Inhibition of RON kinase potentiates anti-CTLA-4 immunotherapy to shrink breast tumors and prevent metastatic outgrowth

Ekiz, H. Atakan; Lai, Shu Chin Alicia; Gundlapalli, Harika; Haroun, Fadi; Williams, Matthew A.; Welm, Alana L.

doi:10.1080/2162402x.2018.1480286

Cited by 24 publications

(23 citation statements)

References 73 publications

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“…In this study, we found that MSP signaling via its receptor, RON, is critical for growth and proliferation of KB1P mammary cancer cells both in vitro and in vivo. These data accord well with previous publications in other mammary tumor models that rely on artificial, ectopic expression of MSP or the RON receptor (6,7,(9)(10)(11)(12)14). Most mechanistic work on the MSP-RON axis has used cell lines derived from the MMTV-PyMT model (6,9,12,14) that overexpress MSP, or genetically engineered mouse models in which Mst1r expression is driven by the MMTV promoter (7,11).…”

Section: Discussionsupporting

confidence: 87%

“…MSP and RON (over)-expression in breast cancer specimens correlates with poor prognosis and distant recurrence (5,6), suggesting that the MSP-RON axis contributes to disease progression. Indeed, experimental models, in which MSP or RON are overexpressed or the RON receptor is inhibited or genetically deleted, show that the MSP-RON axis drives mammary tumor progression and metastasis (6)(7)(8)(9)(10)(11)(12)(13)(14).…”

Section: Recepteur D'origine Nantais or Ron Is A Receptor Tyrosine Kimentioning

confidence: 99%

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The MSP-RON axis stimulates cancer cell growth in models of triple negative breast cancer

Millar

Kilbey

Remak

et al. 2020

Preprint

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Triple negative breast cancer is the most aggressive subtype of breast cancer with poor prognosis and high rates of relapse. The lack of actionable targets for TNBC has contributed to the high mortality rates of this disease, and new candidate molecules for potential manipulation are urgently required. Here, we show that macrophage-stimulating protein (MSP) and its tyrosine kinase receptor, RON, are potent drivers of cancer cell growth and tumor progression in a mouse model of TNBC driven by the loss of Trp53 and Brca1. After comparison of two genetically engineered mouse models of TNBC, we found that mammary tumors from K14-Cre;Brca1 F/F ;Trp53 F/F (KB1P) mice exhibit high endogenous levels of MSP and RON expression. We show that MSP stimulates AKT and ERK1/2 activation as well as cancer cell growth in KB1P cell lines, while genetic and pharmacological inhibition of RON prevents these effects. Similarly, KB1P tumor progression in mice was robustly attenuated by treatment with a RON inhibitor with accompanied reduction in the proliferation marker, Ki-67.Our findings in a mouse model where MSP and RON expression are naturally increased provide evidence that this receptor and its ligand are viable candidate molecules for targeted treatment of TNBC.

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Section: Discussionsupporting

confidence: 87%

Section: Recepteur D'origine Nantais or Ron Is A Receptor Tyrosine Kimentioning

confidence: 99%

The MSP-RON axis stimulates cancer cell growth in models of triple negative breast cancer

Millar

Kilbey

Remak

et al. 2020

Preprint

View full text Add to dashboard Cite

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“…In addition, Ruiz-Torres et al (48) demonstrated that the RON signaling pathway is associated with the immunosuppressive microenvironment in breast cancer. Ekiz et al (49) described that inhibition of RON kinase potentiates checkpoint immunotherapy in breast cancer. It is expected that the effectiveness of RON targeting anticancer therapy can be…”

Section: Ron Expression --------------------------------mentioning

confidence: 99%

Receptor tyrosine kinase, RON, promotes tumor progression by regulating EMT and the MAPK signaling pathway in human oral squamous cell carcinoma

Kim

Lee

et al. 2019

Int J Oncol

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The receptor tyrosine kinase, recepteur d'origine nantais (RON), is known to be associated with the progression, metastasis, and prognosis of various types of cancers. Nevertheless, the role of RON in human oral squamous cell carcinoma (OSCC) is unclear. This study evaluated whether RON affects oncogenic behavior, oncogenic signaling pathways, and clinical outcomes, including survival, in human OSCC. Reverse transcription-PCR, quantitative PCR, western blotting and immunohistochemical staining were used to determine mRNA and protein expression levels of RON. Cell invasion, migration and apoptosis assays were used to assess the functional effects of small interfering RNA-mediated knockdown of RON or snail family transcriptional repressor 2 (SLUG). RON knockdown suppressed tumor cell invasion and migration and enhanced apoptosis in human OSCC cells. RON knockdown also decreased the phosphorylation of MAPK signaling proteins, such as ERK1/2, JNK and p38. In addition, RON knockdown suppressed the expression of the epithelial mesenchymal transition (EMT)-related transcription factor, SLUG. SLUG knockdown blocked the enhancement of cell invasion and migration induced by macrophage-stimulation protein (MSP)-mediated RON activation in OSCC cells. The cell morphology was changed to spindle-like shape under MSP-mediated RON activation in OSCC cells. RON was overexpressed in both fresh and paraffin-embedded human OSCC tissues. Taken together, these results indicate that RON contributed to tumor progression by regulating the EMT-related factor, SLUG, and the MAPK pathway in OSCC. This study may provide a theoretical basis for the application of RON-targeting agents, currently being studied in various cancer fields, for the treatment of OSCC.

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“…CTLA-4 refers to an inhibitory molecule, which is expressed on the activated T cells, besides critically contributing to the balance existing between the pro-and anti-immune responses by downregulating the T cell signaling 23 . It has been reported that CTLA-4 overexpressed had a correlation with the poor prognosis in autoimmune diseases as well as the speci c kinds of cancer, including osteosarcoma and Ewing's sarcoma [24][25][26][27] ; however, the latent part played by CTLA-4 polymorphism in malignant bone tumors patients continue to be unclear. There are a number of research works that have investigated the correlation existing between the + 49G/A of the CTLA-4 gene and the susceptibility to malignant bone tumors, nevertheless, these results from published articles remained not just controversial but inconclusive as well.…”

Section: Discussionmentioning

confidence: 99%

Association of The Cytotoxic T Lymphocyte Antigen-4 +49G/A Gene Polymorphism with Susceptibility to Malignant Bone Tumors

Guo

2020

Preprint

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Background Earlier research works have studied the part that cytotoxic T-lymphocyte antigen-4 (CTLA-4) plays in the carcinogenesis of malignant bone tumors, nonetheless, findings had inconsistency. The current investigation aims at clarifying the association between CTLA-4 polymorphism and malignant bone tumor susceptibility through the meta-analysis.Methods We searched pertinent research works in not just PubMed, but also EMBASE, Cochrane library, and Chinese National Knowledge Infrastructure (CNKI) databases in humans published before October 2019. The use of the pooled odds ratio (OR) with its 95% confidence interval (95%CI) was made for estimating the strengths of the correlation existing between the CTLA-4 genetic polymorphism and malignant bone tumors susceptibility. An aggregate of six research works with 1191 malignant bone tumors patients and 1418 controls were selected eventually. The pooled results shed light on the fact that CTLA-4 +49G/A polymorphism had a significant correlation with an augmented vulnerability to the malignant bone tumors (A vs. G: OR=1.37, 95%CI=1.22-1.54; GA vs. GG: OR=1.20, 95%CI=1.01-1.42; AA vs. GG: OR=2.13, 95%CI=1.63-2.78; GA+AA vs. GG: OR=1.35, 95%CI=1.15-1.59; AA vs. GG+GA: OR=2.02, 95%CI=1.60-2.56). Subgroup analysis indicated that there exists a statistically significant correlation between CTLA-4 +49G/A polymorphism and augmented susceptibility to the malignant bone tumor in the population-based or hospital-based samples, and Ewing’s sarcoma or osteosarcoma. Moreover, there was also not observed any considerable heterogeneity across the research works. Results Our results suggest that the CTLA-4 +49G/A polymorphism may play a pivotal part in the carcinogenesis of malignant bone tumors. Conclusions More research works, on the basis of the large sample sizes as well as homogeneous specimens, are needed in order to verify these results.

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Inhibition of RON kinase potentiates anti-CTLA-4 immunotherapy to shrink breast tumors and prevent metastatic outgrowth

Cited by 24 publications

References 73 publications

The MSP-RON axis stimulates cancer cell growth in models of triple negative breast cancer

The MSP-RON axis stimulates cancer cell growth in models of triple negative breast cancer

Receptor tyrosine kinase, RON, promotes tumor progression by regulating EMT and the MAPK signaling pathway in human oral squamous cell carcinoma

Association of The Cytotoxic T Lymphocyte Antigen-4 +49G/A Gene Polymorphism with Susceptibility to Malignant Bone Tumors

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