
BIORXIV . ORG {
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Title:
A detailed landscape of genomic alterations in malignant peripheral nerve sheath tumor cell lines challenges the current MPNST diagnosis | bioRxiv
Description:
Background Malignant peripheral nerve sheath tumors (MPNSTs) are soft tissue sarcomas that arise from the peripheral nervous system. Half of the tumors develop in the context of the genetic disease Neurofibromatosis type 1 (NF1) and the rest are sporadic sarcomas. MPNSTs have a dismal prognosis due to their aggressiveness and tendency to metastasize, and new treatment options are needed. The diagnosis of MPNSTs can be challenging, especially outside of the NF1 context since specific histological criteria have not been completely established. Genomic analysis may both facilitate differential diagnoses and suggest precision medicine strategies. Methods We generated a complete genomic resource of a set of widely used human NF1-related and sporadic MPNST cell lines by applying ploidy analysis, whole genome and whole exome sequencing and SNP-array analysis, complemented by methylome-based classification and immunofluorescence of cell identity markers (SOX9, SOX10, S100B). Results NF1 MPNST cell lines faithfully recapitulated the genomic copy number profile of primary MPNSTs. Structural variants were key players in the complete inactivation of most recurrently altered tumor suppressor genes (TSGs) ( NF1, CDKN2A, SUZ12/EED ), while small variants played a minor role in the NF1 context, both concerning TSG inactivation and due to the absence of gain-of-function mutations. In clear contrast, the sporadic cell lines (STS-26T, HS-Sch-2, HS-PSS) did not recapitulate the copy number profile of primary MPNSTs. They carried different TSG inactivation and exhibited gain-of-function mutations by predicted kinase activation or generation of fusion genes. Mutational frequencies and signatures emerged as promising informative tools for aiding in MPNST differential diagnosis. Due to the multiple genomic differences exhibited, we complemented their characterization using a methylome-based classifier. All NF1-related cell lines were assigned within the MPNST group, while sporadic cell lines clustered either with melanomas or with an uncertain MPNST-like sarcoma group. The staining of cell identity markers reinforced the idea of a potential misdiagnose of the MPNSTs used to derive the sporadic cell lines analyzed. Conclusions Deep genomic analysis, together with methylome-based sarcoma classification and cell identity marker analysis, challenged the MPNST identity of sporadic cell lines. Results presented here open an opportunity to revise MPNST differential diagnosis and classification. ### Competing Interest Statement The authors have declared no competing interest. * MPNST : Malignant peripheral nerve sheath tumor NF1 : Neurofibromatosis type 1 STR : Short tandem repeats TSG : Tumor suppressor genes PRC2 : Polycomb repressive complex 2 LOH : Loss of heterozygosity VAF : Variant allele frequency BAF : B-allele frequency LRR : Log-R ratio SNV : Single nucleotide variant SV : Structural variant CNV : Copy number variant
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Keywords {๐}
cell, lines, mpnst, biology, genomic, mpnsts, sporadic, context, analysis, results, peripheral, tumor, diagnosis, profile, identity, variant, medrxiv, subject, reviews, clinical, preprint, malignant, nerve, sheath, due, differential, methylomebased, classification, copy, number, inactivation, genes, tsg, biorxiv, university, trials, epidemiology, search, fernรกndez, view, orcid, pdf, tumors, sarcomas, neurofibromatosis, type, options, complete, set, nfrelated,
Topics {โ๏ธ}
epidemiology subject categories nf1-related cell lines clinical trials copy number profile peripheral nervous system promising informative tools biorxiv subject category sporadic cell lines genetics microbiology cell identity markers mpnst differential diagnosis fusion genes methylome-based sarcoma classification epidemiology papers reviews human nf1-related treatment options tsg inactivation author/funder health-related information keyword advanced search structural variants nf1 context methylome-based classifier copyright holder facilitate differential diagnoses methylome-based classification mpnst identity applying ploidy analysis snp-array analysis tumors develop specific histological criteria predicted kinase activation generous financial support chan zuckerberg initiative imperial college london vrije universiteit amsterdam articles animal behavior complete genomic resource juana fernรกndez rodriguez soft tissue sarcomas small variants played mpnst group uncertain mpnst competing interest statement dismal prognosis due genomic analysis sporadic sarcomas nf1
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