EGFRvIII expression and isocitrate dehydrogenase mutations in patients with glioma

Taher, Mohiuddin M.; Dairi, Ghida; Butt, Ejaz; Alquthami, Khalid; Alkhalidi, Hisham; Jastania, Raid A; Nageeti, T.; Bogari, Neda M.; Athar, Mohammad; Al‐Allaf, Faisal A.; Valerie, Kristoffer

doi:10.3892/ol.2020.12247

Cited by 3 publications

(5 citation statements)

References 67 publications

(100 reference statements)

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“…They can be targeted by the genetically modified chimeric antigen receptor (CAR) T cells or oncolytic viral therapy, in which viruses are genetically engineered in order to selectively infect and replicate in tumor cells, therefore resulting in not only cellular lysis, but also the activation of immunogenic cell death pathways [118,119]. Even if EGFRvIII is mostly associated with IDH-wildtype gliomas, there are some cases in which IDH mutation and EGFRvIII are found together [120,121]. Alternatively, PDGFRA, which is known to be upregulated in IDH-mutant gliomas [122], has recently been shown to be targeted by CAR T cell therapy in other cancer types [123].…”

Section: Car T Cell Therapymentioning

confidence: 99%

IDH Mutations in Glioma: Double-Edged Sword in Clinical Applications?

2021

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Discovery of point mutations in the genes encoding isocitrate dehydrogenases (IDH) in gliomas about a decade ago has challenged our view of the role of metabolism in tumor progression and provided a new stratification strategy for malignant gliomas. IDH enzymes catalyze the conversion of isocitrate to alpha-ketoglutarate (α-KG), an intermediate in the citric acid cycle. Specific mutations in the genes encoding IDHs cause neomorphic enzymatic activity that produces D-2-hydroxyglutarate (2-HG) and result in the inhibition of α-KG-dependent enzymes such as histone and DNA demethylases. Thus, chromatin structure and gene expression profiles in IDH-mutant gliomas appear to be different from those in IDH-wildtype gliomas. IDH mutations are highly common in lower grade gliomas (LGG) and secondary glioblastomas, and they are among the earliest genetic events driving tumorigenesis. Therefore, inhibition of mutant IDH enzymes in LGGs is widely accepted as an attractive therapeutic strategy. On the other hand, the metabolic consequences derived from IDH mutations lead to selective vulnerabilities within tumor cells, making them more sensitive to several therapeutic interventions. Therefore, instead of shutting down mutant IDH enzymes, exploiting the selective vulnerabilities caused by them might be another attractive and promising strategy. Here, we review therapeutic options and summarize current preclinical and clinical studies on IDH-mutant gliomas.

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Section: Car T Cell Therapymentioning

confidence: 99%

IDH Mutations in Glioma: Double-Edged Sword in Clinical Applications?

2021

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“…Compared with the Ion AmpliSeq Comprehensive Cancer Panel and Ion AmpliSeq Cancer HotSpot Panel, the custom panel used in the present NGS analysis (Ion AmpliSeq Cancer Panel v1) contains primers for only 46 genes, as shown in Table 1 . The IDH1 intronic mutation (c.414+9T>A) was previously reported in this HBL tumor by us; however, no missense mutations were detected in IDH1 and IDH2 genes in this tumor [ 28 ]. Ion AmpliSeq™ Cancer Panel v1 contains the primers for the VHL gene; however, no VHL mutations were detected in this tumor.…”

Section: Discussionmentioning

confidence: 85%

“…4471262) consists of 50 oncogenes and tumor suppressor genes that are frequently mutated in several types of cancers. The mutation profiling of a-CPP, MPE, and other brain tumors was reported in previous studies using these custom gene panels on the Ion Proton instrument [ 20 - 23 , 28 ]. Compared with the Ion AmpliSeq Comprehensive Cancer Panel and Ion AmpliSeq Cancer HotSpot Panel, the custom panel used in the present NGS analysis (Ion AmpliSeq Cancer Panel v1) contains primers for only 46 genes, as shown in Table 1 .…”

Section: Discussionmentioning

confidence: 99%

“…for further mutation identification. The VCF file data were analyzed using Ion Reporter v5.18.4.0 (Thermo Fisher Scientific, Inc.), which calculated allele coverage, allele frequency, allele ratio, variant impact, clinical significance, Polymorphism Phenotyping v2 (PolyPhen-2) score, Phred score, Sorting Intolerant from Tolerant (SIFT) score, Grantham score, and Functional Analysis Through Hidden Markov Models (FATHMM) score [ 22 , 28 ]. The PolyPhen-2 score predicts the potential impact of substitution in the variant on the structural and functional aspects of the protein.…”

Section: Case Presentationmentioning

confidence: 99%

“…True mutations were considered based on a Phred quality score >20 and mutations with a p‑value <0.05 were considered significant. Variants that do not fall into this criterion were filtered out [ 22 , 28 ].…”

Section: Case Presentationmentioning

confidence: 99%

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Supratentorial Sporadic Hemangioblastoma: A Case Report With Mutation Profiling Using Next-Generation DNA Sequencing

Taher¹,

Bantan²,

Alwalily³

et al. 2023

Cureus

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The present study aimed to determine genomic changes in sporadic intracranial hemangioblastoma (HBL), and the mutation patterns were analyzed using next-generation DNA sequencing (NGS). In this NGS analysis of the HBL tumor, 67 variants of 41 genes were identified. Of these, 64 were single-nucleotide variants (SNVs), two were exonic insertions and deletions (INDEL), and one was an intronic INDEL. In total, 15 were missense exonic variants, including an insertion variant in the NRAS gene, c.1_2insA, and a deletion variant, c.745delT, in the HNF1A gene, both of these mutations produced a termination codon. Other exonic missense variants found in the tumor were CTNNB1 , FGFR3 , KDR , SMO , HRAS , RAI1 , and a TP53 variant (c.430C>G). Moreover, the results of the present study revealed a novel variant, c.430C>G, in TP53 and two missense variants of SND1 (c.1810G>C and c.1814G>C), which were also novel. ALK (rs760315884) and FGFR2 (rs1042522) missense variants were reported previously. Notably, a total of 10 previously reported single-nucleotide polymorphisms (SNPs) were found in this tumor in genes including MLH1 (rs769364808), FGFR3 (rs769364808), two variants (rs1873778 and rs2228230) in PDGFRA , KIT (rs55986963), APC (rs41115), and RET (rs1800861). The results of this study revealed a synonymous mutation (SNP) in c.1104 G>T; p. (Ser368Ser) in the MLH1 gene. In this amino acid (AA) codon, two other variants are also known to cause missense substitutions, c.1103C>G; p. (Ser368Trp); COSM6986674) and c.1103C>T; p.(Ser368Leu; COSM3915870), were found in hematopoietic and urinary tract tissue, respectively. However, three SNPs found in genes such as ALK , KDR , and ABL1 in the HBL tumor in this study were not reported in UCSC, COSMIC, and ClinVar databases. Additionally, 19 intronic variants were identified in this tumor. One intronic SNV was present in each of the following genes: EGFR , ERBB4 , KDR , SMO , CDKN2B , PTEN , PTPN11 , RB1 , AKT1 , and ERBB2 . In PIK3CA and FBXL18 genes, two intronic variants were present, and in the SND1 gene, three intronic variants were detected in the HBL tumor presented in this study. Notably, only one of these was reported in the catalog of somatic mutations in canc...

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