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Abstract

2,2′,4,4′ -tetrabromodiphenyl ether (BDE47), a well-known endocrine disruptor of the estrogen receptor (ER) is toxic to the mitochondria and spermatogenesis. This study aimed to explore the mechanism of BDE47 on spermatogenesis in mammals. Adult male Institute of Cancer Research (ICR) mice were gavaged daily with BDE47 (0, 1, or 10 mg/kg bw) for 8 weeks. Testicular weight, sperm production and motility, morphology of spermatogenic cells, nuclear respiratory factor 1 (Nrf1) level, and its expression in testes were determined. In vitro, cell viability, and key molecules in the ER-Nrf1-mitochondrial transcription factor A (Tfam)-mitochondria pathway in the immortalized mouse spermatogonia line (GC1) were determined at 48 h and 0–5 h after exposure; RNA interference (RNAi) was also performed to verify that the decreased Nrf1 was associated with mitochondrial dysfunction and the impaired viability of germ cells. The results indicated that BDE47 impaired testis weight and spermatogenesis, impaired mitochondria and germ cells, and decreased Nrf1 in the testes of mice. In vitro, after 48 h exposure, BDE47 reduced cell viability, Nrf1 protein, and mRNA of Nrf1, Tfam, ATP synthase subunit β (Atp5b), and cytochrome c oxidase subunit I (mt-CO1) in GC1 while also reducing mRNA of Nrf1 and Tfam promptly (from 1 to 5 h) after exposure. Furthermore, Nrf1 RNA interference decreased viability and mitochondrial function in GC1. These results indicated that BDE47 disrupts spermatogenesis in mice, probably by interfering with the ER-Nrf1-Tfam-mitochondria pathway, and Nrf1 is a target molecule of BDE47 estrogen receptor.

Keywords

BDE47 estrogen receptor mitochondria Nrf1 spermatogenesis

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References

Chen

Seifikar

Larocque

, et al. (2019) Using a multi-stage hESC model to characterize BDE-47 toxicity during neurogenesis. Toxicological Sciences 171(1): 221–234.

Eid

Ito

Horibe

, et al. (2018) A method for in vivo induction and ultrastructural detection of mitophagy in sertoli cells. Methods in Molecular Biology 1748: 103–112.

Gosavi

Knudsen

Birnbaum

, et al. (2013) Mimicking of estradiol binding by flame retardants and their metabolites: a crystallographic analysis. Environmental Health Perspectives 121(10): 1194–1199.

Hershkovitz

Kurolap

Gonzaga-Jauregui

, et al. (2019) A novel TUFM homozygous variant in a child with mitochondrial cardiomyopathy expands the phenotype of combined oxidative phosphorylation deficiency 4. Journal of Human Genetics 64(6): 589–595.

Huang

Cui

Guo

, et al. (2015) 2,2′,4,4′-Tetrabromodiphenyl ether disrupts spermatogenesis, impairs mitochondrial function and induces apoptosis of early leptotene spermatocytes in rats. Reproductive Toxicology 51: 114–124.

Huang

Wang

Cui

(2016) 2,2′,4,4′-Tetrabromodiphenyl ether injures cell viability and mitochondrial function of mouse spermatocytes by decreasing mitochondrial proteins Atp5b and Uqcrc1. Environmental Toxicology and Pharmacology 46: 301–310.

Kanaya

Bernal

Chang

, et al. (2019) Molecular mechanisms of polybrominated diphenyl ethers (BDE-47, BDE-100, and BDE-153) in human breast cancer cells and patient-derived xenografts. Toxicological Sciences 169(2): 380–398.

Klinge

(2020) Estrogenic control of mitochondrial function. Redox Biology 31: 101435.

Liu

Zhou

, et al. (2018) Foxg1 deletion impairs the development of the epithalamus. Molecular Brain 11(1): 5.

10.

Liu

Sun

, et al. (2011) In vitro profiling of endocrine disrupting potency of 2,2′,4,4′-tetrabromodiphenyl ether (BDE47) and related hydroxylated analogs (HO-PBDEs). Marine Pollution Bulletin 63(5–12): 287–296.

11.

Mima

Greenwald

Ohlander

(2018) Environmental toxins and male fertility. Current Urology Reports 19(7): 50.

12.

Orta-García

Ochoa-Martínez

ÁC

Varela-Silva

, et al. (2018) Polybrominated diphenyl ethers (PBDEs) levels in blood samples from children living in the metropolitan area of Guadalajara, Jalisco, Mexico. International Journal of Environmental Health Research 28(1): 90–101.

13.

Scaia

Volonteri

Czuchlej

, et al. (2015) Effect of estradiol on apoptosis, proliferation and steroidogenic enzymes in the testes of the toad Rhinella arenarum (Amphibia, Anura). General and Comparative Endocrinology 221: 244–254.

14.

Thomas

Zheng

Garces

, et al. (2014) Evidence based selection of commonly used RT-qPCR reference genes for the analysis of mouse skeletal muscle. PloS One 9(2): e88653.

15.

Zhuang

Pan

, et al. (2020) BDE-47 induced apoptosis in zebrafish embryos through mitochondrial ROS-mediated JNK signaling. Chemosphere 258: 127385.

16.

Zhang

Zhao

Jiang

, et al. (2011) Ultrastructural study on human placentae from women subjected to assisted reproductive technology treatments. Biology of Reproduction 85(3): 635–642.

17.

Zhang

Sun

, et al. (2013) Cytochrome P450 3A1 mediates 2,2′,4,4′-Tetrabromodiphenyl ether-induced reduction of spermatogenesis in adult rats. PloS one 8(6): e66301.

18.

Zhou

Nie

Prins

, et al. (2002) Localization of androgen and estrogen receptors in adult male mouse reproductive tract. Journal of Andrology 23(6): 870–881.

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2,2′,4,4′-Tetrabromodiphenyl ether disrupts spermatogenesis in mice by interfering with the ER-Nrf1-Tfam-mitochondria pathway

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