Bmi-1 Is a Crucial Regulator of Prostate Stem Cell Self-Renewal and Malignant Transformation

Lukacs, Rita U.; Memarzadeh, Sanaz; Wu, Hong; Witte, Owen N.

doi:10.1016/j.stem.2010.11.013

Cited by 245 publications

(221 citation statements)

References 52 publications

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“…Aberrant expression of BMI1 is associated with the bypass of senescence, increased proliferation, and oncogenic phenotypes such as increased migration, invasion, and metastasis of cancer cells (14,15,18,25,43). BMI1 is also known to promote CSC properties and therapy resistance in breast and prostate cancers (17,44). Hence, the therapeutic targeting of BMI1 can potentially help in the prevention, treatment, and recurrence of breast, prostate, and possibly other cancers.…”

Section: Discussionmentioning

confidence: 99%

MicroRNA-31 Is a Transcriptional Target of Histone Deacetylase Inhibitors and a Regulator of Cellular Senescence

Cho

Dimri

2015

Journal of Biological Chemistry

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Background: Histone deacetylase inhibitor (HDACi) inhibits expression of polycomb group proteins and can differentially regulate expression of miRNAs. Results: HDACi up-regulated expression of miR-31, which down-regulated BMI1 and induced cellular senescence. Conclusion: miR-31 is a novel target of HDACi, and is a novel regulator of cellular senescence. Significance: HDACi can be used to induce miR-31, which in turn can cause senescence in cancer cells.

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Section: Discussionmentioning

confidence: 99%

MicroRNA-31 Is a Transcriptional Target of Histone Deacetylase Inhibitors and a Regulator of Cellular Senescence

Cho

Dimri

2015

Journal of Biological Chemistry

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“…The lineage relationship between basal and luminal cells has recently been under heavy debate. Although renal capsule or subcutaneous transplantation experiments support the traditional view that basal cells have the ability to regenerate the prostate gland by repopulating all prostate epithelial lineages [1][2][3][4] , evidence from the rescued explants of p63-null mice suggest that luminal cells can sustain a prostate structure independently of basal cells 5 . In addition, with transgenic reporter mice, a population of castration-resistant Nkx3.1-expressing luminal cells has been shown to be able to generate not only luminal cells but also other prostatic epithelial lineages 6 .…”

mentioning

confidence: 97%

“…Generally, it is believed that basal cells are likely the cellular origin of prostate cancer 3,4,10,11 . However, it is also known that prostate cancer always displays a remarkable luminal phenotype including the amplification of luminal cells rather than basal cells and overproduction of luminal-derived prostate-specific protein (PSA) 12,13 .…”

mentioning

confidence: 99%

Symmetrical and asymmetrical division analysis provides evidence for a hierarchy of prostate epithelial cell lineages

et al. 2014

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Although symmetrical and asymmetrical divisions of stem cells have been extensively studied in invertebrate and mammalian neural epithelia, their role remains largely unknown in mammalian non-neural epithelial development, regeneration and tumorigenesis. Here, using basal and luminal cell-specific markers and cell lineage tracing transgenic mice, we report that in developing prostatic epithelia, basal and luminal cells exhibit distinct division modes. While basal cells display both symmetric and asymmetric divisions leading to different cell fates, luminal cells only exhibit symmetrical divisions. Examination of cell division modes in prostate-specific Pten-null mice indicates that both luminal and basal cells can be cellular origins for prostate cancer. Furthermore, analysis of Sox2-expressing cells in p63 and Pten-null mice suggests that basal cells contribute to the luminal population and tumorigenesis. These findings provide direct evidence for the existence of a hierarchy of epithelial cell lineages during prostate development, regeneration and tumorigenesis.

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“…14,18e24 Recently, increasing evidence has linked EMT to stem cell properties, indicating that the key molecules inducing EMT may also promote a stem or progenitor cellelike phenotype with capabilities of self-renewal and increased tumorigenicity. 25e27 PC stem-like cells express proteins such as Oct4, Sox2, Nanog, Nestin, CD133, CD44, 28,29 and BMI1, 30 of which BMI1 is a member of the polycombrepressive complex and a crucial suppressor of prosenescence mediated by p16 INK4a , p14 ARF , and p15 INK4b . 31e33 Twist1 has been recently shown to induce BMI1 expression through a direct binding to the BMI1 promoter, 34 thus linking stem-like properties of cancer cells to EMT.…”

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confidence: 99%

Jak2-Stat5a/b Signaling Induces Epithelial-to-Mesenchymal Transition and Stem-Like Cell Properties in Prostate Cancer

Talati

Ellsworth

et al. 2015

The American Journal of Pathology

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Active Stat5a/b predicts early recurrence and disease-specific death in prostate cancer (PC), which both typically are caused by development of metastatic disease. Herein, we demonstrate that Stat5a/b induces epithelial-to-mesenchymal transition (EMT) of PC cells, as shown by Stat5a/b regulation of EMT marker expression (Twist1, E-cadherin, N-cadherin, vimentin, and fibronectin) in PC cell lines, xenograft tumors in vivo, and patient-derived PCs ex vivo using organ explant cultures. Jak2-Stat5a/b signaling induced functional end points of EMT as well, indicated by disruption of epithelial cell monolayers and increased migration and adhesion of PC cells to fibronectin. Knockdown of Twist1 suppressed Jak2-Stat5a/beinduced EMT properties of PC cells, which were rescued by re-introduction of Twist1, indicating that Twist1 mediates Stat5a/b-induced EMT in PC cells. While promoting EMT, Jak2-Stat5a/b signaling induced stemlike properties in PC cells, such as sphere formation and expression of cancer stem cell markers, including BMI1. Mechanistically, both Twist1 and BMI1 were critical for Stat5a/b induction of stem-like features, because genetic knockdown of Twist1 suppressed Stat5a/b-induced BMI1 expression and sphere formation in stem cell culture conditions, which were rescued by re-introduction of BMI1. By using human prolactin knock-in mice, we demonstrate that prolactin-Stat5a/b signaling promoted metastases formation of PC cells in vivo. In conclusion, our data support the concept that Jak2-Stat5a/b signaling promotes metastatic progression of PC by inducing EMT and stem cell properties in PC cells. Most prostate cancer (PC)erelated deaths are because of development of metastatic disease. A central process in metastatic dissemination of PC is epithelial-to-mesenchymal transition (EMT), during which cancer cells attain more motile and invasive properties, invade through the basement membrane, and survive in systemic circulation. 1e3 Extravasation at distant organ sites is followed by adhesion of cancer cells to extracellular matrix proteins, such as fibronectin, 4e6 leading to formation of premetastatic niches and subsequent formation of macroscopic metastases. 7e9 Hallmarks of EMT in PC include disruption of adherens junctions through down-regulation of E-cadherin, 2 concomitant with a development of a migratory phenotype and up-regulation of mesenchymal markers, such as N-cadherin, vimentin, and fibronectin. 10,11 Loss of E-cadherin results from mutations, DNA methylation, or silencing of E-cadherin promoter

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Bmi-1 Is a Crucial Regulator of Prostate Stem Cell Self-Renewal and Malignant Transformation

Cited by 245 publications

References 52 publications

MicroRNA-31 Is a Transcriptional Target of Histone Deacetylase Inhibitors and a Regulator of Cellular Senescence

MicroRNA-31 Is a Transcriptional Target of Histone Deacetylase Inhibitors and a Regulator of Cellular Senescence

Symmetrical and asymmetrical division analysis provides evidence for a hierarchy of prostate epithelial cell lineages

Jak2-Stat5a/b Signaling Induces Epithelial-to-Mesenchymal Transition and Stem-Like Cell Properties in Prostate Cancer

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