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1. P04.05 Targeted Gene-Expression analysis during malignant transformation in primary and secondary malignant meningioma

Author

Maier, A D, primary, Meddis, A, additional, Haslund-Vinding, J, additional, Mirian, C, additional, Areskeviciute, A, additional, Nguyen, P, additional, Westergaard, C, additional, Melchior, L C, additional, Munch, T N, additional, Skjøth-Rasmussen, J, additional, Poulsgaard, L, additional, Ziebell, M, additional, Bartek Jr, J, additional, Broholm, H, additional, Poulsen, F R, additional, Gerds, T A, additional, Scheie, D, additional, and Mathiesen, T, additional

Published
2021
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3. TARGETED GENE-EXPRESSION ANALYSIS DURING MALIGNANT TRANSFORMATION IN PRIMARY AND SECONDARY MALIGNANT MENINGIOMA

Author

Maier, A. D., Meddis, A., Haslund-Vinding, J., Mirian, C., Areskeviciute, A., Nguyen, P., Westergaard, C., Melchior, L. C., Munch, T. N., Skjoth-Rasmussen, J., Poulsgaard, L., Ziebell, M., Bartek, J., Broholm, H., Poulsen, F. R., Gerds, T. A., Scheie, D., Mathiesen, T., Maier, A. D., Meddis, A., Haslund-Vinding, J., Mirian, C., Areskeviciute, A., Nguyen, P., Westergaard, C., Melchior, L. C., Munch, T. N., Skjoth-Rasmussen, J., Poulsgaard, L., Ziebell, M., Bartek, J., Broholm, H., Poulsen, F. R., Gerds, T. A., Scheie, D., and Mathiesen, T.

Published
2021

5. Multiple Extracranial Metastases from Primary Gliosarcoma in a Patient with Two Previous Different Primary Cancers

Author

Capion, T., Hauerberg, J., Broholm, H., and Muhic, A.

Subjects
Article Subject
Abstract

Gliosarcoma (GS) constitutes a minor fraction of primary glioblastoma (GBM), which is the most frequent malignant brain tumor in adults. Despite the fact that malignant gliomas are highly invasive, extracranial metastases are very rarely seen, and the mechanisms behind extracranial dissemination are still unclarified. We report a case of a 55-year-old male with a prior history of two distinct primary cancer types who, as a third independent type, developed GS with penetrating tumor growth to the skull and subcutaneous soft tissue via explosive spreading through a titanium net as well as extracranial metastases to the lumbar spine, paravertebral musculature, and most likely the right lung. The case illuminates the clinical challenge of diagnosing extracranial metastases from primary GBM and GS as these are still unexpected, especially in cases with possible competing diagnoses.

Published
2019
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11. P17.91 * CLINICAL VARIABLES SERVE AS PREDICTIVE FACTORS IN A MODEL FOR CLINICAL RESPONSE TO BEVACIZUMAB IN RECURRENT GLIOBLASTOMA MULTIFORME: AN OBSERVATIONAL STUDY OF A COHORT OF CONSECUTIVE NON-SELECTED PATIENTS FROM A SINGLE INSTITUTION

Author

Urup, T., primary, Grunnet, K., additional, Christensen, I. J., additional, Michaelsen, S. R., additional, Broholm, H., additional, Stockhausen, M. T., additional, Lassen, U., additional, and Poulsen, H. S., additional

Published
2014
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13. EGFR expression and glioblastoma outcome

Author

Sjöström, Sara, Ghasimi, Soma, Broholm, H., Brannstrom, Thomas, Johansen, C., Collatz-Laier, H., Henriksson, Roger, Andersson, Ulrika, Melin, Beatrice, Sjöström, Sara, Ghasimi, Soma, Broholm, H., Brannstrom, Thomas, Johansen, C., Collatz-Laier, H., Henriksson, Roger, Andersson, Ulrika, and Melin, Beatrice

Published
2012

14. Genetic variations in VEGF and VEGFR2 and glioblastoma outcome

Author

Sjöström, Sara, Wibom, Carl, Andersson, Ulrika, Brännstrom, Thomas, Broholm, H, Johansen, C, Collatz-Laier, H, Liu, Y, Bondy, M, Henriksson, Roger, Melin, Beatrice, Sjöström, Sara, Wibom, Carl, Andersson, Ulrika, Brännstrom, Thomas, Broholm, H, Johansen, C, Collatz-Laier, H, Liu, Y, Bondy, M, Henriksson, Roger, and Melin, Beatrice

Abstract

Vascular endothelial growth factor (VEGF) and its receptors (VEGFR) are central components in the development and progression of glioblastoma. To investigate if genetic variation in VEGF and VEGFR2 is associated with glioblastoma prognosis, we examined blood samples from 154 glioblastoma cases collected in Sweden and Denmark between 2000 and 2004. Seventeen tagging single nucleotide polymorphisms (SNPs) in VEGF and 27 in VEGFR2 were genotyped and analysed, covering 90% of the genetic variability within the genes. In VEGF, we found no SNPs associated with survival. In VEGFR2, we found two SNPs significantly associated to survival, namely rs2071559 and rs12502008. However, these results are likely to be false positives due to multiple testing and could not be confirmed in a separate dataset. Overall, this study provides little evidence that VEGF and VEGFR2 polymorphisms are important for glioblastoma survival.

Published
2011
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15. Genetic variations in VEGF and VEGFR2 and glioblastoma outcome

Author

Sjöström, S, Wibom, C, Andersson, U, Brännström, T, Broholm, H, Johansen, C, Laier, Helle Collatz, Liu, Y, Bondy, M, Henriksson, R, Nielsen, Bjørn Melin, Sjöström, S, Wibom, C, Andersson, U, Brännström, T, Broholm, H, Johansen, C, Laier, Helle Collatz, Liu, Y, Bondy, M, Henriksson, R, and Nielsen, Bjørn Melin

Abstract

Vascular endothelial growth factor (VEGF) and its receptors (VEGFR) are central components in the development and progression of glioblastoma. To investigate if genetic variation in VEGF and VEGFR2 is associated with glioblastoma prognosis, we examined blood samples from 154 glioblastoma cases collected in Sweden and Denmark between 2000 and 2004. Seventeen tagging single nucleotide polymorphisms (SNPs) in VEGF and 27 in VEGFR2 were genotyped and analysed, covering 90% of the genetic variability within the genes. In VEGF, we found no SNPs associated with survival. In VEGFR2, we found two SNPs significantly associated to survival, namely rs2071559 and rs12502008. However, these results are likely to be false positives due to multiple testing and could not be confirmed in a separate dataset. Overall, this study provides little evidence that VEGF and VEGFR2 polymorphisms are important for glioblastoma survival.

Published
2010

16. Myoepithelial carcinoma of the orbit: a clinicopathological and histopathological study

Author

Tran, Thuy Linh, Broholm, H, Daugaard, Søren, Fugelholm, K, Poulsgaard, Lars, Prause, Jan Ulrik, Kennedy, Susan M., Heegaard, Steffen, Tran, Thuy Linh, Broholm, H, Daugaard, Søren, Fugelholm, K, Poulsgaard, Lars, Prause, Jan Ulrik, Kennedy, Susan M., and Heegaard, Steffen

Abstract

Two cases of invasive myoepithelial carcinoma arising from the paranasal sinuses and invading the orbit are presented. Patient 1, a 53-year-old man, had a 3-month history of proptosis, pain and epiphora of the right eye. The second patient, a 24-year-old man, had for a week been complaining of protrusion of his left eye and of orbital pain. Computed tomography scan and magnetic resonance imaging revealed tumour masses in the frontal, ethmoidal and maxillary sinuses with invasion of the orbit and the frontal lobe. Biopsies from both cases showed spindle and epithelioid tumour cells. Mitotic figures were frequent. Immunohistochemical staining showed positive reaction for bcl-2, calponin, cytokeratins, CD99, S100, muscle-specific antigen, smooth muscle antigen and vimentin. The Ki-67 index was between 30-50% and 5-25%, respectively. Ultrastructurally, intermediate filaments, perinuclear tonofilaments and desmosomes were present. Based on these findings, a diagnosis of myoepithelial carcinoma of mixed cell type in both cases was evident. Both patients died shortly after the diagnosis was made even though both underwent radical surgery. Myoepithelial carcinoma of the paranasal sinuses is very rare and only six cases have been reported previously. We present the first two cases of myoepithelial carcinoma in the paranasal sinuses with invasion of the orbit. This is also the first report of myoepithelial carcinoma arising in the ethmoidal sinus.

Published
2010

17. MNS16A minisatellite genotypes in relation to risk of glioma and meningioma and to glioblastoma outcome

Author

Andersson, U., Osterman, P., Sjostrom, S., Johansen, C., Henriksson, R., Brannstrom, T., Broholm, H., Christensen, H.C., Ahlbom, A., Auvinen, A., Feychting, M., Lonn, S., Kiuru, A., Swerdlow, A., Schoemaker, M., Roos, G., Malmer, B., Andersson, U., Osterman, P., Sjostrom, S., Johansen, C., Henriksson, R., Brannstrom, T., Broholm, H., Christensen, H.C., Ahlbom, A., Auvinen, A., Feychting, M., Lonn, S., Kiuru, A., Swerdlow, A., Schoemaker, M., Roos, G., and Malmer, B.

Abstract

The human telomerase reverse transcriptase (hTERT) gene is upregulated in a majority of malignant tumours. A variable tandem repeat, MNS16A, has been reported to be of functional significance for hTERT expression. Published data on the clinical relevance of MNS16A variants in brain tumours have been contradictory. The present population-based study in the Nordic countries and the United Kingdom evaluated brain-tumour risk and survival in relation to MNS16A minisatellite variants in 648 glioma cases, 473 meningioma cases and 1,359 age, sex and geographically matched controls. By PCR-based genotyping all study subjects with fragments of 240 or 271 bp were judged as having short (S) alleles and subjects with 299 or 331 bp fragments as having long (L) alleles. Relative risk of glioma or meningioma was estimated with logistic regression adjusting for age, sex and country. Overall survival was analysed using Kaplan-Meier estimates and equality of survival distributions using the log-rank test and Cox proportional hazard ratios. The MNS16A genotype was not associated with risk of occurrence of glioma, glioblastoma (GBM) or meningioma. For GBM there were median survivals of 15.3, 11.0 and 10.7 months for the LL, LS and SS genotypes, respectively; the hazard ratio for having the LS genotype compared with the LL was significantly increased HR 2.44 (1.56-3.82) and having the SS genotype versus the LL was nonsignificantly increased HR 1.46 (0.81-2.61). When comparing the LL versus having one of the potentially functional variants LS and SS, the HR was 2.10 (1.41-3.1). However, functionality was not supported as there was no trend towards increasing HR with number of S alleles. Collected data from our and previous studies regarding both risk and survival for the MNS16A genotypes are contradictory and warrant further investigations Udgivelsesdato: 2009/8/15

Published
2009

18. Detecting chromosomal alterations at 1p and 19q by FISH and DNA fragment analysis - a comparative study in human gliomas

Author

Broholm, H., Born, P.W., Guterbaum, D., Dyrbye, H., Laursen, H., Broholm, H., Born, P.W., Guterbaum, D., Dyrbye, H., and Laursen, H.

Abstract

Histological classification of gliomas is important for treatment and as a prognostic predictor, but classification by histology alone can be a challenge. Molecular genetic investigations, in particular the combined loss of the short arm of chromosome 1 and the long arm of chromosome 19 (LOH1p/19q), has become a significant predictor of outcome in oligodendrogliomas. 1p/19q alterations can be investigated by fluorescence in situ hybridization (FISH), but controversies persist in the interpretation ofresults. Another technique is polymerase chain reaction (PCR) analysis using microsatellites as primers and capillary electrophoresis or southern blot as detection method. The objective of the present study was to compare the accuracy, reliability and feasibility of detecting chromosomal changes at 1p/19q with PCR microsatellite analysis and FISH in glial tumors in the clinical laboratory, where often only small formalin-fixed paraffin-embedded samples are available. Commercial DNA and normal cortex were used for comparison. The material comprised 41 glial tumors including 10 oligodendrogliomas (WHO Grades II and III, 5 each), 10 mixed oligoastrocytomas (WHO Grades II and III, 5 each), 10 astrocytomas (WHO Grades II and III, 5 each), and 11 glioblastomas (WHO Grade IV). Our data confirmed a correlation between FISH and LOH fragment analysis in classical oligodendrogliomas and in mixed oligoastrocytomas. Disparity was found among the glioblastomas, where fragment analysis showed 1p/19q loss in three cases, with no changes detected by FISH. The fragment analysis seems reliable and implementable for LOH 1p/19q investigation without patient-related control material Udgivelsesdato: 2008/11

Published
2008

20. MEDICAL RADIATION THERAPIES

Author

Ahmed, I., primary, Biswas, A., additional, Krishnamurthy, S., additional, Julka, P., additional, Rath, G., additional, Back, M., additional, Huang, D., additional, Gzell, C., additional, Chen, J., additional, Kastelan, M., additional, Gaur, P., additional, Wheeler, H., additional, Badiyan, S. N., additional, Robinson, C. G., additional, Simpson, J. R., additional, Tran, D. D., additional, Rich, K. M., additional, Dowling, J. L., additional, Chicoine, M. R., additional, Leuthardt, E. C., additional, Kim, A. H., additional, Huang, J., additional, Michaelsen, S. R., additional, Christensen, I. J., additional, Grunnet, K., additional, Stockhausen, M.-T., additional, Broholm, H., additional, Kosteljanetz, M., additional, Poulsen, H. S., additional, Tieu, M., additional, Lovblom, E., additional, Macnamara, M., additional, Mason, W., additional, Rodin, D., additional, Tai, E., additional, Ubhi, K., additional, Laperriere, N., additional, Millar, B.-A., additional, Menard, C., additional, Perkins, B., additional, Chung, C., additional, Clarke, J., additional, Molinaro, A., additional, Phillips, J., additional, Butowski, N., additional, Chang, S., additional, Perry, A., additional, Costello, J., additional, DeSilva, A., additional, Rabbitt, J., additional, Prados, M., additional, Cohen, A. L., additional, Anker, C., additional, Shrieve, D., additional, Hall, B., additional, Salzman, K., additional, Jensen, R., additional, Colman, H., additional, Farber, O., additional, Weinberg, U., additional, Palti, Y., additional, Fisher, B., additional, Chen, H., additional, Macdonald, D., additional, Lesser, G., additional, Coons, S., additional, Brachman, D., additional, Ryu, S., additional, Werner-Wasik, M., additional, Bahary, J.-P., additional, Chakravarti, A., additional, Mehta, M., additional, Gupta, T., additional, Nair, V., additional, Epari, S., additional, Godasastri, J., additional, Moiyadi, A., additional, Shetty, P., additional, Juvekar, S., additional, Jalali, R., additional, Herrlinger, U., additional, Schafer, N., additional, Steinbach, J., additional, Weyerbrock, A., additional, Hau, P., additional, Goldbrunner, R., additional, Kohnen, R., additional, Urbach, H., additional, Stummer, W., additional, Glas, M., additional, Houillier, C., additional, Ghesquieres, H., additional, Chabrot, C., additional, Soussain, C., additional, Ahle, G., additional, Choquet, S., additional, Faurie, P., additional, Bay, J.-O., additional, Vargaftig, J., additional, Gaultier, C., additional, Nicolas-Virelizier, E., additional, Hoang-Xuan, K., additional, Iskanderani, O., additional, Izar, F., additional, Benouaich-Amiel, A., additional, Filleron, T., additional, Moyal, E., additional, Iweha, C., additional, Jain, S., additional, Melian, E., additional, Sethi, A., additional, Albain, K., additional, Shafer, D., additional, Emami, B., additional, Kong, X.-T., additional, Green, S., additional, Filka, E., additional, Green, R., additional, Yong, W., additional, Nghiemphu, P., additional, Cloughesy, T., additional, Lai, A., additional, Mallick, S., additional, Roy, S., additional, Purkait, S., additional, Gupta, S., additional, Julka, P. K., additional, Rath, G. K., additional, Marosi, C., additional, Thaler, J., additional, Ay, C., additional, Kaider, A., additional, Reitter, E.-M., additional, Haselbock, J., additional, Preusser, M., additional, Flechl, B., additional, Zielinski, C., additional, Pabinger, I., additional, Miyatake, S.-I., additional, Furuse, M., additional, Miyata, T., additional, Yoritsune, E., additional, Kawabata, S., additional, Kuroiwa, T., additional, Muragaki, Y., additional, Maruyama, T., additional, Iseki, H., additional, Akimoto, J., additional, Ikuta, S., additional, Nitta, M., additional, Maebayashi, K., additional, Saito, T., additional, Okada, Y., additional, Kaneko, S., additional, Matsumura, A., additional, Karasawa, K., additional, Nakazato, Y., additional, Kayama, T., additional, Nabors, L. B., additional, Fink, K. L., additional, Mikkelsen, T., additional, Grujicic, D., additional, Tarnawski, R., additional, Nam, D.-H., additional, Mazurkiewicz, M., additional, Salacz, M., additional, Ashby, L., additional, Thurzo, L., additional, Zagonel, V., additional, Depenni, R., additional, Perry, J. R., additional, Henslee-Downey, J., additional, Picard, M., additional, Reardon, D. A., additional, Nambudiri, N., additional, Nayak, L., additional, LaFrankie, D., additional, Wen, P., additional, Ney, D., additional, Carlson, J., additional, Damek, D., additional, Blatchford, P., additional, Gaspar, L., additional, Kavanagh, B., additional, Waziri, A., additional, Lillehei, K., additional, Reddy, K., additional, Chen, C., additional, Rashed, I., additional, Barton, K., additional, Anderson, D., additional, Prabhu, V., additional, Rusch, R., additional, Belongia, M., additional, Maheshwari, M., additional, Firat, S., additional, Schiff, D., additional, Desjardins, A., additional, Glantz, M., additional, Chamberlain, M., additional, Shapiro, W., additional, Gopal, S., additional, Judy, K., additional, Patel, S., additional, Mahapatra, A., additional, Shan, J., additional, Gupta, D., additional, Shih, K., additional, Bacha, J. A., additional, Brown, D., additional, Garner, W. J., additional, Steino, A., additional, Schwart, R., additional, Kanekal, S., additional, Li, M., additional, Lopez, L., additional, Burris, H. A., additional, Soderberg-Naucler, C., additional, Rahbar, A., additional, Stragliotto, G., additional, Song, A. J., additional, Kumar, A. M. S., additional, Murphy, E. S., additional, Tekautz, T., additional, Suh, J. H., additional, Recinos, V., additional, Chao, S. T., additional, Spoor, J., additional, Korami, K., additional, Kloezeman, J., additional, Balvers, R., additional, Dirven, C., additional, Lamfers, M., additional, Leenstra, S., additional, Sumrall, A., additional, Haggstrom, D., additional, Crimaldi, A., additional, Symanowski, J., additional, Giglio, P., additional, Asher, A., additional, Burri, S., additional, Sunkersett, G., additional, Khatib, Z., additional, Prajapati, C. M., additional, Magalona, E. E., additional, Mariano, M., additional, Sih, I. M., additional, Torcuator, R., additional, Taal, W., additional, Oosterkamp, H., additional, Walenkamp, A., additional, Beerenpoot, L., additional, Hanse, M., additional, Buter, J., additional, Honkoop, A., additional, Boerman, D., additional, de Vos, F., additional, Jansen, R., additional, van der Berkmortel, F., additional, Brandsma, D., additional, Enting, R., additional, Kros, J., additional, Bromberg, J., additional, van Heuvel, I., additional, Smits, M., additional, van der Holt, R., additional, Vernhout, R., additional, van den Bent, M., additional, Wick, W., additional, Suarez, C., additional, Rodon, J., additional, Forsyth, P., additional, Gueorguieva, I., additional, Cleverly, A., additional, Burkholder, T., additional, Desaiah, D., additional, Lahn, M., additional, Zach, L., additional, Guez, D., additional, Last, D., additional, Daniels, D., additional, Nissim, O., additional, Grober, Y., additional, Hoffmann, C., additional, Nass, D., additional, Talianski, A., additional, Spiegelmann, R., additional, Cohen, Z., additional, and Mardor, Y., additional

Published
2013
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21. Endocannabinoid metabolism in human glioblastomas and meningiomas compared to human non-tumour brain tissue

Author

Petersen, G., Moesgaard, B., Hansen, Harald S., Schmid, P.C., Schmid, H.H.O., Broholm, H., Kosteljanetz, M., Petersen, G., Moesgaard, B., Hansen, Harald S., Schmid, P.C., Schmid, H.H.O., Broholm, H., and Kosteljanetz, M.

Abstract

The endogenous levels of the two cannabinoid receptor ligands 2-arachidonoyl glycerol and anandamide, and their respective congeners, monoacyl glycerols and N-acylethanolamines, as well as the phospholipid precursors of N-acylethanolamines, were measured by gas chromatography-mass spectrometry in glioblastoma (WHO grade IV) tissue and meningioma (WHO grade I) tissue and compared with human non-tumour brain tissue. Furthermore, the metabolic turnover of N-acylethanolamines was compared by measurements of the enzymatic activity of N-acyltransferase, N-acylphosphatidylethanolamine-hydrolysing phospholipase D and fatty acid amide hydrolase in the same three types of tissue. Glioblastomas were characterized by enhanced levels of N-acylethanolamines (eightfold, 128 ± 59 pmol/µmol lipid phosphorus) including anandamide (17-fold, 4.6 ± 3.1 pmol/µmol lipid phosphorus) and several species of N-acylphosphatidylethanolamines (three to eightfold). This was accompanied by a more than 60% reduction in the enzyme activities of N- acylphosphatidylethanolamine-hydrolysing phospholipase D and fatty acid amide hydrolase. By contrast, meningiomas were characterized by a massively enhanced level of 2-monoacyl glycerols (20-fold, 2293 ± 361 pmol/µmol lipid phosphorus) including 2-arachidonoyl glycerol (20-fold, 1524 ± 361 pmol/µmol lipid phosphorus). This was accompanied by an enhanced in vitro conversion of phosphatidylcholine to monoacyl glycerol (fivefold). The enhanced level of the 2-arachidonoyl glycerol, anandamide and other N-acylethanolamines detected in the two types of tumour tissue may possibly act as endogenous anti-tumour mediators by stimulation of both cannabinoid and non-cannabinoid receptor-mediated mechanisms.

Published
2005

24. Risk factors for oligodendroglial tumors: A pooled international study

Author

McCarthy, B. J., primary, Rankin, K. M., additional, Aldape, K., additional, Bondy, M. L., additional, Brannstrom, T., additional, Broholm, H., additional, Feychting, M., additional, Il'yasova, D., additional, Inskip, P. D., additional, Johansen, C., additional, Melin, B. S., additional, Ruder, A. M., additional, Butler, M. A., additional, Scheurer, M. E., additional, Schuz, J., additional, Schwartzbaum, J. A., additional, Wrensch, M. R., additional, and Davis, F. G., additional

Published
2010
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26. Nitric oxide synthase activity in human pituitary adenomas

Author

Kruse, Anders, Broholm, H., Rubin, I., Schmidt, K., Lauritzen, M., Kruse, Anders, Broholm, H., Rubin, I., Schmidt, K., and Lauritzen, M.

Abstract

Objectives - The purpose of the present study was to examine human pituitary adenomas for nitric oxide synthase (NOS) activity by immunohistochemical and enzymatic methods. Materials and methods - Adenomatous tissue from 16 patients were obtained during operation and stained immunohistochemically for hormone production and for the three NOS isoenzymes. Cell types that expressed NOS immunoreactivity (IR) were identified, and the NOS isoform was noted. NOS activity was measured enzymatically by the conversion of L-arginine to L-citrulline in tissue samples. Results - Endothelial cells of pituitary adenomas showed increase of eNOS IR compared with control tissue. The nNOS and iNOS IR were the same in adenomas and controls. There was no correlation between NOS IR and NOS activity measured enzymatically and the endocrine activity of the tumour or other clinical variables. Conclusion - The observation of increased eNOS IR in endothelial cells of adenomas may suggest that NO plays a role in the regulation of blood flow in pituitary adenomas.

Published
2002

27. Nitric oxide synthase expression of oligodendrogliomas

Author

Broholm, H., Brændstrup, O., Lauritzen, M., Broholm, H., Brændstrup, O., and Lauritzen, M.

Abstract

In the central nervous system, nitric oxide (NO) has a variety of biological functions including vasorelaxation and neurotransmission. The synthesis of NO is catalyzed by NO synthases (NOS) existing in 3 isoforms, neuronal NOS (nNOS), inducible NOS (iNOS) and endothelial NOS (eNOS). NO synthase has implications in the pathophysiology of primary glial brain tumors with enhanced expression of nNOS and eNOS in high-grade astrocytic tumors, WHO grades III and IV. Only minor groups of pure oligodendrogliomas have been investigated. The aim of the investigation was to study the expression of the 3 NOS isoforms in this genetically divergent group of primary gliomas and to correlate the findings with tumor grade and expression pattern for the major group of gliomas - the astrocytomas. We examined the NOS expression in 35 oligodendrogliomas, WHO grade II, and 7 anaplastic oligodendrogliomas, WHO grade III, by immunohistochemical methods using formalin-fixed paraffin-embedded material. We observed only a minor expression of nNOS and sparse expression of eNOS in the tumor cells, but a vivid expression of eNOS in the vascular endothelial cells in both the tumor and the surrounding tissue. The rich expression of eNOS in oligodendroglioma vessels independent of tumor grade may suggest that blood flow and angiogenesis in these richly vascularized tumors are modified by NO. Interestingly, enhanced expression of inducible NOS was observed in the oligodendroglial tumor cells in 19 of 35 oligodendrogliomas (54%) and in 2 of 7 anaplastic oligodendrogliomas (29%). This is diverging for iNOS expression in astroglial tumors and the data could be indicative of iNOS exerting anti-tumor activity which may protract the progression from low-grade oligodendrogliomas to more anaplastic types.

Published
2001

32. [Ingen Titel]

Author

C. Broholm, H. and C. Broholm, H.

Published
1944

33. Molecular Characterization of the Danish Prion Diseases Cohort With Special Emphasis on Rare and Unique Cases

Author

Piero Parchi, Helle Broholm, Linea Cecilie Melchior, Sabina Capellari, Aušrinė Areškevičiūtė, Eva Løbner Lund, David Scheie, Anna Bartoletti-Stella, Areskeviciute A., Broholm H., Melchior L.C., Bartoletti-Stella A., Parchi P., Capellari S., Scheie D., and Lund E.L.

Subjects
Male, Denmark, animal diseases, Genetic counseling, Population, Classification of prion disease, Disease, Neuropathology, Octapeptide repeat insertion, White matter Kuru plaques, Creutzfeldt-Jakob Syndrome, Prion Diseases, Pathology and Forensic Medicine, Cohort Studies, 03 medical and health sciences, Cellular and Molecular Neuroscience, 0302 clinical medicine, Humans, Medicine, education, Aged, 030304 developmental biology, Aged, 80 and over, Genetics, 0303 health sciences, education.field_of_study, business.industry, Point mutation, Sporadic fatal insomnia, Prion protein gene, Brain, General Medicine, Middle Aged, medicine.disease, White Matter, Molecular characterization, nervous system diseases, Neurology, Cohort, Prion, Kuru, Female, Neurology (clinical), business, 030217 neurology & neurosurgery, Cohort study
Abstract

The purpose of this study was to perform an updated reclassification of all definite prion disease cases with available fresh-frozen samples referred to the Danish Reference Center over the past 40 years, putting a special emphasis on the molecular characterization of novel disease subtypes. Investigation of the Danish prion diseases cohort revealed rare sporadic Creutzfeldt-Jakob disease cases with mixed subtypes and subtypes with previously uncharacterized white matter plaques, a new case of sporadic fatal insomnia, and 3 novel mutations, including 2 large octapeptide repeat insertions, and a point mutation in the prion protein gene. The evaluation of methionine and valine distribution at codon 129 among the prion disease patients in the cohort revealed the increased prevalence of methionine homozygotes compared to the general population. This observation was in line with the prevalence reported in other Caucasian prion disease cohort studies. Reclassification of the old prion diseases cohort revealed unique cases, the molecular characterization of which improves prion diseases classification, diagnostic accuracy, genetic counseling of affected families, and the understanding of disease biology.

Published
2019

34. A Novel Eight Octapeptide Repeat Insertion in PRNP Causing Prion Disease in a Danish Family

Author

Linea Melchior, Peter Høgh, Piero Parchi, David Scheie, Eva Løbner Lund, Helle Broholm, Aušrinė Areškevičiūtė, Anna Bartoletti-Stella, Sabina Capellari, Pia Rude Nielsen, Areskeviciute A., Hogh P., Bartoletti-Stella A., Melchior L.C., Nielsen P.R., Parchi P., Capellari S., Broholm H., Scheie D., and Lund E.L.

Subjects
Adult, Male, Heterozygote, Prions, Disease, Biology, medicine.disease_cause, Prion Proteins, Lipofuscin, Prion Diseases, Pathology and Forensic Medicine, PRNP, 03 medical and health sciences, Cellular and Molecular Neuroscience, 0302 clinical medicine, medicine, Humans, Dementia, Family, Age of Onset, Allele, Gene, Alleles, Exome sequencing, Genetics, Mutation, Movement Disorders, Mental Disorders, Prion protein gene, General Medicine, Middle Aged, medicine.disease, Phenotype, Pedigree, Eight-octapeptide repeat insertion mutation, Neurology, Inherited prion disease, Early-onset dementia, Disease Progression, Female, Neurology (clinical), 030217 neurology & neurosurgery, Microsatellite Repeats
Abstract

Octapeptide repeat insertions (OPRI) found in the prion protein gene (PRNP) constitute a subgroup of pathogenic mutations linked to inherited prion diseases, a hallmark of which is a misfolded prion protein. The number of repeats in OPRI has been associated with different disease phenotypes. However, due to the rarity of the cases and heterogenous disease manifestations, the recognition and classification of these variants has been difficult. Here, we report the first Danish family, the fifth worldwide, carrying a novel 8-OPRI with a unique sequence of the additional 8 inserts: R1-R2-R2-R3-R2-R2-R2a-R2-R3g-R2-R2-R3-R4. The mutation was found on the allele coding for methionine at codon 129 in the PRNP gene. The clinical exome sequencing revealed that no other dementia-associated genes harbored pathogenic alterations. Mutation carriers had onset of symptoms in their early thirties, but disease duration varied from 5 to 11 years. Progressive dementia with psychiatric and motor symptoms were the most prominent clinical features. Clinical, pathological, and genetic characteristics of other 4 reported families with 8-OPRI were reviewed and compared with the findings in the Danish family.

Published
2019

35. The Glioma International Case-Control Study: A Report From the Genetic Epidemiology of Glioma International Consortium

Author

Jill S. Barnholtz-Sloan, Francis Ali-Osman, Elizabeth B. Claus, Daniel H. Lachance, Renke Zhou, Margaret Wrensch, Ching C. Lau, Sanjay Shete, Irina Alafuzoff, Christopher I. Amos, Melissa L. Bondy, Kenneth Aldape, Tarik Tihan, Robert B. Jenkins, Richard S. Houlston, Michael E. Scheurer, Rose Lai, Christoffer Johansen, Faith G. Davis, Peter Collins, Jonine L. Bernstein, Beatrice Melin, E. Susan Amirian, Joellen M. Schildkraut, Helle Broholm, Ryan Merrell, Georgina Armstrong, Siegal Sadetzki, Marc K. Rosenblum, Thomas Brännström, Caterina Giannini, Sara H. Olson, Dora Il'yasova, Amirian E.S., Armstrong G.N., Zhou R., Lau C.C., Claus E.B., Barnholtz-Sloan J.S., Il'Yasova D., Schildkraut J., Ali-Osman F., Sadetzki S., Johansen C., Houlston R.S., Jenkins R.B., Lachance D., Olson S.H., Bernstein J.L., Merrell R.T., Wrensch M.R., Davis F.G., Lai R., Shete S., Amos C.I., Scheurer M.E., Aldape K., Alafuzoff I., Brannstrom T., Broholm H., Collins P., Giannini C., Rosenblum M., Tihan T., Melin B.S., and Bondy M.L.

Subjects
Oncology, Male, Epidemiology, Practice of Epidemiology, International Cooperation, Biospecimen Collection, Medical and Health Sciences, Mathematical Sciences, Brain cancer, Retrospective Studie, Risk Factors, glioma, 80 and over, Medicine, Aged, 80 and over, Molecular Epidemiology, Incidence, methodology, Glioma, Middle Aged, Multiple data, Female, Case-Control Studie, Human, Adult, medicine.medical_specialty, Adolescent, Young Adult, Rare Diseases, Clinical Research, Internal medicine, Genetics, cancer, Humans, Genetic Predisposition to Disease, Retrospective Studies, Aged, business.industry, Risk Factor, case-control studies, Human Genome, Case-control study, glioblastoma, Neurosciences, Small sample, medicine.disease, Brain Disorders, Brain Cancer, study profile, Genetic epidemiology, Immunology, Gene-Environment Interaction, business, Glioblastoma
Abstract

Decades of research have established only a few etiological factors for glioma, which is a rare and highly fatal brain cancer. Common methodological challenges among glioma studies include small sample sizes, heterogeneity of tumor subtypes, and retrospective exposure assessment. Here, we briefly describe the Glioma International Case-Control (GICC) Study (recruitment, 2010-2013), a study being conducted by the Genetic Epidemiology of Glioma International Consortium that integrates data from multiple data collection sites, uses a common protocol and questionnaire, and includes biospecimen collection. To our knowledge, the GICC Study is the largest glioma study to date that includes collection of blood samples, which will allow for genetic analysis and interrogation of gene-environment interactions.

Published
2015

36. Human cytomegalovirus hijacks host stress response fueling replication stress and genome instability.

Author

Merchut-Maya JM, Bartek J Jr, Bartkova J, Galanos P, Pantalone MR, Lee M, Cui HL, Shilling PJ, Brøchner CB, Broholm H, Maya-Mendoza A, Söderberg-Naucler C, and Bartek J

Subjects
Carcinogenesis genetics, Genomic Instability, Humans, Promoter Regions, Genetic, Virus Replication, Cytomegalovirus genetics, Cytomegalovirus metabolism, DNA Damage
Abstract

Viral infections enhance cancer risk and threaten host genome integrity. Although human cytomegalovirus (HCMV) proteins have been detected in a wide spectrum of human malignancies and HCMV infections have been implicated in tumorigenesis, the underlying mechanisms remain poorly understood. Here, we employed a range of experimental approaches, including single-molecule DNA fiber analysis, and showed that infection by any of the four commonly used HCMV strains: AD169, Towne, TB40E or VR1814 induced replication stress (RS), as documented by host-cell replication fork asymmetry and formation of 53BP1 foci. The HCMV-evoked RS triggered an ensuing host DNA damage response (DDR) and chromosomal instability in both permissive and non-permissive human cells, the latter being particularly relevant in the context of tumorigenesis, as such cells can survive and proliferate after HCMV infection. The viral major immediate early enhancer and promoter (MIEP) that controls expression of the viral genes IE72 (IE-1) and IE86 (IE-2), contains transcription-factor binding sites shared by promoters of cellular stress-response genes. We found that DNA damaging insults, including those relevant for cancer therapy, enhanced IE72/86 expression. Thus, MIEP has been evolutionary shaped to exploit host DDR. Ectopically expressed IE72 and IE86 also induced RS and increased genomic instability. Of clinical relevance, we show that undergoing standard-of-care genotoxic radio-chemotherapy in patients with HCMV-positive glioblastomas correlated with elevated HCMV protein markers after tumor recurrence. Collectively, these results are consistent with our proposed concept of HCMV hijacking transcription-factor binding sites shared with host stress-response genes. We present a model to explain the potential oncomodulatory effects of HCMV infections through enhanced replication stress, subverted DNA damage response and induced genomic instability., (© 2022. The Author(s), under exclusive licence to ADMC Associazione Differenziamento e Morte Cellulare.)

Published
2022
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37. Diagnostic accuracy and clinical impact of [18F]FET PET in childhood CNS tumors.

Author

Marner L, Lundemann M, Sehested A, Nysom K, Borgwardt L, Mathiasen R, Wehner PS, Henriksen OM, Thomsen C, Skjøth-Rasmussen J, Broholm H, Østrup O, Forman JL, Højgaard L, and Law I

Subjects
Adult, Child, Humans, Magnetic Resonance Imaging, Positron-Emission Tomography, Radiopharmaceuticals, Tyrosine, Brain Neoplasms, Glioma
Abstract

Background: Central nervous system (CNS) tumors cause the highest death rates among childhood cancers, and survivors frequently have severe late effects. Magnetic resonance imaging (MRI) is the imaging modality of choice, but its specificity can be challenged by treatment-induced signal changes. In adults, O-(2-[18F]fluoroethyl)-l-tyrosine ([18F]FET) PET can assist in interpreting MRI findings. We assessed the clinical impact and diagnostic accuracy of adding [18F]FET PET to MRI in children with CNS tumors., Methods: A total of 169 [18F]FET PET scans were performed in 97 prospectively and consecutively included patients with known or suspected childhood CNS tumors. Scans were performed at primary diagnosis, before or after treatment, or at relapse., Results: Adding [18F]FET PET to MRI impacted clinical management in 8% [95% confidence interval (CI): 4%-13%] of all scans (n = 151) and in 33% [CI: 17%-53%] of scans deemed clinically indicated due to difficult decision making on MRI alone (n = 30). Using pathology or follow-up as reference standard, the addition of [18F]FET PET increased specificity (1.00 [0.82-1.00] vs 0.48 [0.30-0.70], P = .0001) and accuracy (0.91 [CI: 0.87-0.96] vs 0.81 [CI: 0.75-0.89], P = .04) in 83 treated lesions and accuracy in 58 untreated lesions (0.96 [CI: 0.91-1.00] vs 0.90 [CI: 0.82-0.92], P < .001). Further, in a subset of patients (n = 15) [18F]FET uptake correlated positively with genomic proliferation index., Conclusions: The addition of [18F]FET PET to MRI helped discriminate tumor from non-tumor lesions in the largest consecutive cohort of pediatric CNS tumor patients presented to date., (© The Author(s) 2021. Published by Oxford University Press on behalf of the Society for Neuro-Oncology. All rights reserved. For permissions, please e-mail: journals.permissions@oup.com.)

Published
2021
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38. The exon-junction complex helicase eIF4A3 controls cell fate via coordinated regulation of ribosome biogenesis and translational output.

Author

Kanellis DC, Espinoza JA, Zisi A, Sakkas E, Bartkova J, Katsori AM, Boström J, Dyrskjøt L, Broholm H, Altun M, Elsässer SJ, Lindström MS, and Bartek J

Subjects
Animals, DNA Helicases metabolism, Eukaryotic Initiation Factor-4A genetics, Eukaryotic Initiation Factor-4A metabolism, Exons genetics, Mice, Ribosomes genetics, Ribosomes metabolism, DEAD-box RNA Helicases genetics, DEAD-box RNA Helicases metabolism, Tumor Suppressor Protein p53 genetics
Abstract

Eukaryotic initiation factor 4A-III (eIF4A3), a core helicase component of the exon junction complex, is essential for splicing, mRNA trafficking, and nonsense-mediated decay processes emerging as targets in cancer therapy. Here, we unravel eIF4A3's tumor-promoting function by demonstrating its role in ribosome biogenesis (RiBi) and p53 (de)regulation. Mechanistically, eIF4A3 resides in nucleoli within the small subunit processome and regulates rRNA processing via R-loop clearance. EIF4A3 depletion induces cell cycle arrest through impaired RiBi checkpoint-mediated p53 induction and reprogrammed translation of cell cycle regulators. Multilevel omics analysis following eIF4A3 depletion pinpoints pathways of cell death regulation and translation of alternative mouse double minute homolog 2 ( MDM2 ) transcript isoforms that control p53. EIF4A3 expression and subnuclear localization among clinical cancer specimens correlate with the RiBi status rendering eIF4A3 an exploitable vulnerability in high-RiBi tumors. We propose a concept of eIF4A3's unexpected role in RiBi, with implications for cancer pathogenesis and treatment., (Copyright © 2021 The Authors, some rights reserved; exclusive licensee American Association for the Advancement of Science. No claim to original U.S. Government Works. Distributed under a Creative Commons Attribution NonCommercial License 4.0 (CC BY-NC).)

Published
2021
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39. Pathologic Characteristics of Pregnancy-Related Meningiomas.

Author

Giraldi L, Lauridsen EK, Maier AD, Hansen JV, Broholm H, Fugleholm K, Scheie D, and Munch TN

Abstract

Meningiomas are the most common intracranial tumor. During pregnancy, explosive growth of a known meningioma occasionally occurs, but the underlying reasons remain unknown. Prolactin has been suggested as a possible key contributor to pregnancy-related meningioma growth. This study sets out to investigate prolactin and prolactin receptor status in 29 patients with pregnancy-related meningiomas in Denmark, from January 1972 to December 2016, as compared to 68 controls aged 20-45 years, also undergoing resection of a meningioma. Furthermore, we investigated potential differences in the progesterone and estrogen receptor statuses, WHO grade, Ki-67 labeling indices, and locations of the resected meningiomas between the cases and controls. Immunohistochemical analyses were performed, and histopathology and intracranial location were assessed with the investigator blinded for the case-control status. None of the samples stained positive for prolactin and very few samples stained positive for prolactin receptors, equally distributed among cases and controls. Estrogen and progesterone receptors generally followed the same distributional pattern between groups, whereas above cut-point Ki-67 labeling indices for both groups were observed. In conclusion, our results did not support the notion of prolactin as a key contributor to pregnancy-related meningioma growth. Rather, the similarities between the cases and controls suggest that meningiomas early in life may comprise a distinct biological entity.

Published
2021
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40. Somatostatin Receptor-Targeted Radiopeptide Therapy in Treatment-Refractory Meningioma: Individual Patient Data Meta-analysis.

Author

Mirian C, Duun-Henriksen AK, Maier A, Pedersen MM, Jensen LR, Bashir A, Graillon T, Hrachova M, Bota D, van Essen M, Spanjol P, Kreis C, Law I, Broholm H, Poulsgaard L, Fugleholm K, Ziebell M, Munch T, Walter MA, and Mathiesen T

Subjects
Disease-Free Survival, Humans, Meningeal Neoplasms metabolism, Meningioma metabolism, Meningeal Neoplasms radiotherapy, Meningioma radiotherapy, Receptors, Somatostatin metabolism, Treatment Failure
Abstract

Somatostatin receptor (SSTR)-targeted peptide receptor radionuclide therapy (PRRT) represents a promising approach for treatment-refractory meningiomas. Methods: We performed an individual patient data meta-analysis, including all published data on meningioma patients treated with SSTR-targeted PRRT. The main outcomes were toxicity, response to treatment, progression-free survival (PFS), and overall survival (OS). We applied the Kaplan-Meier method to estimate survival probabilities and report incidence rates per 100 person-years. We applied Cox proportional hazards models to determine the effect of covariates. Results: We screened 537 papers and identified 6 eligible cohort studies. We included a total of 111 patients who had treatment-refractory meningioma and received SSTR-targeted PRRT. Disease control was achieved in 63% of patients. The 6-mo PFS rates were 94%, 48%, and 0% for World Health Organization grades I, II, and III, respectively. The risk of disease progression decreased by 13% per 1,000-MBq increase in the total applied activity. The 1-y OS rates were 88%, 71%, and 52% for World Health Organization grades I, II, and III, respectively. The risk of death decreased by 17% per 1,000-MBq increase in the total applied activity. The main side effects comprised transient hematotoxicity, such as anemia in 22% of patients, leukopenia in 13%, lymphocytopenia in 24%, and thrombocytopenia in 17%. Conclusion: To our knowledge, this individual patient data meta-analysis represents the most comprehensive analysis of the benefits of and adverse events associated with SSTR-targeted PRRT for treatment-refractory meningioma. The treatment was well tolerated, achieved disease control in most cases, and showed promising results regarding PFS and OS., (© 2021 by the Society of Nuclear Medicine and Molecular Imaging.)

Published
2021
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41. Distinct circular RNA expression profiles in pediatric ependymomas.

Author

Ahmadov U, Bendikas MM, Ebbesen KK, Sehested AM, Kjems J, Broholm H, and Kristensen LS

Subjects
Adolescent, Child, Child, Preschool, Female, High-Throughput Nucleotide Sequencing, Humans, Infant, Male, RNA, Circular, Sequence Analysis, RNA, Brain Neoplasms genetics, Ependymoma genetics
Abstract

Pediatric ependymomas frequently develop in the cerebellum and are currently treated using non-specific therapies, in part, because few somatically mutated driver genes are present, and the underlying pathobiology is poorly described. Circular RNAs (circRNAs) constitute as a large class of primarily non-coding RNAs with important roles in tumorigenesis, but they have not been described in pediatric ependymomas. To advance our molecular understanding of ependymomas, we performed Next Generation Sequencing of rRNA-depleted total RNA of 10 primary ependymoma and three control samples. CircRNA expression patterns were correlated to disease stage, outcome, age, and gender. We found a profound global downregulation of circRNAs in ependymoma relative to control samples. Many differentially expressed circRNAs were discovered and circSMARCA5 and circ-FBXW7, which are described as tumor suppressors in glioma and glioblastomas in adults, were among the most downregulated. Moreover, patients with a dismal outcome clustered separately from patients with a good prognosis in unsupervised hierarchical cluster analyses. Next, NanoString nCounter experiments were performed, using a custom-designed panel targeting 66 selected circRNAs, on a larger cohort that also included medulloblastomas and pilocytic astrocytomas. These experiments indicated that circRNA expression profiles are different among distinct pediatric brain tumor subtypes. In particular, circRNAs derived from RMST, LRBA, WDR78, DRC1 and BBS9 genes were specifically upregulated in ependymomas. In conclusion, circRNAs have different expression profiles in ependymomas relative to controls and between survivors and patients with a dismal outcome, suggesting that circRNAs could be exerted as diagnostic and prognostic biomarkers in the future if further validated in larger cohorts., (© 2020 The Authors. Brain Pathology published by John Wiley & Sons Ltd on behalf of International Society of Neuropathology.)

Published
2021
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42. TERT promoter mutations in primary and secondary WHO grade III meningioma.

Author

Maier AD, Stenman A, Svahn F, Mirian C, Bartek J Jr, Juhler M, Zedenius J, Broholm H, and Mathiesen T

Subjects
Adolescent, Adult, Aged, Aged, 80 and over, Child, Cohort Studies, Female, Humans, Male, Meningeal Neoplasms pathology, Meningioma pathology, Middle Aged, Neoplasm Grading, Point Mutation, Promoter Regions, Genetic, Young Adult, Meningeal Neoplasms genetics, Meningioma genetics, Neoplasm Recurrence, Local genetics, Telomerase genetics
Abstract

Purpose: TERT promoter mutation (TERTp Mut ) has a strong association to recurrence and has been suggested to act as a driver mutation for malignant transformation of WHO grade I and II meningiomas. TERTp Mut has been investigated in selected high-grade meningioma samples. The existence of TERTp Mut across recurrent tumors in a population-based cohort needs to be investigated in order to identify when TERTp Mut emerges across recurrent samples and to validate prognostic impact among WHO grade III tumors., Methods: We gathered material from a consecutive single-center cohort of 40 patients with malignant meningioma (WHO grade III) treated between 2000 and 2018, including specimens from primary and secondary malignant meningiomas with the corresponding earlier benign specimens and later malignant recurrences. In total 107 tumor samples were studied by Sanger sequencing for TERT promoter mutational status., Results: Seven of 40 patients (17.5%) harbored TERTp Mut thus validating the incidence of TERTp Mut in previous non-population-based cohorts. In 6/7 patients, the TERTp Mut was present at initial surgery (WHO grade I-III) while in one patient the TERTp Mut was found de novo when the meningioma became malignant. The incidences were 2/1.000.000/year for TERTp Mut WHO grade III meningioma and 8/1.000.000/year for TERTp wt WHO grade III meningioma in our catchment area. We found a 1.7 times higher recurrence rate (CI 95% 0.65-4.44) and a 2.5 higher mortality rate per 10 person-years (CI 95% 1.01-6.19) for TERTp Mut compared to TERTp wt ., Conclusion: TERTp Mut can occur independently of malignant progression in meningioma and was most often present from the first tumor sample across recurring tumors. TERTp Mut in WHO grade III may represent a marker of an aggressive subset of tumors., (© 2020 International Society of Neuropathology.)

Published
2021
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43. Regional Differences in Neuroinflammation-Associated Gene Expression in the Brain of Sporadic Creutzfeldt-Jakob Disease Patients.

Author

Areškevičiūtė A, Litman T, Broholm H, Melchior LC, Nielsen PR, Green A, Eriksen JO, Smith C, and Lund EL

Subjects
Aged, Brain pathology, Cellular Microenvironment genetics, Cellular Microenvironment immunology, Computational Biology methods, Creutzfeldt-Jakob Syndrome pathology, Disease Susceptibility, Female, Gene Expression Profiling, Humans, Male, Middle Aged, Transcriptome, Biomarkers, Brain metabolism, Creutzfeldt-Jakob Syndrome etiology, Creutzfeldt-Jakob Syndrome metabolism, Gene Expression
Abstract

Neuroinflammation is an essential part of neurodegeneration. Yet, the current understanding of neuroinflammation-associated molecular events in distinct brain regions of prion disease patients is insufficient to lay the ground for effective treatment strategies targeting this complex neuropathological process. To address this problem, we analyzed the expression of 800 neuroinflammation-associated genes to create a profile of biological processes taking place in the frontal cortex and cerebellum of patients who suffered from sporadic Creutzfeldt-Jakob disease. The analysis was performed using NanoString nCounter technology with human neuroinflammation panel+. The observed gene expression patterns were regionally and sub-regionally distinct, suggesting a variable neuroinflammatory response. Interestingly, the observed differences could not be explained by the molecular subtypes of sporadic Creutzfeldt-Jakob disease. Furthermore, analyses of canonical pathways and upstream regulators based on differentially expressed genes indicated an overlap between biological processes taking place in different brain regions. This suggests that even smaller-scale spatial data reflecting subtle changes in brain cells' functional heterogeneity and their immediate pathologic microenvironments are needed to explain the observed differential gene expression in a greater detail.

Published
2020
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44. Mitotic and Proliferative Indices in WHO Grade III Meningioma.

Author

Daniela Maier A, Brøchner CB, Bartek J Jr, Eriksson F, Ugleholdt H, Broholm H, and Mathiesen T

Abstract

Meningiomas with inherently high mitotic indices and poor prognosis, such as WHO grade III meningiomas, have not been investigated separately to establish interchangeability between conventional mitotic index counted on H&E stained slides (MI) and mitotic index counted on phosphohistone-H3 stained slides (PHH3 MI). This study investigates the agreement of MI and PHH3 MI and to analyze the association of progression-free survival (PFS) and MI, PHH3 MI, and the proliferative index (PI, Ki-67) in WHO grade III meningioma. Tumor specimens from 24 consecutive patients were analyzed for expression of Ki-67, PHH3 MI, and MI. Quantification was performed independently by two observers who made replicate counts in hot spots and overall tumor staining. Repeatability in replicate counts from MI and PHH3 MI was low in both observers. Consequently, we could not report the agreement. MI, PHH3 MI and hot spot counts of Ki-67 were associated with PFS (MI hot spot HR = 1.61, 95% CI 1.12-2.31, p = 0.010; PHH3 MI hot spot HR = 1.59, 95% CI 1.15-2.21, p = 0.006; Ki-67 hot spot HR = 1.06, 95% CI 1.02-1.11. p = 0.004). We found markedly low repeatability of manually counted MI and PHH3 MI in WHO grade III meningioma, and we could not conclude that the two methods agreed. Subsequently, quantification with better repeatability should be sought. All three biomarkers were associated with PFS.

Published
2020
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45. Angiotensinogen promoter methylation predicts bevacizumab treatment response of patients with recurrent glioblastoma.

Author

Urup T, Gillberg L, Kaastrup K, Lü MJS, Michaelsen SR, Andrée Larsen V, Christensen IJ, Broholm H, Lassen U, Grønbaek K, and Poulsen HS

Subjects
Adult, Aged, Biomarkers, Tumor genetics, Biomarkers, Tumor metabolism, Brain Neoplasms drug therapy, Brain Neoplasms genetics, Cohort Studies, CpG Islands, DNA Methylation, Female, Glioblastoma drug therapy, Glioblastoma genetics, Humans, Logistic Models, Male, Middle Aged, Neoplasm Recurrence, Local genetics, Neoplasm Recurrence, Local prevention & control, Promoter Regions, Genetic, Angiotensinogen genetics, Angiotensinogen metabolism, Antineoplastic Agents, Immunological therapeutic use, Bevacizumab therapeutic use, Brain Neoplasms metabolism, Glioblastoma metabolism, Neoplasm Recurrence, Local metabolism, Renin-Angiotensin System genetics
Abstract

Patients with recurrent glioblastoma achieving response to bevacizumab combined with chemotherapy have clinical improvement and prolonged survival. High gene expression of angiotensinogen (AGT) is associated with a poor bevacizumab response. Because AGT expression is epigenetically regulated, we aimed to investigate whether AGT promoter methylation in tumor tissue predicts response to bevacizumab combination therapy in patients with recurrent glioblastoma. The study included 159 patients with recurrent glioblastoma, treated with bevacizumab combination treatment (training cohort, n = 77; validation cohort, n = 82). All patients could be evaluated for treatment response and biomarkers. DNA methylation of 4 CpG sites in the AGT promoter was measured using pyrosequencing. A model for nonresponse was established using logistic regression analysis. In the training cohort, lower methylation of each of the four CpG sites in the AGT promoter was significantly associated with nonresponse (all P < 0.05). Moreover, the mean methylation level of all four CpG sites was associated with an increased likelihood of not achieving response to bevacizumab combination therapy (twofold decrease: odds ratio = 3.01; 95% confidence interval: 1.41-6.44; P = 0.004). We developed a model for nonresponse in the training cohort, where a threshold of mean AGT promoter methylation levels was set to below 12%. The model could predict bevacizumab nonresponse with 96% specificity. Importantly, this predictor was also significantly associated with nonresponse in the validation cohort (P = 0.037). Taken together, our findings suggest that low AGT promoter methylation in tumor tissue predicts nonresponse to bevacizumab combination treatment in patients with recurrent glioblastoma. We have, thus, established and successfully validated a predictor for nonresponse that can be used to identify patients who will not benefit from bevacizumab combination therapy., (© 2020 The Authors. Published by FEBS Press and John Wiley & Sons Ltd.)

Published
2020
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46. Clinical Characteristics of Gliosarcoma and Outcomes From Standardized Treatment Relative to Conventional Glioblastoma.

Author

Frandsen S, Broholm H, Larsen VA, Grunnet K, Møller S, Poulsen HS, and Michaelsen SR

Abstract

Background: Gliosarcoma (GS) is a rare histopathologic variant of glioblastoma (GBM) characterized by a biphasic growth pattern consisting of both glial and sarcomatous components. Reports regarding its relative prognosis compared to conventional GBM are conflicting and although GS is treated as conventional GBM, supporting evidence is lacking. The aim of this study was to characterize demographic trends, clinical outcomes and prognostic variables of GS patients receiving standardized therapy and compare these to conventional GBM. Methods: Six hundred and eighty GBM patients, treated with maximal safe resection followed by radiotherapy with concomitant and adjuvant temozolomide at a single institution, were retrospectively reevaluated by reviewing histopathological records and tumor tissue for identification of GS patients. Clinico-pathological- and tumor growth characteristics were obtained via assessment of medical records and imaging analysis. Kaplan-Meier survival estimates were compared with log-rank testing, while Cox-regression modeling was tested for prognostic factors in GS patients. Results: The cohort included 26 primary gliosarcoma (PGS) patients (3.8%) and 7 secondary gliosarcoma (SGS) patients (1.0%). Compared to conventional GBM tumors, PGS tumors were significantly more often MGMT-unmethylated (73.9%) and located in the temporal lobe (57.7%). GS tumors often presented dural contact, while extracranial metastasis was only found in 1 patient. No significant differences were found between PGS and conventional GBM in progression-free-survival (6.8 and 7.6 months, respectively, p = 0.105) and in overall survival (13.4 and 15.7 months, respectively, p = 0.201). Survival following recurrence was not significantly different between PGS, SGS, and GBM. Temporal tumor location and MGMT status were found associated with PGS survival ( p = 0.036 and p = 0.022, respectively). Conclusion: Despite histopathological and location difference between GS and GBM tumors, the patients present similar survival outcome from standardized treatment. These findings support continued practice of radiation and temozolomide for GS patients., (Copyright © 2019 Frandsen, Broholm, Larsen, Grunnet, Møller, Poulsen and Michaelsen.)

Published
2019
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47. Recurrent glioblastoma versus late posttreatment changes: diagnostic accuracy of O-(2-[18F]fluoroethyl)-L-tyrosine positron emission tomography (18F-FET PET).

Author

Bashir A, Mathilde Jacobsen S, Mølby Henriksen O, Broholm H, Urup T, Grunnet K, Andrée Larsen V, Møller S, Skjøth-Rasmussen J, Skovgaard Poulsen H, and Law I

Subjects
Adult, Aged, Aged, 80 and over, Brain Neoplasms diagnostic imaging, Brain Neoplasms metabolism, Brain Neoplasms therapy, Chemoradiotherapy mortality, Combined Modality Therapy, Female, Follow-Up Studies, Glioblastoma diagnostic imaging, Glioblastoma metabolism, Glioblastoma therapy, Humans, Immunotherapy mortality, Male, Middle Aged, Neoplasm Recurrence, Local diagnostic imaging, Neoplasm Recurrence, Local metabolism, Neoplasm Recurrence, Local therapy, Prognosis, Radiopharmaceuticals metabolism, Retrospective Studies, Survival Rate, Tyrosine metabolism, Young Adult, Brain Neoplasms pathology, Glioblastoma pathology, Neoplasm Recurrence, Local pathology, Positron-Emission Tomography methods, Tyrosine analogs & derivatives
Abstract

Background: Diagnostic accuracy in previous studies of O-(2-[18F]-fluoroethyl)-L-tyrosine (18F-FET) PET in patients with suspected recurrent glioma may be influenced by prolonged dynamic PET acquisitions, heterogeneous populations, different non-standard-of-care therapies, and PET scans performed at different time points post radiotherapy. We investigated the diagnostic accuracy of a 20-minute 18F-FET PET scan in MRI-suspected recurrent glioblastoma 6 months after standard radiotherapy and its ability to prognosticate overall survival (OS)., Methods: In total, 146 glioblastoma patients with 168 18F-FET PET scans were reviewed retrospectively. Patients with MRI responses to bevacizumab or undergoing re-irradiation or immunotherapy after 18F-FET PET were excluded. Maximum and mean tumor-to-background ratios (TBRmax, TBRmean) and biological tumor volume (BTV) were recorded and verified by histopathology or clinical/radiological follow-up. Thresholds of 18F-FET parameters were determined by receiver operating characteristic (ROC) analysis. Prognostic factors were investigated in Cox proportional hazards models., Results: Surgery was performed after 104 18F-FET PET scans, while clinical/radiological surveillance was used following 64, identifying 152 glioblastoma recurrences and 16 posttreatment changes. ROC analysis yielded thresholds of 2.0 for TBRmax, 1.8 for TBRmean, and 0.55 cm3 for BTV in differentiating recurrent glioblastoma from posttreatment changes with the best performance of TBRmax (sensitivity 99%, specificity 94%; P < 0.0001) followed by BTV (sensitivity 98%, specificity 94%; P < 0.0001). Using these thresholds, 166 18F-FET PET scans were correctly classified. Increasing BTV was associated with shorter OS (P < 0.0001)., Conclusion: A 20-minute 18F-FET PET scan is a powerful tool to distinguish posttreatment changes from recurrent glioblastoma 6-month postradiotherapy, and predicts OS., (© The Author(s) 2019. Published by Oxford University Press on behalf of the Society for Neuro-Oncology. All rights reserved. For permissions, please e-mail: journals.permissions@oup.com.)

Published
2019
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48. Early Postoperative 18 F-FET PET/MRI for Pediatric Brain and Spinal Cord Tumors.

Author

Marner L, Nysom K, Sehested A, Borgwardt L, Mathiasen R, Henriksen OM, Lundemann M, Munck Af Rosenschöld P, Thomsen C, Bøgeskov L, Skjøth-Rasmussen J, Juhler M, Kruse A, Broholm H, Scheie D, Lauritsen T, Forman JL, Wehner PS, Højgaard L, and Law I

Subjects
Adolescent, Astrocytoma diagnostic imaging, Brain diagnostic imaging, Brain Neoplasms surgery, Child, Child, Preschool, Female, Fluorodeoxyglucose F18, Follow-Up Studies, Glioma diagnostic imaging, Humans, Infant, Infant, Newborn, Male, Multimodal Imaging, Neoplasm, Residual diagnostic imaging, Pediatrics, Postoperative Period, Prospective Studies, Reoperation, Reproducibility of Results, Rhabdoid Tumor diagnostic imaging, Sensitivity and Specificity, Spinal Cord Neoplasms surgery, Teratoma diagnostic imaging, Tomography, X-Ray Computed, Young Adult, Brain Neoplasms diagnostic imaging, Magnetic Resonance Imaging, Positron-Emission Tomography, Spinal Cord Neoplasms diagnostic imaging
Abstract

Complete resection is the treatment of choice for most pediatric brain tumors, but early postoperative MRI for detection of residual tumor may be misleading because of MRI signal changes caused by the operation. PET imaging with amino acid tracers in adults increases the diagnostic accuracy for brain tumors, but the literature in pediatric neurooncology is limited. A hybrid PET/MRI system is highly beneficial in children, reducing the number of scanning procedures, and this is to our knowledge the first larger study using PET/MRI in pediatric neurooncology. We evaluated if additional postoperative 18 F-fluoro-ethyl-tyrosine ( 18 F-FET) PET in children and adolescents would improve diagnostic accuracy for the detection of residual tumor as compared with MRI alone and would assist clinical management. Methods: Twenty-two patients (7 male; mean age, 9.5 y; range, 0-19 y) were included prospectively and consecutively in the study and had 27 early postoperative 18 F-FET PET exams performed preferentially in a hybrid PET/MRI system (NCT03402425). Results: Using follow-up (93%) or reoperation (7%) as the reference standard, PET combined with MRI discriminated tumor from treatment effects with a lesion-based sensitivity/specificity/accuracy (95% confidence intervals) of 0.73 (0.50-1.00)/1.00 (0.74-1.00)/0.87 (0.73-1.00) compared with MRI alone: 0.80 (0.57-1.00)/0.75 (0.53-0.94)/0.77 (0.65-0.90); that is, the specificity for PET/MRI was 1.00 as compared with 0.75 for MRI alone ( P = 0.13). In 11 of 27 cases (41%), results from the 18 F-FET PET scans added relevant clinical information, including one scan that directly influenced clinical management because an additional residual tumor site was identified. 18 F-FET uptake in reactive changes was frequent (52%), but correct interpretation was possible in all cases. Conclusion: The high specificity for detecting residual tumor suggests that supplementary 18 F-FET PET is relevant in cases where reoperation for residual tumor is considered., (© 2019 by the Society of Nuclear Medicine and Molecular Imaging.)

Published
2019
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49. Extracranial metastases in glioblastoma-Two case stories.

Author

Schou Nørøxe D, Regner Michaelsen S, Broholm H, Møller S, Skovgaard Poulsen H, and Lassen U

Abstract

The clinician should always consider extracranial metastases in glioblastoma. Increased risk factors are young age at diagnosis, histology of gliosarcoma, and prior intracranial tumor surgery. Clinical guidelines are needed for this rare event, including consideration for prophylactic intervention., Competing Interests: None declared.

Published
2018
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50. VEGF-C sustains VEGFR2 activation under bevacizumab therapy and promotes glioblastoma maintenance.

Author

Michaelsen SR, Staberg M, Pedersen H, Jensen KE, Majewski W, Broholm H, Nedergaard MK, Meulengracht C, Urup T, Villingshøj M, Lukacova S, Skjøth-Rasmussen J, Brennum J, Kjær A, Lassen U, Stockhausen MT, Poulsen HS, and Hamerlik P

Subjects
Angiogenesis Inhibitors pharmacology, Animals, Apoptosis, Autocrine Communication, Biomarkers, Tumor genetics, Biomarkers, Tumor metabolism, Cell Cycle, Cell Proliferation, Female, Gene Expression Regulation, Neoplastic, Glioblastoma drug therapy, Glioblastoma metabolism, Humans, Mice, Mice, Nude, Signal Transduction, Tumor Cells, Cultured, Vascular Endothelial Growth Factor C genetics, Vascular Endothelial Growth Factor Receptor-2 genetics, Xenograft Model Antitumor Assays, Bevacizumab pharmacology, Glioblastoma pathology, Vascular Endothelial Growth Factor C metabolism, Vascular Endothelial Growth Factor Receptor-2 metabolism
Abstract

Background: Glioblastoma ranks among the most lethal cancers, with current therapies offering only palliation. Paracrine vascular endothelial growth factor (VEGF) signaling has been targeted using anti-angiogenic agents, whereas autocrine VEGF/VEGF receptor 2 (VEGFR2) signaling is poorly understood. Bevacizumab resistance of VEGFR2-expressing glioblastoma cells prompted interrogation of autocrine VEGF-C/VEGFR2 signaling in glioblastoma., Methods: Autocrine VEGF-C/VEGFR2 signaling was functionally investigated using RNA interference and exogenous ligands in patient-derived xenograft lines and primary glioblastoma cell cultures in vitro and in vivo. VEGF-C expression and interaction with VEGFR2 in a matched pre- and post-bevacizumab treatment cohort were analyzed by immunohistochemistry and proximity ligation assay., Results: VEGF-C was expressed by patient-derived xenograft glioblastoma lines, primary cells, and matched surgical specimens before and after bevacizumab treatment. VEGF-C activated autocrine VEGFR2 signaling to promote cell survival, whereas targeting VEGF-C expression reprogrammed cellular transcription to attenuate survival and cell cycle progression. Supporting potential translational significance, targeting VEGF-C impaired tumor growth in vivo, with superiority to bevacizumab treatment., Conclusions: Our results demonstrate VEGF-C serves as both a paracrine and an autocrine pro-survival cytokine in glioblastoma, promoting tumor cell survival and tumorigenesis. VEGF-C permits sustained VEGFR2 activation and tumor growth, where its inhibition appears superior to bevacizumab therapy in improving tumor control.

Published
2018
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