HES1 promoter activation dynamics reveal the plasticity, stemness and heterogeneity in neuroblastoma cancer stem cells

Author:

Riya Paul Ann12,Basu Budhaditya13,Surya Suresh12,Parvathy Surendran12,Lalitha Soundararajan12ORCID,Jyothi Nair Pradeep12,Meera Vadakkath12,Jaikumar Vishnu Sunil4,Sunitha Padmanabhan5,Shahina Afzal5,Sukumaran Rashmi5,Nair Achuthsankar Sukumaran5,Dhanesh Sivadasan Bindu1,Jiffy John6,Nelson-Sati Shijulal6ORCID,Maliekal Tessy Thomas7,Das Ani Venmanad8,James Jackson123ORCID

Affiliation:

1. Rajiv Gandhi Centre for Biotechnology (DBT-RGCB) 1 Neuro Stem Cell Biology Laboratory, Neurobiology Division , , Thiruvananthapuram, Kerala 695 014 , India

2. Department of Biotechnology,The University of Kerala 2 , Thiruvananthapuram, Kerala 695 581 , India

3. Regional Centre for Biotechnology (DBT-RCB) 3 , Faridabad, Haryana 121001 , India

4. Rajiv Gandhi Centre for Biotechnology (DBT-RGCB) 4 Animal Research Facility , , Thiruvananthapuram, Kerala 695 014 , India

5. University of Kerala 5 Department of Computational Biology and Bioinformatics , , Thiruvananthapuram, Kerala , India

6. Rajiv Gandhi Centre for Biotechnology (DBT-RGCB) 6 Transdisciplinary Biology , , Thiruvananthapuram, Kerala 695 014 , India

7. Rajiv Gandhi Centre for Biotechnology (DBT-RGCB) 7 Cancer Research -10 , , Thiruvananthapuram, Kerala 695 014 , India

8. Rajiv Gandhi Centre for Biotechnology (DBT-RGCB) 8 Cancer Research -12 , , Thiruvananthapuram, Kerala 695 014 , India

Abstract

ABSTRACT Notch signaling and its downstream gene target HES1 play a critical role in regulating and maintaining cancer stem cells (CSCs), similar to as they do during embryonic development. Here, we report a unique subclass of Notch-independent Hes-1 (NIHes-1)-expressing CSCs in neuroblastoma. These CSCs maintain sustained HES1 expression by activation of HES1 promoter region upstream of classical CBF-1 binding sites, thereby completely bypassing Notch receptor-mediated activation. These stem cells have self-renewal ability and potential to generate tumors. Interestingly, we observed that NIHes-1 CSCs could transition to Notch-dependent Hes-1-expressing (NDHes-1) CSCs where HES1 is expressed by Notch receptor-mediated promoter activation. We observed that NDHes-1-expressing CSCs also had the potential to transition to NIHes-1 CSCs and during this coordinated bidirectional transition, both CSCs gave rise to the majority of the bulk cancer cells, which had an inactive HES1 promoter (PIHes-1). A few of these PIHes-1 cells were capable of reverting into a CSC state. These findings explain the existence of a heterogenic mode of HES1 promoter activation within the IMR-32 neuroblastoma cell line and the potential to switch between them. This article has an associated First Person interview with the first authors of the paper.

Funder

Rajiv Gandhi Centre for Biotechnology

Department of Biotechnology, Ministry of Science and Technology, India

Council for Scientific and Industrial Research

University Grants Commission

Publisher

The Company of Biologists

Subject

Cell Biology

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