Cytoglobin in tumor hypoxia: novel insights into cancer suppression

Chakraborty, Sankalpa; John, Rince; Nag, Alo

doi:10.1007/s13277-014-1992-z

Cited by 22 publications

(23 citation statements)

References 104 publications

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“…Cytoglobin is able to bind oxygen, and it is known to regulate oxygen levels in cancer cells during hypoxia [19]. Cytoglobin is a stress-related gene, and its expression level is upregulated during oxidative stress in tumors [19]. Our data has shown that the level of cytoglobin is increased many folds in NSCLC cells and tumor xenografts ( Figure 2 C and 2D).…”

Section: Discussionmentioning

confidence: 71%

“…In cancer cells and tumor xenografts, an increase in heme synthesis and uptake occurs concomitantly with increased levels of hemoproteins such as cytoglobin ( Figure 2C), cytochrome c, Cox-2 and CYP1B1. Cytoglobin is able to bind oxygen, and it is known to regulate oxygen levels in cancer cells during hypoxia [19]. Cytoglobin is a stress-related gene, and its expression level is upregulated during oxidative stress in tumors [19].…”

Section: Discussionmentioning

confidence: 99%

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Evaluating the Association of Heme and Heme Metabolites with Lung Cancer Bioenergetics and Progression

Hooda¹,

Mm²,

Li³

2015

Metabolomics

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of hemoproteins are increased in cancer vs. normal cells (Table 1) [8]. We found that the levels of proteins involved in both heme biosynthesis (ALAS1) and heme uptake (HCP1 and HRG-1), and the levels of oxygen-utilizing hemoproteins, such as cytochromes and cytoglobins, are upregulated in NSCLC cells compared to normal cells [10]. We also found that the rates of oxygen consumption are elevated in cancer cells compared to normal cells. Additionally, we examined the effect of glucose and glutamine, the two major nutrients for cancer cells, on oxygen consumption. Overall, our data reveal a key role of heme in the progression of lung cancer. This may lead to new strategies in the diagnosis and treatment of lung cancer. Materials and Methods Lung cell lines, cell count and reagentsHBEC30KT and HCC4017 cell lines representing normal nonmalignant and NSCLC cells were provided by Dr. John Minna's lab (UTSW) as a gift [9,22]. They were developed from the same patient and were maintained in ACL4 supplemented with 2% FBS under 5% CO 2 at 37 o C [9]. All other NSCLC cell lines including H1395, H1299, Calu-3, A549, H2009 and H460 were purchased from ATCC, and were maintained in RPMI1640 with 5% FBS. All tissue culture medium,

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Section: Discussionmentioning

confidence: 71%

Section: Discussionmentioning

confidence: 99%

Evaluating the Association of Heme and Heme Metabolites with Lung Cancer Bioenergetics and Progression

Hooda¹,

Mm²,

Li³

2015

Metabolomics

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“…Hypoxia induces Cygb upregulation and protects cancer cells from ONS-induced apoptosis. [23][24][25][26] Thus the anti-tumor effect and underlying mechanism of Cygb need to be further explored.…”

Section: The Interaction Of Ons Withmentioning

confidence: 99%

“…Interestingly, Cygb appears to confer intriguing protective properties in tumor cell against oxidative stress injury. Hypoxia induces Cygb upregulation and protects cancer cells from ONS‐induced apoptosis . Thus the anti‐tumor effect and underlying mechanism of Cygb need to be further explored.…”

Section: Introductionmentioning

confidence: 99%

Cytoglobin ameliorates the stemness of hepatocellular carcinoma via coupling oxidative‐nitrosative stress signals

Zhang

Pei

Yang

et al. 2018

Molecular Carcinogenesis

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Cancer stem cells (CSCs) account for tumor self‐renewal and heterogeneity. Oxidative‐nitrosative stress (ONS) is an independent etiologic factor throughout tumorigenesis. Emerging evidences indicated that the interaction of ONS with CSCs contributes to tumor progression and resistance to chemoradiotherapy. Cytoglobin (Cygb) is a member of human hexacoordinate hemoglobin family and acts as a dynamic mediator of redox homeostasis. We observed that Cygb is significantly deregulated in human hepatocellular carcinoma (HCC) tissue and its decrease aggravates the growth of liver cancer stem cells (LCSCs) and increases the subpopulation of CD133(+) LCSCs. Cygb restoration inhibits HCC proliferation and LCSC growth, and decreases the subpopulation of CD133 (+) LCSCs in vitro. We found that Cygb absence promotes LCSC phenotypes and PI3 K/AKT activation, whereas Cygb restoration inhibits LCSC phenotypes and PI3 K/AKT activation. Furthermore, exogenous antioxidants can eliminate the inhibitory effect of Cygb to LCSC growth and phenotypes, as well as PI3 K/AKT activation. Collectively, this study demonstrated that cytoglobin functions as a tumor suppressor and targets CSCs at an ONS‐dependent manner. Thus, Cygb restoration could be a novel and promising therapeutic strategy against HCC with aberrant ROS/RNS accumulation.

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“…However, this is a double-edged-sword as Cygb appears to function not only as a tumor suppressor but also protects hypoxic tumors against therapy. The potential role of Cygb in cancer suppression and hypoxic tumor protection has been recently reviewed (15).…”

Section: Neuroglobin and Neuroprotectionmentioning

confidence: 99%

Redox and Peroxidase Activities of the Hemoglobin Superfamily: Relevance to Health and Disease

Reeder

2017

Antioxidants & Redox Signaling

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Cytoglobin in tumor hypoxia: novel insights into cancer suppression

Cited by 22 publications

References 104 publications

Evaluating the Association of Heme and Heme Metabolites with Lung Cancer Bioenergetics and Progression

Evaluating the Association of Heme and Heme Metabolites with Lung Cancer Bioenergetics and Progression

Cytoglobin ameliorates the stemness of hepatocellular carcinoma via coupling oxidative‐nitrosative stress signals

Redox and Peroxidase Activities of the Hemoglobin Superfamily: Relevance to Health and Disease

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