Upregulated Autophagy in Sertoli Cells of Ethanol-Treated Rats Is Associated with Induction of Inducible Nitric Oxide Synthase (iNOS), Androgen Receptor Suppression and Germ Cell Apoptosis

Horibe, Akio; Eid, Nabil; Ito, Yuko; Hamaoka, Hitomi; Tanaka, Yoshihisa; Kondo, Yoichi

doi:10.3390/ijms18051061

Cited by 27 publications

(56 citation statements)

References 62 publications

(151 reference statements)

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“…In contrast, the induction of the meiosis gatekeeper STRA8 at the onset of meiosis is associated with a repression of autophagy and with ULK1 and TFEB downregulation ( Ferder et al, 2019 ). In Sertoli cells, TFEB mediates the initiation of autophagy upon exposure to toxins such as ethanol, in order to promote cell survival and sustain spermatogenesis ( Horibe et al, 2017 ). Interestingly, ULK1 directly relates autophagy with the mTOR pathway, which regulates many metabolic processes and essential cell functions in response to the nutrient and energy status of the cell ( Kim et al, 2011 ).…”

Section: Discussionmentioning

confidence: 99%

Accelerating Onset of Puberty Through Modification of Early Life Nutrition Induces Modest but Persistent Changes in Bull Sperm DNA Methylation Profiles Post-puberty

et al. 2020

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Section: Discussionmentioning

confidence: 99%

Accelerating Onset of Puberty Through Modification of Early Life Nutrition Induces Modest but Persistent Changes in Bull Sperm DNA Methylation Profiles Post-puberty

et al. 2020

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“…Morphologically, autophagy is characterized by the formation of isolation membranes that engulf a region of the cell forming early AVs or autophagosomes, which are mediated by LC3 (a specific autophagosome marker). The latter then fuse with lysosomes to form late AVs or autolysosomes, and the contents are degraded by cathepsins [3,4]. Autophagy may be a selective process in the clearance of damaged mitochondria (mitophagy) or excessive lipid droplets (lipophagy) in hepatocytes in association with exposure to acute or chronic ethanol intake.…”

Section: Introductionmentioning

confidence: 99%

“…Fourth, germ cells and spermatozoa, in particular, depend on lactate production by SCs via autophagy and glycolysis for viability and motility under normal and stressed conditions [10,11]. Fifth, autophagy upregulation has been found to be a prosurvival mechanism for cultured SCs upon exposure to heat stress [11] or high dose of ethanol [4].…”

Section: Introductionmentioning

confidence: 99%

“…Excessive alcohol intake has been reported to enhance germ cell apoptosis, resulting in infertility problems via mechanisms related to oxidative stress, upregulation of inducible nitric oxide synthase (iNOS) and mitochondrial dysfunction [4,5,6]. The authors recently reported that acute ethanol exposure upregulated autophagy in SCs of adult rats, and that this was accompanied by elevated germ cell apoptosis, androgen receptor (AR) suppression in testicular somatic cells and enhanced expression of iNOS in SCs [4]. The rat spermatogenic cycle includes 14 stages, each involving specific morphological and functional criteria (simplified into four groups consisting of stages I–VI, VII–VIII, IX–XI and XII–XIV) [12].…”

Section: Introductionmentioning

confidence: 99%

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Ethanol-Induced Autophagy in Sertoli Cells Is Specifically Marked at Androgen-Dependent Stages of the Spermatogenic Cycle: Potential Mechanisms and Implications

Horibe¹,

Eid

Ito

et al. 2019

IJMS

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In a recent study, we reported that acute ethanol exposure enhanced autophagy in Sertoli cells (SCs) of adult rats. However, further research is needed to clarify the specific spermatogenic stage exhibiting the highest autophagic response, the mechanisms behind such specificity, and the related relevance to sperm. This brief report provides results indicating that stages VII–VIII (androgen-dependent or spermiation stages) of the spermatogenic cycle exhibited more marked autophagic response in acute-ethanol treated rats (ETRs) than other stages based on suppression of androgen receptor (AR), analysis of microtubule-associated protein 1 light chain 3 (LC3) (an autophagosomal marker) immunostaining in SCs, double labeling of LC3 and lysosomal proteins and electron microscopy. Ultrastructural observations and TUNEL method revealed a notable presence of phagocytosed apoptotic germ cells and retained sperm in SCs of ETRs at these specific stages—a finding rarely observed in control testes. In addition, PTEN-induced putative kinase 1 ( PINK1) (a sensor of mitochondrial damage and mitophagy) and giant lipid droplets were found to have accumulated in SCs of ETRs at same stages. Our data show novel findings indicating that stages VII–VIII of the spermatogenic cycle exhibit high levels of autophagy, specifically under stress conditions, as expressed by the term autophagic stages. This stage-specific upregulation of autophagy in SCs may be related to AR suppression, mitochondrial damage, lipid accumulation, and phagocytosis of apoptotic cells. The phenomenon may be an essential part of ensuring the viability of SCs and supporting germ cells in toxic environments.

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“…receptor expression in testis (Horibe et al, 2017;Horibe, Eid, Ito, Otsuki, & Kondo, 2019). It has been also demonstrated that testicular proteins such as steroidogenic acute regulatory (StAR) protein (Jana, Jana, De, & Guha, 2010;Radhakrishnakartha, Appu, & Indira, 2014) and cytochrome P450 side-chain cleavage enzyme (P450scc) are lower expressed in ethanol animals (Radhakrishnakartha et al, 2014).…”

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Effect of ethanol on the changes in testicular protein expression in adult male rats

Tangsrisakda

Iamsaard

2020

Andrologia

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It is well known that ethanol consumption is the cause of liver disease (Kawaratani et al., 2013), gastric and colon cancers (Na & Lee, 2017), and renal dysfunctions (Kumar & Vasudevan, 2008). In addition, ethanol has a detrimental effect on sexual behaviour and fertility (Ávila et al., 2016; Gude, 2012). Previous studies showed that ethanol consumption could affect male reproductive system in adult male rats (Nishi et al., 2018; Yari, Karamian, Asadbegy, Hoseini, & Moazzami Farida, 2018). Previous study showed damaging of seminiferous tubules and reduced testosterone levels in sexually mature rats treated with ethanol for 14 consecutive days (Yari et al., 2018). These results implied early direct effect of ethanol on spermatogenesis and androgen production, but not real effect since the duration of total spermatogenesis in the rat is 50 days and epididymal transit takes approximately 7 days, respectively (Adler, 1996; Creasy, 1997). In both human and animal models, ethanol administration decreased normal sperm morphology, sperm concentration,

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Upregulated Autophagy in Sertoli Cells of Ethanol-Treated Rats Is Associated with Induction of Inducible Nitric Oxide Synthase (iNOS), Androgen Receptor Suppression and Germ Cell Apoptosis

Cited by 27 publications

References 62 publications

Accelerating Onset of Puberty Through Modification of Early Life Nutrition Induces Modest but Persistent Changes in Bull Sperm DNA Methylation Profiles Post-puberty

Accelerating Onset of Puberty Through Modification of Early Life Nutrition Induces Modest but Persistent Changes in Bull Sperm DNA Methylation Profiles Post-puberty

Ethanol-Induced Autophagy in Sertoli Cells Is Specifically Marked at Androgen-Dependent Stages of the Spermatogenic Cycle: Potential Mechanisms and Implications

Effect of ethanol on the changes in testicular protein expression in adult male rats

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