Your search keyword '"Gisela Keller"' showing total 115 results

1. Post‐neoadjuvant assessment of tumour budding according to ITBCC subgroups delivers stage‐ and regression‐grade independent prognostic information in intestinal‐type gastric adenocarcinoma

Author

Moritz Jesinghaus, Anna‐Lina Herz, Meike Kohlruss, Miguel Silva, Albert Grass, Sebastian Lange, Alexander Novotny, Katja Ott, Thomas Schmidt, Matthias Gaida, Alexander Hapfelmeier, Carsten Denkert, Wilko Weichert, and Gisela Keller

Subjects

gastric adenocarcinoma, tumour budding, neoadjuvant therapy, prognosis, Pathology, RB1-214

Abstract

Abstract Tumour budding (TB) has been associated with adverse clinicopathological factors and poor survival in a plethora of therapy‐naïve carcinoma entities including gastric adenocarcinoma (GC). As conventional histopathological grading is usually omitted in the post‐neoadjuvant setting of GC, our study aimed to investigate the prognostic impact of TB in GCs resected after neoadjuvant therapy. We evaluated TB according to the criteria from the International Tumour Budding Consensus Conference (ITBCC) in 167 post‐neoadjuvant resections of intestinal‐type GC and correlated the results with overall survival (OS) and clinicopathological parameters. GCs were categorised into Bd1 (0–4 buds, low TB), Bd2 (5–9 buds, intermediate TB), and Bd3 (≥10 buds, high TB). Carcinomas with intermediate and high TB were significantly enriched in higher ypTNM stages and strongly associated with reduced 5‐year OS in univariable analyses (p

Published

2022

2. Corrigendum to 'Dissecting the genetic heterogeneity of gastric cancer'

Author

Timo Hess, Carlo Maj, Jan Gehlen, Oleg Borisov, Stephan L. Haas, Ines Gockel, Michael Vieth, Guillaume Piessen, Hakan Alakus, Yogesh Vashist, Carina Pereira, Michael Knapp, Vitalia Schüller, Alexander Quaas, Heike I. Grabsch, Jessica Trautmann, Ewa Malecka-Wojciesko, Anna Mokrowiecka, Jan Speller, Andreas Mayr, Julia Schröder, Axel M. Hillmer, Dominik Heider, Florian Lordick, Ángeles Pérez-Aísa, Rafael Campo, Jesús Espinel, Fernando Geijo, Concha Thomson, Luis Bujanda, Federico Sopeña, Ángel Lanas, María Pellisé, Claudia Pauligk, Thorsten Oliver Goetze, Carolin Zelck, Julian Reingruber, Emadeldin Hassanin, Peter Elbe, Sandra Alsabeah, Mats Lindblad, Magnus Nilsson, Nicole Kreuser, René Thieme, Francesca Tavano, Roberta Pastorino, Dario Arzani, Roberto Persiani, Jin-On Jung, Henrik Nienhüser, Katja Ott, Ralf R. Schumann, Oliver Kumpf, Susen Burock, Volker Arndt, Anna Jakubowska, Małgorzta Ławniczak, Victor Moreno, Vicente Martín, Manolis Kogevinas, Marina Pollán, Justyna Dąbrowska, Antonio Salas, Olivier Cussenot, Anne Boland-Auge, Delphine Daian, Jean-Francois Deleuze, Erika Salvi, Maris Teder-Laving, Gianluca Tomasello, Margherita Ratti, Chiara Senti, Valli De Re, Agostino Steffan, Arnulf H. Hölscher, Katharina Messerle, Christiane Josephine Bruns, Armands Sīviņš, Inga Bogdanova, Jurgita Skieceviciene, Justina Arstikyte, Markus Moehler, Hauke Lang, Peter P. Grimminger, Martin Kruschewski, Nikolaos Vassos, Claus Schildberg, Philipp Lingohr, Karsten Ridwelski, Hans Lippert, Nadine Fricker, Peter Krawitz, Per Hoffmann, Markus M. Nöthen, Lothar Veits, Jakob R. Izbicki, Adrianna Mostowska, Federico Martinón-Torres, Daniele Cusi, Rolf Adolfsson, Geraldine Cancel-Tassin, Aksana Höblinger, Ernst Rodermann, Monika Ludwig, Gisela Keller, Andres Metspalu, Hermann Brenner, Joerg Heller, Markus Neef, Michael Schepke, Franz Ludwig Dumoulin, Lutz Hamann, Renato Cannizzaro, Michele Ghidini, Dominik Plaßmann, Michael Geppert, Peter Malfertheiner, Olivier Glehen, Tomasz Skoczylas, Marek Majewski, Jan Lubiński, Orazio Palmieri, Stefania Boccia, Anna Latiano, Nuria Aragones, Thomas Schmidt, Mário Dinis-Ribeiro, Rui Medeiros, Salah-Eddin Al-Batran, Mārcis Leja, Juozas Kupcinskas, María A. García-González, Marino Venerito, and Johannes Schumacher

Subjects

Medicine, Medicine (General), R5-920

Published

2023

3. Dissecting the genetic heterogeneity of gastric cancerResearch in context

Author

Timo Hess, Carlo Maj, Jan Gehlen, Oleg Borisov, Stephan L. Haas, Ines Gockel, Michael Vieth, Guillaume Piessen, Hakan Alakus, Yogesh Vashist, Carina Pereira, Michael Knapp, Vitalia Schüller, Alexander Quaas, Heike I. Grabsch, Jessica Trautmann, Ewa Malecka-Wojciesko, Anna Mokrowiecka, Jan Speller, Andreas Mayr, Julia Schröder, Axel M. Hillmer, Dominik Heider, Florian Lordick, Ángeles Pérez-Aísa, Rafael Campo, Jesús Espinel, Fernando Geijo, Concha Thomson, Luis Bujanda, Federico Sopeña, Ángel Lanas, María Pellisé, Claudia Pauligk, Thorsten Oliver Goetze, Carolin Zelck, Julian Reingruber, Emadeldin Hassanin, Peter Elbe, Sandra Alsabeah, Mats Lindblad, Magnus Nilsson, Nicole Kreuser, René Thieme, Francesca Tavano, Roberta Pastorino, Dario Arzani, Roberto Persiani, Jin-On Jung, Henrik Nienhüser, Katja Ott, Ralf R. Schumann, Oliver Kumpf, Susen Burock, Volker Arndt, Anna Jakubowska, Małgorzta Ławniczak, Victor Moreno, Vicente Martín, Manolis Kogevinas, Marina Pollán, Justyna Dąbrowska, Antonio Salas, Olivier Cussenot, Anne Boland-Auge, Delphine Daian, Jean-Francois Deleuze, Erika Salvi, Maris Teder-Laving, Gianluca Tomasello, Margherita Ratti, Chiara Senti, Valli De Re, Agostino Steffan, Arnulf H. Hölscher, Katharina Messerle, Christiane Josephine Bruns, Armands Sīviņš, Inga Bogdanova, Jurgita Skieceviciene, Justina Arstikyte, Markus Moehler, Hauke Lang, Peter P. Grimminger, Martin Kruschewski, Nikolaos Vassos, Claus Schildberg, Philipp Lingohr, Karsten Ridwelski, Hans Lippert, Nadine Fricker, Peter Krawitz, Per Hoffmann, Markus M. Nöthen, Lothar Veits, Jakob R. Izbicki, Adrianna Mostowska, Federico Martinón-Torres, Daniele Cusi, Rolf Adolfsson, Geraldine Cancel-Tassin, Aksana Höblinger, Ernst Rodermann, Monika Ludwig, Gisela Keller, Andres Metspalu, Hermann Brenner, Joerg Heller, Markus Neef, Michael Schepke, Franz Ludwig Dumoulin, Lutz Hamann, Renato Cannizzaro, Michele Ghidini, Dominik Plaßmann, Michael Geppert, Peter Malfertheiner, Olivier Gehlen, Tomasz Skoczylas, Marek Majewski, Jan Lubiński, Orazio Palmieri, Stefania Boccia, Anna Latiano, Nuria Aragones, Thomas Schmidt, Mário Dinis-Ribeiro, Rui Medeiros, Salah-Eddin Al-Batran, Mārcis Leja, Juozas Kupcinskas, María A. García-González, Marino Venerito, and Johannes Schumacher

Subjects

Gastric cancer, Oesophageal adenocarcinoma, Genome-wide association study (GWAS), Transcriptome-wide association study (TWAS), Medicine, Medicine (General), R5-920

Abstract

Summary: Background: Gastric cancer (GC) is clinically heterogenous according to location (cardia/non-cardia) and histopathology (diffuse/intestinal). We aimed to characterize the genetic risk architecture of GC according to its subtypes. Another aim was to examine whether cardia GC and oesophageal adenocarcinoma (OAC) and its precursor lesion Barrett’s oesophagus (BO), which are all located at the gastro-oesophageal junction (GOJ), share polygenic risk architecture. Methods: We did a meta-analysis of ten European genome-wide association studies (GWAS) of GC and its subtypes. All patients had a histopathologically confirmed diagnosis of gastric adenocarcinoma. For the identification of risk genes among GWAS loci we did a transcriptome-wide association study (TWAS) and expression quantitative trait locus (eQTL) study from gastric corpus and antrum mucosa. To test whether cardia GC and OAC/BO share genetic aetiology we also used a European GWAS sample with OAC/BO. Findings: Our GWAS consisting of 5816 patients and 10,999 controls highlights the genetic heterogeneity of GC according to its subtypes. We newly identified two and replicated five GC risk loci, all of them with subtype-specific association. The gastric transcriptome data consisting of 361 corpus and 342 antrum mucosa samples revealed that an upregulated expression of MUC1, ANKRD50, PTGER4, and PSCA are plausible GC-pathomechanisms at four GWAS loci. At another risk locus, we found that the blood-group 0 exerts protective effects for non-cardia and diffuse GC, while blood-group A increases risk for both GC subtypes. Furthermore, our GWAS on cardia GC and OAC/BO (10,279 patients, 16,527 controls) showed that both cancer entities share genetic aetiology at the polygenic level and identified two new risk loci on the single-marker level. Interpretation: Our findings show that the pathophysiology of GC is genetically heterogenous according to location and histopathology. Moreover, our findings point to common molecular mechanisms underlying cardia GC and OAC/BO. Funding: German Research Foundation (DFG).

Published

2023

4. Elevated microsatellite instability at selected tetranucleotide (EMAST) repeats in gastric cancer: a distinct microsatellite instability type with potential clinical impact?

Author

Anna‐Lina Herz, Sarah Wisser, Meike Kohlruss, Julia Slotta‐Huspenina, Moritz Jesinghaus, Bianca Grosser, Katja Steiger, Alexander Novotny, Alexander Hapfelmeier, Thomas Schmidt, Matthias M Gaida, Wilko Weichert, and Gisela Keller

Subjects

EMAST, microsatellite instability, gastric adenocarcinoma, neoadjuvant chemotherapy, prognosis, Pathology, RB1-214

Abstract

Abstract We investigated the clinical impact of elevated microsatellite instability at selected tetranucleotide (EMAST) repeats in the context of neoadjuvant chemotherapy (CTx) in gastric/gastro‐oesophageal adenocarcinomas. We analysed 583 resected tumours (272 without and 311 after CTx) and 142 tumour biopsies before CTx. If at least two or three of the five tetranucleotide repeat markers tested showed instability, the tumours were defined as EMAST (2+) or EMAST (3+), respectively. Expression of mismatch repair proteins including MSH3 was analysed using immunohistochemistry. Microsatellite instability (MSI) and Epstein–Barr virus (EBV) positivity were determined using standard assays. EMAST (2+) and (3+) were detected in 17.8 and 11.5% of the tumours, respectively. The frequency of EMAST (2+) or (3+) in MSI‐high (MSI‐H) tumours was 96.2 or 92.5%, respectively, demonstrating a high overlap with this molecular subtype, and the association of EMAST and MSI status was significant (each overall p

Published

2022

5. Prognostic implication of molecular subtypes and response to neoadjuvant chemotherapy in 760 gastric carcinomas: role of Epstein–Barr virus infection and high‐ and low‐microsatellite instability

Author

Meike Kohlruss, Bianca Grosser, Marie Krenauer, Julia Slotta‐Huspenina, Moritz Jesinghaus, Susanne Blank, Alexander Novotny, Magdalena Reiche, Thomas Schmidt, Liridona Ismani, Alexander Hapfelmeier, Daniel Mathias, Petra Meyer, Matthias M Gaida, Lukas Bauer, Katja Ott, Wilko Weichert, and Gisela Keller

Subjects

microsatellite instability, Epstein–Barr virus, adenocarcinoma, gastric, gastro‐oesophageal junction, outcome, Pathology, RB1-214

Abstract

Abstract Epstein–Barr virus positivity (EBV(+)) and high‐microsatellite instability (MSI‐H) have been identified as molecular subgroups in gastric carcinoma. The aim of our study was to determine the prognostic and predictive relevance of these subgroups in the context of platinum/5‐fluorouracil (5‐FU) based preoperative chemotherapy (CTx). Additionally, we investigated the clinical relevance of the low‐MSI (MSI‐L) phenotype. We analysed 760 adenocarcinomas of the stomach or the gastro‐oesophageal junction encompassing 143 biopsies before CTx and 617 resected tumours (291 without and 326 after CTx). EBV was determined by PCR and in situ hybridisation for selected cases. MSI was analysed by PCR using five microsatellite markers and classified as MSI‐H and MSI‐L. Frequencies of EBV(+), MSI‐H and MSI‐L in the biopsies before CTx were 4.2, 10.5 and 4.9% respectively. EBV(+) or MSI‐H did not correlate with response, but MSI‐L was associated with better response (p = 0.011). In the resected tumours, frequencies of EBV(+), MSI‐H and MSI‐L were 3.9, 9.6 and 4.5% respectively. Overall survival (OS) was significantly different in the non‐CTx group (p = 0.014). Patients with EBV(+) tumours showed the best OS, followed by MSI‐H. MSI‐L was significantly associated with worse OS (hazard ratio [HR], 2.21; 95% confidence interval [CI], 1.21–4.04, p = 0.01). In the resected tumours after CTx, MSI‐H was also associated with increased OS (HR, 0.54; 95% CI, 0.26–1.09, p = 0.085). In multivariable analysis, molecular classification was an independent prognostic factor in the completely resected (R0) non‐CTx group (p = 0.035). In conclusion, MSI‐H and EBV(+) are not predictive of response to neoadjuvant platinum/5‐FU based CTx, but they are indicative of a good prognosis. In particular, MSI‐H indicates a favourable prognosis irrespective of treatment with CTx. MSI‐L predicts good response to CTx and its negative prognostic effect for patients treated with surgery alone suggests that MSI‐L might help to identify patients with potentially high‐benefit from preoperative CTx.

Published

2019

6. Genetic and immunological biomarkers predict metastatic disease recurrence in stage III colon cancer

Author

Andreas Sperlich, Alexander Balmert, Dietrich Doll, Sabine Bauer, Fabian Franke, Gisela Keller, Dirk Wilhelm, Anna Mur, Michael Respondek, Helmut Friess, Ulrich Nitsche, and Klaus-Peter Janssen

Subjects

Chemotherapy, Disease-free survival, Predictors of recurrence, KRAS, BRAF, SASH1, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract Background Even though the post-operative outcome varies greatly among patients with nodal positive colon cancer (UICC stage III), personalized prediction of systemic disease recurrence is currently insufficient. We investigated in a retrospective setting whether genetic and immunological biomarkers can be applied for stratification of distant metastasis occurrence risk. Methods Eighty four patients with complete resection (R0) of stage III colon cancer from two clinical centres were analysed for genetic biomarkers: microsatellite instability, oncogenic mutations in KRAS exon2 and BRAF exon15, expression of osteopontin and the metastasis-associated genes SASH1 and MACC1. Tumor-infiltrating CD3 and CD8 positive T-cells were quantified by immunocytochemistry. Results were correlated with outcome and response to 5-FU based adjuvant chemotherapy, using Cox’s proportional hazard models and integrative two-step cluster analysis. Results Distant metastasis risk was significantly correlated with oncogenic KRAS mutations (p = 0.015), expression of SASH1 (p = 0.016), and the density of CD8-positive T-cells (p = 0.007) in Kaplan-Meier analysis. Upon multivariate Cox-regression analysis, KRAS mutation (p = 0.008) and density of CD8-positive TILs (p = 0.009) were retained as prognostic parameters for metachronous distant metastasis. Integrative two-step cluster analysis was used to combine all genetic markers, allowing stratification of patient subgroups. Post-operative distant metastasis risk ranged from 31% (low-risk) to 41% (intermediate), and 57% (high-risk) (p = 0.032). Increased expression of osteopontin (p = 0.019) and low density of CD8-positive T-cells (p = 0.043) were significantly associated with unfavourable response to 5-FU. Conclusions Integrative biomarker analysis allows stratification of stage III colon cancer patients for the risk of metastatic disease recurrence and may indicate response to 5-FU. Thus, biomarker analysis might facilitate the use of adjuvant therapy for high risk patients.

Published

2018

7. The impact of cyclin D1 mRNA isoforms, morphology and p53 in mantle cell lymphoma: p53 alterations and blastoid morphology are strong predictors of a high proliferation index

Author

Julia Slotta-Huspenina, Ina Koch, Laurence de Leval, Gisela Keller, Margit Klier, Karin Bink, Marcus Kremer, Mark Raffeld, Falko Fend, and Leticia Quintanilla-Martinez

Subjects

Diseases of the blood and blood-forming organs, RC633-647.5

Abstract

Background Mantle cell lymphoma is a clinically heterogeneous disease characterized by overexpression of cyclin D1 protein. Blastoid morphology, high proliferation, and secondary genetic aberrations are markers of aggressive behavior. Expression profiling of mantle cell lymphoma revealed that predominance of the 3’UTR-deficient, short cyclin D1 mRNA isoform was associated with high cyclin D1 levels, a high “proliferation signature” and poor prognosis.Design and Methods Sixty-two cases of mantle cell lymphoma were analyzed for cyclin D1 mRNA isoforms and total cyclin D1 levels by real-time reverse transcriptase polymerase chain reaction, and TP53 alterations were assessed by immunohistochemistry and molecular analysis. Results were correlated with proliferation index and clinical outcome.Results Predominance of the short cyclin D1 mRNA was found in 14 (23%) samples, including four with complete loss of the standard transcript. TP53 alterations were found in 15 (24%) cases. Predominance of 3’UTR-deficient mRNA was significantly associated with high cyclin D1 mRNA levels (P=0.009) and more commonly found in blastoid mantle cell lymphoma (5/11, P=0.060) and cases with a proliferation index of >20% (P=0.026). Both blastoid morphology (11/11, P

Published

2012

8. Expression profiling of stem cell-related genes in neoadjuvant-treated gastric cancer: a NOTCH2, GSK3B and β-catenin gene signature predicts survival.

Author

Lukas Bauer, Rupert Langer, Karen Becker, Alexander Hapfelmeier, Katja Ott, Alexander Novotny, Heinz Höfler, and Gisela Keller

Subjects

Medicine, Science

Abstract

Cancer stem cell (CSC) based gene expression signatures are associated with prognosis in various tumour types and CSCs are suggested to be particularly drug resistant. The aim of our study was first, to determine the prognostic significance of CSC-related gene expression in residual tumour cells of neoadjuvant-treated gastric cancer (GC) patients. Second, we wished to examine, whether expression alterations between pre- and post-therapeutic tumour samples exist, consistent with an enrichment of drug resistant tumour cells. The expression of 44 genes was analysed in 63 formalin-fixed, paraffin embedded tumour specimens with partial tumour regression (10-50% residual tumour) after neoadjuvant chemotherapy by quantitative real time PCR low-density arrays. A signature of combined GSK3B(high), β-catenin (CTNNB1)(high) and NOTCH2(low) expression was strongly correlated with better patient survival (p

Published

2012

9. Microsatellite instability and sex-specific differences of survival in gastric cancer after neoadjuvant chemotherapy without and with taxane: An observational study in real world patients

Author

Theresa Hiltner, Meike Kohlruss, Anna-Lina Herz, Sylvie Lorenzen, Alexander Novotny, Alexander Hapfelmeier, Moritz Jesinghaus, Julia Slotta-Huspenina, Leila Sisic, Matthias M. Gaida, Wilko Weichert, Katja Ott, and Gisela Keller

Subjects

Cancer Research, Oncology, General Medicine

Abstract

Purpose To investigate the prognostic role of microsatellite instability (MSI) in association with sex of patients treated with platinum/fluoropyrimidine neoadjuvant chemotherapy (CTx) with or without a taxane-containing compound. Methods Of the 505 retrospectively analyzed patients with gastric or gastroesophageal adenocarcinoma, 411 patients were treated without taxane and 94 patients with a taxane-containing compound. MSI was determined using standard assays. Results Females demonstrated a better overall survival (OS) than males in the non-taxane group (HR, 0.59; 95% CI 0.41–0.86; p = 0.005), whereas no significant difference was found in the taxane group (HR 1.22; 95% CI 0.55–2.73, p = 0.630). MSI-High (-H) was associated with a better prognosis in both groups (without taxane: HR 0.56; 95% CI 0.33–0.97; p = 0.038; with taxane: HR 0.28; 95% CI 0.04–2.02, p = 0.204). In the non-taxane group, female MSI-H patients showed the best OS (HR 0.18, 95% CI 0.05–0.73; p = 0.016), followed by the female microsatellite stable (MSS) (HR 0.67, 95% CI 0.46–0.98, p = 0.040) and the male MSI-H group (HR 0.76; 95% CI 0.42–1.37, p = 0.760) taken the male MSS group as reference. In the taxane group, female and male MSI-H patients demonstrated the best OS (female MSI-H: HR 0.05, 95% CI 0.00–240.46; male MSI-H: HR 0.45, 95% CI 0.61–3.63, p = 0.438), whereas the female MSS group showed a decreased OS (HR 1.39 95% CI 0.62–3.12, p = 0.420) compared to male MSS patients. Conclusion OS in gastric/gastroesophageal cancer after CTx might depend on sex and MSI status and may differ between patients treated with or without a taxane compound in the chemotherapeutic regimen.

Published

2023

10. Data from Enhanced Activation of Epidermal Growth Factor Receptor Caused by Tumor-Derived E-Cadherin Mutations

Author

Birgit Luber, Heinz Höfler, Claus Hann von Weyhern, Rupert Langer, Sandra Rauser, Karl-Friedrich Becker, Christine Hermannstädter, Gisela Keller, Justus Duyster, Jörg Mages, Margit Fuchs, Axel Walch, and Anja Bremm

Abstract

Mutations of the tumor suppressor E-cadherin and overexpression of the receptor tyrosine kinase epidermal growth factor receptor (EGFR) are among the most frequent genetic alterations associated with diffuse-type gastric carcinoma. Accumulating evidence suggests a functional relationship between E-cadherin and EGFR that regulates both proteins. We report that somatic mutation of E-cadherin is associated with increased activation of EGFR followed by enhanced recruitment of the downstream acting signaling components growth factor receptor binding protein 2 and Shc, and activation of Ras. Reduced complex formation of mutant E-cadherin — with an in frame deletion of exon 8 in the extracellular domain resulting in reduced adhesion and increased motility — with EGFR was observed compared with wild-type E-cadherin. We conclude that reduced binding of mutant E-cadherin to EGFR in a multicomponent complex or reduced stability of the complex may enhance EGFR surface motility, thereby facilitating EGFR dimerization and activation. Furthermore, reduced surface localization due to enhanced internalization of mutant E-cadherin compared with the wild-type protein was observed. The internalization of EGFR was decreased in response to epidermal growth factor stimulation in cells expressing mutant E-cadherin, suggesting that mutation of E-cadherin also influences the endocytosis of EGFR. Moreover, we show increased activation of EGFR in gastric carcinoma samples with mutant E-cadherin lacking exons 8 or 9. In summary, we describe activation of EGFR by mutant E-cadherin as a novel mechanism in tumor cells that explains the enhanced motility of tumor cells in the presence of an extracellular mutation of E-cadherin. [Cancer Res 2008;68(3):707–14]

Published

2023

11. Supplementary Tables S1-S3 from Enhanced Activation of Epidermal Growth Factor Receptor Caused by Tumor-Derived E-Cadherin Mutations

Author

Birgit Luber, Heinz Höfler, Claus Hann von Weyhern, Rupert Langer, Sandra Rauser, Karl-Friedrich Becker, Christine Hermannstädter, Gisela Keller, Justus Duyster, Jörg Mages, Margit Fuchs, Axel Walch, and Anja Bremm

Abstract

Supplementary Tables S1-S3 from Enhanced Activation of Epidermal Growth Factor Receptor Caused by Tumor-Derived E-Cadherin Mutations

Published

2023

12. Supplementary Results, Figure 1, Methods and Materials from Enhanced Activation of Epidermal Growth Factor Receptor Caused by Tumor-Derived E-Cadherin Mutations

Author

Birgit Luber, Heinz Höfler, Claus Hann von Weyhern, Rupert Langer, Sandra Rauser, Karl-Friedrich Becker, Christine Hermannstädter, Gisela Keller, Justus Duyster, Jörg Mages, Margit Fuchs, Axel Walch, and Anja Bremm

Abstract

Supplementary Results, Figure 1, Methods and Materials from Enhanced Activation of Epidermal Growth Factor Receptor Caused by Tumor-Derived E-Cadherin Mutations

Published

2023

13. Dissecting the genetic heterogeneity of gastric cancer

Author

Timo Hess, Carlo Maj, Jan Gehlen, Oleg Borisov, Stephan L. Haas, Ines Gockel, Michael Vieth, Guillaume Piessen, Hakan Alakus, Yogesh Vashist, Carina Pereira, Michael Knapp, Vitalia Schüller, Alexander Quaas, Heike I. Grabsch, Jessica Trautmann, Ewa Malecka-Wojciesko, Anna Mokrowiecka, Jan Speller, Andreas Mayr, Julia Schröder, Axel M. Hillmer, Dominik Heider, Florian Lordick, Ángeles Pérez-Aísa, Rafael Campo, Jesús Espinel, Fernando Geijo, Concha Thomson, Luis Bujanda, Federico Sopeña, Ángel Lanas, María Pellisé, Claudia Pauligk, Thorsten Oliver Goetze, Carolin Zelck, Julian Reingruber, Emadeldin Hassanin, Peter Elbe, Sandra Alsabeah, Mats Lindblad, Magnus Nilsson, Nicole Kreuser, René Thieme, Francesca Tavano, Roberta Pastorino, Dario Arzani, Roberto Persiani, Jin-On Jung, Henrik Nienhüser, Katja Ott, Ralf R. Schumann, Oliver Kumpf, Susen Burock, Volker Arndt, Anna Jakubowska, Małgorzta Ławniczak, Victor Moreno, Vicente Martín, Manolis Kogevinas, Marina Pollán, Justyna Dąbrowska, Antonio Salas, Olivier Cussenot, Anne Boland-Auge, Delphine Daian, Jean-Francois Deleuze, Erika Salvi, Maris Teder-Laving, Gianluca Tomasello, Margherita Ratti, Chiara Senti, Valli De Re, Agostino Steffan, Arnulf H. Hölscher, Katharina Messerle, Christiane Josephine Bruns, Armands Sīviņš, Inga Bogdanova, Jurgita Skieceviciene, Justina Arstikyte, Markus Moehler, Hauke Lang, Peter P. Grimminger, Martin Kruschewski, Nikolaos Vassos, Claus Schildberg, Philipp Lingohr, Karsten Ridwelski, Hans Lippert, Nadine Fricker, Peter Krawitz, Per Hoffmann, Markus M. Nöthen, Lothar Veits, Jakob R. Izbicki, Adrianna Mostowska, Federico Martinón-Torres, Daniele Cusi, Rolf Adolfsson, Geraldine Cancel-Tassin, Aksana Höblinger, Ernst Rodermann, Monika Ludwig, Gisela Keller, Andres Metspalu, Hermann Brenner, Joerg Heller, Markus Neef, Michael Schepke, Franz Ludwig Dumoulin, Lutz Hamann, Renato Cannizzaro, Michele Ghidini, Dominik Plaßmann, Michael Geppert, Peter Malfertheiner, Olivier Gehlen, Tomasz Skoczylas, Marek Majewski, Jan Lubiński, Orazio Palmieri, Stefania Boccia, Anna Latiano, Nuria Aragones, Thomas Schmidt, Mário Dinis-Ribeiro, Rui Medeiros, Salah-Eddin Al-Batran, Mārcis Leja, Juozas Kupcinskas, María A. García-González, Marino Venerito, and Johannes Schumacher

Subjects

Genome-wide association study (GWAS), Oesophageal adenocarcinoma, General Medicine, Gastric cancer, Medical Genetics, Settore MED/42 - IGIENE GENERALE E APPLICATA, General Biochemistry, Genetics and Molecular Biology, Medicinsk genetik, Transcriptome-wide association study (TWAS)

Abstract

Background: Gastric cancer (GC) is clinically heterogenous according to location (cardia/non-cardia) and histopathology (diffuse/intestinal). We aimed to characterize the genetic risk architecture of GC according to its subtypes. Another aim was to examine whether cardia GC and oesophageal adenocarcinoma (OAC) and its precursor lesion Barrett's oesophagus (BO), which are all located at the gastro-oesophageal junction (GOJ), share polygenic risk architecture. Methods: We did a meta-analysis of ten European genome-wide association studies (GWAS) of GC and its subtypes. All patients had a histopathologically confirmed diagnosis of gastric adenocarcinoma. For the identification of risk genes among GWAS loci we did a transcriptome-wide association study (TWAS) and expression quantitative trait locus (eQTL) study from gastric corpus and antrum mucosa. To test whether cardia GC and OAC/BO share genetic aetiology we also used a European GWAS sample with OAC/BO. Findings: Our GWAS consisting of 5816 patients and 10,999 controls highlights the genetic heterogeneity of GC according to its subtypes. We newly identified two and replicated five GC risk loci, all of them with subtype-specific association. The gastric transcriptome data consisting of 361 corpus and 342 antrum mucosa samples revealed that an upregulated expression of MUC1, ANKRD50, PTGER4, and PSCA are plausible GC-pathomechanisms at four GWAS loci. At another risk locus, we found that the blood-group 0 exerts protective effects for non-cardia and diffuse GC, while blood-group A increases risk for both GC subtypes. Furthermore, our GWAS on cardia GC and OAC/BO (10,279 patients, 16,527 controls) showed that both cancer entities share genetic aetiology at the polygenic level and identified two new risk loci on the single-marker level. Interpretation: Our findings show that the pathophysiology of GC is genetically heterogenous according to location and histopathology. Moreover, our findings point to common molecular mechanisms underlying cardia GC and OAC/BO. Funding: German Research Foundation (DFG).

Published

2023

14. The immunologic tumor microenvironment in endometrioid endometrial cancer in the morphomolecular context: mutual correlations and prognostic impact depending on molecular alterations

Author

Katja Steiger, Nicole Pfarr, Bernhard Haller, Georg Philipp Schmidt, Peer-Hendrik Kuhn, Christine E Brambs, Moritz Jesinghaus, Jutta Engel, Wilko Weichert, Barbara Willvonseder, Melanie Boxberg, Holger Bronger, Gisela Keller, Fabian Stögbauer, and Aurelia Noske

Subjects

Adult, Cancer Research, Immunology, Context (language use), Biology, MLH1, 03 medical and health sciences, Lymphocytes, Tumor-Infiltrating, 0302 clinical medicine, Endometrioid endometrial cancer, Biomarkers, Tumor, Tumor Microenvironment, medicine, PMS2, Humans, Immunology and Allergy, Immunologic microenvironment, Aged, Retrospective Studies, 030304 developmental biology, Aged, 80 and over, 0303 health sciences, Tumor microenvironment, Endometrial cancer, Molecular subgroups, Middle Aged, Prognosis, medicine.disease, ddc, Endometrial Neoplasms, Survival Rate, MSH6, Oncology, MSH2, 030220 oncology & carcinogenesis, Mutation, Cancer research, Immunohistochemistry, Original Article, Prognostic impact, Female, Microsatellite Instability, Carcinoma, Endometrioid, Follow-Up Studies

Abstract

Objective POLE-mutant, microsatellite-instable (MSI), p53-mutant and non-specific molecular profile (NSMP) are TCGA-defined molecular subgroups of endometrial cancer (EC). Hypothesizing that morphology and tumor immunology might differ depending on molecular background concerning composition and prognostic impact, we aimed to comprehensively interconnect morphologic, immunologic and molecular data. Methods TCGA-defined molecular groups were determined by immunohistochemistry and sequencing in n = 142 endometrioid EC. WHO-defined histopathological grading was performed. The immunologic microenvironment (iTME) was characterised by the quantification of intraepithelial and stromal populations of tumor-infiltrating lymphocytes (TIL: overall T-cells; T-Killer cells; regulatory T-cells (Treg)). Immunologic parameters were correlated with WHO-grading, TCGA-subgroups and prognosis. Results High density TIL were significantly more frequent in high-grade (G3) compared to low-grade (G1/2) EC in the whole cohort and in the subgroup of POLE-wildtype-/microsatellite-stable-EC. MSI was associated with high-level TIL-infiltration when taking into account the type of mismatch repair defect (MLH1/PMS2; MSH2/MSH6). Prognostic impact of biomarkers depended on molecular subgroups: In p53-mutant EC, Treg were independently prognostic, in NSMP, the unique independently prognostic biomarker was WHO-grading. Conclusions EC morphology and immunology differ depending on genetics. Our study delineated two molecularly distinct subgroups of immunogenic EC characterized by high-density TIL-infiltration: MSI EC and high-grade POLE-wildtype/microsatellite-stable-EC. Prognostic impact of TIL-populations relied on TCGA-subgroups indicating specific roles for TIL depending on molecular background. In NSMP, histopathological grading was the only prognostic biomarker demonstrating the relevance of WHO-grading in an era of molecular subtyping.

Published

2020

15. An Integrated Cellular and Molecular Model of Gastric Neuroendocrine Cancer Evolution Highlights Therapeutic Targets

Author

Joscha Griger, Sebastian A. Widholz, Moritz Jesinghaus, Niklas de Andrade Krätzig, Sebastian Lange, Thomas Engleitner, Juan José Montero, Ekaterina Zhigalova, Rupert Öllinger, Veveeyan Suresh, Wiebke Winkler, Svenja Lier, Olga Baranov, Riccardo Trozzo, Najib Ben Khaled, Björn Konukiewitz, Katja Steiger, Nicole Pfarr, Ashish Rajput, David Sailer, Gisela Keller, Peter Schirmacher, Christoph Röcken, Klaus W. Fagerstedt, Julia Mayerle, Günter Schneider, Wilko Weichert, Dinis Calado, Thomas Sommermann, Günter Klöppel, Klaus Rajewsky, Dieter Saur, and Roland Rad

Subjects

History, Polymers and Plastics, Business and International Management, Industrial and Manufacturing Engineering

Published

2022

16. Significant Tumor Regression after Neoadjuvant Chemotherapy in Gastric Cancer, but Poor Survival of the Patient? Role of MHC Class I Alterations

Author

Theresa Hiltner, Noémi Szörenyi, Meike Kohlruss, Alexander Hapfelmeier, Anna-Lina Herz, Julia Slotta-Huspenina, Moritz Jesinghaus, Alexander Novotny, Sebastian Lange, Katja Ott, Wilko Weichert, and Gisela Keller

Subjects

Cancer Research, adenocarcinoma, tumor regression, Article, gastric, gastroesophageal junction, prognosis, neoadjuvant chemotherapy, HLA, B2M, allelic imbalance, loss of heterozygosity, ddc, Oncology

Abstract

We aimed to determine the clinical and prognostic relevance of allelic imbalance (AI) of the major histocompatibility complex (MHC) class I genes, encompassing the human leukocyte antigen (HLA) class I and beta-2 microglobulin (B2M) genes, in the context of neoadjuvant platinum/fluoropyrimidine chemotherapy (CTx). Biopsies before CTx were studied in 158 patients with adenocarcinoma of the stomach or gastroesophageal junction. The response was histopathologically evaluated. AI was detected by multiplex PCRs analysis of four or five microsatellite markers in HLA and B2M regions, respectively. AI with no marker was significantly associated with response or survival. However, subgroup analysis revealed differences. AI at marker D6S265, close to the HLA-A gene, was associated with an obvious increased risk in responding (HR, 3.62; 95% CI, 0.96–13.68, p = 0.058) but not in non-responding patients (HR, 0.92; 95% CI, 0.51–1.65, p = 0.773). Markers D6S273 and D6S2872 showed similar results. The interaction between AI at D6S265 and response to CTx was significant in a multivariable analysis (p = 0.010). No associations were observed for B2M markers. Our results underline the importance of intact neoantigen presentation specifically for responding patients and may help explain an unexpectedly poor survival of a patient despite significant tumor regression after neoadjuvant platinum/fluoropyrimidine CTx.

Published

2023

17. Elevated microsatellite instability at selected tetranucleotide (EMAST) repeats in gastric cancer: a distinct microsatellite instability type with potential clinical impact?

Author

Anna-Lina, Herz, Sarah, Wisser, Meike, Kohlruss, Julia, Slotta-Huspenina, Moritz, Jesinghaus, Bianca, Grosser, Katja, Steiger, Alexander, Novotny, Alexander, Hapfelmeier, Thomas, Schmidt, Matthias M, Gaida, Wilko, Weichert, and Gisela, Keller

Subjects

Epstein-Barr Virus Infections, Herpesvirus 4, Human, Stomach Neoplasms, Humans, Microsatellite Instability, Microsatellite Repeats

Abstract

We investigated the clinical impact of elevated microsatellite instability at selected tetranucleotide (EMAST) repeats in the context of neoadjuvant chemotherapy (CTx) in gastric/gastro-oesophageal adenocarcinomas. We analysed 583 resected tumours (272 without and 311 after CTx) and 142 tumour biopsies before CTx. If at least two or three of the five tetranucleotide repeat markers tested showed instability, the tumours were defined as EMAST (2+) or EMAST (3+), respectively. Expression of mismatch repair proteins including MSH3 was analysed using immunohistochemistry. Microsatellite instability (MSI) and Epstein-Barr virus (EBV) positivity were determined using standard assays. EMAST (2+) and (3+) were detected in 17.8 and 11.5% of the tumours, respectively. The frequency of EMAST (2+) or (3+) in MSI-high (MSI-H) tumours was 96.2 or 92.5%, respectively, demonstrating a high overlap with this molecular subtype, and the association of EMAST and MSI status was significant (each overall p 0.001). EMAST (2+ or 3+) alone in MSI-H and EBV-negative tumours demonstrated only a statistically significant association of EMAST (2+) positivity and negative lymph node status (42.3% in EMAST (2+) and 28.8% in EMAST negative, p = 0.045). EMAST alone by neither definition was significantly associated with overall survival (OS) of the patients. The median OS for EMAST (2+) patients was 40.0 months (95% confidence interval [CI] 16.4-63.6) compared with 38.7 months (95% CI 26.3-51.1) for the EMAST-negative group (p = 0.880). The median OS for EMAST (3+) patients was 46.7 months (95% CI 18.2-75.2) and 38.7 months (95% CI 26.2-51.2) for the negative group (p = 0.879). No statistically significant association with response to neoadjuvant CTx was observed (p = 0.992 and p = 0.433 for EMAST (2+) and (3+), respectively). In conclusion, our results demonstrate a nearly complete intersection between MSI-H and EMAST and they indicate that EMAST alone is not a distinct instability type associated with noticeable clinico-pathological characteristics of gastric carcinoma patients.

Published

2021

18. Diverse 'just-right' levels of chromosomal instability and their clinical implications in neoadjuvant treated gastric cancer

Author

Bianca Grosser, Marie Krenauer, Meike Kohlruss, Matthias M. Gaida, Alexander Hapfelmeier, Katja Steiger, Nicole Pfarr, Magdalena Reiche, Julia Slotta-Huspenina, Moritz Jesinghaus, Alexander Novotny, Thomas Schmidt, Wilko Weichert, Lukas Bauer, Katja Ott, and Gisela Keller

Subjects

Oncology, Adult, Male, Cancer Research, medicine.medical_specialty, Tumour regression, medicine.medical_treatment, Context (language use), Predictive markers, Article, Prognostic markers, Stomach Neoplasms, Internal medicine, Chromosome instability, Chromosomal Instability, medicine, Humans, ddc:610, neoplasms, Aged, Aged, 80 and over, Chemotherapy, business.industry, Stomach, Cancer, Microsatellite instability, Middle Aged, medicine.disease, female genital diseases and pregnancy complications, Neoadjuvant Therapy, ddc, medicine.anatomical_structure, Surgical oncology, Microsatellite, Female, Gastric cancer, business

Abstract

Background The Cancer Genome Atlas (TCGA) consortium described EBV positivity(+), high microsatellite instability (MSI-H), genomic stability (GS) and chromosomal instability (CIN) as molecular subtypes in gastric carcinomas (GC). We investigated the predictive and prognostic value of these subtypes with emphasis on CIN in the context of neoadjuvant chemotherapy (CTx) in GC. Methods TCGA subgroups were determined for 612 resected adenocarcinomas of the stomach and gastro-oesophageal junction (291 without, 321 with CTx) and 143 biopsies before CTx. EBV and MSI-H were analysed by standard assays. CIN was detected by multiplex PCRs analysing 22 microsatellite markers. Besides the TCGA classification, CIN was divided into four CIN-subgroups: low, moderate, substantial, high. Mutation profiling was performed for 52 tumours by next-generation sequencing. Results EBV(+) (HR, 0.48; 95% CI, 0.23–1.02), MSI-H (HR, 0.56; 95% CI, 0.35–0.89) and GS (HR, 0.72; 95% CI, 0.45–1.13) were associated with increased survival compared to CIN in the resected tumours. Considering the extended CIN-classification, CIN-substantial was a negative prognostic factor in uni- and multivariable analysis in resected tumours with CTx (each p p = 0.026), but was not prognostically relevant. Conclusion A refined CIN classification reveals tumours with different biological characteristics and potential clinical implications.

Published

2021

19. Whole Exome Sequencing of Biliary Tubulopapillary Neoplasms Reveals Common Mutations in Chromatin Remodeling Genes

Author

Günter Klöppel, Julia Weber, Thomas Engleitner, Roland Rad, Gisela Keller, Björn Konukiewitz, Sebastian Lange, Alexander Muckenhuber, Irene Esposito, Katja Steiger, Wilko Weichert, Claudia Gross, Nicole Pfarr, Nazmi Volkan Adsay, Benjamin Goeppert, Moritz Jesinghaus, Anna Melissa Schlitter, Adsay, Volkan (ORCID 0000-0002-1308-3701 & YÖK ID286248), Gross, Claudia, Engleitner, Thomas, Lange, Sebastian, Weber, Julia, Jesinghaus, Moritz, Konukiewitz, Bjoern, Muckenhuber, Alexander, Steiger, Katja, Pfarr, Nicole, Goeppert, Benjamin, Keller, Gisela, Weichert, Wilko, Kloeppel, Gunter, Rad, Roland, Esposito, Irene, Schlitter, Anna Melissa, and School of Medicine

Subjects

0301 basic medicine, Cancer Research, Biology, medicine.disease_cause, Article, Chromatin remodeling, whole exome sequencing, 03 medical and health sciences, 0302 clinical medicine, CDKN2A, bile duct, medicine, GNAS complex locus, Copy-number variation, pancreas, Exome sequencing, RC254-282, Genetics, intraductal tubulopapillary neoplasms, Pancreas, Bile duct, Intraductal tubulopapillary neoplasms, Whole exome sequencing, Chromatin remodeling genes, chromatin remodeling genes, Genetic heterogeneity, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, biology.protein, KRAS, Carcinogenesis

Abstract

Simple summary: Intraductal tubulopapillary neoplasms (ITPN) have recently been described as rare precursor lesions of pancreatic ductal adenocarcinoma and cholangiocarcinoma. Despite a high number of associated invasive adenocarcinomas at the time of diagnosis, patients with ITPN tend to have a much better clinical outcome than those with classical pancreato-biliary adenocarcinoma. Furthermore, rare molecular studies of ITPN show an unexpected lack of hotspot mutations in common driver genes of pancreato-biliary adenocarcinoma, including KRAS. This article reports the first large comprehensive and comparative molecular study of pancreato-biliary ITPN. In the absence of KRAS mutations, we found a high genetic heterogeneity with enrichment in core signaling pathways, including putative actionable genomic targets in one-third of the cases. Whereas, pancreatic ITPN demonstrates a highly distinct genetic profile, differing from classical pancreatic carcinogenesis, biliary ITPN and classical cholangiocarcinoma share common alterations in key genes of the chromatin remodeling pathway, and therefore, appear more closely related than pancreatic ITPN and classical pancreatic ductal adenocarcinoma PDAC. The molecular carcinogenesis of intraductal tubulopapillary neoplasms (ITPN), recently described as rare neoplasms in the pancreato-biliary tract with a favorable prognosis despite a high incidence of associated pancreato-biliary adenocarcinoma, is still poorly understood. To identify driver genes, chromosomal gains and losses, mutational signatures, key signaling pathways, and potential therapeutic targets, the molecular profile of 11 biliary and 6 pancreatic ITPNs, associated with invasive adenocarcinoma in 14/17 cases, are studied by whole exome sequencing (WES). The WES of 17 ITPNs reveals common copy number variants (CNVs) broadly distributed across the genome, with recurrent chromosomal deletions primarily in 1p36 and 9p21 affecting the tumor suppressors CHD5 and CDKN2A, respectively, and gains in 1q affecting the prominent oncogene AKT3. The identified somatic nucleotide variants (SNVs) involve few core signaling pathways despite high genetic heterogeneity with diverse mutational spectra: Chromatin remodeling, the cell cycle, and DNA damage/repair. An OncoKB search identifies putative actionable genomic targets in 35% of the cases (6/17), including recurrent missense mutations of the FGFR2 gene in biliary ITPNs (2/11, 18%). Our results show that somatic SNV in classical cancer genes, typically associated with pancreato-biliary carcinogenesis, were absent (KRAS, IDH1/2, GNAS, and others) to rare (TP53 and SMAD4, 6%, respectively) in ITPNs. Mutational signature pattern analysis reveals a predominance of an age-related pattern. Our findings highlight that biliary ITPN and classical cholangiocarcinoma display commonalities, in particular mutations in genes of the chromatin remodeling pathway, and appear, therefore, more closely related than pancreatic ITPN and classical pancreatic ductal adenocarcinoma., German Research Foundation (DFG)

Published

2021

20. Sexual difference matters: females with high microsatellite instability show increased survival after neoadjuvant chemotherapy in gastric cancer

Author

Meike Kohlruss, Katja Ott, Bianca Grosser, Moritz Jesinghaus, Julia Slotta-Huspenina, Alexander Novotny, Alexander Hapfelmeier, Thomas Schmidt, Matthias M. Gaida, Wilko Weichert, and Gisela Keller

Subjects

adenocarcinoma, gastroesophageal junction, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, molecular subtype, lcsh:RC254-282, gastric, Article, digestive system diseases, age, sex, microsatellite instability, prognosis, ddc:610, neoadjuvant chemotherapy

Abstract

Simple Summary Here we report a sex- and age-specific analysis of 717 patients with gastric/gastro-esophageal adenocarcinomas treated with or without neoadjuvant chemotherapy (CTx) regarding overall survival (OS) and response to CTx. The analysis was also performed in molecular subtypes determined previously. Females demonstrated a significantly increased OS particularly in the group of patients treated with neoadjuvant CTx. Specifically in this patient group and taken into account the molecular subtypes, females with high microsatellite instability (MSI-H) showed the best survival followed by the male MSI-H, the female microsatellite stable (MSS) group and the male MSS group. Thus, we show an effect of sex on OS in gastric/gastro-esophageal cancer in particular for patients treated with neoadjuvant CTx. The superior survival of women with MSI-H tumors among the CTx patients implies that the combined consideration of these factors could contribute to an individualized treatment of the patients. Abstract We aimed to investigate patients with gastric/gastro-esophageal adenocarcinomas for sex- and age-specific differences regarding overall survival (OS) and response to neoadjuvant chemotherapy (CTx) under consideration of tumor specific molecular subtypes. Overall, 717 patients were analyzed, including 426 patients treated with and 291 treated without neoadjuvant CTx. Microsatellite instability (MSI) and Epstein-Barr virus positivity (EBV+) were determined previously. Females demonstrated a significantly increased OS (p = 0.035), particularly in the subgroup treated with CTx (p = 0.054). No significant differences regarding age were found. In the molecular subgroups, no sex-related differences were observed in the non-CTx group. However in the CTx group, females with MSI-high (H) tumors showed the best OS (p = 0.043), followed by the male MSI-H (p = 0.198) and female MSS (p = 0.114) compared to the male MSS group as reference. The interaction between sex and MSI in this patient group was noticeable (p = 0.053) and was included as a relevant factor in multivariable analyses. In conclusion, our results show an effect of sex on OS in gastric/gastro-esophageal cancer specifically for patients treated with neoadjuvant CTx. The superior survival of women with MSI-H tumors after neoadjuvant CTx implies that combined consideration of these factors could contribute to an individualized treatment of the patients.

Published

2021

21. Development and validation of deep learning classifiers to detect Epstein-Barr virus and microsatellite instability status in gastric cancer: a retrospective multicentre cohort study

Author

Hakan Alakus, Hyunki Kim, Alexander Quaas, Matthew Nankivell, Myeong-Cherl Kook, Meike Kohlruss, William H. Allum, Gisela Keller, Franco Roviello, Christian Trautwein, Andrew J Irvine, Nicholas P. West, Jeremy D. Hayden, Philip Quirke, Lara R. Heij, Nadine T. Gaisa, Bianca Grosser, Ruth E Langley, Bastian Dislich, Dirk Jäger, Xiuxiang Tan, Rupert Langer, Alessia D'Ignazio, Takaki Yoshikawa, Jakob Nikolas Kather, David Cunningham, Heike I. Grabsch, Hannah Sophie Muti, Matthias P. Ebert, Tom Luedde, Ralf Huss, Alexander T. Pearson, Young-Woo Kim, Jae Ho Cheong, Takashi Oshima, RS: GROW - R2 - Basic and Translational Cancer Biology, and Pathologie

Subjects

Oncology, medicine.medical_specialty, Receiver operating characteristic, business.industry, MICROSATELLITE INSTABILITY, External validation, Medicine (miscellaneous), Microsatellite instability, Cancer, Health Informatics, Retrospective cohort study, Articles, medicine.disease, medicine.disease_cause, Epstein–Barr virus, ddc, Health Information Management, Internal medicine, medicine, Decision Sciences (miscellaneous), ddc:610, business, GASTRIC-CANCER, Cohort study, Predictive biomarker

Abstract

The lancet / Digital health 3(10), e654-e664 (2021). doi:10.1016/S2589-7500(21)00133-3, Published by The Lancet, London

Published

2021

22. Genetic and immunological biomarkers predict metastatic disease recurrence in stage III colon cancer

Author

Helmut Friess, Klaus-Peter Janssen, Dirk Wilhelm, Andreas Sperlich, Michael Respondek, Dietrich Doll, Fabian Christoph Franke, Alexander Balmert, Anna Mur, Ulrich Nitsche, Sabine Bauer, and Gisela Keller

Subjects

Male, 0301 basic medicine, Oncology, Cancer Research, Systemic disease, Colorectal cancer, medicine.medical_treatment, Disease, medicine.disease_cause, 0302 clinical medicine, Surgical oncology, Predictors of recurrence, Aged, 80 and over, Middle Aged, Prognosis, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, ddc, 030220 oncology & carcinogenesis, Colonic Neoplasms, Female, Fluorouracil, KRAS, Research Article, Adult, Genetic Markers, medicine.medical_specialty, Disease-free survival, lcsh:RC254-282, BRAF, 03 medical and health sciences, Internal medicine, Biomarkers, Tumor, Genetics, medicine, Adjuvant therapy, Humans, Chemotherapy, SASH1, Aged, Neoplasm Staging, Retrospective Studies, business.industry, Microsatellite instability, medicine.disease, 030104 developmental biology, Neoplasm Recurrence, Local, business

Abstract

Background Even though the post-operative outcome varies greatly among patients with nodal positive colon cancer (UICC stage III), personalized prediction of systemic disease recurrence is currently insufficient. We investigated in a retrospective setting whether genetic and immunological biomarkers can be applied for stratification of distant metastasis occurrence risk. Methods Eighty four patients with complete resection (R0) of stage III colon cancer from two clinical centres were analysed for genetic biomarkers: microsatellite instability, oncogenic mutations in KRAS exon2 and BRAF exon15, expression of osteopontin and the metastasis-associated genes SASH1 and MACC1. Tumor-infiltrating CD3 and CD8 positive T-cells were quantified by immunocytochemistry. Results were correlated with outcome and response to 5-FU based adjuvant chemotherapy, using Cox’s proportional hazard models and integrative two-step cluster analysis. Results Distant metastasis risk was significantly correlated with oncogenic KRAS mutations (p = 0.015), expression of SASH1 (p = 0.016), and the density of CD8-positive T-cells (p = 0.007) in Kaplan-Meier analysis. Upon multivariate Cox-regression analysis, KRAS mutation (p = 0.008) and density of CD8-positive TILs (p = 0.009) were retained as prognostic parameters for metachronous distant metastasis. Integrative two-step cluster analysis was used to combine all genetic markers, allowing stratification of patient subgroups. Post-operative distant metastasis risk ranged from 31% (low-risk) to 41% (intermediate), and 57% (high-risk) (p = 0.032). Increased expression of osteopontin (p = 0.019) and low density of CD8-positive T-cells (p = 0.043) were significantly associated with unfavourable response to 5-FU. Conclusions Integrative biomarker analysis allows stratification of stage III colon cancer patients for the risk of metastatic disease recurrence and may indicate response to 5-FU. Thus, biomarker analysis might facilitate the use of adjuvant therapy for high risk patients. Electronic supplementary material The online version of this article (10.1186/s12885-018-4940-2) contains supplementary material, which is available to authorized users.

Published

2018

23. Evidence for PTGER4 ,PSCA, and MBOAT7 as risk genes for gastric cancer on the genome and transcriptome level

Author

Jesús Espinel, Ines Gockel, Daniela Collette, Thomas Schmidt, Gisela Keller, Katja Butterbach, Yogesh K. Vashist, Martin Kruschewski, Michael Knapp, P. Malfertheiner, Anne C. Böhmer, Angel Lanas, Elisabeth Mangold, Rafael Campo, Oliver Pech, Lutz Hamann, Markus Moehler, Jessica Becker, Aksana Höblinger, Jan Gehlen, Concha Thomson, Maria Asuncion Garcia-Gonzalez, Katharina Weise, Peter P. Grimminger, Hakan Alakus, Hermann Brenner, Hans Lippert, Jakob R. Izbicki, Sebastian J. Hofer, Hauke Lang, Evita Gasenko, Philipp Lingohr, Nicole Kreuser, Timo Hess, Fernando Geijo, Markus M. Nöthen, Marino Venerito, Iurii Krasniuk, Florian Lordick, Michael Vieth, Karsten Ridwelski, Claus Schildberg, Alexander F. Hagel, Christiane J. Bruns, Ralf R. Schumann, Katharina Messerle, Lothar Veits, Johannes Schumacher, Katja Ott, Julia Schröder, Marcis Leja, Vitalia Schüller, Limas Kupčinskas, Federico Sopena, Ernst Rodermann, Juozas Kupcinskas, Nikolaos Vassos, Ángeles Pérez-Aisa, Monika Ludwig, Ugne Gyvyte, Luis Bujanda, and Sophie K. M. Heinrichs

Subjects

Male, 0301 basic medicine, Cancer Research, Genotype, Quantitative Trait Loci, eQTL study, Biology, GPI-Linked Proteins, Polymorphism, Single Nucleotide, Genome, Transcriptome, 03 medical and health sciences, Antigens, Neoplasm, Stomach Neoplasms, Gene expression, medicine, Humans, SNP, Genetic Predisposition to Disease, Radiology, Nuclear Medicine and imaging, Gene, Genetic Association Studies, Original Research, Cancer Biology, Genetics, Gene Expression Profiling, Chromosome Mapping, Membrane Proteins, Chromosome, Cancer, medicine.disease, Neoplasm Proteins, Gene Expression Regulation, Neoplastic, 030104 developmental biology, Oncology, genetic association study, Case-Control Studies, Expression quantitative trait loci, gene expression, Chromosomes, Human, Pair 5, Female, Receptors, Prostaglandin E, EP4 Subtype, Acyltransferases, Chromosomes, Human, Pair 8

Abstract

Genetic associations between variants on chromosome 5p13 and 8q24 and gastric cancer (GC) have been previously reported in the Asian population. We aimed to replicate these findings and to characterize the associations at the genome and transcriptome level. We performed a fine-mapping association study in 1926 GC patients and 2012 controls of European descent using high dense SNP marker sets on both chromosomal regions. Next, we performed expression quantitative trait locus (eQTL) analyses using gastric transcriptome data from 143 individuals focusing on the GC associated variants. On chromosome 5p13 the strongest association was observed at rs6872282 (P = 2.53 x 10(-04)) and on chromosome 8q24 at rs2585176 (P = 1.09 x 10(-09)). On chromosome 5p13 we found cis-eQTL effects with an up-regulation of PTGER4 expression in GC risk allele carrier (P = 9.27 x 10(-11)). On chromosome 8q24 we observed cis-eQTL effects with an upregulation of PSCA expression in GC risk allele carrier (P = 2.17 x 10(-47)). In addition, we found trans-eQTL effects for the same variants on 8q24 with a downregulation of MBOAT7 expression in GC risk allele carrier (P = 3.11 x 10(-09)). In summary, we confirmed and refined the previously reported GC associations at both chromosomal regions. Our data point to shared etiological factors between Asians and Europeans. Furthermore, our data imply an upregulated expression of PTGER4 and PSCA as well as a downregulated expression of MBOAT7 in gastric tissue as risk-conferring GC pathomechanisms.

Published

2018

24. Comprehensive analysis of the MLH1 promoter region in 480 patients with colorectal cancer and 1150 controls reveals new variants including one with a heritable constitutional MLH1 epimutation

Author

Anna Benet-Pagès, Gisela Keller, Monika Morak, Daniela Gonzales-Fassrainer, Ayseguel Ibisler, Ellen Jessen, Melanie Locher, Andreas Laner, Trisari Massdorf, Elke Holinski-Feder, and Anke M. Nissen

Subjects

0301 basic medicine, Genetics, Promoter, Methylation, Biology, MLH1, digestive system diseases, MSH6, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, MSH2, 030220 oncology & carcinogenesis, PMS2, Epigenetics, Allele, Genetics (clinical)

Abstract

BackgroundGermline defects in MLH1, MSH2, MSH6 and PMS2 predisposing for Lynch syndrome (LS) are mainly based on sequence changes, whereas a constitutional epimutation of MLH1(CEM) is exceptionally rare. This abnormal MLH1 promoter methylation is not hereditary when arising de novo, whereas a stably heritable and variant-induced CEM was described for one single allele. We searched for MLH1 promoter variants causing a germline or somatic methylation induction or transcriptional repression.MethodsWe analysed the MLH1 promoter sequence in five different patient groups with colorectal cancer (CRC) (n=480) composed of patients with i) CEM (n=16), ii) unsolved loss of MLH1 expression in CRC (n=37), iii) CpG-island methylator-phenotype CRC (n=102), iv) patients with LS (n=83) and v) MLH1-proficient CRC (n=242) as controls. 1150 patients with non-LS tumours also served as controls to correctly judge the results.ResultsWe detected 10 rare MLH1 promoter variants. One novel, complex MLH1 variant c.-63_-58delins18 is present in a patient with CRC with CEM and his sister, both showing a complete allele-specific promoter methylation and transcriptional silencing. The other nine promoter variants detected in 17 individuals were not associated with methylation. For four of these, a normal, biallelic MLH1 expression was found in the patients' cDNA.ConclusionWe report the second promoter variant stably inducing a hereditary CEM. Concerning the classification of promoter variants, we discuss contradictory results from the literature for two variants, describe classification discrepancies between existing rules for five variants, suggest the (re-)classification of five promoter variants to (likely) benign and regard four variants as functionally unclear.

Published

2018

25. Loss of MSH2 and MSH6 due to heterozygous germline defects in MSH3 and MSH6

Author

Anna Benet-Pagès, Martina Kerscher, Gisela Keller, Sarah Käsbauer, Andreas Laner, Elke Holinski-Feder, Monika Morak, Trisari Massdorf, Anke M. Nissen, and Hans K. Schackert

Subjects

Male, 0301 basic medicine, Heterozygote, congenital, hereditary, and neonatal diseases and abnormalities, Cancer Research, Loss of Heterozygosity, Biology, MLH1, Germline, Loss of heterozygosity, 03 medical and health sciences, 0302 clinical medicine, Germline mutation, Genetics, medicine, Humans, neoplasms, Germ-Line Mutation, Genetics (clinical), nutritional and metabolic diseases, Microsatellite instability, medicine.disease, Colorectal Neoplasms, Hereditary Nonpolyposis, digestive system diseases, Pedigree, DNA-Binding Proteins, MSH6, MutS Homolog 2 Protein, 030104 developmental biology, Oncology, MSH3, MSH2, 030220 oncology & carcinogenesis, MutS Homolog 3 Protein, Cancer research, Female

Abstract

Lynch Syndrome (LS) is the most common dominantly inherited colorectal cancer (CRC) predisposition and is caused by a heterozygous germline defect in one of the DNA mismatch repair (MMR) genes MLH1, MSH2, MSH6, or PMS2. High microsatellite instability (MSI-H) and loss of MMR protein expression in tumours reflecting a defective MMR are indicators for LS, as well as a positive family history of early onset CRC. MSH2 and MSH6 form a major functional heterodimer, and MSH3 is an alternative binding partner for MSH2. So far, the role of germline MSH3 variants remains unclear, as to our knowledge heterozygous truncating variants are not regarded causative for LS, but were detected in patients with CRC, and recently biallelic MSH3 defects have been identified in two patients with adenomatous polyposis. By gene screening we investigated the role of MSH3 in 11 LS patients with truncating MSH6 germline variants and an unexplained MSH2 protein loss in their corresponding MSI-H tumours. We report the first two LS patients harbouring heterozygous germline variants c.1035del and c.2732T>G in MSH3 coincidentally with truncating variants in MSH6. In the patient with truncating germline variants in MSH3 and MSH6, two additional somatic second hits in both genes abrogate all binding partners for the MSH2 protein which might subsequently be degraded. The clinical relevance of MSH3 germline variants is currently under re-evaluation, and heterozygous MSH3 defects alone do not seem to induce a LS phenotype, but might aggravate the MSH6 phenotype in affected family members.

Published

2017

26. Colorectal mixed adenoneuroendocrine carcinomas and neuroendocrine carcinomas are genetically closely related to colorectal adenocarcinomas

Author

Gisela Keller, Ruza Arsenic, Björn Konukiewitz, Roland Penzel, Albrecht Stenzinger, Magdalena Reiche, Moritz Jesinghaus, Katja Steiger, Gratiana Hermann, Nicole Pfarr, Wilko Weichert, Volker Endris, Günter Klöppel, and Matthias Kloor

Subjects

Adult, Male, Proto-Oncogene Proteins B-raf, 0301 basic medicine, medicine.medical_specialty, Pathology, Adenocarcinoma, Biology, medicine.disease_cause, Pathology and Forensic Medicine, Proto-Oncogene Proteins p21(ras), Surgical pathology, 03 medical and health sciences, 0302 clinical medicine, Germline mutation, medicine, Carcinoma, Humans, Aged, Retrospective Studies, Aged, 80 and over, Microsatellite instability, Middle Aged, medicine.disease, Carcinoma, Neuroendocrine, 030104 developmental biology, 030220 oncology & carcinogenesis, Mutation, Female, Microsatellite Instability, KRAS, Colorectal Neoplasms, Hematopathology, Carcinogenesis

Abstract

Colorectal mixed adenoneuroendocrine carcinomas are rare and clinically aggressive neoplasms with considerable morphological heterogeneity. Data on their genomic characteristics and molecular associations to either conventional colorectal adenocarcinomas or poorly differentiated neuroendocrine neoplasms is still scarce, hampering optimized patient treatment and care. Tissue from 19 colorectal mixed adenoneuroendocrine carcinomas and eight colorectal poorly differentiated neuroendocrine neoplasms (neuroendocrine carcinomas) was microdissected and subjected to next-generation sequencing using a colorectal adenocarcinoma-specific panel comprising 196 amplicons covering 32 genes linked to colorectal adenocarcinoma, and poorly differentiated neuroendocrine neoplasm tumorigenesis. Mixed adenoneuroendocrine carcinomas were also examined for microsatellite instability and MLH-1 promoter methylation status. In three mixed adenoneuroendocrine carcinomas, exocrine and endocrine components were analyzed separately. Genetic testing of colorectal mixed adenoneuroendocrine carcinomas identified 43 somatic mutations clustering in 13/32 genes. Sixteen (84%) tumors harbored at least one somatic mutation, two tumors (11%) displayed high microsatellite instability. Compared with colorectal adenocarcinomas, mixed adenoneuroendocrine carcinomas were more frequently BRAF (37%; P=0.006), and less frequently KRAS (21%; P=0.043) and APC (16%; P=0.001) mutated. Point mutations in neuroendocrine neoplasm-related genes like RB1 or RET were not detected, but one tumor harbored a heterozygous RB1 deletion. Separately analyzed adenocarcinoma and neuroendocrine carcinoma components revealed a shared mutational trunk of driver genes involved in colorectal adenocarcinoma carcinogenesis. Colorectal neuroendocrine carcinomas were similar in their mutation profile to colorectal adenocarcinomas, but compared with mixed adenoneuroendocrine carcinomas, had a higher rate of APC mutations (P=0.027). Our data indicate that colorectal mixed adenoneuroendocrine carcinomas and neuroendocrine carcinomas are genetically closely related to colorectal adenocarcinomas, suggesting that the cells giving rise to these tumors primarily have an intestinal coinage. The identification of BRAF mutations and the frequently present KRAS wild-type status principally render some mixed adenoneuroendocrine carcinomas eligible to targeted treatment strategies used for colorectal adenocarcinomas.

Published

2017

27. A novel pretherapeutic gene expression-based risk score for treatment guidance in gastric cancer

Author

Bianca Grosser, Alexander Hapfelmeier, Alexander Novotny, Moritz Jesinghaus, Wilko Weichert, Magdalena Reiche, Julia Slotta-Huspenina, Susanne Blank, Meike Kohlruss, Thomas Schmidt, Katja Ott, Lukas Bauer, and Gisela Keller

Subjects

0301 basic medicine, Oncology, medicine.medical_specialty, Context (language use), 03 medical and health sciences, 0302 clinical medicine, Stomach Neoplasms, Internal medicine, Antineoplastic Combined Chemotherapy Protocols, medicine, Carcinoma, Humans, Genetic Predisposition to Disease, Framingham Risk Score, business.industry, Stomach, Gene Expression Profiling, Hazard ratio, Cancer, Hematology, medicine.disease, Prognosis, Confidence interval, Surgery, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Cohort, business

Abstract

Perioperative chemotherapy is an established treatment of advanced gastric cancer patients. Treatment selection is based on clinical staging (cT). We aimed to establish and validate a prognostic score including clinical and molecular factors, to optimize treatment decisions for these patients.We analyzed 626 carcinomas of the stomach and of the gastro-esophageal junction from two academic centers including primarily resected and pre-/perioperatively treated patients. Patients were divided into a training (N = 269) and validation (N = 357) set. Expression of 11 target genes was measured by quantitative PCR in resected tumors. A risk score to predict overall survival (OS) was generated and validated. Intra-tumoral heterogeneity was assessed by analyzing 50 tumor areas from 10 patients.A risk score including the expression of CCL5, CTNNB1, EXOSC3 and LZTR1 and the clinical parameters cT, tumor localization and histopathologic type suggested two groups with a significant difference in OS [hazard ratio (HR) 0.30; 95% confidence interval (CI) 0.17-0.52]. The risk score was successfully validated in an independent cohort (HR 0.32; 95% CI 0.21-0.51; P 0.001) as well as in subgroups of primarily resected (HR 0.30; 95% CI 0.17-0.54; P 0.001) and pre-/perioperatively treated patients (HR 0.37; 95% CI 0.17-0.81; P = 0.009). A significant difference in OS of high- and low-risk patients was also found in primarily resected patients with intestinal (HR 0.45; 95% CI 0.23-0.90; P = 0.020) and nonintestinal-type carcinomas (HR 0.1; 95% CI 0.02-0.42; P 0.001). Intra-tumor heterogeneity analysis indicated a classification reliability of 95% for a supposed analysis of three biopsies.The identified risk score could substantially contribute to an improved management of gastric cancer patients in the context of perioperative chemotherapy.

Published

2017

28. Evidence for PTGER4, PSCA and MBOAT7 as risk genes for gastric cancer on the genome and transcriptome level

Author

Ines Gockel, Thomas Schmidt, Markus M. Nöthen, Markus Möhler, Karsten Ridwelski, Florian Lordick, Claus Schildberg, Yogesh K. Vashist, Alexander F. Hagel, MA Gonzalez-Carmona, Michael Vieth, Hans Lippert, Angel Lanas, Ralf R. Schumann, Limas Kupčinskas, Philipp Lingohr, Iurii Krasniuk, Peter P. Grimminger, M Ludwig, Johannes Schumacher, Martin Kruschewski, Oliver Pech, Ugne Gyvyte, Timo Hess, A Höblinger, Sophie K. M. Heinrichs, P. Malfertheiner, E. Mangold, J. R. Izbicki, Lutz Hamann, M.W. Büchler, Christiane J. Bruns, Marcis Leja, Katja Ott, Lothar Veits, Marino Venerito, Maria Asuncion Garcia-Gonzalez, Hermann Brenner, Katja Butterbach, E Rodermann, J Becker, Juozas Kupcinskas, Gisela Keller, and Michael Knapp

Subjects

Transcriptome, Genetics, medicine, Cancer, Biology, medicine.disease, Gene, Genome

Published

2017

29. Comprehensive analysis of the

Author

Monika, Morak, Ayseguel, Ibisler, Gisela, Keller, Ellen, Jessen, Andreas, Laner, Daniela, Gonzales-Fassrainer, Melanie, Locher, Trisari, Massdorf, Anke M, Nissen, Anna, Benet-Pagès, and Elke, Holinski-Feder

Subjects

Adult, Male, DNA Methylation, Middle Aged, Colorectal Neoplasms, Hereditary Nonpolyposis, Gene Expression Regulation, Neoplastic, Humans, Female, Genetic Predisposition to Disease, Colorectal Neoplasms, MutL Protein Homolog 1, Promoter Regions, Genetic, Alleles, Germ-Line Mutation

Abstract

Germline defects inWe analysed theWe detected 10 rareWe report the second promoter variant stably inducing a hereditary CEM. Concerning the classification of promoter variants, we discuss contradictory results from the literature for two variants, describe classification discrepancies between existing rules for five variants, suggest the (re-)classification of five promoter variants to (likely) benign and regard four variants as functionally unclear.

Published

2017

30. Independent Validation of a Prognostic Genomic Signature (ColoPrint) for Patients With Stage II Colon Cancer

Author

Helmut Friess, Inès Goossens, Eliane Zeestraten, Tibor Schuster, Annuska M. Glas, Gisela Keller, Robert D. Rosenberg, Matthias Maak, Paul Roepman, Mireille Snel, Ulrich Nitsche, Klaus-Peter Janssen, and Iris Simon

Subjects

Adult, Male, stage II, Oncology, medicine.medical_specialty, Colorectal cancer, Risk Assessment, Internal medicine, Biomarkers, Tumor, medicine, Adjuvant therapy, Humans, Registries, Aged, Neoplasm Staging, Proportional Hazards Models, Aged, 80 and over, Proportional hazards model, business.industry, Gene Expression Profiling, Hazard ratio, Reproducibility of Results, Microsatellite instability, Genomic signature, Genomics, Middle Aged, Gene signature, medicine.disease, Confidence interval, Surgery, colon cancer, Colonic Neoplasms, gene expression, Female, prognosis, Neoplasm Recurrence, Local, business, genomic signature

Abstract

Objectives: The aim of this study was to independently validate a genomic signature developed both to assess recurrence risk in stage II patients and to assist in treatment decisions. Background: Adjuvant therapy is recommended for high-risk patients with stage II colon cancer, but better tools to assess the patients’ prognosis accurately are still required. Methods: Previously, an 18-gene signature had been developed and validated on an independent cohort, using full genome microarrays. In this study, the gene signature was translated and validated as a robust diagnostic test (ColoPrint), using customized 8-pack arrays. In addition, clinical validation of the diagnostic ColoPrint assay was performed on 135 patients who underwent curative resection (R0) for colon cancer stage II in Munich. Fresh-frozen tissue, microsatellite instability status, clinical parameters, and follow-up data for all patients were available. The diagnostic ColoPrint readout was determined blindly from the clinical data. Results: ColoPrint identified most stage II patients (73.3%) as at low risk. The 5-year distant-metastasis free survival was 94.9% for low-risk patients and 80.6% for high-risk patients. In multivariable analysis, ColoPrint was the only significant parameter to predict the development of distant metastasis with a hazard ratio of 4.28 (95% confidence interval, 1.36–13.50; P = 0.013). Clinical risk parameters from the American Society of Clinical Oncology (ASCO) recommendation did not add power to the ColoPrint classification. Technical validation of ColoPrint confirmed stability and reproducibility of the diagnostic platform. Conclusions: ColoPrint is able to predict the development of distant metastasis of patients with stage II colon cancer and facilitates the identification of patients who may be safely managed without chemotherapy.

Published

2013

31. ALK alterations in thyroid cancer

Author

Gisela Keller, Irene Kleinlein, Tanja Seehaus, Heinrich Furst, Markus Kremer, and Wilko Weichert

Subjects

business.industry, Cancer research, Medicine, business, medicine.disease, Thyroid cancer

Published

2016

32. WNT6 is a novel target gene of caveolin-1 promoting chemoresistance to epirubicin in human gastric cancer cells

Author

Fan Lian, Matthias P. Ebert, Philipp Ströbel, Ralf Hofheinz, Elke Burgermeister, G Yuan, R Langer, RM Schmid, Wolfgang Zimmermann, Gisela Keller, Ivonne Regel, Christoph Röcken, T Friedrich, and Ivana Hitkova

Subjects

Adult, Male, Cancer Research, animal structures, Anthracycline, Caveolin 1, Antineoplastic Agents, Biology, Molecular oncology, WNT6, Mice, Transcription Factor 4, Stomach Neoplasms, Cell Line, Tumor, Antineoplastic Combined Chemotherapy Protocols, Genetics, medicine, Animals, Humans, Doxorubicin, Promoter Regions, Genetic, Molecular Biology, Conserved Sequence, Aged, Epirubicin, Aged, 80 and over, Basic Helix-Loop-Helix Leucine Zipper Transcription Factors, Cancer, Middle Aged, Cell cycle, medicine.disease, Molecular biology, Gene Expression Regulation, Neoplastic, Wnt Proteins, Drug Resistance, Neoplasm, Cancer cell, Female, Signal Transduction, Transcription Factors, medicine.drug

Abstract

Resistance to chemotherapy is a major obstacle for curative treatment of human gastric cancer (GC). However, the underlying molecular mechanisms are largely unknown. Wingless-type MMTV integration site family members (WNTs) are secreted glycoproteins involved in embryogenesis and, on inappropriate expression in the adult, in cancer. Here, we show expression of WNT6 in GC patient specimens, human GC cell lines and in a mouse model of GC. In human GC cells, WNT6 expression was enhanced by caveolin-1 (Cav1), a scaffold protein of plasma membrane caveolae. WNT6 knock-down and overexpression experiments demonstrated that WNT6 increased the resistance to apoptotic cell death induced by the anthracycline chemotherapeutics epirubicin (Epi) and doxorubicin (Dox). Epi increased the activity of the human WNT6 promoter through Cav1-dependent binding of β-catenin to the proximal WNT6 promoter. Epi increased both WNT6/Wnt6 and Cav1 expression in human GC cells and within the tumor area of a murine model of GC (CEA424-SV40 TAg). In GC patients, WNT6 expression was positively associated with the tumor stage and the nodal status, and inversely correlated with the response to ECF (Epi, cisplatin, 5-fluorouracil) chemotherapy. These results showed that WNT6 and Cav1 are upregulated by chemotherapeutics and enhance the resistance of GC cells to anthracycline drugs. Understanding the molecular mechanisms driving WNT6/Cav1-induced drug resistance will provide benefits in developing new therapies for GC.

Published

2012

33. The impact of cyclin D1 mRNA isoforms, morphology and p53 in mantle cell lymphoma: p53 alterations and blastoid morphology are strong predictors of a high proliferation index

Author

Karin Bink, Ina Koch, Margit Klier, Julia Slotta-Huspenina, Falko Fend, Gisela Keller, Marcus Kremer, Leticia Quintanilla-Martinez, Mark Raffeld, and Laurence de Leval

Subjects

Adult, Male, Proliferation index, Lymphoma, Mantle-Cell, Biology, Cyclin D1 Mrna, Isoforms, Mantle Cell Lymphoma, Prognosis, Real-Time Polymerase Chain Reaction, Blastoid, Immunoenzyme Techniques, Cyclin D1, RNA Isoforms, medicine, Humans, RNA, Messenger, 3' Untranslated Regions, In Situ Hybridization, Fluorescence, Aged, Cell Proliferation, Aged, 80 and over, Messenger RNA, Reverse Transcriptase Polymerase Chain Reaction, Hematology, Middle Aged, mRNA, Mantle cell lymphoma, medicine.disease, biology.organism_classification, Molecular biology, Reverse transcriptase, Gene expression profiling, Mutation, Immunohistochemistry, Female, Tumor Suppressor Protein p53, Original Articles and Brief Reports

Abstract

Background Mantle cell lymphoma is a clinically heterogeneous disease characterized by overexpression of cyclin D1 protein. Blastoid morphology, high proliferation, and secondary genetic aberrations are markers of aggressive behavior. Expression profiling of mantle cell lymphoma revealed that predominance of the 3'UTR-deficient, short cyclin D1 mRNA isoform was associated with high cyclin D1 levels, a high "proliferation signature" and poor prognosis. Design and Methods Sixty-two cases of mantle cell lymphoma were analyzed for cyclin D1 mRNA isoforms and total cyclin D1 levels by real-time reverse transcriptase polymerase chain reaction, and TP53 alterations were assessed by immunohistochemistry and molecular analysis. Results were correlated with proliferation index and clinical outcome. Results Predominance of the short cyclin D1 mRNA was found in 14 (23%) samples, including four with complete loss of the standard transcript. TP53 alterations were found in 15 (24%) cases. Predominance of 3'UTR-deficient mRNA was significantly associated with high cyclin D1 mRNA levels (P=0.009) and more commonly found in blastoid mantle cell lymphoma (5/11, P=0.060) and cases with a proliferation index of >20% (P=0.026). Both blastoid morphology (11/11, P

Published

2012

34. CyclinD1 and interleukin-1 receptor antagonist polymorphisms are associated with prognosis in neoadjuvant-treated gastric carcinoma

Author

Katja Ott, Alexander Hapfelmeier, Nils Henningsen, Stefan Hois, Karen Becker, Susanne Plaschke, Heinz Höfler, Florian Lordick, Gisela Keller, and Gertraud Stocker

Subjects

Adult, Male, Cancer Research, medicine.medical_specialty, DNA Repair, Genotype, medicine.medical_treatment, Antineoplastic Agents, Kaplan-Meier Estimate, Adenocarcinoma, Polymerase Chain Reaction, Polymorphism, Single Nucleotide, Gastroenterology, Young Adult, Gene Frequency, Stomach Neoplasms, Internal medicine, medicine, Humans, Cyclin D1, Allele, Stomach cancer, Alleles, Aged, Neoplasm Staging, Chemotherapy, business.industry, Cell Cycle, Cancer, Interleukin, Middle Aged, medicine.disease, Neoadjuvant Therapy, Survival Rate, Interleukin 1 Receptor Antagonist Protein, Interleukin 1 receptor antagonist, Oncology, Multivariate Analysis, Immunology, Female, Fluorouracil, Cisplatin, ERCC1, business

Abstract

Purpose We evaluated DNA polymorphisms in genes related to DNA repair, cell-cycle control and tumour microenvironment to determine possible associations with response and survival in neoadjuvant-treated gastric cancer patients. Patients and methods One hundred and seventy eight patients who received platinum/5FU-based chemotherapy were genotyped for 10 polymorphisms in nine genes ( ERCC1 : Asn118Asn, C > T ; ERCC1 : 8092C>A; TP53 : Arg72Pro, G ; cyclinD1 : Pro241Pro, G > A ; STK15 : Phe31Ile, A > T ; VEGF : 936 C > T ; TNF-α : -308 G > A ; interleukin-1b (IL-1B) : -511 C > T ; IL-1 receptor antagonist (IL-1RN) : variable tandem repeat; IL-8 : -251 T > A ). Genotypes were correlated with histopathological and clinical response and overall (OS) and progression-free survival (PFS). Results Only the cyclinD1 genotypes were associated with clinical response ( P χ 2 = 0.044 ). Significantly worse survival rates were noted in patients homozygous for the G-allele as compared to patients with the AG or AA genotypes of the cyclinD1 polymorphism (OS: P log-rank =0.024; PFS: P log-rank =0.007) and in patients homozygous for the short allele compared to all other genotypes at the IL-1RN polymorphic locus (OS: P log-rank =0.026; PFS: P log-rank =0.013). The combination of both unfavourable genotypes demonstrated strong prognostic relevance (OS: P log-rank =0.006; PFS: P log-rank =0.001). Multivariate analysis for OS in the group of completely resected patients ( n =139) revealed statistical significance for ypM ( P P cyclinD1/IL-1RN genotypes ( P =0.043). Conclusion The cyclinD1 and IL-1RN polymorphisms were associated with survival. The combination of specific cyclinD1 and IL-1RN genotypes showed a particular prognostic relevance and should be considered an independent prognostic marker for neoadjuvant-treated gastric cancer patients.

Published

2009

35. MethyQESD, a robust and fast method for quantitative methylation analyses in HNPCC diagnostics using formalin-fixed and paraffin-embedded tissue samples

Author

Wolfgang Dietmaier, Gisela Keller, Katrin Kurz, Marcus Bettstetter, Corinna Vogel, Monika Morak, Ferdinand Hofstaedter, Petra Ruemmele, Stefan Dechant, and Elke Holinski-Feder

Subjects

congenital, hereditary, and neonatal diseases and abnormalities, Tissue Fixation, Biology, MLH1, Pathology and Forensic Medicine, Formaldehyde, medicine, Humans, Promoter Regions, Genetic, neoplasms, Molecular Biology, Adaptor Proteins, Signal Transducing, DNA Primers, Paraffin Embedding, Base Sequence, Nuclear Proteins, Reproducibility of Results, nutritional and metabolic diseases, Microsatellite instability, Cancer, Promoter, Cell Biology, Methylation, DNA Methylation, medicine.disease, Colorectal Neoplasms, Hereditary Nonpolyposis, digestive system diseases, ROC Curve, DNA methylation, Cancer research, Microsatellite, DNA mismatch repair, MutL Protein Homolog 1

Abstract

Promoter hypermethylation occurs in various tumors and leads to silencing of tumor-relevant genes. Thus, promoter methylation analysis (MA) has been established as an important tool in cancer research and diagnostics. Here we present MethyQESD (methylation-quantification of endonuclease-resistant DNA) as a fast, easy, precise and reliable method for quantitative MA without the need of bisulfite-treatment or fluorescent probes. Though MethyQESD principally works with any gene promoter we established MethyQESD for the mismatch repair gene MLH1 and tested its utility to differentiate between sporadic microsatellite unstable (MSI-H) colorectal cancer and hereditary nonpolyposis colorectal cancer (HNPCC) by quantitative MLH1 MA. We investigated formalin-fixed and paraffin-embedded tissue samples from a previously published, well-characterized tumor collective comprising 25 HNPCC, 14 sporadic MSI-H CRC and 16 sporadic microsatellite stable (MSS) CRC. We found a high accuracy of MethyQESD by spiking experiments with dilution series of methylated (SW48 cancer cell line) and unmethylated (blood) DNA (Pearson's r=0.9997 (proximal MLH1 promoter region), r=0.9976 (distal MLH1 promoter region)). MethyQESD and conventional quantitative MA using of 96 formalin-fixed and paraffin-embedded CRC showed a high degree of concordance of both methods (Pearson's r=0.885). HNPCC tumors showed either null MLH1 methylation or a significantly lower degree of MLH1 methylation than sporadic MSI-H CRC (P

Published

2008

36. Therapy Related Markers and Response Prediction Towards Multimodal Treatment of Carcinomas of the Upper Gastrointestinal Tract

Author

Heinz Höfler, Rupert Langer, and Gisela Keller

Subjects

Pharmacology, Oncology, medicine.medical_specialty, Therapy related, business.industry, Gastroenterology, Internal medicine, Genetics, Molecular Medicine, Medicine, Multimodal treatment, Upper gastrointestinal, business, Molecular Biology, Genetics (clinical)

Published

2008

37. Glutathione-S-transferase P1, T1 and M1 genetic polymorphisms in neoadjuvant-treated locally advanced gastric cancer: GSTM1-present genotype is associated with better prognosis in completely resected patients

Author

Gisela Keller, Florian Lordick, Katja Ott, J. R. Siewert, Heinz Höfler, Karen Becker, and Kurt Ulm

Subjects

Male, medicine.medical_specialty, Genotype, medicine.medical_treatment, Antineoplastic Agents, Polymerase Chain Reaction, Gastroenterology, Disease-Free Survival, GSTP1, Gastrectomy, Stomach Neoplasms, Internal medicine, Multiplex polymerase chain reaction, medicine, Humans, Stomach cancer, neoplasms, Glutathione Transferase, Retrospective Studies, Chemotherapy, Polymorphism, Genetic, integumentary system, biology, business.industry, Cancer, Middle Aged, Hepatology, Prognosis, medicine.disease, Neoadjuvant Therapy, Glutathione S-transferase, Glutathione S-Transferase pi, Immunology, biology.protein, Lymph Node Excision, Female, Cisplatin, business

Abstract

Neoadjuvant chemotherapy in gastric cancer is now standard in the Western world; however, only 30–40% of the patients respond to induction therapy. Pretherapeutic predictors of response and prognosis would be of utmost interest to individualize treatment. Glutathione-S-transferase enzymes detoxify therapeutic drugs such as platin derivates and may influence outcome of the treated patients. Therefore, glutathione-S-transferase (GST) polymorphisms were assessed as predictive markers in cisplatinum-based neoadjuvant-treated gastric cancer. DNA was isolated from 139 patients with locally advanced gastric cancer (cT3/4 anyN cM0) before chemotherapy. Multiplex polymerase chain reaction was used for GSTT1 and GSTM1 genes, and allelic discrimination assay with the TaqMan system for the GSTP1 gene. One hundred ten patients could be analyzed for GSTT1 (T-:23; T + 87), 112 for GSTM1 (M-:52; M +:60) and 132 for GSTP1 (Ile/Ile: 55; Ile/Val: 59; Val/Val: 18). There was no significant correlation between any of the GSTT1, GSTM1, or GSTP1 genotypes and patients’ characteristics or histopathological data; only the GSTM1+ genotype was associated with the non-intestinal subtype of the Lauren classification (p = 0.045). GSTT1, GSTM1, and GSTP1 genotypes were not correlated with response to chemotherapy (p = 0.57, p = 0.38, p = 0.33). In R0 resected patients, we found an improved survival for patients with the GSTM1-present genotype compared to patients with the GSTM1-null genotype (p = 0.017). Moreover, the GSTM1-present genotype showed a significantly better tumor-related (p = 0.017) and disease-free survival (p = 0.029). None of the common GST polymorphisms predicts response in our study, but the GSTM1+ genotype was associated with a better prognosis in completely resected patients. Further investigations on chemotherapy-associated gene polymorphisms are warranted.

Published

2008

38. No association between MUTYH and MSH6 germline mutations in 64 HNPCC patients

Author

Verena, Steinke, Nils, Rahner, Monika, Morak, Gisela, Keller, Hans K, Schackert, Heike, Görgens, Wolff, Schmiegel, Brigitte, Royer-Pokora, Wolfgang, Dietmaier, Matthias, Kloor, Christoph, Engel, Peter, Propping, Stefan, Aretz, and J, Schaefer

Subjects

Silent mutation, congenital, hereditary, and neonatal diseases and abnormalities, Biology, medicine.disease_cause, DNA Glycosylases, Loss of heterozygosity, Germline mutation, Gene Frequency, MUTYH, Genetics, medicine, Humans, Missense mutation, neoplasms, Germ-Line Mutation, Genetics (clinical), Mutation, nutritional and metabolic diseases, Middle Aged, Colorectal Neoplasms, Hereditary Nonpolyposis, digestive system diseases, DNA-Binding Proteins, MSH6, MSH2, Case-Control Studies, Cancer research, Female

Abstract

Hereditary non-polyposis colorectal cancer (HNPCC) is an autosomal dominant tumour predisposition syndrome caused by germline mutations in mismatch repair (MMR) genes. In contrast to MLH1 and MSH2, germline mutations in MSH6 are associated with a milder and particularly variable phenotype. Based on the reported interaction of the MMR complex and the base excision repair protein MUTYH, it was hypothesised that MUTYH mutations serve as phenotypical modifiers in HNPCC families. Recently, a significantly higher frequency of heterozygosity for MUTYH mutations among MSH6 mutation carriers was reported. We examined 64 MSH6 mutation carriers (42 truncating mutations, 19 missense mutations and 3 silent mutations) of the German HNPCC Consortium for MUTYH mutations by sequencing the whole coding region of the gene. Monoallelic MUTYH mutations were identified in 2 of the 64 patients (3.1%), no biallelic MUTYH mutation carrier was found. The frequency of MUTYH mutations was not significantly higher than that in healthy controls, neither in the whole patient group (P=0.30) nor in different subgroups regarding mutation type. Our results do not support the association between MSH6 mutations and heterozygosity for MUTYH mutations.

Published

2008

39. High EPHB2 mutation rate in gastric but not endometrial tumors with microsatellite instability

Author

Juan C. Díaz-Chico, Robert M.W. Hofstra, Diego Arango, Renee C. Niessen, Ana Ferreira, Raquel Ramírez, Alberto Plaja, E. Espin, Raquel Seruca, Germán Rodríguez, Sérgia Velho, Simó Schwartz, Hiroyuki Yamamoto, Laureano León, Luis Cirnes, Nicolás Díaz-Chico, Gisela Keller, Kohzoh Imai, Manel Armengol, Veronica Davalos, C. Bilbao, Johannes Gebert, Orlando Falcón, Manuel Perucho, G. Dallenbach-Hellweg, Stefan M. Woerner, and Higinio Dopeso

Subjects

EXPRESSION, Cancer Research, Mutation rate, congenital, hereditary, and neonatal diseases and abnormalities, Receptor, EphB2, DNA Mutational Analysis, FRAMESHIFT MUTATIONS, RECEPTOR TYROSINE KINASE, Biology, medicine.disease_cause, Polymerase Chain Reaction, Receptor tyrosine kinase, Frameshift mutation, Stomach Neoplasms, Genetics, medicine, TARGET GENES, Humans, cancer, EPHB2, endometrium, Frameshift Mutation, Molecular Biology, Polymorphism, Single-Stranded Conformational, colorectal, Mutation, Endometrial cancer, Microsatellite instability, Cancer, COLORECTAL TUMORS, DNA, Neoplasm, medicine.disease, Molecular biology, digestive system diseases, Endometrial Neoplasms, Cancer research, biology.protein, Female, microsatellite instability, Carcinogenesis, stomach, Microsatellite Repeats

Abstract

The EPH/EFN family of receptor tyrosine kinases regulates cell adhesion and migration and has an important role in controlling cell positioning in the normal intestinal epithelium. Inactivation of EPHB2 has recently been shown to accelerate tumorigenesis in the colon and rectum, and we have previously demonstrated frequent frameshift mutations (41%) in an A9 coding microsatellite repeat in exon 17 of EPHB2 in colorectal tumors with microsatellite instability (MSI). In this study, we extended these analyses to extracolonic MSI cancers, and found frameshift EPHB2 mutations in 39% (25/64) of gastric tumors and 14% (8/56) of endometrial tumors. Regression analysis of these EPHB2 mutation data on the basis of our previously proposed statistical model identified EPHB2 as a selective target of frameshift mutations in MSI gastric cancers but not in MSI endometrial carcinomas. These results suggest a functional role for EPHB2 in gastric tumor progression, and emphasize the differences between the tumorigenic processes in MSI gastrointestinal and endometrial cancer.

Published

2007

40. Clinical Significance of NOTCH1 and NOTCH2 Expression in Gastric Carcinomas: An Immunohistochemical Study

Author

Alexander Hapfelmeier, Axel Walch, Alexander Novotny, Karen Becker, Katja Ott, Lukas Bauer, Rupert Langer, Julia Slotta-Huspenina, Agnes Takacs, and Gisela Keller

Subjects

Oncology, Cancer Research, medicine.medical_specialty, Pathology, endocrine system, receptor NOTCH2, medicine.medical_treatment, receptor NOTCH1, Notch signaling pathway, 610 Medicine & health, chemotherapy, lcsh:RC254-282, Text mining, Internal medicine, Tumor stage, Medicine, Clinical significance, Original Research, Chemotherapy, Tissue microarray, stomach neoplasms, business.industry, Cancer, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, medicine.disease, ddc, embryonic structures, immunohistochemistry, 570 Life sciences, biology, Immunohistochemistry, Prognosis, Receptor Notch1, Receptor Notch2, Stomach Neoplasms, sense organs, prognosis, business

Abstract

BACKGROUND NOTCH signaling can exert oncogenic or tumor suppressive functions and can contribute to chemotherapy resistance in cancer. In this study, we aimed to clarify the clinicopathological significance and the prognostic and predictive value of NOTCH1 and NOTCH2 expression in gastric cancer (GC). METHODS NOTCH1 and NOTCH2 expression was determined immunohistochemically in 142 primarily resected GCs using tissue microarrays and in 84 pretherapeutic biopsies from patients treated by neoadjuvant chemotherapy. The results were correlated with survival, response to therapy, and clinico-pathological features. RESULTS Primarily resected patients with NOTCH1-negative tumors demonstrated worse survival. High NOTCH1 expression was associated with early-stage tumors and with significantly increased survival in this subgroup. Higher NOTCH2 expression was associated with early-stage and intestinal-type tumors and with better survival in the subgroup of intestinal-type tumors. In pretherapeutic biopsies, higher NOTCH1 and NOTCH2 expression was more frequent in non-responding patients, but these differences were statistically not significant. CONCLUSION Our findings suggested that, in particular, NOTCH1 expression indicated good prognosis in GC. The close relationship of high NOTCH1 and NOTCH2 expression with early tumor stages may indicate a tumor-suppressive role of NOTCH signaling in GC. The role of NOTCH1 and NOTCH2 in neoadjuvantly treated GC is limited.

Published

2015

41. Genotype-Phenotype Comparison of German MLH1 and MSH2 Mutation Carriers Clinically Affected With Lynch Syndrome: A Report by the German HNPCC Consortium

Author

Christoph Engel, Johannes Gebert, Gabriela Moeslein, Karsten Schulmann, Hans K. Schackert, Wolff Schmiegel, Constanze Pagenstecher, Timm O. Goecke, Josef Rueschoff, Elke Holinski-Feder, Stefan Krüger, Nicolaus Friedrichs, Matthias Kloor, Markus Loeffler, Elisabeth Mangold, Erdmute Kunstmann, Holger Vogelsang, Gisela Keller, Peter Propping, and Wolfgang Dietmaier

Subjects

Adult, Male, Heterozygote, Cancer Research, Genotype, medicine.disease_cause, MLH1, White People, Germline mutation, Germany, medicine, Humans, Germ-Line Mutation, Adaptor Proteins, Signal Transducing, Genetics, Mutation, Rectal Neoplasms, business.industry, Age Factors, Nuclear Proteins, Neoplasms, Second Primary, medicine.disease, Colorectal Neoplasms, Hereditary Nonpolyposis, Immunohistochemistry, Phenotype, digestive system diseases, Lynch syndrome, MutS Homolog 2 Protein, Oncology, Cohort, Female, DNA mismatch repair, Carrier Proteins, MutL Protein Homolog 1, business, Microsatellite Repeats

Abstract

Purpose Lynch syndrome is linked to germline mutations in mismatch repair genes. We analyzed the genotype-phenotype correlations in the largest cohort so far reported. Patients and Methods Following standard algorithms, we identified 281 of 574 unrelated families with deleterious germline mutations in MLH1 (n = 124) or MSH2 (n = 157). A total of 988 patients with 1,381 cancers were included in this analysis. Results We identified 181 and 259 individuals with proven or obligatory and 254 and 294 with assumed MLH1 and MSH2 mutations, respectively. Age at diagnosis was younger both in regard to first cancer (40 v 43 years; P < .009) and to first colorectal cancer (CRC; 41 v 44 years; P = .004) in MLH1 (n = 435) versus MSH2 (n = 553) mutation carriers. In both groups, rectal cancers were remarkably frequent, and the time span between first and second CRC was smaller if the first primary occurred left sided. Gastric cancer was the third most frequent malignancy occurring without a similarly affected relative in most cases. All prostate cancers occurred in MSH2 mutation carriers. Conclusion The proportion of rectal cancers and shorter time span to metachronous cancers indicates the need for a defined treatment strategy for primary rectal cancers in hereditary nonpolyposis colorectal cancer patients. Male MLH1 mutation carriers require earlier colonoscopy beginning at age 20 years. We propose regular gastric surveillance starting at age 35 years, regardless of the familial occurrence of this cancer. The association of prostate cancer with MSH2 mutations should be taken into consideration both for clinical and genetic counseling practice.

Published

2006

42. Absence of association between cyclin D1 (CCND1) G870A polymorphism and age of onset in hereditary nonpolyposis colorectal cancer

Author

Stefan Krüger, Christoph Engel, Andrea Bier, Elisabeth Mangold, Constanze Pagenstecher, Magnus von Knebel Doeberitz, Elke Holinski-Feder, Gabriela Moeslein, Gisela Keller, Erdmute Kunstmann, Waltraut Friedl, Jens Plaschke, Josef Rüschoff, Hans K. Schackert, and null The German HNPCC-Consortium

Subjects

Adult, Male, congenital, hereditary, and neonatal diseases and abnormalities, Cancer Research, Adolescent, Genotype, Colorectal cancer, Biology, MLH1, Gene Frequency, medicine, Humans, Cyclin D1, Age of Onset, neoplasms, Aged, Genetics, Polymorphism, Genetic, Middle Aged, medicine.disease, Colorectal Neoplasms, Hereditary Nonpolyposis, Phenotype, digestive system diseases, Genotype frequency, Oncology, MSH2, Cancer research, Female, DNA mismatch repair, Age of onset

Abstract

CCND1 encodes cyclin D1, which plays an important role in the G 1 to S phase transition of the cell cycle. A common polymorphism (c.G870A) increases alternate splicing. Hereditary nonpolyposis colorectal cancer (HNPCC) is caused by mutations in mismatch repair (MMR) genes, mainly MSH2 and MLH1 , and shows a wide range in the age of its onset (AO), suggesting the existence of other modifying genetic factors. To date, two studies have investigated the association between CCND1 G/A variation and AO in HNPCC with contradictory results in 86 and 146 MMR mutation carriers, respectively. To clarify the role of the CCND1 G/A variation in HNPCC, we performed a study in 406 individuals carrying exclusively clear cut pathogenic mutations in MSH2 or MLH1 . We did not observe a significant difference in genotype frequencies of affected and unaffected mutation carriers and healthy controls. A significant association between CCND1 genotypes and AO was found neither in the global comparison (log-rank, P =0.2981; Wilcoxon, P =0.2567) nor in a multivariate Cox regression analysis (hazard ratios 1.111, 95%CI 0.950–1.299, P =0.188 and 1.090, 95%CI 0.868–1.369, P =0.459 for the additive and dominant effect, respectively). We conclude, that the CCND1 G870A sequence variation is not a genetic modifier of the phenotype of HNPCC.

Published

2006

43. Prevalence of the mismatch-repair-deficient phenotype in colonic adenomas arising in HNPCC patients: results of a 5-year follow-up study

Author

Annegret Müller, Heinz Becker, Christoph Poremba, Josef Rüschoff, Wolfgang Dietmaier, Frank Brasch, Gisela Keller, Reinhard Büttner, Tina Bocker Edmonston, Jürgen Faß, Gabriela Westphal, Nicolaus Friedrichs, Matthias Kloor, Daniela Aust, and Carmen Beckmann

Subjects

Adenoma, Oncology, congenital, hereditary, and neonatal diseases and abnormalities, medicine.medical_specialty, Pathology, DNA Repair, Base Pair Mismatch, MLH1, Germline mutation, Internal medicine, Prevalence, medicine, Carcinoma, Humans, neoplasms, business.industry, Gastroenterology, nutritional and metabolic diseases, Microsatellite instability, Cancer, medicine.disease, Colorectal Neoplasms, Hereditary Nonpolyposis, digestive system diseases, MSH6, Phenotype, Molecular Diagnostic Techniques, MSH2, Microsatellite Instability, business, Follow-Up Studies

Abstract

In hereditary nonpolyposis colorectal cancer (HNPCC) syndrome, more than 90% of the carcinomas show microsatellite instability (MSI) due to a loss of mismatch repair (MMR) function. Although adenomas are very common in HNPCC and demonstrate an accelerated adenoma-carcinoma sequence, data about the prevalence and development of MSI in these early neoplastic lesions are lacking. To determine whether MSI and loss of MMR-protein expression are already present in early stages of tumorigenesis and could therefore be used as a screening tool to identify HNPCC patients before they develop an invasive carcinoma, we analyzed 71 adenomas of 36 HNPCC patients during a 5-year follow-up study. These 36 patients were part of a cohort of 122 HNPCC patients who were investigated at the Institute of Pathology, Klinikum Kassel, as part of the multicentric German HNPCC Consortium, which currently serves more than 2,880 registered families. The diagnosis of HNPCC was based either on the detection of a pathogenic germline mutation in the MSH2, MLH1, or MSH6 genes or in cases where a pathogenic mutation was not found; diagnosis of HNPCC was made, because all patients fulfilled the Amsterdam or Bethesda criteria and revealed a high degree of MSI (MSI-H) as well as loss of one of the MMR proteins by IHC in the cancer tissue. We found that most adenomas (58/71) were MSI-H and had loss of MMR-protein expression. Of the 71 adenomas, 3 were MSI-H with expression of all MMR proteins, and 3 out of 71 displayed loss of a MMR protein with the microsatellites being classified as microsatellite stable (MSS). However, 7 of the 31 adenomas that were located more than 5 cm away from the carcinoma revealed an MSS status (n=6) or low in MSI (n=1) and expressed all MMR proteins. In summary, a significant percentage of HNPCC-associated adenomas (7/31, 22.6%) developing at a distance of more than 5 cm from the corresponding carcinoma did not show the MSI-H MMR-deficient phenotype and expressed all MMR genes. To our knowledge, this is the first study that shows that in most HNPCC patients, the mutator pathway is already detectable in adenomas, but MMR-proficient adenomas can also be found. Therefore, screening for MMR deficiency should not be applied routinely in adenomas with the goal to identify HNPCC patients.

Published

2006

44. Thethymidylate synthase tandem repeat promoter polymorphism: A predictor for tumor-related survival in neoadjuvant treated locally advanced gastric cancer

Author

Ulrich Fink, Jörg Rüdiger Siewert, Christoph Schuhmacher, Katja Ott, Florian Lordick, Noemi Marton, Alexander Novotny, Heinz Höfler, Karen Becker, James Mueller, Holger Vogelsang, Michael Kobl, Gisela Keller, and Kurt Ulm

Subjects

Adult, Male, Cancer Research, Pathology, medicine.medical_specialty, Genotype, Polymorphism, Single Nucleotide, Thymidylate synthase, Gene Frequency, Tandem repeat, Stomach Neoplasms, medicine, Humans, Promoter Regions, Genetic, Stomach cancer, Genotyping, Methylenetetrahydrofolate Reductase (NADPH2), Aged, Aged, 80 and over, biology, Cancer, Thymidylate Synthase, Middle Aged, Prognosis, medicine.disease, Survival Analysis, Neoadjuvant Therapy, Treatment Outcome, Oncology, Tandem Repeat Sequences, Fluorouracil, Methylenetetrahydrofolate reductase, Multivariate Analysis, Cancer research, biology.protein, Female, medicine.drug

Abstract

We evaluated DNA polymorphisms in the thymidylate synthase (TS) and 5,10-methylene-tetrahydrofolate reductase (MTHFR) genes for an association with response and survival in locally advanced gastric cancer treated with 5-FU based preoperative chemotherapy (CTx). DNA of 238 patients (CTx-group: total n = 135, completely resected (R0) n = 102; without CTx: R0 n = 103) was isolated from blood or from nontumorous tissues. In the CTx-group, genotyping of the tandem repeat and the G/C polymorphism in the triple repeat in the promoter region of the TS gene and of the C677T polymorphism of the MTHFR gene was performed. None of the TS or MTHFR genotypes were associated with histopathological response and only the TS tandem repeat polymorphism was significantly related to survival (all patients n = 135, p = 0.002; R0 resected patients n = 102, p = 0.007; log-rank test). Multivariate analysis revealed ypN (p0.001) and the TS tandem repeat polymorphism as independent prognostic factors in the CTx-R0-group (p = 0.003). Analyzing the prognostic significance of the TS polymorphisms in the R0-group without CTx, TS genotypes were not significantly associated with survival. Comparing survival between R0 patients with and without CTx in the respective TS genotype groups of the tandem repeat polymorphism, a significant survival benefit for the patients with CTx was found for the 2rpt/2rpt (n = 49; p = 0.002) and 2rpt/3rpt genotypes (n = 99; p = 0.004), but not for the 3rpt/3rpt genotype (n = 57; p = 0.93). Patients' survival after CTx was associated with the TS tandem repeat polymorphism. CTx did not improve survival of patients with the 3rpt/3rpt genotype. Thus, a different therapy might be more appropriate for these patients.

Published

2006

45. Hereditary non-polyposis colorectal cancer: clinical and molecular evidence for a new entity of hereditary colorectal cancer

Author

Peter Lohse, Reinhard Kopp, Uwe Schiemann, Jens Daum, Monika Grabowski, Yvonne Mueller-Koch, Brigitte Kerker, Manfred Gross, Elke Holinski-Feder, Gisela Keller, Gabriele Henke, Holger Vogelsang, Daniela E. Aust, Michael H. Muders, Ingrid Becker, and Michael Scholz

Subjects

Adult, Male, Oncology, medicine.medical_specialty, Pathology, Letter, Familial Colorectal Cancer Type X, Colorectal cancer, Molecular evidence, MLH1, Neoplastic Syndromes, Hereditary, Internal medicine, medicine, Humans, Age of Onset, Adaptor Proteins, Signal Transducing, Splenic flexure, business.industry, Gastroenterology, Nuclear Proteins, Nucleic Acid Hybridization, Microsatellite instability, Middle Aged, medicine.disease, Colorectal Neoplasms, Hereditary Nonpolyposis, Neoplasm Proteins, Pedigree, MutS Homolog 2 Protein, MSH2, Population Surveillance, Mutation, Disease Progression, Female, Age of onset, Carrier Proteins, MutL Protein Homolog 1, business, Microsatellite Repeats

Abstract

Hereditary non-polyposis colorectal cancer (HNPCC) is clinically defined by familial clustering of colorectal cancer and other associated tumours.By thorough molecular and clinical evaluation of 41 families, two different groups were characterised: group 1, 25 families with truncating mutations in MLH1 or MSH2 (12 novel mutations); and group 2, 16 Amsterdam positive families without mutations in these genes and without microsatellite instability in their corresponding tumours.Significant clinical differences between these two groups were found. Firstly, earlier age of onset for all colorectal cancers (median 41 v 55 years; p0.001) and all tumours (median 43 v 56 years; p = 0.022) was observed, comparing groups 1 and 2. Secondly, 68% of the index colorectal cancers were localised proximally of the splenic flexure in group 1 compared with 14% in group 2 (p0.010). Thirdly, more synchronous and metachronous colorectal (p = 0.017) and extracolorectal tumours (p0.001) were found in group 1. Fourthly, a higher colorectal adenoma/carcinoma ratio (p = 0.030) and a tendency towards more synchronous or metachronous adenomas in group 2 (p = 0.084) was observed, indicating a slower progression of adenomas to carcinomas. As three mutation negative tumours revealed chromosomal instability after comparative genomic hybridisation, these tumours may be caused by one or more highly penetrant disease alleles from the chromosomal instability pathway.These data show that HNPCC includes at least two entities with clinical and molecular differences. This will have implications for surveillance programmes and for cancer research.

Published

2005

46. Desmoglein 2 is expressed abnormally rather than mutated in familial and sporadic gastric cancer

Author

Holger Vogelsang, Ingrid Becker, Karin Biedermann, Susanne Plaschke, Jörg Rüdiger Siewert, Gisela Keller, and Heinz Höfler

Subjects

Adult, Male, Pathology, medicine.medical_specialty, Biology, medicine.disease_cause, Desmoglein, Germline, Pathology and Forensic Medicine, Germline mutation, Stomach Neoplasms, medicine, Humans, Missense mutation, Genetic Predisposition to Disease, Stomach cancer, Germ-Line Mutation, Aged, Aged, 80 and over, Family Health, Mutation, Desmoglein 2, Cancer, DNA, Neoplasm, Desmosomes, Middle Aged, medicine.disease, Immunohistochemistry, Neoplasm Proteins, Gene Expression Regulation, Neoplastic, Cytoskeletal Proteins, Desmoplakins, Cancer research, Female, Desmogleins, Carcinogenesis, Cell Adhesion Molecules

Abstract

Alterations of the cell adhesion molecule E-cadherin have been demonstrated in sporadic and hereditary gastric carcinomas. A cell adhesion molecule with functional similarity to E-cadherin is desmoglein 2 (Dsg2), a major component of the desmosomes. In this study, we investigated whether alterations of Dsg2 are involved in gastric carcinogenesis and whether germline mutations contribute to a genetic predisposition in familial gastric cancer patients with no germline mutations in the E-cadherin gene. Seventy-five formalin-fixed, paraffin-embedded tissues from 37 familial and 38 sporadic gastric carcinomas were analysed for Dsg2 expression by immunohistochemistry. DNA from 31 familial gastric cancer patients was analysed for germline mutations and five sporadic tumours were analysed for somatic mutations by DHPLC. Of the 75 tumours, 25 (33%) demonstrated abnormal (reduced and/or non-membrane-associated) Dsg2 expression. There was a trend towards more frequent abnormal expression in diffuse type (42%) than in intestinal type tumours (18%) (p = 0.066). One germline missense variant leading to a non-conservative amino acid change (c. 2810 C > A, Thr 937 Asn) was found in a familial gastric cancer patient with a diffuse type tumour. No somatic mutations were identified. The observed abnormal expression of Dsg2 protein suggests that this molecule is involved in the carcinogenesis of a subset of gastric carcinomas, in particular of the diffuse type. Somatic mutations in the gene do not seem to be a very frequent inactivation event and the finding of no clear pathogenic germline mutation rules out Dsg2 as a major gastric cancer predisposition gene.

Published

2005

47. Novel strategy for optimal sequential application of clinical criteria, immunohistochemistry and microsatellite analysis in the diagnosis of hereditary nonpolyposis colorectal cancer

Author

Josef Rüschoff, Susanne Stemmler, Christopher Poremba, Hans K. Schackert, Markus Loeffler, Christian Pox, Peter Kienle, Matthias Kloor, Elisabeth Mangold, Christoph Engel, Jochen Forberg, Constanze Pagenstecher, Elke Holinski-Feder, Petra Rümmele, Gabriela Moeslein, Wolfgang Dietmaier, Nicolaus Friedrichs, Gisela Keller, Jens Plaschke, and Reinhard Buettner

Subjects

Adult, Male, Oncology, Cancer Research, medicine.medical_specialty, Pathology, Amsterdam criteria, Time Factors, DNA Repair, Base Pair Mismatch, Colorectal cancer, Guidelines as Topic, MLH1, Logistic regression, Sensitivity and Specificity, Diagnosis, Differential, Germline mutation, stomatognathic system, Predictive Value of Tests, Internal medicine, medicine, Humans, Genetic Testing, Germ-Line Mutation, Adaptor Proteins, Signal Transducing, business.industry, Nuclear Proteins, Middle Aged, medicine.disease, Colorectal Neoplasms, Hereditary Nonpolyposis, Immunohistochemistry, MutS Homolog 2 Protein, MSH2, Female, DNA mismatch repair, Carrier Proteins, MutL Protein Homolog 1, business, DNA Damage, Microsatellite Repeats

Abstract

Clinical criteria, microsatellite analysis (MSA) and immunohistochemistry (IHC) are important diagnostic tools for identification of hereditary nonpolyposis colorectal cancer (HNPCC) patients who are likely to carry pathogenic germline mutations in mismatch repair genes. Based on MSA and IHC results and subsequent mutation analyses of 1,119 unrelated index patients meeting the Amsterdam II criteria or the classical Bethesda guidelines, we analyzed the value of these tools to predict MLH1 and MSH2 mutations with the aim of establishing optimal strategies for their most efficient sequential use. The overall prevalence of pathogenic germline mutations in our cohort was 20.6% (95% CI = 18.3-23.0%) and 61.8% (95% CI = 56.8-66.6%), respectively, after MSA/IHC-based preselection. IHC was highly predictive (99.1%) and specific (99.6%) with regard to MSA. However, 14 out of 230 mutations (6%) escaped detection by IHC. Thus, IHC cannot be recommended to substitute MSA fully. Nonetheless, IHC is important to indicate the gene that is likely to be affected. To combine both methods efficiently, we propose a novel screening strategy that provides 2 alternative ways of sequential IHC and MSA application, either using IHC or MSA in the first place. A logistic regression model based on the age of the index patient at first tumor diagnosis and the number of fulfilled HNPCC criteria is used to allocate individual patients to that alternative pathway that is expected to be least expensive. A cost analysis reveals that about 25% of the costs can be saved using this strategy.

Published

2005

48. Molekularpathologische Diagnostik beim erblichen Dickdarmkarzinom

Author

Gisela Keller, Mueller W, Josef Rüschoff, Matthias Kloor, Muders M, Plaschke J, Petra Rümmele, Christopher Poremba, Müller A, Roggendorf B, Brasch F, Micaela Mathiak, Daniela Aust, Blasenbreu-Vogt S, and Reinhard Büttner

Subjects

Oncology, medicine.medical_specialty, business.industry, Colorectal cancer, Genetic counseling, Cancer, Microsatellite instability, MLH1, medicine.disease, digestive system diseases, Pathology and Forensic Medicine, MSH6, MSH2, Internal medicine, PMS2, Medicine, business

Abstract

Although twin studies indicate that inherited genetic factors contribute to about 35% of colorectal cancers (CRC), the exact genetic background has currently been elucidated in only 5-10% of cases. These comprise several hereditary cancer predisposition syndromes that present with a high number of syn- or metachronous neoplasms within an affected person and/or family. Many of these tumors exhibit typical histopathological changes. In general, one should discriminate between cancer syndromes associated with adenomatous and non-adenomatous (i.e., hamartomatous) polyps, the latter being quite rare. The patient's age often serves as a substantial hint to hereditary cancer. The next step of diagnostic work-up includes analysis of microsatellite instability (MSI) together with immunohistochemical detection of a loss of expression in one of the most frequently affected mismatch repair genes (MSH2, MSH6; MLH1, PMS2). Finally, the molecular demonstration of a gene mutation in the blood or germline is the most expensive and tedious procedure. This requires a signed informed consent from the patient after appropriate genetic counseling.

Published

2004

49. Relationship between E-cadherin gene mutation and p53 gene mutation, p53 accumulation, Bcl-2 expression and Ki-67 staining in diffuse-type gastric carcinoma

Author

Birgit Luber, Ingrid Becker, Susanne Plaschke, Karl-Friedrich Becker, Elena Fricke, Martina Rudelius, Christina Schott, Christine Hermannstädter, Raymonde Busch, Gisela Keller, Erika Rosivatz, and Heinz Höfler

Subjects

Cancer Research, Mutation, biology, Tumor suppressor gene, Mutant, Gene mutation, medicine.disease, medicine.disease_cause, Oncology, Ki-67, biology.protein, Carcinoma, medicine, Cancer research, Immunohistochemistry, Adenocarcinoma

Abstract

E-cadherin mutations are found in 50% of diffuse-type gastric carcinoma, but not in intestinal gastric carcinoma. Because cell-cell adhesion mediated by E-cadherin plays an important role in epithelial cell survival, E-cadherin mutations could alter the apoptotic behavior of tumor cells. p53 and Bcl-2 family members are also important regulators of cellular apoptosis. This is the first study that investigates the relationship between E-cadherin gene mutation and p53 gene mutation, p53 accumulation, Bcl-2 expression, and Ki-67 expression in diffuse-type gastric carcinoma (24 cases, E-cadherin mutation status: wild-type in 8 patients and mutant in 16 patients). The mutation status of exons 5-8 of p53 was analyzed by denaturing high pressure liquid chromatography (DHPLC) in formalin-fixed, paraffin-embedded tumor sections, followed by direct sequencing of cases with aberrant chromatographic patterns. p53 mutations were found in 1 of 8 tumors without E-cadherin mutation (12.5%) and in 1 of 16 tumors with E-cadherin mutation (6.3%), a difference that was not statistically significant (p = 1.00). p53 accumulation was found in 8 of 24 tumors (33.3%) by immunohistochemical staining. p53 accumulation was significantly more frequent in tumors without E-cadherin mutations (5 of 8 tumors, 62.5%) than in gastric carcinoma tissues with E-cadherin mutations (3 of 16 tumors, 18.8%, p = 0.03). Bcl-2 staining was not observed in gastric carcinoma cells without E-cadherin mutations, but was detectable in 5 of 16 tumors with E-cadherin mutations (31.3%), a difference that was not statistically significant (p = 0.13). No relationship was observed between Ki-67 staining and the E-cadherin mutation status (p = 1.00). These data suggest that the presence of E-cadherin mutations can significantly alter the accumulation of the apoptosis-regulating p53 protein, whereas no correlation with the p53 mutation status or with Ki-67 staining was observed.

Published

2002

50. A retrospective comparative exploratory study on two Methylentetrahydrofolate Reductase (MTHFR) polymorphisms in esophagogastric cancer: the A1298C MTHFR polymorphism is an independent prognostic factor only in neoadjuvantly treated gastric cancer patients

Author

Christoph Springfeld, Thomas Bruckner, Florian Lordick, Gisela Keller, Susanne Blank, Rajesh Kumar, Rupert Langer, Sivaramakrishna P. Rachakonda, Katja Ott, Wilko Weichert, and Karen Becker

Subjects

Male, Cancer Research, Pathology, Esophageal Neoplasms, medicine.medical_treatment, Kaplan-Meier Estimate, Gastroenterology, Gene Frequency, Risk Factors, Surgical oncology, Germany, Antineoplastic Combined Chemotherapy Protocols, Medicine, 610 Medicine & health, Neoadjuvant therapy, Esophagogastric adenocarcinoma, biology, Neoadjuvant Therapy, Phenotype, Treatment Outcome, medicine.anatomical_structure, Oncology, Chemotherapy, Adjuvant, Adenocarcinoma, Female, Esophagogastric Junction, Research Article, medicine.medical_specialty, Prognostic factors, Genetic polymorphisms, Gastrectomy, Stomach Neoplasms, Internal medicine, Genetics, Carcinoma, Humans, Genetic Predisposition to Disease, Esophagus, Methylenetetrahydrofolate Reductase (NADPH2), Proportional Hazards Models, Retrospective Studies, Polymorphism, Genetic, business.industry, A1298C, Cancer, Folate metabolism, medicine.disease, digestive system diseases, C677T, Esophagectomy, Methylentetrahydrofolate reductase, Methylenetetrahydrofolate reductase, Multivariate Analysis, biology.protein, 570 Life sciences, business

Abstract

Background Methylentetrahydrofolate reductase (MTHFR) plays a major role in folate metabolism and consequently could be an important factor for the efficacy of a treatment with 5-fluorouracil. Our aim was to evaluate the prognostic and predictive value of two well characterized constitutional MTHFR gene polymorphisms for primarily resected and neoadjuvantly treated esophagogastric adenocarcinomas. Methods 569 patients from two centers were analyzed (gastric cancer: 218, carcinoma of the esophagogastric junction (AEG II, III): 208 and esophagus (AEG I): 143). 369 patients received neoadjuvant chemotherapy followed by surgery, 200 patients were resected without preoperative treatment. The MTHFR C677T and A1298C polymorphisms were determined in DNA from peripheral blood lymphozytes. Associations with prognosis, response and clinicopathological factors were analyzed retrospectively within a prospective database (chi-square, log-rank, cox regression). Results Only the MTHFR A1298C polymorphisms had prognostic relevance in neoadjuvantly treated patients but it was not a predictor for response to neoadjuvant chemotherapy. The AC genotype of the MTHFR A1298C polymorphisms was significantly associated with worse outcome (p = 0.02, HR 1.47 (1.06-2.04). If neoadjuvantly treated patients were analyzed based on their tumor localization, the AC genotype of the MTHFR A1298C polymorphisms was a significant negative prognostic factor in patients with gastric cancer according to UICC 6th edition (gastric cancer including AEG type II, III: HR 2.0, 95% CI 1.3-2.0, p = 0.001) and 7th edition (gastric cancer without AEG II, III: HR 2.8, 95% CI 1.5-5.7, p = 0.003), not for AEG I. For both definitions of gastric cancer the AC genotype was confirmed as an independent negative prognostic factor in cox regression analysis. In primarily resected patients neither the MTHFR A1298C nor the MTHFR C677T polymorphisms had prognostic impact. Conclusions The MTHFR A1298C polymorphisms was an independent prognostic factor in patients with neoadjuvantly treated gastric adenocarcinomas (according to both UICC 6th or 7th definitions for gastric cancer) but not in AEG I nor in primarily resected patients, which confirms the impact of this enzyme on chemotherapy associated outcome.

Published

2014