Your search keyword '"Werner, Jens"' showing total 108 results

1. Surgical Outcome After Distal Pancreatectomy With and Without Portomesenteric Venous Resection in Patients with Pancreatic Adenocarcinoma: A Transatlantic Evaluation of Patients in North America, Germany, Sweden, and The Netherlands (GAPASURG)

Author

Stoop, Thomas F., Augustinus, Simone, Björnsson, Bergthor, Tingstedt, Bobby, Andersson, Bodil, Wolfgang, Christopher L., Werner, Jens, Johansen, Karin, Stommel, Martijn W. J., Katz, Matthew H. G., Ghadimi, Michael, House, Michael G., Ghorbani, Poya, Molenaar, I. Quintus, de Wilde, Roeland F., Mieog, J. Sven D., Keck, Tobias, Wellner, Ulrich F., Uhl, Waldemar, Besselink, Marc G., Pitt, Henry A., and Del Chiaro, Marco

Published

2024

2. Transatlantic differences in the use and outcome of minimally invasive pancreatoduodenectomy: an international multi-registry analysis

Author

de Graaf, Nine, Augustinus, Simone, Wellner, Ulrich F., Johansen, Karin, Andersson, Bodil, Beane, Joal D., Björnsson, Bergthor, Busch, Olivier R., Davis, Catherine H., Ghadimi, Michael, Gleeson, Elizabeth M., Groot Koerkamp, Bas, Hogg, Melissa E., van Santvoort, Hjalmar C., Tingstedt, Bobby, Uhl, Waldemar, Werner, Jens, Williamsson, Caroline, Zeh, Herbert J., Zureikat, Amer H., Abu Hilal, Mohammad, Pitt, Henry A., Besselink, Marc G., and Keck, Tobias

Published

2024

3. REDISCOVER guidelines for borderline-resectable and locally advanced pancreatic cancer: management algorithm, unanswered questions, and future perspectives

Author

Boggi, Ugo, Kauffmann, Emanuele F., Napoli, Niccolò, Barreto, S. George, Besselink, Marc G., Fusai, Giuseppe K., Hackert, Thilo, Hilal, Mohammad Abu, Marchegiani, Giovanni, Salvia, Roberto, Shrikhande, Shailesh V., Truty, Mark, Werner, Jens, Wolfgang, Christopher, Bannone, Elisa, Capretti, Giovanni, Cattelani, Alice, Coppola, Alessandro, Cucchetti, Alessandro, De Sio, Davide, Di Dato, Armando, Di Meo, Giovanna, Fiorillo, Claudio, Gianfaldoni, Cesare, Ginesini, Michael, Hidalgo Salinas, Camila, Lai, Quirino, Miccoli, Mario, Montorsi, Roberto, Pagnanelli, Michele, Poli, Andrea, Ricci, Claudio, Sucameli, Francesco, Tamburrino, Domenico, Viti, Virginia, Cameron, John, Clavien, Pierre-Alain, and Asbun, Horacio J.

Published

2024

4. SPOCK2 gene expression is downregulated in pancreatic ductal adenocarcinoma cells and correlates with prognosis of patients with pancreatic cancer

Author

Aghamaliyev, Ughur, Su, Kaifeng, Weniger, Maximilian, Koch, Dominik, D‘Haese, Jan G., Werner, Jens, and Bazhin, Alexandr V.

Published

2023

5. Serum biomarker panel diagnostics in pancreatic ductal adenocarcinoma: the clinical utility of soluble interleukins, IFN-γ, TNF-α and PD-1/PD-L1 in comparison to established serum tumor markers

Author

Dorman, Klara, Gerckens, Miriam, Kruger, Stephan, Krueger, Kimberly, Mayer, Zsuzsanna, Rupp, Alexander, Zhang, Danmei, Weiss, Lena, Westphalen, C. Benedikt, Haas, Michael, Guenther, Michael, Ormanns, Steffen, Klawonn, Frank, Werner, Jens, von Bergwelt-Baildon, Michael, Heinemann, Volker, Boeck, Stefan, and Holdenrieder, Stefan

Published

2023

6. Prolonged time to treatment initiation in advanced pancreatic cancer patients has no major effect on treatment outcome: a retrospective cohort study controlled for lead time bias and waiting time paradox

Author

Kruger, Stephan, Schirle, Karoline, Haas, Michael, Crispin, Alexander, Schirra, Jörg, Mayerle, Julia, D’Haese, Jan G., Kunz, Wolfgang G., Ricke, Jens, Ormanns, Steffen, Kirchner, Thomas, Kobold, Sebastian, Ilmer, Matthias, Gebauer, Leonie, Westphalen, Christoph B., von Bergwelt-Baildon, Michael, Werner, Jens, Heinemann, Volker, and Boeck, Stefan

Published

2020

7. Succession of transiently active tumor‐initiating cell clones in human pancreatic cancer xenografts

Author

Ball, Claudia R, Oppel, Felix, Ehrenberg, Karl Roland, Dubash, Taronish D, Dieter, Sebastian M, Hoffmann, Christopher M, Abel, Ulrich, Herbst, Friederike, Koch, Moritz, Werner, Jens, Bergmann, Frank, Ishaque, Naveed, Schmidt, Manfred, von Kalle, Christof, Scholl, Claudia, Fröhling, Stefan, Brors, Benedikt, Weichert, Wilko, Weitz, Jürgen, and Glimm, Hanno

Published

2017

8. Acinar cell carcinoma of the pancreas: a rare disease with different diagnostic and therapeutic implications than ductal adenocarcinoma

Author

Kruger, Stephan, Haas, Michael, Burger, Philipp Johannes, Ormanns, Steffen, Modest, Dominik Paul, Westphalen, Christoph Benedikt, Kleespies, Axel, Angele, Martin Kurt, Hartwig, Werner, Bruns, Christiane Josephine, Kirchner, Thomas, Werner, Jens, Heinemann, Volker, and Boeck, Stefan

Published

2016

9. Paraneoplastic Syndromes in Pancreatic Cancer

Author

Werner, Jens, Herzig, Stephan, Neoptolemos, John P., Urrutia, Raul, Abbruzzese, James L., and Büchler, Markus W.

Published

2010

10. Isolation and culture of primary human pancreatic stellate cells that reflect the context of their tissue of origin

Author

Strobel, Oliver, Dadabaeva, Nigora, Felix, Klaus, Hackert, Thilo, Giese, Nathalia A., Jesenofsky, Ralf, and Werner, Jens

Published

2016

11. Clinical Impact of Structured Post-Operative Surveillance in Resected Pancreatic Adenocarcinoma: Results from a Retrospective Cohort Study.

Author

Zhang, Danmei, Kruger, Stephan, Schirle, Karoline, Heinemann, Volker, Dorman, Klara, Westphalen, Christoph Benedikt, Weiss, Lena, Gebauer, Leonie, Günther, Michael, Ormanns, Steffen, Werner, Jens, von Bergwelt-Baildon, Michael, Boeck, Stefan, and Haas, Michael

Subjects

ADENOCARCINOMA, COHORT analysis, PANCREATIC duct, CLINICAL deterioration, PROGRESSION-free survival, PANCREATIC surgery, PANCREATIC intraepithelial neoplasia

Abstract

Introduction: To this date, surgery remains the only potentially curative approach in the treatment of pancreatic cancer. To analyse the clinical impact of a structured post-operative follow-up programme, we retrospectively analysed a cohort of resected pancreatic adenocarcinoma patients treated at LMU Munich. Methods: Pancreatic adenocarcinoma patients who underwent resection and presented for regular follow-up visits at our centre between 2002 and 2017 were identified from two existing study cohorts. Diagnosis of recurrences was categorised by timing (within or outside a scheduled follow-up visit) and detection modality (imaging, CA 19-9 increase, or clinical deterioration) and correlated with disease-free survival and overall survival (OS). Results: One hundred and twenty-five patients with resected pancreatic adenocarcinoma were included in this analysis. Median OS in the whole cohort was 21.1 months. Of these 125 patients, 103 (82.4%) patients had a documented relapse. Tumour recurrences detected within a scheduled follow-up visit (n = 86, 83.5%) compared to recurrences becoming apparent at an unplanned visit (n = 17, 16.5%) were associated with a significantly improved OS (median 25.5 vs. 20.2 months, p = 0.019). Compared to patients with recurrence detected by clinical deterioration (n = 4, 3.9%), patients with recurrences detected by imaging or laboratory abnormalities (n = 99, 96.0%) had a longer median OS (24.8 vs. 15.1 months, p = 0.007). Discussion: A structured follow-up after pancreatic ductal adenocarcinoma resection may have an impact on patient outcome. Prospective trials are needed to evaluate the clinical impact of post-operative follow-up programmes. [ABSTRACT FROM AUTHOR]

Published

2023

12. The impact of adjuvant therapy on outcome in UICC stage I pancreatic cancer.

Author

Guenther, Michael, Boeck, Stefan, Heinemann, Volker, Werner, Jens, Engel, Jutta, and Ormanns, Steffen

Subjects

PANCREATIC cancer, PROPENSITY score matching, PANCREATIC duct, ADJUVANT chemotherapy, PROGRESSION-free survival

Abstract

Adjuvant chemotherapy has become standard of care for pancreatic ductal adenocarcinoma (PDAC) as it improves patient outcome. However, its clinical meaning in early‐stage, UICC I tumors remains uncertain. We examined the effect of adjuvant therapy on disease‐free survival (DFS) and overall survival (OS) of UICC stage I PDAC patients treated at an academic tertiary care center between 2000 and 2016. Among 124 patients (69 male, 55 female; median age 68 years, range 41‐84 years) with UICC stage I disease, adjuvant therapy improved both DFS (19.8 vs 12.8 months, HR 0.59, 95% CI: 0.37‐0.94, P =.03) and OS (40.9 vs 20.3 months, HR 0.54, 95% CI: 0.35‐0.84, P =.005). Multivariate analyses and propensity score matching confirmed the prognostic impact of adjuvant therapy independent of localization, differentiation and R‐status. Thus, every patient with UICC I PDAC should receive adjuvant chemotherapy as it may improve outcome significantly. Our findings support the concept of PDAC as systemic disease from early stages on. [ABSTRACT FROM AUTHOR]

Published

2022

13. Differentiation of multiple types of pancreatico-biliary tumors by molecular analysis of clinical specimens

Author

Gress, Thomas M., Kestler, Hans A., Lausser, Ludwig, Fiedler, Lisa, Sipos, Bence, Michalski, Christoph W., Werner, Jens, Giese, Nathalia, Scarpa, Aldo, and Buchholz, Malte

Published

2012

14. Multimodales interdisziplinäres Therapiekonzept des duktalen Pankreaskarzinoms

Author

Fritz, Stefan, Werner, Jens, and Hartwig, Werner

Published

2008

15. Chirurgische Therapie des Pankreaskarzinoms

Author

Kolb, Armin, Büchler, Markus W., and Werner, Jens

Published

2008

16. Bacterial Lipopolysaccharide as a Negative Predictor of Adjuvant Gemcitabine Efficacy in Pancreatic Cancer.

Author

Guenther, Michael, Gil, Lina, Surendran, Sai Agash, Palm, Melanie Alexandra, Heinemann, Volker, Bergwelt-Baildon, Michael von, Mayerle, Julia, Engel, Jutta, Werner, Jens, Boeck, Stefan, and Ormanns, Steffen

Subjects

LIPOPOLYSACCHARIDES, PANCREATIC cancer

Abstract

Adjuvant gemcitabine (aGC) is one standard of care after pancreatic ductal adenocarcinoma (PDAC) resection. No biomarker for its efficacy is established. As bacteria mediate gemcitabine resistance, we analyzed whether lipopolysaccharide (LPS) as surrogate for bacterial colonization is prognostic in PDAC patients treated with aGC or without aGC adjuvant gemcitabine. We detected LPS in 86 tumors from 376 patients, which defined a specific microbiome as revealed by 16 s-rRNA-sequencing. In the 230 aGC patients, LPS conferred worse disease-free survival (8.3 vs 13.7 months; hazard ratio = 1.75, 95% confidence interval = 1.22 to 2.49; log-rank P  = .002) and overall survival (21.7 vs 28.5 months; hazard ratio = 1.80, 95% confidence interval = 1.23 to 2.57; log-rank P  = .001) but not in the 146 naGC patients, which was confirmed in an independent validation cohort (n = 178). LPS may serve as a negative predictor for aGC efficacy in PDAC, which suggests a role for microbiome modification to overcome bacteria-mediated chemotherapy resistance. [ABSTRACT FROM AUTHOR]

Published

2022

17. Reduced basal and stimulated leukocyte adherence in tumor endothelium of experimental pancreatic cancer

Author

Schmidt, Jan, Ryschich, Eduard, Maksan, Sasa-Marcel, Werner, Jens, Gebhard, Martha Maria, Herfarth, Christian, and Klar, Ernst

Published

1999

18. Improvement of survival after surgical resection of pancreatic cancer independent of adjuvant chemotherapy in the past two decades – A meta-regression.

Author

Weniger, Maximilian, Miksch, Rainer C., Maisonneuve, Patrick, Werner, Jens, and D'Haese, Jan G.

Subjects

SURGICAL excision, ADJUVANT chemotherapy, PANCREATIC cancer, ONCOLOGIC surgery, PANCREATIC surgery, RANDOMIZED controlled trials

Abstract

Surgical resection improves survival in pancreatic ductal adenocarcinoma (PDAC) and adjuvant chemotherapy adds an additional survival-benefit. While surgical technique has improved in recent years, it remains unclear whether these improvements translate into a survival benefit independent of adjuvant chemotherapy. Thus, we aimed to clarify whether survival of patients who were treated with either Gemcitabine (GEM) or who were observed only in randomized controlled trials on adjuvant chemotherapy of PDAC improved over time. A systematic search of MEDLINE/PubMed was performed to identify randomized controlled trials on adjuvant chemotherapy of PDAC. The search was limited to studies with arms on GEM monotherapy or postoperative observation and studies were grouped by the median year of enrolment and the use of GEM. Subsequently, a meta-regression on the effect of the median year of enrolment on patient survival was performed. A total of 13 studies with 2469 patients was included, with median years of enrollment ranging from 1996 to 2015. While disease-free survival decreased in patients with postoperative observation (18.0 vs. 5.0 months, p = 0.001), median survival improved over time in patients with postoperative observation (15.8 vs. 18.4 months, p = 0.01) and in patients treated with adjuvant GEM (22.8 vs. 35.0 months, p < 0.001). One- (p ≤ 0.01) and two-year survival (p = 0.056) improved in both patients treated with adjuvant GEM and those observed only. Survival after surgical resection of PDAC has improved since 1996, even in patients who did not receive adjuvant chemotherapy. Improved surgical technique and postoperative management are likely to be causative factors. • Median survival has improved after survival of PDAC since 1996 • Median survival improved in patients observed only over time • Median survival improved in patients treated with adjuvant gemcitabine over time [ABSTRACT FROM AUTHOR]

Published

2020

19. Epithelial to Stromal Re-Distribution of Primary Cilia during Pancreatic Carcinogenesis

Author

Schimmack, Simon, Kneller, Sarah, Dadabaeva, Nigora, Bergmann, Frank, Taylor, Andrew, Hackert, Thilo, Werner, Jens, and Strobel, Oliver

Subjects

endocrine system diseases, Carcinogenesis, lcsh:Medicine, Endocrine System, Epithelium, Pancreatic Cancer, Exocrine Glands, Cell Signaling, Animal Cells, Pancreatitis, Chronic, Gastrointestinal Tumors, Medicine and Health Sciences, Humans, Hedgehog Proteins, Cilia, lcsh:Science, Pancreas, Cells, Cultured, Connective Tissue Cells, Pancreatic Stellate Cells, lcsh:R, Biology and Life Sciences, Cancers and Neoplasms, Epithelial Cells, Cell Biology, Smoothened Receptor, digestive system diseases, Patched-1 Receptor, Biological Tissue, Oncology, Microscopy, Fluorescence, Connective Tissue, Hedgehog Signaling, Disease Progression, lcsh:Q, Cellular Structures and Organelles, Anatomy, Cellular Types, Stromal Cells, Neoplasm Grading, Research Article, Signal Transduction, Carcinoma, Pancreatic Ductal

Abstract

Background The Hedgehog (HH) pathway is a mediator in pancreatic ductal adenocarcinoma (PDAC). Surprisingly, previous studies suggested that primary cilia (PC), the essential organelles for HH signal transduction, were lost in PDAC. The aim of this study was to determine the presence of PC in human normal pancreas, chronic pancreatitis, and during carcinogenesis to PDAC with focus on both epithelia and stroma. Methods PC were analyzed in paraffin sections from normal pancreas, chronic pancreatitis, intraductal papillary-mucinous neoplasia, and PDAC, as well as in primary human pancreatic stellate cells (PSC) and pancreatic cancer cell lines by double immunofluorescence staining for acetylated α-tubuline and γ-tubuline. Co-staining for the HH receptors PTCH1, PTCH2 and SMO was also performed. Results PC are gradually lost during pancreatic carcinogenesis in the epithelium: the fraction of cells with PC gradually and significantly decreased from 32% in ducts of normal pancreas, to 21% in ducts of chronic pancreatitis, to 18% in PanIN1a, 6% in PanIN2, 3% in PanIN3 and to 1.2% in invasive PDAC. However, this loss of PC in the neoplastic epithelium is accompanied by a gain of PC in the surrounding stroma. The fraction of stromal cells with PC significantly increased from 13% around normal ducts to about 30% around PanIN and PDAC. HH-receptors were detected in tumor stroma but not in epithelial cells. PC are also present in PSC and pancreatic cancer cell lines. Conclusion PC are not lost during pancreatic carcinogenesis but re-distributed from the epithelium to the stroma. This redistribution may explain the re-direction of HH signaling towards the stroma during pancreatic carcinogenesis.

Published

2016

20. TERT gene harbors multiple variants associated with pancreatic cancer susceptibility

Author

Campa, Daniele, Rizzato, Cosmeri, Stolzenberg Solomon, Rachael, Pacetti, Paola, Vodicka, Pavel, Cleary, Sean P, Capurso, Gabriele, Bueno de Mesquita, H. B. As, Werner, Jens, Gazouli, Maria, Butterbach, Katja, Ivanauskas, Audrius, Giese, Nathalia, Petersen, Gloria M, Fogar, Paola, Wang, Zhaoming, Bassi, Claudio, Ryska, Miroslav, Theodoropoulos, George E, Kooperberg, Charles, Donghui, Li, Greenhalf, William, Pasquali, Claudio, Hackert, Thilo, Fuchs, Charles S, Mohelnikova Duchonova, Beatrice, Sperti, Cosimo, Funel, Niccola, Dieffenbach, Aida Karina, Wareham, Nicholas J, Buring, Julie, Holcátová, Ivana, Costello, Eithne, Zambon, Carlo Federico, Kupcinskas, Juozas, Risch, Harvey A, Kraft, Peter, Bracci, Paige M, Pezzilli, Raffaele, Olson, Sara H, Sesso, Howard D, Hartge, Patricia, Strobel, Oliver, Małecka Panas, Ewa, Visvanathan, Kala, Arslan, Alan A, Pedrazzoli, Sergio, Souček, Pavel, Gioffreda, Domenica, Key, Timothy J, Talar Wojnarowska, Renata, Scarpa, Aldo, Mambrini, Andrea, Jacobs, Eric J, Jamroziak, Krzysztof, Klein, Alison, Tavano, Francesca, Bambi, Franco, Landi, Stefano, Austin, Melissa A, Vodickova, Ludmila, Brenner, Hermann, Chanock, Stephen J, Delle Fave, Gianfranco, Piepoli, Ada, Cantore, Maurizio, Zheng, Wei, Wolpin, Brian M, Amundadottir, Laufey T, and Canzian, Federico

Subjects

Adult, Male, Cancer Research, Adolescent, pancreatic cancer, telomerase, Polymorphism, Single Nucleotide, Article, Linkage Disequilibrium, susceptibility, Young Adult, 80 and over, Humans, Genetic Predisposition to Disease, Polymorphism, Aged, Aged, 80 and over, Medicine(all), Carcinoma, Single Nucleotide, Middle Aged, Pancreatic Neoplasms, Oncology, Pancreatic Ductal, Case-Control Studies, Mutation, polymorphisms, Carcinoma, Pancreatic Ductal, Female, Telomerase

Abstract

A small number of common susceptibility loci have been identified for pancreatic cancer, one of which is marked by rs401681 in the TERT-CLPTM1L gene region on chromosome 5p15.33. Because this region is characterized by low linkage disequilibrium, we sought to identify whether additional single nucleotide polymorphisms (SNPs) could be related to pancreatic cancer risk, independently of rs401681. We performed an in-depth analysis of genetic variability of the telomerase reverse transcriptase (TERT) and the telomerase RNA component (TERC) genes, in 5,550 subjects with pancreatic cancer and 7,585 controls from the PANcreatic Disease ReseArch (PANDoRA) and the PanScan consortia. We identified a significant association between a variant in TERT and pancreatic cancer risk (rs2853677, odds ratio=0.85; 95% confidence interval=0.80-0.90, p=8.3 × 10-8). Additional analysis adjusting rs2853677 for rs401681 indicated that the two SNPs are independently associated with pancreatic cancer risk, as suggested by the low linkage disequilibrium between them (r2=0.07, D′=0.28). Three additional SNPs in TERT reached statistical significance after correction for multiple testing: rs2736100 (p=3.0 × 10-5), rs4583925 (p=4.0 × 10-5) and rs2735948 (p=5.0 × 10-5). In conclusion, we confirmed that the TERT locus is associated with pancreatic cancer risk, possibly through several independent variants. What's new? Most pancreatic cancer patients do not survive long after diagnosis, and, so far, there are not many genetic markers to help screen for the disease. In search of genetic predictors of pancreatic cancer, the authors zoomed in on a region linked to susceptibility to the disease. They measured the frequency of different variants of two genes, telomerase reverse transcriptase and telomerase RNA component, among thousands of pancreatic cancer patients and controls. They identified several variants of the TERT gene that indicate a boosted pancreatic cancer risk, and which may develop into useful prognostic tools.

Published

2015

21. MiRNAs are Unlikely to be Involved in Retinoid Receptor Gene Regulation in Pancreatic Cancer Cells.

Author

Yin, Shuai, Bleul, Tim, Zhu, Yifan, Isayev, Orkhan, Werner, Jens, and Bazhin, Alexandr V.

Subjects

RETINOIDS, MICRORNA, PANCREATIC cancer genetics, GENETIC regulation, BIOINFORMATICS

Abstract

Background/Aims: Retinoid receptors and retinoic acid were reported to be down-regulated in pancreatic duct adenocarcinoma (PDAC) compared to normal pancreas. Yet the mechanism of the down-regulation of retinoid receptors is not well defined. The aim of this study was to find out whether selected dysregulated miRNAs in PDAC are responsible for the decreased level of retinoid receptors. Methods: Bioinformatics, real-time PCR, western blot analysis as well as molecular manipulation with miRNA in cells of PDAC were carried out. Results: We first performed bioinformatics research to identify conserved target sequences for deregulated miRNAs within the 3'UTR region of retinoid receptor mRNA. This research revealed binding sites for miR-138, -27a, -27b, -206, -613, -9-5p, -27a/b-3p and -27a. Next, we investigated the expression of selected retinoid receptors and miRNAs in PDAC cell lines and in the Human Pancreatic Duct Epithelial (HPDE) cell line. Further, we investigated the effects of modifying expression levels of selected miRNAs using miRNA inhibitors or mimics. We demonstrated that none of these miRNAs can target the selected retinoid receptors in vitro. Conclusions: miR-27a, miR-27b, miR-9, miR10a and miR-10b were up-regulated in PDAC cells compared to HPDE cells. The up-regulation of these miRNAs was not responsible for the down-regulation of RARa, RARß, RXRa and RXRß in PDAC cells. [ABSTRACT FROM AUTHOR]

Published

2017

22. ITOC2 – 033. Influence of interferon-alpha combined with chemo (radio) therapy on immunological parameters in pancreatic adenocarcinoma

Author

Bazhin V. Alexandr, Werner Jens, and Karakhanova Svetlana

Subjects

Cancer Research, Chemotherapy, business.industry, medicine.medical_treatment, Monocyte, Alpha interferon, Immunotherapy, medicine.disease, In vitro, medicine.anatomical_structure, Oncology, Pancreatic cancer, Immunology, medicine, Carcinoma, Cancer research, Adenocarcinoma, business

Abstract

Prognosis of patients with carcinoma of the exocrine pancreas is particularly poor. A combination of chemotherapy with immunotherapy could be an option for treatment of pancreatic cancer. The aim of this study was to perform an immunomonitoring of the CapRI-2 patients, and tumour-bearing mice treated with combination of chemo (radio) therapies with interferon-2α. Low doses of interferon-2α led to a decrease in total leucocyte and an increase in monocyte counts. Furthermore, we observed a positive effect of interferon-2α therapy on the dendritic cells and NK cell activation immediately after the first injection. In addition, we recorded an increased amount of interferon-γ and interleukin-10 (IL-10) in the serum following the interferon-2α therapy. These data clearly demonstrate that pancreatic carcinoma patients show an immunomodulatory response to interferon-2α therapy. Analysis of immunosuppressive cells in the Panc02 orthotopic mouse model of pancreatic cancer revealed an accumulation of the myeloid-derived suppressor cells in spleens and tumours of the mice treated with interferon-2α and 5-fluorouracil. The direct effect of the drugs on myeloid-derived suppressor cells was also registered in vitro . These data expose the importance of both immunoactivating and immunosuppressive mechanisms induced by combined chemo-immunotherapy.

Published

2015

23. Repurposing Established Compounds to Target Pancreatic Cancer Stem Cells (CSCs).

Author

Renz, Bernhard W., D'Haese, Jan G., Werner, Jens, Westphalen, C. Benedikt, and Ilmer, Matthias

Subjects

PANCREATIC cancer, PANCREATIC cancer treatment, CANCER stem cells, CANCER chemotherapy, ANTINEOPLASTIC agents, PROGNOSIS

Abstract

The diagnosis of pancreatic ductal adenocarcinoma (PDAC) carries a dismal prognosis, in particular, when patients present with unresectable disease. While significant progress has been made in understanding the biology of PDAC, this knowledge has not translated into a clear clinical benefit and current chemotherapeutic strategies only offer a modest improvement in overall survival. Accordingly, novel approaches are desperately needed. One hypothesis that could--at least in part--explain the desolate response of PDAC to chemotherapy is the so-called cancer stem cell (CSC) concept, which attributes specific traits, such as chemoresistance, metastatic potential and a distinct metabolism to a small cellular subpopulation of the whole tumor. At the same time, however, some of these attributes could make CSCs more permissive for novel therapeutic strategies with compounds that are already in clinical use. Most recently, several publications have tried to enlighten the field with the idea of repurposing established drugs for antineoplastic use. As such, recycling drugs could present an intriguing and fast-track method with new therapeutic paradigms in anti-cancer and anti-CSC treatments. Here, we aim to summarize important aspects and novel findings of this emerging field. [ABSTRACT FROM AUTHOR]

Published

2017

24. Switch in KRAS mutational status during an unusual course of disease in a patient with advanced pancreatic adenocarcinoma: implications for translational research.

Author

Baechmann, Sibylle, Ormanns, Steffen, Haas, Michael, Kruger, Stephan, Remold, Anna, Modest, Dominik Paul, Kirchner, Thomas, Jung, Andreas, Werner, Jens, Heinemann, Volker, and Boeck, Stefan

Subjects

PANCREATIC cancer, ADENOCARCINOMA, GENETIC mutation, TRANSLATIONAL research, ANTINEOPLASTIC agents, DRUG efficacy, FLUOROURACIL, CANCER relapse, MEDICAL research, PANCREATIC tumors, PROTEINS, PANCREATICODUODENECTOMY, DUCTAL carcinoma, DEOXYCYTIDINE, THERAPEUTICS, TUMOR treatment, CANCER treatment

Abstract

Background: Despite the introduction of novel effective treatment regimens like gemcitabine plus nab-paclitaxel and FOLFIRINOX, pancreatic ductal adenocarcinoma (PDAC) remains one of the most aggressive epithelial tumors. Among the genetic alterations frequently found in PDAC, mutations in the KRAS gene might play a prognostic role regarding overall survival and may also have the potential to predict the efficacy of anti-EGFR treatment.Case Presentation: We report the clinical case of a 69 year old Caucasian female that was diagnosed with histologically confirmed locally advanced PDAC with lymph node involvement in August 2010. At the time of first diagnosis, tumor tissue obtained from an open regional lymph node biopsy showed a poorly differentiated adenocarcinoma with a wild type sequence within exon 2 (codon 12/13) of the KRAS gene. The patient initially received single-agent gemcitabine and a subsequent 5-FU-based chemoradiotherapy with a sequential maintenance chemotherapy with oral capecitabine resulting in a long term disease control. Local disease progression occurred in May 2014 and the patient underwent pancreaticoduodenectomy in September 2014. A novel KRAS gene mutation (c.35G > T, p.G12 V) in exon 2 (codon 12) was detected within the surgical specimen. As of January 2016 the patient is still alive and without evidence of the underlying disease.Conclusions: Specifically in the context of clinical trials and translational research in PDAC a re-assessment of molecular biomarkers, i. e. KRAS, at defined time points (e. g. relapse, disease progression, unusual clinical course) may be indicated in order to detect a potential switch in biomarker status during the course of disease. [ABSTRACT FROM AUTHOR]

Published

2017

25. Synthesis and functionalization of protease-activated nanoparticles with tissue plasminogen activator peptides as targeting moiety and diagnostic tool for pancreatic cancer.

Author

Dobiasch, Sophie, Szanyi, Szilard, Kjaev, Aleko, Werner, Jens, Strauss, Albert, Weis, Christian, Grenacher, Lars, Kapilov-Buchman, Katya, Israel, Liron-Limor, Lellouche, Jean-Paul, Locatelli, Erica, Comes Franchini, Mauro, Vandooren, Jennifer, Opdenakker, Ghislain, and Felix, Klaus

Subjects

PROTEOLYTIC enzymes, NANOPARTICLES, TISSUE plasminogen activator, PEPTIDES, FUNCTIONAL groups, PANCREATIC cancer treatment, MOLECULAR biology, NANOTECHNOLOGY

Abstract

Background: Functionalized nanoparticles (NPs) are one promising tool for detecting specific molecular targets and combine molecular biology and nanotechnology aiming at modern imaging. We aimed at ligand-directed delivery with a suitable target-biomarker to detect early pancreatic ductal adenocarcinoma (PDAC). Promising targets are galectins (Gal), due to their strong expression in and on PDAC-cells and occurrence at early stages in cancer precursor lesions, but not in adjacent normal tissues. Results: Molecular probes (10-29 AA long peptides) derived from human tissue plasminogen activator (t-PA) were selected as binding partners to galectins. Affinity constants between the synthesized t-PA peptides and Gal were determined by microscale thermophoresis. The 29 AA-long t-PA-peptide-1 with a lactose-functionalized serine revealed the strongest binding properties to Gal-1 which was 25-fold higher in comparison with the native t-PA protein and showed additional strong binding to Gal-3 and Gal-4, both also over-expressed in PDAC. t-PA-peptide-1 was selected as vector moiety and linked covalently onto the surface of biodegradable iron oxide nanoparticles (NPs). In particular, CAN-doped maghemite NPs (CAN-Mag), promising as contrast agent for magnetic resonance imaging (MRI), were selected as magnetic core and coated with different biocompatible polymers, such as chitosan (CANMag- Chitosan NPs) or polylactic co glycolic acid (PLGA) obtaining polymeric nanoparticles (CAN-Mag@PNPs), already approved for drug delivery applications. The binding efficacy of t-PA-vectorized NPs determined by exposure to different pancreatic cell lines was up to 90%, as assessed by flow cytometry. The in vivo targeting and imaging efficacy of the vectorized NPs were evaluated by applying murine pancreatic tumor models and assessed by 1.5 T magnetic resonance imaging (MRI). The t-PA-vectorized NPs as well as the protease-activated NPs with outer shell decoration (CAN-Mag@PNPs-PEG-REGAcp-PEG/tPA-pep1Lac) showed clearly detectable drop of subcutaneous and orthotopic tumor staining-intensity indicating a considerable uptake of the injected NPs. Post mortem NP deposition in tumors and organs was confirmed by Fe staining of histopathology tissue sections. Conclusions: The targeted NPs indicate a fast and enhanced deposition of NPs in the murine tumor models. The CAN-Mag@PNPs-PEG-REGAcp-PEG/tPA-pep1Lac interlocking steps strategy of NPs delivery and deposition in pancreatic tumor is promising. [ABSTRACT FROM AUTHOR]

Published

2016

26. The potential diagnostic value of serum microRNA signature in patients with pancreatic cancer.

Author

Johansen, Julia S., Calatayud, Dan, Albieri, Vanna, Schultz, Nicolai A., Dehlendorff, Christian, Werner, Jens, Jensen, Benny V., Pfeiffer, Per, Bojesen, Stig E., Giese, Nathalia, Nielsen, Kaspar R., Nielsen, Svend E., Yilmaz, Mette, Holländer, Niels H., and Andersen, Klaus K.

Abstract

Biomarkers for early diagnosis of patients with pancreatic cancer (PC) are needed. Our aim was to identify panels of miRNAs in serum in combination with CA 19-9 for use in the diagnosis of PC. Four hundred seventeen patients with PC were included prospectively from Denmark ( n = 306) and Germany ( n = 111). Controls included 59 patients with chronic pancreatitis (CP) and 248 healthy subjects (HS). MiRNAs were analyzed in pretreatment serum samples from 3 cohorts: discovery cohort (754 human miRNAs, TaqMan® Human MicroRNA assay, Applied Biosystem; PC n = 133, controls n = 72); training cohort (34 miRNAs, real-time qPCR using the Fluidigm BioMark™ System; PC n = 198, controls n = 184); validation cohort (13 miRNAs, real-time qPCR using the Fluidigm BioMark™ System; PC n = 86, controls n = 51). We found that 34 miRNAs in serum from PC patients in the discovery cohort were expressed differently than in controls. These miRNAs were tested in the training cohort, and four diagnostic panels were constructed that included 5 or 12 miRNAs (miR-16, −18a, −20a, −24, −25, −27a, −29c, −30a.5p, −191, −323.3p, −345 and −483.5p). Diagnostic accuracy of detecting PC in the training cohort was AUC (Index I 0.85; II 0.87; III 0.85; IV 0.95; CA 19-9 0.93); specificity (I 0.71; II 0.76; III 0.66; IV 0.90 (fixed sensitivity at 0.85); CA 19-9 0.93). Combining serum CA 19-9 and Index II best discriminated Stages I and II PC from HS [AUC 0.93 (0.90-0.96), sensitivity 0.77 (0.69-0.84), specificity 0.94 (0.90-0.96) and accuracy 0.88 (0.84-0.91)]. In conclusion, we identified four diagnostic panels based on 5 or 12 miRNAs in serum that could distinguish patients with PC from HS and CP. [ABSTRACT FROM AUTHOR]

Published

2016

27. Isolated pulmonary metastases define a favorable subgroup in metastatic pancreatic cancer.

Author

Kruger, Stephan, Haas, Michael, Burger, Philipp Johannes, Ormanns, Steffen, Modest, Dominik Paul, Westphalen, Christoph Benedikt, Michl, Marlies, Kleespies, Axel, Angele, Martin Kurt, Hartwig, Werner, Bruns, Christiane Josephine, Niyazi, Maximilian, Roeder, Falk, Kirchner, Thomas, Werner, Jens, Heinemann, Volker, and Boeck, Stefan

Abstract

Purpose Liver metastasis represents the first site of dissemination in >80% of metastatic pancreatic cancer (PC) patients. Pulmonary metastasis as first site of dissemination in PC is a rare event and might define a biologically distinct subgroup in metastatic PC. Methods Consecutive PC patients who were diagnosed or treated with isolated pulmonary metastases at our high-volume comprehensive cancer center were included in a prospectively maintained database between 2002 and 2015. Medical records and correlating computed tomography findings (CT) were retrospectively analyzed. Results A total of 40 PC patients with isolated pulmonary metastases were identified. Pulmonary metastases represented disease recurrence after initial resection of PC in 22 patients and disease progression of locally advanced pancreatic cancer in 5 patients. 14 out of 27 PC patients (56%) had received chemoradiotherapy for localized disease prior to pulmonary metastasis. Data on 1st-line treatment for pulmonary metastases was available for 38 patients: most patients (71%) received a gemcitabine-based chemotherapy regimen, 5 patients (13%) received best supportive care. After a median follow-up of 37.3 months, median survival after diagnosis of pulmonary metastasis was estimated with 25.5 months (95% CI 19.1–31.8); a significantly improved survival after diagnosis of pulmonary metastasis was observed for patients with less than 10 lung metastases (31.3 vs 18.7 months, p = 0.003) and for an unilateral localization of lung involvement (31.3 vs 21.8 months, p = 0.03). Conclusions Our results suggest a favorable outcome of PC patients with isolated pulmonary metastases. Further research is warranted to elucidate the specific molecular characteristics of this rare subgroup. [ABSTRACT FROM AUTHOR]

Published

2016

28. Pancreaticoduodenectomy for adenocarcinoma of the pancreatic head is justified in elderly patients: A Retrospective Cohort Study.

Author

Renz, Bernhard W., Khalil, Philippe N., Mikhailov, Michael, Graf, Sandra, Schiergens, Tobias S., Niess, Hanno, Boeck, Stefan, Heinemann, Volker, Hartwig, Werner, Werner, Jens, Bruns, Christiane J., and Kleespies, Axel

Subjects

ADENOCARCINOMA, AGE distribution, PANCREATIC tumors, SURGICAL complications, PANCREATICODUODENECTOMY, TREATMENT effectiveness, RETROSPECTIVE studies, SURGICAL anastomosis

Abstract

Background: The increasing elderly population is an inevitable trend worldwide in developed countries. Therefore, we aimed to assess the experience of a tertiary pancreatic center with a very homogenous population comprising only patients diagnosed with PDAC of the pancreatic head in patients older than 75 years of age compared to their younger counterparts regarding the benefit in life expectancy and tumor biological aggressiveness.Methods: 300 patients underwent partial pancreaticoduodenectomy (PD) or pylorus preserving pancreaticoduodenectomy (PPPD) for PDAC of the pancreatic head between 2002 and 2012 and were evaluated with regard to their co-morbidities, clinicopathological and perioperative variables, postoperative morbidity, mortality and long term survival. Therefore, two groups according to the age at the procedure (A: <75 years, n = 241, B: ≥75 years, n = 59) were designed.Results: There were no differences between groups with regard to gender, performed procedure (PPPD or PD), operation time, blood loss, tumor invasiveness and grade of tumor differentiation, R-status, lymph node ratio, 30-day mortality, length of stay and adjuvant chemotherapy. Extended resections including total pancreatectomy were slightly more often performed in younger patients (p = 0.071) and trended toward a higher rate of surgical complications in patients <75 years of age (p = 0.183). A higher rate of preoperative co-morbidities in elderly patients (group B), was associated with more postoperative non-surgical complications (p = 0.002) in this group of patients. However, the median overall survival (19.2 vs. 18.4 months) did not differ significantly between groups.Conclusions: Major pancreatic surgery for ductal adenocarcinoma of the pancreatic head is justified in elderly patients. With careful patients' selection and prudent perioperative management, elderly patients will have a similar long term outcome despite the higher rate of postoperative morbidity based on non-surgical complications. [ABSTRACT FROM AUTHOR]

Published

2016

29. Transcriptional co-factor Transducin beta-like ( TBL) 1 acts as a checkpoint in pancreatic cancer malignancy.

Author

Stoy, Christian, Sundaram, Aishwarya, Rios Garcia, Marcos, Wang, Xiaoyue, Seibert, Oksana, Zota, Annika, Wendler, Susann, Männle, David, Hinz, Ulf, Sticht, Carsten, Muciek, Maria, Gretz, Norbert, Rose, Adam J, Greiner, Vera, Hofmann, Thomas G., Bauer, Andrea, Hoheisel, Jörg, Berriel Diaz, Mauricio, Gaida, Matthias M, and Werner, Jens

Abstract

Pancreatic ductal adenocarcinoma ( PDAC) is the fourth leading cause of cancer fatalities in Western societies, characterized by high metastatic potential and resistance to chemotherapy. Critical molecular mechanisms of these phenotypical features still remain unknown, thus hampering the development of effective prognostic and therapeutic measures in PDAC. Here, we show that transcriptional co-factor Transducin beta-like ( TBL) 1 was over-expressed in both human and murine PDAC. Inactivation of TBL1 in human and mouse pancreatic cancer cells reduced cellular proliferation and invasiveness, correlating with diminished glucose uptake, glycolytic flux, and oncogenic PI3 kinase signaling which in turn could rescue TBL1 deficiency-dependent phenotypes. TBL1 deficiency both prevented and reversed pancreatic tumor growth, mediated transcriptional PI3 kinase inhibition, and increased chemosensitivity of PDAC cells in vivo. As TBL1 mRNA levels were also found to correlate with PI3 kinase levels and overall survival in a cohort of human PDAC patients, TBL1 was identified as a checkpoint in the malignant behavior of pancreatic cancer and its expression may serve as a novel molecular target in the treatment of human PDAC. [ABSTRACT FROM AUTHOR]

Published

2015

30. Pancreatic Adenocarcinoma.

Author

Strobel, Oliver, Hinz, Ulf, Gluth, Alexander, Hank, Thomas, Hackert, Thilo, Bergmann, Frank, Werner, Jens, and Büchler, Markus W.

Published

2015

31. Adjuvant radiotherapy and chemoradiation with gemcitabine after R1 resection in patients with pancreatic adenocarcinoma.

Author

Habermehl, Daniel, Brecht, Ingo C., Bergmann, Frank, Rieken, Stefan, Werner, Jens, Büchler, Markus W., Springfeld, Christoph, Jäger, Dirk, Debus, Jürgen, and Combs, Stephanie E.

Subjects

RADIOTHERAPY, IMMUNOLOGICAL adjuvants, IMMUNOMODULATORS, ADENOCARCINOMA, CANCER treatment, PANCREATIC cancer treatment, PANCREATIC diseases, PHYSIOLOGY, THERAPEUTICS

Abstract

Background: The purpose of the study was to evaluate the effect of radiation therapy and chemoradiation with gemcitabine (GEM) after R1 resection in patients with pancreatic adenocarcinoma (PAC). Methods: We performed a retrospective analysis of 25 patients who were treated with postoperative radiotherapy (RT) or chemoradiation (CRT) after surgery with microscopically positive resection margins for primary pancreatic cancer (PAC). Median age was 60 years (range 34 to 74 years), and there were 17 male and 8 female patients. Fractionated RT was applied with a median dose of 49.6 Gy (range 36 to 54 Gy). Eight patients received additional intraoperative radiotherapy (IORT) with a median dose of 12 Gy. Results: Median overall survival (mOS) of all treated patients was 22 months (95% confidence interval (CI) 7.9 to 36.1 months) after date of resection and 21.1 months (95% CI 7.6 to 34.6 months) after start of (C)RT. Median progression-free survival (mPFS) was 13.0 months (95% CI 0.93 to 25 months). Grading (G2 vs. G3, P = 0.005) and gender (female vs. male, P = 0.01) were significantly correlated with OS. There was a significant difference in mPFS between male and female patients (P = 0.008). A total of 11 from 25 patients experienced local tumour progression, and 19 patients were diagnosed with either locoregional or distant failure. Conclusions: We demonstrated that GEM-based CRT can be applied in analogy to neoadjuvant protocols in the adjuvant setting for PAC patients at high risk for disease recurrence after incomplete resection. Patients undergoing additive CRT have a rather good OS and PFS compared to historical control patient groups. [ABSTRACT FROM AUTHOR]

Published

2015

32. Chondroitin Sulfate Proteoglycan CSPG4 as a Novel Hypoxia-Sensitive Marker in Pancreatic Tumors.

Author

Keleg, Shereen, Titov, Alexandr, Heller, Anette, Giese, Thomas, Tjaden, Christine, Ahmad, Sufian S., Gaida, Matthias M., Bauer, Andrea S., Werner, Jens, and Giese, Nathalia A.

Subjects

CHONDROITIN sulfate proteoglycan, HYPOXEMIA, BIOMARKERS, PANCREATIC tumors, GENE expression, CYSTADENOMA

Abstract

CSPG4 marks pericytes, undifferentiated precursors and tumor cells. We assessed whether the shed ectodomain of CSPG4 (sCSPG4) might circulate and reflect potential changes in CSPG4 tissue expression (pCSPG4) due to desmoplastic and malignant aberrations occurring in pancreatic tumors. Serum sCSPG4 was measured using ELISA in test (n = 83) and validation (n = 221) cohorts comprising donors (n = 11+26) and patients with chronic pancreatitis (n = 11+20) or neoplasms: benign (serous cystadenoma SCA, n = 13+20), premalignant (intraductal dysplastic IPMNs, n = 9+55), and malignant (IPMN-associated invasive carcinomas, n = 4+14; ductal adenocarcinomas, n = 35+86). Pancreatic pCSPG4 expression was evaluated using qRT-PCR (n = 139), western blot analysis and immunohistochemistry. sCSPG4 was found in circulation, but its level was significantly lower in pancreatic patients than in donors. Selective maintenance was observed in advanced IPMNs and PDACs and showed a nodal association while lacking prognostic relevance. Pancreatic pCSPG4 expression was preserved or elevated, whereby neoplastic cells lacked pCSPG4 or tended to overexpress without shedding. Extreme pancreatic overexpression, membranous exposure and tissuehigh/seralow-discordance highlighted stroma-poor benign cystic neoplasm. SCA is known to display hypoxic markers and coincide with von-Hippel-Lindau and Peutz-Jeghers syndromes, in which pVHL and LBK1 mutations affect hypoxic signaling pathways. In vitro testing confined pCSPG4 overexpression to normal mesenchymal but not epithelial cells, and a third of tested carcinoma cell lines; however, only the latter showed pCSPG4-responsiveness to chronic hypoxia. siRNA-based knockdowns failed to reduce the malignant potential of either normoxic or hypoxic cells. Thus, overexpression of the newly established conditional hypoxic indicator, CSPG4, is apparently non-pathogenic in pancreatic malignancies but might mark distinct epithelial lineage and contribute to cell polarity disorders. Surficial retention on tumor cells renders CSPG4 an attractive therapeutic target. Systemic ‘drop and restoration’ alterations accompanying IPMN and PDAC progression indicate that the interference of pancreatic diseases with local and remote shedding/release of sCSPG4 into circulation deserves broad diagnostic exploration. [ABSTRACT FROM AUTHOR]

Published

2014

33. Triptolide reverses hypoxia-induced epithelial-mesenchymal transition and stem-like features in pancreatic cancer by NF-κB downregulation.

Author

Liu, Li, Salnikov, Alexei V., Bauer, Nathalie, Aleksandrowicz, Ewa, Labsch, Sabrina, Nwaeburu, Clifford, Mattern, Jürgen, Gladkich, Jury, Schemmer, Peter, Werner, Jens, and Herr, Ingrid

Abstract

Pancreatic ductal adenocarcinoma (PDA) is one of the most lethal malignancies characterized by an intense tumor stroma with hypoperfused regions, a significant inflammatory response and pronounced therapy resistance. New therapeutic agents are urgently needed. The plant-derived agent triptolide also known as 'thunder god vine' has a long history in traditional Chinese medicine for treatment of rheumatoid arthritis and cancer and is now in a clinical phase II trial for establishing the efficacy against a placebo. The authors mimicked the situation in patient tumors by induction of hypoxia in experimental models of pancreatic cancer stem cells (CSCs) and evaluated the therapeutic effect of triptolide. Hypoxia led to induction of colony and spheroid formation, aldehyde dehydrogenase 1 (ALDH1) and NF-κB activity, migratory potential and a switch in morphology to a fibroblastoid phenotype, as well as stem cell- and epithelial-mesenchymal transition-associated protein expression. Triptolide efficiently inhibited hypoxia-induced transcriptional signaling and downregulated epithelial-mesenchymal transition (EMT) and CSC features in established highly malignant cell lines, whereas sensitive cancer cells or nonmalignant cells were less affected. In vivo triptolide inhibited tumor take and tumor growth. In primary CSCs isolated from patient tumors, triptolide downregulated markers of CSCs, proliferation and mesenchymal cells along with upregulation of markers for apoptosis and epithelial cells. This study is the first to show that triptolide reverses EMT and CSC characteristics and therefore may be superior to current chemotherapeutics for treatment of PDA. [ABSTRACT FROM AUTHOR]

Published

2014

34. Phase I study evaluating the treatment of patients with locally advanced pancreatic cancer with carbon ion radiotherapy: the PHOENIX-01 trial.

Author

Combs, Stephanie E., Habermehl, Daniel, Kieser, Meinhard, Dreher, Constantin, Werner, Jens, Haselmann, Renate, Jäkel, Oliver, Jäger, Dirk, Büchler, Markus W., and Debus, Jürgen

Subjects

PANCREATIC cancer, RADIOTHERAPY, ELECTRONS, CELLULAR pathology, RELATIVE biological effectiveness (Radiobiology), THERAPEUTIC use of antimetabolites, ANTIMETABOLITES, ANTINEOPLASTIC agents, CLINICAL trials, COMPARATIVE studies, RESEARCH methodology, MEDICAL cooperation, MEDICAL protocols, PANCREATIC tumors, RADIATION doses, RESEARCH, TUMOR classification, EVALUATION research, TREATMENT effectiveness, DEOXYCYTIDINE, THERAPEUTICS

Abstract

Background: Treatment options for patients with locally advanced pancreatic cancer include surgery, chemotherapy as well as radiotherapy. In many cases, surgical resection is not possible, and therefore treatment alternatives have to be performed. Chemoradiation has been established as a convincing treatment alternative for locally advanced pancreatic cancer. Carbon ions offer physical and biological characteristics. Due to their inverted dose profile and the high local dose deposition within the Bragg peak precise dose application and sparing of normal tissue is possible. Moreover, in comparison to photons, carbon ions offer an increased relative biological effectiveness (RBE), which can be calculated between 1.16 and 2.46 depending on the pancreatic cancer cell line as well as the endpoint analyzed. Japanese Data on the evaluation of carbon ion radiation therapy showed promising results for patients with pancreatic cancer.Methods and Design: The present PHOENIX-01 trial evaluates carbon ion radiotherapy using the active rasterscanning technique in patients with advanced pancreatic cancer in combination with weekly gemcitabine and adjuvant gemcitabine. Primary endpoint is toxicity, secondary endpoints are overall survival, progression-free survival and response.Discussion: The physical and biological properties of the carbon ion beam promise to improve the therapeutic ratio in patients with pancreatic cancer: Due to the inverted dose profile dose deposition in the entry channel of the beam leads to sparing of normal tissue; the Bragg peak can be directed into the defined target volume, and the sharp dose fall-off thereafter again spares normal tissue behind the target volume. The higher RBE of carbon ions, which has been shown also for pancreatic cancer cell lines in the preclinical setting, is likely to contribute to an increase in local control, and perhaps in OS. Early data from Japanese centers have shown promising results. In conclusion, this is the first trial to evaluate actively delivered carbon ion beams in patients with locally advanced pancreatic cancer within a dose-escalation strategy.Trial Registration: NCT01795274. [ABSTRACT FROM AUTHOR]

Published

2013

35. Diagnostic and Prognostic Impact of Circulating YKL-40, IL-6, and CA 19.9 in Patients with Pancreatic Cancer.

Author

Schultz, Nicolai A., Christensen, Ib J., Werner, Jens, Giese, Nathalia, Jensen, Benny V., Larsen, Ole, Bjerregaard, Jon K., Pfeiffer, Per, Calatayud, Dan, Nielsen, Svend E., Yilmaz, Mette K., Holländer, Niels H., Wøjdemann, Morten, Bojesen, Stig E., Nielsen, Kaspar R., and Johansen, Julia S.

Subjects

CARTILAGE cells, GLYCOPROTEINS, INTERLEUKIN-6, CARBOHYDRATES, PANCREATIC cancer diagnosis, CANCER patients, PANCREATIC cancer, BIOMARKERS, CHEMILUMINESCENCE assay, PROGNOSIS

Abstract

Purpose: We tested the hypothesis that high plasma YKL-40 and IL-6 associate with pancreatic cancer and short overall survival. Patients and Methods: In all, 559 patients with pancreatic cancer from prospective biomarker studies from Denmark (n = 448) and Germany (n = 111) were studied. Plasma YKL-40 and IL-6 were determined by ELISAs and serum CA 19.9 by chemiluminescent immunometric assay. Results: Odds ratios (ORs) for prediction of pancreatic cancer were significant for all biomarkers, with CA 19.9 having the highest AUC (CA 19.9: OR = 2.28, 95% CI 1.97 to 2.68, p<0.0001, AUC = 0.94; YKL-40: OR = 4.50, 3.99 to 5.08, p<0.0001, AUC = 0.87; IL-6: OR = 3.68, 3.08 to 4.44, p<0.0001, AUC = 0.87). Multivariate Cox analysis (YKL-40, IL-6, CA 19.9, age, stage, gender) in patients operated on showed that high preoperative IL-6 and CA 19.9 (dichotomized according to normal values) were independently associated with short overall survival (CA 19.9: HR = 2.51, 1.22–5.15, p = 0.013; IL-6: HR = 2.03, 1.11 to 3.70, p = 0.021). Multivariate Cox analysis of non-operable patients (Stage IIB-IV) showed that high pre-treatment levels of each biomarker were independently associated with short overall survival (YKL-40: HR = 1.30, 1.03 to 1.64, p = 0.029; IL-6: HR = 1.71, 1.33 to 2.20, p<0.0001; CA 19.9: HR = 1.54, 1.06 to 2.24, p = 0.022). Patients with preoperative elevation of both IL-6 and CA 19.9 had shorter overall survival (p<0.005) compared to patients with normal levels of both biomarkers (45% vs. 92% alive after 12 months). Conclusions: Plasma YKL-40 and IL-6 had less diagnostic impact than CA 19.9. Combination of pretreatment YKL-40, IL-6, and CA 19.9 may have clinical value to identify pancreatic cancer patients with the poorest prognosis. [ABSTRACT FROM AUTHOR]

Published

2013

36. Somatic Mutations in Exocrine Pancreatic Tumors: Association with Patient Survival.

Author

Rachakonda, P. Sivaramakrishna, Bauer, Andrea S., Xie, Huaping, Campa, Daniele, Rizzato, Cosmeri, Canzian, Federico, Beghelli, Stefania, Greenhalf, William, Costello, Eithne, Schanne, Michaela, Heller, Anette, Scarpa, Aldo, Neoptolemos, John P., Werner, Jens, Büchler, Markus, Hoheisel, Jörg D., Hemminki, Kari, Giese, Nathalia, and Kumar, Rajiv

Subjects

SOMATIC mutation, EXOCRINE pancreatic insufficiency, ADENOCARCINOMA, GASTROINTESTINAL cancer, PUBLIC health research, EPIDEMIOLOGICAL research, GENETIC mutation

Abstract

KRAS mutations are major factors involved in initiation and maintenance of pancreatic tumors. The impact of different mutations on patient survival has not been clearly defined. We screened tumors from 171 pancreatic cancer patients for mutations in KRAS and CDKN2A genes. Mutations in KRAS were detected in 134 tumors, with 131 in codon 12 and only 3 in codon 61. The GGT>GAT (G12D) was the most frequent mutation and was present in 60% (80/134). Deletions and mutations in CDKN2A were detected in 43 tumors. Analysis showed that KRAS mutations were associated with reduced patient survival in both malignant exocrine and ductal adenocarcinomas (PDAC). Patients with PDACs that had KRAS mutations showed a median survival of 17 months compared to 30 months for those without mutations (log-rank P = 0.07) with a multivariate hazard ratio (HR) of 2.19 (95%CI 1.09–4.42). The patients with G12D mutation showed a median survival of 16 months (log-rank-test P = 0.03) and an associated multivariate HR 2.42 (95%CI 1.14–2.67). Although, the association of survival in PDAC patients with CDKN2A aberrations in tumors was not statistically significant, the sub-group of patients with concomitant KRAS mutations and CDKN2A alterations in tumors were associated with a median survival of 13.5 months compared to 22 months without mutation (log-rank-test P = 0.02) and a corresponding HR of 3.07 (95%CI 1.33–7.10). Our results are indicative of an association between mutational status and survival in PDAC patients, which if confirmed in subsequent studies can have potential clinical application. [ABSTRACT FROM AUTHOR]

Published

2013

37. Chemoradiation in patients with isolated recurrent pancreatic cancer - therapeutical efficacy and probability of re-resection.

Author

Habermehl, Daniel, Brecht, Ingo C., Bergmann, Frank, Welzel, Thomas, Rieken, Stefan, Werner, Jens, Schirmacher, Peter, Büchler, Markus W., Debus, Jürgen, and Combs, Stephanie E.

Subjects

PANCREATIC cancer, CANCER relapse, SURGICAL excision, ABDOMINAL surgery, TOXICITY testing, BIOPSY

Abstract

Background: In the present retrospective analysis we analysed the therapeutic outcome of a set of patients, who were treated with chemoradiation (CRT) for recurrent pancreatic cancer (RPC) in a single institution. Patients and Methods: Forty-one patients had a history of primary resection for pancreatic cancer. In case of an unresectable recurrency patients were treated with CRT at our institution between 2002 and 2010 with a median dose of 48.4 Gy (range 39.6-54 Gy). Concurrent chemotherapy regimes included Gemcitabine (GEM) in 37/41 patients (90%) and Fluorouracil (FU) or Capecitabine (CAP) in 4/41 patients (10%). Patients were re-evaluated after CRT with computed tomography and/or explorative laparotomy. During re-resection or laparotomy 15 patients received an additional intraoperative radiotherapy (IORT) with a median dose of 15 Gy (range 12-15 Gy). Median age was 65 years (range 39-76 years) and there were 26 male and 15 female patients. Results: The median overall survival (mOS), local control (LC) and progression-free survival (PFS) were 16.1, 13.8 and 6.9 months respectively for all patients after the first day of CRT. Re-resection was possible in five patients (12%) and a complete remission (CR) as defined by tumor-free biopsy was seen in 6 patients (15%). When re-resection could be achieved after CRT mOS was improved to 28.3 months (n = 5 patients, 95%-CI 10.2 - 46.3 months). Patients receiving IORT had a significantly improved mOS compared to no IORT (p = 0.034). Fifteen patients (37%) experienced a local tumour progression and main site of distant metastasis was the liver (11 patients, 27%).Overall treatment-related toxicity was mild, grade III hematologic toxicity was observed in 11 patients (27%). Conclusion: In summary we observed a good therapeutic response with mild to moderate toxicity levels for CRT in RPC. Overall survival and PFS were clearly improved in case of induction of a complete remission (tumor-free biopsies) or after achieving a re-resection, thus providing a curative intended therapy even in case of disease recurrence. [ABSTRACT FROM AUTHOR]

Published

2013

38. Diagnosis of Pancreatic Ductal Adenocarcinoma and Chronic Pancreatitis by Measurement of microRNA Abundance in Blood and Tissue.

Author

Bauer, Andrea S., Keller, Andreas, Costello, Eithne, Greenhalf, William, Bier, Melanie, Borries, Anne, Beier, Markus, Neoptolemos, John, Büchler, Markus, Werner, Jens, Giese, Nathalia, and Hoheisel, Jörg D.

Subjects

PANCREATIC cancer, CANCER patients, PANCREATITIS, CANCER treatment, TISSUES, ENDOCRINE glands, BLOOD testing

Abstract

A solid process for diagnosis could have a substantial impact on the successful treatment of pancreatic cancer, for which currently mortality is nearly identical to incidence. Variations in the abundance of all microRNA molecules from peripheral blood cells and pancreas tissues were analyzed on microarrays and in part validated by real-time PCR assays. In total, 245 samples from two clinical centers were studied that were obtained from patients with pancreatic ductal adenocarcinoma or chronic pancreatitis and from healthy donors. Utilizing the minimally invasive blood test, receiver operating characteristic (ROC) curves and the corresponding area under the curve (AUC) analysis demonstrated very high sensitivity and specificity of a distinction between healthy people and patients with either cancer or chronic pancreatitis; respective AUC values of 0.973 and 0.950 were obtained. Confirmative and partly even more discriminative diagnosis could be performed on tissue samples with AUC values of 1.0 and 0.937, respectively. In addition, discrimination between cancer and chronic pancreatitis was achieved (AUC = 0.875). Also, several miRNAs were identified that exhibited abundance variations in both tissue and blood samples. The results could have an immediate diagnostic value for the evaluation of tumor reoccurrence in patients, who have undergone curative surgical resection, and for people with a familial risk of pancreatic cancer. [ABSTRACT FROM AUTHOR]

Published

2012

39. Aggressive local treatment containing intraoperative radiation therapy (IORT) for patients with isolated local recurrences of pancreatic cancer: a retrospective analysis.

Author

Roeder, Falk, Timke, Carmen, Uhl, Matthias, Habl, Gregor, Hensley, Frank W., Buechler, Markus W., Krempien, Robert, Huber, Peter E., Debus, Juergen, and Werner, Jens

Subjects

CANCER patients, CANCER treatment, CANCER relapse, INTRAOPERATIVE radiotherapy, THERAPEUTICS

Abstract

Background: To evaluate the use of intraoperative radiation therapy (IORT) in the multimodality treatment of patients with isolated local recurrences of pancreatic cancer. Methods: We retrospectively analyzed 36 patients with isolated local recurrences of pancreatic cancer who have been treated with a combination of surgery, IORT and EBRT. Median time from initial treatment to recurrence was 20 months. All patients were surgically explored. In 18 patients a gross total resection was achieved, whereas the other half received only debulking or no resection at all. All patients received IORT with a median dose of 15 Gy. Additional EBRT was applied to 31 patients with a median dose of 45 Gy, combined with concurrent, mainly gemcitabine-based chemotherapy. Results: Median follow-up in surviving patients was 23 months. Local progression was found in 6 patients after a median time of 17 months, resulting in estimated 1- and 2-year local control rates of 91% and 67%, respectively. Distant failure was observed in 23 patients, mainly in liver or peritoneal space. The median estimated progression-free survival was 9 months with 1- and 2-year rates of 40% and 26%, respectively. We found an encouraging estimated median overall survival of 19 months, transferring into 1- and 2-year rates of 66% and 45%. Notably 6 of 36 patients (17%) lived for more than 3 years. Severe postoperative complications were found in 3 and chemoradiation-related grade III toxicity in 6 patients. No severe IORT related toxicity was observed. Conclusion: Combination of surgery, IORT and EBRT in patients with isolated local recurrences of pancreatic cancer resulted in encouraging local control and overall survival in our cohort with acceptable toxicity. Our approach seems to be superior to palliative chemotherapy or chemoradiation alone and should be further investigated in a prospective setting specifically addressing isolated local recurrences of pancreatic cancer. [ABSTRACT FROM AUTHOR]

Published

2012

40. Pancreatic Cancer Susceptibility Loci and Their Role in Survival.

Author

Rizzato, Cosmeri, Campa, Daniele, Giese, Nathalia, Werner, Jens, Rachakonda, P. Sivaramakrishna, Kumar, Rajiv, Schanné, Michaela, Greenhalf, William, Costello, Eithne, Khaw, Kay-tee, Key, Tim J., Siddiq, Afshan, Lorenzo-Bermejo, Justo, Burwinkel, Barbara, Neoptolemos, John P., Büchler, Markus W., Hoheisel, Jörg D., Bauer, Andrea, and Canzian, Federico

Subjects

PANCREATIC cancer, CANCER patients, DNA polymerases, CELL nuclei, HEREDITY

Abstract

Pancreatic cancer has one of the worst mortality rates of all cancers. Little is known about its etiology, particularly regarding inherited risk. The PanScan project, a genome-wide association study, identified several common polymorphisms affecting pancreatic cancer susceptibility. Single nucleotide polymorphisms (SNPs) in ABO, sonic hedgehog (SHH), telomerase reverse transcriptase (TERT), nuclear receptor subfamily 5, group A, member 2 (NR5A2) were found to be associated with pancreatic cancer risk. Moreover the scan identified loci on chromosomes 13q22.1 and 15q14, to which no known genes or other functional elements are mapped. We sought to replicate these observations in two additional, independent populations (from Germany and the UK), and also evaluate the possible impact of these SNPs on patient survival. We genotyped 15 SNPs in 690 cases of pancreatic ductal adenocarcinoma (PDAC) and in 1277 healthy controls. We replicated several associations between SNPs and PDAC risk. Furthermore we found that SNP rs8028529 was weakly associated with a better overall survival (OS) in both populations. We have also found that NR5A2 rs12029406•T allele was associated with a shorter survival in the German population. In conclusion, we found that rs8028529 could be, if these results are replicated, a promising marker for both risk and prognosis for this lethal disease. [ABSTRACT FROM AUTHOR]

Published

2011

41. Prognostic Significance of Erythropoietin in Pancreatic Adenocarcinoma.

Author

Welsch, Thilo, Zschäbitz, Stefanie, Becker, Verena, Giese, Thomas, Bergmann, Frank, Hinz, Ulf, Keleg, Shereen, Heller, Anette, Sipos, Bence, Klingmüller, Ursula, Büchler, Markus W., Werner, Jens, and Giese, Nathalia A.

Subjects

PANCREATIC cancer, PROGNOSTIC tests, ERYTHROPOIETIN, ADENOCARCINOMA, PANCREATITIS, ECTOPIC tissue, HEALTH outcome assessment, GENE expression

Abstract

Background: Erythropoietin (Epo) administration has been reported to have tumor-promoting effects in anemic cancer patients. We investigated the prognostic impact of endogenous Epo in patients with pancreatic ductal adenocarcinoma (PDAC). Methodology: The clinico-pathological relevance of hemoglobin (Hb, n = 150), serum Epo (sEpo, n = 87) and tissue expression of Epo/Epo receptor (EpoR, n = 104) was analyzed in patients with PDAC. Epo/EpoR expression, signaling, growth, invasion and chemoresistance were studied in Epo-exposed PDAC cell lines. Results: Compared to donors, median preoperative Hb levels were reduced by 15% in both chronic pancreatitis (CP, p<0.05) and PDAC (p<0.001), reaching anemic grade in one third of patients. While inversely correlating to Hb (r =20.46), 95% of sEPO values lay within the normal range. The individual levels of compensation were adequate in CP (observed to predicted ratio, O/P = 0.99) but not in PDAC (O/P = 0.85). Strikingly, lower sEPO values yielding inadequate Epo responses were prominent in non-metastatic M0-patients, whereas these parameters were restored in metastatic M1-group (8 vs. 13 mU/mL; O/P = 0.82 vs. 0.96; p<0.01)--although Hb levels and the prevalence of anemia were comparable. Higher sEpo values (upper quartile ≥16 mU/ml) were not significantly different in M0 (20%) and M1 (30%) groups, but were an independent prognostic factor for shorter survival (HR 2.20, 10 vs. 17 months, p<0.05). The pattern of Epo expression in pancreas and liver suggested ectopic release of Epo by capillaries/vasa vasorum and hepatocytes, regulated by but not emanating from tumor cells. Epo could initiate PI3K/Akt signaling via EpoR in PDAC cells but failed to alter their functions, probably due to co-expression of the soluble EpoR isoform, known to antagonize Epo. Conclusion/Significance: Higher sEPO levels counteract anemia but worsen outcome in PDAC patients. Further trials are required to clarify how overcoming a sEPO threshold ≥16 mU/ml by endogenous or exogenous means may predispose to or promote metastatic progression. [ABSTRACT FROM AUTHOR]

Published

2011

42. Current State of Surgical Management of Pancreatic Cancer.

Author

Hackert, Thilo, Büchler, Markus W., and Werner, Jens

Subjects

CANCER treatment, CANCER patients, PANCREATIC cancer treatment, CANCER-related mortality, THERAPEUTICS, CANCER relapse

Abstract

Pancreatic cancer is still associated with a poor prognosis and remains-as the fourth leading cause of cancer related mortality-a therapeutic challenge. Overall long-term survival is about 1-5%, and in only 10-20% of pancreatic cancer patients is potentially curative surgery possible, increasing five-year survival rates to approximately 20-25%. Pancreatic surgery is a technically challenging procedure and has significantly changed during the past decades with regard to technical aspects as well as perioperative care. Standardized resections can be carried out with low morbidity and mortality below 5% in high volume institutions. Furthermore, there is growing evidence that also more extended resections including multivisceral approaches, vessel reconstructions or surgery for tumor recurrence can be carried out safely with favorable outcomes. The impact of adjuvant treatment, especially chemotherapy, has increased dramatically within recent years, leading to significantly improved postoperative survival, making pancreatic cancer therapy an interdisciplinary approach to achieve best results. [ABSTRACT FROM AUTHOR]

Published

2011

43. Anaplastic pancreatic cancer: Presentation, surgical management, and outcome.

Author

Strobel, Oliver, Hartwig, Werner, Bergmann, Frank, Hinz, Ulf, Hackert, Thilo, Grenacher, Lars, Schneider, Lutz, Fritz, Stefan, Gaida, Matthias M., Büchler, Markus W., and Werner, Jens

Subjects

PANCREATIC cancer, ONCOLOGIC surgery, HEALTH outcome assessment, ADENOCARCINOMA, BIOPSY, OSTEOCLASTS, CANCER prognosis

Abstract

Background: Anaplastic pancreatic cancers are rare neoplasms. The available data are focused on pathologic and molecular features, and little is known about the clinical presentation and management. The outcome of operative exploration and resection is unknown. Methods: From a prospective database, all consecutive operations for anaplastic pancreatic cancer performed at our institution were identified. The clinicopathologic details were analyzed and the outcome was compared with a matched group of typical pancreatic ductal adenocarcinomas (nested case-control study). Results: Eighteen patients with anaplastic pancreatic cancer were identified. The patients had a median age of 64 years. The tumors were large (median diameter, 4 cm) and showed peripheral contrast enhancement in radiologic imaging. Fifteen (83%) patients underwent resection, a palliative bypass procedure was performed in 1 (6%) patient, and 2 patients underwent exploration with biopsy only. Perioperative morbidity was 39% and mortality was 6%. The median survival rate in patients with anaplastic pancreatic cancer was 5.7 months and was less than in the control group of patients with pancreatic ductal adenocarcinoma (15.7 months). In anaplastic pancreatic cancer, the median duration of survival was significantly greater after R0/R1 resection, as compared with palliative surgery (7.1 vs 2.3 months). The duration of survival was significantly greater in neoplasms with osteoclast-like giant cells. In 3 (17%) patients, long-term survival of 33, 49, and 161 months was observed. Conclusion: Anaplastic pancreatic cancer is an aggressive type of pancreatic cancer with a short median survival; however, because of the observation of prolonged survival after resection, resection should be performed whenever possible. The presence of osteoclast-like giant cells is associated with a favorable prognosis. [ABSTRACT FROM AUTHOR]

Published

2011

44. Randomized controlled phase I/II study to investigate immune stimulatory effects by low dose radiotherapy in primarily operable pancreatic cancer.

Author

Timke, Carmen, Winnenthal, Hubertus Schmitz, Klug, Felix, Roeder, Falk F. F., Bonertz, Andreas, Reissfelder, Christoph, Rochet, Nathalie, Koch, Moritz, Tjaden, Christine, Buechler, Markus W., Debus, Juergen, Werner, Jens, Beckhove, Philipp, Weitz, Jürgen, and Huber, Peter E.

Subjects

RADIOTHERAPY, PANCREATIC cancer, T cells, IMMUNE response, MORTALITY

Abstract

Background: The efficiencies of T cell based immunotherapies are affected by insufficient migration and activation of tumor specific effector T cells in the tumor. Accumulating evidence exists on the ability of ionizing radiation to modify the tumor microenvironment and generate inflammation. The aim of this phase I/II clinical trial is to evaluate whether low dose single fraction radiotherapy can improve T cell associated antitumor immune response in patients with pancreatic cancer. Methods/Design: This trial has been designed as an investigator initiated; prospective randomised, 4-armed, controlled Phase I/II trial. Patients who are candidates for resection of pancreatic cancer will be randomized into 4 arms. A total of 40 patients will be enrolled. The patients receive 0 Gy, 0.5 Gy, 2 Gy or 5 Gy radiation precisely targeted to their pancreatic carcinoma. Radiation will be delivered by external beam radiotherapy using a 6 MV Linac with IMRT technique 48 h prior to the surgical resection. The primary objective is the determination of an active local external beam radiation dose, leading to tumor infiltrating T cells as a surrogate parameter for antitumor activity. Secondary objectives include local tumor control and recurrence patterns, survival, radiogenic treatment toxicity and postoperative morbidity and mortality, as well as quality of life. Further, frequencies of tumor reactive T cells in blood and bone marrow as well as whole blood cell transcriptomics and plasma-proteomics will be correlated with clinical outcome. An interim analysis will be performed after the enrolment of 20 patients for safety reasons. The evaluation of the primary endpoint will start four weeks after the last patient's enrolment. Discussion: This trial will answer the question whether a low dose radiotherapy localized to the pancreatic tumor only can increase the number of tumor infiltrating T cells and thus potentially enhance the antitumor immune response. The study will also investigate the prognostic and predictive value of radiation-induced T cell activity along with transcriptomic and proteomic data with respect to clinical outcome. Trial registration: ClinicalTrials.gov - NCT01027221. [ABSTRACT FROM AUTHOR]

Published

2011

45. New pre-analytical approach for the deep proteome analysis of sera from pancreatitis and pancreas cancer patients.

Author

Fakelman, Frederik, Felix, Klaus, Büchler, Markus W., and Werner, Jens

Subjects

CANCER patients, PANCREATIC cancer, PROTEOMICS, PANCREATITIS, BIOMARKERS, SERODIAGNOSIS, AUTOIMMUNE diseases, INSULIN

Abstract

The presence of high-abundance proteins and the wide dynamic range of protein-distribution complicates the proteome analysis of crude serum. The aim was to establish a new preanalytical protocol for analysis of the deep serum-proteome for biomarker discovery. Methods: We investigated the stability and functionality of ProteoMiner™ and tested the new protocol by SELDI-TOF-MS profiling with serum samples obtained from patients with different pancreatic diseases. Results: We developed a high-throughput protocol and proved the convenience of ProteoMiner™ in the 96-well format to provide insights into the deep serum proteome and facilitate the detection of novel serum biomarkers. Serum samples spiked with defined amounts of insulin, processed with ProteoMiner™ and analyzed by SELDI-TOF-MS revealed that the concentration of the spiked insulin was not altered by ProteoMiner™ treatment. Conclusion: ProteoMiner™ technology is robust preanalytical step and can be used in a high-throughput format for analysis of low-abundant proteins in serum. [ABSTRACT FROM AUTHOR]

Published

2010

46. Expression of L1CAM, COX-2, EGFR, c-KIT and Her2/neu in anaplastic pancreatic cancer: putative therapeutic targets?

Author

Bergmann, Frank, Moldenhauer, Gerhard, Herpel, Esther, Gaida, Matthias M, Strobel, Oliver, Werner, Jens, Esposito, Irene, Müerköster, Susanne Sebens, Schirmacher, Peter, and Kern, Michael A.

Subjects

PANCREATIC cancer, GIANT cell tumors, HISTOPATHOLOGY, CYCLOOXYGENASES, ADENOCARCINOMA

Abstract

Bergmann F, Moldenhauer G, Herpel E, Gaida M M, Strobel O, Werner J, Esposito I, Sebens Müerköster S, Schirmacher P & Kern M A (2010) Histopathology 56, 440–448 Expression of L1CAM, COX-2, EGFR, c-KIT and Her2/neu in anaplastic pancreatic cancer: putative therapeutic targets? Aims: Undifferentiated (anaplastic) pancreatic cancer and undifferentiated pancreatic carcinoma with osteoclast-like giant cells (giant cell tumour) are rare variants of pancreatic ductal adenocarcinoma. Representing biologically highly aggressive neoplasms, they are frequently diagnosed at an advanced stage. The response to established chemo- or radiochemotherapeutic treatment regimens is poor, and undifferentiated pancreatic cancer generally has a dismal prognosis. As additional therapeutic options have not yet been investigated in undifferentiated pancreatic cancer, the aim was to analyse the expression of putative therapeutic targets that have shown promising results in various other neoplasms. Methods and results: Fifteen cases of undifferentiated pancreatic cancer (seven containing osteoclast-like giant cells) were investigated clinicopathologically and immunohistochemically for putative therapeutic targets. Whereas L1CAM, cyclooxygenase (COX)-2 and epidermal growth factor receptor (EGFR) were found to be significantly expressed in 80%, 93% and 87% of the investigated tumours, respectively, there was no substantial expression of c-kit (CD117) and there was no detectable expression of Her2/neu. Conclusions: The expression of L1CAM, COX-2 and EGFR in the majority of undifferentiated pancreatic carcinomas suggests that they might represent targets for adjuvant therapy in anaplastic pancreatic cancer. On the other hand, c-kit and Her2/neu seem to have no relevance for the therapy of these tumours. [ABSTRACT FROM AUTHOR]

Published

2010

47. Vascular Structure and Microcirculation of Experimental Pancreatic Carcinoma in Rats.

Author

Schmidt, Jan, Ryschich, Eduard, Daniel, Volker, Herzog, Lueder, Werner, Jens, Herfarth, Christian, Longnecker, Daniel S., Gebhard, Martha M., and Klar, Ernst

Subjects

NEOVASCULARIZATION, PANCREATIC cancer

Abstract

Objective: To study angiogenesis and microcirculation in experimental pancreatic carcinoma. Design: Open experimental study. Setting: 2 University hospitals, Germany and USA. Animals: 16 male Lewis rats. Interventions: Induction of a duct-like pancreatic cancer in the pancreas and peritoneum by interposition of fragments of tumour between 2 inert transparent polymethylmethacrylate plates. Main outcome measures: Microcirculation in the tumour and interaction between leucocytes, tumour, and endothelium investigated by intravital microscopy. Results: The density of vessels in the carcinoma was significantly less than in normal pancreatic tissue (p = 0.0004). The vasculature of the tumour was characterised by a lack of differentiation in architecture of vessels, formation of sinusoidal and lacunar vessels and sudden changes in diameter of vessels. Red blood cell velocity differed among tumour vessels, but mean values were similar to those of normal exocrine pancreas. The mixed lymphocyte culture test indicated that the cell line DSL6A was immunogenic. However, high-affinity leucocyte-endothelium-interaction was significantly reduced in the tumour's microcirculation after both orthotopic and heterotopic implantation (p = 0.002). Rates of apoptosis were suppressed in heterotopic tumours compared with orthotopic ones. Tumour growth was faster in heterotopic tumours. Conclusions: Experimental duct-like pancreatic carcinoma can be differentiated from normal pancreas by: chaotic arrangement of vessels with loss of differentiation of architecture and heterogeneous distribution; the formation of sinusoidal or lacunar vessels; lower vascular density with similar erythrocyte velocity; increase in mean diameter of vessels; reduced leucocyte-endothelium interaction despite confirmed immunogeneity independent of wall shear rates. The site of implantation influences apoptosis and growth rates. [ABSTRACT FROM AUTHOR]

Published

2000

48. Cathepsin D Expression and Gemcitabine Resistance in Pancreatic Cancer.

Author

Mahajan, Ujjwal M, Goni, Elisabetta, Langhoff, Enno, Li, Qi, Costello, Eithne, Greenhalf, William, Kruger, Stephan, Ormanns, Steffen, Halloran, Christopher, Ganeh, Paula, Marron, Manuela, Lämmerhirt, Felix, Zhao, Yue, Beyer, Georg, Weiss, Frank-Ulrich, Sendler, Matthias, Bruns, Christiane J, Kohlmann, Thomas, Kirchner, Thomas, and Werner, Jens

Subjects

CATHEPSIN D, PANCREATIC cancer treatment, FLUOROURACIL

Abstract

Background Cathepsin-D (CatD), owing to its dual role as a proteolytic enzyme and as a ligand, has been implicated in cancer progression. The role of CatD in pancreatic ductal adenocarcinoma is unknown. Methods CatD expression quantified by immunohistochemistry of tumor-tissue microarrays of 403 resected pancreatic cancer patients from the ESPAC-Tplus trial, a translational study within the ESPAC (European Study Group for Pancreatic Cancer) trials, was dichotomously distributed to low and high H scores (cut off 22.35) for survival and multivariable analysis. The validation cohort (n = 69) was recruited based on the hazard ratio of CatD from ESPAC-Tplus. 5-fluorouracil-, and gemcitabine-resistant pancreatic cancer cell lines were employed for mechanistic experiments. All statistical tests were two-sided. Results Median overall survival was 23.75 months and median overall survival for patients with high CatD expression was 21.09 (95% confidence interval [CI] = 17.31 to 24.80) months vs 27.20 (95% CI = 23.75 to 31.90) months for low CatD expression (χ2LR, 1DF = 4.00; P  = .04). Multivariable analysis revealed CatD expression as a predictive marker in gemcitabine-treated (z stat = 2.33; P  = .02) but not in 5-fluorouracil-treated (z stat = 0.21; P  = .82) patients. An independent validation cohort confirmed CatD as a negative predictive marker for survival (χ2LR, 1DF = 6.80; P  = .009) and as an independent predictive marker in gemcitabine-treated patients with a hazard ratio of 3.38 (95% CI = 1.36 to 8.38, P = .008). Overexpression of CatD was associated with a concomitant suppression of the acid sphingomyelinase, and silencing of CatD resulted in upregulation of acid sphingomyelinase with rescue of gemcitabine resistance. Conclusions Adjuvant gemcitabine is less effective in pancreatic ductal adenocarcinoma with high CatD expression, and thus CatD could serve as a marker for biomarker-driven therapy. [ABSTRACT FROM AUTHOR]

Published

2020

49. Immune Cell and Stromal Signature Associated With Progression-Free Survival of Patients With Resected Pancreatic Ductal Adenocarcinoma.

Author

Mahajan, Ujjwal Mukund, Langhoff, Eno, Goni, Elisabetta, Costello, Eithne, Greenhalf, William, Halloran, Christopher, Ormanns, Steffen, Kruger, Stephan, Boeck, Stefan, Ribback, Silvia, Beyer, Georg, Dombroswki, Frank, Weiss, Frank-Ulrich, Neoptolemos, John P., Werner, Jens, D'Haese, Jan G., Bazhin, Alexandr, Peterhansl, Julian, Pichlmeier, Svenja, and Büchler, Markus W.

Abstract

Background & Aims Changes to the microenvironment of pancreatic ductal adenocarcinomas (PDACs) have been associated with poor outcomes of patients. We studied the associations between composition of the pancreatic stroma (fibrogenic, inert, dormant, or fibrolytic stroma) and infiltration by inflammatory cells and times of progression-free survival (PFS) of patients with PDACs after resection. Methods We obtained 1824 tissue microarray specimens from 385 patients included in the European Study Group for Pancreatic Cancer trial 1 and 3 and performed immunohistochemistry to detect alpha smooth muscle actin, type 1 collagen, CD3, CD4, CD8, CD68, CD206, and neutrophils. Tumors that expressed high and low levels of these markers were compared with patient outcomes using Kaplan-Meier curves and multivariable recursive partitioning for discrete-time survival tree analysis. Prognostic index was delineated by a multivariable Cox proportional hazards model of immune cell and stromal markers and PFS. Findings were validated using 279 tissue microarray specimens from 93 patients in a separate cohort. Results Levels of CD3, CD4, CD8, CD68, and CD206 were independently associated with tumor recurrence. Recursive partitioning for discrete-time survival tree analysis identified a high level of CD3 as the strongest independent predictor for longer PFS. Tumors with levels of CD3 and high levels of CD206 associated with a median PFS time of 16.6 months and a median prognostic index of –0.32 (95% confidence interval [CI] –0.35 to –0.31), whereas tumors with low level of CD3 cell and low level of CD8 and high level of CD68 associated with a median PFS time of 7.9 months and a prognostic index of 0.32 (95% CI 0.050–0.32); we called these patterns histologic signatures. Stroma composition, when unassociated with inflammatory cell markers, did not associate significantly with PFS. In the validation cohort, the histologic signature resulted in an error matrix accuracy of predicted response of 0.75 (95% CI 0.64–0.83; accuracy P <.001). Conclusions In an analysis of PDAC tissue microarray specimens, we identified and validated a histologic signature, based on leukocyte and stromal factors, that associates with PFS times of patients with resected PDACs. Immune cells might affect the composition of the pancreatic stroma to affect progression of PDAC. These findings provide new insights into the immune response to PDAC. Graphical abstract [ABSTRACT FROM AUTHOR]

Published

2018

50. The role of interleukin-18 in pancreatitis and pancreatic cancer.

Author

Li, Zhiqiang, Yu, Xiao, Werner, Jens, Bazhin, Alexandr V., and D'Haese, Jan G.

Subjects

*PANCREATIC cancer, *INTERLEUKIN-18, *KILLER cells, *PANCREATIC diseases, *CROHN'S disease, *ANTIBODY-dependent cell cytotoxicity, *MACROPHAGES

Abstract

• Interleukin-18 (IL-18) is a member of the IL-1 family of cytokines. • IL-18 is involved in Th1 and Th2 immune responses, and in activation of NK cells and macrophages. • IL-18 directly upregulates perforin- and FasL-dependent cytotoxicity of NK and CD8+ T cells. • Mechanism of IL-18 activity is the activation of NF-kB and STAT-4. • IL-18 plays an important role in various pathologies. Originally described as an interferon (IFN)-γ-inducing factor, interleukin (IL)-18 has been reported to be involved in Th1 and Th2 immune responses, as well as in activation of NK cells and macrophages. There is convincing evidence that IL-18 plays an important role in various pathologies (i.e. inflammatory diseases, cancer, chronic obstructive pulmonary disease, Crohn's disease and others). Recently, IL-18 has also been shown to execute specific effects in pancreatic diseases, including acute and chronic pancreatitis, as well as pancreatic cancer. The aim of this study was to give a profound review of recent data on the role of IL-18 and its potential as a therapeutic target in pancreatic diseases. The existing data on this topic are in part controversial and will be discussed in detail. Future studies should aim to confirm and clarify the role of IL-18 in pancreatic diseases and unravel their molecular mechanisms. [ABSTRACT FROM AUTHOR]

Published

2019