Multiplatform molecular profiling uncovers two subgroups of malignant peripheral nerve sheath tumors with distinct therapeutic vulnerabilities

Author:

Suppiah Suganth,Mansouri Sheila,Mamatjan YasinORCID,Liu Jeffrey C.,Bhunia Minu M.ORCID,Patil Vikas,Rath PrisniORCID,Mehani BharatiORCID,Heir Pardeep,Bunda Severa,Velez-Reyes German L.,Singh OliviaORCID,Ijad Nazanin,Pirouzmand Neda,Dalcourt Tatyana,Meng Ying,Karimi Shirin,Wei Qingxia,Nassiri FarshadORCID,Pugh Trevor J.ORCID,Bader Gary D.ORCID,Aldape Kenneth D.ORCID,Largaespada David A.ORCID,Zadeh GelarehORCID

Abstract

AbstractMalignant peripheral nerve sheath tumor (MPNST) is a highly aggressive sarcoma, and a lethal neurofibromatosis type 1-related malignancy, with little progress made on treatment strategies. Here, we apply a multiplatform integrated molecular analysis on 108 tumors spanning the spectrum of peripheral nerve sheath tumors to identify candidate drivers of MPNST that can serve as therapeutic targets. Unsupervised analyses of methylome and transcriptome profiles identify two distinct subgroups of MPNSTs with unique targetable oncogenic programs. We establish two subgroups of MPNSTs: SHH pathway activation in MPNST-G1 and WNT/ß-catenin/CCND1 pathway activation in MPNST-G2. Single nuclei RNA sequencing characterizes the complex cellular architecture and demonstrate that malignant cells from MPNST-G1 and MPNST-G2 have neural crest-like and Schwann cell precursor-like cell characteristics, respectively. Further, in pre-clinical models of MPNST we confirm that inhibiting SHH pathway in MPNST-G1 prevent growth and malignant progression, providing the rational for investigating these treatments in clinical trials.

Funder

U.S. Department of Defense

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry,Multidisciplinary

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