihan Zilber, Zachary Schipma, Matthew De Jesus, Adam Mahmoodzadeh, Amir Akrami, Ashley Chang, Hsiang-Chun Ardehali, Hossein bioRxiv Article BACKGROUND: Proper nuclear organization is critical for cardiomyocyte (CM) function, as global structural remodeling of nuclear morphology and chromatin structure underpins the development and progression of cardiovascular disease. Previous reports have implicated a role for DNA damage in cardiac hypertrophy, however, the mechanism for this process is not well delineated. AMPK family of proteins regulate metabolism and DNA damage response (DDR). Here, we examine whether a member of this family, SNF1-related kinase (SNRK), which plays a role in cardiac metabolism, is also involved in hypertrophic remodeling through changes in DDR and structural properties of the nucleus. METHODS: We subjected cardiac specific (cs)-Snrk(−/−) mice to trans-aortic banding (TAC) to assess the effect on cardiac function and DDR. In parallel, we modulated SNRK in vitro and assessed its effects on DDR and nuclear parameters. We also used phospho-proteomics to identify novel proteins that are phosphorylated by SNRK. Finally, co-immunoprecipitation (co-IP) was used to verify Destrin (DSTN) as the binding partner of SNRK that modulates its effects on the nucleus and DDR. RESULTS: cs-Snrk(−/−) mice display worse cardiac function and cardiac hypertrophy in response to TAC, and an increase in DDR marker pH2AX in their hearts. Additionally, in vitro Snrk knockdown results in increased DNA damage and chromatin compaction, along with alterations in nuclear flatness and 3D volume. Phospho-proteomic studies identified a novel SNRK target, DSTN, a member of F-actin depolymerizing factor (ADF) proteins that directly binds to and depolymerize F-actin. SNRK binds to DSTN, and DSTN downregulation reverses excess DNA damage and changes in nuclear parameters, in addition to cellular hypertrophy, with SNRK knockdown. We also demonstrate that SNRK knockdown promotes excessive actin depolymerization, measured by the increased ratio of globular (G-) actin to F-actin. Finally, Jasplakinolide, a pharmacological stabilizer of F-actin, rescues the increased DNA damage and aberrant nuclear morphology in SNRK downregulated cells. CONCLUSIONS: These results indicate that SNRK is a key player in cardiac hypertrophy and DNA damage through its interaction with DSTN. This interaction fine-tunes actin polymerization to reduce DDR and maintain proper CM nuclear shape and morphology. Cold Spring Harbor Laboratory 2023-07-14 /pmc/articles/PMC10370003/ /pubmed/37503243 http://dx.doi.org/10.1101/2023.07.14.549060 Text en https://creativecommons.org/licenses/by-nc-nd/4.0/This work is licensed under a Creative Commons Attribution-NonCommercial-NoDerivatives 4.0 International License (https://creativecommons.org/licenses/by-nc-nd/4.0/) , which allows reusers to copy and distribute the material in any medium or format in unadapted form only, for noncommercial purposes only, and only so long as attribution is given to the creator.
spellingShingle Article
Stanczyk, Paulina
Tatekoshi, Yuki
Shapiro, Jason S.
Nayudu, Krithika
Chen, Yihan
Zilber, Zachary
Schipma, Matthew
De Jesus, Adam
Mahmoodzadeh, Amir
Akrami, Ashley
Chang, Hsiang-Chun
Ardehali, Hossein
DNA damage and nuclear morphological changes in cardiac hypertrophy are mediated by SNRK through actin depolymerization
title DNA damage and nuclear morphological changes in cardiac hypertrophy are mediated by SNRK through actin depolymerization
title_full DNA damage and nuclear morphological changes in cardiac hypertrophy are mediated by SNRK through actin depolymerization
title_fullStr DNA damage and nuclear morphological changes in cardiac hypertrophy are mediated by SNRK through actin depolymerization
title_full_unstemmed DNA damage and nuclear morphological changes in cardiac hypertrophy are mediated by SNRK through actin depolymerization
title_short DNA damage and nuclear morphological changes in cardiac hypertrophy are mediated by SNRK through actin depolymerization
title_sort dna damage and nuclear morphological changes in cardiac hypertrophy are mediated by snrk through actin depolymerization
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10370003/
https://www.ncbi.nlm.nih.gov/pubmed/37503243
http://dx.doi.org/10.1101/2023.07.14.549060
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