Prostate-Specific Membrane Antigen Expression Is a Potential Prognostic Marker in Endometrial Adenocarcinoma

Mhawech‐Fauceglia, Paulette; Smiraglia, Dominic J.; Bshara, Wiam; Andrews, Chris; Schwaller, Juerg; South, Stacey A.; Higgs, Donald; Lele, Shashikant; Herrmann, Françoís; Odunsi, Kunle

doi:10.1158/1055-9965.epi-07-0511

Cited by 21 publications

(18 citation statements)

References 26 publications

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“…A recent microarray analysis on patient tissues revealed that strong AR expression was detected in benign prostate (83%), localized prostate cancer (100%), and lymph node metastasis (80%), but less (40%) in metastatic hormone-resistant prostate cancer (3). It was also noticed that two highly aggressive androgen-independent prostate cancer cell lines: DU145 and PC-3 are double-negative of AR and PSMA (29) and the loss of their AR and PSMA expression is due to epigenetic silencing by CpG island hypermethylation of their promoter regions (29–31). The DU145 and PC-3 lines were derived from brain and bone metastases of prostate cancer, whereas the AR(+), PSMA(+) LNCaP cell line was derived from a lymph node metastasis.…”

Section: Discussionmentioning

confidence: 99%

Prolonged androgen deprivation leads to downregulation of androgen receptor and prostate-specific membrane antigen in prostate cancer cells

Liu

Fulton

et al. 2012

International Journal of Oncology

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Emergence of androgen-independent cancer cells during androgen deprivation therapy presents a significant challenge to successful treatment outcomes in prostate cancer. Elucidating the role of androgen deprivation in the transition from an androgen-dependent to an androgen-independent state may enable the development of more effective therapeutic strategies against prostate cancer. Herein, we describe an in vitro model for assessing the effects of continuous androgen-deprivation on prostate cancer cells (LNCaP) with respect to the expression of two prostate-specific markers: the androgen receptor (AR) and prostate-specific membrane antigen (PSMA). Compared with androgen-containing normal growth medium, androgen-deprived medium apparently induced the concomitant downregulation of AR and PSMA over time. Decreased protein levels were confirmed by fluorescence imaging, western blotting and enzymatic activity studies. In contrast to the current understanding of AR and PSMA in prostate cancer progression, our data demonstrated that androgen-deprivation induced a decrease in AR and PSMA levels in androgen-sensitive LNCaP cells, which may be associated with the development of more aggressive disease-state following androgen deprivation therapy.

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Section: Discussionmentioning

confidence: 99%

Prolonged androgen deprivation leads to downregulation of androgen receptor and prostate-specific membrane antigen in prostate cancer cells

Liu

Fulton

et al. 2012

International Journal of Oncology

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“…Mhawech-Fauceglia et al (2008) assessed PSA expression in 49 endometrial adenocarcinoma tissue specimens. The study reported weak expression of PSA in the glands of normal endometrium and that 67.7% of EC tissues had no/weak staining for PSA.…”

Section: Endometrial Cancermentioning

confidence: 99%

“…High PSA mRNA levels were associated with stage I disease but not with tumour grade or subtype. Interestingly, multivariate survival analysis associated loss of PSA expression with worse disease-free survival (Mhawech-Fauceglia et al 2008). Circulating levels of PSA are increased in women with PCOS and are directly correlated with hyperandrogenism (Mardanian & Heidari 2011).…”

Section: Endometrial Cancermentioning

confidence: 99%

Evidence of androgen action in endometrial and ovarian cancers

Gibson

Simitsidellis

Collins

et al. 2014

Endocrine-Related Cancer

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Endometrial cancer (EC) and ovarian cancer are common gynaecological malignancies. The impact of androgen action in these cancers is poorly understood; however, there is emerging evidence to suggest that targeting androgen signalling may be of therapeutic benefit. Epidemiological evidence suggests that there is an increased risk of EC associated with exposure to elevated levels of androgens, and genetic variants in genes related to both androgen biosynthesis and action are associated with an increased risk of both EC and ovarian cancer. Androgen receptors (ARs) may be a potential therapeutic target in EC due to reported anti-proliferative activities of androgens. By contrast, androgens may promote growth of some ovarian cancers and anti-androgen therapy has been proposed. Introduction of new therapies targeting ARs expressed in EC or ovarian cancer will require a much greater understanding of the impacts of cell context-specific AR-dependent signalling and how ARs can crosstalk with other steroid receptors during progression of disease. This review considers the evidence that androgens may be important in the aetiology of EC and ovarian cancer with discussion of evidence for androgen action in normal and malignant endometrial and ovarian tissue.

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“…7,8), PSMA (9), and PSCA (10,11). Although these protein targets are frequently expressed by prostate cancer cells, they are also expressed by normal prostate tissue and may not be critical for the survival of the tumor; hence, their expression might be downregulated by cancer cells during the course of immune targeting or disease progression (12)(13)(14)(15)(16). Thus, there remains a need to identify immune targets of prostate cancer that are highly expressed in metastatic disease and/or critical to the progression of the disease, as simultaneous antigen targeting may be important to prevent the outgrowth of escape variants arising during the course of targeted therapy.…”

Section: Introductionmentioning

confidence: 99%

Expression and Immunotherapeutic Targeting of the SSX Family of Cancer–Testis Antigens in Prostate Cancer

et al. 2011

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Recent U.S. Food and Drug Administration approval of the first immunotherapy for prostate cancer encourages efforts to improve immune targeting of this disease. The synovial sarcoma X chromosome breakpoint (SSX) proteins comprise a set of cancer-testis antigens that are upregulated in MHC class I-deficient germline cells and in various types of advanced cancers with a poor prognosis. Humoral and cell-mediated immune responses to the SSX family member SSX2 can arise spontaneously in prostate cancer patients. Thus, SSX2 and other proteins of the SSX family may offer useful targets for tumor immunotherapy. In this study, we evaluated the expression of SSX family members in prostate cancer cell lines and tumor biopsies to identify which members might be most appropriate for immune targeting. We found that SSX2 was expressed most frequently in prostate cell lines, but that SSX1 and SSX5 were also expressed after treatment with the DNA demethylating agent 5-aza-2 0 -deoxycytidine. Immunohistochemical analysis of microarrayed tissue biopsies confirmed a differential level of SSX protein expression in human prostate cancers. Notably, SSX expression in patient tumor samples was restricted to metastatic lesions (5/22; 23%) and no expression was detected in primary prostate tumors examined (0/73; P < 0.001). We determined that cross-reactive immune responses to a dominant HLA-A2-specific SSX epitope (p103-111) could be elicited by immunization of A2/DR1 transgenic mice with SSX vaccines. Our findings suggest that multiple SSX family members are expressed in metastatic prostate cancers which are amenable to simultaneous targeting. Cancer Res; 71(21); 6785-95. Ó2011 AACR.

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Prostate-Specific Membrane Antigen Expression Is a Potential Prognostic Marker in Endometrial Adenocarcinoma

Cited by 21 publications

References 26 publications

Prolonged androgen deprivation leads to downregulation of androgen receptor and prostate-specific membrane antigen in prostate cancer cells

Prolonged androgen deprivation leads to downregulation of androgen receptor and prostate-specific membrane antigen in prostate cancer cells

Evidence of androgen action in endometrial and ovarian cancers

Expression and Immunotherapeutic Targeting of the SSX Family of Cancer–Testis Antigens in Prostate Cancer

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