TRPM‐2 gene expression in normal rat ventral prostate following castration and exposure to diethylstilbestrol, flutamide, MK‐906 (finasteride), and coumarin

Russo, Paul; Warner, John; Huryk, Robert; Perez, G; Heston, Warren D.W.

doi:10.1002/pros.2990240504

Cited by 19 publications

(18 citation statements)

References 29 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Expression of TRPM-2 increases with androgen withdrawal (13,14) and has been used extensively as a marker of apoptotic activity in the prostate (13,(15)(16)(17). TRPM-2 mRNA for the intraprostatic dose responses was quantified using slot blots (Fig.…”

Section: Resultsmentioning

confidence: 99%

“…The effect on the prostate of finasteride and other 5␣-reductase inhibitors is a high degree of cell atrophy with minimal evidence of cell loss. Finasteride administration does not result in upregulation of TRPM-2 mRNA in the prostates of treated rats (6,7,16), although there was an increase in TRPM-2 protein using another 5␣-reductase inhibitor (3). Inhibition of apoptosis occurs at an intraprostatic testosterone concentration ‫ف(‬ 10 ng/g tissue) approximately half that seen with finasteride treatment and a DHT concentration half that of a normal intact rat.…”

Section: Discussionmentioning

confidence: 99%

See 1 more Smart Citation

Relative potency of testosterone and dihydrotestosterone in preventing atrophy and apoptosis in the prostate of the castrated rat.

Wright¹,

Thomas²,

Douglas³

et al. 1996

J. Clin. Invest.

116

View full text Add to dashboard Cite

Although dihydrotestosterone (DHT) is the principal androgen in the prostate, testosterone can also act as an androgen in this tissue. To determine the relative potencies of testosterone and DHT in preventing prostate regression, castrated rats were implanted for 4 d with varying doses of testosterone in the presence or absence of the 5 ␣ -reductase inhibitor finasteride. In the absence of finasteride, testosterone in the prostate is converted to DHT, creating an intraprostatic DHT dose response. In the presence of finasteride, this conversion is blocked, and an intraprostatic testosterone dose response is achieved. DHT was 2.4 times more potent than testosterone at maintaining normal prostate weight and duct lumen mass, a measure of epithelial cell function. The two androgens were equipotent at preventing DNA fragementation and expression of testosterone-repressed prostate message, two measures of apoptosis (cell death). The intraprostatic testosterone concentration that results from finasteride treatment in rats is sufficient to inhibit apoptosis but will not maintain normal epithelial cell activity. In conclusion, whereas DHT is more potent than testosterone at stimulating prostate epithelial cell function as measured by ductal mass, the two androgens are equipotent at preventing prostate cell death after castration. These results explain why finasteride causes prostate involution in the rat with minimal evidence of prostate cell death.

show abstract

Section: Resultsmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Relative potency of testosterone and dihydrotestosterone in preventing atrophy and apoptosis in the prostate of the castrated rat.

Wright¹,

Thomas²,

Douglas³

et al. 1996

J. Clin. Invest.

116

View full text Add to dashboard Cite

show abstract

“…The association between Ku70 and CLU͞XIP8 may correlate with the pathophysiology of CLU͞XIP8-related diseases and provides a useful clinical or environmental marker of IR, renal, or heart injury. The association of clu͞xip8 expression with apoptosis (i.e., TRPM-2, a marker for apoptosis) was first made when clu͞xip8 was identified and cloned as the major mRNA species induced during regression of the rat ventral prostate after castration (23). The association of this protein with apoptosis was confirmed in many other biological systems (19,22).…”

Section: B A1 A2mentioning

confidence: 97%

Nuclear clusterin/XIP8, an x-ray-induced Ku70-binding protein that signals cell death

Yang

Leskov

Hosley-Eberlein

et al. 2000

Proc. Natl. Acad. Sci. U.S.A.

273

291

View full text Add to dashboard Cite

Clusterin [CLU, a.k.a. TRPM-2, SGP-2, or ionizing radiation (IR)-induced protein-8 (XIP8)] was implicated in apoptosis, tissue injury, and aging. Its function remains elusive. We reisolated CLU͞XIP8 by yeast twohybrid analyses using as bait the DNA double-strand break repair protein Ku70. We show that a delayed (2-3 days), low-dose (0.02-10 Gy) IR-inducible nuclear CLU͞XIP8 protein coimmunoprecipitated and colocalized (by confocal microscopy) in vivo with Ku70͞Ku80, a DNA damage sensor and key double-strand break repair protein, in human MCF-7:WS8 breast cancer cells. Overexpression of nuclear CLU͞XIP8 or its minimal Ku70 binding domain (120 aa of CLU͞XIP8 C terminus) in nonirradiated MCF-7:WS8 cells dramatically reduced cell growth and colony-forming ability concomitant with increased G 1 cell cycle checkpoint arrest and increased cell death. Enhanced expression and accumulation of nuclear CLU͞XIP8-Ku70͞Ku80 complexes appears to be an important cell death signal after IR exposure.

show abstract

“…26 However, different opinions of the possible pro-and antiapoptotic activities for this protein and the ability of alternative splicing of its transcript to code for different isoforms prompted a meticulous series of different isoforms studies to assess the precise impact of CLU on apoptosis. Here, comparing with wild-type parental SKOV3 cells, SKOV3-CLU F and SKOV3-CLU T , in which the CLU protein constantly localized in the cytoplasm, showed no obvious changes in cellular growth.…”

Section: Subcellular Localization Of Clu Isforms In Skov3 Cells and Tmentioning

confidence: 99%

Roles of clusterin in progression, chemoresistance and metastasis of human ovarian cancer

Xue

Wang

et al. 2009

Intl Journal of Cancer

View full text Add to dashboard Cite

Clusterin (CLU) is a multivalent glycoprotein with ubiquitous tissue distribution. To address the possible differential functional roles assumed by different isoforms of CLU in the progression of human ovarian cancer, we constructed 2 human ovarian cancer cell models that represent examples of contradistinctive CLU expression levels. One is constitutively overexpressing different clusterin isoforms in SKOV3 cells by transfection of the 3 different expression vectors, another is silencing the intrinsically expressing clusterin in cisplatin-resistant human A2780-cis(CP70) tumor cells with the usage of shRNA-mediated CLU gene silencing. Then, the different cellular localization, biological effects, and functional roles played in tumor progression and drug resistances were studied. We found that (i) in the distinct cellular contexts of human ovarian carcinoma SKOV3 and CP70 cells assayed, sCLU is a central molecule in cell homeostasis that functions as a cytoprotective protein, whereas nCLU is proapoptotic; (ii) In SKOV3 cells, nuclear localization of the truncated CLU is NLS dependent, without which the pnCLU protein was sequestrated in cytoplasm to prevent cytotoxicity. (iii) sCLU plays a significant role in the development of the chemoresistance phenotype in ovarian cancer cells. Moreover, with the CLU-specific shRNA oligonucleotides, we successfully sensitized cells for chemotherapy, and inhibited cells' proliferation, migration and invasion. Collectively, our results reveal that, CLU gene expression might play a crucial role in ovarian cancer progression, adaptation and eventual resistance to chemotherapy through differential processing of CLU isoforms. Specifically, sCLU as an antiapoptotic protein, upregulated in an adaptive cell-survival manner by chemotherapy, confers resistance to various cell-death triggers. ' UICCKey words: clusterin; ovarian carcinoma; RNAi; chemoresistance; metastasis Ovarian cancer, the leading cause of death from gynecological malignancy, is the seventh most common malignancy in women worldwide and is the fourth leading cause of death from malignant disease among American women. In more than two thirds of the cases, patients show widespread metastatic dissemination at time of the initial presentation. 1 Because of advances in surgical management and chemotherapeutic options over the last 3 decades, the median survival rate for ovarian cancer patients has improved. Nevertheless, overall survival has not significantly changed. Cisplatin-based combination chemotherapy is initially an effective mechanism to arrest malignancy. However, after preliminary success in tumor regression, recurrence and resistance to further chemotherapeutic treatment often ensues. This amplification in drug resistance has also been correlated with the development of a broad cross-resistance in ovarian cancer to other unrelated chemotherapeutic compounds. 2 Therefore, shortages of suitable biologic markers, and limitations in the timely screening methods, early metastasis and resistance to anticancer chemother...

show abstract

TRPM‐2 gene expression in normal rat ventral prostate following castration and exposure to diethylstilbestrol, flutamide, MK‐906 (finasteride), and coumarin

Cited by 19 publications

References 29 publications

Relative potency of testosterone and dihydrotestosterone in preventing atrophy and apoptosis in the prostate of the castrated rat.

Relative potency of testosterone and dihydrotestosterone in preventing atrophy and apoptosis in the prostate of the castrated rat.

Nuclear clusterin/XIP8, an x-ray-induced Ku70-binding protein that signals cell death

Roles of clusterin in progression, chemoresistance and metastasis of human ovarian cancer

Contact Info

Product

Resources

About