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2. Expression of Histone Deacetylases 1, 2 and 3 in histological subtypes of testicular germ cell tumours

Author

Fritzsche, F R, Hasler, A, Bode, P K, Adams, H, Seifert, H H, Sulser, T, Moch, H, Barghorn, A, Kristiansen, G, and University of Zurich

Subjects
2734 Pathology and Forensic Medicine, 10062 Urological Clinic, 616 - Patología. Medicina clínica. Oncología, 10022 Division of Surgical Research, HDAC, 10049 Institute of Pathology and Molecular Pathology, 610 Medicine & health, 2722 Histology, Immunohistochemistry
Abstract

In this study we aimed to evaluate the protein expression of class I histone deacetylases (HDAC) in testicular germ cell tumours (GCT) and to analyse differences between the histological subtypes of testicular GCT. 325 testicular GCT were included in a tissue microarray with each histological subtype of the tumour being separately represented on this array. Expression of class I HDAC isoforms 1, 2 and 3 was assessed by immunohistochemistry. While HDAC2 and 3 were highly expressed in all histological subtypes of GCT, HDAC1 was almost consistently expressed at lower levels. We observed significant differences in the expression of the respective HDACs between seminoma and non-seminoma GCT tissue components. Interestingly, choriocarcinomas showed generally high expression values for all three class I HDAC isoforms. Relevant correlations with clinicopathological parameters could not be demonstrated. Contrasting published findings on other tumour entities, no immediate practical diagnostic or prognostic value for HDAC1-3 in GCT could be inferred. However, the high expression levels might still be indicative for a treatment response to HDAC inhibitors which ought to be evaluated in further studies.

Published
2011

5. Silver-enhanced in situ hybridization for detection of polyomavirus DNA in patients with BK virus nephropathy

Author

Fritzsche, F R, Pianca, S, Gaspert, A, Varga, Z, Wang, L, Farrell, M P, Chen, X B, Hirsch, H H, Springer, E, Fehr, T, Myles, J, Tubbs, R, Moch, H, Fritzsche, F R, Pianca, S, Gaspert, A, Varga, Z, Wang, L, Farrell, M P, Chen, X B, Hirsch, H H, Springer, E, Fehr, T, Myles, J, Tubbs, R, and Moch, H

Abstract

BK virus nephropathy is not an infrequent complication of renal transplantation associated with high rates of graft loss. Although antibodies against SV40 antigen detect different viruses of the polyomavirus family, immunohistochemistry is widely used to confirm the diagnosis of BK virus nephropathy in renal biopsies. Here we aimed to validate the novel silver-enhanced in situ hybridization (SISH) technique for the automated detection of BK virus in renal transplant biopsies. Two different patient cohorts were included. Twenty-nine consecutive patients suspicious for BK virus infection were investigated by SISH and chromogenic in situ hybridization. An additional 26 renal biopsies positive by SV40 immunohistochemistry from 19 patients were analyzed by SISH. Polyomavirus DNA serum levels, as determined by nested PCR analysis, were available for all of these patients. The presence of BK virus DNA in renal tubular cells was identified in 5 of the suspicious cases by both, SISH and chromogenic in situ hybridization . One additional patient was only positive in the SISH. In the second cohort, SISH was positive in all SV40 positive biopsies, but SISH signals were less extensive than SV40 immunohistochemistry. Our results show that the BK virus SISH is an ancillary tool for the detection of polyomavirus DNA in renal biopsies using bright-field microscopy. However, its diagnostic value in comparison with standard immunohistochemistry seems to be limited.

Published
2011

6. Pathological processing techniques and final diagnosis of breast cancer sentinel lymph nodes

Author

Fritzsche, F R, Reineke, T, Morawietz, L, Kristiansen, G, Dietel, M, Fink, D, Rageth, C, Honegger, C, Caduff, R, Moch, H, Varga, Z, Fritzsche, F R, Reineke, T, Morawietz, L, Kristiansen, G, Dietel, M, Fink, D, Rageth, C, Honegger, C, Caduff, R, Moch, H, and Varga, Z

Abstract

BACKGROUND: Recommendations for intraoperative and postoperative breast sentinel lymph node (SLN) processing differ widely. Micrometastases and isolated tumor cells (ITC) have recently been proposed as prognostically and therapeutically relevant. We compared 3 SLN protocols with regard to intraoperative and postoperative diagnosis. MATERIALS AND METHODS: SLN in cohort I (270 patients) were intraoperatively assessed by stereomicroscopy. Intraoperative frozen section (IFS) was used only in stereomicroscopically suspicious SLN. In cohort II (197 patients), all SLN were examined with only 1 IFS. Final SLN workup in cohorts I and II consisted of complete step sectioning with immunohistochemistry. In cohort III (268 patients) 2 or more IFS were performed followed by 3 step sections and immunohistochemistry. RESULTS: pN1 stages were significantly higher in cohorts I and II (33.3% and 34.0% respectively) than in cohort III (24.6%). Intraoperative false negativity for the detection of metastases (pN1) ranged from 54.4% (cohort I) and 35.8% (cohort II) to 21.2% (cohort III). In contrast, ITC were detected significantly more frequently in cohort I (9.3%) and cohort II (14.7%) than in cohort III (1.9%). CONCLUSIONS: Higher rates of SLN metastases and ITC in cohort I/II compared to cohort III suggest that IFS may result in tissue loss thus increasing the risk of missing metastases. Sparse IFS but complete postoperative SLN workup with step sectioning and immunohistochemistry provides more accurate information regarding minimal disease in SLN, but often results in delayed axillary lymph node dissection. This is important for preoperative patient information and recommendations in SLN processing protocols.

Published
2010

7. Pulmonary Kaposi's sarcoma after heart transplantation: a case report

Author

Fritzsche, F R, Tutic, M, Opitz, I, Hunziker, R, Kristiansen, G, Montani, M, Fritzsche, F R, Tutic, M, Opitz, I, Hunziker, R, Kristiansen, G, and Montani, M

Abstract

INTRODUCTION: Kaposi's sarcomas have been associated with different conditions of immunosuppression and are also known to be a typical complication of solid organ transplantations. CASE PRESENTATION: We report of a 65 year old man of Turkish origin with a history of heart transplantation 10 months ago who presented for clarification of his dyspnoea. The patient had a known history of chronic obstructive pulmonary disease and a smoking history of 40 pack years. Radiologically, three progressively growing intrapulmonary nodules were detected. The histology was diagnostic for a Kaposi's sarcoma. Visceral and especially primary intrapulmonary Kaposi's sarcomas are very rare and have been described to have a rather unfavourable prognosis. CONCLUSION: Even with a history suggestive for conventional lung cancer, Kaposi's sarcomas should be considered in patients after transplantation of solid organs. It should be noticed that in a minority of cases this tumour exists in the absence of the typical cutaneous lesions.

Published
2010

8. Insulin-like growth factor II mRNA binding protein 3 (IMP3) is overexpressed in prostate cancer and correlates with higher Gleason scores

Author

Ikenberg, K, Fritzsche, F R, Zuerrer-Haerdi, U, Hofmann, I, Hermanns, T, Seifert, H, Müntener, M, Provenzano, M; https://orcid.org/0000-0001-6993-5718, Sulser, T, Behnke, S, Gerhardt, J, Mortezavi, A, Wild, P, Hofstädter, F, Burger, M, Moch, H, Kristiansen, G, Ikenberg, K, Fritzsche, F R, Zuerrer-Haerdi, U, Hofmann, I, Hermanns, T, Seifert, H, Müntener, M, Provenzano, M; https://orcid.org/0000-0001-6993-5718, Sulser, T, Behnke, S, Gerhardt, J, Mortezavi, A, Wild, P, Hofstädter, F, Burger, M, Moch, H, and Kristiansen, G

Abstract

BACKGROUND: The oncofetal protein insulin-like growth factor II mRNA binding protein 3 (IMP3) is an important factor for cell-migration and adhesion in malignancies. Recent studies have shown a remarkable overexpression of IMP3 in different human malignant neoplasms and also revealed it as an important prognostic marker in some tumor entities. To our knowledge, IMP3 expression has not been investigated in prostate carcinomas so far. METHODS: Immunohistochemical stainings for IMP3 were performed on tissue microarray (TMA) organized samples from 507 patients: 31 normal prostate tissues, 425 primary carcinomas and 51 prostate cancer metastases or castration-resistant prostate cancers (CRPC). IMP3 immunoreactivity was semiquantitatively scored and correlated with clinical-pathologic parameters including survival. RESULTS: IMP3 is significantly stronger expressed in prostate carcinomas compared to normal prostate tissues (p < 0.0001), but did not show significant correlation with the pT-stage, the proliferation index (MIB1), preoperative serum PSA level and the margin status. Only a weak and slightly significant correlation was found with the Gleason score and IMP3 expression failed to show prognostic significance in clinico-pathological correlation-analyses. CONCLUSIONS: Although IMP3 is overexpressed in a significant proportion of prostate cancer cases, which might be of importance for novel therapeutic approaches, it does not appear to possess any immediate diagnostic or prognostic value, limiting its potential as a tissue biomarker for prostate cancer. These results might be corroborated by the fact, that two independent tumor cohorts were separately reviewed.

Published
2010

9. Periostin is up-regulated in high grade and high stage prostate cancer

Author

Tischler, V, Fritzsche, F R, Wild, P J, Stephan, C, Seifert, H H, Riener, M O, Hermanns, T, Mortezavi, A, Gerhardt, J, Schraml, P, Jung, K, Moch, H, Soltermann, A, Kristiansen, G, Tischler, V, Fritzsche, F R, Wild, P J, Stephan, C, Seifert, H H, Riener, M O, Hermanns, T, Mortezavi, A, Gerhardt, J, Schraml, P, Jung, K, Moch, H, Soltermann, A, and Kristiansen, G

Abstract

BACKGROUND: Expression of periostin is an indicator of epithelial-mesenchymal transition in cancer but a detailed analysis of periostin expression in prostate cancer has not been conducted so far. METHODS: Here, we evaluated periostin expression in prostate cancer cells and peritumoural stroma immunohistochemically in two independent prostate cancer cohorts, including a training cohort (n = 93) and a test cohort (n = 325). Metastatic prostate cancers (n = 20), hormone refractory prostate cancers (n = 19) and benign prostatic tissues (n = 38) were also analyzed. RESULTS: In total, strong epithelial periostin expression was detectable in 142 of 418 (34.0%) of prostate carcinomas and in 11 of 38 benign prostate glands (28.9%). Increased periostin expression in carcinoma cells was significantly associated with high Gleason score (p < 0.01) and advanced tumour stage (p < 0.05) in the test cohort. Whereas periostin expression was weak or absent in the stroma around normal prostate glands, strong periostin expression in tumour stroma was found in most primary and metastatic prostate cancers. High stromal periostin expression was associated with higher Gleason scores (p < 0.001). There was a relationship between stromal periostin expression and shortened PSA relapse free survival times in the training cohort (p < 0.05). CONCLUSIONS: Our data indicate that periostin up-regulation is related to increased tumour aggressiveness in prostate cancer and might be a promising target for therapeutical interventions in primary and metastatic prostate cancer.

Published
2010

10. GOLPH2 expression may serve as diagnostic marker in seminomas

Author

Fritzsche, F R, Kristiansen, G, Riener, M-O, Dietel, M, Oelrich, B, Fritzsche, F R, Kristiansen, G, Riener, M-O, Dietel, M, and Oelrich, B

Abstract

BACKGROUND: GOLPH2 (Golgi phosphoprotein 2) is a novel Golgi membrane protein. Despite its unknown physiologic function, however, it has been proposed as a biomarker for hepatocellular and prostate carcinoma due to its upregulation in those cancer entities. Whether the overexpression of GOLPH2 is tumour specific or a generic parameter of malignancy and whether this finding is true for additional carcinomas has not been determined. In this study, we aimed to evaluate the expression pattern of GOLPH2 in testicular seminomas, the most common histologic subtype of testicular neoplasm. METHODS: GOLPH2 protein expression was assessed by immunohistochemistry in 69 testicular seminomas and compared to the expression rates in matching normal testicular tissue and intratubular germ cell neoplasia of unclassified type (IGCNU). In addition, a subset of Leydig cell tumours was analyzed accordingly. RESULTS: GOLPH2 was consistently overexpressed (89.9%) in seminomas. Matching non-neoplastic tissue showed weak or negative staining. The observed differences between non-neoplastic and neoplastic tissue were statistically highly significant (p < 0.001). There were no significant associations with tumour status. Interestingly, GOLPH2 was also highly expressed in the intertubular Leydig cells as well as in Leydig cell tumours. CONCLUSIONS: GOLPH2 protein is highly expressed in seminomas and in Leydig cell tumours. This study fosters the association of GOLPH2 with malignant neoplastic processes. The staining pattern is easily assessable and consistent which is a favourable property especially in clinical settings. GOLPH2 could be a novel immunohistochemical marker for the assessment of testicular neoplasms, especially against the background that in analogy to hepatocellular carcinomas complementary GOLPH2 serum levels might be helpful in detecting metastases or recurrent tumour. Therefore serum studies and analyses of GOLPH2 expression in non-seminomatous germ cell tumours are

Published
2010

11. Down-regulation of the pro-apoptotic XIAP associated factor-1 (XAF1) during progression of clear-cell renal cancer

Author

Kempkensteffen, C, Fritzsche, F R, Johannsen, M, Weikert, S, Hinz, S, Dietel, M, Riener, M O, Moch, H, Jung, K, Krause, H, Miller, K, Kristiansen, G, Kempkensteffen, C, Fritzsche, F R, Johannsen, M, Weikert, S, Hinz, S, Dietel, M, Riener, M O, Moch, H, Jung, K, Krause, H, Miller, K, and Kristiansen, G

Abstract

BACKGROUND: Decreased expression of the interferon-stimulated, putative tumour suppressor gene XAF1 has been shown to play a role during the onset, progression and treatment failure in various malignancies. However, little is yet known about its potential implication in the tumour biology of clear-cell renal cell cancer (ccRCC). METHODS: This study assessed the expression of XAF1 protein in tumour tissue obtained from 291 ccRCC patients and 68 normal renal tissue samples, utilizing immunohistochemistry on a tissue-micro-array. XAF1 expression was correlated to clinico-pathological tumour features and prognosis. RESULTS: Nuclear XAF1 expression was commonly detected in normal renal- (94.1%) and ccRCC (91.8%) samples, without significant differences of expression levels. Low XAF1 expression in ccRCC tissue, however, was associated with progression of tumour stage (p = 0.040) and grade (p < 0.001). Low XAF1 tumour levels were also prognostic of significantly shortened overall survival times in univariate analysis (p = 0.018), but did not provide independent prognostic information. CONCLUSION: These data suggest down-regulation of XAF1 expression to be implicated in ccRCC progression and implies that its re-induction may provide a therapeutic approach. Although the prognostic value of XAF1 in ccRCC appears to be limited, its predictive value remains to be determined, especially in patients with metastatic disease undergoing novel combination therapies of targeted agents with Interferon-alpha.

Published
2009

12. Large mixed germ cell tumor in a young patient presenting as an intrapulmonary mass

Author

Fritzsche, F R, Kristiansen, G, Frauenfelder, T, Opitz, I, Bode, P, Moch, H, Montani, M, Fritzsche, F R, Kristiansen, G, Frauenfelder, T, Opitz, I, Bode, P, Moch, H, and Montani, M

Abstract

We present the case of a 26-year-old man with a bland medical history, who presented to the general practitioner because of severe cough and dyspnea. The chest X-ray revealed a massive organ-displacing tumor in the right chest not delineable from the mediastinum. The subsequent needle core biopsy was diagnostic for a mixed germ cell tumor comprising immature teratoma and seminoma. After an initially good response to chemotherapy, tumor markers and tumor size were progressive. The right-sided pneumonectomy revealed an intrapulmonary tumor with cystic and solid components, hemorrhage, and necrosis with a tumor diameter of 18cm. Histology confirmed a teratoma with mature and immature components accompanied by residual seminomatous tumor cells. Despite maximal intensive care, the patient died four weeks after surgery from acute respiratory distress syndrome. We describe this exceptional large intrapulmonary germ cell tumor and discuss the spectrum of such rare tumors.

Published
2009

13. GOLPH2 expression in renal cell cancer

Author

Fritzsche, F R, Riener, M O, Dietel, M, Moch, H, Jung, K, Kristiansen, G, Fritzsche, F R, Riener, M O, Dietel, M, Moch, H, Jung, K, and Kristiansen, G

Abstract

BACKGROUND: Renal cell carcinomas (RCC) are among the most common and most lethal genitourinary malignancies. GOLPH2 (golgi phosphoprotein 2, GOLM1) has recently been proposed as a biomarker for hepatocellular and prostate cancer. In this study we analysed the expression patterns and the prognostic and diagnostic value of GOLPH2 in RCC. METHODS: GOLPH2 protein expression was analysed by immunohistochemistry in 104 clinically well characterized RCC cases in comparison with matched normal kidney tissue and in association with clinico-pathological parameters. Statistical analyses including Kaplan Meier analyses were performed with SPSS version 15.0. RESULTS: GOLPH2 was highly expressed in normal renal tubules and in almost half of RCC with a statistically significant predominance in the papillary and chromophobe histological subtypes. No other associations with clinico-pathological parameters were detectable. The Kaplan-Meier curves showed a weak trend for unfavourable prognosis of tumours with high GOLPH2 expression, but failed significance. CONCLUSION: GOLPH2 protein is expressed in normal renal tissue (especially in distal tubular epithelia) and is down-regulated in the majority of clear cell RCC. In papillary and chromophobe RCC GOLPH2 expression is consistently present. In contrast to its diagnostic value in hepatocellular and prostatic carcinomas, a prognostic or diagnostic value of GOLPH2 in RCC appears to be unlikely.

Published
2008

14. ADAM9 is highly expressed in renal cell cancer and is associated with tumour progression

Author

Fritzsche, F R, Wassermann, K, Jung, M, Tölle, A, Kristiansen, I, Lein, M, Johannsen, M, Dietel, M, Jung, K, Kristiansen, G, Fritzsche, F R, Wassermann, K, Jung, M, Tölle, A, Kristiansen, I, Lein, M, Johannsen, M, Dietel, M, Jung, K, and Kristiansen, G

Abstract

BACKGROUND: A Disintegrin And Metalloprotease (ADAM) 9 has been implicated in tumour progression of various solid tumours, however, little is known about its role in renal cell carcinoma. We evaluated the expression of ADAM9 on protein and transcript level in a clinico-pathologically characterized renal cell cancer cohort. METHODS: 108 renal cancer cases were immunostained for ADAM9 on a tissue-micro-array. For 30 additional cases, ADAM9 mRNA of microdissected tumour and normal tissue was analyzed via quantitative RT-PCR. SPSS 14.0 was used to apply crosstables (Fisher's exact test and chi2-test), correlations and univariate as well as multivariate survival analyses. RESULTS: ADAM9 was significantly up-regulated in renal cancer in comparison to the adjacent normal tissue on mRNA level. On protein level, ADAM9 was significantly associated with higher tumour grade, positive nodal status and distant metastasis. Furthermore, ADAM9 protein expression was significantly associated with shortened patient survival in the univariate analysis. CONCLUSION: ADAM9 is strongly expressed in a large proportion of renal cell cancers, concordant with findings in other tumour entities. Additionally, ADAM9 expression is significantly associated with markers of unfavourable prognosis. Whether the demonstrated prognostic value of ADAM9 is independent from other tumour parameters will have to be verified in larger study cohorts.

Published
2008

19. Pulmonary Kaposi's sarcoma after heart transplantation: a case report

Author

Roger Hunziker, Glen Kristiansen, Matteo Montani, Michaela Tutic, Florian R. Fritzsche, Isabelle Opitz, University of Zurich, and Fritzsche, F R

Subjects
Heart transplantation, Medicine(all), medicine.medical_specialty, Pathology, business.industry, 10042 Clinic for Diagnostic and Interventional Radiology, medicine.medical_treatment, lcsh:R, lcsh:Medicine, Case Report, Immunosuppression, 610 Medicine & health, General Medicine, 2700 General Medicine, medicine.disease, Dermatology, Transplantation, Surgical oncology, 10049 Institute of Pathology and Molecular Pathology, Medicine, Sarcoma, Complication, business, Lung cancer, Pulmonary Kaposi's Sarcoma
Abstract

Introduction Kaposi's sarcomas have been associated with different conditions of immunosuppression and are also known to be a typical complication of solid organ transplantations. Case presentation We report the case of a 65-year-old Turkish man with a history of heart transplantation 10 months ago who presented for clarification of his dyspnea. The patient had a known history of chronic obstructive pulmonary disease and a smoking history of 40 pack years. Radiologically, three progressively growing intra-pulmonary nodules were detected. The histology was diagnostic for a Kaposi's sarcoma. Visceral and especially primary intra-pulmonary Kaposi's sarcomas are very rare and have been described to have a rather unfavorable prognosis. Conclusions Even with a history suggestive for conventional lung cancer, Kaposi's sarcomas should be considered in patients after transplantation of solid organs. It should be noted that in a minority of cases this tumor exists in the absence of the typical cutaneous lesions.

Published
2010

20. Large mixed germ cell tumor in a young patient presenting as an intrapulmonary mass

Author

Matteo Montani, Isabelle Opitz, Florian R. Fritzsche, Peter K. Bode, Thomas Frauenfelder, Glen Kristiansen, Holger Moch, University of Zurich, and Fritzsche, F R

Subjects
Adult, Male, Pathology, medicine.medical_specialty, Lung Neoplasms, 10255 Clinic for Thoracic Surgery, medicine.medical_treatment, 610 Medicine & health, Pathology and Forensic Medicine, 1307 Cell Biology, Pneumonectomy, Fatal Outcome, Intensive care, 10049 Institute of Pathology and Molecular Pathology, Biomarkers, Tumor, Medicine, Humans, Chemotherapy, business.industry, 10042 Clinic for Diagnostic and Interventional Radiology, Teratoma, Mediastinum, Cell Biology, Seminoma, medicine.disease, Combined Modality Therapy, 2734 Pathology and Forensic Medicine, medicine.anatomical_structure, Disease Progression, Immature teratoma, Radiography, Thoracic, business, Tomography, X-Ray Computed, Germ cell
Abstract

We present the case of a 26-year-old man with a bland medical history, who presented to the general practitioner because of severe cough and dyspnea. The chest X-ray revealed a massive organ-displacing tumor in the right chest not delineable from the mediastinum. The subsequent needle core biopsy was diagnostic for a mixed germ cell tumor comprising immature teratoma and seminoma. After an initially good response to chemotherapy, tumor markers and tumor size were progressive. The right-sided pneumonectomy revealed an intrapulmonary tumor with cystic and solid components, hemorrhage, and necrosis with a tumor diameter of 18cm. Histology confirmed a teratoma with mature and immature components accompanied by residual seminomatous tumor cells. Despite maximal intensive care, the patient died four weeks after surgery from acute respiratory distress syndrome. We describe this exceptional large intrapulmonary germ cell tumor and discuss the spectrum of such rare tumors.

Published
2009
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