Reclassification of Mixed Oligoastrocytic Tumors Using a Genetically Integrated Diagnostic Approach

Kim, Seong Ik; Lee, Yujin; Won, Jae Kyung; Park, Shin Young; Choi, Seung Hong

doi:10.4132/jptm.2017.09.25

Cited by 3 publications

(4 citation statements)

References 19 publications

(31 reference statements)

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“…Fourth, IDH1/2 status was not available in all the patients, (57,7% of patients cohort). However, a large number of studies shows that IDH1/2 mutation occurs in all 1p19q-codeleted tumors and the great majority of diffuse gliomas grade II/III also falls into the IDH mutant category [44,6,7,45,46,24,47]. Finally, as is true across all imaging modalities, the manual tumor outlining performed in our study is subjective and reproducibility may be challenged when used in combination with advanced imaging techniques.…”

Section: Discussionmentioning

confidence: 92%

Dynamic susceptibility contrast and diffusion MR imaging identify oligodendroglioma as defined by the 2016 WHO classification for brain tumors: histogram analysis approach

et al. 2019

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Purpose According to the revised World Health Organization (WHO) classification of tumors of the central nervous system (CNS) of 2016, oligodendrogliomas are now defined primarily by a specific molecular signature (presence of IDH mutation and 1p19q codeletion). The purpose of our study was to assess the value of dynamic susceptibility contrast MR imaging (DSC-MRI) and diffusionweighted imaging (DWI) to characterize oligodendrogliomas and to distinguish them from astrocytomas. Methods Seventy-one adult patients with untreated WHO grade II and grade III diffuse infiltrating gliomas and known 1p/19q codeletion status were retrospectively identified and analyzed using relative cerebral blood volume (rCBV) and apparent diffusion coefficient (ADC) maps based on wholetumor volume histograms. The Mann-Whitney U test and logistic regression were used to assess the ability of rCBV and ADC to differentiate between oligodendrogliomas and astrocytomas both independently, but also related to the WHO grade. Prediction performance was evaluated in leaveone-out-cross validation (LOOCV). Results Oligodendrogliomas showed significantly higher microvascularity (higher rCBVMean ≥ 0.80, p=0.013) and higher vascular heterogeneity (lower rCBVPeak ≤ 0.044, p=0.015) than astrocytomas. Diffuse gliomas with higher cellular density (lower ADCMean ≤ 1094 × 10-6 mm 2 /s, p=0.009) were more likely to be oligodendrogliomas than astrocytomas. Histogram analysis of rCBV and ADC were able to differentiate between diffuse astrocytomas (WHO grade II) and anaplastic astrocytomas (WHO grade III). Conclusion Histogram derived rCBV and ADC parameter may be used as biomarkers for identification of oligodendrogliomas and may help characterize diffuse gliomas based upon their genetic characteristics.

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Section: Discussionmentioning

confidence: 92%

Dynamic susceptibility contrast and diffusion MR imaging identify oligodendroglioma as defined by the 2016 WHO classification for brain tumors: histogram analysis approach

et al. 2019

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“…The probes used to perform FISH were as follows: Vysis LSI 1p36 SpectrumOrange/1q25 SpectrumGreen Probes and Vysis LSI 19q13 SpectrumOrange/ 19p13 SpectrumGreen Probes (Abbott Molecular, Vysis, Des Plaines, IL, USA); Vysis LSI CDKN2A SpectrumOrange/CEP 9 SpectrumGreen Probes (Abbott Molecular); Vysis LSI EGFR SpectrumOrange/CEP 7 SpectrumGreen Probes (Abbott Molecular); Vysis LSI PTEN/CEP 10 Dual Color Probe (Abbott Molecular). Each molecular test was performed and interpreted as previously described [23,24]. Homozygous deletion of the CD-KN2A gene was determined when > 15% of tumor cells lost two test signals in the presence of at least one reference signal in 100 non-overlapping counted nuclei [25].…”

Section: Other Immunohistochemical and Molecular Testing Variablesmentioning

confidence: 99%

The prognostic significance of p16 expression pattern in diffuse gliomas

Park

Kang

Lim

et al. 2021

J Pathol Transl Med

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“…Oligoastr oc y toma (OA) is a subset of brain tumors that present with an appearance of mixed astrocytic and oligodendroglioma glial cell [1]. About 2.3-23 % of all reported gliomas are diagnosed as oligoastrocytoma, the OA incidence rate is 0.16-1.47 cases per 100,000 population per year [2][3][4].…”

Section: Introductionmentioning

confidence: 99%

“…It could be explained by the lack of clear histological criteria for this tumor. Only in 1993 OA was included into the WHO classification of brain tumors [3,5]. No purposeful histological studies of OA on significant material have Ukrainian Neurosurgical Journal pISSN 1810-3154 eISSN 2412-8791…”

Section: Introductionmentioning

confidence: 99%

Heterogeneity of oligoastrocytoma: morphology, surgery, and survival in the series of 163 patients. Retrospective study

Kliuchka

Rozumenko

et al. 2018

Ukr Neurosurg J

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Introduction. The current approach to oligoastrocytoma (OA) treatment includes surgery taking into account the anatomical and physiological accessibility using various radio-and chemotherapy protocols. Nevertheless, it should be recognized that influence of OA histological structure on the surgery of these tumors has not conclusively established.Objective. To improve diagnostic and surgical tactics in oligoastrocytoma by comparing determined clinical-histological patterns. Materials and methods.Retrospective clinical-morphological comparison and analysis of treatment results in 163 patients with OA were performed taking into account histological structure. OAII (WHO) was diagnosed in 32 patients (19.6 %), 131 patients (80.4 %) developed OAIII (WHO). Results. In 52 OA cases (32 %) oligodendroglial component (oOA) prevailed, in 48 OA cases (29 %) astrocytic component (aOA) prevailed, in 63 OA cases (39 %) there was relatively equal cells distribution of both components (оаОА). The surgical treatment of 163 patients included the following: gross total removal, 60 patients (31.4 %); subtotal removal, 98 patients (60.2 %); and partial removal, 4 patients (2.4 %). A total of 106 (65.0 %) patients presented with Karnofsky Performance Status Scale (KPS) ≥ 80. One hundred and fifty-three patients (93.9 %) experienced postsurgery KPS ≥ 80. There was no perioperative death. All 163 patients received radiation therapy and 87 patients (53.4 %) received chemotherapy as well. A significant difference (p< 0.05) in overall survival (OS) was found between surgery results of OA histological groups. Clinical and MRI/CT findings significantly correlated with histological types of OA as well as results of treatment: the overall survival in patients with oOA was 100.5 ± 4.6 months, aOA -48.2 ± 4.5 months, oaOA -76.6 ± 4.9 months, averaging 49.9 ± 2.4 months. Conclusions.Diagnosing, surgery, and survival of OA are determined by the uniqueness of the histological structure of these tumors, the interaction of their components, topography and expansion direction. The key to successful results is a differential approach to planning diagnostic tactics, method of removal and management in late post-op period.

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Reclassification of Mixed Oligoastrocytic Tumors Using a Genetically Integrated Diagnostic Approach

Cited by 3 publications

References 19 publications

Dynamic susceptibility contrast and diffusion MR imaging identify oligodendroglioma as defined by the 2016 WHO classification for brain tumors: histogram analysis approach

Dynamic susceptibility contrast and diffusion MR imaging identify oligodendroglioma as defined by the 2016 WHO classification for brain tumors: histogram analysis approach

The prognostic significance of p16 expression pattern in diffuse gliomas

Heterogeneity of oligoastrocytoma: morphology, surgery, and survival in the series of 163 patients. Retrospective study

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