ALT Neuroblastoma Chemoresistance Due to Telomere Dysfunction-induced ATM Activation is Reversible with ATM Inhibitor AZD0156

Overview

Journal Sci Transl Med

Specialties General Medicine
Science

Date 2021 Aug 19

PMID 34408079

Citations 26

Authors

Balakrishna Koneru

Ahsan Farooqi

Thinh H Nguyen

Wan Hsi Chen

Ashly Hindle

Cody Eslinger

Monish Ram Makena

Trevor A Burrow

Joanne Wilson

Aaron Smith

Venkatesh Pilla Reddy

Elaine Cadogan

Stephen T Durant

C Patrick Reynolds

Affiliations

Soon will be listed here.

Abstract

Cancers overcome replicative immortality by activating either telomerase or an alternative lengthening of telomeres (ALT) mechanism. ALT occurs in ~25% of high-risk neuroblastomas, and progression in patients with ALT neuroblastoma during or after front-line therapy is frequent and often fatal. Temozolomide + irinotecan is commonly used as salvage therapy for neuroblastoma. Patient-derived cell lines and xenografts established from patients with relapsed ALT neuroblastoma demonstrated de novo resistance to temozolomide + irinotecan [SN-38 in vitro, < 0.05; in vivo mouse event-free survival (EFS), < 0.0001] vs. telomerase-positive neuroblastomas. We observed that ALT neuroblastoma cells manifested constitutive ataxia-telangiectasia mutated (ATM) activation due to spontaneous telomere dysfunction which was not observed in telomerase-positive neuroblastoma cells. We demonstrated that induction of telomere dysfunction resulted in ATM activation that, in turn, conferred resistance to temozolomide + SN-38 (4.2-fold change in IC, < 0.001). ATM knockdown (shRNA) or inhibition using a clinical-stage small-molecule inhibitor (AZD0156) reversed resistance to temozolomide + irinotecan in ALT neuroblastoma cell lines in vitro ( < 0.001) and in four ALT xenografts in vivo (EFS, < 0.0001). AZD0156 showed modest to no enhancement of temozolomide + irinotecan activity in telomerase-positive neuroblastoma cell lines and xenografts. Ataxia telangiectasia and Rad3 related (ATR) inhibition using AZD6738 did not enhance temozolomide + SN-38 activity in ALT neuroblastoma cells. Thus, ALT neuroblastoma chemotherapy resistance occurs via ATM activation and is reversible with ATM inhibitor AZD0156. Combining AZD0156 with temozolomide + irinotecan warrants clinical testing for neuroblastoma.

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