Review of allelic loss and gain in prostate cancer

Bova, G. Steven; Isaacs, William B.

doi:10.1007/bf00184607

Cited by 60 publications

(33 citation statements)

References 46 publications

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“…The frequent finding of gain on chromosome 12q is in good agreement with a recent publication (Sattler et al, 1999) reporting on frequent copy number gains in human prostate cancer. Losses on 8p and 6q as well as gains on 8q and of chromosome 7, which were considered to be typical aberrations for prostate cancer (for review see Bova and Isaacs, 1996), were also detected in primary tumours investigated in this study, but at a lower frequency. This fact can be partly explained by the smaller number of cases in our study compared to the literature data.…”

Section: Tumour Progression In Prostate Cancer 205supporting

confidence: 52%

“…Application of CGH and fluorescence in situ hybridization (FISH) to primary tumours of prostatic adenocarcinomas revealed consistent changes on chromosomes 7, 8p, 10, 13q, 16, 17 and 18q (Brothman et al, 1994;Macoska et al, 1994;Matsuyama et al, 1994;Joos et al, 1995;Qian et al, 1995;Visakorpi et al, 1995;Bova and Isaacs, 1996;Cher et al, 1996;Huang et al, 1996;Deubler et al, 1997). However, cytogenetic changes in prostatic intraepithelial neoplasias (PIN) which are considered as premalignant lesions and which are often present besides the invasive tumour are only poorly characterized cytogenetically (Alers et al, 1995;Qian et al, 1995;Zitzelsberger et al, 1998).…”

mentioning

confidence: 98%

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Chromosomal changes during development and progression of prostate adenocarcinomas

Zitzelsberger

Engert²,

Walch

et al. 2001

Br J Cancer

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Summary Chromosomal copy number changes were investigated in 16 prostate carcinomas, 12 prostatic intraepithelial neoplasias (PIN; 4 low-grade and 8 high-grade) adjacent to the invasive tumour areas, and 5 regional lymph node metastases. For this purpose, comparative genomic hybridization (CGH) was performed and a copy number karyotype for each histomorphological entity was created. CGH on microdissected cells from non-neoplastic glands was carried out on 3 different cases to demonstrate the reliability of the overall procedure. None of the non-neoplastic tissue samples revealed chromosome copy number changes. In PIN areas, chromosomal imbalances were detected on chromosomes 7, 8q, Xq (gains), and on 4q, 5q, 8p, 13q and 18q (losses). In the primary tumours, recurrent (at least 25% of cases) gains on chromosomes 12q and 15q, and losses on 2q, 4q, 5q, Xq, 13q and 18q became apparent. Losses on 8p and 6q as well as gains on 8q and of chromosome 7 were also detected at lower frequencies than previously reported. The pooled CGH data from the primary carcinomas revealed a novel region of chromosomal loss on 4q which is also frequently affected in other tumour entities like oesophageal adenocarcinomas and is supposed to harbour a new tumour suppressor gene. Gains on chromosome 9q and of chromosome 16 and loss on chromosome 13q were observed as common aberrations in metastases and primary tumours. These CGH results indicate an accumulation of chromosomal imbalances during the PIN-carcinoma-metastasis sequence and an early origin of tumour-specific aberrations in PIN areas.

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Section: Tumour Progression In Prostate Cancer 205supporting

confidence: 52%

mentioning

confidence: 98%

Chromosomal changes during development and progression of prostate adenocarcinomas

Zitzelsberger

Engert²,

Walch

et al. 2001

Br J Cancer

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“…Molecular genetic studies have identified multiple genetic changes in prostate cancers (5,6). These include loss or gain of specific regions or whole chromosomes, gene amplification, and structural alterations that lead to overexpression or activation of oncogenes or inactivation of putative tumor suppressor genes (5,6).…”

mentioning

confidence: 99%

“…These include loss or gain of specific regions or whole chromosomes, gene amplification, and structural alterations that lead to overexpression or activation of oncogenes or inactivation of putative tumor suppressor genes (5,6). For example, frequent allelic loss of the LPL gene (8p22) in prostate cancer suggests that a tumor suppressor gene (or genes) is located in this region (7)(8)(9)(10)(11).…”

mentioning

confidence: 99%

Loss of p53 and c-myc Overrepresentation in Stage T2-3N1-3M0 Prostate Cancer are Potential Markers for Cancer Progression

et al. 2002

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To determine whether genetic changes are markers of cancer progression and patient survival in Stage T 2-3 N 1-3 M 0 prostatic carcinoma, we compared 26 patients who died of tumor relapse after prostatectomy and lymphadenectomy (case group) with 26 matched patients who were alive at the time of the matched case's death (control group). Nine unmatched cases were also included in this study. In 37 cases, paired primary tumors (119 foci) and lymph node metastases (114 foci) were available for study. Fluorescence in situ hybridization (FISH) with centromere-specific probes for chromosomes 7, 8, and 17 and region-specific probes for D7S486 (7q31), c-myc (8q24), LPL (8p22), and p53 (17p13) was performed on available primary carcinomas and lymph node metastases. In primary tumor foci, ؉7q31, ؊8p22, ؉c-myc, substantial additional increases of myc (AI-c-myc), and ؊p53 were observed in 65%, 74%, 43%, 29%, and 31% of foci, respectively. AI-c-myc was strongly associated with higher cancer Gleason score (P ‫؍‬ .003). Heterogeneity of genetic changes was frequently observed among multiple cancer foci. Lymph node metastases of prostate cancer usually shared genetic changes with paired primary tumors. In addition, the genetic change pattern with ؊8p, ؉c-myc or AI-c-myc, ؉7q, and ؉p53 was slightly higher in lymph node metastases (22%) than in primary tumors (6%) (P ‫؍‬ .08). In matched case and control patients, simultaneous gain of 7q31 (؉7q31) and CEP7 (؉CEP7) was identified in 59% and 68% of specimens for case and control groups, respectively (P ‫؍‬ .48). Loss of 8p22 (؊8p22) was identified in 77% and 69% of specimens for case and control groups, respectively (P ‫؍‬ 1.0). Simultaneous gain of c-myc (؉c-myc) and CEP8 (؉CEP8) without overt additional increase of c-myc copy number relative to CEP8 copy number, was identified in 38% and 54% of specimens for case and control groups, respectively (P ‫؍‬ .27). AI-c-myc was identified in 54% and 23% of specimens for case and control groups, respectively (odds ratio ‫؍‬ 3.0, P ‫؍‬ .06). Loss of p53 (؊p53) was identified in 46% and 15% of specimens for case and control groups, respectively (odds ratio Prostate cancer is the most common malignancy and the second leading cause of cancer death in men in the United States (1). Patients with pelvic lymph node metastases of prostatic carcinoma, but no evidence of systemic progression are commonly classified as having Stage T 2-3 N 1-3 M 0 prostate cancer (2). These cancers have an indeterminate natural history (3). Choosing different types of therapy (radiation, surgery, or hormonal therapy) for these

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“…LOH involving specific chromosomes has been demonstrated in prostate carcinomas. 75 The most commonly observed LOH involved 16q and 10q, with 30% of the examined cases demonstrating losses. 76 Additional LOH loci in prostate cancer included 3p, 7q, 9q, 10p, 10q, 11p, 13q, 16p, 16q, 17p and 18q.…”

Section: Hormone-refractory Prostate Cancermentioning

confidence: 99%

Hormone-refractory prostate cancer: a multi-step and multi-event process

Taille

Vacherot²,

Salomon³

et al. 2001

Prostate Cancer Prostatic Dis

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Since the pioneering studies of Huggins in 1941, it has been known that prostate cancer cells, like certain normal epithelial cells, can chronically depend on a critical level of androgenic stimulation for their continuous growth and survival. The entire issue of the development of resistance to androgen ablation therapy for metastatic prostate cancer is based on the fact that a portion of cells can survive without androgen stimulation. The cell mechanism of androgen independent status is unclear. For some authors, a portion of the cells present within a patient with a prostate cancer before therapy is naturally androgen independent (selection hypothesis). However, this hypothesis does not consider gene alteration during prostate cancer natural history and probably hormone-refractory prostate cancer (HRPC) is due to a multi-step and multi-event process. In this literature review, different cell pathways that lead to HRPC are described.

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Review of allelic loss and gain in prostate cancer

Cited by 60 publications

References 46 publications

Chromosomal changes during development and progression of prostate adenocarcinomas

Chromosomal changes during development and progression of prostate adenocarcinomas

Loss of p53 and c-myc Overrepresentation in Stage T2-3N1-3M0 Prostate Cancer are Potential Markers for Cancer Progression

Hormone-refractory prostate cancer: a multi-step and multi-event process

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