The Senescence-associated Secretory Phenotype Mediates Oncogene-induced Senescence in Pediatric Pilocytic Astrocytoma

Juliane L. Buhl(German Cancer Research Center), Florian Selt(German Cancer Research Center), Thomas Hielscher(German Cancer Research Center), Romain Guiho(King's College London), Jonas Ecker(German Cancer Research Center), Felix Sahm(German Cancer Research Center), Johannes Ridinger(German Cancer Research Center), Dennis Riehl(European Molecular Biology Organization), Diren Usta(German Cancer Research Center), Britta Ismer(German Cancer Research Center), Alexander C. Sommerkamp(German Cancer Research Center), Juan Pedro Martı́nez-Barberá(King's College London), Annika K. Wefers(German Cancer Research Center), Marc Remke(German Cancer Research Center), Daniel Picard(German Cancer Research Center), Stefan Pusch(German Cancer Research Center), Jan Gronych(German Cancer Research Center), Ina Oehme(German Cancer Research Center), Cornelis M. van Tilburg(German Cancer Research Center), Marcel Kool(German Cancer Research Center), Daniela Kühn(German Cancer Research Center), David Capper(German Cancer Research Center), Andreas von Deimling(German Cancer Research Center), Martin U. Schuhmann(University Children's Hospital Tübingen), Christel Herold‐Mende(Heidelberg University), Andrey Korshunov(German Cancer Research Center), Tilman Brummer(German Cancer Research Center), Stefan M. Pfister(German Cancer Research Center), David Jones(German Cancer Research Center), Olaf Witt(German Cancer Research Center), Till Milde(German Cancer Research Center)
Clinical Cancer Research
December 7, 2018
10.1158/1078-0432.ccr-18-1965
Cited by 84Open Access
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Abstract

Abstract Purpose: Pilocytic astrocytoma is the most common childhood brain tumor, characterized by constitutive MAPK activation. MAPK signaling induces oncogene-induced senescence (OIS), which may cause unpredictable growth behavior of pilocytic astrocytomas. The senescence-associated secretory phenotype (SASP) has been shown to regulate OIS, but its role in pilocytic astrocytoma remains unknown. Experimental Design: The patient-derived pilocytic astrocytoma cell culture model, DKFZ-BT66, was used to demonstrate presence of the SASP and analyze its impact on OIS in pilocytic astrocytoma. The model allows for doxycycline-inducible switching between proliferation and OIS. Both states were studied using gene expression profiling (GEP), Western blot, ELISA, and cell viability testing. Primary pilocytic astrocytoma tumors were analyzed by GEP and multiplex assay. Results: SASP factors were upregulated in primary human and murine pilocytic astrocytoma and during OIS in DKFZ-BT66 cells. Conditioned medium induced growth arrest of proliferating pilocytic astrocytoma cells. The SASP factors IL1B and IL6 were upregulated in primary pilocytic astrocytoma, and both pathways were regulated during OIS in DKFZ-BT66. Stimulation with rIL1B but not rIL6 reduced growth of DKFZ-BT66 cells and induced the SASP. Anti-inflammatory treatment with dexamethasone induced regrowth of senescent cells and inhibited the SASP. Senescent DKFZ-BT66 cells responded to senolytic BCL2 inhibitors. High IL1B and SASP expression in pilocytic astrocytoma tumors was associated with favorable progression-free survival. Conclusions: We provide evidence for the SASP regulating OIS in pediatric pilocytic astrocytoma, with IL1B as a relevant mediator. SASP expression could enable prediction of progression in patients with pilocytic astrocytoma. Further investigation of the SASP driving the unpredictable growth of pilocytic astrocytomas, and its possible therapeutic application, is warranted.

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