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Target Concepts:
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Query: UMLS:C0282612 (
PIN
)
2,291
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Multiple genetic alterations are associated with prostate carcinogenesis. Tumor-suppressor genes phosphatase and tensin homolog deleted on chromosome 10 (Pten) and androgen upregulated gene 19 (U19), which encodes
ELL-associated factor 2
(
EAF2
), are frequently inactivated or downregulated in advanced prostate cancers. Previous studies showed that
EAF2
knockout caused tumors in multiple organs and
prostatic intraepithelial neoplasia
(
PIN
) in mice. However,
EAF2
-knockout mice did not develop prostate cancer even at 2 years of age. To further define the roles of
EAF2
in prostate carcinogenesis, we crossed the Pten+/- and EAF2+/- mice in the C57/BL6 background to generate
EAF2
-/-Pten+/-, Pten+/-,
EAF2
-/- and wild-type mice. The prostates from virgin male mice with the above four genotypes were analyzed at 7 weeks, 19 weeks and 12 months of age. Concomitant loss of
EAF2
function and inactivation of one Pten allele induced spontaneous prostate cancer in 33% of the mice. Prostatic tissues from intact
EAF2
-/- Pten+/- mice exhibited higher levels of phospho-Akt, -p44/42 and microvessel density. Moreover, phospho-Akt remained high after castration. Consistently, there was a synergistic increase in prostate epithelial proliferation in both intact and castrated
EAF2
-/-Pten+/- mice. Using laser-capture microdissection coupled with real-time reverse transcription-PCR, we confirmed that co-downregulation of
EAF2
and Pten occurred in >50% clinical prostate cancer specimens with Gleason scores of 8-9 (n=11), which is associated with poor prognosis. The above findings together demonstrated synergistic functional interactions and clinical relevance of concurrent
EAF2
and Pten downregulation in prostate carcinogenesis.
...
PMID:Concomitant loss of EAF2/U19 and Pten synergistically promotes prostate carcinogenesis in the mouse model. 2370 62
ELL-associated factor 2
(
EAF2
) is an androgen-responsive tumor suppressor frequently deleted in advanced prostate cancer that functions as a transcription elongation factor of RNA Pol II through interaction with the ELL family proteins.
EAF2
knockout mice on a 129P2/OLA-C57BL/6J background developed late-onset lung adenocarcinoma, hepatocellular carcinoma, B-cell lymphoma and high-grade
prostatic intraepithelial neoplasia
. In order to further characterize the role of
EAF2
in the development of prostatic defects, the effects of
EAF2
loss were compared in different murine strains. In the current study, aged
EAF2
(-/-) mice on both the C57BL/6J and FVB/NJ backgrounds exhibited mPIN lesions as previously reported on a 129P2/OLA-C57BL/6J background. In contrast to the 129P2/OLA-C57BL/6J mixed genetic background, the mPIN lesions in C57BL/6J and FVB/NJ
EAF2
(-/-) mice were associated with stromal defects characteristic of a reactive stroma and a statistically significant increase in prostate microvessel density. Stromal inflammation and increased microvessel density was evident in
EAF2
-deficient mice on a pure C57BL/6J background at an early age and preceded the development of the histologic epithelial hyperplasia and neoplasia found in the prostates of older
EAF2
(-/-) animals. Mice deficient in
EAF2
had an increased recovery rate and a decreased overall response to the effects of androgen deprivation.
EAF2
expression in human cancer was significantly down-regulated and microvessel density was significantly increased compared to matched normal prostate tissue; furthermore
EAF2
expression was negatively correlated with microvessel density. These results suggest that the
EAF2
knockout mouse on the C57BL/6J and FVB/NJ genetic backgrounds provides a model of
PIN
lesions associated with an altered prostate microvasculature and reactive stromal compartment corresponding to that reported in human prostate tumors.
...
PMID:Development of a reactive stroma associated with prostatic intraepithelial neoplasia in EAF2 deficient mice. 2426 Feb 46
Elongation factor for RNA polymerase II 2 (ELL2) and
ELL-associated factor 2
(
EAF2
) are two functionally related androgen responsive gene-encoded proteins with prostate tumor suppressor characteristics.
EAF2
and ELL2 have both been shown to be down-regulated in advanced prostate cancer, and mice with either
Eaf2
or
Ell2
deficiency developed murine
prostatic intraepithelial neoplasia
(mPIN), increased cellular proliferation and increased vascularity. Functional studies have revealed that
EAF2
and ELL2 can bind to each other and have similar roles in regulating cell proliferation, angiogenesis and prostate homeostasis. Here, cell line experiments showed that knockdown of
EAF2
or ELL2 induced an increase in proliferation and migration in C4-2 and 22Rv1 prostate cancer cells. Concurrent knockdown of
EAF2
and ELL2 increased proliferation and migration similarly to the loss of
EAF2
or ELL2 alone. Mice with homozygous deletion of
Ell2
or heterozygous deletion of
Eaf2
developed mPIN lesions characterized by increased epithelial proliferation, intraductal microvessel density, and infiltrating intraductal CD3-positive T-cells compared to wild-type controls. Mice with combined heterozygous deletion of
Eaf2
and
Ell2
developed mPIN lesions that were similar to those observed in mice with deficiency in Eaf2 or Ell2 alone. These results suggest that
EAF2
and ELL2 have similar functions and are likely to require each other in their regulation of prostate epithelial cell proliferation and migration in prostate cancer cells as well as their tumor suppressive properties in the murine prostate.
...
PMID:Concurrent EAF2 and ELL2 loss phenocopies individual EAF2 or ELL2 loss in prostate cancer cells and murine prostate. 3069 79
ELL-associated factor 1 is a transcription elongation factor that shares significant homology and functional similarity to the androgen-responsive prostate tumor suppressor
ELL-associated factor 2
. EAF2 is frequently down-regulated in advanced prostate cancer and Eaf2 deletion in the mouse induced the development of murine
prostatic intraepithelial neoplasia
. Here we show that similar to EAF2, EAF1 is frequently down-regulated in advanced prostate cancer. Co-downregulation of EAF1 and EAF2 occurred in 40% of clinical specimens with Gleason score >7. We developed and characterized a murine model of prostate-epithelial specific deletion of Eaf1 in the prostate and crossed it with our previously generated mouse with conventional deletion of Eaf2. The prostates of Eaf1 deletion mice displayed murine
prostatic intraepithelial neoplasia
lesions with increased proliferation and inflammation. Combined deletion of Eaf1 and Eaf2 in the murine model induced an increased incidence in mPIN lesions characterized by increased proliferation and CD3+ T cells and CD19+ B cells infiltration compared to individual deletion of either Eaf1 or Eaf2 in the murine prostate. These results suggest that EAF1 may play a tumor suppressive role in the prostate. Cooperation between EAF1 and EAF2 may be important for prostate maintaining prostate epithelial homeostasis, and concurrent loss of these two tumor suppressors may promote prostate tumorigenesis and progression.
...
PMID:Conditional Deletion of Eaf1 Induces Murine Prostatic Intraepithelial Neoplasia in Mice. 3122 79
Defining the cell of origin for prostatic carcinogenesis is fundamentally important for understanding the mechanisms leading to prostate cancer. Lineage tracing studies have demonstrated that luminal epithelial cells are capable of self-replication in multiple organs, including the adult murine prostate, and cell of prostate cancer origin studies have shown that while both the luminal and basal murine prostate epithelial cells are capable of neoplastic transformation, luminal cells are more efficient as the origin of prostate cancer.
ELL-associated factor 2
(
EAF2
) is an androgen responsive tumor suppressive protein expressed by prostate luminal epithelial cells that is frequently down-regulated in primary prostate tumors.
EAF2
knockdown induces prostate cancer cell proliferation and invasion
in vitro
and mice with
Eaf2
deficiency develop epithelial hyperplasia and murine
prostatic intraepithelial neoplasia
(mPIN) lesions. Here, we utilized an Eaf2 knockout, PSA-CreER
T2
transgenic model crossed with a fluorescent reporter line to show that
Eaf2
deficiency induces mPIN lesions derived from the luminal cell lineage. These results suggest that
PIN
lesions in the Eaf2 knockout mouse were derived from prostate luminal epithelial cells, further suggesting that the prostatic luminal epithelial cell is the major origin of prostate carcinogenesis.
...
PMID:EAF2 loss induces prostatic intraepithelial neoplasia from luminal epithelial cells in mice. 3221 50
