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Disseminated oligodendroglial-like leptomeningeal tumors: preliminary diagnostic and therapeutic results for a novel tumor entity corrected
by
Henssler, Andreas
, Müller, Wolf
, Pekrun, Arnulf
, Hirsch, Franz Wolfgang
, Preuss, Matthias
, Hauch, Holger
, Meixensberger, Jürgen
, Nathrath, Michaela
, Kuchelmeister, Klaus
, Christiansen, Holger
, Merkenschlager, Andreas
, Kiess, Wieland
, Kästner, Stefanie
, Pietsch, Torsten
2015
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Disseminated oligodendroglial-like leptomeningeal tumors: preliminary diagnostic and therapeutic results for a novel tumor entity corrected
by
Henssler, Andreas
, Müller, Wolf
, Pekrun, Arnulf
, Hirsch, Franz Wolfgang
, Preuss, Matthias
, Hauch, Holger
, Meixensberger, Jürgen
, Nathrath, Michaela
, Kuchelmeister, Klaus
, Christiansen, Holger
, Merkenschlager, Andreas
, Kiess, Wieland
, Kästner, Stefanie
, Pietsch, Torsten
in
2015
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Disseminated oligodendroglial-like leptomeningeal tumors: preliminary diagnostic and therapeutic results for a novel tumor entity corrected
by
Henssler, Andreas
, Müller, Wolf
, Pekrun, Arnulf
, Hirsch, Franz Wolfgang
, Preuss, Matthias
, Hauch, Holger
, Meixensberger, Jürgen
, Nathrath, Michaela
, Kuchelmeister, Klaus
, Christiansen, Holger
, Merkenschlager, Andreas
, Kiess, Wieland
, Kästner, Stefanie
, Pietsch, Torsten
2015
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Disseminated oligodendroglial-like leptomeningeal tumors: preliminary diagnostic and therapeutic results for a novel tumor entity corrected
Journal Article
Disseminated oligodendroglial-like leptomeningeal tumors: preliminary diagnostic and therapeutic results for a novel tumor entity corrected
2015
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Overview
Pediatric tumors of the central nervous system composed of oligoid tumor cells showing diffuse leptomeningeal spread without a primary mass lesion seem to represent a novel tumor entity. The terms \"diffuse leptomeningeal glioneural tumor\" or-preferably-\"disseminated oligodendroglial-like leptomeningeal tumor of childhood\" (DOGLT) were proposed. Four patients were identified with clinico-neuropathologic findings compatible with DOGLT and a mean follow-up time of 54 months was determined. Seven different biopsies obtained from the four patients were histologically evaluated. Clinical course, diagnostic measures, histopathologic and radiologic features and treatment suggestions were recorded, on the basis of which diagnostic and therapeutic algorithm was proposed. Patients with DOGLT presented with hydrocephalus as first symptom, requiring neurosurgical therapy. Open arachnoid biopsy was necessary to confirm diagnosis. The oligoid cells in a desmoplastic or focally myxoid matrix showed OLIG2-, MAP2-, S-100 and rare HuC/HuD protein-immunopositivity. IDH1 (R132H)- and CD99-immunohistochemistry was negative in all patients. None of the evaluable biopsies of three patients showed chromosome 1p/19q deletion, neither as isolated nor combined allelic loss. Chemotherapy according to the SIOP-LGG 2004 standard induction and consolidation protocol resulted in complete response and partial response, respectively, in 50 % of the patients. However, after discontinuation of chemotherapy, two patients experienced tumor progression and one of them succumbed to the disease after 19 months. Radiological criteria as well as preliminary treatment results are presented after observation of four clinical cases. Prognosis and long-term clinical courses remain to be observed.Pediatric tumors of the central nervous system composed of oligoid tumor cells showing diffuse leptomeningeal spread without a primary mass lesion seem to represent a novel tumor entity. The terms \"diffuse leptomeningeal glioneural tumor\" or-preferably-\"disseminated oligodendroglial-like leptomeningeal tumor of childhood\" (DOGLT) were proposed. Four patients were identified with clinico-neuropathologic findings compatible with DOGLT and a mean follow-up time of 54 months was determined. Seven different biopsies obtained from the four patients were histologically evaluated. Clinical course, diagnostic measures, histopathologic and radiologic features and treatment suggestions were recorded, on the basis of which diagnostic and therapeutic algorithm was proposed. Patients with DOGLT presented with hydrocephalus as first symptom, requiring neurosurgical therapy. Open arachnoid biopsy was necessary to confirm diagnosis. The oligoid cells in a desmoplastic or focally myxoid matrix showed OLIG2-, MAP2-, S-100 and rare HuC/HuD protein-immunopositivity. IDH1 (R132H)- and CD99-immunohistochemistry was negative in all patients. None of the evaluable biopsies of three patients showed chromosome 1p/19q deletion, neither as isolated nor combined allelic loss. Chemotherapy according to the SIOP-LGG 2004 standard induction and consolidation protocol resulted in complete response and partial response, respectively, in 50 % of the patients. However, after discontinuation of chemotherapy, two patients experienced tumor progression and one of them succumbed to the disease after 19 months. Radiological criteria as well as preliminary treatment results are presented after observation of four clinical cases. Prognosis and long-term clinical courses remain to be observed.
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