Pediatric low-grade glioma in the era of molecular diagnostics

Ryall, Scott; Tabori, Uri; Hawkins, Cynthia

doi:10.1186/s40478-020-00902-z

Cited by 240 publications

(297 citation statements)

References 231 publications

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“…The pattern rather corresponds to more aggressive tumor types not identifiable by conventional histologic criteria, up to now. 38,[49][50][51][52][53]…”

Section: Response To Salvage Treatment and Biologymentioning

confidence: 99%

Loss of efficacy of subsequent nonsurgical therapy after primary treatment failure in pediatric low‐grade glioma patients—Report from the German SIOP‐LGG 2004 cohort

Kandels

Pietsch

Bison

et al. 2020

Intl Journal of Cancer

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First-line treatment of pediatric low-grade glioma using surgery, radio-or chemotherapy fails in a relevant proportion of patients. We analyzed efficacy of subsequent surgical and nonsurgical therapies of the German cohort of the SIOP-LGG 2004 study (2004-2012, 1558 registered patients; median age at diagnosis 7.6 years, median observation time 9.2 years, overall survival 98%/96% at 5/10 years, 15% neurofibromatosis type 1 [NF1]). During follow-up, 1078/1558 patients remained observed without (n = 217), with 1 (n = 707), 2 (n = 124) or 3 to 6 (n = 30) tumor volume reductions; 480/1558 had 1 (n = 332), 2 (n = 80), 3 or more (n = 68) nonsurgical treatment-lines, accompanied by up to 4 tumor-reductive surgeries in 215/480; 265/480 patients never underwent any neurosurgical tumor volume reduction (163/265 optic pathway glioma). Patients with progressing tumors after first-line adjuvant treatment were at increased risk of suffering further progressions. Risk factors were young age (<1 year) at start of treatment, tumor dissemination or progression within 18 months after start of chemotherapy. Progression-free survival rates declined with subsequent treatment-lines, yet remaining higher for patients with NF1. In non-NF1-associated tumors, vinblastine monotherapy vs platinum-based chemotherapy was noticeably less effective when used as second-line treatment. Yet, for the entire cohort, results did not favor a certain sequence of specific treatment options. Rather, all can be aligned as a portfolio of choices which need careful balancing of risks and benefits. Future molecular data may predict long-term tumor biology.

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“…The pattern rather corresponds to more aggressive tumor types not identifiable by conventional histologic criteria, up to now. 38,[49][50][51][52][53]…”

Section: Response To Salvage Treatment and Biologymentioning

confidence: 99%

Loss of efficacy of subsequent nonsurgical therapy after primary treatment failure in pediatric low‐grade glioma patients—Report from the German SIOP‐LGG 2004 cohort

Kandels

Pietsch

Bison

et al. 2020

Intl Journal of Cancer

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“…Interestingly, the presence of T-cells within tumors was inversely correlated with the expression of SOX2 ( online supplementary figure 1B ). Although most pediatric LGG share activation of the BRAF-MAPK pathway as a common genomic alteration, 8 the mechanism underlying BRAF activation in PXA/GG is commonly the V600E mutation, while BRAF-KIAA1549 fusion is observed in PAs. 8 T-cells against driver mutations have been limited in some settings, presumably due to selection based on HLA genotype.…”

Section: Resultsmentioning

confidence: 99%

“…Although most pediatric LGG share activation of the BRAF-MAPK pathway as a common genomic alteration, 8 the mechanism underlying BRAF activation in PXA/GG is commonly the V600E mutation, while BRAF-KIAA1549 fusion is observed in PAs. 8 T-cells against driver mutations have been limited in some settings, presumably due to selection based on HLA genotype. 21 In order to test whether the BRAF V600E mutation could be immunogenic in pediatric tumors, we synthesized peptides encompassing this mutation and used these to detect and expand BRAF V600E -specific T-cells in culture.…”

Section: Resultsmentioning

confidence: 99%

Subtype and grade-dependent spatial heterogeneity of T-cell infiltration in pediatric glioma

Robinson

Vasquez

Kaushal

et al. 2020

J Immunother Cancer

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Brain tumors are the leading cause of cancer-related mortality in children and have distinct genomic and molecular features compared with adult glioma. However, the properties of immune cells in these tumors has been vastly understudied compared with their adult counterparts. We combined multiplex immunofluorescence immunohistochemistry coupled with machine learning and single-cell mass cytometry to evaluate T-cells infiltrating pediatric glial tumors. We show that low-grade tumors are characterized by greater T-cell density compared with high-grade glioma (HGG). However, even among low-grade tumors, T-cell infiltration can be highly variable and subtype-dependent, with greater T-cell density in pleomorphic xanthoastrocytoma and ganglioglioma. CD3+ T-cell infiltration correlates inversely with the expression of SOX2, an embryonal stem cell marker commonly expressed by glial tumors. T-cells within both HGG and low-grade glioma (LGG) exhibit phenotypic heterogeneity and tissue-resident memory T-cells consist of distinct subsets of CD103+ and TCF1+ cells that exhibit distinct spatial localization patterns. TCF1+ T-cells are located closer to the vessels while CD103+ resident T-cells reside within the tumor further away from the vasculature. Recurrent tumors are characterized by a decline in CD103+ tumor-infiltrating T-cells. BRAFV600E mutation is immunogenic in children with LGG and may serve as a target for immune therapy. These data provide several novel insights into the subtype-dependent and grade-dependent changes in immune architecture in pediatric gliomas and suggest that harnessing tumor-resident T-cells may be essential to improve immune control in glioma.

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“…Pediatric low-grade neuroepithelial tumors (P-LGNTs) encompass a group of central nervous system neoplasms that includes long-term epilepsy-associated tumors (LEATs), such as ganglioglioma and dysembryoplastic neuroepithelial tumor (DNT). P-LGNTs have different characteristics than their adult counterparts, and are commonly driven by genomic alterations in the Ras/mitogen-activated protein kinase (MAPK) pathway, such as mutations in BRAF and NF - 1 [ 23 , 29 ]. Recent large-scale genomic studies and genome-wide methylation analyses allowed a thorough characterization of P-LGNTs [ 24 ], and cIMPACT-NOW (the Consortium to Inform Molecular and Practical Approaches to CNS Tumor Taxonomy) currently classifies P–LGNTs as distinct disease entities [ 4 , 17 ].…”

Section: Introductionmentioning

confidence: 99%

BRAF V600E mutation mediates FDG-methionine uptake mismatch in polymorphous low-grade neuroepithelial tumor of the young

Tateishi

Ikegaya

Udaka

et al. 2020

acta neuropathol commun

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We present a case of a 14-year old boy with tumor-associated refractory epilepsy. Positron emission tomography imaging demonstrated a region with heterogeneous high 11C-methionine uptake and a region with homogenous low 18F-fluorodeoxyglucose uptake within the tumor. Histopathological and genomic analyses confirmed the tumor as BRAF V600E-mutated polymorphous low-grade neuroepithelial tumor of the young (PLNTY). Within the high-methionine-uptake region, we observed increased protein levels of L-type amino acid transporter 1 (LAT1), a major transporter of methionine; c-Myc; and constituents of the mitogen-activated protein kinase (MAPK) pathway. We also found that LAT1 expression was linked to the BRAF V600E mutation and subsequent activation of MAPK signaling and c-Myc. Pharmacological and genetic inhibition of the MAPK pathway suppressed c-Myc and LAT1 expression in BRAF V600E-mutated PLNTY and glioblastoma cells. The BRAF inhibitor dabrafenib moderately suppressed cell viability in PLNTY. Collectively, our results indicate that BRAF V600E mutation-activated MAPK signaling and downstream c-Myc induces specific metabolic alterations in PLNTY, and may represent an attractive target in the treatment of the disease.

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Pediatric low-grade glioma in the era of molecular diagnostics

Cited by 240 publications

References 231 publications

Loss of efficacy of subsequent nonsurgical therapy after primary treatment failure in pediatric low‐grade glioma patients—Report from the German SIOP‐LGG 2004 cohort

Loss of efficacy of subsequent nonsurgical therapy after primary treatment failure in pediatric low‐grade glioma patients—Report from the German SIOP‐LGG 2004 cohort

Subtype and grade-dependent spatial heterogeneity of T-cell infiltration in pediatric glioma

BRAF V600E mutation mediates FDG-methionine uptake mismatch in polymorphous low-grade neuroepithelial tumor of the young

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