Basal epithelial stem cells are efficient targets for prostate cancer initiation

Lawson, Devon A.; Zong, Yang; Memarzadeh, Sanaz; Li, Xin; Huang, Jiaoti; Witte, Owen N.

doi:10.1073/pnas.0913873107

Cited by 240 publications

(235 citation statements)

References 36 publications

Supporting

Mentioning

218

Contrasting

Order By: Relevance

“…However, the ''initiation events'' were the basis for their selection as the epithelial source for these studies, since this instability facilitates induction of malignancy in response to CAFs and/or hormonal carcinogenesis; normal epithelial cells from primary specimens are not susceptible to carcinogenesis using these assays [13,38]. While there are key differences between BPH-1 cells and primary epithelial cells, including the methylation of the CD133, with silencing of up to 50% of BPH-1 cells [39], our data are supported by several previous studies in mice [4] and in primary human cells [3] showing that basal cells are a cell of origin of prostate cancer. In our study, we have extended these initial findings to further subfractionate the basal population and show the CD133 À cells are susceptible to tumorigenesis.…”

Section: Discussionsupporting

confidence: 77%

“…Most importantly, the finding that cells of origin of prostate cancer reside in the basal compartment is consistent with findings in human and murine tissues by Witte and coinvestigators who used high expression of Trop2 and CD49f to enrich for prostatic basal cells [3,4,33]. In addition to this, Wang et al showed luminal stem cells (CARNs) are also a cell of origin of prostate cancer in mouse prostate [1].…”

Section: Discussionsupporting

confidence: 71%

“…Although prostate cancer can arise from luminal (stem) cells [1,2], the concept that basal-enriched stem cells can also be cells of origin of prostate cancer is new and controversial [3,4]. In order to confirm that benign basal cells can be malignantly transformed, we used cells from the initiated but nontumorigenic BPH-1 epithelial cell line [20] that form tumors in recombination with tumor stroma (CAFs) [13].…”

Section: Selection Of Epithelial Stem Cellsmentioning

confidence: 99%

“…A minor luminal stem cell population was shown to be an efficient target for oncogenic transformation in mice [1], although this was not surprising given that mouse models of prostate cancer are commonly induced by luminal-specific promoters, including probasin and/or prostate-specific antigen (PSA) [2]. More surprisingly, murine and human basal epithelial stem cells expressing high Trop2 and CD49f were also susceptible to malignant transformation [3,4]. Altogether, these exemplary studies demonstrated that both basal and luminal cell types contain potential cells of origin of prostate cancer [1,3].…”

Section: Introductionmentioning

confidence: 99%

See 3 more Smart Citations

Human Epithelial Basal Cells Are Cells of Origin of Prostate Cancer, Independent of CD133 Status

et al. 2012

View full text Add to dashboard Cite

Normal prostatic epithelium is composed of basal and luminal cells. Prostate cancer can be initiated in both benign basal and luminal stem cells, but because basal cell markers are not expressed in patient tumors, the former result was unexpected. Since the cells of origin of prostate cancer are important therapeutic targets, we sought to provide further proof that basal stem cells have tumorigenic potential. Prostatic basal cells were enriched based on a2b1integrin hi expression and further enriched for stem cells using CD133 in nontumorigenic BPH-1 cells. Human embryonic stem cells (hESCs) were also used as a source of normal stem cells. To test their tumorigenicity, we used two alternate stromal-based approaches; (a) recombination with human cancer-associated fibroblasts (CAFs) or (b) recombination with embryonic stroma (urogenital mesenchyme) and treated host mice with testosterone and 17b-estradiol. Enriched a2b1integrin hi basal cells from BPH-1 cells resulted in malignant tumor formation using both assays of tumorigenicity. Surprisingly, the tumorigenic potential did not reside in the CD133 1 stem cells but was consistently observed in the CD133 2 population. CAFs also failed to induce prostatic tumors from hESCs. These data confirmed that benign human basal cells include cells of origin of prostate cancer and reinforced their importance as therapeutic targets. In addition, our data suggested that the more proliferative CD133 2 basal cells are more susceptible to tumorigenesis compared to the CD133 1 -enriched stem cells. These findings challenge the current dogma that normal stem cells and cells of origin of cancer are the same cell type(s).

show abstract

Section: Discussionsupporting

confidence: 77%

Section: Discussionsupporting

confidence: 71%

Section: Selection Of Epithelial Stem Cellsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 2 more Smart Citations

Human Epithelial Basal Cells Are Cells of Origin of Prostate Cancer, Independent of CD133 Status

et al. 2012

View full text Add to dashboard Cite

show abstract

“…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

View full text Add to dashboard Cite

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.

show abstract

PIM protein kinases regulate the level of the long noncoding RNA H19 to control stem cell gene transcription and modulate tumor growth

et al. 2020

View full text Add to dashboard Cite

The proviral integration site for Moloney murine leukemia virus (PIM) serine/threonine kinases have an oncogenic and prosurvival role in hematological and solid cancers. However, the mechanism by which these kinases drive tumor growth has not been completely elucidated. To determine the genes controlled by these protein kinases, we carried out a microarray analysis in T‐cell acute lymphoblastic leukemia (T‐ALL) comparing early progenitor (ETP‐ALL) cell lines whose growth is driven by PIM kinases to more mature T‐ALL cells that have low PIM levels. This analysis demonstrated that the long noncoding RNA (lncRNA) H19 was associated with increased PIM levels in ETP‐ALL. Overexpression or knockdown of PIM in these T‐ALL cell lines controlled the level of H19 and regulated the methylation of the H19 promoter, suggesting a mechanism by which PIM controls H19 transcription. In these T‐ALL cells, the expression of PIM1 induced stem cell gene expression (SOX2, OCT‐4, and NANOG) through H19. Identical results were found in prostate cancer (PCa) cell lines where PIM kinases drive cancer growth, and both H19 and stem cell gene levels. Small molecule pan‐PIM inhibitors (PIM‐i) currently in clinical trials reduced H19 expression in both of these tumor types. Importantly, the knockdown of H19 blocked the ability of PIM to induce stem cell genes in T‐ALL cells, suggesting a novel signal transduction cascade. In PCa, increases in SOX2 levels have been shown to cause both resistance to the androgen deprivation therapy (ADT) and the induction of neuroendocrine PCa, a highly metastatic form of this disease. Treatment of PCa cells with a small molecule pan‐PIM‐i reduced stem cell gene transcription and enhanced ADT, while overexpression of H19 suppressed the ability of pan‐PIM‐i to regulate hormone blockade. Together, these results demonstrate that the PIM kinases control the level of lncRNA H19, which in turn modifies stem cell gene transcription regulating tumor growth.

show abstract

Basal epithelial stem cells are efficient targets for prostate cancer initiation

Cited by 240 publications

References 36 publications

Human Epithelial Basal Cells Are Cells of Origin of Prostate Cancer, Independent of CD133 Status

Human Epithelial Basal Cells Are Cells of Origin of Prostate Cancer, Independent of CD133 Status

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

PIM protein kinases regulate the level of the long noncoding RNA H19 to control stem cell gene transcription and modulate tumor growth

Contact Info

Product

Resources

About