Your search keyword '"Fritzsche, F R"' showing total 4 results

1. GOLPH2 protein expression as a novel tissue biomarker for prostate cancer: implications for tissue-based diagnostics.

Author

Kristiansen, G., Fritzsche, F. R., Wassermann, K., Jäger, C., Tölle, A., Lein, M., Stephan, C., Jung, K., Pilarsky, C., Dietel, M., Moch, H., Jäger, C, and Tölls, A

Subjects

*PROSTATE cancer, *GOLGI apparatus, *ANTIGENS, *IMMUNOHISTOCHEMISTRY, *PROSTATECTOMY, *BASAL cell carcinoma

Abstract

GOLPH2 is coding the 73-kDa type II Golgi membrane antigen GOLPH2/GP73. Upregulation of GOLPH2 mRNA has been recently reported in expression array analyses of prostate cancer. As GOLPH2 protein expression in prostate tissues is currently unknown, this study aimed at a comprehensive analysis of GOLPH2 protein in benign and malignant prostate lesions. Immunohistochemically detected GOLPH2 protein expression was compared with the basal cell marker p63 and the prostate cancer marker alpha-methylacyl-CoA racemase (AMACR) in 614 radical prostatectomy specimens. GOLPH2 exhibited a perinuclear Golgi-type staining pattern and was preferentially seen in prostatic gland epithelia. Using a semiquantitative staining intensity score, GOLPH2 expression was significantly higher in prostate cancer glands compared with normal glands (P<0.001). GOLPH2 protein was upregulated in 567 of 614 tumours (92.3%) and AMACR in 583 of 614 tumours (95%) (correlation coefficient 0.113, P = 0.005). Importantly, GOLPH2 immunohistochemistry exhibited a lower level of intratumoral heterogeneity (25 vs 45%). Further, GOLPH2 upregulation was detected in 26 of 31 (84%) AMACR-negative prostate cancer cases. These data clearly suggest GOLPH2 as an additional ancillary positive marker for tissue-based diagnosis of prostate cancer. [ABSTRACT FROM AUTHOR]

Published

2008

2. European and US publications in the 50 highest ranking pathology journals from 2000 to 2006.

Author

Fritzsche, F. R., Oelrich, B., Dietel, M., Jung, K., and Kristiansen, G.

Subjects

*PERIODICALS, *PATHOLOGY, *SCIENTISTS

Abstract

Aims: To analyse the contributions of the 15 primary member states of the European Union and selected non-European countries to pathological research between 2000 and 2006. Methods: Pathological journals were screened using ISI Web of Knowledge database. The number of publications and related impact factors were determined for each country. Relevant socioeconomic indicators were related to the scientific output, Subsequently, results were compared to publications in 10 of the leading biomedical journals. Results: The research output remained generally stable. In Europe, the UK, Germany, France, Italy and Spain ranked top concerning contributions to publications and impact factors in the pathological and leading general biomedical journals. With regard to socioeconomic data, smaller, mainly northern European countries showed a relatively higher efficiency. Of the lager countries, the UK is the most efficient in that respect. The rising economic powers of China and India were consistently in the rear. Conclusions: Results mirror the leading role of the USA in pathology research but also show the relevance of European scientists. The scientometric approach in this study provides a new fundamental and comparative overview of pathology research in the European Union and the USA which could help to benchmark scientific output among countries. [ABSTRACT FROM AUTHOR]

Published

2008

3. Endogenous myoglobin in human breast cancer is a hallmark of luminal cancer phenotype.

Author

Kristiansen, G., Rose, M., Geisler, C., Fritzsche, F. R., Gerhardt, J., Lüke, C., Ladhoff, A.-M., Knüchel, R., Dietel, M., Moch, H., Varga, Z., Theurillat, J.-P., Gorr, T. A., Dahl, E., Lüke, C, and Knüchel, R

Subjects

*MYOGLOBIN, *BREAST cancer, *IMMUNOFLUORESCENCE, *HYPOXEMIA, *IMMUNOHISTOCHEMISTRY, *ESTRADIOL, *THERAPEUTICS, *RNA analysis, *ADENOCARCINOMA, *RESEARCH, *HORMONE-dependent tumors, *CANCER invasiveness, *RESEARCH methodology, *PROGNOSIS, *MEDICAL cooperation, *EVALUATION research, *COMPARATIVE studies, *CELL lines, *BREAST tumors, *LONGITUDINAL method, *PHENOTYPES

Abstract

Background: We aimed to clarify the incidence and the clinicopathological value of non-muscle myoglobin (Mb) in a large cohort of non-invasive and invasive breast cancer cases.Methods: Matched pairs of breast tissues from 10 patients plus 17 breast cell lines were screened by quantitative PCR for Mb mRNA. In addition, 917 invasive and 155 non-invasive breast cancer cases were analysed by immunohistochemistry for Mb expression and correlated to clinicopathological parameters and basal molecular characteristics including oestrogen receptor-alpha (ERalpha)/progesteron receptor (PR)/HER2, fatty acid synthase (FASN), hypoxia-inducible factor-1alpha (HIF-1alpha), HIF-2alpha, glucose transporter 1 (GLUT1) and carbonic anhydrase IX (CAIX). The spatial relationship of Mb and ERalpha or FASN was followed up by double immunofluorescence. Finally, the effects of estradiol treatment and FASN inhibition on Mb expression in breast cancer cells were analysed.Results: Myoglobin mRNA was found in a subset of breast cancer cell lines; in microdissected tumours Mb transcript was markedly upregulated. In all, 71% of tumours displayed Mb protein expression in significant correlation with a positive hormone receptor status and better prognosis. In silico data mining confirmed higher Mb levels in luminal-type breast cancer. Myoglobin was also correlated to FASN, HIF-2alpha and CAIX, but not to HIF-1alpha or GLUT1, suggesting hypoxia to participate in its regulation. Double immunofluorescence showed a cellular co-expression of ERalpha or FASN and Mb. In addition, Mb levels were modulated on estradiol treatment and FASN inhibition in a cell model.Conclusion: We conclude that in breast cancer, Mb is co-expressed with ERalpha and co-regulated by oestrogen signalling and can be considered a hallmark of luminal breast cancer phenotype. This and its possible new role in fatty acid metabolism may have fundamental implications for our understanding of Mb in solid tumours. [ABSTRACT FROM AUTHOR]

Published

2010

4. Histone deacetylases 1, 2 and 3 are highly expressed in prostate cancer and HDAC2 expression is associated with shorter PSA relapse time after radical prostatectomy.

Author

Weichert, W., Röske, A., Gekeler, V., Beckers, T., Stephan, C., Jung, K., Fritzsche, F. R., Niesporek, S., Denkert, C., Dietel, M., Kristiansen, G., and Röske, A

Subjects

*PROSTATECTOMY, *PROSTATE surgery, *TRANSURETHRAL prostatectomy, *PROSTATE cancer, *MALE reproductive organs, *CLINICAL medicine, *MEDICAL research, *MEDICAL experimentation on humans

Abstract

High activity of histone deacetylases (HDACs) causes epigenetic alterations associated with malignant cell behaviour. Consequently, HDAC inhibitors have entered late-phase clinical trials as new antineoplastic drugs. However, little is known about expression and function of specific HDAC isoforms in human tumours including prostate cancer. We investigated the expression of class I HDACs in 192 prostate carcinomas by immunohistochemistry and correlated our findings to clinicopathological parameters including follow-up data. Class I HDAC isoforms were strongly expressed in the majority of the cases (HDAC1: 69.8%, HDAC2: 74%, HDAC3: 94.8%). High rates of HDAC1 and HDAC2 expression were significantly associated with tumour dedifferentiation. Strong expression of all HDACs was accompanied by enhanced tumour cell proliferation. In addition, HDAC2 was an independent prognostic marker in our prostate cancer cohort. In conclusion, we showed that the known effects of HDACs on differentiation and proliferation of cancer cells observed in vitro can also be confirmed in vivo. The class I HDAC isoforms 1, 2 and 3 are differentially expressed in prostate cancer, which might be important for upcoming studies on HDAC inhibitors in this tumour entity. Also, the highly significant prognostic value of HDAC2 clearly deserves further study. [ABSTRACT FROM AUTHOR]

Published

2008