Differential expression of glucose transporter GLUT8 during mouse spermatogenesis

Gómez, O.; Romero, Amparo; Terrado, José; Mesonero, José E.

doi:10.1530/rep.1.00750

Cited by 45 publications

(55 citation statements)

References 30 publications

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“…SLC2A8 is a recently cloned member of the class III facilitative transporters and is expressed in the blastocyst stage embryo, heart, skeletal muscle, brain, spleen, prostate, intestine, and testis (Carayannopoulos et al 2000, Doege et al 2000, Gomez et al 2006. Currently, we have confirmed that SLC2A8 is highly expressed in the Leydig cells as well as in the innermost cells of the seminiferous tubules in the mouse testis and localizes in the acrosome, midpiece, and principal piece of the mouse sperm (Kim & Moley 2007).…”

Section: Introductionsupporting

confidence: 53%

“…However, factors involved in the development of male infertility with insulin-dependent diabetes are poorly understood. SLC2A8 is highly expressed in the testis (Carayannopoulos et al 2000, Doege et al 2000, Gomez et al 2006, Kim & Moley 2007) and as such may play a major role in substrate delivery to develop sperm. These observations led us to focus on SLC2A expression in diabetic male mice.…”

Section: Discussionmentioning

confidence: 99%

“…We have also reported that SLC2A9 protein expression was significantly increased in the kidney and liver from STZinduced diabetic mice compared with non-diabetic mice (Keembiyehetty et al 2006). Although SLC2A8 (Ibberson et al 2002, Schurmann et al 2002, Chen et al 2003, Gomez et al 2006, Kim & Moley 2007) and SLC2A9 (Kim & Moley 2007) are expressed in the testis and sperm, it is not known whether their expression or localization is altered in the diabetic male reproductive system or not. The objective of this study was to determine whether sperm quality, fertilization capacity, and subsequent embryo development are altered in diabetic male mice and whether differences in facilitative glucose transporter (SLC2A) expression in the testis and sperm exist.…”

Section: Introductionmentioning

confidence: 94%

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Paternal effect on embryo quality in diabetic mice is related to poor sperm quality and associated with decreased glucose transporter expression

Kim

Moley

2008

Reproduction

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The objective of this study was to determine whether sperm quality, fertilization capacity, and subsequent embryo development are altered in diabetic male mice and whether differences in facilitative glucose transporter (GLUT; now known as solute carrier family 2, SLC2A) expression in the testis and sperm exist. Using two type 1 diabetic mouse models, SLC2A expression in the testis and sperm was determined by western immunoblotting and immunofluorescence staining. To address sperm quality and fertilization capacity, computer-assisted sperm analysis and in vitro fertilization were performed. SLC2A1, SLC2A3, and SLC2A5 did not change in expression in the testes or sperm between diabetic and non-diabetic mice. SLC2A8 and SLC2A9b were less expressed in the testes of both diabetic models versus controls. SLC2A9a was not expressed in the Akita testis or sperm when compared with strain-matched controls. 3b-hydroxysteroid dehydrogenase (HSD3B) expression was significantly decreased in the Leydig cells from the diabetic mice. Sperm concentration and motility were significantly lower in both the diabetics when compared with the control. These parameters normalized in Akita diabetic males treated with insulin. In addition, fertilization rates were significantly lower in the Akita group (17.9%) and the streptozotocin (STZ)-injected male group (43.6%) when compared with the normal group (88.8%). Interestingly, of the fertilized zygotes, embryo developmental rates to the blastocyst stage were lower in both diabetic models (7.1% Akita and 50.0% STZ) when compared with controls (71.7%). Male diabetes may cause male subfertility by altering steroidogenesis, sperm motility, and SLC2A expression. This is the first study to link a paternal metabolic abnormality to a sperm effect on cell division and subsequent embryonic development. Reproduction (2008) 136 313-322

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Section: Introductionsupporting

confidence: 53%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 94%

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Paternal effect on embryo quality in diabetic mice is related to poor sperm quality and associated with decreased glucose transporter expression

Kim

Moley

2008

Reproduction

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“…SLC2A4 is well known as the important insulin-sensitive transporter and is expressed in insulin-responsive tissues [6,7]. SLC2A8 is a recently cloned member of the class III facilitative transporters and is expressed in the heart, skeletal muscle, brain, spleen, prostate, intestine, and testis and in the developing embryo at blastocyst stage [8][9][10][11]. We have shown that SLC2A8 is an insulin-sensitive transporter in mouse blastocyst and testis [8,12].…”

Section: Introductionmentioning

confidence: 99%

Regulation of Facilitative Glucose Transporters and AKT/MAPK/PRKAA Signaling via Estradiol and Progesterone in the Mouse Uterine Epithelium1

Kim

Moley

2009

Biology of Reproduction

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Adequate uterine glucose metabolism is an essential part of embryo implantation and the development of an adequate uterofetal environment. However, expression of facilitative glucose transporters (GLUTs [solute transporter family SLC2A]) and AKT/MAPK/PRKAA (PRKAA) signaling has not been described in the mouse uterine cells, to our knowledge. The objective of this study was to determine the hormonal regulation of SLC2A protein expression and AKT/MAPK/PRKAA signaling in the mouse uterine epithelial cells during estrous cycles and periimplantation periods. SLC2As 1, 4, 8, and 9B were highly expressed in the luminal and glandular epithelia of estrous stage. In metestrous and diestrous stages, expression of SLC2As 1, 4, 8, and 9B was lower than that in proestrous stage. Levels of activated phospho-AKT (p-AKT), p-MAPK3, and p-MAPK1 also varied during the estrous cycle. Estrogen and progesterone injection in an ovariectomized mouse (delayed implantation model) resulted in a decrease and an increase, respectively, in expression of GLUTs in the luminal epithelial cells of the uterus.

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“…8,[22][23][24][25] Mammalian testes and spermatozoa are known to utilize various glucose transporters (GLUTs) [26][27][28][29] that serve to transport glucose and/or fructose for critical sperm cell metabolism and function. 27,28,30,31 We have recently shown that CSC induces oxidative stress, DNA damage, and seminiferous tubule cell apoptosis in mice, ultimately leading to altered sperm motility. We also examined the effect of CSC exposure on a spermatocyte cell line, which represents the premeiotic stage of spermatogenesis (eg, primary spermatocytes).…”

Section: Introductionmentioning

confidence: 99%

Modeling the Effect of Cigarette Smoke on Hexose Utilization in Spermatocytes

et al. 2015

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We set out to determine whether the addition of an aryl hydrocarbon receptor (AHR) antagonist has an effect on glucose/ fructose utilization in the spermatocyte when exposed to cigarette smoke condensate (CSC). We exposed male germ cells to 5 and 40 mg/mL of CSC + 10 mmol/L of AHR antagonist at various time points. Immunoblot expression of specific glucose/ fructose transporters was compared to control. Radiolabeled uptake of 2-deoxyglucose (2-DG) and fructose was also performed. Spermatocytes utilized fructose nearly 50-fold more than 2-DG. Uptake of 2-DG decreased after CSC þ AHR antagonist exposure. Glucose transporters (GLUTs) 9a and 12 declined after CSC þ AHR antagonist exposure. Synergy between CSC and the AHR antagonist in spermatocytes may disrupt the metabolic profile in vitro. Toxic exposures alter energy homeostasis in early stages of male germ cell development, which could contribute to later effects explaining decreases in sperm motility in smokers.

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Differential expression of glucose transporter GLUT8 during mouse spermatogenesis

Cited by 45 publications

References 30 publications

Paternal effect on embryo quality in diabetic mice is related to poor sperm quality and associated with decreased glucose transporter expression

Paternal effect on embryo quality in diabetic mice is related to poor sperm quality and associated with decreased glucose transporter expression

Regulation of Facilitative Glucose Transporters and AKT/MAPK/PRKAA Signaling via Estradiol and Progesterone in the Mouse Uterine Epithelium1

Modeling the Effect of Cigarette Smoke on Hexose Utilization in Spermatocytes

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