TY - JOUR
T1 - Nrf2 Modulates the Hybrid Epithelial/Mesenchymal Phenotype and Notch Signaling During Collective Cancer Migration
AU - Vilchez Mercedes, Samuel A.
AU - Bocci, Federico
AU - Ahmed, Mona
AU - Eder, Ian
AU - Zhu, Ninghao
AU - Levine, Herbert
AU - Onuchic, José N.
AU - Jolly, Mohit Kumar
AU - Wong, Pak Kin
N1 - Funding Information:
This work was supported by National Science Foundation by sponsoring the Center for Theoretical Biological Physics – award PHY-2019745 (JO and HL) and by awards PHY-1605817 (HL), CHE-1614101 (JO) and CBET-1802947 (PW). FB was also supported by the NSF grant DMS1763272 and a grant from the Simons Foundation (594598, QN). MJ was supported by Ramanujan Fellowship awarded by SERB, DST, Government of India (SB/S2/RJN-049/2018). JO is a CPRIT Scholar in Cancer Research sponsored by the Cancer Prevention and Research Institute of Texas.
Funding Information:
This work was supported by National Science Foundation by sponsoring the Center for Theoretical Biological Physics – award PHY-2019745 (JO and HL) and by awards PHY-1605817 (HL), CHE-1614101 (JO) and CBET-1802947 (PW). FB was also supported by the NSF grant DMS1763272 and a grant from the Simons Foundation (594598, QN). MJ was supported by Ramanujan Fellowship awarded by SERB, DST, Government of India (SB/S2/RJN-049/2018). JO is a CPRIT Scholar in Cancer Research sponsored by the Cancer Prevention and Research Institute of Texas.
Publisher Copyright:
Copyright © 2022 Vilchez Mercedes, Bocci, Ahmed, Eder, Zhu, Levine, Onuchic, Jolly and Wong.
PY - 2022/4/8
Y1 - 2022/4/8
N2 - Hybrid epithelial/mesenchymal cells (E/M) are key players in aggressive cancer metastasis. It remains a challenge to understand how these cell states, which are mostly non-existent in healthy tissue, become stable phenotypes participating in collective cancer migration. The transcription factor Nrf2, which is associated with tumor progression and resistance to therapy, appears to be central to this process. Here, using a combination of immunocytochemistry, single cell biosensors, and computational modeling, we show that Nrf2 functions as a phenotypic stability factor for hybrid E/M cells by inhibiting a complete epithelial-mesenchymal transition (EMT) during collective cancer migration. We also demonstrate that Nrf2 and EMT signaling are spatially coordinated near the leading edge. In particular, computational analysis of an Nrf2-EMT-Notch network and experimental modulation of Nrf2 by pharmacological treatment or CRISPR/Cas9 gene editing reveal that Nrf2 stabilizes a hybrid E/M phenotype which is maximally observed in the interior region immediately behind the leading edge. We further demonstrate that the Nrf2-EMT-Notch network enhances Dll4 and Jagged1 expression at the leading edge, which correlates with the formation of leader cells and protruding tips. Altogether, our results provide direct evidence that Nrf2 acts as a phenotypic stability factor in restricting complete EMT and plays an important role in coordinating collective cancer migration.
AB - Hybrid epithelial/mesenchymal cells (E/M) are key players in aggressive cancer metastasis. It remains a challenge to understand how these cell states, which are mostly non-existent in healthy tissue, become stable phenotypes participating in collective cancer migration. The transcription factor Nrf2, which is associated with tumor progression and resistance to therapy, appears to be central to this process. Here, using a combination of immunocytochemistry, single cell biosensors, and computational modeling, we show that Nrf2 functions as a phenotypic stability factor for hybrid E/M cells by inhibiting a complete epithelial-mesenchymal transition (EMT) during collective cancer migration. We also demonstrate that Nrf2 and EMT signaling are spatially coordinated near the leading edge. In particular, computational analysis of an Nrf2-EMT-Notch network and experimental modulation of Nrf2 by pharmacological treatment or CRISPR/Cas9 gene editing reveal that Nrf2 stabilizes a hybrid E/M phenotype which is maximally observed in the interior region immediately behind the leading edge. We further demonstrate that the Nrf2-EMT-Notch network enhances Dll4 and Jagged1 expression at the leading edge, which correlates with the formation of leader cells and protruding tips. Altogether, our results provide direct evidence that Nrf2 acts as a phenotypic stability factor in restricting complete EMT and plays an important role in coordinating collective cancer migration.
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U2 - 10.3389/fmolb.2022.807324
DO - 10.3389/fmolb.2022.807324
M3 - Article
C2 - 35480877
AN - SCOPUS:85128713472
SN - 2296-889X
VL - 9
JO - Frontiers in Molecular Biosciences
JF - Frontiers in Molecular Biosciences
M1 - 807324
ER -