Literature DB >> 8806197

Prostate cancer--biology of metastasis and its clinical implications.

J T Dong1, C W Rinker-Schaeffer, T Ichikawa, J C Barrett, J T Isaacs.   

Abstract

Prostate cancer is one of the most commonly diagnosed cancers and is a major cause of cancer death in men. Although the majority of the diagnosed prostate cancers will remain localized and never produce clinical symptoms during the lifetime of the host, a subset of these cancers will progress to a more malignant state requiring therapeutic intervention. Acquisition of metastatic ability by prostatic cancer cells is the most lethal aspect of prostatic cancer progression. Once this has occurred, definitive therapy is required before the initially localized metastatic cells escape from the prostate. At present, metastatic prostate cancer is incurable. Therefore, there is an urgent need to develop molecular markers that can be used to predict the metastatic potential of prostate cancers. Using somatic cell hybridization, we have demonstrated that acquisition of metastatic ability requires both the loss of metastasis-suppressor function(s) and the activation of oncogenes. In further studies using micro-cell-mediated chromosomal transfer, we located genes on human chromosome, 8, 10cen-q23, 11p11.2-13, and 17pter-q23, which, when introduced into rat prostatic cancer cells, are capable of suppressing their metastatic ability without affecting their tumorigenicity or growth rate in vivo. Initially we focused upon the human chromosome 11p11.2-13 region to clone metastasis-suppressor gene(s) positionally. One such gene, termed KAI-1, encodes a membrane glycoprotein. KAI-1 has been mapped to the p11.2 region of human chromosome 11 by fluorescence in-situ hybridization analysis. Expression of KAI-1 has been detected in all normal human tissues thus far tested, including prostate tissue. When introduced into rat metastatic prostatic cancer cells, KAI-1 significantly suppressed the metastasis without affecting the tumor growth rate. KAI-1 expression is high in human normal prostate and benign prostatic hyperplasia but is dramatically lower in cancer cell lines derived from metastatic prostate tumors.

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Year:  1996        PMID: 8806197     DOI: 10.1007/bf00186898

Source DB:  PubMed          Journal:  World J Urol        ISSN: 0724-4983            Impact factor:   4.226


  63 in total

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4.  Down modulation of fibronectin messenger RNA in metastasizing rat prostatic cancer cells revealed by differential hybridization analysis.

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7.  Localization of metastasis suppressor gene(s) for rat prostatic cancer to the long arm of human chromosome 10.

Authors:  N Nihei; T Ichikawa; Y Kawana; H Kuramochi; H Kugo; M Oshimura; A M Killary; C W Rinker-Schaeffer; J C Barrett; J T Isaacs
Journal:  Genes Chromosomes Cancer       Date:  1995-10       Impact factor: 5.006

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Journal:  Int J Cancer       Date:  1991-04-01       Impact factor: 7.396

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10.  Identification of the motility-related protein (MRP-1), recognized by monoclonal antibody M31-15, which inhibits cell motility.

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  13 in total

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2.  Dr. Coffey's visionary contributions to urological research in China and Japan.

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3.  Focal adhesion kinase (FAK) phosphorylation is not required for genistein-induced FAK-beta-1-integrin complex formation.

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Review 4.  Molecular pathology of tumor metastasis. I. Predictive pathology.

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5.  Frequent loss of KAI1 expression in squamous and lymphoid neoplasms. An immunohistochemical study of archival tissues.

Authors:  J Geradts; R Maynard; M J Birrer; D Hendricks; S L Abbondanzo; K M Fong; J C Barrett; D P Lombardi
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Review 6.  Prostate cancer: PET with 18F-FDG, 18F- or 11C-acetate, and 18F- or 11C-choline.

Authors:  Hossein Jadvar
Journal:  J Nucl Med       Date:  2010-12-13       Impact factor: 10.057

7.  Prospective evaluation of 18F-NaF and 18F-FDG PET/CT in detection of occult metastatic disease in biochemical recurrence of prostate cancer.

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8.  Role of Imaging in Prostate Cancer.

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Review 9.  Molecular imaging of prostate cancer with 18F-fluorodeoxyglucose PET.

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10.  Unusual uptakes on 18F-fluorocholine positron emission tomography/computed tomography (PET/CT): a retrospective study of 368 prostate cancer patients referred for a biochemical recurrence or an initial staging.

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