Chronic developmental hypoxia alters mitochondrial oxidative capacity and reactive oxygen species production in the fetal rat heart in a sex‐dependent manner

Insufficient oxygen supply (hypoxia) during fetal development leads to cardiac remodeling and a predisposition to cardiovascular disease in later life. Previous work has shown hypoxia causes oxidative stress in the fetal heart and alters the activity and expression of mitochondrial proteins in a sex...

Descripción completa

Detalles Bibliográficos
Autores principales: Smith, Kerri L. M., Swiderska, Agnieszka, Lock, Mitchell C., Graham, Lucia, Iswari, Wulan, Choudhary, Tashi, Thomas, Donna, Kowash, Hager M., Desforges, Michelle, Cottrell, Elizabeth C., Trafford, Andrew W., Giussani, Dino A., Galli, Gina L. J.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley and Sons Inc. 2022
Materias:
Original Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9540814/
https://www.ncbi.nlm.nih.gov/pubmed/35941749
http://dx.doi.org/10.1111/jpi.12821
_version_ 1784803785842884608
author Smith, Kerri L. M.
Swiderska, Agnieszka
Lock, Mitchell C.
Graham, Lucia
Iswari, Wulan
Choudhary, Tashi
Thomas, Donna
Kowash, Hager M.
Desforges, Michelle
Cottrell, Elizabeth C.
Trafford, Andrew W.
Giussani, Dino A.
Galli, Gina L. J.
author_facet Smith, Kerri L. M.
Swiderska, Agnieszka
Lock, Mitchell C.
Graham, Lucia
Iswari, Wulan
Choudhary, Tashi
Thomas, Donna
Kowash, Hager M.
Desforges, Michelle
Cottrell, Elizabeth C.
Trafford, Andrew W.
Giussani, Dino A.
Galli, Gina L. J.
author_sort Smith, Kerri L. M.
collection PubMed
description Insufficient oxygen supply (hypoxia) during fetal development leads to cardiac remodeling and a predisposition to cardiovascular disease in later life. Previous work has shown hypoxia causes oxidative stress in the fetal heart and alters the activity and expression of mitochondrial proteins in a sex‐dependent manner. However, the functional effects of these modifications on mitochondrial respiration remain unknown. Furthermore, while maternal antioxidant treatments are emerging as a promising new strategy to protect the hypoxic fetus, whether these treatments convey similar protection to cardiac mitochondria in the male or female fetus has not been investigated. Therefore, using an established rat model, we measured the sex‐dependent effects of gestational hypoxia and maternal melatonin treatment on fetal cardiac mitochondrial respiration, reactive oxygen species (ROS) production, and lipid peroxidation. Pregnant Wistar rats were subjected to normoxia or hypoxia (13% oxygen) during gestational days (GDs) 6–20 (term ~22 days) with or without melatonin treatment (5 µg/ml in maternal drinking water). On GD 20, mitochondrial aerobic respiration and H(2)O(2) production were measured in fetal heart tissue, together with lipid peroxidation and citrate synthase (CS) activity. Gestational hypoxia reduced maternal body weight gain (p < .01) and increased placental weight (p < .05) but had no effect on fetal weight or litter size. Cardiac mitochondria from male but not female fetuses of hypoxic pregnancy had reduced respiratory capacity at Complex II (CII) (p < .05), and an increase in H(2)O(2) production/O(2) consumption (p < .05) without any changes in lipid peroxidation. CS activity was also unchanged in both sexes. Despite maternal melatonin treatment increasing maternal and fetal plasma melatonin concentration (p < .001), melatonin treatment had no effect on any of the mitochondrial parameters investigated. To conclude, we show that gestational hypoxia leads to ROS generation from the mitochondrial electron transport chain and affects fetal cardiac mitochondrial respiration in a sex‐dependent manner. We also show that maternal melatonin treatment had no effect on these relationships, which has implications for the development of future therapies for hypoxic pregnancies.
format Online
Article
Text
id pubmed-9540814
institution National Center for Biotechnology Information
language English
publishDate 2022
publisher John Wiley and Sons Inc.
record_format MEDLINE/PubMed
spelling pubmed-95408142022-10-14 Chronic developmental hypoxia alters mitochondrial oxidative capacity and reactive oxygen species production in the fetal rat heart in a sex‐dependent manner Smith, Kerri L. M. Swiderska, Agnieszka Lock, Mitchell C. Graham, Lucia Iswari, Wulan Choudhary, Tashi Thomas, Donna Kowash, Hager M. Desforges, Michelle Cottrell, Elizabeth C. Trafford, Andrew W. Giussani, Dino A. Galli, Gina L. J. J Pineal Res Original Articles Insufficient oxygen supply (hypoxia) during fetal development leads to cardiac remodeling and a predisposition to cardiovascular disease in later life. Previous work has shown hypoxia causes oxidative stress in the fetal heart and alters the activity and expression of mitochondrial proteins in a sex‐dependent manner. However, the functional effects of these modifications on mitochondrial respiration remain unknown. Furthermore, while maternal antioxidant treatments are emerging as a promising new strategy to protect the hypoxic fetus, whether these treatments convey similar protection to cardiac mitochondria in the male or female fetus has not been investigated. Therefore, using an established rat model, we measured the sex‐dependent effects of gestational hypoxia and maternal melatonin treatment on fetal cardiac mitochondrial respiration, reactive oxygen species (ROS) production, and lipid peroxidation. Pregnant Wistar rats were subjected to normoxia or hypoxia (13% oxygen) during gestational days (GDs) 6–20 (term ~22 days) with or without melatonin treatment (5 µg/ml in maternal drinking water). On GD 20, mitochondrial aerobic respiration and H(2)O(2) production were measured in fetal heart tissue, together with lipid peroxidation and citrate synthase (CS) activity. Gestational hypoxia reduced maternal body weight gain (p < .01) and increased placental weight (p < .05) but had no effect on fetal weight or litter size. Cardiac mitochondria from male but not female fetuses of hypoxic pregnancy had reduced respiratory capacity at Complex II (CII) (p < .05), and an increase in H(2)O(2) production/O(2) consumption (p < .05) without any changes in lipid peroxidation. CS activity was also unchanged in both sexes. Despite maternal melatonin treatment increasing maternal and fetal plasma melatonin concentration (p < .001), melatonin treatment had no effect on any of the mitochondrial parameters investigated. To conclude, we show that gestational hypoxia leads to ROS generation from the mitochondrial electron transport chain and affects fetal cardiac mitochondrial respiration in a sex‐dependent manner. We also show that maternal melatonin treatment had no effect on these relationships, which has implications for the development of future therapies for hypoxic pregnancies. John Wiley and Sons Inc. 2022-08-17 2022-10 /pmc/articles/PMC9540814/ /pubmed/35941749 http://dx.doi.org/10.1111/jpi.12821 Text en © 2022 The Authors. Journal of Pineal Research published by John Wiley & Sons Ltd. https://creativecommons.org/licenses/by/4.0/This is an open access article under the terms of the http://creativecommons.org/licenses/by/4.0/ (https://creativecommons.org/licenses/by/4.0/) License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited.
spellingShingle Original Articles
Smith, Kerri L. M.
Swiderska, Agnieszka
Lock, Mitchell C.
Graham, Lucia
Iswari, Wulan
Choudhary, Tashi
Thomas, Donna
Kowash, Hager M.
Desforges, Michelle
Cottrell, Elizabeth C.
Trafford, Andrew W.
Giussani, Dino A.
Galli, Gina L. J.
Chronic developmental hypoxia alters mitochondrial oxidative capacity and reactive oxygen species production in the fetal rat heart in a sex‐dependent manner
title Chronic developmental hypoxia alters mitochondrial oxidative capacity and reactive oxygen species production in the fetal rat heart in a sex‐dependent manner
title_full Chronic developmental hypoxia alters mitochondrial oxidative capacity and reactive oxygen species production in the fetal rat heart in a sex‐dependent manner
title_fullStr Chronic developmental hypoxia alters mitochondrial oxidative capacity and reactive oxygen species production in the fetal rat heart in a sex‐dependent manner
title_full_unstemmed Chronic developmental hypoxia alters mitochondrial oxidative capacity and reactive oxygen species production in the fetal rat heart in a sex‐dependent manner
title_short Chronic developmental hypoxia alters mitochondrial oxidative capacity and reactive oxygen species production in the fetal rat heart in a sex‐dependent manner
title_sort chronic developmental hypoxia alters mitochondrial oxidative capacity and reactive oxygen species production in the fetal rat heart in a sex‐dependent manner
topic Original Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9540814/
https://www.ncbi.nlm.nih.gov/pubmed/35941749
http://dx.doi.org/10.1111/jpi.12821
work_keys_str_mv AT smithkerrilm chronicdevelopmentalhypoxiaaltersmitochondrialoxidativecapacityandreactiveoxygenspeciesproductioninthefetalratheartinasexdependentmanner
AT swiderskaagnieszka chronicdevelopmentalhypoxiaaltersmitochondrialoxidativecapacityandreactiveoxygenspeciesproductioninthefetalratheartinasexdependentmanner
AT lockmitchellc chronicdevelopmentalhypoxiaaltersmitochondrialoxidativecapacityandreactiveoxygenspeciesproductioninthefetalratheartinasexdependentmanner
AT grahamlucia chronicdevelopmentalhypoxiaaltersmitochondrialoxidativecapacityandreactiveoxygenspeciesproductioninthefetalratheartinasexdependentmanner
AT iswariwulan chronicdevelopmentalhypoxiaaltersmitochondrialoxidativecapacityandreactiveoxygenspeciesproductioninthefetalratheartinasexdependentmanner
AT choudharytashi chronicdevelopmentalhypoxiaaltersmitochondrialoxidativecapacityandreactiveoxygenspeciesproductioninthefetalratheartinasexdependentmanner
AT thomasdonna chronicdevelopmentalhypoxiaaltersmitochondrialoxidativecapacityandreactiveoxygenspeciesproductioninthefetalratheartinasexdependentmanner
AT kowashhagerm chronicdevelopmentalhypoxiaaltersmitochondrialoxidativecapacityandreactiveoxygenspeciesproductioninthefetalratheartinasexdependentmanner
AT desforgesmichelle chronicdevelopmentalhypoxiaaltersmitochondrialoxidativecapacityandreactiveoxygenspeciesproductioninthefetalratheartinasexdependentmanner
AT cottrellelizabethc chronicdevelopmentalhypoxiaaltersmitochondrialoxidativecapacityandreactiveoxygenspeciesproductioninthefetalratheartinasexdependentmanner
AT traffordandreww chronicdevelopmentalhypoxiaaltersmitochondrialoxidativecapacityandreactiveoxygenspeciesproductioninthefetalratheartinasexdependentmanner
AT giussanidinoa chronicdevelopmentalhypoxiaaltersmitochondrialoxidativecapacityandreactiveoxygenspeciesproductioninthefetalratheartinasexdependentmanner
AT galliginalj chronicdevelopmentalhypoxiaaltersmitochondrialoxidativecapacityandreactiveoxygenspeciesproductioninthefetalratheartinasexdependentmanner

Ejemplares similares