Germline and somaticNF1 gene mutation spectrum in NF1-associated malignant peripheral nerve sheath tumors (MPNSTs)

Upadhyaya, Meena; Kluwe, Lan; Spurlock, Gillian; Monem, Bisma Qamar; Majounie, Elisa; Mantripragada, Kiran Kumar; Ruggieri, Martino; Chuzhanova, Nadia; Evans, D. Gareth; Ferner, Rosalie E.; Thomas, Nicholas Stuart Tudor; Guha, Abhijit; Mautner, Victor

doi:10.1002/humu.20601

Cited by 105 publications

(103 citation statements)

References 57 publications

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“…17,18 Indeed, three of the somatic NF1 mutations characterised here (p.R816X, p.R304X, p.L1569X) have previously been identified as somatic lesions (two of these three mutations are CpG located and therefore compatible with a mechanism of methylation-mediated deamination of 5-methylcytosine) in both benign and malignant tumours. [41][42][43][44][45][46] A total of seven novel somatic NF1 missense mutations were identified during the course of this study.…”

Section: Discussionmentioning

confidence: 70%

“…47 In our study, MLPA analysis succeeded in identifying only a single intragenic deletion in one neurofibroma, indicating that mitotic recombination was the likely mechanism for LOH in the remaining 24 neurofibromas. Our previous studies found significantly higher levels (approximately 70 and 90%, respectively) of NF1-associated LOH in both PNFs and MPNSTs, 17,18 an indication that NF1-LOH may be less prominent in benign neurofibromas than in PNFs and malignant tumours. One potential confounding factor here is cellular heterogeneity, but we do not consider that this would have substantially hampered the detection of intragenic deletions and duplications by MLPA in this study.…”

Section: Discussionmentioning

confidence: 75%

“…10,11 Currently, our understanding of the biological mechanisms underlying NF1 tumourigenesis is rather limited, although recent studies in mouse have (i) confirmed a direct role for the tumour microenvironment and (ii) identified skin-derived precursor cells as the cell of origin for cutaneous neurofibromas. 12 In studies of NF1 patients, somatic mutations affecting a number of other tumour suppressor genes, including TP53, CDKN2A and RB1 (variously involved in cell cycle regulation, DNA synthesis and apoptosis), have also been identified in MPNSTs, [13][14][15][16][17] PNFs 18,19 and those cutaneous neurofibromas that have been removed from NF1 patients who carry a particularly high tumour burden. 20 It is currently unclear (i) why some types of neurofibroma are present from birth, whereas others develop only during adolescence, (ii) what initiates neurofibroma growth and (iii) what determines the number of tumours that develop in a given individual.…”

Section: Introductionmentioning

confidence: 99%

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Exploring the somatic NF1 mutational spectrum associated with NF1 cutaneous neurofibromas

et al. 2011

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Neurofibromatosis type-1 (NF1), caused by heterozygous inactivation of the NF1 tumour suppressor gene, is associated with the development of benign and malignant peripheral nerve sheath tumours (MPNSTs). Although numerous germline NF1 mutations have been identified, relatively few somatic NF1 mutations have been described in neurofibromas. Here we have screened 109 cutaneous neurofibromas, excised from 46 unrelated NF1 patients, for somatic NF1 mutations. NF1 mutation screening (involving loss-of-heterozygosity (LOH) analysis, multiplex ligation-dependent probe amplification and DNA sequencing) identified 77 somatic NF1 point mutations, of which 53 were novel. LOH spanning the NF1 gene region was evident in 25 neurofibromas, but in contrast to previous data from MPNSTs, it was absent at the TP53, CDKN2A and RB1 gene loci. Analysis of DNA/RNA from neurofibroma-derived Schwann cell cultures revealed NF1 mutations in four tumours whose presence had been overlooked in the tumour DNA. Bioinformatics analysis suggested that four of seven novel somatic NF1 missense mutations (p.A330T, p.Q519P, p.A776T, p.S1463F) could be of functional/clinical significance. Functional analysis confirmed this prediction for p.S1463F, located within the GTPase-activating protein-related domain, as this mutation resulted in a 150-fold increase in activated GTP-bound Ras. Comparison of the relative frequencies of the different types of somatic NF1 mutation observed with those of their previously reported germline counterparts revealed significant (P¼0.001) differences. Although non-identical somatic mutations involving either the same or adjacent nucleotides were identified in three pairs of tumours from the same patients (Po0.0002), no association was noted between the type of germline and somatic NF1 lesion within the same individual.

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Section: Discussionmentioning

confidence: 70%

Section: Discussionmentioning

confidence: 75%

Section: Introductionmentioning

confidence: 99%

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Exploring the somatic NF1 mutational spectrum associated with NF1 cutaneous neurofibromas

et al. 2011

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“…This observation is in accordance with previous data showing a B90% identification rate of the two NF1 hits in MPNSTs. 37 One-third (8/28) of the NF1 hits were Figure 1 Mutation dilution sequencing using NGS and Sanger methods. NGS allowed the mutation detection in all dilutions and also presented a quantitative aspect, providing the number of mutated reads.…”

Section: Discussionmentioning

confidence: 99%

“…The high prevalence of such rearrangements in MPNST contrast with the 5-10% found in constitutional DNAs from NF1 patients and is in accordance with previously identified MPNST somatic NF1 mutation spectrum. 37 As molecular analysis of the NF1 gene is challenging, NF1 tumour mutation-spectrum may have been less studied than other genes with gain-of-function mutations. However, NF1 was recently identified as one of the most significantly somatic mutated genes in the Cancer Genome Atlas (TCGA) that provided molecular tumour maps using exome sequencing in more than 3000 tumours from 12 cancer types.…”

Section: Discussionmentioning

confidence: 99%

Neurofibromatosis type 1 molecular diagnosis: what can NGS do for you when you have a large gene with loss of function mutations?

et al. 2014

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Molecular diagnosis of neurofibromatosis type 1 (NF1) is challenging owing to the large size of the tumour suppressor gene NF1, and the lack of mutation hotspots. A somatic alteration of the wild-type NF1 allele is observed in NF1-associated tumours. Genetic heterogeneity in NF1 was confirmed in patients with SPRED1 mutations. Here, we present a targeted next-generation sequencing (NGS) of NF1 and SPRED1 using a multiplex PCR approach (230 amplicons of B150 bp) on a PGM sequencer. The chip capacity allowed mixing 48 bar-coded samples in a 4-day workflow. We validated the NGS approach by retrospectively testing 30 NF1-mutated samples, and then prospectively analysed 279 patients in routine diagnosis. On average, 98.5% of all targeted bases were covered by at least 20X and 96% by at least 100X. An NF1 or SPRED1 alteration was found in 246/279 (88%) and 10/279 (4%) patients, respectively. Genotyping throughput was increased over 10 times, as compared with Sanger, with B90h for consumables per sample. Interestingly, our targeted NGS approach also provided quantitative information based on sequencing depth allowing identification of multiexons deletion or duplication. We then addressed the NF1 somatic mutation detection sensitivity in mosaic NF1 patients and tumours.

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Diagnostic and Management Considerations Posed by Multiple Café au Lait Spots

Riccardi¹

2009

Arch Dermatol

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Germline and somaticNF1 gene mutation spectrum in NF1-associated malignant peripheral nerve sheath tumors (MPNSTs)

Cited by 105 publications

References 57 publications

Exploring the somatic NF1 mutational spectrum associated with NF1 cutaneous neurofibromas

Exploring the somatic NF1 mutational spectrum associated with NF1 cutaneous neurofibromas

Neurofibromatosis type 1 molecular diagnosis: what can NGS do for you when you have a large gene with loss of function mutations?

Diagnostic and Management Considerations Posed by Multiple Café au Lait Spots

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