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Sunitinib added to FOLFIRI versus FOLFIRI in patients with chemorefractory advanced adenocarcinoma of the stomach or lower esophagus : a randomized, placebo-controlled phase II AIO trial with serum biomarker program (2016)

Background: As a multi-targeted anti-angiogenic receptor tyrosine kinase (RTK) inhibitor sunitinib (SUN) has been established for renal cancer and gastrointestinal stromal tumors. In advanced refractory esophagogastric cancer patients, monotherapy with SUN was associated with good tolerability but limited tumor response. Methods: This double-blind, placebo-controlled, multicenter, phase II clinical trial was conducted to evaluate the efficacy, safety and tolerability of SUN as an adjunct to second and third-line FOLFIRI (NCT01020630). Patients were randomized to receive 6-week cycles including FOLFIRI plus sodium folinate (Na-FOLFIRI) once every two weeks and SUN or placebo (PL) continuously for four weeks followed by a 2-week rest period. The primary study endpoint was progression-free survival (PFS). Preplanned serum analyses of VEGF-A, VEGF-D, VEGFR2 and SDF-1α were performed retrospectively. Results: Overall, 91 patients were randomized, 45 in each group (one patient withdrew). The main grade ≥3 AEs were neutropenia and leucopenia, observed in 56 %/20 % and 27 %/16 % for FOLFIRI + SUN/FOLFIRI + PL, respectively. Median PFS was similar, 3.5 vs. 3.3 months (hazard ratio (HR) 1.11, 95 % CI 0.70–1.74, P = 0.66) for FOLFIRI + SUN vs. FOLFIRI + PL, respectively. For FOLFIRI + SUN, a trend towards longer median overall survival (OS) compared with placebo was observed (10.4 vs. 8.9 months, HR 0.82, 95 % CI 0.50–1.34, one-sided P = 0.21). In subgroup serum analyses, significant changes in VEGF-A (P = 0.017), VEGFR2 (P = 0.012) and VEGF-D (P < 0.001) serum levels were observed. Conclusions: Although sunitinib combined with FOLFIRI did not improve PFS and response in chemotherapy-resistant gastric cancer, a trend towards better OS was observed. Further biomarker-driven studies with other anti-angiogenic RTK inhibitors are warranted. Trial registration: This study was registered prospectively in the NCT Clinical Trials Registry (ClinicalTrials.gov) under NCT01020630 on November 23, 2009 after approval by the leading ethics committee of the Medical Association of Rhineland-Palatinate, Mainz, in coordination with the participating ethics committees (see Additional file 2) on September 16, 2009.

Urologische Prostatakrebsvorsorge im Rahmen der Movember-Gesundheitsinitiative 2019 am Universitätsklinikum Frankfurt (2020)

Wenzel, Mike ; Humke, Clara Julia ; Wicker, Sabine ; Mani, Jens ; Engl, Tobias A. ; Hintereder, Gudrun ; Vogl, Thomas J. ; Wild, Peter Johannes ; Köllermann, Jens ; Rödel, Claus ; Asgharie, S. ; Theißen, Lena Hermine ; Welte, Maria-Noemi ; Kluth, Luis ; Mandel, Philipp ; Chun, Felix ; Preißer, Felix Martin ; Becker, Andreas

hintergrund: Männer in Deutschland sterben früher als Frauen und nehmen weniger häufig Krebsvorsorgeuntersuchungen wahr. Fragestellung: Ziel war die prospektive Evaluation einer „Movember-Gesundheitsinitiative“ am Universitätsklinikum Frankfurt (UKF) im November 2019. Methoden: Im Rahmen der „Movember-Gesundheitsinitiative“ wurde allen männlichen Mitarbeitern des UKF ab dem 45. Lebensjahr und bei erstgradiger familiärer Vorbelastung eines Prostatakarzinoms ab dem 40. Lebensjahr im November 2019 gemäß S3-Leitlinien der Deutschen Gesellschaft für Urologie (DGU) eine Prostatakarzinom-Vorsorgeuntersuchung angeboten. Ergebnisse: Insgesamt nahmen 14,4 % der Mitarbeiter teil. Eine familiäre Vorbelastung gaben insgesamt 14,0 % Teilnehmer an. Das mediane Alter betrug 54 Jahre. Der mediane PSA(prostataspezifisches Antigen)-Wert lag bei 0,9 ng/ml, der mediane PSA-Quotient bei 30 %. Bei 5 % (n = 6) zeigte sich ein suspekter Tastbefund in der DRU (digital-rektale Untersuchung). Nach Altersstratifizierung (≤ 50 vs. > 50 Lebensjahre) zeigten sich signifikante Unterschiede im medianen PSA-Wert (0,7 ng/ml vs. 1,0 ng/ml, p < 0,01) und der bereits zuvor durchgeführten urologischen Vorsorge (12,1 vs. 42,0 %, p < 0,01). Vier Teilnehmer (3,3 %) zeigten erhöhte Gesamt-PSA-Werte. Bei 32,2 % der Teilnehmer zeigte sich mindestens ein kontrollbedürftiger Befund. Insgesamt wurden 6 Prostatabiopsien durchgeführt. Hierbei zeigte sich in einem Fall ein intermediate-risk Prostatakarzinom (Gleason 3 + 4, pT3a, pPn1, pNx, R0). Schlussfolgerungung: Im Rahmen der UKF-Movember-Gesundheitsinitiative 2019 konnten durch ein Vorsorgeangebot 121 Männer für eine Prostatakrebs-Vorsorge inklusive PSA-Testung gewonnen werden. Auffällige/kontrollbedürftige Befunde zeigten sich bei 32,2 %. Bei einem Mitarbeiter wurde ein therapiebedürftiges Prostatakarzinom entdeckt und therapiert.

Der neue Armutsseismograf – die "Tafeln" : wer engagiert sich in dieser sozialen Bewegung? ; Studie zu Helfern und bedürftigen Menschen (2009)

Becker, Jens

Rezension zu: Stefan Selke: Fast ganz unten. Wie man in Deutschland durch die Hilfe von Lebensmitteltafeln satt wird. Verlag Westfälisches Dampfboot, Münster 2008. ISBN 978-3-89691-754-6 231 Seiten, 19,90 Euro.

"... dann wird die Rente nicht mehr das sein, was sie vielleicht für meine Eltern noch ist" : Alterssicherung und Alterssicherungspolitik aus Sicht der Bevölkerung (2007)

Becker, Jens ; Nüchter, Oliver

Das deutsche Rentensystem und der Generationenvertrag sind unter Druck geraten. Demografische Verschiebungen, anhaltende Massenarbeitslosigkeit sowie die Übertragung des westdeutschen Systems der Altersvorsorge auf die neuen Bundesländer führten zu einem Paradigmenwechsel in der Alterssicherungspolitik. Durch die mit der Riester-Förderung eingeführte private Altersvorsorge, das Alterseinkünftegesetz und die 2006 beschlossene sukzessive Erhöhung des Renteneintrittsalters auf 67 Jahre im Jahre 2029 sind die rentenpolitischen Konsolidierungsmaßnahmen vorerst zu einem Abschluss gekommen. Der Generationenvertrag, nach dem »der Anspruch der Rentner auf Sicherung ihres Lebensstandards und der Anspruch der Beitragszahler auf Berücksichtigung ihrer Leistungsfähigkeit gleichermaßen beachtet werden müssen«/1/, wurde somit durch die Stärkung der privaten und betrieblichen Vorsorge und eine Verlängerung der Lebensarbeitszeit ergänzt. ...

Cross section measurements of the e+e− → D*+D*− and e+e− → D*+D− processes at center-of-mass energies from 4.085 to 4.600 GeV (2022)

Ablikim, Medina ; Achasov, Mikhail N. ; Adlarson, Patrik ; Albrecht, Malte ; Aliberti, Riccardo ; Amoroso, Antonio ; An, M. R. ; An, Qi ; Bai, X. H. ; Bai, Yu ; Bakina, Olga ; Baldini Ferroli, Rinaldo ; Balossino, Ilaria ; Ban, Yong ; Batozskaya, V. ; Becker, D. ; Begzsuren, Khurelbaatar ; Berger, Niklaus ; Bertani, Monica ; Bettoni, Diego ; Bianchi, Fabrizio ; Bloms, Johannes ; Bortone, Alberto ; Boyko, Igor R. ; Briere, Roy A. ; Brüggemann, Anja ; Cai, Hao ; Cai, Xiao ; Calcaterra, Alessandro ; Cao, G. F. ; Cao, N. ; Çetin, Serkant Ali ; Chang, J. F. ; Chang, W. L. ; Chelkov, G. ; Chen, C. ; Chen, G. ; Chen, H. S. ; Chen, M. L. ; Chen, S. J. ; Chen, T. ; Chen, X. R. ; Chen, X. T. ; Chen, Y. B. ; Chen, Z. J. ; Cheng, W. S. ; Chu, X. ; Cibinetto, Gianluigi ; Cossio, Fabio ; Cui, J. J. ; Dai, H. L. ; Dai, J. P. ; Dbeyssi, A. ; de Boer, R. E. ; Dedovich, Dmitri V. ; Deng, Z. Y. ; Denig, Achim ; Denysenko, Igor ; Destefanis, Marco Giovanni Maria ; De Mori, Francesca ; Ding, Yanchun ; Dong, J. ; Dong, L. Y. ; Dong, M. Y. ; Dong, X. ; Du, S. X. ; Egorov, P. ; Fan, Y. L. ; Fang, J. ; Fang, S. S. ; Fang, W. X. ; Fang, Y. ; Farinelli, R. ; Fava, Luciano ; Feldbauer, Florian ; Felici, Giulietto ; Feng, C. Q. ; Feng, J. H. ; Fischer, K. ; Fritsch, Miriam ; Fritzsch, C. F. ; Fu, C. D. ; Gao, H. ; Gao, Y. N. ; Gao, Yang ; Garbolino, Sara ; Garzia, Isabella ; Ge, P. T. ; Geng, C. ; Gersabeck, Evelina ; Gilman, A. ; Götzen, Klaus ; Gong, L. ; Gong, W. X. ; Gradl, Wolfgang ; Greco, M. ; Gu, M. H. ; Guan, C. Y. ; Guo, A. Q. ; Guo, L. B. ; Guo, R. P. ; Guo, Y. P. ; Guskov, A. ; Han, T. T. ; Han, W. Y. ; Hao, X. Q. ; Harris, Frederick Allan ; He, K. K. ; He, K. L. ; Heinsius, Fritz-Herbert ; Heinz, C. H. ; Heng, Y. K. ; Herold, Christoph ; Himmelreich, Mathilde ; Holtmann, Tobias ; Hou, G. Y. ; Hou, Y. R. ; Hou, Z. L. ; Hu, H. M. ; Hu, J. F. ; Hu, T. ; Hu, Y. ; Huang, G. S. ; Huang, K. X. ; Huang, L. Q. ; Huang, L. Q. ; Huang, X. T. ; Huang, Y. P. ; Huang, Z. ; Hussain, Tahir ; Hüsken, Nils ; Imoehl, William ; Irshad, M. ; Jackson, J. ; Jaeger, S. ; Janchiv, S. ; Ji, Q. ; Ji, Q. P. ; Ji, X. B. ; Ji, X. L. ; Ji, Y. Y. ; Jia, Z. K. ; Jiang, H. B. ; Jiang, S. S. ; Jiang, X. S. ; Jiang, Y. ; Jiao, J. B. ; Jiao, Z. ; Jin, S. ; Jin, Y. ; Jing, M. Q. ; Johansson, Tord ; Kalantar-Nayestanaki, Nasser ; Kang, X. S. ; Kappert, R. ; Kavatsyuk, Myroslav O. ; Ke, B. C. ; Keshk, I. K. ; Khoukaz, Alfons ; Kiese, P. ; Kiuchi, R. ; Kliemt, Ralf ; Koch, L. ; Kolcu, O. B. ; Kopf, Bertram ; Kuemmel, M. ; Kuessner, M. ; Kupsc, Andrzej ; Kühn, Wolfgang ; Lane, J. J. ; Lange, Jens Sören ; Larin, Paul ; Lavania, A. ; Lavezzi, Lia ; Lei, Z. H. ; Leithoff, Hans Heinrich ; Lellmann, Max ; Lenz, T. ; Li, C. ; Li, C. ; Li, C. H. ; Li, Cheng ; Li, D. M. ; Li, F. ; Li, G. ; Li, H. ; Li, H. ; Li, H. B. ; Li, H. J. ; Li, H. N. ; Li, J. Q. ; Li, J. S. ; Li, J. W. ; Li, Ke ; Li, L. J. ; Li, L. K. ; Li, Lei ; Li, M. H. ; Li, P. R. ; Li, S. X. ; Li, S. Y. ; Li, T. ; Li, W. D. ; Li, W. G. ; Li, X. H. ; Li, Xing Long ; Li, Xiaoyu ; Li, Z. Y. ; Liang, H. ; Liang, H. ; Liang, H. ; Liang, Y. F. ; Liang, Y. T. ; Liao, G. R. ; Liao, L. Z. ; Libby, J. ; Limphirat, A. ; Lin, C. X. ; Lin, D. X. ; Lin, T. ; Liu, B. J. ; Liu, C. X. ; Liu, D. ; Liu, F. H. ; Liu, Fang ; Liu, Feng ; Liu, G. M. ; Liu, H. ; Liu, H. M. ; Liu, Huanhuan ; Liu, Huihui ; Liu, J. B. ; Liu, J. L. ; Liu, J. Y. ; Liu, K. ; Liu, K. Y. ; Liu, Ke ; Liu, L. ; Liu, M. H. ; Liu, P. L. ; Liu, Q. ; Liu, S. B. ; Liu, T. ; Liu, W. K. ; Liu, W. M. ; Liu, X. ; Liu, Y. ; Liu, Y. B. ; Liu, Z. A. ; Liu, Z. Q. ; Lou, X. C. ; Lu, F. X. ; Lu, H. J. ; Lu, J. G. ; Lu, X. L. ; Lu, Y. ; Lu, Y. P. ; Lu, Z. H. ; Luo, C. L. ; Luo, M. X. ; Luo, T. ; Luo, X. L. ; Lyu, X. R. ; Lyu, Y. F. ; Ma, F. C. ; Ma, H. L. ; Ma, L. L. ; Ma, M. M. ; Ma, Q. M. ; Ma, R. Q. ; Ma, R. T. ; Ma, X. Y. ; Ma, Y. ; Maas, Frank E. ; Maggiora, Marco ; Maldaner, Stephan ; Malde, S. ; Malik, Qadeer Afzal ; Mangoni, Alessio ; Mao, Y. J. ; Mao, Z. P. ; Marcello, S. ; Meng, Z. X. ; Messchendorp, Johannes Gerhardus ; Mezzadri, Giulio ; Miao, H. ; Min, T. J. ; Mitchell, Ryan Edward ; Mo, X. H. ; Muchnoi, Nikolai Yu. ; Muramatsu, Hajime ; Nefedov, Y. ; Nerling, Frank ; Nikolaev, Ivan Borisovich ; Ning, Z. ; Nisar, Shabana ; Niu, Y. ; Olsen, Stephen L. ; Ouyang, Q. ; Pacetti, Simone ; Pan, X. ; Pan, Y. ; Pathak, A. ; Pathak, A. ; Pelizäus, Marc ; Peng, H. P. ; Peters, Klaus ; Pettersson, J. ; Ping, J. L. ; Ping, R. G. ; Plura, S. ; Pogodin, S. ; Poling, Ronald ; Prasad, Vindhyawasini ; Qi, F. Z. ; Qi, H. ; Qi, H. R. ; Qi, M. ; Qi, T. Y. ; Qian, S. ; Qian, W. B. ; Qian, Z. ; Qiao, C. F. ; Qin, J. J. ; Qin, L. Q. ; Qin, X. P. ; Qin, X. S. ; Qin, Z. H. ; Qiu, J. F. ; Qu, S. Q. ; Qu, S. Q. ; Rashid, K. H. ; Redmer, C. F. ; Ren, K. J. ; Rivetti, Angelo ; Rodin, Viktor ; Da Rocha Rolo, Manuel Dionisio ; Rong, Gang ; Rosner, Christoph ; Ruan, S. N. ; Sang, H. S. ; Sarantsev, Andrei V. ; Schelhaas, Yasemin ; Schnier, Claudius ; Schoenning, Karin ; Scodeggio, Marco ; Shan, K. Y. ; Shan, W. ; Shan, X. Y. ; Shangguan, J. F. ; Shao, L. G. ; Shao, M. ; Shen, C. P. ; Shen, H. F. ; Shen, X. Y. ; Shi, B.-A. ; Shi, H. C. ; Shi, J. Y. ; Shi, R. S. ; Shi, X. ; D Shi, X. ; Song, J. J. ; Song, W. M. ; Song, Y. X. ; Sosio, Stefano ; Spataro, Stefano ; Stieler, F. ; Su, K. X. ; Su, P. P. ; Su, Y.-J. ; Sun, G. X. ; Sun, H. ; Sun, H. K. ; Sun, J. F. ; Sun, L. ; Sun, S. S. ; Sun, T. ; Sun, W. Y. ; Sun, X ; Sun, Y. J. ; Sun, Y. Z. ; Sun, Z. T. ; Tan, Y. H. ; Tan, Y. X. ; Tang, C. J. ; Tang, G. Y. ; Tang, J. ; Y Tao, L. ; Tao, Q. T. ; Teng, J. X. ; Thoren, Viktor ; Tian, W. H. ; Tian, Y. ; Uman, I. ; Wang, B. ; Wang, B. L. ; Wang, D. Y. ; Wang, F. ; Wang, H. J. ; Wang, H. P. ; Wang, K. ; Wang, L. L. ; Wang, M. ; Wang, M. Z. ; Wang, Meng ; Wang, S. ; Wang, T. ; Wang, T. J. ; Wang, W. ; Wang, W. H. ; Wang, W. P. ; Wang, X. ; Wang, X. F. ; Wang, X. L. ; Wang, Y. D. ; Wang, Y. F. ; Wang, Y. H. ; Wang, Y. Q. ; Wang, Ying ; Wang, Z. ; Wang, Z. Y. ; Wang, Ziyi ; Wei, D. H. ; Weidner, Frederik ; Wen, S. P. ; White, D. J. ; Wiedner, Ulrich ; Wilkinson, Guy ; Wolke, M. ; Wollenberg, Leonard ; Wu, J. F. ; Wu, L. H. ; Wu, L. J. ; Wu, X. ; Wu, X. H. ; Wu, Y. ; Wu, Z. ; Xia, L. ; Xiang, T. ; Xiao, D. ; Xiao, H. ; Xiao, S. Y. ; Xiao, Y. L. ; Xiao, Z. J. ; Xie, X. H. ; Xie, Y. ; Xie, Y. G. ; Xie, Y. H. ; Xie, Z. P. ; Xing, T. Y. ; Xu, C. F. ; Xu, C. J. ; Xu, G. F. ; Xu, Q. J. ; Xu, S. Y. ; Xu, X. P. ; Xu, Y. C. ; Yan, F. ; Yan, L. ; Yan, W. B. ; Yan, W. C. ; Yang, H. J. ; Yang, H. L. ; Yang, H. X. ; Yang, L. ; Yang, S. L. ; Yang, Tao ; Yang, Y. X. ; Yang, Yifan ; Ye, M. ; Ye, M. H. ; Yin, J. H. ; You, Z. Y. ; Yu, B. X. ; Yu, C. X. ; Yu, G. ; Yu, T. ; Yuan, C. Z. ; Yuan, L. ; Yuan, S. C. ; Yuan, X. Q. ; Yuan, Y. ; Yuan, Z. Y. ; Yue, C. X. ; Zafar, A. A. ; Zeng, F. R. ; Zeng Zeng, X. ; Zeng, Y. ; Zhan, Y. H. ; Zhang, A. Q. ; Zhang, B. L. ; Zhang, B. X. ; Zhang, D. H. ; Zhang, G. Y. ; Zhang, Haitao ; Zhang, H. H. ; Zhang, H. H. ; Zhang, H. Y. ; Zhang, J. L. ; Zhang, J. Q. ; Zhang, J. W. ; Zhang, J. X. ; Zhang, J. Y. ; Zhang, J. Z. ; Zhang, Jianyu ; Zhang, Jiawei ; Zhang, L. M. ; Zhang, L. Q. ; Zhang, Lei ; Zhang, P. ; Zhang, Q. Y. ; Zhang, Shulei ; Zhang, X. D. ; Zhang, X. M. ; Zhang, X. Y. ; Zhang, X. Y. ; Zhang, Y. ; Zhang, Y. T. ; Zhang, Y. H. ; Zhang, Yan ; Zhang, Yao ; Zhang, Z. H. ; Zhang, Z. Y. ; Zhang, Z. Y. ; Zhao, G. ; Zhao, J. ; Zhao, J. Y. ; Zhao, J. Z. ; Zhao, Lei ; Zhao, Ling ; Zhao, M. G. ; Zhao, Q. ; Zhao, S. J. ; Zhao, Y. B. ; Zhao, Y. X. ; Zhao, Z. G. ; Zhemchugov, Alexey ; Zheng, B. ; Zheng, J. P. ; Zheng, Y. H. ; Zhong, B. ; Zhong, C. ; Zhong, X. ; Zhou, H. ; Zhou, L. P. ; Zhou, X. ; Zhou, X. K. ; Zhou, X. R. ; Zhou, X. Y. ; Zhou, Y. Z. ; Zhu, Jianhui ; Zhu, K. ; Zhu, K. J. ; Zhu, L. X. ; Zhu, S. H. ; Zhu, T. J. ; Zhu, W. J. ; Zhu, Y. C. ; Zhu, Z. A. ; Zou, B. S. ; Zou, J. H.

The Born cross sections of the e+e− → D*+D*− and e+e− → D*+D− processes are measured using e+e− collision data collected with the BESIII experiment at center-of-mass energies from 4.085 to 4.600 GeV, corresponding to an integrated luminosity of 15.7 fb−1. The results are consistent with and more precise than the previous measurements by the Belle, Babar and CLEO collaborations. The measurements are essential for understanding the nature of vector charmonium and charmonium-like states.

Impact of "time-from-biopsy-to-prostatectomy" on adverse oncological results in patients with intermediate and high-risk prostate cancer (2020)

Engl, Tobias ; Mandel, Philipp ; Höh, Robert Benedikt ; Preißer, Felix Martin ; Wenzel, Mike ; Humke, Clara Julia ; Welte, Maria-Noemi ; Köllermann, Jens ; Wild, Peter Johannes ; Deuker, Marina ; Kluth, Luis A. ; Roos, Frederik ; Chun, Felix ; Becker, Andreas

Objective: Many patients with localized prostate cancer (PCa) do not immediately undergo radical prostatectomy (RP) after biopsy confirmation. The aim of this study was to investigate the influence of “time-from-biopsy-to- prostatectomy” on adverse pathological outcomes. Materials and Methods: Between January 2014 and December 2019, 437 patients with intermediate- and high risk PCa who underwent RP were retrospectively identified within our prospective institutional database. For the aim of our study, we focused on patients with intermediate- (n = 285) and high-risk (n = 151) PCa using D'Amico risk stratification. Endpoints were adverse pathological outcomes and proportion of nerve-sparing procedures after RP stratified by “time-from-biopsy-to-prostatectomy”: ≤3 months vs. >3 and < 6 months. Medians and interquartile ranges (IQR) were reported for continuously coded variables. The chi-square test examined the statistical significance of the differences in proportions while the Kruskal-Wallis test was used to examine differences in medians. Multivariable (ordered) logistic regressions, analyzing the impact of time between diagnosis and prostatectomy, were separately run for all relevant outcome variables (ISUP specimen, margin status, pathological stage, pathological nodal status, LVI, perineural invasion, nerve-sparing). Results: We observed no difference between patients undergoing RP ≤3 months vs. >3 and <6 months after diagnosis for the following oncological endpoints: pT-stage, ISUP grading, probability of a positive surgical margin, probability of lymph node invasion (LNI), lymphovascular invasion (LVI), and perineural invasion (pn) in patients with intermediate- and high-risk PCa. Likewise, the rates of nerve sparing procedures were 84.3 vs. 87.4% (p = 0.778) and 61.0% vs. 78.8% (p = 0.211), for intermediate- and high-risk PCa patients undergoing surgery after ≤3 months vs. >3 and <6 months, respectively. In multivariable adjusted analyses, a time to surgery >3 months did not significantly worsen any of the outcome variables in patients with intermediate- or high-risk PCa (all p > 0.05). Conclusion: A “time-from-biopsy-to-prostatectomy” of >3 and <6 months is neither associated with adverse pathological outcomes nor poorer chances of nerve sparing RP in intermediate- and high-risk PCa patients.

Mri-fusion targeted vs. Systematic prostate biopsy–how does the biopsy technique affect gleason grade concordance and upgrading after radical prostatectomy? (2019)

Rührup, Jessica ; Preißer, Felix Martin ; Theißen, Lena ; Wenzel, Mike ; Roos, Frederik ; Becker, Andreas ; Kluth, Luis ; Bodelle, Boris ; Köllermann, Jens ; Chun, Felix ; Mandel, Philipp

Introduction: MRI-targeted biopsy (TB) increases overall prostate-cancer (PCa) detection-rates and decreases the risk of insignificant PCa detection. However, the impact of these findings on the definite pathology after radical prostatectomy (RP) is under debate. Materials and Methods: Between 01/2014 and 12/2018, 366 patients undergoing prostate biopsy and RP were retrospectively analyzed. The correlation between biopsy Gleason-score (highest Gleason-score in a core) and the RP Gleason-score in patients undergoing systematic biopsy (SB-group) (n = 221) or TB+SB (TB-group, n = 145) was tested using the ISUP Gleason-group grading (GGG, scale 1–5). Sub analyses focused on biopsy GGG 1 and GGG ≥ 2. Results: Proportions of biopsy GGG 1–5 in the SB-group and TB-group were 24.4, 37.6, 19, 10.9, 8.1% and 13.8, 43.4, 24.2, 13.8, 4.8%, respectively (p = 0.07). Biopsy and pathologic GGG were concordant in 108 of 221 (48.9%) in SB- and 74 of 145 (51.1%) in TB-group (p = 0.8). Gleason upgrading was recorded in 33.5 and 31.7% in SB- vs. TB-group (p = 0.8). Patients with biopsy GGG 1 undergoing RP showed an upgrading in 68.5%(37/54) in SB- and 75%(15/20) in TB-group (p = 0.8). In patients with biopsy GGG ≥ 2 concordance increased for both biopsy approaches (54.5 vs. 55.2% for SB- vs. TB-group, p = 0.9). Discussion: Irrespective of differences in PCa detection-rates between TB- and SB-groups, no significant differences in GGG concordance and upgrading between patients of both groups undergoing biopsy, followed by RP, were recorded. Concordance rates increased in men with biopsy GGG ≥ 2. TB seems to detect more patients with PCa without a difference in concordance with final pathology.

Association of polo-like kinase 3 and PhosphoT273 caspase 8 levels with disease-related outcomes among cervical squamous cell carcinoma patients treated with chemoradiation and brachytherapy (2019)

Fleischmann, Max ; Martin, Daniel ; Peña-Llopis, Samuel ; Oppermann, Julius ; Müller-von der Grün, Jens ; Diefenhardt, Markus ; Chatzikonstantinou, Georgios ; Fokas, Emmanouil ; Rödel, Claus ; Strebhardt, Klaus ; Becker, Sven ; Rödel, Franz ; Tselis, Nikolaos

Introduction: Definitive chemoradiation (CRT) followed by high-dose-rate (HDR) brachytherapy (BT) represents state-of-the-art treatment for locally-advanced cervical cancer. Despite use of this treatment paradigm, disease-related outcomes have stagnated in recent years, indicating the need for biomarker development and improved patient stratification. Here, we report the association of Polo-like kinase (PLK) 3 expression and Caspase 8 T273 phosphorylation levels with survival among patients with cervical squamous cell carcinoma (CSCC) treated with CRT plus BT. Methods: We identified 74 patients with FIGO Stage Ib to IVb cervix squamous cell carcinoma. Baseline immunohistochemical scoring of PLK3 and pT273 Caspase 8 levels was performed on pre-treatment samples. Correlation was then assessed between marker expression and clinical endpoints, including cumulative incidences of local and distant failure, cancer-specific survival (CSS) and overall survival (OS). Data were then validated using The Cancer Genome Atlas (TCGA) dataset. Results: PLK3 expression levels were associated with pT273 Caspase 8 levels (p = 0.009), as well as N stage (p = 0.046), M stage (p = 0.026), and FIGO stage (p = 0.001). By the same token, pT273 Caspase 8 levels were associated with T stage (p = 0.031). Increased PLK3 levels corresponded to a lower risk of distant relapse (p = 0.009), improved CSS (p = 0.001), and OS (p = 0.003). Phospho T273 Caspase 8 similarly corresponded to decreased risk of distant failure (p = 0.021), and increased CSS (p < 0.001) and OS (p < 0.001) and remained a significant predictor for OS on multivariate analysis. TCGA data confirmed the association of low PLK3 expression with resistance to radiotherapy and BT (p < 0.05), as well as increased propensity for metastasis (p = 0.019). Finally, a combined PLK3 and pT273 Caspase 8 score predicted for decreased distant relapse (p = 0.005), and both improved CSS (p < 0.001) and OS (p < 0.001); this combined score independently predicted distant failure (p = 0.041) and CSS (p = 0.003) on multivariate analyses. Conclusion: Increased pre-treatment tumor levels of PLK3 and pT273 Caspase 8 correspond to improved disease-related outcomes among cervical cancer patients treated with CRT plus BT, representing a potential biomarker in this context.

Efficient laser-driven proton acceleration from a cryogenic solid hydrogen target (2019)

Polz, Jens ; Robinson, Alexander P. L. ; Kalinin, Anton ; Becker, Georg Alexander ; Costa Fraga, Rui Alexandre ; Hellwing, Marco ; Hornung, Marco ; Keppler, Sebastian ; Kessler, Alexander ; Klöpfel, Diethard ; Liebetrau, Hartmut ; Schorcht, Frank ; Hein, Joachim ; Zepf, Matthäus ; Grisenti, Robert Evaristo ; Kaluza, Malte Christoph

We report on the successful implementation and characterization of a cryogenic solid hydrogen target in experiments on high-power laser-driven proton acceleration. When irradiating a solid hydrogen filament of 10 μm diameter with 10-Terawatt laser pulses of 2.5 J energy, protons with kinetic energies in excess of 20 MeV exhibiting non-thermal features in their spectrum were observed. The protons were emitted into a large solid angle reaching a total conversion efficiency of several percent. Two-dimensional particle-in-cell simulations confirm our results indicating that the spectral modulations are caused by collisionless shocks launched from the surface of the the high-density filament into a low-density corona surrounding the target. The use of solid hydrogen targets may significantly improve the prospects of laser-accelerated proton pulses for future applications.

Immunohistochemistry for prostate biopsy - impact on histological prostate cancer diagnoses and clinical decision making (2021)

Mandel, Philipp ; Wenzel, Mike ; Höh, Robert Benedikt ; Welte, Maria-Noemi ; Preißer, Felix Martin ; Inam, Tahir ; Wittler, Clarissa ; Humke, Clara Julia ; Köllermann, Jens ; Wild, Peter Johannes ; Würnschimmel, Christoph ; Tilki, Derya ; Graefen, Markus ; Kluth, Luis ; Karakiewicz, Pierre I. ; Chun, Felix ; Becker, Andreas

Background: To test the value of immunohistochemistry (IHC) staining in prostate biopsies for changes in biopsy results and its impact on treatment decision-making. Methods: Between January 2017–June 2020, all patients undergoing prostate biopsies were identified and evaluated regarding additional IHC staining for diagnostic purpose. Final pathologic results after radical prostatectomy (RP) were analyzed regarding the effect of IHC at biopsy. Results: Of 606 biopsies, 350 (58.7%) received additional IHC staining. Of those, prostate cancer (PCa) was found in 208 patients (59.4%); while in 142 patients (40.6%), PCa could be ruled out through IHC. IHC patients harbored significantly more often Gleason 6 in biopsy (p < 0.01) and less suspicious baseline characteristics than patients without IHC. Of 185 patients with positive IHC and PCa detection, IHC led to a change in biopsy results in 81 (43.8%) patients. Of these patients with changes in biopsy results due to IHC, 42 (51.9%) underwent RP with 59.5% harboring ≥pT3 and/or Gleason 7–10. Conclusions: Patients with IHC stains had less suspicious characteristics than patients without IHC. Moreover, in patients with positive IHC and PCa detection, a change in biopsy results was observed in >40%. Patients with changes in biopsy results partly underwent RP, in which 60% harbored significant PCa.

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