Your search keyword '"ron receptor tyrosine kinase"' showing total 24 results

1. The MSP‐RON pathway regulates liver fibrosis through transforming growth factor beta‐dependent epithelial–mesenchymal transition.

Author

Weng, Tianhao, Yan, Dong, Shi, Danrong, Zhu, Miaojin, Liu, Yizhi, Wu, Zhigang, Tang, Taoming, Zhu, Linwei, Zhang, Hong, Yao, Hangping, and Li, Lanjuan

Subjects

*TRANSFORMING growth factors, *TRANSFORMING growth factors-beta, *EPITHELIAL-mesenchymal transition, *EPIDERMAL growth factor receptors, *PROTEIN expression, *SMALL molecules, *FIBROSIS

Abstract

Background: Liver fibrosis is pathologically important in the liver cirrhosis progression. The epithelial–mesenchymal transition (EMT) is crucial for organ fibrosis. Macrophage‐stimulating protein (MSP) and its receptor tyrosine kinase, RON, promote cellular EMT. However, their role in liver fibrosis is unclear. Here, we clarify the biological profile, potential mechanisms and therapeutic targets of the MSP‐RON pathway in liver fibrosis. Materials and methods: Macrophage‐stimulating protein expression and its correlation with clinicopathological characteristics of cirrhosis were evaluated in 57 clinical cases and a control group. The effect of MSP‐RON pathway in liver fibrosis was determined in vitro and in vivo. The therapeutic effects of MSP or RON inhibition on liver fibrosis were evaluated in a mouse liver fibrosis model. Results: Macrophage‐stimulating protein is upregulated in liver cirrhosis, which was associated with poor patient prognosis. The MSP‐RON pathway promoted hepatocytes EMT. MSP‐RON‐induced EMT depends on the transforming growth factor beta (TGF‐β) pathway and is regulated by TGF‐β inhibitors. In animal models, an MSP blocking antibody and a small molecule inhibitor of RON, BMS‐777607, both inhibited liver fibrosis progression. Conclusion: Our study revealed that MSP is an important biomarker in liver cirrhosis progression and can be used to prognose patients. The MSP‐RON pathway promotes the EMT of hepatocytes and the progress of fibrosis via a TGF‐β related pathway. Consequently, we identified a new treatment strategy for liver cirrhosis through targeted inhibition of MSP/RON. This research increases the understanding of EMT‐modulated liver fibrosis and provides new insights into biomarkers and therapeutic targets of liver fibrosis. [ABSTRACT FROM AUTHOR]

Published

2021

2. Therapeutic efficacy of a novel humanized antibody-drug conjugate recognizing plexin-semaphorin-integrin domain in the RON receptor for targeted cancer therapy

Author

Xiang-Min Tong, Liang Feng, Sreedhar Reddy Suthe, Tian-Hao Weng, Chen-Yu Hu, Yi-Zhi Liu, Zhi-Gang Wu, Ming-Hai Wang, and Hang-Ping Yao

Subjects

RON receptor tyrosine kinase, PSI domain, Monoclonal antibody, Humanization, Antibody-drug conjugates, Receptor internalization, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract Background Antibody-drug conjugates (ADCs) targeting the RON receptor, a tumorigenic factor contributing to cancer malignancy, has been considered as a novel strategy for cancer therapy. Here we describe a humanized antibody recognizing the RON plexin-semaphorin-integrin (PSI) domain with increased drug delivery capability for potential clinical application. Method Monoclonal antibody PCM5B14 specific to the human and monkey RON PSI domain was generated and characterized by various immunological methods. Humanized antibody H5B14 was created by grafting PCM5B14 complementarity-determining regions into human IgG1/κ acceptor frameworks and conjugated with monomethyl auristatin E and duocarmycin to form two H5B14-based ADCs. Stability of H5B14-based ADCs in human plasma was measured using hydrophobic interaction chromatography. Various biochemical and biological assays were used to determine ADC- regulated RON internalization, cell viability, spheroid formation, and death of cancer stem-like cells. Efficacies of H5B14-based ADCs in vivo were validated using tumor xenograft models. Maximal tolerated doses of H5B14-based ADCs were established in mice. Results H5B14 was highly specific to the human RON PSI domain and superior over other anti-RON ADCs in induction of RON internalization in various cancer cell lines tested. H5B14-based ADCS had a drug to antibody ratio of ~ 3.70:1 and were stable in human plasma with a minimal dissociation within a 10-day period. Functionally, H5B14-mediated drug delivery decreased cell viability at early stages with an average IC50 at ~ 20 nM in multiple cancer cell lines examined. H5B14-based ADCs also inhibited spheroid formation and caused death of cancer stem-like cells with RON+/CD44+/ESA+ phenotypes. In vivo, H5B14-based ADCs in a single injection inhibited tumor xenograft growth mediated by multiple cancer cell lines. Tumoristatic concentrations calculated from xenograft tumor models were in the range of 0.63 to 2.0 mg/kg bodyweight. Significantly, H5B14-based ADCs were capable of eradicating tumors at variable levels across multiple xenograft models regardless their malignant statuses. Toxicologically, H5B14-based ADCs were well tolerated in mice up to 60 mg/kg. Conclusion H5B14-based ADCs targeting the RON PSI domain are superior in inducing RON internalization, leading to robust drug delivery and overall inhibition and eradication of tumors in multiple xenograft models. These findings warrant H5B14-based ADCs for clinical trials in the future.

Published

2019

3. Therapeutic efficacy, pharmacokinetic profiles, and toxicological activities of humanized antibody-drug conjugate Zt/g4-MMAE targeting RON receptor tyrosine kinase for cancer therapy

Author

Hang-Ping Yao, Liang Feng, Sreedhar Reddy Suthe, Ling-Hui Chen, Tian-Hao Weng, Chen-Yu Hu, Eun Sung Jun, Zhi-Gang Wu, Wei-Lin Wang, Song Cheol Kim, Xiang-Min Tong, and Ming-Hai Wang

Subjects

Pancreatic cancer, RON receptor tyrosine kinase, Antibody-rug conjugates, Pharmacokinetics, Xenograft tumor model, Therapeutic efficacy, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract Background Aberrant expression of the RON receptor tyrosine kinase is a pathogenic feature and a validated drug target in various types of cancers. Currently, therapeutic antibodies targeting RON for cancer therapy are under intensive evaluation. Here we report the development and validation of a novel humanized anti-RON antibody-drug conjugate for cancer therapy. Methods Antibody humanization was achieved by grafting sequences of complementarity-determining regions from mouse monoclonal antibody Zt/g4 into human IgG1/κ acceptor frameworks. The selected humanized Zt/g4 subclone H1L3 was conjugated with monomethyl auristatin E using a dipeptide linker to form H-Zt/g4-MMAE. Pharmacokinetic analysis of H-Zt/g4-MMAE was determined using hydrophobic interaction chromatography and a MMAE ADC ELISA kit. Biochemical and biological assays were used for measuring RON expression, internalization, cell viability and death. Therapeutic efficacies of H-Zt/g4-MMAE were validated in vivo using three pancreatic cancer xenograft models. Toxicological activities of H-Zt/g4-MMAE were determined in mouse and cynomolgus monkey. Results H-Zt/g4-MMAE had a drug to antibody ratio of 3.77:1 and was highly stable in human plasma with a dissociation rate less than 5% within a 20 day period. H-Zt/g4-MMAE displayed a favorable pharmacokinetic profile in both mouse and cynomolgus monkey. In vitro, H-Zt/g4-MMAE induced RON internalization, which results in killing of pancreatic cancer cells with IC50 values at 10–20 nM. In vivo, H-Zt/g4-MMAE inhibited pancreatic cancer xenograft growth with tumoristatic concentrations at 1~3 mg/kg bodyweight. Significantly, H-Zt/g4-MMAE eradicated tumors across multiple xenograft models regardless their chemoresistant and metastatic statuses. Moreover, H-Zt/g4-MMAE inhibited and eradicated xenografts mediated by pancreatic cancer stem-like cells and by primary cells from patient-derived tumors. Toxicologically, H-Zt/g4-MMAE is well tolerated in mice up to 60 mg/kg. In cynomolgus monkey, H-Zt/g4-MMAE up to 30 mg/kg had a manageable and reversible toxicity profile. Conclusions H-Zt/g4-MMAE is superior in eradication of pancreatic cancer xenografts with favorable pharmacokinetic profiles and manageable toxicological activities. These findings warrant the transition of H-Zt/g4-MMAE into clinical trials in the future.

Published

2019

4. Aberrant RON and MET Co-overexpression as Novel Prognostic Biomarkers of Shortened Patient Survival and Therapeutic Targets of Tyrosine Kinase Inhibitors in Pancreatic Cancer

Author

Chen-Yu Hu, Xiang-Ming Xu, Bo Hong, Zhi-Gang Wu, Yun Qian, Tian-Hao Weng, Yi-Zhi Liu, Tao-Ming Tang, Ming-Hai Wang, and Hang-Ping Yao

Subjects

pancreatic cancer, tyrosine kinase inhibitors, RON receptor tyrosine kinase, MET receptor tyrosine kinase, prognosis biomarker, therapeutic target, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

RON (recepteur d'origine nantais) and MET (hepatocyte growth factor receptor) are tyrosine kinase receptors. Various cancers have aberrant RON and MET expression and activation, which contribute to cancer cell proliferation, invasiveness, and metastasis. Here, we explored RON and MET expression in pancreatic cancer and their relationship with overall survival (OS) time, and evaluated their significance as therapeutic targets of tyrosine kinase inhibitors in pancreatic cancer. We enrolled 227 patients with pancreatic cancer in the study. RON and MET expression was analyzed by immunohistochemical staining. Four human pancreatic cancer cell lines expressing variable levels of RON or MET and four MET superfamily inhibitors (BMS777607, PHA665752, INCB28060, Tivantinib) were used. The effect of the four tyrosine kinase inhibitors on cell viability, migration, and apoptosis were determined using cell viability, scratch wound healing, and Caspase-Glo 3/7 assays. Cellular signaling was analyzed by immunoprecipitation and western blotting. The therapeutic efficacy of the tyrosine kinase inhibitors was determined with mouse xenograft pancreatic cancer models in vivo. There was wide aberrant RON and MET expression in the cancer tissues. In 227 pancreatic cancer samples, 33% had RON overexpression, 41% had MET overexpression, and 15.4% had RON and MET co-overexpression. RON and MET expression were highly correlated. RON and MET expression levels were significantly related to OS. Patients with RON and MET co-overexpression had poorer OS. BMS777607 and PHA665752 inhibited pancreatic cancer cell viability and migration, and promoted apoptosis by inhibiting RON and MET phosphorylation and further inhibiting the downstream signaling pathways in vitro. They also inhibited tumor growth and further inhibited phosphorylated (phosphor)-RON and phospho-MET expression in the mouse xenograft models in vivo effectively. INCB28060, which inhibits the MET signaling pathway alone, was not effective. RON and MET can be important indicators of prognosis in pancreatic cancer. Tyrosine kinase inhibitors targeting RON and MET in pancreatic cancer are a novel and potential approach for pancreatic cancer therapy.

Published

2019

5. RON and MET Co-overexpression Are Significant Pathological Characteristics of Poor Survival and Therapeutic Targets of Tyrosine Kinase Inhibitors in Triple-Negative Breast Cancer.

Author

Tian-Hao Weng, Min-Ya Yao, Xiang-Ming Xu, Chen-Yu Hu, Shu-Hao Yao, Yi-Zhi Liu, Zhi-Gang Wu, Tao-Ming Tang, Pei-Fen Fu, Ming-Hai Wang, and Hang-Ping Yao

Subjects

*PROTEIN-tyrosine kinases, *KINASE inhibitors, *TRIPLE-negative breast cancer, *TREATMENT effectiveness, *CELL migration

Abstract

Purpose: Triple-negative breast cancer (TNBC) is highly malignant and has poor prognosis and a high mortality rate. The lack of effective therapy has spurred our investigation of new targets for treating this malignant cancer. Here, we identified RON (macrophage-stimulating 1 receptor) and MET (MET proto-oncogene, receptor tyrosine kinase) as a prognostic biomarker and therapeutic targets for potential TNBC treatment. Materials and Methods: We analyzed RON and MET expression in 187 primary TNBC clinical samples with immunohistochemistry. We validated the targeted therapeutic effects of RON and MET in TNBC using three tyrosine kinase inhibitors (TKIs): BMS-777607, INCB28060, and tivantinib. The preclinical therapeutic efficacy of the TKIs was mainly estimated using a TNBC xenograft model. Results: Patients with TNBC had widespread, abnormal expression of RON and MET. There was RON overexpression, MET overexpression, and RON and MET co-overexpression in 63 (33.7%), 63 (33.7%), and 43 cases (23.0%), respectively, which had poor prognosis and short survival. In vivo, the TKI targeting RON ant MET inhibited the activation of the downstream signaling molecules, inhibited TNBC cell migration and proliferation, and increased TNBC cell apoptosis; in the xenograft model, they significantly inhibited tumor growth and shrank tumor volumes. The TKI targeting RON and Met, such as BMS-777607 and tivantinib, yielded stronger anti-tumor effects than INCB28060. Conclusion: RON and MET co-overexpression can be significant pathological characteristics in TNBC for poor prognosis. TKIs targeting RON and MET have stronger drug development potential for treating TNBC. [ABSTRACT FROM AUTHOR]

Published

2020

6. Aberrant RON and MET Co-overexpression as Novel Prognostic Biomarkers of Shortened Patient Survival and Therapeutic Targets of Tyrosine Kinase Inhibitors in Pancreatic Cancer.

Author

Hu, Chen-Yu, Xu, Xiang-Ming, Hong, Bo, Wu, Zhi-Gang, Qian, Yun, Weng, Tian-Hao, Liu, Yi-Zhi, Tang, Tao-Ming, Wang, Ming-Hai, and Yao, Hang-Ping

Subjects

PROTEIN-tyrosine kinases, PANCREATIC cancer, MET receptor, KINASE inhibitors, CANCER cell migration

Abstract

RON (recepteur d'origine nantais) and MET (hepatocyte growth factor receptor) are tyrosine kinase receptors. Various cancers have aberrant RON and MET expression and activation, which contribute to cancer cell proliferation, invasiveness, and metastasis. Here, we explored RON and MET expression in pancreatic cancer and their relationship with overall survival (OS) time, and evaluated their significance as therapeutic targets of tyrosine kinase inhibitors in pancreatic cancer. We enrolled 227 patients with pancreatic cancer in the study. RON and MET expression was analyzed by immunohistochemical staining. Four human pancreatic cancer cell lines expressing variable levels of RON or MET and four MET superfamily inhibitors (BMS777607, PHA665752, INCB28060, Tivantinib) were used. The effect of the four tyrosine kinase inhibitors on cell viability, migration, and apoptosis were determined using cell viability, scratch wound healing, and Caspase-Glo 3/7 assays. Cellular signaling was analyzed by immunoprecipitation and western blotting. The therapeutic efficacy of the tyrosine kinase inhibitors was determined with mouse xenograft pancreatic cancer models in vivo. There was wide aberrant RON and MET expression in the cancer tissues. In 227 pancreatic cancer samples, 33% had RON overexpression, 41% had MET overexpression, and 15.4% had RON and MET co-overexpression. RON and MET expression were highly correlated. RON and MET expression levels were significantly related to OS. Patients with RON and MET co-overexpression had poorer OS. BMS777607 and PHA665752 inhibited pancreatic cancer cell viability and migration, and promoted apoptosis by inhibiting RON and MET phosphorylation and further inhibiting the downstream signaling pathways in vitro. They also inhibited tumor growth and further inhibited phosphorylated (phosphor)-RON and phospho-MET expression in the mouse xenograft models in vivo effectively. INCB28060, which inhibits the MET signaling pathway alone, was not effective. RON and MET can be important indicators of prognosis in pancreatic cancer. Tyrosine kinase inhibitors targeting RON and MET in pancreatic cancer are a novel and potential approach for pancreatic cancer therapy. [ABSTRACT FROM AUTHOR]

Published

2019

7. Metabolic Profiling Reveals Aggravated Non-Alcoholic Steatohepatitis in High-Fat High-Cholesterol Diet-Fed Apolipoprotein E-Deficient Mice Lacking Ron Receptor Signaling

Author

Joselyn N. Allen, Adwitia Dey, Jingwei Cai, Jingtao Zhang, Yuan Tian, Mary Kennett, Yanling Ma, T. Jake Liang, Andrew D. Patterson, and Pamela A. Hankey-Giblin

Subjects

Ron receptor tyrosine kinase, macrophage stimulating protein (MSP), non-alcoholic steatohepatitis, lipid metabolism, mass spectrometry, nuclear magnetic resonance, Microbiology, QR1-502

Abstract

Non-alcoholic steatohepatitis (NASH) represents the progressive sub-disease of non-alcoholic fatty liver disease that causes chronic liver injury initiated and sustained by steatosis and necroinflammation. The Ron receptor is a tyrosine kinase of the Met proto-oncogene family that potentially has a beneficial role in adipose and liver-specific inflammatory responses, as well as glucose and lipid metabolism. Since its discovery two decades ago, the Ron receptor has been extensively investigated for its differential roles on inflammation and cancer. Previously, we showed that Ron expression on tissue-resident macrophages limits inflammatory macrophage activation and promotes a repair phenotype, which can retard the progression of NASH in a diet-induced mouse model. However, the metabolic consequences of Ron activation have not previously been investigated. Here, we explored the effects of Ron receptor activation on major metabolic pathways that underlie the development and progression of NASH. Mice lacking apolipoprotein E (ApoE KO) and double knockout (DKO) mice that lack ApoE and Ron were maintained on a high-fat high-cholesterol diet for 18 weeks. We observed that, in DKO mice, the loss of ligand-dependent Ron signaling aggravated key pathological features in steatohepatitis, including steatosis, inflammation, oxidation stress, and hepatocyte damage. Transcriptional programs positively regulating fatty acid (FA) synthesis and uptake were upregulated in the absence of Ron receptor signaling, whereas lipid disposal pathways were downregulated. Consistent with the deregulation of lipid metabolism pathways, the DKO animals exhibited increased accumulation of FAs in the liver and decreased level of bile acids. Altogether, ligand-dependent Ron receptor activation provides protection from the deregulation of major metabolic pathways that initiate and aggravate non-alcoholic steatohepatitis.

Published

2020

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

Author

Huseyin Atakan Ekiz, Shu-Chin Alicia Lai, Harika Gundlapalli, Fadi Haroun, Matthew A. Williams, and Alana L. Welm

Subjects

immunotherapy, breast cancer, metastasis, ron receptor tyrosine kinase, anti-ctla-4, anti-pd-1, mmtv-pymt, Immunologic diseases. Allergy, RC581-607, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

The advent of immune checkpoint blockade as a new strategy for immunotherapy has changed the outlook for many aggressive cancers. Although complete tumor eradication is attainable in some cases, durable clinical responses are observed only in a small fraction of patients, underlining urgent need for improvement. We previously showed that RON, a receptor tyrosine kinase expressed in macrophages, suppresses antitumor immune responses, and facilitates progression and metastasis of breast cancer. Here, we investigated the molecular changes that occur downstream of RON activation in macrophages, and whether inhibition of RON can cooperate with checkpoint immunotherapy to eradicate tumors. Activation of RON by its ligand, MSP, altered the gene expression profile of macrophages drastically and upregulated surface levels of CD80 and PD-L1, ligands for T-cell checkpoint receptors CTLA-4 and PD-1. Genetic deletion or pharmacological inhibition of RON in combination with anti-CTLA-4, but not with anti-PD-1, resulted in improved clinical responses against orthotopically transplanted tumors compared to single-agent treatment groups, resulting in complete tumor eradication in 46% of the animals. Positive responses to therapy were associated with higher levels of T-cell activation markers and tumor-infiltrating lymphocytes. Importantly, co-inhibition of RON and anti-CTLA-4 was also effective in clearing metastatic breast cancer cells in lungs, resulting in clinical responses in nearly 60% of the mice. These findings suggest that RON inhibition can be a novel approach to potentiate responses to checkpoint immunotherapy in breast cancer.

Published

2018

9. RON Receptor Tyrosine Kinase in Tumorigenic Stemness as a Therapeutic Target of Antibody-drug Conjugates for Eradication of Triple-negative Breast Cancer Stem Cells.

Author

Suthe SR, Yao HP, Weng TH, and Wang MH

Subjects

Humans, Animals, Mice, Mice, Nude, Epithelial-Mesenchymal Transition, Cell Line, Tumor, Antibodies, Monoclonal therapeutic use, Carcinogenesis, Stem Cells, Immunoconjugates pharmacology, Immunoconjugates therapeutic use, Triple Negative Breast Neoplasms drug therapy

Abstract

Background: Cancer stem-like cells in triple-negative breast cancer (TNBC-SLCs) are the tumorigenic core for malignancy. Aberrant expression of the RON receptor tyrosine kinase has implications in TNBC tumorigenesis and malignancy., Objective: In this study, we identified the RON receptor as a pathogenic factor contributing to TNBC cell stemness and validated anti-RON antibody-drug conjugate Zt/g4-MMAE for eradication of RONexpressing TNBC-SLCs., Methods: Immunofluorescence and Western blotting were used for analyzing cellular marker expression. TNBC-SLCs were isolated by magnetic-immunofluorescence cell-sorting techniques. Spheroids were generated using the ultralow adhesion culture methods. Levels of TNBC-SLC chemosensitivity were determined by MTS assays. TNBC-SLC mediated tumor growth was determined in athymic nude mice. The effectiveness of Zt/g4-induced RON internalization was measured by immunofluorescence analysis. Efficacies of Zt/g4-MMAE in killing TNBC-SLCs in vitro and in eradicating TNBC-SLCmediated tumors were determined in mouse models. All data were statistically analyzed using the GraphPad Prism 7 software., Results: Increased RON expression existed in TNBC-SLCs with CD44+/CD24- phenotypes and ALDH activities and facilitated epithelial to mesenchymal transition. RON-positive TNBC-SLCs enhanced spheroid-formatting capability compared to RON-negative TNBC-SLCs, which were sensitive to small molecule kinase inhibitor BMS-777607. Increased RON expression also promoted TNBC-SLC chemoresistance and facilitated tumor growth at an accelerated rate. In vitro, Zt/g4-MMAE caused massive TNBC-SLC death with an average IC50 value of ~1.56 μg per/ml and impaired TNBC cell spheroid formation. In mice, Zt/g4-MMAE effectively inhibited and/or eradicated TNBC-SLC mediated tumors in a single agent regimen., Conclusion: Sustained RON expression contributes to TNBC-SLC tumorigenesis. Zt/g4-MMAE is found to be effective in vivo in killing TNBC-SLC-mediated xenograft tumors. Our findings highlight the feasibility of Zt/g4-MMAE for the eradication of TNBC-SLCs in the future., (Copyright© Bentham Science Publishers; For any queries, please email at epub@benthamscience.net.)

Published

2023

10. Therapeutic efficacy of a novel humanized antibody-drug conjugate recognizing plexin-semaphorin-integrin domain in the RON receptor for targeted cancer therapy

Author

Tong, Xiang-Min, Feng, Liang, Suthe, Sreedhar Reddy, Weng, Tian-Hao, Hu, Chen-Yu, Liu, Yi-Zhi, Wu, Zhi-Gang, Wang, Ming-Hai, and Yao, Hang-Ping

Published

2019

11. Therapeutic efficacy, pharmacokinetic profiles, and toxicological activities of humanized antibody-drug conjugate Zt/g4-MMAE targeting RON receptor tyrosine kinase for cancer therapy

Author

Yao, Hang-Ping, Feng, Liang, Suthe, Sreedhar Reddy, Chen, Ling-Hui, Weng, Tian-Hao, Hu, Chen-Yu, Jun, Eun Sung, Wu, Zhi-Gang, Wang, Wei-Lin, Kim, Song Cheol, Tong, Xiang-Min, and Wang, Ming-Hai

Published

2019

12. RON and MET Co-overexpression Are Significant Pathological Characteristics of Poor Survival and Therapeutic Targets of Tyrosine Kinase Inhibitors in Triple-Negative Breast Cancer

Author

Min-Ya Yao, Shu-Hao Yao, Ming-Hai Wang, Hangping Yao, Yi-Zhi Liu, Pei-Fen Fu, Tianhao Weng, Tao-Ming Tang, Chen-Yu Hu, Zhigang Wu, and Xiang-Ming Xu

Subjects

0301 basic medicine, Cancer Research, Tyrosine kinase inhibitor, Apoptosis, Triple Negative Breast Neoplasms, Proto-Oncogene Mas, Tyrosine-kinase inhibitor, Receptor tyrosine kinase, chemistry.chemical_compound, Mice, 0302 clinical medicine, Cell Movement, Tumor Cells, Cultured, MET receptor tyrosine kinase, Triple-negative breast cancer, Aged, 80 and over, biology, Middle Aged, Proto-Oncogene Proteins c-met, Prognosis, Gene Expression Regulation, Neoplastic, Survival Rate, Oncology, 030220 oncology & carcinogenesis, Immunohistochemistry, Female, Original Article, RON receptor tyrosine kinase, Tyrosine kinase, Adult, medicine.drug_class, Mice, Nude, 03 medical and health sciences, Breast cancer, medicine, Biomarkers, Tumor, Animals, Humans, Tivantinib, Protein Kinase Inhibitors, Targeting therapy, Aged, Cell Proliferation, business.industry, Cancer, Receptor Protein-Tyrosine Kinases, medicine.disease, Xenograft Model Antitumor Assays, 030104 developmental biology, chemistry, Cancer research, biology.protein, business, Follow-Up Studies

Abstract

Purpose Triple-negative breast cancer (TNBC) is highly malignant and has poor prognosis and a high mortality rate. The lack of effective therapy has spurred our investigation of new targets for treating this malignant cancer. Here, we identified RON (macrophage-stimulating 1 receptor) and MET (MET proto-oncogene, receptor tyrosine kinase) as a prognostic biomarker and therapeutic targets for potential TNBC treatment.Materials and MethodsWe analyzed RON and MET expression in 187 primary TNBC clinical samples with immunohistochemistry. We validated the targeted therapeutic effects of RON and MET in TNBC using three tyrosine kinase inhibitors (TKIs): BMS-777607, INCB28060, and tivantinib. The preclinical therapeutic efficacy of the TKIs was mainly estimated using a TNBC xenograft model.ResultsPatients with TNBC had widespread, abnormal expression of RON and MET. There was RON overexpression, MET overexpression, and RON and MET co-overexpression in 63 (33.7%), 63 (33.7%), and 43 cases (23.0%), respectively, which had poor prognosis and short survival. In vivo, the TKI targeting RON ant MET inhibited the activation of the downstream signaling molecules, inhibited TNBC cell migration and proliferation, and increased TNBC cell apoptosis; in the xenograft model, they significantly inhibited tumor growth and shrank tumor volumes. The TKI targeting RON and Met, such as BMS-777607 and tivantinib, yielded stronger anti-tumor effects than INCB28060.ConclusionRON and MET co-overexpression can be significant pathological characteristics in TNBC for poor prognosis. TKIs targeting RON and MET have stronger drug development potential for treating TNBC.

Published

2019

13. Therapeutic efficacy of a novel humanized antibody-drug conjugate recognizing plexin-semaphorin-integrin domain in the RON receptor for targeted cancer therapy

Author

Tian Hao Weng, Zhi Gang Wu, Yi Zhi Liu, Xiang Min Tong, Liang Feng, Ming Hai Wang, Hangping Yao, Sreedhar Reddy Suthe, and Chen Yu Hu

Subjects

0301 basic medicine, Cancer Research, Immunoconjugates, PSI domain, Receptor internalization, Humanized antibody, Mice, chemistry.chemical_compound, 0302 clinical medicine, Neoplasms, Antineoplastic Combined Chemotherapy Protocols, Immunology and Allergy, Antibody-drug conjugates, Internalization, media_common, biology, Epithelial cancer, cancer stem cells, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Humanization, Oncology, Monomethyl auristatin E, 030220 oncology & carcinogenesis, Drug delivery, Molecular Medicine, Female, RON receptor tyrosine kinase, Oligopeptides, Research Article, Monoclonal antibody, Maximum Tolerated Dose, medicine.drug_class, media_common.quotation_subject, Immunology, Antibodies, Monoclonal, Humanized, lcsh:RC254-282, Duocarmycins, 03 medical and health sciences, Protein Domains, In vivo, Cancer stem cell, Cell Line, Tumor, medicine, Animals, Humans, Pharmacology, CD44, Receptor Protein-Tyrosine Kinases, Tumor xenograft model, Therapeutic efficacy, Xenograft Model Antitumor Assays, body regions, 030104 developmental biology, chemistry, Cancer research, biology.protein

Abstract

Background Antibody-drug conjugates (ADCs) targeting the RON receptor, a tumorigenic factor contributing to cancer malignancy, has been considered as a novel strategy for cancer therapy. Here we describe a humanized antibody recognizing the RON plexin-semaphorin-integrin (PSI) domain with increased drug delivery capability for potential clinical application. Method Monoclonal antibody PCM5B14 specific to the human and monkey RON PSI domain was generated and characterized by various immunological methods. Humanized antibody H5B14 was created by grafting PCM5B14 complementarity-determining regions into human IgG1/κ acceptor frameworks and conjugated with monomethyl auristatin E and duocarmycin to form two H5B14-based ADCs. Stability of H5B14-based ADCs in human plasma was measured using hydrophobic interaction chromatography. Various biochemical and biological assays were used to determine ADC- regulated RON internalization, cell viability, spheroid formation, and death of cancer stem-like cells. Efficacies of H5B14-based ADCs in vivo were validated using tumor xenograft models. Maximal tolerated doses of H5B14-based ADCs were established in mice. Results H5B14 was highly specific to the human RON PSI domain and superior over other anti-RON ADCs in induction of RON internalization in various cancer cell lines tested. H5B14-based ADCS had a drug to antibody ratio of ~ 3.70:1 and were stable in human plasma with a minimal dissociation within a 10-day period. Functionally, H5B14-mediated drug delivery decreased cell viability at early stages with an average IC50 at ~ 20 nM in multiple cancer cell lines examined. H5B14-based ADCs also inhibited spheroid formation and caused death of cancer stem-like cells with RON+/CD44+/ESA+ phenotypes. In vivo, H5B14-based ADCs in a single injection inhibited tumor xenograft growth mediated by multiple cancer cell lines. Tumoristatic concentrations calculated from xenograft tumor models were in the range of 0.63 to 2.0 mg/kg bodyweight. Significantly, H5B14-based ADCs were capable of eradicating tumors at variable levels across multiple xenograft models regardless their malignant statuses. Toxicologically, H5B14-based ADCs were well tolerated in mice up to 60 mg/kg. Conclusion H5B14-based ADCs targeting the RON PSI domain are superior in inducing RON internalization, leading to robust drug delivery and overall inhibition and eradication of tumors in multiple xenograft models. These findings warrant H5B14-based ADCs for clinical trials in the future.

Published

2019

14. Metabolic Profiling Reveals Aggravated Non-Alcoholic Steatohepatitis in High-Fat High-Cholesterol Diet-Fed Apolipoprotein E-Deficient Mice Lacking Ron Receptor Signaling

Author

T. Jake Liang, Jingwei Cai, Yuan Tian, Jingtao Zhang, Joselyn N. Allen, Yanling Ma, Adwitia Dey, Mary J. Kennett, Pamela A. Hankey-Giblin, and Andrew D. Patterson

Subjects

0301 basic medicine, Apolipoprotein E, medicine.medical_specialty, Endocrinology, Diabetes and Metabolism, lcsh:QR1-502, Inflammation, Biology, Biochemistry, lcsh:Microbiology, Article, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, lipid metabolism, medicine, macrophage stimulating protein (MSP), Receptor, Molecular Biology, mass spectrometry, Fatty liver, Lipid metabolism, medicine.disease, nuclear magnetic resonance, 030104 developmental biology, Endocrinology, Ron receptor tyrosine kinase, 030211 gastroenterology & hepatology, non-alcoholic steatohepatitis, Steatohepatitis, Steatosis, medicine.symptom, Tyrosine kinase

Abstract

Non-alcoholic steatohepatitis (NASH) represents the progressive sub-disease of non-alcoholic fatty liver disease that causes chronic liver injury initiated and sustained by steatosis and necroinflammation. The Ron receptor is a tyrosine kinase of the Met proto-oncogene family that potentially has a beneficial role in adipose and liver-specific inflammatory responses, as well as glucose and lipid metabolism. Since its discovery two decades ago, the Ron receptor has been extensively investigated for its differential roles on inflammation and cancer. Previously, we showed that Ron expression on tissue-resident macrophages limits inflammatory macrophage activation and promotes a repair phenotype, which can retard the progression of NASH in a diet-induced mouse model. However, the metabolic consequences of Ron activation have not previously been investigated. Here, we explored the effects of Ron receptor activation on major metabolic pathways that underlie the development and progression of NASH. Mice lacking apolipoprotein E (ApoE KO) and double knockout (DKO) mice that lack ApoE and Ron were maintained on a high-fat high-cholesterol diet for 18 weeks. We observed that, in DKO mice, the loss of ligand-dependent Ron signaling aggravated key pathological features in steatohepatitis, including steatosis, inflammation, oxidation stress, and hepatocyte damage. Transcriptional programs positively regulating fatty acid (FA) synthesis and uptake were upregulated in the absence of Ron receptor signaling, whereas lipid disposal pathways were downregulated. Consistent with the deregulation of lipid metabolism pathways, the DKO animals exhibited increased accumulation of FAs in the liver and decreased level of bile acids. Altogether, ligand-dependent Ron receptor activation provides protection from the deregulation of major metabolic pathways that initiate and aggravate non-alcoholic steatohepatitis.

Published

2020

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

Author

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

Subjects

0301 basic medicine, lcsh:Immunologic diseases. Allergy, medicine.medical_treatment, Immunology, mmtv-pymt, lcsh:RC254-282, Receptor tyrosine kinase, Metastasis, 03 medical and health sciences, 0302 clinical medicine, Immune system, breast cancer, medicine, Immunology and Allergy, metastasis, Receptor, biology, business.industry, Kinase, anti-ctla-4, Immunotherapy, anti-pd-1, medicine.disease, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Immune checkpoint, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Cancer research, biology.protein, ron receptor tyrosine kinase, immunotherapy, business, lcsh:RC581-607, CD80

Abstract

The advent of immune checkpoint blockade as a new strategy for immunotherapy has changed the outlook for many aggressive cancers. Although complete tumor eradication is attainable in some cases, durable clinical responses are observed only in a small fraction of patients, underlining urgent need for improvement. We previously showed that RON, a receptor tyrosine kinase expressed in macrophages, suppresses antitumor immune responses, and facilitates progression and metastasis of breast cancer. Here, we investigated the molecular changes that occur downstream of RON activation in macrophages, and whether inhibition of RON can cooperate with checkpoint immunotherapy to eradicate tumors. Activation of RON by its ligand, MSP, altered the gene expression profile of macrophages drastically and upregulated surface levels of CD80 and PD-L1, ligands for T-cell checkpoint receptors CTLA-4 and PD-1. Genetic deletion or pharmacological inhibition of RON in combination with anti-CTLA-4, but not with anti-PD-1, resulted in improved clinical responses against orthotopically transplanted tumors compared to single-agent treatment groups, resulting in complete tumor eradication in 46% of the animals. Positive responses to therapy were associated with higher levels of T-cell activation markers and tumor-infiltrating lymphocytes. Importantly, co-inhibition of RON and anti-CTLA-4 was also effective in clearing metastatic breast cancer cells in lungs, resulting in clinical responses in nearly 60% of the mice. These findings suggest that RON inhibition can be a novel approach to potentiate responses to checkpoint immunotherapy in breast cancer.

Published

2018

16. HGFL-mediated RON signaling supports breast cancer stem cell phenotypes via activation of non-canonical β-catenin signaling

Author

Sasha J. Ruiz-Torres, Rebekah Karns, Nancy M. Benight, Elyse E. Lower, Jun-Lin Guan, and Susan E. Waltz

Subjects

0301 basic medicine, breast cancer stem cells, Population, medicine.disease_cause, Metastasis, 03 medical and health sciences, 0302 clinical medicine, Breast cancer, breast cancer, β-CATENIN, Medicine, education, education.field_of_study, Tumor microenvironment, business.industry, MST1R, medicine.disease, 3. Good health, 030104 developmental biology, Oncology, Tumor progression, 030220 oncology & carcinogenesis, Immunology, Cancer research, RON receptor tyrosine kinase, Stem cell, business, Carcinogenesis, HGFL, Research Paper

Abstract

// Sasha J. Ruiz-Torres 1 , Nancy M. Benight 1 , Rebekah A. Karns 2 , Elyse E. Lower 3 , Jun-Lin Guan 1 and Susan E. Waltz 1, 4 1 Department of Cancer Biology, University of Cincinnati College of Medicine, Cincinnati, OH 45267, USA 2 Division of Bioinformatics, Cincinnati Children’s Hospital Medical Center, Cincinnati, OH 45229, USA 3 Department of Internal Medicine, University of Cincinnati Medical Center, Cincinnati, OH 45267, USA 4 Research Service, Cincinnati Veterans Affairs Medical Center, Cincinnati, OH 45267, USA Correspondence to: Susan E. Waltz, email: susan.waltz@uc.edu Keywords: RON receptor tyrosine kinase, HGFL, breast cancer stem cells, β-CATENIN, breast cancer Received: March 29, 2017 Accepted: July 11, 2017 Published: July 22, 2017 ABSTRACT Breast cancer stem cells (BCSCs), which drive tumor progression, recurrence, and metastasis, are considered a major challenge for breast cancer treatments, thus the discovery of novel pathways regulating BCSC maintenance remains essential to develop new strategies to effectively target this population and combat disease mortality. The HGFL-RON signaling is overexpressed in human breast cancers and is associated with increased breast cancer progression, metastasis, and poor prognosis. Here, we report that overexpression of RON/MST1R and HGFL/MST1 in cell lines and primary tumors increases BCSC self-renewal, numbers, and tumorigenic potential after syngeneic transplantation. Transcriptome analyses also reveal that the HGFL-RON signaling pathway regulates additional BCSC functions and supports an immunosuppressive microenvironment to stimulate tumor formation and progression. Moreover, we show that genetic and chemical downregulation of HGFL-RON signaling disrupts BCSC phenotypes and tumor growth by suppressing the RON-mediated phosphorylation/activation of β-CATENIN/CTNNB1 and its effector NF-κB/RELA. These studies indicate that HGFL-RON signaling regulates BCSC phenotypes and the tumor microenvironment to drive tumorigenesis and present HGFL/RON as novel therapeutic targets to effectively eradicate BCSCs in patients.

Published

2017

17. Epithelial and Macrophage RON Receptor Signaling Regulates the Antitumor Immune Response in Prostate Cancer

Author

Sullivan, Camille

Subjects

Cellular Biology, RON receptor tyrosine kinase, prostate cancer immunotherapy, tumor-associated macrophage, macrophage activation, tumor microenvironment, antitumor immune response

Abstract

Prostate cancer is the second most common cancer in men and the second leading cause of cancer-related deaths in men in the United States, with 191,930 men estimated to be diagnosed with prostate cancer and 33,330 patients expected to succumb to this disease in 2020 alone. Standard-of-care treatments, including active surveillance, surgery, radiation, and androgen deprivation therapy, provide positive clinical outcomes in patients with localized and regional disease. However, these strategies fail to effectively treat advanced prostate cancer, leading to a 5-year survival rate of 31% in patients with distant stage disease. Cancer immunotherapy has emerged as a powerful therapeutic strategy by enhancing the host immune response, particularly cytotoxic CD8+ T cells, to attack tumors. These strategies have proven successful in numerous cancers, such as melanoma, non-small cell lung cancer, and bladder cancer, however prostate cancer remains poorly responsive to these agents. The work presented in this dissertation demonstrates that the RON receptor tyrosine kinase, an oncogene implicated in the tumorigenesis of several epithelial cancers, is a critical regulator of the antitumor immune response in prostate cancer. Our studies herein identify novel RON-mediated communication networks between prostate tumor cells and immune cells as well as between different immune cell populations in the tumor microenvironment. We show that RON signaling in prostate epithelial cells and macrophages supports M2 macrophage activation and modulates the infiltration of multiple immune cell types with known roles in regulating prostate tumor growth and progression, such as CD4+ and CD8+ T cells. Importantly, our studies reveal that loss of RON signaling in macrophages promotes CD8+ T cell activation. Our deeper analyses show that the regulation of M2 macrophage activation by RON is in part through upregulation of RON expression in macrophages. Further, our preliminary data suggest that RON signaling in either prostate epithelial cells or in macrophages may trigger the activation of multiple pro-tumorigenic and immunosuppressive signaling pathways, including STAT3, AKT, and MAPK, potentially leading to the coordinated regulation of immunostimulatory and immunosuppressive molecule production. Specifically, our preliminary findings suggest that RON may enlist multiple soluble factors, such as HGFL and IL-33, to maintain macrophage RON expression and support M2 activation. Taken together, our work implicates that RON signaling directs multiple mechanisms involving cellular and secreted mediators to drive immunosuppression in prostate cancer, leading to resistance to immunotherapy. Thus, we provide strong rationale for the RON receptor as a promising immunotherapeutic target to overcome the shortcomings of current strategies and provide superior clinical outcomes in patients.

Published

2020

18. Metabolic Profiling Reveals Aggravated Non-Alcoholic Steatohepatitis in High-Fat High-Cholesterol Diet-Fed Apolipoprotein E-Deficient Mice Lacking Ron Receptor Signaling.

Author

Allen, Joselyn N., Dey, Adwitia, Cai, Jingwei, Zhang, Jingtao, Tian, Yuan, Kennett, Mary, Ma, Yanling, Liang, T. Jake, Patterson, Andrew D., and Hankey-Giblin, Pamela A.

Subjects

FATTY liver, INFLAMMATION, HIGH cholesterol diet, LIPID metabolism, HEPATOCYTE growth factor, BIOTRANSFORMATION (Metabolism), APOLIPOPROTEIN E

Abstract

Non-alcoholic steatohepatitis (NASH) represents the progressive sub-disease of non-alcoholic fatty liver disease that causes chronic liver injury initiated and sustained by steatosis and necroinflammation. The Ron receptor is a tyrosine kinase of the Met proto-oncogene family that potentially has a beneficial role in adipose and liver-specific inflammatory responses, as well as glucose and lipid metabolism. Since its discovery two decades ago, the Ron receptor has been extensively investigated for its differential roles on inflammation and cancer. Previously, we showed that Ron expression on tissue-resident macrophages limits inflammatory macrophage activation and promotes a repair phenotype, which can retard the progression of NASH in a diet-induced mouse model. However, the metabolic consequences of Ron activation have not previously been investigated. Here, we explored the effects of Ron receptor activation on major metabolic pathways that underlie the development and progression of NASH. Mice lacking apolipoprotein E (ApoE KO) and double knockout (DKO) mice that lack ApoE and Ron were maintained on a high-fat high-cholesterol diet for 18 weeks. We observed that, in DKO mice, the loss of ligand-dependent Ron signaling aggravated key pathological features in steatohepatitis, including steatosis, inflammation, oxidation stress, and hepatocyte damage. Transcriptional programs positively regulating fatty acid (FA) synthesis and uptake were upregulated in the absence of Ron receptor signaling, whereas lipid disposal pathways were downregulated. Consistent with the deregulation of lipid metabolism pathways, the DKO animals exhibited increased accumulation of FAs in the liver and decreased level of bile acids. Altogether, ligand-dependent Ron receptor activation provides protection from the deregulation of major metabolic pathways that initiate and aggravate non-alcoholic steatohepatitis. [ABSTRACT FROM AUTHOR]

Published

2020

19. RON and MET Co-overexpression Are Significant Pathological Characteristics of Poor Survival and Therapeutic Targets of Tyrosine Kinase Inhibitors in Triple-Negative Breast Cancer.

Author

Weng TH, Yao MY, Xu XM, Hu CY, Yao SH, Liu YZ, Wu ZG, Tang TM, Fu PF, Wang MH, and Yao HP

Subjects

Adult, Aged, Aged, 80 and over, Animals, Apoptosis, Biomarkers, Tumor genetics, Cell Movement, Cell Proliferation, Female, Follow-Up Studies, Gene Expression Regulation, Neoplastic, Humans, Mice, Mice, Nude, Middle Aged, Prognosis, Proto-Oncogene Mas, Proto-Oncogene Proteins c-met genetics, Receptor Protein-Tyrosine Kinases genetics, Survival Rate, Triple Negative Breast Neoplasms drug therapy, Triple Negative Breast Neoplasms metabolism, Triple Negative Breast Neoplasms pathology, Tumor Cells, Cultured, Xenograft Model Antitumor Assays, Biomarkers, Tumor metabolism, Protein Kinase Inhibitors pharmacology, Proto-Oncogene Proteins c-met metabolism, Receptor Protein-Tyrosine Kinases metabolism, Triple Negative Breast Neoplasms mortality

Abstract

Purpose: Triple-negative breast cancer (TNBC) is highly malignant and has poor prognosis and a high mortality rate. The lack of effective therapy has spurred our investigation of new targets for treating this malignant cancer. Here, we identified RON (macrophage-stimulating 1 receptor) and MET (MET proto-oncogene, receptor tyrosine kinase) as a prognostic biomarker and therapeutic targets for potential TNBC treatment., Materials and Methods: We analyzed RON and MET expression in 187 primary TNBC clinical samples with immunohistochemistry. We validated the targeted therapeutic effects of RON and MET in TNBC using three tyrosine kinase inhibitors (TKIs): BMS-777607, INCB28060, and tivantinib. The preclinical therapeutic efficacy of the TKIs was mainly estimated using a TNBC xenograft model., Results: Patients with TNBC had widespread, abnormal expression of RON and MET. There was RON overexpression, MET overexpression, and RON and MET co-overexpression in 63 (33.7%), 63 (33.7%), and 43 cases (23.0%), respectively, which had poor prognosis and short survival. In vivo, the TKI targeting RON ant MET inhibited the activation of the downstream signaling molecules, inhibited TNBC cell migration and proliferation, and increased TNBC cell apoptosis; in the xenograft model, they significantly inhibited tumor growth and shrank tumor volumes. The TKI targeting RON and Met, such as BMS-777607 and tivantinib, yielded stronger anti-tumor effects than INCB28060., Conclusion: RON and MET co-overexpression can be significant pathological characteristics in TNBC for poor prognosis. TKIs targeting RON and MET have stronger drug development potential for treating TNBC.

Published

2020

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

Author

Ekiz, Huseyin Atakan, Lai, Shu-Chin Alicia, Gundlapalli, Harika, Haroun, Fadi, Welm, Alana L., and Williams, Matthew A.

Subjects

*IMMUNOTHERAPY, *BREAST cancer

Abstract

The advent of immune checkpoint blockade as a new strategy for immunotherapy has changed the outlook for many aggressive cancers. Although complete tumor eradication is attainable in some cases, durable clinical responses are observed only in a small fraction of patients, underlining urgent need for improvement. We previously showed that RON, a receptor tyrosine kinase expressed in macrophages, suppresses antitumor immune responses, and facilitates progression and metastasis of breast cancer. Here, we investigated the molecular changes that occur downstream of RON activation in macrophages, and whether inhibition of RON can cooperate with checkpoint immunotherapy to eradicate tumors. Activation of RON by its ligand, MSP, altered the gene expression profile of macrophages drastically and upregulated surface levels of CD80 and PD-L1, ligands for T-cell checkpoint receptors CTLA-4 and PD-1. Genetic deletion or pharmacological inhibition of RON in combination with anti-CTLA-4, but not with anti-PD-1, resulted in improved clinical responses against orthotopically transplanted tumors compared to single-agent treatment groups, resulting in complete tumor eradication in 46% of the animals. Positive responses to therapy were associated with higher levels of T-cell activation markers and tumor-infiltrating lymphocytes. Importantly, co-inhibition of RON and anti-CTLA-4 was also effective in clearing metastatic breast cancer cells in lungs, resulting in clinical responses in nearly 60% of the mice. These findings suggest that RON inhibition can be a novel approach to potentiate responses to checkpoint immunotherapy in breast cancer. [ABSTRACT FROM AUTHOR]

Published

2018

21. Pathological role of the RON receptor tyrosine kinase in colorectal cancer: Characterization of a short-form RON variant

Author

Spidel, Celee M., Weidanz, Jon, Srivenugopal, Kalkunte, Gunaje, Jayarama, Abbruscato, Thomas J., and Wang, Ming-Hai

Subjects

RON receptor tyrosine kinase, Colorectal cancer

Abstract

RON is a member of the MET family of receptor tyrosine kinases. When activated by its ligand, macrophage stimulating protein (MSP), RON initiates downstream signaling events that result in cell dissociation, migration, and invasion. Several RON variants that arise through mRNA splicing or by an alternate translational start site have been identified, some with oncogenic potential. The purpose of the present study was to characterize and determine any pathogenic roles of a naturally occurring 52 kD N-terminal truncated RON (sf-RON). Sf-RON was found to be overexpressed in 37% of 35 primary and 30% of 10 metastatic colorectal carcinomas (CRCs). Sf-RON was also expressed and constitutively phosphorylated in three CRC cell lines. Cloning sf-RON from a CRC cell line and transfecting it into AA/C1 colon epithelial cells resulted in constitutive activation with increased Map kinase p44/42 (ERK1/2) phosphorylation. Sf-RON expression also caused a decrease in E-cadherin, an important cell adhesion molecule whose downregulation is associated with poor survival in cancer. These changes in cell signaling were accompanied by a change in cell-shape and increased cellular growth and migration. Taken together, sf-RON may play a role in the progression of CRC to a more malignant phenotype.

Published

2006

22. HGFL-mediated RON signaling supports breast cancer stem cell phenotypes via activation of non-canonical β-catenin signaling.

Author

Ruiz-Torres SJ, Benight NM, Karns RA, Lower EE, Guan JL, and Waltz SE

Abstract

Breast cancer stem cells (BCSCs), which drive tumor progression, recurrence, and metastasis, are considered a major challenge for breast cancer treatments, thus the discovery of novel pathways regulating BCSC maintenance remains essential to develop new strategies to effectively target this population and combat disease mortality. The HGFL-RON signaling is overexpressed in human breast cancers and is associated with increased breast cancer progression, metastasis, and poor prognosis. Here, we report that overexpression of RON/MST1R and HGFL/MST1 in cell lines and primary tumors increases BCSC self-renewal, numbers, and tumorigenic potential after syngeneic transplantation. Transcriptome analyses also reveal that the HGFL-RON signaling pathway regulates additional BCSC functions and supports an immunosuppressive microenvironment to stimulate tumor formation and progression. Moreover, we show that genetic and chemical downregulation of HGFL-RON signaling disrupts BCSC phenotypes and tumor growth by suppressing the RON-mediated phosphorylation/activation of β-CATENIN/CTNNB1 and its effector NF-κB/RELA. These studies indicate that HGFL-RON signaling regulates BCSC phenotypes and the tumor microenvironment to drive tumorigenesis and present HGFL/RON as novel therapeutic targets to effectively eradicate BCSCs in patients., Competing Interests: CONFLICTS OF INTEREST The authors declare no conflicts of interest.

Published

2017

23. RON inhibits HIV-1 transcription in monocytes/macrophages.

Abstract

Investigates the repression of HIV-1 transcription in monocytes/macrophages by RON receptor tyrosine kinase. Contribution of the activation of macrophages and microglia cells after HIV-1 infection and their production of inflammatory mediators to HIV-associated central nervous system diseases; Initiation of signaling pathways that negatively regulate HIV-1 transcription in monocytes; Decline of the protein levels in the brain to assure efficient replication.

Published

2005

24. Structural basis for the binding specificity of human Recepteur d'Origine Nantais (RON) receptor tyrosine kinase to macrophage-stimulating protein.

Author

Chao KL, Gorlatova NV, Eisenstein E, and Herzberg O

Subjects

Amino Acid Sequence, Crystallography, X-Ray, Humans, Ligands, Models, Molecular, Molecular Sequence Data, Protein Binding, Protein Structure, Tertiary, Proto-Oncogene Proteins c-met metabolism, Sequence Alignment, Solutions, Structure-Activity Relationship, Ultracentrifugation, Hepatocyte Growth Factor chemistry, Hepatocyte Growth Factor metabolism, Proto-Oncogene Proteins chemistry, Proto-Oncogene Proteins metabolism, Receptor Protein-Tyrosine Kinases chemistry, Receptor Protein-Tyrosine Kinases metabolism

Abstract

Recepteur d'origine nantais (RON) receptor tyrosine kinase and its ligand, serum macrophage-stimulating protein (MSP), play important roles in inflammation, cell growth, migration, and epithelial to mesenchymal transition during tumor development. The binding of mature MSPαβ (disulfide-linked α- and β-chains) to RON ectodomain modulates receptor dimerization, followed by autophosphorylation of tyrosines in the cytoplasmic receptor kinase domains. Receptor recognition is mediated by binding of MSP β-chain (MSPβ) to the RON Sema. Here we report the structure of RON Sema-PSI-IPT1 (SPI1) domains in complex with MSPβ at 3.0 Å resolution. The MSPβ serine protease-like β-barrel uses the degenerate serine protease active site to recognize blades 2, 3, and 4 of the β-propeller fold of RON Sema. Despite the sequence homology between RON and MET receptor tyrosine kinase and between MSP and hepatocyte growth factor, it is well established that there is no cross-reactivity between the two receptor-ligand systems. Comparison of the structure of RON SPI1 in complex with MSPβ and that of MET receptor tyrosine kinase Sema-PSI in complex with hepatocyte growth factor β-chain reveals the receptor-ligand selectivity determinants. Analytical ultracentrifugation studies of the SPI1-MSPβ interaction confirm the formation of a 1:1 complex. SPI1 and MSPαβ also associate primarily as a 1:1 complex with a binding affinity similar to that of SPI1-MSPβ. In addition, the SPI1-MSPαβ ultracentrifuge studies reveal a low abundance 2:2 complex with ∼ 10-fold lower binding affinity compared with the 1:1 species. These results support the hypothesis that the α-chain of MSPαβ mediates RON dimerization., (© 2014 by The American Society for Biochemistry and Molecular Biology, Inc.)

Published

2014