Inhibition of porcupine prolongs metastasis free survival in a mouse xenograft model of Ewing sarcoma

Masanori Hayashi; Alissa Baker; Seth D. Goldstein; Catherine M. Albert; Kyle W. Jackson; Gregory McCarty; Ulf D. Kahlert; David M. Loeb

doi:10.18632/oncotarget.19432

Inhibition of porcupine prolongs metastasis free survival in a mouse xenograft model of Ewing sarcoma

Masanori Hayashi, Alissa Baker, Seth D. Goldstein, Catherine M. Albert, Kyle W. Jackson, Gregory McCarty, Ulf D. Kahlert, David M. Loeb

School of Medicine

Research output: Contribution to journal › Article › peer-review

11 Scopus citations

Abstract

The most pressing unmet clinical need for patients with Ewing sarcoma (ES) is the prevention and treatment of metastasis. The Wnt signaling pathway regulates a number of cellular functions associated with metastasis, including proliferation, motility, and stem cell self-renewal. Functional interaction between Wnt ligands and their receptors requires palmitoylation by Porcupine (Porcn), making this an ideal therapeutic target. We studied the effect of WNT974, a potent, selective Porcn inhibitor, on ES metastasis. In vitro, WNT974 does not affect ES proliferation or sarcosphere formation, but suppresses multiple transcriptional regulators of metastasis and inhibits cell migration. In vivo, in an orthotopic implantation/amputation model of spontaneous distant metastasis, single agent WNT974 treatment leads to a significant delay in formation of lung metastasis and a substantial improvement in post-amputation survival without a major effect on primary tumor growth. The drug produces no survival benefit in a tail vein injection model, supporting the hypothesis that WNT974 inhibits early steps in the metastatic cascade, such as migration and invasion. Our findings strongly implicate Wnt signaling in the early steps of ES metastasis and demonstrate that WNT974 has the potential to significantly improve the survival of ES patients through the specific inhibition of metastasis.

Original language	English (US)
Pages (from-to)	78265-78276
Number of pages	12
Journal	Oncotarget
Volume	8
Issue number	45
DOIs	https://doi.org/10.18632/oncotarget.19432
State	Published - 2017

Keywords

Ewing sarcoma
Metastasis
Patient-derived xenograft
Preclinical model
Wnt signaling

ASJC Scopus subject areas

Oncology

Access to Document

10.18632/oncotarget.19432

Cite this

@article{10a4f6790fef4dfd8583a0f405f5ab23,

title = "Inhibition of porcupine prolongs metastasis free survival in a mouse xenograft model of Ewing sarcoma",

abstract = "The most pressing unmet clinical need for patients with Ewing sarcoma (ES) is the prevention and treatment of metastasis. The Wnt signaling pathway regulates a number of cellular functions associated with metastasis, including proliferation, motility, and stem cell self-renewal. Functional interaction between Wnt ligands and their receptors requires palmitoylation by Porcupine (Porcn), making this an ideal therapeutic target. We studied the effect of WNT974, a potent, selective Porcn inhibitor, on ES metastasis. In vitro, WNT974 does not affect ES proliferation or sarcosphere formation, but suppresses multiple transcriptional regulators of metastasis and inhibits cell migration. In vivo, in an orthotopic implantation/amputation model of spontaneous distant metastasis, single agent WNT974 treatment leads to a significant delay in formation of lung metastasis and a substantial improvement in post-amputation survival without a major effect on primary tumor growth. The drug produces no survival benefit in a tail vein injection model, supporting the hypothesis that WNT974 inhibits early steps in the metastatic cascade, such as migration and invasion. Our findings strongly implicate Wnt signaling in the early steps of ES metastasis and demonstrate that WNT974 has the potential to significantly improve the survival of ES patients through the specific inhibition of metastasis.",

keywords = "Ewing sarcoma, Metastasis, Patient-derived xenograft, Preclinical model, Wnt signaling",

author = "Masanori Hayashi and Alissa Baker and Goldstein, {Seth D.} and Albert, {Catherine M.} and Jackson, {Kyle W.} and Gregory McCarty and Kahlert, {Ulf D.} and Loeb, {David M.}",

note = "Funding Information: The authors thank Charles Eberhart, Christine Pratilas, and Sara Sukumar for helpful discussions and suggestions. This work was supported by National Institutes of Health grant (1R01CA138212-01) (DML) and the Liddy Shriver Sarcoma Initiative (DML) as well as the Core Grant supporting the Sidney Kimmel Comprehensive Cancer Center, 2P30 CA006973. Work was also supportedby Giant Food Children's Cancer Research Fund and the National Pediatric Cancer Foundation. M.H. was supported by a Pablove Foundation Pediatric Cancer Research grant and by the SARC Sarcoma SPORE Career Development Award (5U54CA168512-02). UDK is supported by the Strategic Research Fund of the Heinrich-Heine University. Publisher Copyright: {\textcopyright} Hayashi et al.",

year = "2017",

doi = "10.18632/oncotarget.19432",

language = "English (US)",

volume = "8",

pages = "78265--78276",

journal = "Oncotarget",

issn = "1949-2553",

publisher = "Impact Journals",

number = "45",

}

TY - JOUR

T1 - Inhibition of porcupine prolongs metastasis free survival in a mouse xenograft model of Ewing sarcoma

AU - Hayashi, Masanori

AU - Baker, Alissa

AU - Goldstein, Seth D.

AU - Albert, Catherine M.

AU - Jackson, Kyle W.

AU - McCarty, Gregory

AU - Kahlert, Ulf D.

AU - Loeb, David M.

N1 - Funding Information: The authors thank Charles Eberhart, Christine Pratilas, and Sara Sukumar for helpful discussions and suggestions. This work was supported by National Institutes of Health grant (1R01CA138212-01) (DML) and the Liddy Shriver Sarcoma Initiative (DML) as well as the Core Grant supporting the Sidney Kimmel Comprehensive Cancer Center, 2P30 CA006973. Work was also supportedby Giant Food Children's Cancer Research Fund and the National Pediatric Cancer Foundation. M.H. was supported by a Pablove Foundation Pediatric Cancer Research grant and by the SARC Sarcoma SPORE Career Development Award (5U54CA168512-02). UDK is supported by the Strategic Research Fund of the Heinrich-Heine University. Publisher Copyright: © Hayashi et al.

PY - 2017

Y1 - 2017

N2 - The most pressing unmet clinical need for patients with Ewing sarcoma (ES) is the prevention and treatment of metastasis. The Wnt signaling pathway regulates a number of cellular functions associated with metastasis, including proliferation, motility, and stem cell self-renewal. Functional interaction between Wnt ligands and their receptors requires palmitoylation by Porcupine (Porcn), making this an ideal therapeutic target. We studied the effect of WNT974, a potent, selective Porcn inhibitor, on ES metastasis. In vitro, WNT974 does not affect ES proliferation or sarcosphere formation, but suppresses multiple transcriptional regulators of metastasis and inhibits cell migration. In vivo, in an orthotopic implantation/amputation model of spontaneous distant metastasis, single agent WNT974 treatment leads to a significant delay in formation of lung metastasis and a substantial improvement in post-amputation survival without a major effect on primary tumor growth. The drug produces no survival benefit in a tail vein injection model, supporting the hypothesis that WNT974 inhibits early steps in the metastatic cascade, such as migration and invasion. Our findings strongly implicate Wnt signaling in the early steps of ES metastasis and demonstrate that WNT974 has the potential to significantly improve the survival of ES patients through the specific inhibition of metastasis.

AB - The most pressing unmet clinical need for patients with Ewing sarcoma (ES) is the prevention and treatment of metastasis. The Wnt signaling pathway regulates a number of cellular functions associated with metastasis, including proliferation, motility, and stem cell self-renewal. Functional interaction between Wnt ligands and their receptors requires palmitoylation by Porcupine (Porcn), making this an ideal therapeutic target. We studied the effect of WNT974, a potent, selective Porcn inhibitor, on ES metastasis. In vitro, WNT974 does not affect ES proliferation or sarcosphere formation, but suppresses multiple transcriptional regulators of metastasis and inhibits cell migration. In vivo, in an orthotopic implantation/amputation model of spontaneous distant metastasis, single agent WNT974 treatment leads to a significant delay in formation of lung metastasis and a substantial improvement in post-amputation survival without a major effect on primary tumor growth. The drug produces no survival benefit in a tail vein injection model, supporting the hypothesis that WNT974 inhibits early steps in the metastatic cascade, such as migration and invasion. Our findings strongly implicate Wnt signaling in the early steps of ES metastasis and demonstrate that WNT974 has the potential to significantly improve the survival of ES patients through the specific inhibition of metastasis.

KW - Ewing sarcoma

KW - Metastasis

KW - Patient-derived xenograft

KW - Preclinical model

KW - Wnt signaling

UR - http://www.scopus.com/inward/record.url?scp=85030465392&partnerID=8YFLogxK

UR - http://www.scopus.com/inward/citedby.url?scp=85030465392&partnerID=8YFLogxK

U2 - 10.18632/oncotarget.19432

DO - 10.18632/oncotarget.19432

M3 - Article

C2 - 29108227

AN - SCOPUS:85030465392

SN - 1949-2553

VL - 8

SP - 78265

EP - 78276

JO - Oncotarget

JF - Oncotarget

IS - 45

ER -

Inhibition of porcupine prolongs metastasis free survival in a mouse xenograft model of Ewing sarcoma

Abstract

Keywords

ASJC Scopus subject areas

Access to Document

Other files and links

Fingerprint

Cite this