| Literature DB >> 27300198 |
Günther Grabner1,2,3, Barbara Kiesel2,4, Adelheid Wöhrer2,5, Matthias Millesi2,4, Aygül Wurzer2,4, Sabine Göd1, Ammar Mallouhi2,6, Engelbert Knosp2,4, Christine Marosi2,7, Siegfried Trattnig1,2, Stefan Wolfsberger2,4, Matthias Preusser2,7, Georg Widhalm8,9.
Abstract
OBJECTIVES: To investigate the value of local image variance (LIV) as a new technique for quantification of hypointense microvascular susceptibility-weighted imaging (SWI) structures at 7 Tesla for preoperative glioma characterization.Entities:
Keywords: 7 Tesla MRI; Diffusely infiltrating gliomas; Glioma characterization; Local image variance; Susceptibility-weighted imaging
Mesh:
Year: 2016 PMID: 27300198 PMCID: PMC5334387 DOI: 10.1007/s00330-016-4451-y
Source DB: PubMed Journal: Eur Radiol ISSN: 0938-7994 Impact factor: 5.315
Patients’ characteristics
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|---|---|---|---|
| number of patients | 30 | (100) | |
| gender | male : female | 1 : 1.5 | |
| age (years) | median (range) | 51 years (21 - 78) | |
| localization | frontal | 10 | (34) |
| insular | 5 | (17) | |
| temporal | 4 | (14) | |
| parietal | 3 | (10) | |
| central | 3 | (10) | |
| occipital | 1 | (3) | |
| trigonal | 1 | (3) | |
| brainstem | 1 | (3) | |
| thalamus | 1 | (3) | |
| corpus callosum | 1 | (3) | |
| MRI contrast - enhancement | |||
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| ring-like | 11 | (36) |
| nodular | 2 | (7) | |
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| none | 12 | (40) |
| patchy/faint | 3 | (10) | |
| focal | 2 | (7) | |
| type of surgery | resection | 19 | (64) |
| stereotactic biopsy | 10 | (33) | |
| open biopsy | 1 | (3) | |
| target for iOP tumour sampling | |||
| MR CE | 13 | (43) | |
| PET | 15 | (50) | |
| CSI | 2 | (7) | |
| diagnosis | |||
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| glioblastoma | 12 | (40) |
| gliosarcoma | 1 | (3) | |
| anaplastic astrocytoma | 5 | (18) | |
| anaplastic oligodendroglioma ( | 2 | (7) | |
| mixed oligoastocytoma ( | 1 | (3) | |
|
| oligodendroglioma | 4 | (13) |
| diffuse astrocytoma | 4 | (13) | |
| mixed oligoastocytoma ( | 1 | (3) | |
| IDH1 mutational status | |||
| IDH1-R132H negative tumour | 15 | (50) | |
| IDH1-R132H positive tumour | 15 | (50) | |
CE contrast - enhancement; CSI chemical shift imaging; HGG high-grade gliomas; iOP intraoperative, LGG low-grade gliomas, MR magnetic resonance imaging, PET positron emission tomography, WHO World Health Organization; IDH1 isocitrate dehydrogenase 1
Fig. 1Illustration of the SWI - local image variance (LIV) calculation. (A) The left image shows a simulation of blood vessels (hypointense structures on a hyperintense background) as typically detected by SWI. As illustrated in this image, the density of these simulated blood vessels increases from the left to the right. Such an increasing density of blood vessels is typically observed in high-grade gliomas. (B) The right image illustrates the corresponding colour-coded SWI-LIV map, where LIV values increase with the density of blood vessels. The LIV values reach their maximum in the area with the highest density of the blood vessels. Note, the simulated SWI image (left image) is a binary image and includes only the values 0 and 1, resulting in SWI-LIV values that are not comparable to patient data
Fig. 3Representative case of a HGG with negative IDH1-R132H mutational status. (A) Preoperative axial T2-weighted MR images and (B) contrast-enhanced T1-weighted sequences show a hyperintense lesion in the posterior portion of the corpus callosum with significant (ring-like) CE. (C) 7 Tesla SWI detects markedly increased intratumoral hypointense structures. (D) The 7 Tesla SWI is overlaid with the corresponding SWI-LIV map. The colour-coded SWI-LIV map in this glioma shows high values (mean SWI-LIV: 135.7) for areas with a high variability that correspond probably to intratumoral regions with high amounts of pathological microvessels and microhaemorrhages. It is of note that the area, where LIV values are shown, represents the segmented tumour ROI. (E) Histopathological examination reveals a HGG (GBM; WHO grade IV) with (F) negative IDH1-R132H mutational status. Original magnification of the H&E stain (E) and IDH1-R132H stain (F) is × 200
Fig. 4Representative case of a LGG with positive IDH1-R132H mutational status. (A) Preoperative axial T2-weighted MR images and (B) contrast-enhanced T1-weighted sequences demonstrate a left frontal hyperintense lesion with non-significant (patchy/faint) CE. (C) 7 Tesla SWI detects only very few hypointense structures and (D) the corresponding colour-coded SWI-LIV map shows low values in the tumour ROI (mean SWI-LIV: 32.2). (E) Histopathological examination reveals a LGG (diffuse astrocytoma WHO grade II) with (F) positive IDH1-R132H mutational status. Original magnification of the H&E stain (E) and IDH1-R132H stain (F) is × 200
Fig. 5Preoperative identification of early malignant transformation in an initially suspected LGG on conventional MRI. (A) Preoperative axial T2-weighted MR images and (B) contrast-enhanced T1-weighted sequences reveal a left frontal hyperintense lesion with non-significant (none) CE. (C) Although no CE is visible on conventional MRI, 7 Tesla SWI depicts markedly increased intratumoural hypointense structures and (D) the corresponding colour-coded SWI-LIV map shows high values in the tumour ROI (mean SWI-LIV: 82.0). (E) Histopathological examination depicts already a HGG (anaplastic oligodendroglioma WHO grade III) with a (F) markedly increased proliferation rate (MIB-1 labelling index: 30 %). Original magnification of the H&E stain (E) and anti–Ki 67 stain (F) is × 200
Correlation of SWI-LIV with the WHO tumour grade, IDH1 mutational status, and type of contrast-enhancement on MRI
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| SWI-LIV |
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| WHO grade | ||||
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| 30.8 | 16.3 |
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| 92.7 | 57.2 | |
| IDH1-R132H mutational status | ||||
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| 38.3 | 21.1 |
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| 109.9 | 57.9 | |
| CE on MRI | ||||
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| 39.0 | 20.4 |
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| 120.1 | 55.2 | |
CE contrast enhancement, HGG high-grade gliomas, IDH1 isocitrate dehydrogenase 1, LGG low-grade gliomas, MRI magnetic resonance imaging, SD standard deviation, SWI susceptibility weighted imaging, WHO World Health Organization
Fig. 2Boxplot diagrams for comparison of SWI-LIV values with tumour grade, IDH1-R132H mutational status and type of CE on MRI. (A) SWI-LIV and tumour grade: The mean SWI-LIV was significantly higher in HGG as compared to LGG (92.7 versus 30.8; p < 0.0001). (B) SWI-LIV and IDH1-R132H mutational status: The mean SWI-LIV was significantly higher in IDH1-R132H negative gliomas as compared to IDH1-R132H positive gliomas (109.9 versus 38.3; p < 0.0001). (C) SWI-LIV and type of CE on MRI: The mean SWI-LIV was significantly higher in gliomas with significant CE as compared to non-significant CE (120.1 versus 39.0; p < 0.0001)