PRC2 loss drives MPNST metastasis and matrix remodeling
Qierra R. Brockman, Amanda Scherer, Gavin R. McGivney, Wade R. Gutierrez, Andrew P. Voigt, Alexandra L. Isaacson, Emily A. Laverty, Grace Roughton, Vickie Knepper-Adrian, Benjamin Darbro, Munir R. Tanas, Christopher S. Stipp, Rebecca D. Dodd
Qierra R. Brockman, Amanda Scherer, Gavin R. McGivney, Wade R. Gutierrez, Andrew P. Voigt, Alexandra L. Isaacson, Emily A. Laverty, Grace Roughton, Vickie Knepper-Adrian, Benjamin Darbro, Munir R. Tanas, Christopher S. Stipp, Rebecca D. Dodd
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Research Article Oncology

PRC2 loss drives MPNST metastasis and matrix remodeling

Abstract

The histone methyltransferase PRC2 plays a complex role in cancer. Malignant peripheral nerve sheath tumors (MPNSTs) are aggressive sarcomas with frequent loss-of-function mutations in PRC2 that are associated with poor outcome. Here, we identify a critical role for PRC2 loss in driving MPNST metastasis. PRC2-dependent metastatic phenotypes included increased collagen-dependent invasion, upregulation of matrix-remodeling enzymes, and elevated lung metastasis in orthotopic mouse models. Furthermore, clinical sample analysis determined that PRC2 loss correlated with metastatic disease, increased fibrosis, and decreased survival in patients with MPNSTs. These results may have broad implications for PRC2 function across multiple cancers and provide a strong rationale for investigating potential therapies targeting ECM-remodeling enzymes and tumor fibrosis to improve outcomes in patients with MPNSTs.

Authors

Qierra R. Brockman, Amanda Scherer, Gavin R. McGivney, Wade R. Gutierrez, Andrew P. Voigt, Alexandra L. Isaacson, Emily A. Laverty, Grace Roughton, Vickie Knepper-Adrian, Benjamin Darbro, Munir R. Tanas, Christopher S. Stipp, Rebecca D. Dodd

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Figure 4

PRC2 deletion upregulates expression of Mmp and Lox enzyme families.

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PRC2 deletion upregulates expression of Mmp and Lox enzyme families. (A)...
(A) MMP enzyme gene expression by quantitative real-time PCR (qRT-PCR) in NP1, NP2, NC1, and NC2 isogenic cell lines shows upregulation of Mmp9 and Mmp2 with loss of either Eed or Suz12. Upregulation of Mmp14 is seen in some cells with PRC2 loss (n = 3). (B) Lox enzyme gene expression by qRT-PCR in NP1, NP2, NC1, and NC2 isogenic cell lines shows upregulation of Lox family genes LoxL2, LoxL3, and LoxL4 with loss of either Eed or Suz12 (n = 3). qRT-PCR data analyzed by 1-way ANOVA with Tukey’s multiple comparisons. Data represent biological replicates with the mean ± SD; *P < 0.05, **P < 0.01, ***P < 0.001, ****P < 0.0001.