The effects of oxidative stress and intracellular calcium on mitochondrial permeability transition pore formation in equine spermatozoa

Zamira Gibb; Robert J. Aitken; Alecia R. Sheridan; Brandan Holt; Stephanie Waugh; Aleona Swegen

doi:10.1096/fba.2023-00051

FASEB BioAdvances (Jun 2024)

The effects of oxidative stress and intracellular calcium on mitochondrial permeability transition pore formation in equine spermatozoa

Zamira Gibb,
Robert J. Aitken,
Alecia R. Sheridan,
Brandan Holt,
Stephanie Waugh,
Aleona Swegen

Affiliations

Zamira Gibb: School of Environmental and Life Sciences, College of Engineering, Science and Environment The University of Newcastle Callaghan New South Wales Australia
Robert J. Aitken: School of Environmental and Life Sciences, College of Engineering, Science and Environment The University of Newcastle Callaghan New South Wales Australia
Alecia R. Sheridan: School of Environmental and Life Sciences, College of Engineering, Science and Environment The University of Newcastle Callaghan New South Wales Australia
Brandan Holt: Faculty of Health, School of Biomedical Sciences Queensland University of Technology Brisbane Queensland Australia
Stephanie Waugh: School of Environmental and Life Sciences, College of Engineering, Science and Environment The University of Newcastle Callaghan New South Wales Australia
Aleona Swegen: School of Environmental and Life Sciences, College of Engineering, Science and Environment The University of Newcastle Callaghan New South Wales Australia

DOI: https://doi.org/10.1096/fba.2023-00051
Journal volume & issue: Vol. 6, no. 6
pp. 143 – 158

Abstract

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Abstract The in vitro storage of stallion spermatozoa for use in artificial insemination leads to oxidative stress and imbalances in calcium homeostasis that trigger the formation of the mitochondrial permeability transition pore (mPTP), resulting in premature cell death. However, little is understood about the dynamics and the role of mPTP formation in mammalian spermatozoa. Here, we identify an important role for mPTP in stallion sperm Ca2+ homeostasis. We show that stallion spermatozoa do not exhibit “classical” features of mPTP; specifically, they are resistant to cyclosporin A‐mediated inhibition of mPTP formation, and they do not require exogenous Ca2+ to form the mPTP. However, chelation of endogenous Ca2+ prevented mPTP formation, indicating a role for intracellular Ca2+ in this process. Furthermore, our findings suggest that this cell type can mobilize intracellular Ca2+ stores to form the mPTP in response to low Ca2+ environments and that under oxidative stress conditions, mPTP formation preceded a measurable increase in intracellular Ca2+, and vice versa. Contrary to previous work that identified mitochondrial membrane potential (MMP) as a proxy for mPTP formation, here we show that a loss of MMP can occur independently of mPTP formation, and thus MMP is not an appropriate proxy for the detection of mPTP formation. In conclusion, the mPTP plays a crucial role in maintaining Ca2+ and reactive oxygen species homeostasis in stallion spermatozoa, serving as an important regulatory mechanism for normal sperm function, thereby contraindicating the in vitro pharmacological inhibition of mPTP formation to enhance sperm longevity.

Published in FASEB BioAdvances

ISSN: 2573-9832 (Online)
Publisher: Wiley
Country of publisher: United States
LCC subjects: Science: Biology (General)
Website: https://onlinelibrary.wiley.com/journal/25739832

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