B-Myc is preferentially expressed in hormonally-controlled tissues and inhibits cellular proliferation

Gregory, Mark A.; Xiao, Qingqing; Lutterbach, Bart

doi:10.1038/sj.onc.1203851

Cited by 24 publications

(29 citation statements)

References 35 publications

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“…It was originally identified in the rat and named after its high expression in the brain (Ingvarsson et al 1988). Subsequently, an even higher expression was reported in the mouse epididymis where its expression is regulated by androgens (Gregory et al 2000, Cornwall et al 2001. Lower levels of expression have been detected in several other hormonally controlled tissues, including the adrenal, pituitary, prostate, ovary, and uterus, and the protein has also been detected in the hypothalamus and testis (Gregory et al 2000).…”

Section: Introductionmentioning

confidence: 92%

“…Subsequently, an even higher expression was reported in the mouse epididymis where its expression is regulated by androgens (Gregory et al 2000, Cornwall et al 2001. Lower levels of expression have been detected in several other hormonally controlled tissues, including the adrenal, pituitary, prostate, ovary, and uterus, and the protein has also been detected in the hypothalamus and testis (Gregory et al 2000). In addition, Bmyc is the predominant Myc family gene expressed during mouse preimplantation development (Domashenko et al 1997).…”

Section: Introductionmentioning

confidence: 99%

“…Due to their high degree of homology, it has been suggested that transcriptional regulation may be partly mediated by competition for the same binding partners with MYC (Resar et al 1993). BMYC has also been shown to be phosphorylated in the TAD at sites conserved with MYC, which further implies interactions with the same partners (Gregory et al 2000). In addition to b-HLH-LZ-mediated binding, two regions responsible for other interactions, namely MYC boxes I and II (MBI and MBII), are well conserved amongs all MYC proteins (Henriksson & Luscher 1996).…”

Section: Introductionmentioning

confidence: 99%

“…However, it contains a transcriptional activation domain (TAD), localizes mainly in the nucleus, and has been shown in vitro to initiate transcription, to inhibit neoplastic transformation, and to inhibit transcriptional activation regulated by MYC (Resar et al 1993, Asker et al 1995. BMYC has also been shown to inhibit cellular proliferation (Gregory et al 2000).…”

Section: Introductionmentioning

confidence: 99%

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Loss of Bmyc results in increased apoptosis associated with upregulation of Myc expression in juvenile murine testis

Turunen

Sipilä²,

Strauss³

et al. 2012

Reproduction

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Bmyc is a member of the Myc family of transcriptional regulators in the mouse and the rat. It is predominantly expressed in hormonally controlled tissues, with highest level of expression in the epididymis. The BMYC protein has been shown to function as a transcription factor in vitro and to inhibit MYC. To study the significance of BMYC in vivo, a Bmyc knockout (KO) mouse model was generated by homologous recombination. The KO mice were viable and fertile and did not display gross morphological or histological changes compared to the WT mice. However, the testes and the epididymides of the KO mice were smaller than those of the WT mice. Correspondingly, a tendency for a lower sperm concentration in the cauda epididymides of the KO mice was detected. The testosterone produced/testis was significantly reduced, and accordingly, the LH levels were increased in the KO mice. Also, the expression levels of Myc and several of its target genes were elevated in the testes of prepubertal KO mice, whereas no differences in gene expression levels were detected in adult mice. Associated with the increased Myc expression, more apoptotic spermatogenic cells were detected in the seminiferous tubules of the KO mice. In conclusion, our data suggest that Bmyc is a regulator of Myc in vivo and that overexpression of Myc in the developing testis leads to increased apoptosis of spermatogenic cells.

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Section: Introductionmentioning

confidence: 92%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 2 more Smart Citations

Loss of Bmyc results in increased apoptosis associated with upregulation of Myc expression in juvenile murine testis

Turunen

Sipilä²,

Strauss³

et al. 2012

Reproduction

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“…42 In adult mice, epididymal expression of c-Mos, A-raf, B-Raf, cRaf, L-Myc, N-Myc, B-Myc, C-Myc, c-Ret and Met have been identified. 43,44 Explanations for epididymal oncogene expression not being accompanied by typical oncogenic activity include: (i) the counter-balancing of antiproliferative gene expression (see above)-the expression of antiproliferative B-Myc protein exceeds that of pro-proliferative c-Myc; 45 (ii) the triggering, by high expression of some oncogenes (e.g., Ras family and C-Myc), of fail-safe mechanisms that induce senescence or apoptosis (see section on 'Intrinsic barriers to tumour formation'), instead of inducing proliferation; 46 (iii) the provision of protection against tumours by endogenous oncogenes. The expression of K-Ras, B-Raf and Myc, expressed in the adult human epididymis, 20 enhances the basal expression of the transcription factor Nrf2 (nuclear factor E2-related factor 2), which controls intracellular levels of ROS through an inducible antioxidant programme.…”

Section: Endogenous Protection Against Mutagenic Microenvironmentsmentioning

confidence: 99%

Why are epididymal tumours so rare?

Yeung¹,

Wang²,

Cooper³

2012

Asian J Androl

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Epididymal tumour incidence is at most 0.03% of all male cancers. It is an enigma why the human epididymis does not often succumb to cancer, when it expresses markers of stem and cancer cells, and constitutively expresses oncogenes, pro-proliferative and pro-angiogenic factors that allow tumour cells to escape immunosurveillance in cancer-prone tissues. The privileged position of the human epididymis in evading tumourigenicity is reflected in transgenic mouse models in which induction of tumours in other organs is not accompanied by epididymal neoplasia. The epididymis appears to: (i) prevent tumour initiation (it probably lacks stem cells and has strong anti-oxidative mechanisms, active tumour suppressors and inactive oncogene products); (ii) foster tumour monitoring and destruction (by strong immuno-surveillance and -eradication, and cellular senescence); (iii) avert proliferation and angiogenesis (with persistent tight junctions, the presence of anti-angiogenic factors and misplaced pro-angiogenic factors), which together (iv) promote dormancy and restrict dividing cells to hyperplasia. Epididymal cells may be rendered non-responsive to oncogenic stimuli by the constitutive expression of factors generally inducible in tumours, and resistant to the normal epididymal environment, which mimics that of a tumour niche promoting tumour growth. The threshold for tumour initiation may thus be higher in the epididymis than in other organs. Several anti-tumour mechanisms are those that maintain spermatozoa quiescent and immunologically silent, so the low incidence of cancer in the epididymis may be a consequence of its role in sperm maturation and storage. Understanding these mechanisms may throw light on cancer prevention and therapy in general.

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Prediction of Epigenetic and Stochastic Gene Expression Profiles of Late Effects after Radiation Exposure

Hirabayashi

Inoue

2012

Toxicology and Epigenetics

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B-Myc is preferentially expressed in hormonally-controlled tissues and inhibits cellular proliferation

Cited by 24 publications

References 35 publications

Loss of Bmyc results in increased apoptosis associated with upregulation of Myc expression in juvenile murine testis

Loss of Bmyc results in increased apoptosis associated with upregulation of Myc expression in juvenile murine testis

Why are epididymal tumours so rare?

Prediction of Epigenetic and Stochastic Gene Expression Profiles of Late Effects after Radiation Exposure

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