FGF8 over-expression in prostate cancer is associated with decreased patient survival and persists in androgen independent disease

Dorkin, Trevor J.; Robinson, Mary C.; Marsh, Colin; Bjartell, Anders; Neal, David E.; Leung, Hing Y.

doi:10.1038/sj.onc.1202624

Cited by 133 publications

(122 citation statements)

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“…Previous expression studies, including work from our own centre, have assayed total FGF8 levels in clinical material (Leung et al, 1996;Dorkin et al, 1999;Valve et al, 2001). Data concerning FGF8 correlation with clinical parameters, however, have been conflicting and may reflect differences in splice form utilisation (Leung et al, 1996;Tanaka et al, 1998;Dorkin et al, 1999;Valve et al, 2001). Transcript studies of isoform expression are limited by reliance on semiquantitative RT -PCR on heterogeneous frozen materials.…”

Section: Discussionmentioning

confidence: 99%

“…These blocks included samples of placenta as well as testis, breast cancer and prostate cancer known to express FGF8 (Tanaka et al, 1998;Dorkin et al, 1999). A dilution of 1 : 500 gave the optimal signals.…”

Section: Immunohistochemistrymentioning

confidence: 99%

“…The peptide was first implicated in prostate cancer when FGF8 mRNA was found to be expressed in prostate cancer cell lines (Ghosh et al, 1996;Schmitt et al, 1996). In clinical prostate cancer, overexpression of FGF8 mRNA was found to be associated with high-grade and late-stage disease (Leung et al, 1996;Dorkin et al, 1999). Subsequent work has shown that distinct isoforms of FGF8 possess different transforming potential.…”

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confidence: 99%

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FGF8 isoform b expression in human prostate cancer

et al. 2003

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Overexpression of fibroblast growth factor 8 (FGF8) mRNA has been previously described in prostate cancer. Of its four isoforms, FGF8b is thought to be the most important in carcinogenesis. We hypothesised that immunodetection of FGF8b in archival prostate cancer specimens is of potential prognostic value. Using a selected cohort of prostate tumours from transurethral (n ¼ 30) and radical prostatectomies (n ¼ 59), an optimised protocol for FGF8b immunoreactivity was used to corroborate expression with clinical parameters. No expression was observed in benign prostates (n ¼ 10). In prostate cancer, immunoreactivity was localised to the malignant epithelium with weak signals in the adjacent stroma. Expression of FGF8b in stage T1 and T2 cancers were 40 and 67%, respectively. In contrast, FGF8b expression was present in 94% of T3 and 100% of T4 cancers. By histological grade, FGF8b was found in 41% of low-grade cancers (Gleason score 4 -6), 60% of intermediate-grade cancers (Gleason score 7 and 92% of high-grade cancers (Gleason score 8 -10). The intensity of expression was significantly associated with stage (P ¼ 0.0004) and grade (Po0.0001) of disease. We further hypothesised that FGF8b overexpression resulted from enhanced transcription and translation rather than from abnormalities involving the FGF8 gene locus. This was tested by means of fluorescent in situ hybridisation in 20 cancer specimens to map the FGF8 gene locus. FGF8 gene copy number in benign and malignant nuclei was found to be similar (2.3370.57 and 2.070.81, respectively P ¼ 0.51). Based on these findings, we propose a multicentre study on cohorts of patients to further evaluate FGF8b as a potential prognostic marker in prostate cancer.

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Section: Discussionmentioning

confidence: 99%

Section: Immunohistochemistrymentioning

confidence: 99%

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confidence: 99%

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FGF8 isoform b expression in human prostate cancer

et al. 2003

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Section: Introductionmentioning

confidence: 99%

“…Clinical studies revealed that FGF8b overexpression was found in the majority of prostate cancer (40-80%) (Dorkin et al, 1999;Gnanapragasam et al, 2002Gnanapragasam et al, , 2003Tanaka et al, 2002;Zhong et al, 2006) and breast cancer (B70-100%) . Moreover, its overexpression was clinically associated with disease progression (mainly staging and grading), poor prognosis, poor survival (Dorkin et al, 1999;Valve et al, 2001), and potentially metastasis in prostate cancer (Gnanapragasam et al, 2003;Valta et al, 2008). Although the molecular mechanisms for FGF8b overexpression in prostate and breast cancers are not fully understood, the human sex hormone androgen (Tanaka et al, 1992) is known to play a key role, even in the case of breast cancer (Castellano et al, 2010Park et al, 2010 (in addition to prostate cancer (Gnanapragasam et al, 2002)).…”

Section: Introductionmentioning

confidence: 99%

FGF8b oncogene mediates proliferation and invasion of Epstein–Barr virus-associated nasopharyngeal carcinoma cells: implication for viral-mediated FGF8b upregulation

et al. 2010

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The fibroblast growth factor 8b (FGF8b) oncogene is known to be primarily involved in the tumorigenesis and progression of hormone-related cancers. Its role in other epithelial cancers has not been investigated, except for esophageal cancer, in which FGF8b overexpression was mainly found in tumor biopsies of male patients. These observations were consistent with previous findings in these cancer types that the male sex-hormone androgen is responsible for FGF8b expression. Nasopharyngeal carcinoma (NPC) is a highly metastatic cancer of head and neck commonly found in Asia. It is etiologically associated with Epstein-Barr Virus (EBV) infection, inflammatory tumor microenvironment and relatively higher male predominance. Here, we reported for the first time that FGF8b is overexpressed in this EBV-associated non-hormone-related cancer of the head and neck, NPC. More importantly, overexpression of FGF8b mRNA and protein was detected in a large majority of NPC tumors from both male and female genders, in addition to multiple NPC cell lines. We hypothesized that FGF8b overexpression may contribute to NPC tumorigenesis. Using EBV-associated NPC cell lines, we demonstrated that specific knockdown of FGF8b by small interfering RNA inhibited cell proliferation, migration and invasion, whereas exogenous FGF8b stimulated these multiple phenotypes. Further mechanistic investigation revealed that in addition to NF-jB signaling (a major inflammatory signaling pathway known to be activated in NPC), an important EBV oncoprotein, the latent membrane protein 1 (LMP1), was found to be a direct inducer of FGF8b overexpression in NPC cells, whereas androgen (testosterone) has minimal effect on FGF8b expression in EBVassociated NPC cells. In summary, our study has identified LMP1 as the first viral oncogene capable of directly inducing FGF8b (an important cellular oncogene) expression in human cancer cells. This novel mechanism of viral-mediated FGF8 upregulation may implicate a new role of oncoviruses in human carcinogenesis.

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aFGF immunoreactivity in prostate cancer and its co-localization with bFGF and FGF8

et al. 1999

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Fibroblast growth factors (FGFs) have been implicated in the development of numerous malignancies including prostate cancer. In a pilot study it has been shown that FGF8 mRNA is up‐regulated in prostate cancer. The aim of the present study was to determine whether aFGF and bFGF were co‐expressed with FGF8 in human prostate cancer. Twenty‐nine cases of prostate cancer of different histological grades were examined. Immunohistochemical analysis was employed to study aFGF and bFGF expression. In the light of the results, aFGF immunoreactivity was studied in a further 43 cases. aFGF and bFGF immunoreactivity was identified in the cytoplasm of the malignant prostatic epithelium. aFGF was overexpressed in 62/72 (86·1 per cent) cases and bFGF in 19/29 (65·5 per cent). High levels of aFGF immunoreactivity were noted in areas of high‐grade prostatic intraepithelial neoplasia (PIN). In this series, aFGF immunoreactivity was most commonly observed and correlated closely with Gleason score and tumour stage ( p=0·007 and 0·007, respectively). Co‐localization of aFGF, bFGF, and FGF8 was detected in 9/29 (31·0 per cent) cases. There was a significant correlation between aFGF and FGF8 expression. In conclusion, aFGF, bFGF, and FGF8 are co‐localized in human prostate cancer; they may have a synergistic effect in prostate cancer growth and progression. Copyright © 1999 John Wiley & Sons, Ltd.

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FGF8 over-expression in prostate cancer is associated with decreased patient survival and persists in androgen independent disease

Cited by 133 publications

References 14 publications

FGF8 isoform b expression in human prostate cancer

FGF8 isoform b expression in human prostate cancer

FGF8b oncogene mediates proliferation and invasion of Epstein–Barr virus-associated nasopharyngeal carcinoma cells: implication for viral-mediated FGF8b upregulation

aFGF immunoreactivity in prostate cancer and its co-localization with bFGF and FGF8

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