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1 r distance-dependent manner in patients with glioma.
2 s like esophageal squamous-cell carcinoma or glioma.
3 effects by mainly activating mTOR pathway in Glioma.
4 ciated with favourable outcome in high-grade glioma.
5 reprogramming may be a fundamental driver of glioma.
6 dehydrogenase (IDH) status in patients with glioma.
7 as a powerful therapeutic tool for treating glioma.
8 ssessment criteria for paediatric high-grade glioma.
9 and chemoresistant diffuse intrinsic pontine glioma.
10 HG and tumor metabolism in IDH-mutated human glioma.
11 nse to temozolomide treatment in mutant IDH1 glioma.
12 malignant clinical and molecular subtypes of glioma.
13 aluable imaging marker for IDH-mutated human glioma.
14 te with integrin alpha6 in patient malignant glioma.
15 ide support for cancer stem cell theories of glioma.
16 ated NTRK2 splice variant, TrkB.T1, in human glioma.
17 ompared with 14 of 31 (45.2%) with enhancing glioma.
18 rognosis and is the most aggressive grade of glioma.
19 nd management of adult patients with diffuse gliomas.
20 awn to differentiate grade II from grade III gliomas.
21 maging methods used to diagnose and classify gliomas.
22 as a robust biomarker for poor prognosis in gliomas.
23 ik3ca(H1047R) to generate high-grade diffuse gliomas.
24 e and CCR2 inhibition in anti-PD-1-resistant gliomas.
25 and follow-up of adult patients with diffuse gliomas.
26 may result in a worse prognosis for IDH(wt) gliomas.
27 are consumed in relatively large amounts by gliomas.
28 tial therapeutic target for the treatment of gliomas.
29 Altered cellular metabolism is a hallmark of gliomas.
30 response assessment in paediatric low-grade gliomas.
31 al outcomes in 56 patients with WHO grade IV gliomas.
32 e use of Ras pathway inhibitors in low-grade gliomas.
33 composition and gene regulation in malignant gliomas.
34 f mutational burden and signatures in 10,294 gliomas.
35 RNA-21 (miR-21) as a prognostic biomarker in gliomas.
36 patients diagnosed with high-risk low-grade gliomas.
37 trophic tyrosine receptor kinases (NTRKs) in gliomas.
38 rol samples from different mouse models with gliomas.
39 well as methylation-based classification of gliomas.
40 trials and clinical practice for high-grade gliomas.
41 ity within the first 2 wk after resection of gliomas.
42 o identify cancer stem cells in leukemia and gliomas.
43 tions with overall survival for only IDH(wt) gliomas.
44 is closely associated with highly malignant gliomas.
45 l burden (hypermutation) is observed in some gliomas(1-5); however, the mechanisms by which hypermuta
46 with white matter in both participants with glioma (2.36 mumol/g/min +/- 0.22 vs 0.75 mumol/g/min +/
47 _INST: 17 patients, 17 lesions, 10 low-grade glioma, 3 cavernoma, 4 focal cortical dysplasia; NEL_INS
49 d), the classification accuracy was 40 of 49 gliomas (82%; 95% CI: 71%, 92%) for model A and 42 of 49
51 Methods: Forty-three patients with cerebral gliomas (9 low-grade, 34 high-grade; 9 primary tumors, 3
52 rty of 35 patients (85.7%) with nonenhancing glioma achieved stable disease compared with 14 of 31 (4
54 induced pig model of high-grade spinal cord glioma and may potentially be used in preclinical therap
56 +/- 18 [standard deviation]; nine men) with glioma and three healthy volunteers (mean age, 44 years
57 young adults with diffuse intrinsic pontine glioma and to develop a consensus on recommendations for
59 cancers, including low-grade and high-grade gliomas and brain metastases (BrMs) originating from div
61 ptember 2018, participants with IDH1-mutated gliomas and healthy participants were prospectively scan
63 inine/valine (G34R/V) mutations drive deadly gliomas and show exquisite regional and temporal specifi
64 ion and increased EGFR expression in primary glioma, and employ a glioma cell line LN229 to identify
65 tures that are distinct from adult low-grade gliomas, and the developing paediatric brain is more sus
71 te the immunosuppressive properties of human gliomas are essential to assess immune-based therapies.
78 diologist-FISH discordances, there were nine gliomas associated with a consensus neuroradiologist con
80 hile the dramatic heterogeneity of malignant gliomas at the genetic and immunological levels remains
81 ed median survival as a monotherapy in KR158 glioma-bearing animals and further increased median and
85 and lactate in the brains of unaffected and glioma-bearing rats following the administration of (2)H
87 -GFP), VSV-EBOVDeltaMLD without GFP targeted glioma but yielded only a modest extension of survival.
88 oncohistone, occurring frequently in midline gliomas but also identified in haematopoietic malignanci
90 in isocitrate dehydrogenase 1-mutated human glioma by using a super-resolution framework to upsample
91 prehensive functional characterization of 96 gliomas by genome-wide piggyBac insertional mutagenesis
92 ardiac glycosides in human glioblastomas and glioma cancer stem-like cells via inhibition of DNA repa
95 oint to a novel role of C4S and C6S in human glioma cell functions, thus possibly representing target
96 lating p120-catenin further prevents diffuse glioma cell infiltration of the mouse brain with margina
97 r goal is to study how the morphology of the glioma cell influences the formation of patterns of coll
98 R expression in primary glioma, and employ a glioma cell line LN229 to identify relevant proteins and
100 ates with susceptibility to this drug across glioma cell lines, revealing ribosomal protein subunit R
103 latory element in the HOTAIR locus increases glioma cell sensitivity to TMZ and alters transcription
106 nerated some of these MGMT rearrangements in glioma cells and demonstrated that the MGMT genomic rear
107 o rat models of glioblastoma (GBM; U87 human glioma cells and patient-derived human glioblastoma canc
110 at mutant isocitrate-dehydrogenase (mIDH)1/2 glioma cells convert alpha-KG to D-2-hydroxyglutarate (D
113 ular cross-sectional area) and tracked human glioma cells that spontaneously migrated within channels
115 come both BBB and multidrug resistance (MDR) glioma cells while providing site-specific magnetic targ
117 proliferation of primary adult and pediatric glioma cells, but not the viability of normal brain cell
118 s obtained by overexpression of GLS2 in T98G glioma cells, including downregulation of oncogene c-Myc
119 stand the dynamic nature of brain tumors and glioma cells, including their invasion of normal brain.
121 In healthy volunteers and participants with glioma, CMRO(2) values in gray matter and white matter v
122 icantly lower MTR(asym) in 1p/19q co-deleted gliomas (co-deleted, 1.17% +/- 0.32%; non-co-deleted, 1.
123 Cox concordance index of ~ 0.85 for the TCGA glioma cohort, however, the gene-level model has twice a
125 (MEGENA), were applied on publicly available glioma, control brain and stem cell gene expression RNA-
127 nalysis of the miR-21 expression in the TCGA glioma dataset revealed that overexpression of miR-21 wa
128 ysis to assess miR-21 expression in the TCGA glioma dataset to validate the relationship between miR-
129 y chromatin regulatory pathways disrupted in gliomas, delineating their physiological function and ou
130 of this study was to explore the effects of glioma development and Temozolomide (TMZ) on fecal micro
135 r the treatment of diffuse intrinsic pontine glioma (DIPG), an aggressive pediatric cancer resident i
139 road map for the discovery of potential new glioma drug targets is suggested, with the goal of trans
140 T as a direct metabolic imaging technique in glioma enabled quantitative visualization of the Warburg
141 been observed in various cancers, including glioma, endometrial cancer, ovarian cancer, and breast c
142 nomic analysis provides unique insights into glioma etiology and the chronology of glioma-causing som
145 tions for the management of adult high-grade glioma, for paediatrics there is inclusion of diffusion-
146 he management of adult patients with diffuse gliomas, for patients and caregivers, and for health-car
150 iptome data, including data from the Chinese Glioma Genome Atlas RNAseq, the Cancer Genome Atlas RNAs
151 ting of associations between ADC metrics and glioma genotypes, including Bonferroni correction for mu
154 ics and immune escape signature by comparing glioma growth in immunocompetent versus immunodeficient
157 ng of innate and adaptive responses inhibits glioma growth, but also activates immune checkpoint.
158 e of neurons and immune cells in controlling glioma growth, relevant to future therapeutic targeting.
159 Clinical trials of treatments for high-grade gliomas have traditionally relied on measures of respons
160 rvival or clinical benefit, with the complex glioma heterogeneity often being the reason to blame.
162 (TMZ) is a frequently used chemotherapy for glioma; however, chemoresistance is a major problem limi
168 antly recurrent somatic alterations in these gliomas including mutant EGFR amplifications and Sub1, T
175 between the increased survival in low-grade glioma (LGG) and complementarity of IDH1 mutants to the
177 roglioma is an important type of lower-grade glioma (LGG), which is a slowly progressing brain tumor.
178 anging study for patients with WHO low-grade glioma (LGG, grade II), as it was the first to demonstra
181 ch into neuropsychiatric disease and cancer, gliomas may be expected to localize to brain regions cha
182 Results Data in a total of 45 patients with glioma (mean age, 51.3 years +/- 14.3 [standard deviatio
183 Results Three participants with IDH1-mutated gliomas (mean age, 50 years +/- 21 [standard deviation];
185 goal of translating these new insights about glioma metabolism into clinical benefits for patients.
186 tifies isocitrate dehydrogenase (IDH)-mutant gliomas misassigned to 1p/19q codeletion status with FIS
187 t the production of a high-grade spinal cord glioma model in pigs using lentiviral gene transfer.
191 tends survival in clinically relevant murine glioma models and provides the basis on which to advance
193 hatase and tensin homologue (PTEN)-deficient glioma mouse models, mRNA-containing exosomes restored t
195 id tumors (n = 229) and pediatric high-grade gliomas (n = 401), we show significant associations with
197 populated with putative cells of origin for glioma, neural stem cells and oligodendrocyte precursor
199 d on their expression in adult and pediatric gliomas, nine of these hits are prioritized as lncRNA Gl
200 Results: For IDH(wt) and IDH(m-noncodel) gliomas, nSUV demonstrated significant positive correlat
201 us in World Health Organization grade II/III gliomas on the basis of standard clinical MRI sequences
202 atosis type 1 (NF1)-associated optic pathway gliomas (OPGs) and a follow-up period of at least 10 yea
206 allenge in follow-up of diffuse infiltrating gliomas, particularly high grade, which leads to a poten
210 diagnosed and histomolecularly characterized glioma patients (glioblastoma, 90%; age range, 20-79 y)
212 e ((18)F-FET) PET for response assessment in glioma patients after adjuvant temozolomide chemotherapy
215 the effect of TET1 expression on survival in glioma patients using open-access data from the Genomic
218 ient data identified as diffuse infiltrating glioma patients whose disease progressed/recurred were u
226 as significantly associated with worse OS in glioma patients; for the other study, which provided dat
227 showed high similarity with human pediatric gliomas per robust aneuploidy, mutational rates, relativ
231 enase (IDH) mutations are highly frequent in glioma, producing high levels of the oncometabolite D-2-
233 hesis that glutamine may be a key marker for glioma progression and indicate that inflammation is ass
234 cells and their microenvironment to promote glioma progression, and it is also a potential therapeut
238 t and the injected dose of gadopiclenol in a glioma rat model compared with those of conventional GBC
239 ril and July 2012, 32 rats implanted with C6 glioma received two intravenous injections at a 24-hour
242 lighted, providing important clues as to how gliomas respond to and adapt to their changing tissue an
243 utamine metabolism and inflammation in human glioma samples and explore the use of glutamine as a pot
248 microsatellite instability in MMR-deficient gliomas, single-cell whole-genome sequencing analysis of
250 IL-33 expression in a large subset of human glioma specimens and murine models correlates with incre
252 poxia by a simple isoform switch to regulate glioma stem cell self-renewal, tumorigenicity, and progr
254 lastoma (GBM), maintains stem-like features (glioma stem cell, GSC) through hypoxia-induced responses
257 shift towards mesenchymal cellular state of glioma stem cells, promoting both invasive and prolifera
260 iptomic profiles defined four transcriptomic glioma subgroups with 91.4% concordance with the WHO-def
262 alterations shared between canine and human gliomas such as the receptor tyrosine kinases, TP53 and
264 ven by MMR defects in chemotherapy-sensitive gliomas that recur after treatment with the chemotherapy
270 resonance spectra were acquired from ex vivo glioma tissue (n = 16, grades II-IV) to quantify metabol
271 omas with those of human pediatric and adult gliomas to characterize evolutionarily conserved mammali
272 ifier confidently classified all but 17 TCGA gliomas to one of the four transcriptomic profile (TP) g
275 ains bromodomain-containing protein BRD9 and glioma tumor suppressor candidate region 1 (GLTSCR1) or
277 n signaling axis as a critical mechanism for glioma tumorigenesis that may serve as a new therapeutic
278 (v)beta(3), moderate in alpha(5)beta(1)) and glioma U87MG (very high in alpha(v)beta(3), moderate/hig
279 functional driver landscapes of EGFR-mutant gliomas, uncovering potential therapeutic strategies, an
280 resents a non-invasive analysis of low-grade gliomas using imaging features based on the updated clas
281 Response criteria for paediatric high-grade glioma vary historically and across different cooperativ
283 ome, and methylation sequencing of 83 canine gliomas, we found alterations shared between canine and
284 s that confer susceptibility to this drug in gliomas, we performed a genome-scale CRISPR knockout scr
289 f post-mortem gene expression, we found that gliomas were localized to brain regions enriched with ex
290 s demonstrated in a patient with mutant-IDH1 glioma where it enables imaging of D-2-hydroxyglutarate
294 r molecular testing should be considered for gliomas with discordant neuroimaging and FISH results.
295 es a robust and objective method to classify gliomas with high agreement to the current WHO guideline
297 We compared the molecular profiles of canine gliomas with those of human pediatric and adult gliomas
299 ents from five institutions with lower-grade gliomas (World Health Organization grade II and III) wer
300 Data in patients with IDH-mutant lower-grade gliomas (World Health Organization grade II/III) and 1p/