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Spermatozoa Develop Molecular Machinery to Recover From Acute Stress

This study was designed to search for the possible mechanism(s) of male (in/sub)fertility by following the molecular response of spermatozoa on acute psychological stress (the most common stress in human society) and on a 20-h time-dependent recovery period. To mimic in vivo acute stress, the rats w...

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Autores principales: Starovlah, Isidora M., Radovic Pletikosic, Sava M., Tomanic, Tamara M., Medar, Marija LJ., Kostic, Tatjana S., Andric, Silvana A.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2022
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9329690/
https://www.ncbi.nlm.nih.gov/pubmed/35909555
http://dx.doi.org/10.3389/fendo.2022.896193
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author Starovlah, Isidora M.
Radovic Pletikosic, Sava M.
Tomanic, Tamara M.
Medar, Marija LJ.
Kostic, Tatjana S.
Andric, Silvana A.
author_facet Starovlah, Isidora M.
Radovic Pletikosic, Sava M.
Tomanic, Tamara M.
Medar, Marija LJ.
Kostic, Tatjana S.
Andric, Silvana A.
author_sort Starovlah, Isidora M.
collection PubMed
description This study was designed to search for the possible mechanism(s) of male (in/sub)fertility by following the molecular response of spermatozoa on acute psychological stress (the most common stress in human society) and on a 20-h time-dependent recovery period. To mimic in vivo acute stress, the rats were exposed to immobilization once every 3 h. The recovery periods were as follows: 0 (immediately after stress and 3 h after the light is on—ZT3), 8 (ZT11), 14 (ZT17), and 20 (ZT23) h after stress. Results showed that acute stress provoked effects evident 20 h after the end of the stress period. Numbers of spermatozoa declined at ZT17 and ZT23, while functionality decreased at ZT3 and ZT11, but recovered at ZT17 and ZT23. Transcriptional profiles of 91% (20/22) of tracked mitochondrial dynamics and functionality markers and 91% (20/22) of signaling molecules regulating both mitochondrial dynamics and spermatozoa number/functionality were disturbed after acute stress and during the recovery period. Most of the changes presented as increased transcription or protein expression at ZT23. The results of the principal component analysis (PCA) showed the clear separation of acute stress recovery effects during active/dark and inactive/light phases. The physiological relevance of these results is the recovered positive-acrosome-reaction, suggesting that molecular events are an adaptive mechanism, regulated by acute stress response signaling. The results of the PCA confirmed the separation of the effects of acute stress recovery on gene expression related to mitochondrial dynamics, cAMP, and MAPK signaling. The transcriptional patterns were different during the active and inactive phases. Most of the transcripts were highly expressed during the active phase, which is expected given that stress occurred at the beginning of the inactive phase. To the best of our knowledge, our results provide a completely new view and the first presentation of the markers of mitochondrial dynamics network in spermatozoa and their correlation with signaling molecules regulating both mitochondrial dynamics and spermatozoa number and functionality during recovery from acute stress. Moreover, the interactions between the proteins important for spermatozoa homeostasis and functionality (MFN2 and PRKA catalytic subunit, MFN2 and p38MAPK) are shown for the first time. Since the existing literature suggests the importance of semen quality and male fertility not only as the fundamental marker of reproductive health but also as the fundamental biomarkers of overall health and harbingers for the development of comorbidity and mortality, we anticipate our result to be a starting point for more investigations considering the mitochondrial dynamics markers or their transcriptional profiles as possible predictors of (in/sub)fertility.
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spelling pubmed-93296902022-07-29 Spermatozoa Develop Molecular Machinery to Recover From Acute Stress Starovlah, Isidora M. Radovic Pletikosic, Sava M. Tomanic, Tamara M. Medar, Marija LJ. Kostic, Tatjana S. Andric, Silvana A. Front Endocrinol (Lausanne) Endocrinology This study was designed to search for the possible mechanism(s) of male (in/sub)fertility by following the molecular response of spermatozoa on acute psychological stress (the most common stress in human society) and on a 20-h time-dependent recovery period. To mimic in vivo acute stress, the rats were exposed to immobilization once every 3 h. The recovery periods were as follows: 0 (immediately after stress and 3 h after the light is on—ZT3), 8 (ZT11), 14 (ZT17), and 20 (ZT23) h after stress. Results showed that acute stress provoked effects evident 20 h after the end of the stress period. Numbers of spermatozoa declined at ZT17 and ZT23, while functionality decreased at ZT3 and ZT11, but recovered at ZT17 and ZT23. Transcriptional profiles of 91% (20/22) of tracked mitochondrial dynamics and functionality markers and 91% (20/22) of signaling molecules regulating both mitochondrial dynamics and spermatozoa number/functionality were disturbed after acute stress and during the recovery period. Most of the changes presented as increased transcription or protein expression at ZT23. The results of the principal component analysis (PCA) showed the clear separation of acute stress recovery effects during active/dark and inactive/light phases. The physiological relevance of these results is the recovered positive-acrosome-reaction, suggesting that molecular events are an adaptive mechanism, regulated by acute stress response signaling. The results of the PCA confirmed the separation of the effects of acute stress recovery on gene expression related to mitochondrial dynamics, cAMP, and MAPK signaling. The transcriptional patterns were different during the active and inactive phases. Most of the transcripts were highly expressed during the active phase, which is expected given that stress occurred at the beginning of the inactive phase. To the best of our knowledge, our results provide a completely new view and the first presentation of the markers of mitochondrial dynamics network in spermatozoa and their correlation with signaling molecules regulating both mitochondrial dynamics and spermatozoa number and functionality during recovery from acute stress. Moreover, the interactions between the proteins important for spermatozoa homeostasis and functionality (MFN2 and PRKA catalytic subunit, MFN2 and p38MAPK) are shown for the first time. Since the existing literature suggests the importance of semen quality and male fertility not only as the fundamental marker of reproductive health but also as the fundamental biomarkers of overall health and harbingers for the development of comorbidity and mortality, we anticipate our result to be a starting point for more investigations considering the mitochondrial dynamics markers or their transcriptional profiles as possible predictors of (in/sub)fertility. Frontiers Media S.A. 2022-07-14 /pmc/articles/PMC9329690/ /pubmed/35909555 http://dx.doi.org/10.3389/fendo.2022.896193 Text en Copyright © 2022 Starovlah, Radovic Pletikosic, Tomanic, Medar, Kostic and Andric https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Endocrinology
Starovlah, Isidora M.
Radovic Pletikosic, Sava M.
Tomanic, Tamara M.
Medar, Marija LJ.
Kostic, Tatjana S.
Andric, Silvana A.
Spermatozoa Develop Molecular Machinery to Recover From Acute Stress
title Spermatozoa Develop Molecular Machinery to Recover From Acute Stress
title_full Spermatozoa Develop Molecular Machinery to Recover From Acute Stress
title_fullStr Spermatozoa Develop Molecular Machinery to Recover From Acute Stress
title_full_unstemmed Spermatozoa Develop Molecular Machinery to Recover From Acute Stress
title_short Spermatozoa Develop Molecular Machinery to Recover From Acute Stress
title_sort spermatozoa develop molecular machinery to recover from acute stress
topic Endocrinology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9329690/
https://www.ncbi.nlm.nih.gov/pubmed/35909555
http://dx.doi.org/10.3389/fendo.2022.896193
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