Targeting KDM1A in Neuroblastoma with NCL-1 Induces a Less Aggressive Phenotype and Suppresses Angiogenesis

Overview

Journal J Clin Med

Specialty General Medicine

Date 2024 Oct 26

PMID 39458030

Authors

Annika Sprussel

Takayoshi Suzuki

Naoki Miyata

Kathy Astrahantseff

Annabell Szymansky

Joern Toedling

Theresa M Thole-Kliesch

Annika Ballagee

Marco Lodrini

Annette Kunkele

Matthias Truss

Lukas C Heukamp

Susanne Mathia

Falk Hertwig

Christian Rosenberger

Angelika Eggert

Hedwig E Deubzer

Johannes H Schulte

Affiliations

Soon will be listed here.

Abstract

The KDM1A histone demethylase regulates the cellular balance between proliferation and differentiation, and is often deregulated in human cancers including the childhood tumor neuroblastoma. We previously showed that KDM1A is strongly expressed in undifferentiated neuroblastomas and correlates with poor patient prognosis, suggesting a possible clinical benefit from targeting KDM1A. Here, we tested the efficacy of NCL-1, a small molecule specifically inhibiting KDM1A in preclinical models for neuroblastoma. NCL-1 mimicked the effects of siRNA-mediated KDM1A knockdown and effectively inhibited KDM1A activity in four neuroblastoma cell lines and a patient-representative cell model. KDM1A inhibition shifted the aggressive tumor cell phenotypes towards less aggressive phenotypes. The proliferation and cell viability was reduced, accompanied by the induction of markers of neuronal differentiation. Interventional NCL-1 treatment of nude mice harboring established neuroblastoma xenograft tumors reduced tumor growth and inhibited cell proliferation. Reduced vessel density and defects in blood vessel construction also resulted, and NCL-1 inhibited the growth and tube formation of HUVEC-C cells in vitro. : Inhibiting KDM1A could attack aggressive neuroblastomas two-fold, by re-directing tumor cells toward a less aggressive, slower-growing phenotype and by preventing or reducing the vascular support of large tumors.

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