Exploring Transcriptional Regulators Ref-1 and STAT3 As Therapeutic Targets in Malignant Peripheral Nerve Sheath Tumours

Overview

Journal Br J Cancer

Specialty Oncology

Date 2021 Mar 4

PMID 33658640

Citations 13

Authors

Silpa Gampala

Fenil Shah

Chi Zhang

Steven D Rhodes

Olivia Babb

Michelle Grimard

Randall S Wireman

Ellie Rad

Brian Calver

Ren-Yuan Bai

Verena Staedtke

Emily L Hulsey

M Reza Saadatzadeh

Karen E Pollok

Yan Tong

Abbi E Smith

D Wade Clapp

Andrew R Tee

Mark R Kelley

Melissa L Fishel

Affiliations

Soon will be listed here.

Abstract

Background: MPNST is a rare soft-tissue sarcoma that can arise from patients with NF1. Existing chemotherapeutic and targeted agents have been unsuccessful in MPNST treatment, and recent findings implicate STAT3 and HIF1-α in driving MPNST. The DNA-binding and transcriptional activity of both STAT3 and HIF1-α is regulated by Redox factor-1 (Ref-1) redox function. A first-generation Ref-1 inhibitor, APX3330, is being tested in cancer clinical trials and could be applied to MPNST.

Methods: We characterised Ref-1 and p-STAT3 expression in various MPNST models. Tumour growth, as well as biomarkers of apoptosis and signalling pathways, were measured by qPCR and western blot following treatment with inhibitors of Ref-1 or STAT3.

Results: MPNSTs from Nf1-ArfPostnCre mice exhibit significantly increased positivity of p-STAT3 and Ref-1 expression when malignant transformation occurs. Inhibition of Ref-1 or STAT3 impairs MPNST growth in vitro and in vivo and induces apoptosis. Genes highly expressed in MPNST patients are downregulated following inhibition of Ref-1 or STAT3. Several biomarkers downstream of Ref-1 or STAT3 were also downregulated following Ref-1 or STAT3 inhibition.

Conclusions: Our findings implicate a unique therapeutic approach to target important MPNST signalling nodes in sarcomas using new first-in-class small molecules for potential translation to the clinic.

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