TY - JOUR A1 - Klement, Rainer J. A1 - Popp, Ilinca A1 - Kaul, David A1 - Ehret, Felix A1 - Grosu, Anca L. A1 - Polat, Bülent A1 - Sweeney, Reinhart A. A1 - Lewitzki, Victor T1 - Accelerated hyper-versus normofractionated radiochemotherapy with temozolomide in patients with glioblastoma: a multicenter retrospective analysis JF - Journal of Neuro-Oncology N2 - Background and Purpose The standard treatment of glioblastoma patients consists of surgery followed by normofractionated radiotherapy (NFRT) with concomitant and adjuvant temozolomide chemotherapy. Whether accelerated hyperfractionated radiotherapy (HFRT) yields comparable results to NFRT in combination with temozolomide has only sparsely been investigated. The objective of this study was to compare NFRT with HFRT in a multicenter analysis. Materials and Methods A total of 484 glioblastoma patients from four centers were retrospectively pooled and analyzed. Three-hundred-ten and 174 patients had been treated with NFRT (30 × 1.8 Gy or 30 × 2 Gy) and HFRT (37 × 1.6 Gy or 30 × 1.8 Gy twice/day), respectively. The primary outcome of interest was overall survival (OS) which was correlated with patient-, tumor- and treatment-related variables via univariable and multivariable Cox frailty models. For multivariable modeling, missing covariates were imputed using multiple imputation by chained equations, and a sensitivity analysis was performed on the complete-cases-only dataset. Results After a median follow-up of 15.7 months (range 0.8-88.6 months), median OS was 16.9 months (15.0-18.7 months) in the NFRT group and 14.9 months (13.2-17.3 months) in the HFRT group (p = 0.26). In multivariable frailty regression, better performance status, gross-total versus not gross-total resection, MGMT hypermethylation, IDH mutation, smaller planning target volume and salvage therapy were significantly associated with longer OS (all p < 0.01). Treatment differences (HFRT versus NFRT) had no significant effect on OS in either univariable or multivariable analysis. Conclusions Since HFRT with temozolomide was not associated with worse OS, we assume HFRT to be a potential option for patients wishing to shorten their treatment time. KW - temozolomide KW - accelerated hyperfractionation KW - altered fractionation KW - glioblastoma KW - radiotherapy Y1 - 2022 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-269806 SN - 1573-7373 VL - 156 IS - 2 ER - TY - JOUR A1 - Zimmermann, Marcus A1 - Richter, Anne A1 - Weick, Stefan A1 - Exner, Florian A1 - Mantel, Frederick A1 - Diefenhardt, Markus A1 - Fokas, Emmanouil A1 - Kosmala, Rebekka A1 - Flentje, Michael A1 - Polat, Bülent T1 - Acute toxicities of patients with locally advanced rectal cancer treated with intensified chemoradiotherapy within the CAO/ARO/AIO-12 trial: comparing conventional versus VMAT planning at a single center JF - Scientific Reports N2 - In locally advanced rectal cancer (LARC) neoadjuvant chemoradiotherapy is regarded as standard treatment. We assessed acute toxicities in patients receiving conventional 3D-conformal radiotherapy (3D-RT) and correlated them with dosimetric parameters after re-planning with volumetric modulated arc therapy (VMAT). Patients were randomized within the multicenter CAO/ARO/AIO-12 trial and received 50.4 Gy in 28 fractions and simultaneous chemotherapy with fluorouracil and oxaliplatin. Organs at risk (OAR) were contoured in a standardized approach. Acute toxicities and dose volume histogram parameters of 3D-RT plans were compared to retrospectively calculated VMAT plans. From 08/2015 to 01/2018, 35 patients with LARC were treated at one study center. Thirty-four patients were analyzed of whom 1 (3%) was UICC stage II and 33 (97%) patients were UICC stage III. Grade 3 acute toxicities occurred in 5 patients (15%). Patients with acute grade 1 cystitis (n = 9) had significantly higher D\(_{mean}\) values for bladder (29.4 Gy vs. 25.2 Gy, p < 0.01) compared to patients without bladder toxicities. Acute diarrhea was associated with small bowel volume (grade 2: 870.1 ccm vs. grade 0–1: 647.3 ccm; p < 0.01) and with the irradiated volumes V5 to V50. Using VMAT planning, we could reduce mean doses and irradiated volumes for all OAR: D\(_{mean}\) bladder (21.9 Gy vs. 26.3 Gy, p < 0.01), small bowel volumes V5–V45 (p < 0.01), D\(_{mean}\) anal sphincter (34.6 Gy vs. 35.6 Gy, p < 0.01) and D\(_{mean}\) femoral heads (right 11.4 Gy vs. 25.9 Gy, left 12.5 Gy vs. 26.6 Gy, p < 0.01). Acute small bowel and bladder toxicities were dose and volume dependent. Dose and volume sparing for all OAR could be achieved through VMAT planning and might result in less acute toxicities. KW - radiotherapy KW - rectal cancer Y1 - 2022 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-301255 VL - 12 ER - TY - JOUR A1 - Bratengeier, Klaus A1 - Holubyev, Kostyantyn T1 - Anisotropy of dose contributions-an instrument to upgrade real time IMRT and VMAT adaptation? JF - Medical Physics N2 - Purpose: To suggest a definition of dose deposition anisotropy for the purpose of ad hoc adaptation of intensity modulated arc therapy (IMRT) and volumetric arc therapy (VMAT), particularly in the vicinity of important organs at risk (OAR), also for large deformations. Methods: Beam's-eye-view (BEV) based fluence warping is a standard adaptation method with disadvantages for strongly varying OAR shapes. 2-Step-adaptation overcomes these difficulties by a deeper analysis of the 3D properties of adaptation processes, but requires separate arcs for every OAR to spare, which makes it impractical for cases with multiple OARs. The authors aim to extend the 2-Step method to arbitrary intensity modulated plan by analyzing the anisotropy of dose contributions. Anisotropy was defined as a second term of Fourier transformation of gantry angle dependent dose contributions. For a cylindrical planning target volume (PTV) surrounding an OAR of varying diameter, the anisotropy and the dose-normalized anisotropy were analyzed for several scenarios of optimized fluence distributions. 2-Step adaptation to decreasing and increasing OAR diameter was performed, and compared to a usual fluence based adaptation method. For two clinical cases, prostate and neck, the VMAT was generated and the behavior of anisotropy was qualitatively explored for deformed organs at risk. # Results: Dose contribution anisotropy in the PTV peaks around nearby OARs. The thickness of the "anisotropy wall" around OAR increases for increasing OAR radius, as also does the width of 2-Step dose saturating fluence peak adjacent to the OAR K. Bratengeier et al., "A comparison between 2-Step IMRT and conventional IMRT planning," Radiother. Oncol. 84, 298-306 (2007)]. Different optimized beam fluence profiles resulted in comparable radial dependence of normalized anisotropy. As predicted, even for patient cases, anisotropy was inflated even more than increasing diameters of OAR. Conclusions: For cylindrically symmetric cases, the dose distribution anisotropy defined in the present work implicitly contains adaptation-relevant information about 3D relationships between PTV and OAR and degree of OAR sparing. For more complex realistic cases, it shows the predicted behavior qualitatively. The authors claim to have found a first component for advancing a 2-Step adaptation to a universal adaptation algorithm based on the BEV projection of the dose anisotropy. Further planning studies to explore the potential of anisotropy for adaptation algorithms using phantoms and clinical cases of differing complexity will follow. KW - modulated arc therapy KW - 2-step IMRT KW - radiation-therapy KW - online adaption KW - prostate-cancer KW - plans KW - IMAT KW - tracking KW - radiotherapy KW - adaption KW - IMRT KW - VMAT Y1 - 2016 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-186833 VL - 43 IS - 11 ER - TY - THES A1 - Popp, Karoline T1 - Die Lagevariabilität des Ring-Stift-Applikators bei der Brachytherapie zur Primärbehandlung des Zervix-Karzinoms T1 - Variability of the pelvic position of a Tandem-Applicator-System in multiple HDR-brachytherapy fractions for primary treatment of cervical cancer N2 - Die primäre Strahlentherapie des Zervix-Karzinoms unter kurativer Absicht besteht immer aus einer Kombination aus Tele- und Brachytherapie. Aus strahlenbiologischen Gründen ist dabei die Ausblendung des Brachytherapie-Volumens zeitlich vor Beginn oder zumindest vor Abschluß der intrauterinen Bestrahlung erforderlich. Aus diesem Grund ist die prospektive Kenntnis der möglichen Variabilität der Applikatorlage und damit der räumlichen Dosisverteilung von großer Bedeutung. In der vorliegenden Arbeit wurde daher die Applikatorlage und ihre Variabilität bei 92 Patientinnen mit jeweils fünf intrauterinen Bestrahlungen retrospektiv untersucht. Mit Hilfe orthogonaler Röntgenaufnahmen von ventral und seitlich wurde die Applikatorlage relativ zu knöchernen Referenzstrukturen des Beckens bestimmt. Der Applikatorursprung lag im Mittel 14mm kaudal der Hüftpfannenebene (55mm kaudal bis 23mm kranial, SD 14mm), 1mm rechts der Beckenmitte (27mm links bis 23mm rechts, SD 6mm) und 26mm dorsal der Hüftkopfmitte (6-53mm dorsal, SD 8mm). Daraus resultierte eine interindividuelle Lagevariabilität von 78mm in kraniokaudaler Richtung, 50mm in lateraler Richtung und 47mm in ventrodorsaler Richtung. Insgesamt betrug die intraindividuelle Variabilität der Applikatorlage unabhängig von einer bestimmten Applikation im Mittel 14mm (2-36mm, SD 6mm) in kraniokaudaler Richtung, 6mm (2-23mm, SD 3mm) in lateraler Richtung und 10mm (2-34mm, SD 6mm) in ventrodorsaler Richtung. Die erste Brachytherapie-Applikation sollte demnach kurz vor der geplanten Ausblendung des Brachytherapie-Volumens aus dem der Teletherapie erfolgen. Die Größe des Blockes richtet sich dann nach der Referenzisodose des Applikatorsystems mit einem Sicherheitsabstand von 2 SD in jeder Richtung, d.h. 24mm in kraniokaudaler und 12mm in lateraler Richtung. N2 - The introduction of 3-D treatment planning in combined tele-brachytherapy for cancer of the uterine cervix allows optimisation of matching the dose distributions. Brachytherapy volume has to be shielded from percutaneous irradiation. As dose distribution is strongly related to the applicator, applicator position was analysed in 92 patients with 5 insertions relative to bony landmarks. The applicator position was located at mean 14 mm caudal (-55 /23 mm SD 14mm), 1mm right (-27/23mm; SD 6mm) and 26 mm dorsal (6/53mm,SD 9mm) of the bony reference system. Consecutively the maximum interindividual variability was 78 mm in longitudinal, 50 mm in lateral and 47 mm in anterior-posterior direction. The intraindividual variability between 5 insertions at mean was 14 mm (2-36mm, SD 6mm) in longitudinal, 6 mm (2-23mm, SD 3mm) in lateral and 10 mm (2-34mm, SD 6mm) in ap direction. Therefore information of applicator position of the first insertion increases prediction of applicator position to a significant amount. If precise dose matching of tele- and brachytherapy is intended, applicator position of the first insertion should be known. KW - Zervixkarzinom KW - Bestrahlung KW - Brachytherapie KW - Applikatorposition KW - cervical cancer KW - radiotherapy KW - brachytherapy KW - position of applicator Y1 - 2003 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-4947 ER - TY - JOUR A1 - Kroeber, Jana A1 - Wenger, Barbara A1 - Schwegler, Manuela A1 - Daniel, Christoph A1 - Schmidt, Manfred A1 - Djuzenova, Cholpon S A1 - Polat, Bülent A1 - Flentje, Michael A1 - Fietkau, Rainer A1 - Distel, Luitpold V. T1 - Distinct increased outliers among 136 rectal cancer patients assessed by \(\gamma\)H2AX JF - Radiation Oncology N2 - Background: In recent years attention has focused on \(\gamma\)H2AX as a very sensitive double strand break indicator. It has been suggested that \(\gamma\)H2AX might be able to predict individual radiosensitivity. Our aim was to study the induction and repair of DNA double strand breaks labelled by \(\gamma\)H2AX in a large cohort. Methods: In a prospective study lymphocytes of 136 rectal cancer (RC) patients and 59 healthy individuals were ex vivo irradiated (IR) and initial DNA damage was compared to remaining DNA damage after 2 Gy and 24 hours repair time and preexisting DNA damage in unirradiated lymphocytes. Lymphocytes were immunostained with anti-\(\gamma\)H2AX antibodies and microscopic images with an extended depth of field were acquired. \(\gamma\)H2AX foci counting was performed using a semi-automatic image analysis software. Results: Distinct increased values of preexisting and remaining \(\gamma\)H2AX foci in the group of RC patients were found compared to the healthy individuals. Additionally there are clear differences within the groups and there are outliers in about 12% of the RC patients after ex vivo IR. Conclusions: The \(\gamma\)H2AX assay has the capability to identify a group of outliers which are most probably patients with increased radiosensitivity having the highest risk of suffering radiotherapy-related late sequelae. KW - histone H2AX KW - blood lymphocytes KW - in vivo KW - foci KW - individual radiosensitivity KW - rectal cancer KW - radiotherapy KW - DNA double strand breaks KW - phosphorylation KW - neck cancer KW - oral mucositis KW - DNA damage KW - radiosensitivity KW - repair KW - \(\gamma\)h2ax Y1 - 2015 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-144085 VL - 10 IS - 36 ER - TY - JOUR A1 - Bratengeier, Klaus A1 - Herzog, Barbara A1 - Wegener, Sonja A1 - Holubyev, Kostyantyn T1 - Finer leaf resolution and steeper beam edges using a virtual isocentre in concurrence to PTV-shaped collimators in standard distance – a planning study JF - Radiation Oncology N2 - Purpose: Investigation of a reduced source to target distance to improve organ at risk sparing during stereotactic irradiation (STX). Methods: The authors present a planning study with perfectly target-volume adapted collimator compared with multi-leaf collimator (MLC) at reduced source to virtual isocentre distance (SVID) in contrast to normal source to isocentre distance (SID) for stereotactic applications. The role of MLC leaf width and 20–80% penumbra was examined concerning the healthy tissue sparing. Several prescription schemes and target diameters are considered. Results: Paddick’s gradient index (GI) as well as comparison of the mean doses to spherical shells at several distances to the target is evaluated. Both emphasize the same results: the healthy tissue sparing in the high dose area around the planning target volume (PTV) is improved at reduced SVID ≤ 70 cm. The effect can be attributed more to steeper penumbra than to finer leaf resolution. Comparing circular collimators at different SVID just as MLC-shaped collimators, always the GI was reduced. Even MLC-shaped collimator at SVID 70 cm had better healthy tissue sparing than an optimal shaped circular collimator at SID 100 cm. Regarding penumbra changes due to varying SVID, the results of the planning study are underlined by film dosimetry measurements with Agility™ MLC. Conclusion: Penumbra requires more attention in comparing studies, especially studies using different planning systems. Reduced SVID probably allows usage of conventional MLC for STX-like irradiations. KW - radiotherapy KW - multi-leaf collimator KW - stereotactic irradiation KW - robotic table motion KW - planning study KW - virtual isocentre Y1 - 2017 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-157543 VL - 12 IS - 88 ER - TY - JOUR A1 - Lisowski, Dominik A1 - Trömel, Jannik A1 - Lutyj, Paul A1 - Lewitzki, Victor A1 - Hartrampf, Philipp E. A1 - Polat, Bülent A1 - Flentje, Michael A1 - Tamihardja, Jörg T1 - Health-related quality of life and clinical outcome after radiotherapy of patients with intracranial meningioma JF - Scientific Reports N2 - This retrospective, single-institutional study investigated long-term outcome, toxicity and health-related quality of life (HRQoL) in meningioma patients after radiotherapy. We analyzed the data of 119 patients who received radiotherapy at our department from 1997 to 2014 for intracranial WHO grade I-III meningioma. Fractionated stereotactic radiotherapy (FSRT), intensity modulated radiotherapy (IMRT) or radiosurgery radiation was applied. The EORTC QLQ-C30 and QLQ-BN20 questionnaires were completed for assessment of HRQoL. Overall survival (OS) for the entire study group was 89.6% at 5 years and 75.9% at 10 years. Local control (LC) at 5 and 10 years was 82.4% and 73.4%, respectively. Local recurrence was observed in 22 patients (18.5%). Higher grade acute and chronic toxicities were observed in seven patients (5.9%) and five patients (4.2%), respectively. Global health status was rated with a mean of 59.9 points (SD 22.3) on QLQ-C30. In conclusion, radiotherapy resulted in very good long-term survival and tumor control rates with low rates of severe toxicities but with a deterioration of long-term HRQoL. KW - CNS cancer KW - outcomes research KW - radiotherapy Y1 - 2022 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-301233 VL - 12 ER - TY - JOUR A1 - Said, Harun M. A1 - Polat, Buelent A1 - Stein, Susanne A1 - Guckenberger, Mathias A1 - Hagemann, Carsten A1 - Staab, Adrian A1 - Katzer, Astrid A1 - Anacker, Jelena A1 - Flentje, Michael A1 - Vordermark, Dirk T1 - Inhibition of N-Myc down regulated gene 1 in in vitro cultured human glioblastoma cells JF - World Journal of Clinical Oncology N2 - AIM: To study short dsRNA oligonucleotides (siRNA) as a potent tool for artificially modulating gene expression of N-Myc down regulated gene 1 (NDRG1) gene induced under different physiological conditions (Normoxia and hypoxia) modulating NDRG1 transcription, mRNA stability and translation. METHODS: A cell line established from a patient with glioblastoma multiforme. Plasmid DNA for transfections was prepared with the Endofree Plasmid Maxi kit. From plates containing 5 x 10(7) cells, nuclear extracts were prepared according to previous protocols. The pSUPER-NDRG1 vectors were designed, two sequences were selected from the human NDRG1 cDNA (5'-GCATTATTGGCATGGGAAC-3' and 5'-ATGCAGAGTAACGTGGAAG-3'. reverse transcription polymerase chain reaction was performed using primers designed using published information on -actin and hypoxia-inducible factor (HIF)-1 mRNA sequences in GenBank. NDRG1 mRNA and protein level expression results under different conditions of hypoxia or reoxygenation were compared to aerobic control conditions using the Mann-Whitney U test. Reoxygenation values were also compared to the NDRG1 levels after 24 h of hypoxia (P < 0.05 was considered significant). RESULTS: siRNA- and iodoacetate (IAA)-mediated downregulation of NDRG1 mRNA and protein expression in vitro in human glioblastoma cell lines showed a nearly complete inhibition of NDRG1 expression when compared to the results obtained due to the inhibitory role of glycolysis inhibitor IAA. Hypoxia responsive elements bound by nuclear HIF-1 in human glioblastoma cells in vitro under different oxygenation conditions and the clearly enhanced binding of nuclear extracts from glioblastoma cell samples exposed to extreme hypoxic conditions confirmed the HIF-1 Western blotting results. CONCLUSION: NDRG1 represents an additional diagnostic marker for brain tumor detection, due to the role of hypoxia in regulating this gene, and it can represent a potential target for tumor treatment in human glioblastoma. The siRNA method can represent an elegant alternative to modulate the expression of the hypoxia induced NDRG1 gene and can help to monitor the development of the cancer disease treatment outcome through monitoring the expression of this gene in the patients undergoing the different therapeutic treatment alternatives available nowadays. KW - Strahlentherapie KW - brain cancer KW - radiotherapy KW - human cancer diseases KW - Short dsRNA oligonucleotides KW - N-Myc down regulated gene 1 Y1 - 2012 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-123385 VL - 3 IS - 7 ER - TY - THES A1 - Glüer, Wibke T1 - Kosmetische Ergebnisse nach Bestrahlung bei Brusterhaltender Therapie des Mammakarzinoms T1 - Cosmetic results following radiation and breast-conserving therapy N2 - Ziel: Auswirkungen der strahlentherapeutischen Vorgehensweise, insbesondere der lokalen Dosisaufsättigung auf das kosmetische Langzeitergebnis und die Rezidivrate nach Brusterhaltender Therapie. Material und Methoden: In die Studie aufgenommen wurden 451 Patientinnen mit Mammakarzinom, die zwischen 1984-1994 in der Universitätsfrauenklinik und der Klinik und Poliklinik für Strahlentherapie der Universität Würzburg brusterhaltend therapiert wurden und bei denen Informationen zum kosmetischen Langzeitergebnis vorlagen. Behandlung: Alle Patientinnen unterzogen sich einer operativen Tumorentfernung und Axilladissektion, sowie einer Strahlenbehandlung. Die Strahlentherapie bestand aus einer homogenen Bestrahlug der betroffenen Brust (50Gy) und einer Tuorbettaufsättigung (20Gy), entweder als interstitieller Boost mit Ir-192 (77 Prozent) oder als Elektronenboost (16 Prozent). Ergebnisse: Die Überlebensrate betrug nach 5 und 10 Jahren 88 bzw. 73 Prozent. Die lokoregionäre Kontrollrate betrug nach 5 und 10 Jahren 90 und 75 Prozent. Es konnte kein statistisch signifikanter Zusammenhang mit der Art der angewandten Tumorbettaufsättigung festgestellt werden. Ein gutes bis exzellentes kosmetisches Ergebnis konnte bei 61 Prozent der Patientinnen erreicht werden. Auch hier besteht kein statistisch signifikanter Zusammenhang mit der gewählten Boostart. N2 - Purpose: Effect of radiotherapy, especially of the type of boost on the late cosmetic outcome and frequency of recurrences after breast-conserving therapy. Methods and materials: 451 patients, treated between 1984-1994 in the Universitätsfrauenklinik and the Klinik und Poliklinik für Strahlentherapie der Universität Würzburg, with evaluable records for cosmetic outcome were analyzed retrospectively. Therapy: All patients had a tumor excision and axillary dissection followed by radiation therapy. The entire breast received an external beam dose of 50Gy. A boost dose of 20Gy to the tumor bed was given with an Ir-192 implant (77 per cent) or with electron beam therapy (16 per cent). Results: The 5- and 10- year survival rates were 88 and 73 per cent. The 5- and 10 year locoregional control rates were 90 and 75 per cent. There were no statistically significant differences wether implant or electron beam were used. 61 Prozent of patients obtained a good or excellent cosmetic result, and no statistically significant differences in cosmetic outcome were seen regardless which of the two methods of therapy was applied. KW - Brustkrebs KW - Strahlentherapie KW - Kosmetik KW - lokale Dosisaufsättigung KW - breast cancer KW - radiotherapy KW - cosmetic KW - boost Y1 - 2000 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-452 ER - TY - THES A1 - Rosenheim, Eva T1 - Operation und adjuvante Bestrahlung bei Oropharynx- und Mundhöhlenkarzinomen - Klinische Ergebnisse an der Universität Würzburg aus den Jahren 1998 - 2010 T1 - Operation and adjuvante radiotherapy of oropharyngeal carcinomas - clinical results at the University of Wuerzburg between the years 1998-2010 N2 - Ergebnisse einer retrospektiven Studie an der Universität Würzburg: Patienten und Methoden: In einer retrospektiven Studie wurden Einflussfaktoren auf die Lokoregionäre Kontrolle, das Gesamtüberleben und das rezidivfreie Überleben von 106 Patienten, mit histologisch gesicherten Oropharynxkarzinomen (28 T1, 46 T2, 25 T3 und 7 T4 Tumore, mit lymphatischer Beteiligung in 78 Fällen), mit uni- und multivariaten Analysen untersucht. Das mediane Alter bei Primärdiagnose betrug 55 Jahre. Es wurde eine mediane Nachbeobachtungszeit 36 Monaten erreicht (zwischen 5 bis 126 Monate). In 18 Fällen (17%) konnte der Primärtumor in sano entfernt werden (Sicherheitsabstand > 3mm). In 34 Fällen (32%) bestand ein knapper Sicherheitsabstand (definitionsgemäß < als 3mm) und in 54 Fällen (51%) waren die Resektatränder nicht frei von Tumorzellen (R1 Resektion). Patienten, welche eine Chemotherapie aufgrund des erhöhten Rezidivrisikos erhielten, machten 24% (25 Patienten) des Patientenkollektivs aus. Behandlungskonzept Das Tumorbett des Primärtumors und die zervikalen lymphatischen Abflussgebiete erhielten mediane Bestrahlungsdosen von 56 Gy (2 Gy/ Behandlung, 5 Fraktionen pro Woche). Patienten mit R0-Resektion erhielten Bestrahlungsdosen von 56-60Gy. Bei Patienten mit knappen Resektatrand wurde das Tumorbett mit einer höheren Dosis von 60-66Gy bestrahlt, R1 Resektionen wurden mit einer Boost-Aufsättigung bis zu einer Gesamtdosis von 66-70 Gy behandelt. Patienten im UICC-Stadium 4, mit erhöhtem Rezidivrisiko, machten 24% (25 Patienten) des Patientenkollektivs aus. Diese Patienten erhielten je nach Nierenfunktion und Blutbild eine zusätzliche Chemotherapie mit Cisplatin (40mg/m² wöchentlich) in 1-4 Zyklen, sowie eine Boost-Aufsättigung des Tumorbettes bis zu einer Gesamtdosis von 66-70 Gy. Ergebnisse der univariaten Analysen mittels Kaplan-Maier Plot Verfahren: lokoregionäre Kontrolle Mit einer medianen Nachbeobachtungszeit von 36 Monaten wurde eine 5 Jahres Rezidivfreiheit bei 87% der Patienten erzielt. Davon wurden 80% der Rezidive innerhalb der ersten 24 Monate diagnostiziert. Bei Patienten mit R0 Status wurde in 16,7 % ein Rezidiv diagnostiziert, bei Patienten mit R1 Situation in 17% und bei Patienten mit knappen Resektatrand wurde nur in 6 % ein Rezidiv diagnostiziert. Als statistisch signifikanter Einflussfaktor des Rezidiv erwies sich nur das Gesamttumorvolumen. Gesamtüberlebensrate Es wurde eine 3- und 5- Jahresüberlebensrate von 75% und 66% erreicht. Die 5JÜR bezüglich der Radikalität der Resektion erreichte bei R0 Resektion 61%, 71% bei Patienten mit knappen Resektatrand und 65% bei R1 Situation. Bei Patienten mit einem T1 Tumorstadium ergab sich eine 5JÜR von 82%, bei T2 67%, bei T3 52% und für Patienten im T4 Stadium ergab sich eine 5JÜR von 43 %. Patienten mit N0-Status verzeichneten eine 5JÜR von 68%, mit N1-Status 82%, N2a,b-Status 68%, N2c-Status 36% und N3-Status ergab 43%. Patienten ohne adjuvante Chemotherapie erzielten eine 5JÜR von 69% und Patienten, die aufgrund des erhöhten Rezidivrisikos eine Chemotherapie erhielten, erreichten 56%. Die Einflussgröße der Rezidiventwicklung erbrachte eine 5JÜR von 13%, wogegen sie bei Patienten ohne Rezidiv 75% betrug. Patienten, welche einen 2. Tumor entwickelten, verzeichneten eine 5JÜR von 45% gegenüber 71% bei Patienten ohne 2.Tumor. Der Vergleich der Bestrahlungsdosen im Tumorbett ergab, dass Patienten mit einer Gesamtdosis unter/gleich 66Gy eine 5JÜR von 71% erreichten und 62% bei Gesamtdosen über 66Gy. Die 5JÜR bezüglich des Tumorvolumens des Primärtumors, inklusive der befallenen Lymphknoten, erbrachte in der ersten Gruppe von unter 10ml Tumorvolumen 77%, von 10 bis 20ml 83%, von 20 bis 50ml 52% und in der vierten Gruppe mit über 50ml Tumorvolumen 33%. Mit einem Grading von 2 wurde 69% und mit einem Grading von 3 wurde bei Patienten eine 5JÜR von 61% berechnet. In der univariaten Analyse mittels des Kaplan-Maier-Plot-Verfahrens, zeigte sich in der 5-Jahres Überlebenskurve eine Signifikanz der Einflussgrößen Tumorstadium (p-Wert 0,003), Rezidivereignis (p-Wert 0,000), 2.Tumor (p-Wert 0,001) und Tumorvolumen (p-Wert 0,000). Rezidivfreies Überleben Das rezidivfreie Überleben betrug nach 3 Jahren 68% und nach 5 Jahren 64%. Bezüglich der Radikalität der Resektion ermittelte man für Patienten mit R0 Resektion nach 5 Jahren ein rezidivfreies Überleben von 61%, 71% bei knappen Resektatrand und 61% bei R1 Situation. Patienten mit einem T1 Stadium erreichten ein 5 jähriges rezidivfreies Überleben in 82%, mit T2 Stadium 67%, mit T3 Stadium 48% und Patienten im T4 Tumorstadium erzielten 43 %. Patienten mit N0-Status verzeichneten ein 5 jähriges rezidivfreies Überleben von 64%, mit N1-Status 82%, N2a,b-Status 68%, N2c-Status 27% und ein N3-Status ergab 43%. Patienten ohne adjuvante Chemotherapie erreichten in 68% und Patienten, welche eine Chemotherapie erhielten, erreichten ein 5 jähriges rezidivfreies Überleben in 52%. Patienten, welche einen 2. Tumor entwickelten, verzeichneten eine 5 jähriges rezidivfreies Überleben von 45%, gegenüber 68% bei Patienten ohne 2.Tumor. Die Gegenüberstellung der Bestrahlungsdosen im Tumorbett ergab, dass Patienten mit einer Gesamtdosis unter/gleich 66Gy ein rezidivfreies 5-jähriges Überleben von 69% erreichten, hingegen Patienten mit mehr als 66Gy Bestrahlungsdosis 60% erzielten. Das 5 jährige rezidivfreie Überleben in Bezug auf das Tumorvolumen des Primärtumors, inklusive der befallenen Lymphknoten, erbrachte in der ersten Gruppe von unter 10ml Tumorvolumen 77%, von 10 bis 20ml 79%, in der dritten Gruppe von 20 bis 50ml 48% und in der vierten Gruppe mit über 50ml Tumorvolumen wurde nach 5 Jahren ein rezidivfreies Überleben von 33% verzeichnet. Mit einem Grading von 2, wurde 66% und mit einem Grading von 3 ergaben sich für die Patienten ein 5 jähriges rezidivfreies Überleben von 61%. In der univariaten Analyse mittels des Kaplan-Maier-Plot-Verfahren, zeigte sich in der Kurve für das 5-jährige rezidivfreie Überleben, eine Signifikanz der Einflussgrößen Tumorstadium (p-Wert 0,003), Lymphknotenstatus (p-Wert 0,048), Chemotherapie (p-Wert 0,047), 2.Tumor (p-Wert 0,003) und Tumorvolumen (p-Wert 0,000). Ergebnisse der multivarianten Analysen In einer multivariaten Cox-Regressions Analyse erwiesen sich die Einflussgrößen des Tumorstadiums und die Entwicklung eines 2. Tumors, bezüglich des Gesamt- und des rezidivfreien Überlebens, als statistisch signifikant. Das Tumorstadium konnte, in Bezug auf das Gesamtüberleben, eine Signifikanz von 0,015 ermittelt werden. Im Hinblick auf das rezidivfreie Überleben konnte ihm eine Signifikanz von 0,03 zugeschreiben werden. Die Einflussgröße des 2.Tumors ergab für das Gesamtüberleben eine Signifikanz von ebenfalls 0,015 und eine Signifikanz von 0,025 bezüglich des rezidivfreien Überlebens. Schlussfolgerung: Mit dem Therapiekonzept konnte eine Verbesserung der 5JÜR und des 5-jährigen rezidivfreien Überlebens erzielt werden. Die Patienten mit knappen Resektatrand wiesen durchweg bessere Ergebnisse auf als Patienten mit R0-Resektion. Als Konsequenz dieser Ergebnisse müsste man eine Angleichung des bisherigen Therapiekonzeptes der R0 Patienten an das der knapp resezierten Patienten vornehmen. Bei Patienten mit einem primär erhöhtem Rezidivrisiko, welche eine simultane Radiochemotherapie erhielten, erzielte man mit diesem Therapiekonzept eine Angleichung der 5JÜR an Patienten ohne dieses. Es zeigte sich hierbei in der multivariaten Analyse, sowohl beim Gesamtüberleben, als auch beim rezidivfreien Überleben kein statistisch signifikanter Unterschied (Gesamtüberleben p-Wert 0,064, rezidivfreies Überleben p-Wert 0,085). N2 - Results of a retrospective study at the University of Wuerzburg: Patients and methods: In a retrospective study factors of influence on the locoregional control, the overall survival and the disease free survival of 106 patients with hisological approved oropharyngeal cancer (28 T1, 46 T2, 25 T3 and 7 T4 tumors with lymphatic involment in 78 cases) were tested with uni and multivariant anyalysis. The mediane age at the date of the primar diagnose was 55 years. A mediane follow up surveillance of 36 months could be achived (between 5 to 126 months). In 18 cases (17%) the primary tumor could be removed in sano (safety margin >3mm). In 34 cases (32%) were detected close resection margins (<3mm) and in 54 cases the resection margins were not free of tumor cells (R1 resection). Patients, who were treated with a chemotherapy, because of the increased recurrency risk, were 24% of the patient database. The concept of medical treatment: The tumorbed of the primary tumor and the cervical lymphatic drain received a radiation dose of 56 Gy (2 Gy/ treatment, 5 fractions a week). Patients with R0 resections received doses from 56 to 60 Gy. Patients with close resections margins received a higher dose of 60 to 66 Gy at the tumorbed and patients with R1 resections were treated with a boost up to 66 to 70Gy. Patients with UICC 4 status with an increased recurrency risk received an additional chemotherapy with cisplatin (40mg/m² a week) in 1 to 4 cycles as well a boost of the tumorbed up to 66 to 70 Gy. Results of the univariant analyses with Kaplan-Maier Plot method: Locoregional control With a median follow up surveillance of 36 months a 5 year disease free survival of 87% was achieved. 80% of the recurrencies were detected within the first 24 months. Patients with R0 status had in 16,7%, patients with R1 status in 17% and patients with close resection margins had in only 6% the diagnose of a recurrence. The only factor of influence with statistical significance was the overall tumor volume. Overall survival A 3 and 5 year overall survival rate of 75% and 66% was achieved. The 5 year survival rate considering the radicality of the resection was 61% with R0 resection, 71% with close resection margins and 65% with R1 situation. Patients with T1 tumor status had a 5 year overall survival rate of 82%, 67% with T2, 52% with T3 and patients with T4 status hat a 5 year survival rate of 43%. Patients with N0 status achieved a 5 year overall survival of 68%, with N1 status 82%, N2a/b status 68%, N2c status and patients with N3 status achieved 43%. Patients without an adjuvative chemotherapy achieved a 5 year survival rate of 69% and patients, who received a chemotherapy because of the increase risk of recurrence achieved a 56% 5 year survival rate. Patients who developed a recurrence hat a 5 year survival rate of 13%, whereas the survival rate of patients without a recurrence was 75%. Patients who developed a second primary tumor had a 5 year survival rate of 45%, versus 71% without a second primary tumor. The comparison of the radiation dose in the tumorbed recorded, that patients with an overall radiation dose of 66Gy or less achieved a 5 year survival rate of 71% and patients with more than 66 Gy radiation dose achieved 62%. The 5 year overall survival considering the overall tumor volume recorded in the first group with less than 10ml 77%, in the second group with 10 to 20ml 83%, in the third group with 20 to 50ml 52% and in the forth group with more than 50ml tumor volume 33% 5 year survival rate. Patients with a grading of 2 had a 69% 5 years survival rate and patients with a grading of 3 had a 61% 5 years survival rate. The univariate analysis with the Kaplan-Maier Plot method detected following factors of influence of the 5 year overall survival: tumor status (p-value 0,003), tumor recurrence (p-value 0,000), a second tumor (p-value 0,001) and the overall tumor volume (p-value 0,000). Disease free survival The disease free survival was 68% after 3 years and 64% after 5 years. Regarding the radicality of the resection for patients with R0 resection was detected a 5 years disease free survival of 61%, 71% for patients with close resection margins and 61% with R1 resection. Patients with a T1 tumor status achieved a 5 years disease free survival rate of 82%, with a T2 status 67%, with a T3 status 48% and patients with a T4 status achieved 43%. Patients with N0 status had a 5 years disease free survival of 64%, with N1 status 82%, with N2a/b status 68%, with N2c status 27% and patients with N3 status 43%. Patients without a chemotherapy achieved 68% and patients who received a chemotherapy had a 5 years disease free survival of 52%. With the development of a second tumor, patients had a 5 years disease free survival of 45%, versus 68% survival rate without a second tumor. The comparison of the radiation dose in the tumorbed resulted, that patients with an overall radiation dose of 66 Gy or less had a 5 years survival rate of 69%, whereas patients with more than 66Gy radiation dose had 60%. The 5 years disease free survival regarding the overall tumor volume of the primar tumor achieved in the first group with less than 10ml tumor volume 77%, from 10 to 20ml 79%, in the third group from 20 to 50ml 48% and in the fourth group with more than 50ml a 5 years disease free survival of 33% could be detected. With a grading of 2 the 5 years disease free survival rate was 66% and with a grading of 3 patients achieved a 61% rate. In the univariate analysis with the Kaplan-Maier Plat method following factors of influence were detected: tumor status (p-value 0,003), lymph node status (p-value 0,048), chemotherapy (p-value 0,047), second tumor (p-value 0,003) and the overall tumor volume (p-value 0,000). Results of the multivariate analysis In the cox regression analysis the tumor status and the development of a second tumor were detected as factors of influence of the 5 year overall survival rate and the 5 year disease free survival survival rate. Regarding to the overall survival rate for the tumor status was detected a statistical significance of 0,015 and regarding the disease free survival was detected a significance of 0,025. The factor of influence of the second tumor had a significance for the overall survival of 0,015 and a significance regarding the disease free survival of 0,025. Conclusion: With the concept of medical treatment there could be achieved an improvement of the 5 year overall survival and the 5 year disease free survival. Patients with close resection margins had throughout better results as patients with a R0 resection. The consequence of those results should be an adjustment of the present concept of medical treatment of the R0 patients to the concept of patients with close resection margins. Patients who received a simultaneous radiochemotherapy, because of the increased risk of recurrence, the present concept of medical treatment effected an adjustment of the 5 year overall survival rate to patients without an increased risk of recurrence. There was no statistical significance in the multivariate analysis at the overall survival as well as at the disease free survival (overall survival p-value 0,064, disease free survival p-value 0,085). KW - Oropharynx-Karzinom KW - Überleben KW - Bestrahlung KW - Rezidiv KW - Überlebensrate KW - oropharyngeal cancer KW - Rezidivrate KW - radiotherapy KW - survival rate KW - recurrence Y1 - 2013 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-139429 ER -