Fate-mapping post-hypoxic tumor cells reveals a ROS-resistant phenotype that promotes metastasis

Godet, Inês; Shin, Yu Jung; Ju, Julia A.; Ye, I Chae; Wang, Guannan; Gilkes, Daniele M.

doi:10.1038/s41467-019-12412-1

Cited by 165 publications

(166 citation statements)

References 75 publications

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“…Additionally, ROS produced by sublethal levels of antibiotics induces antibiotic resistance, but ROS triggered by lethal levels of antibiotics promotes bacterial killing and suppresses resistance (Van Acker & Coenye, 2017; Zhao, Hong, & Drlica, 2014). As a critical factor affecting several cancer hallmarks, ROS is also involved in the acquisition of self‐sufficiency in proliferation signals by a ligand‐independent receptor tyrosine kinase transactivation as well as the loss of contact inhibition and anchorage‐dependence cell growth (Godet et al, 2019; Ishikawa et al, 2008; Poillet‐Perez, Despouy, Delage‐Mourroux, & Boyer‐Guittaut, 2015; Wang, Hou, Su, Zhao, & Shi, 2017). Moreover, ROS can affect many signaling pathways, including mitogen‐activated protein kinases signaling pathways (MAPK) (Avisetti, Babu, & Kalivendi, 2014; Shen & Liu, 2006; Zibara et al, 2017).…”

Section: Introductionmentioning

confidence: 99%

Functionalization of Ti substrate with pH‐responsive naringin‐ZnO nanoparticles for the reconstruction of large bony after osteosarcoma resection

Yang

Tao

Gong

et al. 2020

J Biomedical Materials Res

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After bone tumor resection, the large bony deficits are commonly reconstructed with Ti‐based metallic endoprosthesis, which provide immediate stable fixation and allow early ambulation and weight bearing. However, when used in osteosarcoma resection, Ti implant‐relative infection and tumor recurrence were recognized as the two critical factors for implantation failure. Hence, in this work, a novel zinc oxide nanoparticle decorating with naringin was prepared and immobilized onto Ti substrate. The drugs delivery profiles proved that in the bacterial infection and Warburg effect of osteosarcoma‐induced acidic condition, naringin and Zn2+ can be released easily from the functional Ti substrate. The anti‐osteosarcoma and antibacterial assay showed the delivered naringin and Zn2+ can induce a remarkable increase of oxidative stress in bacteria (Escherichia coli and Staphylococcus aureus) and osteosarcoma (Saos‐2 cells) by producing reactive oxygen species (ROS). Accumulation of ROS results in damage of bacterial biofilm and bacterial membrane, leading to the leakage of bacterial RNA and DNA. Meanwhile, the increase of ROS induces osteosarcoma cell apoptosis by activating ROS/extracellular signal‐regulated kinase signaling pathway. Furthermore, in vitro cellular experiments, including cell viability, alkaline phosphatase activity, collagen secretion, extracellular matrix mineralization level, indicated that the functional Ti substrate exhibited great potential for osteoblasts proliferation and differentiation. Hence, this study provides a simple and promising strategy of developing multifunctional Ti‐based implants for the reconstruction of large bony after osteosarcoma resection.

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Section: Introductionmentioning

confidence: 99%

Functionalization of Ti substrate with pH‐responsive naringin‐ZnO nanoparticles for the reconstruction of large bony after osteosarcoma resection

Yang

Tao

Gong

et al. 2020

J Biomedical Materials Res

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“…Because the MARCer construct is constitutively expressed, short episodes of hypoxia could induce labelling, but this may not be seen in proximity to EF5 due to re-oxygenation between the time tamoxifen was given and injection of EF5. Other research has also shown that hypoxic cells move out of hypoxic EF5 + or pimonidazole + areas (Harada et al, 2012;Erapaneedi et al, 2016;Conway et al, 2018;Godet et al, 2019) followed by random distribution. The transient nature of the hypoxic state may explain that the induction of tdTomato expression does not correlate with the level of acute hypoxia 2, 5, 9, 16, 21 days later.…”

Section: Discussionmentioning

confidence: 92%

“…This is likely due to the requirement of O2 for GFP folding and fluorescence (Heim et al, 1994;Kumagai et al, 2013), making it a suboptimal fluorescent marker to track current hypoxia. On the other hand, Godet et al were able to visualise GFP under 0.5% O2 (Godet et al, 2019). Also, processing of the samples exposes them to atmospheric oxygen, possibly introducing enough oxygen for GFP maturation ex vivo.…”

Section: Discussionmentioning

confidence: 99%

“…Although many of the molecular mechanisms of how cells respond to hypoxia are known, how the hypoxic cells may contribute to poor prognosis is still poorly understood. It is known that hypoxic cells are more resistant to treatment and more likely to disseminate and develop into metastases (Harada et al, 2012;Muz et al, 2015;Godet et al, 2019). However, a direct demonstration of the cell autonomous phenotypes of hypoxic tumour cells within the primary tumour and their interplay with the tumour microenvironment remains understudied.…”

Section: Introductionmentioning

confidence: 99%

“…Godet et al recently showed through an alternative hypoxia lineage tracing system, that post-hypoxic tumour cells in mice maintain a ROS-resistant phenotype. This provides a survival advantage in the blood stream therefore promoting their ability to form distant metastases (Godet et al, 2019). One limitation of the aforementioned systems is the relatively long time in continuous hypoxia needed before labelling of cells was achieved, limiting the systems predominantly to areas of sustained chronic hypoxia.…”

Section: Introductionmentioning

confidence: 99%

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A lineage-tracing tool to map the fate of hypoxic tumour cells

Vermeer

Ient

Markelc

et al. 2020

Preprint

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Statement: Here we developed and characterised a novel HIF-1α-Cre fusion gene to trace the progeny of hypoxic tumour cells in a temporal and spatially resolved manner using intravital microscopy. 2 AbstractIntratumoural hypoxia is a common characteristic of malignant treatment-resistant cancers. However, hypoxia-modification strategies for the clinic remain elusive. To date little is known on the behaviour of individual hypoxic tumour cells in their microenvironment. To explore this issue in a spatial and temporally-controlled manner we developed a genetically encoded sensor by fusing the O2-labile Hypoxia-Inducible Factor 1α to eGFP and a tamoxifen-regulated Cre recombinase. Under normoxic conditions HIF-1α is degraded but under hypoxia, the HIF-1α-GFP-Cre-ER T2 fusion protein is stabilised and in the presence of tamoxifen activates a tdTomato reporter gene that is constitutively expressed in hypoxic progeny. We visualise the random distribution of hypoxic tumour cells from hypoxic or necrotic regions and vascularised areas using immunofluorescence and intravital microscopy. Once tdTomato expression is induced, it is stable for at least 4 weeks. Using this system, we could show that the post-hypoxic cells were more proliferative in vivo than non-labelled cells. Our results demonstrate that single-cell lineage tracing of hypoxic tumour cells can allow visualisation of their behaviour in living tumours using intravital microscopy. This tool should prove valuable for the study of dissemination and treatment response of post-hypoxic tumour cells in vivo and ex vivo at single-cell resolution.

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Identification and validation of a combined hypoxia and immune index for triple‐negative breast cancer

et al. 2020

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The interaction between hypoxia and immune status has been confirmed in various cancer settings, and corresponding treatments have been investigated. However, reliable biomarkers are needed for individual treatment, so we sought to develop a novel scoring system based on hypoxia and immune status. Prognostic hypoxia-immune status-related signatures of patients with triple-negative breast cancer (TNBC) were identified in The Cancer Genome Atlas (TCGA) (N = 158), Molecular Taxonomy of Breast Cancer International Consortium (METABRIC) (N = 297), and GSE58812 (N = 107). LASSO Cox regression was used for model construction. Hypoxia and immune status expression profiles were analyzed, and infiltrating immune cells were compared. Quantitative real-time PCR (qRT-PCR) was used for validation in the Sun Yat-sen University Cancer Center (SYSUCC) cohort, and immunofluorescence was applied for the detection of hypoxia and immune markers in cancer tissues. Ten cross-cohort prognostic hypoxia-immune signatures were included to construct the comprehensive index of hypoxia and immune (CIHI) in the METABRIC cohort. Two subgroups of patients with distinct hypoxia-immune status conditions were identified using CIHI: hypoxia high /immune low and hypoxia low /immune high , with a significantly better overall survival (OS) rate in the latter (P < 0.01). The prognostic value of CIHI was further validated in the TCGA, GSE58812, and SYSUCC cohorts (P < 0.01).

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Fate-mapping post-hypoxic tumor cells reveals a ROS-resistant phenotype that promotes metastasis

Cited by 165 publications

References 75 publications

Functionalization of Ti substrate with pH‐responsive naringin‐ZnO nanoparticles for the reconstruction of large bony after osteosarcoma resection

Functionalization of Ti substrate with pH‐responsive naringin‐ZnO nanoparticles for the reconstruction of large bony after osteosarcoma resection

A lineage-tracing tool to map the fate of hypoxic tumour cells

Identification and validation of a combined hypoxia and immune index for triple‐negative breast cancer

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