Metronomic topotecan impedes tumor growth ofMYCN-amplified neuroblastoma cellsin vitroandin vivoby therapy induced senescence | Zendy

Sabine TaschnerMandl | Zendy; Magdalena Schwarz | Zendy; Johanna Blaha | Zendy; Maximilian Kauer | Zendy; Florian Kromp | Zendy; Nelli Frank | Zendy; Fikret Rifatbegovic | Zendy; Tamara Weiss | Zendy; Ruth Ladenstein | Zendy; M. Hohenegger | Zendy; Inge M. Ambros | Zendy; Peter F. Ambros | Zendy

Open Access

Metronomic topotecan impedes tumor growth ofMYCN-amplified neuroblastoma cellsin vitroandin vivoby therapy induced senescence

Author(s) -

Sabine TaschnerMandl,

Magdalena Schwarz,

Johanna Blaha,

Maximilian Kauer,

Florian Kromp,

Nelli Frank,

Fikret Rifatbegovic,

Tamara Weiss,

Ruth Ladenstein,

M. Hohenegger,

Inge M. Ambros,

Peter F. Ambros

Publication year - 2015

Publication title -

oncotarget

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 1.373

H-Index - 127

ISSN - 1949-2553

DOI - 10.18632/oncotarget.6527

Subject(s) - neuroblastoma , senescence , topotecan , apoptosis , in vivo , cell cycle checkpoint , medicine , cancer research , cancer , pharmacology , cell cycle , biology , cell culture , chemotherapy , genetics

Poor prognosis and frequent relapses are major challenges for patients with high-risk neuroblastoma (NB), especially when tumors show MYCN amplification. High-dose chemotherapy triggers apoptosis, necrosis and senescence, a cellular stress response leading to permanent proliferative arrest and a typical senescence-associated secretome (SASP). SASP components reinforce growth-arrest and act immune-stimulatory, while others are tumor-promoting. We evaluated whether metronomic, i.e. long-term, repetitive low-dose, drug treatment induces senescence in vitro and in vivo. And importantly, by using the secretome as a discriminator for beneficial versus adverse effects of senescence, drugs with a tumor-inhibiting SASP were identified.We demonstrate that metronomic application of chemotherapeutic drugs induces therapy-induced senescence, characterized by cell cycle arrest, p21(WAF/CIP1) up-regulation and DNA double-strand breaks selectively in MYCN-amplified NB. Low-dose topotecan (TPT) was identified as an inducer of a favorable SASP while lacking NFKB1/p50 activation. In contrast, Bromo-deoxy-uridine induced senescent NB-cells secret a tumor-promoting SASP in a NFKB1/p50-dependent manner. Importantly, TPT-treated senescent tumor cells act growth-inhibitory in a dose-dependent manner on non-senescent tumor cells and MYCN expression is significantly reduced in vitro and in vivo. Furthermore, in a mouse xenotransplant-model for MYCN-amplified NB metronomic TPT leads to senescence selectively in tumor cells, complete or partial remission, prolonged survival and a favorable SASP.This new mode-of-action of metronomic TPT treatment, i.e. promoting a tumor-inhibiting type of senescence in MYCN-amplified tumors, is clinically relevant as metronomic regimens are increasingly implemented in therapy protocols of various cancer entities and are considered as a feasible maintenance treatment option with moderate adverse event profiles.

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