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9 results on '"Martin Schuhmann"'

2. Natural and cryptic peptides dominate the immunopeptidome of atypical teratoid rhabdoid tumors

Author

Martin Ebinger, Hans-Georg Rammensee, Juliane S Walz, Ana Marcu, Andreas Schlosser, Torsten Pietsch, Martin Schuhmann, Anne Keupp, Nico Trautwein, Pascal Johann, Matthias Wölfl, Johanna Lager, Camelia Maria Monoranu, Lisa M Henkel, Ulrich Wilhelm Thomale, Erdwine Klinker, Paul G Schlegel, Florian Oyen, Yair Reisner, and Matthias Eyrich

Subjects
Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282
Published
2021
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3. COX2 expression is associated with proliferation and tumor extension in vestibular schwannoma but is not influenced by acetylsalicylic acid intake

Author

Felix Behling, Vanessa Ries, Marco Skardelly, Irina Gepfner-Tuma, Martin Schuhmann, Florian-Heinrich Ebner, Ghazaleh Tabatabai, Antje Bornemann, Jens Schittenhelm, and Marcos Tatagiba

Subjects
Cyclooxygenase 2, Acetylsalicylic acid, Aspirin, Vestibular schwannoma, Acoustic neuroma, Neurofibromatosis, Neurology. Diseases of the nervous system, RC346-429
Abstract

Abstract Acetylsalicylic acid has been linked to a lower risk for different cancer types, presumably through its inhibitory effect on cyclooxygenase 2. This has also been investigated in vestibular schwannomas with promising results suggesting an antiproliferative effect and recently the intake has been recommended for vestibular schwannomas as a conservative treatment option. We constructed tissue microarrays from paraffin-embedded tissue samples of 1048 vestibular schwannomas and analyzed the expression of cyclooxygenase 2 and the proliferation marker MIB1 (Molecular Immunology Borstel) via immunohistochemistry together with clinical data (age, gender, tumor extension, prior radiotherapy, neurofibromatosis type 2, tumor recurrence, cyclooxygenase 2 responsive medication). Univariate analysis showed that cyclooxygenase 2 expression was increased with age, female gender, prior radiotherapy and larger tumor extension. MIB1 expression was also associated with higher cyclooxygenase 2 expression. Schwannomas of neurofibromatosis type 2 patients had lower cyclooxygenase 2 levels. Use of acetylsalicylic acid, non-steroidal anti-inflammatory drugs, glucocorticoids or other immunosuppressants did not show differences in cyclooxygenase 2 or MIB1 expression. Instead, cyclooxygenase 2 expression increases with tumor extension while MIB1 expression is not associated with tumor size. Overall, cyclooxygenase 2 expression is associated with proliferation but not influenced by regular intake of acetylsalicylic acid or other cyclooxygenase 2-responsive medications. Acetylsalicylic acid intake does not alter cyclooxygenase 2 expression and has no antiproliferative effect in vestibular.

Published
2019
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4. Chronic Pleural Effusion in Ventriculoperitoneal Shunt due to Diaphragmatic CSF Fistula. Report of a case treated by Endoscopic Choroid Plexus Coagulation and literature review

Author

Simon Schmid, Andrea Bevot, Felix Neunhoeffer, Jörg Michel, Matthias Kumpf, Matthias Reimold, Michael Hofbeck, and Martin Schuhmann

Subjects
Pediatrics, Perinatology and Child Health, Surgery, Neurology (clinical), General Medicine
Abstract

Chronic pleural cerebrospinal fluid (CSF) effusion is a rare complication after ventriculoperitoneal (VP) shunt insertion and only 18 cases in children and adults have been described so far without catheter dislocation to the intrathoracic cavity. We report on a 4-year-old girl with a complex history of underlying neurogenetic disorder, a hypoxic ischemic encephalopathy after influenza A Infection with septic shock and severe acute respiratory distress syndrome, followed by meningitis at the age of 10 months. In consequence she developed a severe cerebral atrophy and postmeningitic hydrocephalus requiring placement of a VP shunt. At age 4 she was admitted with community acquired mycoplasma pneumonia and developed increasing pleural effusions leading to severe respiratory distress and requiring continuous chest tube drainage (up to 1000 -1400 ml/day), that could not be weaned. ß trace protein, in CSF present at concentrations > 6 mg/l, was found in the pleural fluid at low concentrations of 2.7 mg/l. An abdomino-thoracic CSF fistula was finally proven by single photon emission computerized tomography combined with low dose computer tomography. After shunt externalization, the pleural effusion stopped and the chest tube was removed. CSF production rate remain high above 500 ml/24h. An atrial CSF shunt could not be placed, since a hemodynamically relevant atrial septum defect with frail circulatory balance would not have tolerated the large CSF volumes. Therefore, she underwent a total bilateral endoscopic choroid plexus laser coagulation (CPC) within the lateral ventricles via bi-occipital burr holes. Postoperatively CSF production rate went close to 0 ml and after external ventricular drain removal no signs and symptoms of hydrocephalus developed during a follow-up of now 2.5 years. In summary, pleural effusions in patients with VP shunt can rarely be caused by an abdomino-thoracic fistula, with non-elevated ß trace protein in the pleural fluid. The majority of reported cases in literature were treated by ventriculo-atrial shunt. This is the 2nd reported case, which has been successfully treated by radical CPC alone including the temporal horn choroid plexus, making the child shunt independent.

Published
2023
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5. Rationale and design of the peripheral nerve tumor registry: an observational cohort study

Author

Nora F. Dengler, Christoph Scholz, Jürgen Beck, Anne-Kathrin Uerschels, Ullrich Sure, Christian Scheller, Christian Strauss, Daniel Martin, Gabriele Schackert, Christian Heinen, Johannes Woitzik, Anna Lawson McLean, Steffen K. Rosahl, Jonas Kolbenschlag, Johannes Heinzel, Martin Schuhmann, Marco Soares Tatagiba, Waltraud Kleist-Welch Guerra, Henry W. S. Schroeder, Ignazio Gaspare Vetrano, Rezvan Ahmadi, Andreas Unterberg, Jennifer Reinsch, Anna Zdunczyk, Meike Unteroberdoerster, Peter Vajkoczy, Sarah Wehner, Michael Becker, Cordula Matthies, Jose Pérez-Tejón, Annie Dubuisson, Damiano G. Barrone, Rikin Trivedi, Crescenzo Capone, Stefano Ferraresi, Jakob Kraschl, Thomas Kretschmer, Thomas Dombert, Frank Staub, Michael Ronellenfitsch, Gerhard Marquardt, Vincent Prinz, Marcus Czabanka, Anne Carolus, Veit Braun, Ralph König, Gregor Antoniadis, Christian Rainer Wirtz, Lukas Rasulic, and Maria Teresa Pedro

Subjects
Neurology, Medizin, Neurology (clinical), General Medicine
Abstract

Peripheral nerve tumors (PNT) are rare lesions. To date, no systematic multicenter studies on epidemiology, clinical symptoms, treatment strategies and outcomes, genetic and histopathologic features, as well as imaging characteristics of PNT were published. The main goal of our PNT Registry is the systematic multicenter investigation to improve our understanding of PNT and to assist future interventional studies in establishing hypotheses, determining potential endpoints, and assessing treatment efficacy.Aims of the PNT registry were set at the 2015 Meeting of the Section of Peripheral Nerve Surgery of the German Society of Neurosurgery. A study protocol was developed by specialists in PNT care. A minimal data set on clinical status, treatment types and outcomes is reported by each participating center at initial contact with the patient and after 1 year, 2 years, and 5 years. Since the study is coordinated by the Charité Berlin, the PNR Registry was approved by the Charité ethics committee (EA4/058/17) and registered with the German Trials Registry (www.drks.de). On a national level, patient inclusion began in June 2016. The registry was rolled out across Europe at the 2019 meeting of the European Association of Neurosurgery in Dublin.Patient recruitment has been initiated at 10 centers throughout Europe and 14 additional centers are currently applying for local ethics approval.To date, the PNT registry has grown into an international study group with regular scientific and clinical exchange awaiting the first results of the retrospective study arm.

Published
2022

6. ETMR-05: Single-cell transcriptomics of ETMR reveals developmental cellular programs and tumor-pericyte communications in the microenvironment [Abstract]

Author

Flavia W de Faria, Carolin Walter, Marta Interlandi, Viktoria Melcher, Nicole Riedel, Monika Graf, Natalia Moreno, Melanie Schoof, Dörthe Holdhof, Christian Thomas, Michael C Frühwald, Bruno Maerkl, Ben Ho, Sarah Sandmann, Julian Varghese, Martin Ebinger, Martin Schuhmann, Aysegül Canak, Annie Huang, Ulrich Schüller, Thomas K Albert, and Kornelius Kerl

Subjects
Cancer Research, Oncology, Neurology (clinical), ddc:610
Abstract

BACKGROUND: Embryonal tumors with multilayered rosettes (ETMR) are pediatric brain tumors bearing a grim prognosis, despite intensive multimodal therapeutic approaches. Insights into cellular heterogeneity and cellular communication of tumor cells with cells of the tumor microenvironment (TME), by applying single-cell (sc) techniques, potentially identify mechanisms of therapy resistance and target-directed treatment approaches. MATERIAL AND METHODS: To explore ETMR cell diversity, we used single-cell RNA sequencing (scRNA-seq) in human (n=2) and murine ETMR (transgenic mode; n=4) samples, spatial transcriptomics, 2D and 3D cultures (including co-cultures with TME cells), multiplex immunohistochemistry and drug screens. RESULTS: ETMR microenvironment is composed of tumor and non-tumor cell types. The ETMR malignant compartment harbour cells representing distinct transcriptional metaprograms, (NSC-like, NProg-like and Neuroblast-like), mirroring embryonic neurogenic cell states and fuelled by neurogenic pathways (WNT, SHH, Hippo). The ETMR TME is composed of oligodendrocyte and neuronal progenitor cells, neuroblasts, microglia, and pericytes. Tumor-specific ligand-receptor interaction analysis showed enrichment of intercellular communication between NProg-like ETMR cells and pericytes (PC). Functional network analyses reveal ETMR-PC interactions related to stem-cell signalling and extracellular matrix (ECM) organization, involving factors of the WNT, BMP, and CxCl12 networks. Results from ETMR-PC co-culture and spatial transcriptomics pointed to a pivotal role of pericytes in keeping ETMR in a germinal neurogenic state, enriched in stem-cell signalling. Drug screening considering cellular heterogeneity and cellular communication suggested novel therapeutic approaches. CONCLUSION: ETMR demonstrated diversity in the microenvironment, with enrichment of cell-cell communications with pericytes, supporting stem-cell signalling and interfering in the organization of the tumor extracellular matrix. Targeting ETMR-PC interactions might bring new opportunities for target-directed therapy.

Published
2022

7. Pediatric colloid cysts: a multinational, multicenter study. An IFNE-ISPN-ESPN collaboration

Author

Jonathan Roth, Yurii Perekopaiko, Danil A. Kozyrev, Shlomi Constantini, Hannah E. Myers, Benjamin L. Chern, Andrew Reisner, Jose Hinojosa Mena-Bernal, Andrea Bartoli, Luca Paun, Saqib Kamran Bakhshi, M Shahzad Shamim, Giuseppe Talamonti, R. Michael Scott, Nir Shimony, Ahmed El Damaty, Rodrigo Mierez, José Silva, Gustavo Sánchez, Andrea Di Rita, Lorenzo Genitori, Barbara Spacca, Yacine Felissi, Abdelhalim Morsli, Giselle Cardozo-Faust, Dhaval Shukla, Dwarakanath Srinivas, Kevin Jude Sudevan, Meriem Amarouche, J. André Grotenhuis, Hieronymus D. Boogaarts, Javier Márquez-Rivas, Mónica Rivero-Garvia, Philippe De Vloo, Frank Van Calenbergh, Henry W. S. Schroeder, Sascha Marx, Ehab El Refaee, Onur Ozgural, Eyüp Bayatli, Gökmen Kahiloğulları, Jayaratnam Jayamohan, Francesco T. Mangano, Jesse M. Skoch, Sudhakar Vadivelu, Charles B. Stevenson, Ricardo Brandao Fonseca, Igor Faquini, Mosaab Alsuwaihel, P. Daniel McNeely, Alexandre Varella Giannetti, Katalin Lorincz, Martin Schuhmann, Sandrine de-Ribaupierre, William C. Gump, Flavio Giordano, George I. Jallo, John Goodden, Ieva Sataite, Domenico Catapano, Ulrich-W. Thomale, Matthias Schulz, Luca Massimi, Gianpiero Tamburrini, Giuseppe Cinalli, Pietro Spennato, and Vincent Jecko

Subjects
colloid cyst, oncology, General Medicine, endoscopy, hydrocephalus
Abstract

OBJECTIVE Colloid cysts (CCs) are rare at all ages, and particularly among children. The current literature on pediatric CC is limited, and often included in mixed adult/pediatric series. The goal of this multinational, multicenter study was to combine forces among centers and investigate the clinical course of pediatric CCs. METHODS A multinational, multicenter retrospective study was performed to attain a large sample size, focusing on CC diagnosis in patients younger than 18 years of age. Collected data included clinical presentation, radiological characteristics, treatment, and outcome. RESULTS One hundred thirty-four children with CCs were included. Patient age at diagnosis ranged from 2.4 to 18 years (mean 12.8 ± 3.4 years, median 13.2 years, interquartile range 10.3–15.4 years; 22% were < 10 years of age). Twenty-two cases (16%) were diagnosed incidentally, including 48% of those younger than 10 years of age. Most of the other patients had symptoms related to increased intracranial pressure and hydrocephalus. The average follow-up duration for the entire group was 49.5 ± 45.8 months. Fifty-nine patients were initially followed, of whom 28 were eventually operated on at a mean of 19 ± 32 months later due to cyst growth, increasing hydrocephalus, and/or new symptoms. There was a clear correlation between larger cysts and symptomatology, acuteness of symptoms, hydrocephalus, and need for surgery. Older age was also associated with the need for surgery. One hundred three children (77%) underwent cyst resection, 60% using a purely endoscopic approach. There was 1 death related to acute hydrocephalus at presentation. Ten percent of operated patients had some form of complication, and 7.7% of operated cases required a shunt at some point during follow-up. Functional outcome was good; however, the need for immediate surgery was associated with educational limitations. Twenty operated cases (20%) experienced a recurrence of their CC at a mean of 38 ± 46 months after the primary surgery. The CC recurrence rate was 24% following endoscopic resection and 15% following open resections (p = 0.28). CONCLUSIONS CCs may present in all pediatric age groups, although most that are symptomatic present after the age of 10 years. Incidentally discovered cysts should be closely followed, as many may grow, leading to hydrocephalus and other new symptoms. Presentation of CC may be acute and may cause life-threatening conditions related to hydrocephalus, necessitating urgent treatment. The outcome of treated children with CCs is favorable.

Published
2022

8. LGG-51. Resection extent and BRAF V600E mutation status determine postoperative growth velocity in pediatric Low-grade glioma: Results from a single-center cohort analysis

Author

David Gorodezki, Jordana Sosa, Ursula Holzer, Manon Queudeville, Julian Zipfel, Andrea Bevot, Jens Schittenhelm, Thomas Nägele, Martin Ebinger, and Martin Schuhmann

Subjects
Cancer Research, Oncology, Neurology (clinical)
Abstract

Despite the favourable outcome and excellent long-term overall survival rates, pediatric LGG show vast variety of clinical behavior and limited predictability regarding progress or senescence. We comparatively analyzed the tumor growth velocity (TGV) of PLGG post subtotal resection (STR) to investigate the impact of surgery, histological subtype, tumor location and the most frequent BRAF aberrations (BRAF V600E mutation vs KIAA1549-BRAF fusion) on tumor growth rates, aiming to identify potential variables to prognosticate further progress or senescence. A total of 53 patients vs 94 patients in the pre- and postoperative cohort, respectively, could be observed over a mean follow-up time of 40.2 vs 60.1 months. Distribution of histopathological diagnosis and tumor sites showed similarity to previously published cohort studies. Comparative analysis of pre- and postoperative TGV showed a significant difference as mean preoperative TGV accounted for 0.264 cm³/mo, while postoperative TGV after 1st, 2nd and 3rd STR showed reduction to 0.085 cm³/mo, 0.024 cm³/mo and -0.016 cm³/mo, respectively (p < 0.001). Results remained significant after excluding patients who had obtained (neo)adjuvant treatment. Resection extent showed remarkable correlation with postoperative reduction of TGV (R = 0.97, P < 0.001). Comparison of postoperative TGV of BRAF V600E mutant LGG and BRAF wild-type LGG showed significant difference of means (0.123 cm³/mo and 0.016 cm³/mo, p = 0.47), consistent to previous analyses, suggesting BRAF V600E positive LGG as a high-risk subgroup. Histological type, tumor location and BRAF-KIAA1549 fusion showed no significant impact on postoperative TGV. The results suggest that surgery, beyond cytoreductive purpose, impacts PLGG kinetics post STR by inducing a significant deceleration of tumor growth. As postoperative growth velocity showed clear correlation to resection extent and residual tumor burden, surgery, as radical as possible while preserving neurological function, appears to remain the mainstay of therapy besides advancing therapeutic approaches.

Published
2022
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