2001
DOI: 10.1016/s0925-4773(00)00551-7
|View full text |Cite
|
Sign up to set email alerts
|

Generation of a prostate epithelial cell-specific Cre transgenic mouse model for tissue-specific gene ablation

Abstract: To facilitate the elucidation of the genetic events that may play an important role in the development or tumorigenesis of the prostate gland, we have generated a transgenic mouse line with prostate-specific expression of Cre recombinase. This line, named PB-Cre4, carries the Cre gene under the control of a composite promoter, ARR2PB which is a derivative of the rat prostate-specific probasin (PB) promoter. Based on RT-PCR detection of Cre mRNA in PB-Cre4 mice or Cre-mediated activation of LacZ activity in PB-… Show more

Help me understand this report

Search citation statements

Order By: Relevance

Paper Sections

Select...
1
1
1
1

Citation Types

11
381
0

Year Published

2002
2002
2018
2018

Publication Types

Select...
9

Relationship

0
9

Authors

Journals

citations
Cited by 351 publications
(398 citation statements)
references
References 24 publications
11
381
0
Order By: Relevance
“…However, its targeting to non-prostate tissues has also been reported. 24 Recently, an osteocalcin promoter was used in a novel strategy for cotargeting both tumor epithelial and bone stromal cells in gene therapy of androgen-independent CaP bone metastasis. 25,26 Current gene therapy clinical trials of prostate cancer utilize a combination of the only two available targeting vector genes with both the rat probasin promoter sequence and human PSA promoter sequence 13,20,27 without the benefit of prior testing in an appropriate transgenic animal model.…”
Section: Psp94 Gene Promoter/enhancer Region-directed Sv40 Tag Expresmentioning
confidence: 99%
“…However, its targeting to non-prostate tissues has also been reported. 24 Recently, an osteocalcin promoter was used in a novel strategy for cotargeting both tumor epithelial and bone stromal cells in gene therapy of androgen-independent CaP bone metastasis. 25,26 Current gene therapy clinical trials of prostate cancer utilize a combination of the only two available targeting vector genes with both the rat probasin promoter sequence and human PSA promoter sequence 13,20,27 without the benefit of prior testing in an appropriate transgenic animal model.…”
Section: Psp94 Gene Promoter/enhancer Region-directed Sv40 Tag Expresmentioning
confidence: 99%
“…The development of murine prostate cancer models, however, is severely hindered by a lack of spontaneous tumor development within the mouse prostate. Several models of murine prostate cancer exist, including those generated through the use of prostate tissue specific promoters to drive expression of the SV40 small t and/or large T antigens [4,5], or the development of transgenics with conditional knockouts [6] or hemizygous knockouts [7]. Another model, the mouse prostate reconstitution model (MPR) developed by retro-viral infection of murine urogenital sinus for the expression of activated oncogenes [8], has been effectively used in immunotherapy studies of prostate cancer [9,10].…”
Section: Introductionmentioning
confidence: 99%
“…It has been well known that the mouse prostate undergoes extensive branching morphogenesis during the first 15 days of life. 30 Probasin promoter-driven Cre excision is barely detectable in the prostate during the first 15 days of neonatal mice, 37 which could be the reason that we did not observe the changes in the pes-ERaKO prostate development. In order to further define the role of epithelial ERa in the early prostatic development, the use of NKX3.1 Cre could be an ideal strategy, because its Cre activity begins to express at embryonic stage E17.5 in a prostatic epithelium-specific manner.…”
Section: Discussionmentioning
confidence: 80%
“…The promoter of probasin is well characterized and widely applied in many animal models. [37][38][39] The expression of probasin Cre (PB-Cre) is prostatic epithelial-specific and is postnatal and gradually increased with highest expression in the lateral lobe, followed by the VP, and then the DP and AP. 37,38 Therefore, PB-Cre can specifically knock out the floxed ERa gene in prostate epithelial cells (pes-ERaKO).…”
Section: Generation and Genotyping Of Pes-erako Micementioning
confidence: 99%