Effect of Zearalenone-Induced Ferroptosis on Mice Spermatogenesis

Yajing Li; Zhendong Zhu; Haixiang Cui; Kexin Ding; Yong Zhao; Xiangping Ma; Adedeji Olufemi Adetunji; Lingjiang Min

doi:10.3390/ani12213026

Animals (Nov 2022)

Effect of Zearalenone-Induced Ferroptosis on Mice Spermatogenesis

Yajing Li,
Zhendong Zhu,
Haixiang Cui,
Kexin Ding,
Yong Zhao,
Xiangping Ma,
Adedeji Olufemi Adetunji,
Lingjiang Min

Affiliations

Yajing Li: College of Animal Science and Technology, Qingdao Agricultural University, Qingdao 266109, China
Zhendong Zhu: College of Animal Science and Technology, Qingdao Agricultural University, Qingdao 266109, China
Haixiang Cui: College of Animal Science and Technology, Qingdao Agricultural University, Qingdao 266109, China
Kexin Ding: College of Animal Science and Technology, Qingdao Agricultural University, Qingdao 266109, China
Yong Zhao: State Key Laboratory of Animal Nutrition, Institute of Animal Sciences, Chinese Academy of Agricultural Sciences, Beijing 100193, China
Xiangping Ma: College of Animal Science and Technology, Qingdao Agricultural University, Qingdao 266109, China
Adedeji Olufemi Adetunji: Department of Animal Sciences, North Carolina Agricultural and Technical State University, Greensboro, NC 27411, USA
Lingjiang Min: College of Animal Science and Technology, Qingdao Agricultural University, Qingdao 266109, China

DOI: https://doi.org/10.3390/ani12213026
Journal volume & issue: Vol. 12, no. 21
p. 3026

Abstract

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Male reproductive health is critically worsening around the world. It has been reported that the mycotoxin ZEA causes reproductive toxicity to domestic animals and affects spermatogenesis, thereby inhibiting male reproductive function. Ferroptosis is a newly identified type of programmed cell death that is different from apoptosis and it depends on iron accumulation and lipid peroxidation. Whether ferroptosis is linked to ZEA’s detrimental effect on spermatogenesis needs to be further explored. This study clarifies ferroptosis’s involvement in ZEA-induced damage on spermatogenesis. The reproductive injury model used in this study was induced by gavaging male mice in the ZEA treatment group with 30 μg/kg of ZEA for five weeks. Results show that ZEA treatment reduced mouse sperm motility and concentration, destroyed the structure of the seminiferous tubules of the testis, damaged the antioxidant defense system, and blocked spermatogenesis. Ferrostatin-1 (Fer-1) inhibition of ferroptosis partially alleviated ZEA-induced oligozoospermia in mice. In addition, ZEA treatment was found to activate a signaling pathway associated with ferroptosis in mouse testis. ZEA also downregulated the expression of Nrf2, SLC7A11, and GPX4, and decreased the protein expression of SLC7A11 and GPX4, resulting in the accumulation of lipid peroxides and an increase in the level of 4-HNE protein in the testis. Importantly, these changes were accompanied by an increase in the relative contents of Fe2+ and Fe3+. Iron accumulation and lipid peroxidation are the causes of ferroptosis in spermatogenic cells, leading to a decrease in sperm motility and concentration. While the administration of Fer-1 at 0.5 and 1 mg/kg also increased the expression of SLC7A11 and GPX4 proteins by upregulating Nrf2 expression, reducing iron accumulation, and reversing ZEA-induced ferroptosis, Fer-1 at 1.5 mg/kg had the best repairing effect for all parameters. In conclusion, ZEA-induced ferroptosis may be mediated by a notable reduction in Nrf2, SLC7A11 and GPX4 expression levels. Overall, ferroptosis is a novel therapeutic target for mitigating ZEA-induced reproductive toxicity.

Published in Animals

ISSN: 2076-2615 (Online)
Publisher: MDPI AG
Country of publisher: Switzerland
LCC subjects: Agriculture: Animal culture: Veterinary medicine; Science: Zoology
Website: http://www.mdpi.com/journal/animals/

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