Cellular prostatic acid phosphatase: a protein tyrosine phosphatase involved in androgen-independent proliferation of prostate cancer

Veeramani, Suresh; Yuan, Ta Chun; Chen, Siu Ju; Lin, Fen Fen; Petersen, Juliette E.; Shaheduzzaman, Syed; Srivastava, Shiv; MacDonald, Richard G.; Lin, Ming Fong

doi:10.1677/erc.1.00950

Cited by 91 publications

(114 citation statements)

References 106 publications

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“…Additionally, EGF or heregulin had no effect on promoting the adhesive ability of C-33 cells (Supplementary Figure 4). We propose that in androgenindependent, AR-positive PCa cells, ErbB-2 protein is constitutively activated and/or elevated as seen in clinical samples due, in part, to the loss or null of cPAcP expression (Signoretti et al, 2000;Veeramani et al, 2005). In those advanced PCa cells, signal pathways initiated by highly activated ErbB-2 lead to a sustained activation of PYK2 and PYK2-mediated functions, which differs from the transient effect activated by ErbB ligands (Zrihan-Licht et al, 2000;van der Horst et al, 2005;Park et al, 2006).…”

Section: Discussionmentioning

confidence: 98%

“…Preliminary data showed that in PAcP siRNA oligomertransfected cells, tyrosyl phosphorylation of ErbB-2 and PYK2 increased, higher than that in the scrambled control siRNA oligomer-transfected cells (Veeramani et al, 2005). We established PAcP-knockdown stable subclones in C-33 cells and analysed their adhesion.…”

Section: Role Of Erbb-2 In Regulating the Pyk2 Activity And The Adhesmentioning

confidence: 98%

“…In androgen-independent human PCa cells, ErbB-2 is greatly activated by tyrosyl phosphorylation, at least in part due to the low or null expression of cellular prostatic acid phosphatase (cPAcP), a prostate-unique tyrosine phosphatase that dephosphorylates ErbB-2 . Increased ErbB-2 activity in PCa cells correlated with their androgen-independent proliferation, anchorage-independent growth and tumorigenicity (Igawa et al, 2002;Veeramani et al, 2005;Chen et al, 2007). ErbB-2 may also promote the adhesion of prostate cells (Vafa et al, 1998) while the underlying molecular basis is not understood.…”

Section: Introductionmentioning

confidence: 99%

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ErbB-2 via PYK2 upregulates the adhesive ability of androgen receptor-positive human prostate cancer cells

et al. 2007

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Aberrant regulation in the adhesive ability of cancer cells is closely associated with their metastatic activity. In this study, we examine the role of ErbB-2 in regulating the adhesive ability of androgen receptor (AR)-positive human prostate cancer (PCa) cells, the major cell population of PCa. Utilizing different LNCaP and MDA PCa2b cells as model systems, we found that ErbB-2 activity was correlated with PYK2 activity and adhesive ability in those cells. Increased ErbB-2 expression or activity in LNCaP C-33 cells enhanced PYK2 activation and cell adhesion, while the high PYK2 activity and the rapid adhesion of LNCaP C-81 cells were decreased by diminishing ErbB-2 expression or activity. Knockdown studies revealed the predominant role of ErbB-2 in regulating LNCaP C-81 cell adhesion. Coimmunoprecipitation showed that C-81 cells had increased interaction between ErbB-2 and PYK2. Elevated ErbB-2 activity in LNCaP cells correlated with increased ERK/MAPK activity and enhanced adhesive ability, which were abolished by the expression of K457A-PYK2 mutant or the treatment of PD98059, a MEK inhibitor. In summary, our data suggested that ErbB-2, via PYK2-ERK/MAPK, upregulates the adhesive ability of AR-positive human PCa cells.

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Section: Discussionmentioning

confidence: 98%

Section: Role Of Erbb-2 In Regulating the Pyk2 Activity And The Adhesmentioning

confidence: 98%

Section: Introductionmentioning

confidence: 99%

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ErbB-2 via PYK2 upregulates the adhesive ability of androgen receptor-positive human prostate cancer cells

et al. 2007

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“…PAP는 PSA와 같은 다른 전립선 암 표지자들보다 형태학적 특징과 높은 상관관계를 지니고 있기 때문에 [9], 이를 바탕으 로 PAP는 과거 수십년간 전립선 암의 표지자(marker)로서 혈 청검사와 조직검사에 널리 사용되어 왔다. 이런 표지자로서의 기능과는 다른 측면으로 전립선이 암이 되는 과정에서 cellular PAP 발현의 감소로 인해 탈 인산화가 제대로 일어나지 않아 세포 성장 신호가 지속적으로 유지되는 현상도 밝혀졌다 [20,22,23,38,42]. 즉, cellular PAP 발현의 감소가 전립선 암 발 생 원인중의 하나가 되고, 이 경우 PAP는 tumor supressor의 역할을 하는 것으로 추정된다 [42] (Table 1).…”

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“…이런 표지자로서의 기능과는 다른 측면으로 전립선이 암이 되는 과정에서 cellular PAP 발현의 감소로 인해 탈 인산화가 제대로 일어나지 않아 세포 성장 신호가 지속적으로 유지되는 현상도 밝혀졌다 [20,22,23,38,42]. 즉, cellular PAP 발현의 감소가 전립선 암 발 생 원인중의 하나가 되고, 이 경우 PAP는 tumor supressor의 역할을 하는 것으로 추정된다 [42] (Table 1). PAP의 전립선 특 이적 발현의 조절 기작 관련해서도 PAP promoter 부위에서의 cis-acting element들이 몇몇 보고된 바 있지만 [27,29,33,34,50] (Fig.…”

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Roles of Prostatic Acid Phosphatase in Prostate Cancer

Kong¹,

Lee²,

Byun³

2011

Journal of Life Science

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Prostatic acid phosphatase (PAP) is one of the widely used biomarkers in the diagnosis of prostate cancer. It was initially identified in 1935 and is the most abundant phosphatase in the human prostate. PAP is a prostate-specific enzyme that is synthesized in prostate epithelial cells. It belongs to the acid phosphatase group that shows enzymatic activity in acidic conditions. PAP is abundant in prostatic fluid and is thought to have a role in fertilization and oligospermia. It also has a potential role in reducing chronic pain. But one of the most apparent functions of PAP is the dephosphorylation of macromolecules such as HER-2 and PI3P that are involved in the ERK1/2 and MAPK pathways, which in turn leads to inhibition of cell growth and tumorigenesis. Currently, clinical trials using PAP DNA vaccine are underway and FDA-approved immunotherapy using PAP is commercially available. Despite these clinically important aspects, molecular mechanisms underlying PAP regulation are not fully understood. The promoter region of PAP was reported to be regulated by NF-κB, TNF-α, IL-1, androgen and androgen receptors. Here, the features of PAP gene and protein structures together with the function, regulation and roles of PAP in prostate cancer are discussed.

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Prostate cell lines as models for biomarker discovery: Performance of current markers and the search for new biomarkers

et al. 2014

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While the existing prostate cancer biomarkers and lysosomal proteins investigated here were not able to specifically differentiate between a panel of nonmalignant and prostate cancer cell lines, endosomal proteins showed some discriminatory capacity. LIMP-2 is a critical regulator of endosome biogenesis and the increased expression observed in prostate cancer cells indicated that other endosome related proteins may also be upregulated and could be investigated as novel biomarkers.

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Cellular prostatic acid phosphatase: a protein tyrosine phosphatase involved in androgen-independent proliferation of prostate cancer

Cited by 91 publications

References 106 publications

ErbB-2 via PYK2 upregulates the adhesive ability of androgen receptor-positive human prostate cancer cells

ErbB-2 via PYK2 upregulates the adhesive ability of androgen receptor-positive human prostate cancer cells

Roles of Prostatic Acid Phosphatase in Prostate Cancer

Prostate cell lines as models for biomarker discovery: Performance of current markers and the search for new biomarkers

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