Inhibition of SETMAR–H3K36me2–NHEJ repair axis in residual disease cells prevents glioblastoma recurrence-Reference-Cited by-同舟云学术

Inhibition of SETMAR–H3K36me2–NHEJ repair axis in residual disease cells prevents glioblastoma recurrence

Published:2020-05-27 Issue:12 Volume:22 Page:1785-1796
ISSN:1522-8517
Container-title:Neuro-Oncology
language:en
Short-container-title:

Author:

Kaur Ekjot¹²,Nair Jyothi¹²,Ghorai Atanu¹,Mishra Saket V¹²,Achareker Anagha¹²,Ketkar Madhura¹²,Sarkar Debashmita¹²,Salunkhe Sameer¹²,Rajendra Jacinth¹,Gardi Nilesh³,Desai Sanket³,Iyer Prajish³,Thorat Rahul⁴,Dutt Amit³²,Moiyadi Aliasgar⁵,Dutt Shilpee³

Affiliation:

1. Shilpee Dutt Laboratory, Advanced Centre for Treatment, Research and Education in Cancer (ACTREC), Tata Memorial Centre, Kharghar, Navi Mumbai, India

2. Homi Bhabha National Institute, Training School Complex, Anushakti Nagar, Mumbai, India

3. Integrated Genomics Laboratory, ACTREC, Kharghar, Navi Mumbai, India

4. Laboratory Animal Facility, ACTREC, Tata Memorial Centre, Kharghar, Navi Mumbai, India

5. Department of Neurosurgery, ACTREC, Tata Memorial Centre, Kharghar, Navi Mumbai, India

Abstract

Abstract Background Residual disease of glioblastoma (GBM) causes recurrence. However, targeting residual cells has failed, due to their inaccessibility and our lack of understanding of their survival mechanisms to radiation therapy. Here we deciphered a residual cell–specific survival mechanism essential for GBM relapse. Methods Therapy resistant residual (RR) cells were captured from primary patient samples and cell line models mimicking clinical scenario of radiation resistance. Molecular signaling of resistance in RR cells was identified using RNA sequencing, genetic and pharmacological perturbations, overexpression systems, and molecular and biochemical assays. Findings were validated in patient samples and an orthotopic mouse model. Results RR cells form more aggressive tumors than the parental cells in an orthotopic mouse model. Upon radiation-induced damage, RR cells preferentially activated a nonhomologous end joining (NHEJ) repair pathway, upregulating Ku80 and Artemis while downregulating meiotic recombination 11 (Mre11) at protein but not RNA levels. Mechanistically, RR cells upregulate the Su(var)3-9/enhancer-of-zeste/trithorax (SET) domain and mariner transposase fusion gene (SETMAR), mediating high levels of H3K36me2 and global euchromatization. High H3K36me2 leads to efficiently recruiting NHEJ proteins. Conditional knockdown of SETMAR in RR cells induced irreversible senescence partly mediated by reduced H3K36me2. RR cells expressing mutant H3K36A could not retain Ku80 at double-strand breaks, thus compromising NHEJ repair, leading to apoptosis and abrogation of tumorigenicity in vitro and in vivo. Pharmacological inhibition of the NHEJ pathway phenocopied H3K36 mutation effect, confirming dependency of RR cells on the NHEJ pathway for their survival. Conclusions We demonstrate that the SETMAR-NHEJ regulatory axis is essential for the survival of clinically relevant radiation RR cells, abrogation of which prevents recurrence in GBM.

Funder

Department of Biotechnology

Department of Science and Technology-Science and Engineering Research Board

National Post Doctoral Fellow

Publisher

Oxford University Press (OUP)

Subject

Cancer Research,Neurology (clinical),Oncology

Link

http://academic.oup.com/neuro-oncology/advance-article-pdf/doi/10.1093/neuonc/noaa128/33542332/noaa128.pdf

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