NOTCH pathway inactivation reprograms stem-like oral cancer cells to JAK-STAT dependent state and provides the opportunity of synthetic lethality

Subhashis Ghosh; Paromita Mitra; Uday Saha; Rimpa Nandi; Subhashree Jena; Arnab Ghosh; Shantanu Saha Roy; Moulinath Acharya; Nidhan Kumar Biswas; Sandeep Singh

Translational Oncology (Jun 2023)

NOTCH pathway inactivation reprograms stem-like oral cancer cells to JAK-STAT dependent state and provides the opportunity of synthetic lethality

Subhashis Ghosh,
Paromita Mitra,
Uday Saha,
Rimpa Nandi,
Subhashree Jena,
Arnab Ghosh,
Shantanu Saha Roy,
Moulinath Acharya,
Nidhan Kumar Biswas,
Sandeep Singh

Affiliations

Subhashis Ghosh: National Institute of Biomedical Genomics, Kalyani, West Bengal 741251, India
Paromita Mitra: National Institute of Biomedical Genomics, Kalyani, West Bengal 741251, India
Uday Saha: National Institute of Biomedical Genomics, Kalyani, West Bengal 741251, India
Rimpa Nandi: National Institute of Biomedical Genomics, Kalyani, West Bengal 741251, India
Subhashree Jena: National Institute of Biomedical Genomics, Kalyani, West Bengal 741251, India
Arnab Ghosh: National Institute of Biomedical Genomics, Kalyani, West Bengal 741251, India
Shantanu Saha Roy: National Institute of Biomedical Genomics, Kalyani, West Bengal 741251, India
Moulinath Acharya: National Institute of Biomedical Genomics, Kalyani, West Bengal 741251, India
Nidhan Kumar Biswas: National Institute of Biomedical Genomics, Kalyani, West Bengal 741251, India
Sandeep Singh: Corresponding author.; National Institute of Biomedical Genomics, Kalyani, West Bengal 741251, India

Journal volume & issue: Vol. 32
p. 101669

Abstract

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Background: We have recently provided the evidence of interconvertible cellular states, driving non-genetic heterogeneity among stem-like oral cancer cells (oral-SLCCs). Here, NOTCH pathway-activity status is explored as one of the possible mechanisms behind this stochastic plasticity. Methods: Oral-SLCCs were enriched in 3D-spheroids. Constitutively-active and inactive status of NOTCH pathway was achieved by genetic or pharmacological approaches. RNA sequencing and real-time PCR was performed for gene expression studies. in vitro cytotoxicity assessments were performed by AlamarBlue assay and in vivo effects were studied by xenograft growth in zebrafish embryo. Results: We have observed stochastic plasticity in oral-SLCCs, spontaneously maintaining both NOTCH-active and inactive states. While cisplatin refraction was associated with post-treatment adaptation to the active-state of NOTCH pathway, oral-SLCCs with inactive NOTCH pathway status showed aggressive tumor growth and poor prognosis. RNAseq analysis clearly suggested the upregulation of JAK-STAT pathway in NOTCH pathway-inactive subset. The 3D-spheroids with lower NOTCH-activity status displayed significantly higher sensitivity to JAK-selective drugs, Ruxolitinib or Tofacitinib or siRNA mediated downregulation of tested partners STAT3/4. Oral-SLCCs were programmed to adapt the inactive status of NOTCH pathway by exposing to γ-secretase inhibitors, LY411575 or RO4929097, followed by targeting with JAK-inhibitors, Ruxolitinib or Tofacitinib. This approach resulted in a very significant inhibition in viability of 3D-spheroids as well as xenograft initiation in Zebrafish embryos. Conclusion: Study revealed for the first time that NOTCH pathway-inactive state exhibit activation of JAK-STAT pathways, as synthetic lethal pair. Therefore, co-inhibition of these pathway may serve as novel therapeutic strategy against aggressive oral cancer.

Published in Translational Oncology

ISSN: 1944-7124 (Print); 1936-5233 (Online)
Publisher: Elsevier
Country of publisher: Netherlands
LCC subjects: Medicine: Internal medicine: Neoplasms. Tumors. Oncology. Including cancer and carcinogens
Website: https://www.journals.elsevier.com/translational-oncology/

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