Efficacy of Temozolomide Therapy in Patients With Aggressive Pituitary Adenomas and Carcinomas—A German Survey

Abstract Context Despite growing evidence that temozolomide (TMZ) therapy is effective for the treatment of aggressive pituitary tumors (APTs) or carcinomas (PCs), individual therapy decisions remain challenging. Objective We therefore aimed to report on clinical characteristics leading to initiatio...

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Published inThe journal of clinical endocrinology and metabolism Vol. 105; no. 3; pp. e660 - e675
Main Authors Elbelt, Ulf, Schlaffer, Sven M, Buchfelder, Michael, Knappe, Ulrich J, Vila, Greisa, Micko, Alexander, Deutschbein, Timo, Unger, Nicole, Lammert, Alexander, Topuzoglu-Müller, Tengü, Bojunga, Jörg, Droste, Michael, Johanssen, Sarah, Kolenda, Herbert, Ritzel, Katrin, Buslei, Rolf, Strasburger, Christian J, Petersenn, Stephan, Honegger, Jürgen
Format Journal Article
LanguageEnglish
Published US Oxford University Press 01.03.2020
Copyright Oxford University Press
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Abstract Abstract Context Despite growing evidence that temozolomide (TMZ) therapy is effective for the treatment of aggressive pituitary tumors (APTs) or carcinomas (PCs), individual therapy decisions remain challenging. Objective We therefore aimed to report on clinical characteristics leading to initiation of TMZ therapy and to add evidence on TMZ long-term effectiveness. Design and subjects Retrospective survey on TMZ treatment in patients with APTs or PCs. TMZ therapy was initiated in 47 patients (22 females) with APTs (n = 34) or PCs (n = 13). Mean age at diagnosis was 45 ± 15 years. The immunohistochemical subtypes were corticotroph (n = 20), lactotroph (n = 18), and nonfunctioning (n = 9) tumors. TMZ therapy started 8 years after initial diagnosis using a standard regimen (median 6 cycles) for the majority of patients. Results Long-term radiological response to TMZ after a median follow-up of 32 months with 4 patients still on TMZ therapy was tumor regression for 9 (20%), stable disease for 8 (17%), and tumor progression for 29 patients (63%) (outcome data available for 46 patients). Progression occurred 16 months after initiation of TMZ. Median estimated progression-free survival was 23 months. Disease stabilization and median progression-free survival did not differ between patients with APTs or PCs. Predictors of tumor response were not identified. Overall, TMZ was well tolerated. Conclusion We performed a nationwide survey on TMZ therapy in patients with APTs and PCs. While early response rates to TMZ are promising, long-term outcome is less favorable. Prolonged TMZ administration should be considered. We were not able to confirm previously reported predictors of tumor response to TMZ.
AbstractList Context Despite growing evidence that temozolomide (TMZ) therapy is effective for the treatment of aggressive pituitary tumors (APTs) or carcinomas (PCs), individual therapy decisions remain challenging. Objective We therefore aimed to report on clinical characteristics leading to initiation of TMZ therapy and to add evidence on TMZ long-term effectiveness. Design and subjects Retrospective survey on TMZ treatment in patients with APTs or PCs. TMZ therapy was initiated in 47 patients (22 females) with APTs (n = 34) or PCs (n = 13). Mean age at diagnosis was 45 ± 15 years. The immunohistochemical subtypes were corticotroph (n = 20), lactotroph (n = 18), and nonfunctioning (n = 9) tumors. TMZ therapy started 8 years after initial diagnosis using a standard regimen (median 6 cycles) for the majority of patients. Results Long-term radiological response to TMZ after a median follow-up of 32 months with 4 patients still on TMZ therapy was tumor regression for 9 (20%), stable disease for 8 (17%), and tumor progression for 29 patients (63%) (outcome data available for 46 patients). Progression occurred 16 months after initiation of TMZ. Median estimated progression-free survival was 23 months. Disease stabilization and median progression-free survival did not differ between patients with APTs or PCs. Predictors of tumor response were not identified. Overall, TMZ was well tolerated. Conclusion We performed a nationwide survey on TMZ therapy in patients with APTs and PCs. While early response rates to TMZ are promising, long-term outcome is less favorable. Prolonged TMZ administration should be considered. We were not able to confirm previously reported predictors of tumor response to TMZ.
Abstract Context Despite growing evidence that temozolomide (TMZ) therapy is effective for the treatment of aggressive pituitary tumors (APTs) or carcinomas (PCs), individual therapy decisions remain challenging. Objective We therefore aimed to report on clinical characteristics leading to initiation of TMZ therapy and to add evidence on TMZ long-term effectiveness. Design and subjects Retrospective survey on TMZ treatment in patients with APTs or PCs. TMZ therapy was initiated in 47 patients (22 females) with APTs (n = 34) or PCs (n = 13). Mean age at diagnosis was 45 ± 15 years. The immunohistochemical subtypes were corticotroph (n = 20), lactotroph (n = 18), and nonfunctioning (n = 9) tumors. TMZ therapy started 8 years after initial diagnosis using a standard regimen (median 6 cycles) for the majority of patients. Results Long-term radiological response to TMZ after a median follow-up of 32 months with 4 patients still on TMZ therapy was tumor regression for 9 (20%), stable disease for 8 (17%), and tumor progression for 29 patients (63%) (outcome data available for 46 patients). Progression occurred 16 months after initiation of TMZ. Median estimated progression-free survival was 23 months. Disease stabilization and median progression-free survival did not differ between patients with APTs or PCs. Predictors of tumor response were not identified. Overall, TMZ was well tolerated. Conclusion We performed a nationwide survey on TMZ therapy in patients with APTs and PCs. While early response rates to TMZ are promising, long-term outcome is less favorable. Prolonged TMZ administration should be considered. We were not able to confirm previously reported predictors of tumor response to TMZ.
Despite growing evidence that temozolomide (TMZ) therapy is effective for the treatment of aggressive pituitary tumors (APTs) or carcinomas (PCs), individual therapy decisions remain challenging.CONTEXTDespite growing evidence that temozolomide (TMZ) therapy is effective for the treatment of aggressive pituitary tumors (APTs) or carcinomas (PCs), individual therapy decisions remain challenging.We therefore aimed to report on clinical characteristics leading to initiation of TMZ therapy and to add evidence on TMZ long-term effectiveness.OBJECTIVEWe therefore aimed to report on clinical characteristics leading to initiation of TMZ therapy and to add evidence on TMZ long-term effectiveness.Retrospective survey on TMZ treatment in patients with APTs or PCs. TMZ therapy was initiated in 47 patients (22 females) with APTs (n = 34) or PCs (n = 13). Mean age at diagnosis was 45 ± 15 years. The immunohistochemical subtypes were corticotroph (n = 20), lactotroph (n = 18), and nonfunctioning (n = 9) tumors. TMZ therapy started 8 years after initial diagnosis using a standard regimen (median 6 cycles) for the majority of patients.DESIGN AND SUBJECTSRetrospective survey on TMZ treatment in patients with APTs or PCs. TMZ therapy was initiated in 47 patients (22 females) with APTs (n = 34) or PCs (n = 13). Mean age at diagnosis was 45 ± 15 years. The immunohistochemical subtypes were corticotroph (n = 20), lactotroph (n = 18), and nonfunctioning (n = 9) tumors. TMZ therapy started 8 years after initial diagnosis using a standard regimen (median 6 cycles) for the majority of patients.Long-term radiological response to TMZ after a median follow-up of 32 months with 4 patients still on TMZ therapy was tumor regression for 9 (20%), stable disease for 8 (17%), and tumor progression for 29 patients (63%) (outcome data available for 46 patients). Progression occurred 16 months after initiation of TMZ. Median estimated progression-free survival was 23 months. Disease stabilization and median progression-free survival did not differ between patients with APTs or PCs. Predictors of tumor response were not identified. Overall, TMZ was well tolerated.RESULTSLong-term radiological response to TMZ after a median follow-up of 32 months with 4 patients still on TMZ therapy was tumor regression for 9 (20%), stable disease for 8 (17%), and tumor progression for 29 patients (63%) (outcome data available for 46 patients). Progression occurred 16 months after initiation of TMZ. Median estimated progression-free survival was 23 months. Disease stabilization and median progression-free survival did not differ between patients with APTs or PCs. Predictors of tumor response were not identified. Overall, TMZ was well tolerated.We performed a nationwide survey on TMZ therapy in patients with APTs and PCs. While early response rates to TMZ are promising, long-term outcome is less favorable. Prolonged TMZ administration should be considered. We were not able to confirm previously reported predictors of tumor response to TMZ.CONCLUSIONWe performed a nationwide survey on TMZ therapy in patients with APTs and PCs. While early response rates to TMZ are promising, long-term outcome is less favorable. Prolonged TMZ administration should be considered. We were not able to confirm previously reported predictors of tumor response to TMZ.
Despite growing evidence that temozolomide (TMZ) therapy is effective for the treatment of aggressive pituitary tumors (APTs) or carcinomas (PCs), individual therapy decisions remain challenging. We therefore aimed to report on clinical characteristics leading to initiation of TMZ therapy and to add evidence on TMZ long-term effectiveness. Retrospective survey on TMZ treatment in patients with APTs or PCs. TMZ therapy was initiated in 47 patients (22 females) with APTs (n = 34) or PCs (n = 13). Mean age at diagnosis was 45 ± 15 years. The immunohistochemical subtypes were corticotroph (n = 20), lactotroph (n = 18), and nonfunctioning (n = 9) tumors. TMZ therapy started 8 years after initial diagnosis using a standard regimen (median 6 cycles) for the majority of patients. Long-term radiological response to TMZ after a median follow-up of 32 months with 4 patients still on TMZ therapy was tumor regression for 9 (20%), stable disease for 8 (17%), and tumor progression for 29 patients (63%) (outcome data available for 46 patients). Progression occurred 16 months after initiation of TMZ. Median estimated progression-free survival was 23 months. Disease stabilization and median progression-free survival did not differ between patients with APTs or PCs. Predictors of tumor response were not identified. Overall, TMZ was well tolerated. We performed a nationwide survey on TMZ therapy in patients with APTs and PCs. While early response rates to TMZ are promising, long-term outcome is less favorable. Prolonged TMZ administration should be considered. We were not able to confirm previously reported predictors of tumor response to TMZ.
Author Honegger, Jürgen
Vila, Greisa
Deutschbein, Timo
Strasburger, Christian J
Petersenn, Stephan
Micko, Alexander
Buslei, Rolf
Droste, Michael
Lammert, Alexander
Bojunga, Jörg
Topuzoglu-Müller, Tengü
Kolenda, Herbert
Elbelt, Ulf
Ritzel, Katrin
Unger, Nicole
Johanssen, Sarah
Buchfelder, Michael
Knappe, Ulrich J
Schlaffer, Sven M
AuthorAffiliation Department of Endocrinology, Diabetes and Nutrition, Charité - Universitätsmedizin Berlin, Berlin, Germany Department of Neurosurgery, University of Erlangen-Nuremberg, Erlangen, Germany Department of Neurosurgery, Johannes Wesling Klinikum, Universitätsklinikum der Ruhruniversität Bochum, Minden, Germany Department of Internal Medicine III, Division of Endocrinology and Metabolism, Medical University Vienna, Vienna, Austria Department of Neurosurgery, Medical University Vienna, Vienna, Austria Department of Internal Medicine I, Division of Endocrinology and Diabetes, University Hospital Würzburg, University of Würzburg, Würzburg, Germany Department of Endocrinology, Diabetes and Metabolism, University Hospital Essen, Essen, Germany Vth Department of Medicine, Medical Faculty Mannheim of the University of Heidelberg, Mannheim, Germany Department of Endocrinology, Diabetes and Preventive Medicine, University Hospital of Cologne, Cologne, Germany Department of Internal Medicine 1, Johann
AuthorAffiliation_xml – name: Department of Endocrinology, Diabetes and Nutrition, Charité - Universitätsmedizin Berlin, Berlin, Germany Department of Neurosurgery, University of Erlangen-Nuremberg, Erlangen, Germany Department of Neurosurgery, Johannes Wesling Klinikum, Universitätsklinikum der Ruhruniversität Bochum, Minden, Germany Department of Internal Medicine III, Division of Endocrinology and Metabolism, Medical University Vienna, Vienna, Austria Department of Neurosurgery, Medical University Vienna, Vienna, Austria Department of Internal Medicine I, Division of Endocrinology and Diabetes, University Hospital Würzburg, University of Würzburg, Würzburg, Germany Department of Endocrinology, Diabetes and Metabolism, University Hospital Essen, Essen, Germany Vth Department of Medicine, Medical Faculty Mannheim of the University of Heidelberg, Mannheim, Germany Department of Endocrinology, Diabetes and Preventive Medicine, University Hospital of Cologne, Cologne, Germany Department of Internal Medicine 1, Johann Wolfgang Goethe-University Hospital, Frankfurt, Germany Medicover Oldenburg MVZ, Oldenburg, Germany Endokrinologikum Berlin, Berlin, Germany Department of Neurosurgery, Agaplesion Diakonieklinikum Rotenburg, Rotenburg, Germany Medizinische Klinik und Poliklinik IV, Klinikum der Universität München, Ludwig-Maximilians-Universität München, Munich, Germany Institute of Pathology, SozialStiftung Bamberg, Bamberg, Germany ENDOC Praxis für Endokrinologie, Andrologie und medikamentöse Tumortherapie, Hamburg, Germany Department of Neurosurgery, University of Tuebingen, Tuebingen, Germany
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  surname: Elbelt
  fullname: Elbelt, Ulf
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  organization: Department of Endocrinology, Diabetes and Nutrition, Charité-Universitätsmedizin Berlin, Berlin, Germany
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  fullname: Schlaffer, Sven M
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  surname: Buchfelder
  fullname: Buchfelder, Michael
  organization: Department of Neurosurgery, University of Erlangen-Nuremberg, Erlangen, Germany
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  givenname: Ulrich J
  surname: Knappe
  fullname: Knappe, Ulrich J
  organization: Department of Neurosurgery, Johannes Wesling Klinikum, Universitätsklinikum der Ruhruniversität Bochum, Minden, Germany
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  surname: Unger
  fullname: Unger, Nicole
  organization: Department of Endocrinology, Diabetes and Metabolism, University Hospital Essen, Essen, Germany
– sequence: 9
  givenname: Alexander
  surname: Lammert
  fullname: Lammert, Alexander
  organization: Vth Department of Medicine, Medical Faculty Mannheim of the University of Heidelberg, Mannheim, Germany
– sequence: 10
  givenname: Tengü
  surname: Topuzoglu-Müller
  fullname: Topuzoglu-Müller, Tengü
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  givenname: Michael
  surname: Droste
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  organization: Medicover Oldenburg MVZ, Oldenburg, Germany
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  organization: Endokrinologikum Berlin, Berlin, Germany
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  fullname: Kolenda, Herbert
  organization: Department of Neurosurgery, Agaplesion Diakonieklinikum Rotenburg, Rotenburg, Germany
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  givenname: Katrin
  surname: Ritzel
  fullname: Ritzel, Katrin
  organization: Medizinische Klinik und Poliklinik IV, Klinikum der Universität München, Ludwig-Maximilians-Universität München, Munich, Germany
– sequence: 16
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  surname: Buslei
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  organization: Institute of Pathology, SozialStiftung Bamberg, Bamberg, Germany
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  givenname: Christian J
  surname: Strasburger
  fullname: Strasburger, Christian J
  organization: Department of Endocrinology, Diabetes and Nutrition, Charité-Universitätsmedizin Berlin, Berlin, Germany
– sequence: 18
  givenname: Stephan
  surname: Petersenn
  fullname: Petersenn, Stephan
  organization: ENDOC Center for Endocrine Tumors, Hamburg, Germany
– sequence: 19
  givenname: Jürgen
  surname: Honegger
  fullname: Honegger, Jürgen
  organization: Department of Neurosurgery, University of Tuebingen, Tuebingen, Germany
BackLink https://www.ncbi.nlm.nih.gov/pubmed/31746334$$D View this record in MEDLINE/PubMed
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ContentType Journal Article
Copyright Endocrine Society 2019. All rights reserved. For permissions, please e-mail: journals.permissions@oup.com 2019
Copyright © Oxford University Press 2015
Endocrine Society 2019. All rights reserved. For permissions, please e-mail: journals.permissions@oup.com.
Copyright_xml – notice: Endocrine Society 2019. All rights reserved. For permissions, please e-mail: journals.permissions@oup.com 2019
– notice: Copyright © Oxford University Press 2015
– notice: Endocrine Society 2019. All rights reserved. For permissions, please e-mail: journals.permissions@oup.com.
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Issue 3
Keywords temozolomide
pituitary carcinoma
aggressive pituitary tumor
progression-free survival
response rate
Language English
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Snippet Abstract Context Despite growing evidence that temozolomide (TMZ) therapy is effective for the treatment of aggressive pituitary tumors (APTs) or carcinomas...
Despite growing evidence that temozolomide (TMZ) therapy is effective for the treatment of aggressive pituitary tumors (APTs) or carcinomas (PCs), individual...
Context Despite growing evidence that temozolomide (TMZ) therapy is effective for the treatment of aggressive pituitary tumors (APTs) or carcinomas (PCs),...
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SubjectTerms Brain cancer
Brain tumors
Cancer
Carcinoma
Diagnosis
Patients
Pituitary
Pituitary gland
Survival
Temozolomide
Tumors
Title Efficacy of Temozolomide Therapy in Patients With Aggressive Pituitary Adenomas and Carcinomas—A German Survey
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