Sox8 is a critical regulator of adult Sertoli cell function and male fertility

O'Bryan, Moira K; Takada, Shuji; Kennedy, Claire Louise; Scott, Greig; Harada, Satoru; Ray, Manas K.; Dai, Qunsheng; Wilhelm, Dagmar; Kretser, D. M. De; Eddy, Edward M.; Koopman, Peter; Mishina, Yuji

doi:10.1016/j.ydbio.2008.01.042

Cited by 96 publications

(88 citation statements)

References 37 publications

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“…Food intake and body weight over the five-day period are shown as percent of the respective values at the onset of the experiment. reduction in adipose tissues is a consequence of the progressive infertility observed in Sox8-deficient males at older ages (23), because alterations in the adipose tissue precede those in the testis and are also observed in females which do not exhibit any fertility problems. We thus have to conclude that the reduction of adipose tissues represents an independent phenotype in Sox8-deficient mice.…”

Section: Discussionmentioning

confidence: 99%

“…1A). On a C57Bl/6J background, the osteopenic phenotype of Sox8-deficient mice is much more pronounced (25) and Sox8-deficient males have been reported to develop progressive infertility with increasing age (23). To avoid confounding effects from the osteopenic phenotype and potential breeding problems, we performed our study with mice on a mixed background.…”

Section: Sox8-deficient Mice Have Reduced Fat Depots At Older Agesmentioning

confidence: 99%

“…Sox8-deficient mice were viable and able to produce offspring (22), although males developed sterility at older ages (23). Dramatic phenotypic manifestations are also not apparent in humans with SOX8 deletions.…”

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confidence: 99%

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Adult-onset degeneration of adipose tissue in mice deficient for the Sox8 transcription factor

Guth

Schmidt

Heß

et al. 2009

Journal of Lipid Research

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Section: Discussionmentioning

confidence: 99%

Section: Sox8-deficient Mice Have Reduced Fat Depots At Older Agesmentioning

confidence: 99%

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Adult-onset degeneration of adipose tissue in mice deficient for the Sox8 transcription factor

Guth

Schmidt

Heß

et al. 2009

Journal of Lipid Research

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“…Sox8 is an important transcription factor during spermatogenesis due to its crucial function in Sertoli cells (30,31). However, there are no reports of Sox8 expression in testicular germ cells.…”

Section: Resultsmentioning

confidence: 99%

Mrhl Long Noncoding RNA Mediates Meiotic Commitment of Mouse Spermatogonial Cells by Regulating Sox8 Expression

Kataruka

Akhade

Kayyar

et al. 2017

Molecular and Cellular Biology

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Long noncoding RNAs (lncRNAs) are important regulators of various biological processes, including spermatogenesis. Our previous studies have revealed the regulatory loop of mrhl RNA and Wnt signaling, where mrhl RNA negatively regulates Wnt signaling and gets downregulated upon Wnt signaling activation. This downregulation of mrhl RNA is important for the meiotic progression of spermatogonial cells. In our present study, we identified the transcription factor Sox8 as the regulatory link between mrhl RNA expression, Wnt signaling activation, and meiotic progression. In contrast to reports from other groups, we report the expression of Sox8 in germ cells and describe the molecular mechanism of Sox8 regulation by mrhl RNA during differentiation of spermatogonial cells. Binding of mrhl RNA to the Sox8 promoter is accompanied by the assembly of other regulatory factors involving Myc-Max-Mad transcription factors, corepressor Sin3a, and coactivator Pcaf. In the context of Wnt signaling, Sox8 directly regulates the expression of premeiotic and meiotic markers. Prolonged Wnt signaling activation in spermatogonial cells leads to changes in global chromatin architecture and a decrease in levels of stem cell markers.KEYWORDS Myc-Mad-Max, Sin3A, Sox8, Wnt signaling, mrhl RNA T he complexity of the eukaryotic genome has been attributed to its multifaceted regulatory networks. Over recent years, significant advancements in high-throughput analyses of the transcriptome have demonstrated the abundance of transcripts that do not code for proteins (noncoding RNAs [ncRNAs]). These ncRNAs are broadly classified as small and long noncoding RNAs. The small ncRNAs, such as microRNA (miRNA) and small interfering RNA (siRNA), play important roles in transcriptional and posttranscriptional gene regulation, while Piwi-associated RNAs (piRNAs) are involved in transposon regulation (1, 2). Another class is that of the long noncoding RNAs (lncRNAs), which are of various sizes between 200 bp and several kilobases (3). The role of lncRNAs in a plethora of functions, for example, dosage compensation (Xist and roX) (4, 5), genomic imprinting (Air and Kcnq1ot1) (6, 7), pluripotency (Evx1as and Hoxb5/6as) (8), cell differentiation and development (Fendrr, Bvht, Miat, Hotair, etc.) (9), nuclear architecture (NEAT1) (10), chromosome segregation (Concr) (11), immune response (lincRNA-EPS, EGOT) (12, 13), etc., have been characterized. lncRNAs bring about such copious functions by employment of diverse mechanisms such as translational inhibition (lincRNA-p21) (14), mRNA degradation (1/2-sbs RNAs) (15), RNA decoys (Gas5) (16)

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“…SOX9 and another group-E family member, SOX8, are both expressed in adult Sertoli cells, leading to the possibility that, like WT1 and RHOX5, these SOX transcription factors function in Sertoli cells to drive spermatogenesis. While this has not been addressed in the case of SOX9, recently O'Bryan et al (2008) examined this issue for SOX8. They found that disruption of the Sox8 gene elicits an age-dependent perturbation of spermatogenesis, characterized by sloughing of spermatocytes and round spermatids, failure in spermiation, disorganization of the spermatogenic cycle and disorientation and inappropriate placement of germ-cell types within the epithelium.…”

Section: (E) Sox8mentioning

confidence: 99%

Transcription and post-transcriptional regulation of spermatogenesis

Bettegowda

Wilkinson

2010

Phil. Trans. R. Soc. B

134

101

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Spermatogenesis in mammals is achieved by multiple players that pursue a common goal of generating mature spermatozoa. The developmental processes acting on male germ cells that culminate in the production of the functional spermatozoa are regulated at both the transcription and posttranscriptional levels. This review addresses recent progress towards understanding such regulatory mechanisms and identifies future challenges to be addressed in this field. We focus on transcription factors, chromatin-associated factors and RNA-binding proteins necessary for spermatogenesis and/ or sperm maturation. Understanding the molecular mechanisms that govern spermatogenesis has enormous implications for new contraceptive approaches and treatments for infertility.

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Sox8 is a critical regulator of adult Sertoli cell function and male fertility

Cited by 96 publications

References 37 publications

Adult-onset degeneration of adipose tissue in mice deficient for the Sox8 transcription factor

Adult-onset degeneration of adipose tissue in mice deficient for the Sox8 transcription factor

Mrhl Long Noncoding RNA Mediates Meiotic Commitment of Mouse Spermatogonial Cells by Regulating Sox8 Expression

Transcription and post-transcriptional regulation of spermatogenesis

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