Mitochondrial GRIM-19 as a potential therapeutic target for STAT3-dependent carcinogenesis of gastric cancer

Huang, Yi; Yang, Meihua; Hu, Huajian; Zhao, Xiaodong; Bao, Liming; Huang, Daochao; Song, Lihua; Li, Yang

doi:10.18632/oncotarget.9167

Cited by 20 publications

(34 citation statements)

References 45 publications

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“…FSP is considered as a marker of fibroblasts in different organs undergoing tissue remodeling and helps to identify fibroblasts derived from EMT in several organs including the liver 5859, 60. Herein, we have shown that possible downstream targets of NFκB and STAT3 pathways including TGFβ, HGF, IL‐6, IL‐8, TNC, collagens I and III were upregulated in fibroblasts infected by H. pylori (cagA+vacA+).…”

Section: Discussionmentioning

confidence: 86%

“…FSP is considered as a marker of fibroblasts in different organs undergoing tissue remodeling and helps to identify fibroblasts derived from EMT in several organs including the liver 58. H. pylori can stimulate TLRs leading to activation of innate immunity against bacterial inflammation, thus creating an inflammatory microenvironment, a prerequisite for tumor development through activation of NF-κB and STAT3 pathways in human GC 59,60. Herein, we have shown that possible downstream targets of NFκB and STAT3 pathways including TGFβ, HGF, IL-6, IL-8, TNC, collagens I and III were upregulated in fibroblasts infected by H. pylori (cagA+vacA+).…”

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confidence: 99%

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Role of Helicobacter pylori infection in cancer‐associated fibroblast‐induced epithelial‐mesenchymal transition in vitro

et al. 2018

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BackgroundMajor human gastrointestinal pathogen Helicobacter pylori (H. pylori) colonizes the gastric mucosa causing inflammation and severe complications including cancer, but the involvement of fibroblasts in the pathogenesis of these disorders in H. pylori‐infected stomach has been little studied. Normal stroma contains few fibroblasts, especially myofibroblasts. Their number rapidly increases in the reactive stroma surrounding inflammatory region and neoplastic tissue; however, the interaction between H. pylori and fibroblasts remains unknown. We determined the effect of coincubation of normal rat gastric fibroblasts with alive H. pylori (cagA+vacA+) and H. pylori (cagA−vacA−) strains on the differentiation of these fibroblasts into cells possessing characteristics of cancer‐associated fibroblasts (CAFs) able to induce epithelial‐mesenchymal transition (EMT) of normal rat gastric epithelial cells (RGM‐1).Materials and MethodsThe panel of CAFs markers mRNA was analyzed in H. pylori (cagA+vacA+)‐infected fibroblasts by RT‐PCR. After insert coculture of differentiated fibroblasts with RGM‐1 cells from 24 up to 48, 72, and 96 hours, the mRNA expression for EMT‐associated genes was analyzed by RT‐PCR.ResultsThe mRNA expression for CAFs markers was significantly increased after 72 hours of infection with H. pylori (cagA+vacA+) but not H. pylori (cagA−vacA−) strain. Following coculture with CAFs, RGM‐1 cells showed significant decrease in E‐cadherin mRNA, and the parallel increase in the expression of Twist and Snail transcription factors mRNA was observed along with the overexpression of mRNAs for TGFβR, HGFR, FGFR, N‐cadherin, vimentin, α‐SMA, VEGF, and integrin‐β1.Conclusion Helicobacter pylori (cagA+vacA+) strain induces differentiation of normal fibroblasts into CAFs, likely to initiate the EMT process in RGM‐1 epithelial cell line.

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“…FSP is considered as a marker of fibroblasts in different organs undergoing tissue remodeling and helps to identify fibroblasts derived from EMT in several organs including the liver 5859, 60. Herein, we have shown that possible downstream targets of NFκB and STAT3 pathways including TGFβ, HGF, IL‐6, IL‐8, TNC, collagens I and III were upregulated in fibroblasts infected by H. pylori (cagA+vacA+).…”

Section: Discussionmentioning

confidence: 86%

“…FSP is considered as a marker of fibroblasts in different organs undergoing tissue remodeling and helps to identify fibroblasts derived from EMT in several organs including the liver 58. H. pylori can stimulate TLRs leading to activation of innate immunity against bacterial inflammation, thus creating an inflammatory microenvironment, a prerequisite for tumor development through activation of NF-κB and STAT3 pathways in human GC 59,60. Herein, we have shown that possible downstream targets of NFκB and STAT3 pathways including TGFβ, HGF, IL-6, IL-8, TNC, collagens I and III were upregulated in fibroblasts infected by H. pylori (cagA+vacA+).…”

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confidence: 99%

Role of Helicobacter pylori infection in cancer‐associated fibroblast‐induced epithelial‐mesenchymal transition in vitro

et al. 2018

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“…As STAT3 promotes tumor progression by inducing tumor cell proliferation, inhibiting apoptosis and increasing tumor invasion and metastasis by enhancing EMT, GRIM19‐mediated STAT3 inhibition is also reported to be associated with tumor suppression in many cancers. In brief, GRIM19 expression is decreased and negatively correlates with STAT3 activation in gastric cancer, colon cancer, breast cancer, ovarian cancer, and HCC, leading to poor patient prognosis. As we show that GRIM19 expression is negatively correlated with STAT3 activation, low GRIM19 expression is the significant factor for poor prognosis in patients with HCC.…”

Section: Discussionmentioning

confidence: 99%

OLFM4 Enhances STAT3 Activation and Promotes Tumor Progression by Inhibiting GRIM19 Expression in Human Hepatocellular Carcinoma

et al. 2019

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Olfactomedin 4 (OLFM4) induces signal transducer and activator of transcription 3 (STAT3) activation by inhibiting gene associated with retinoid‐interferon‐induced mortality 19 (GRIM19), a strong STAT3 suppressor gene; however, the mechanisms of OLFM4 for regulating GRIM19‐STAT3 cascade in hepatocellular carcinoma (HCC) remain unclear. The functions and regulations of OLFM4, GRIM19, and STAT3 activation in HCC progression were evaluated using surgical specimens collected from 111 HCC patients or 2 HCC cell lines in vitro . Moreover, the cancer stem cell–like property of OLFM4 mediated by leucine‐rich repeat‐containing G protein‐coupled receptor 5 (LGR5), known as an intestinal stem cell marker, was investigated. OLFM4 was increased in HCC compared with adjacent liver tissue. The multivariate analysis revealed that high OLFM4 expression was an independent factor for poor prognosis. OLFM4 expression was negatively correlated with GRIM19 expression and positively correlated with STAT3 activation in HCC, thereby increasing cell cycle progression. OLFM4 knockdown in HCC cells increased GRIM19 expression and inhibited STAT3 activation; however, after double knockdown of GRIM19 and OLFM4, STAT3 activation decreased by OLFM4 knockdown was increased again. OLFM4 knockdown increased cell apoptosis, inhibited cell proliferation, and suppressed cancer stem cell–like property in HCC cells. The incidence of hematogenous recurrence was higher in HCC patients with high OLFM4 expression, suggesting that anoikis resistance of HCC was enhanced by OLFM4. In clinical cases, LGR5 expression and CD133 expression was correlated with OLFM4 expression in HCC, leading to poor patient prognosis. In vitro , LGR5 enhanced cancer stem cell–like property by up‐regulating OLFM4 through the Wnt signaling pathway. Conclusion : OLFM4 is induced by the LGR5‐Wnt signaling pathway and is strongly associated with aggressive tumor progression and poor prognosis in HCC by regulating STAT3‐induced tumor cell proliferation and cancer stem cell–like property. Therefore, OLFM4 is a novel prognostic predictor and a potential therapeutic target for patients with HCC.

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“…GRIM-19 is also a component of complex I in the electron transport chain and acts as a chaperone to recruit STAT3 into the inner mitochondrial membrane, thus modulating its mitochondria-specific functions [ 135 ]. Recently, Huang and colleagues suggested mitochondrial GRIM-19 as potential therapeutic target for STAT3-dependent carcinogenesis of gastric cancer [ 73 ].…”

Section: Stat3-interacting Proteinsmentioning

confidence: 99%

STAT3 Interactors as Potential Therapeutic Targets for Cancer Treatment

Laudisi

Cherubini

Monteleone

et al. 2018

IJMS

107

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Signal transducers and activators of transcription (STATs) mediate essential signaling pathways in different biological processes, including immune responses, hematopoiesis, and neurogenesis. Among the STAT members, STAT3 plays crucial roles in cell proliferation, survival, and differentiation. While STAT3 activation is transient in physiological conditions, STAT3 becomes persistently activated in a high percentage of solid and hematopoietic malignancies (e.g., melanoma, multiple myeloma, breast, prostate, ovarian, and colon cancers), thus contributing to malignant transformation and progression. This makes STAT3 an attractive therapeutic target for cancers. Initial strategies aimed at inhibiting STAT3 functions have focused on blocking the action of its activating kinases or sequestering its DNA binding ability. More recently, the diffusion of proteomic-based techniques, which have allowed for the identification and characterization of novel STAT3-interacting proteins able to modulate STAT3 activity via its subcellular localization, interact with upstream kinases, and recruit transcriptional machinery, has raised the possibility to target such cofactors to specifically restrain STAT3 oncogenic functions. In this article, we summarize the available data about the function of STAT3 interactors in malignant cells and discuss their role as potential therapeutic targets for cancer treatment.

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Mitochondrial GRIM-19 as a potential therapeutic target for STAT3-dependent carcinogenesis of gastric cancer

Cited by 20 publications

References 45 publications

Role of Helicobacter pylori infection in cancer‐associated fibroblast‐induced epithelial‐mesenchymal transition in vitro

Role of Helicobacter pylori infection in cancer‐associated fibroblast‐induced epithelial‐mesenchymal transition in vitro

OLFM4 Enhances STAT3 Activation and Promotes Tumor Progression by Inhibiting GRIM19 Expression in Human Hepatocellular Carcinoma

STAT3 Interactors as Potential Therapeutic Targets for Cancer Treatment

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