Your search keyword '"LGALS3BP"' showing total 97 results

1. Screening differentially expressed proteins to distinguish thymoma (B1 and B3) from thymic cysts based on tandem mass tag (TMT) technology.

Author

Shi, Jingwei, Yang, Rusong, Chen, Xin, Wang, Yan, Shi, Ye, Wang, Yongsheng, and Liu, Zhengcheng

Subjects

*CARRIER proteins, *GENE ontology, *PROTEOMICS, *ENCYCLOPEDIAS & dictionaries, *BIOMARKERS, *THYMOMA

Abstract

The therapeutic approach to thymic cysts remains a subject of controversy. Predicted biomarkers for identifying thymic cysts and thymoma (THYM) are crucial. In this research, patients diagnosed with thymic cysts (MTC, n = 6) and thymoma (B1, n = 6; B3, n = 6) were enrolled. Proteins of superior quality were subjected to TMT labeling and UPLC-MS, and differentially expressed proteins (DEPs) were identified. Gene Ontology (GO), Kyoto Encyclopedia of Genes and Genomes (KEGG), and protein-protein interactive network analyses were applied to the DEPs. Some key differentially expressed genes(DEGs) were corroborated through GEPIA 32. The pan-cancer expression levels of key DEGs remarkably linked with prognosis were determined utilizing The University of ALabama at Birmingham CANcer data analysis Portal (UALCAN). Eventually, 49 DEPs were identified in the B1 vs. MTC comparison (17 upregulated and 32 downregulated), 27 in the B3 vs. MTC comparison (8 upregulated and 19 downregulated), and 38 in the B3 vs. B1 comparison (9 upregulated and 29 downregulated). IL13RA1 (down), galectin-3 binding protein (LGALS3BP)(up), PRCSH (down), C3 (down), MXRA5 (down), TNN (down), CFHR1 (down), SUN3 (down) were jointly altered in both B1 vs. NZ and B3 vs. NZ. GEPIA validated that LGALS3BP was significantly upregulated in thymoma patients. In conclusion, LGALS3BP might be an essential biomarker to identify thymoma from the thymic cyst. [ABSTRACT FROM AUTHOR]

Published

2024

2. Screening differentially expressed proteins to distinguish thymoma (B1 and B3) from thymic cysts based on tandem mass tag (TMT) technology

Author

Jingwei Shi, Rusong Yang, Xin Chen, Yan Wang, Ye Shi, Yongsheng Wang, and Zhengcheng Liu

Subjects

Thymic cyst, Thymoma, Proteomics, LGALS3BP, Surgery, RD1-811, Anesthesiology, RD78.3-87.3

Abstract

Abstract The therapeutic approach to thymic cysts remains a subject of controversy. Predicted biomarkers for identifying thymic cysts and thymoma (THYM) are crucial. In this research, patients diagnosed with thymic cysts (MTC, n = 6) and thymoma (B1, n = 6; B3, n = 6) were enrolled. Proteins of superior quality were subjected to TMT labeling and UPLC-MS, and differentially expressed proteins (DEPs) were identified. Gene Ontology (GO), Kyoto Encyclopedia of Genes and Genomes (KEGG), and protein-protein interactive network analyses were applied to the DEPs. Some key differentially expressed genes(DEGs) were corroborated through GEPIA 32. The pan-cancer expression levels of key DEGs remarkably linked with prognosis were determined utilizing The University of ALabama at Birmingham CANcer data analysis Portal (UALCAN). Eventually, 49 DEPs were identified in the B1 vs. MTC comparison (17 upregulated and 32 downregulated), 27 in the B3 vs. MTC comparison (8 upregulated and 19 downregulated), and 38 in the B3 vs. B1 comparison (9 upregulated and 29 downregulated). IL13RA1 (down), galectin-3 binding protein (LGALS3BP)(up), PRCSH (down), C3 (down), MXRA5 (down), TNN (down), CFHR1 (down), SUN3 (down) were jointly altered in both B1 vs. NZ and B3 vs. NZ. GEPIA validated that LGALS3BP was significantly upregulated in thymoma patients. In conclusion, LGALS3BP might be an essential biomarker to identify thymoma from the thymic cyst.

Published

2024

3. West Nile Virus-Induced Expression of Senescent Gene Lgals3bp Regulates Microglial Phenotype within Cerebral Cortex.

Author

Arutyunov, Artem, Durán-Laforet, Violeta, Ai, Shenjian, Ferrari, Loris, Murphy, Robert, Schafer, Dorothy P., and Klein, Robyn S.

Subjects

*WEST Nile fever, *WEST Nile virus, *CELL populations, *COGNITIVE aging, *GENE expression

Abstract

Microglia, the resident macrophages of the central nervous system, exhibit altered gene expression in response to various neurological conditions. This study investigates the relationship between West Nile Virus infection and microglial senescence, focusing on the role of LGALS3BP, a protein implicated in both antiviral responses and aging. Using spatial transcriptomics, RNA sequencing and flow cytometry, we characterized changes in microglial gene signatures in adult and aged mice following recovery from WNV encephalitis. Additionally, we analyzed Lgals3bp expression and generated Lgals3bp-deficient mice to assess the impact on neuroinflammation and microglial phenotypes. Our results show that WNV-activated microglia share transcriptional signatures with aged microglia, including upregulation of genes involved in interferon response and inflammation. Lgals3bp was broadly expressed in the CNS and robustly upregulated during WNV infection and aging. Lgals3bp-deficient mice exhibited reduced neuroinflammation, increased homeostatic microglial numbers, and altered T cell populations without differences in virologic control or survival. These data indicate that LGALS3BP has a role in regulating neuroinflammation and microglial activation and suggest that targeting LGALS3BP might provide a potential route for mitigating neuroinflammation-related cognitive decline in aging and post-viral infections. [ABSTRACT FROM AUTHOR]

Published

2024

4. CA9, CYFIP2 and LGALS3BP—A Novel Biomarker Panel to Aid Prognostication in Glioma.

Author

Hudson, Amanda L., Cho, Angela, Colvin, Emily K., Hayes, Sarah A., Wheeler, Helen R., and Howell, Viive M.

Subjects

*PROTEINS, *GLIOMAS, *CANCER relapse, *RESEARCH funding, *TUMOR markers, *TUMOR grading, *MULTIVARIATE analysis, *PROTEOMICS, *STATISTICS, *SURVIVAL analysis (Biometry), *DISEASE progression, *OVERALL survival, *SENSITIVITY & specificity (Statistics)

Abstract

Simple Summary: Glioma is a deadly disease with few treatment options. Early detection of recurrence and progression will help in the clinical management of glioma patients. Biomarkers or molecules that can accurately predict clinical outcomes are becoming extremely important. This study aimed to identify biomarkers of progression and overall survival in glioma. A three-protein panel that could accurately distinguish between long and short survival was identified. Incorporating such biomarkers into clinical practice could significantly aid clinical management. Brain cancer is a devastating and life-changing disease. Biomarkers are becoming increasingly important in addressing clinical issues, including in monitoring tumour progression and assessing survival and treatment response. The goal of this study was to identify prognostic biomarkers associated with glioma progression. Discovery proteomic analysis was performed on a small cohort of astrocytomas that were diagnosed as low-grade and recurred at a higher grade. Six proteins were chosen to be validated further in a larger cohort. Three proteins, CA9, CYFIP2, and LGALS3BP, were found to be associated with glioma progression and, in univariate analysis, could be used as prognostic markers. However, according to the results of multivariate analysis, these did not remain significant. These three proteins were then combined into a three-protein panel. This panel had a specificity and sensitivity of 0.7459 for distinguishing between long and short survival. In silico data confirmed the prognostic significance of this panel. [ABSTRACT FROM AUTHOR]

Published

2024

5. Impaired bisecting GlcNAc reprogrammed M1 polarization of macrophage

Author

Xin He, Bowen Wang, Wenli Deng, Jinhua Cao, Zengqi Tan, Xiang Li, and Feng Guan

Subjects

Bisecting GlcNAc, Glycosylation, Macrophage, Polarization, LGALS3BP, Medicine, Cytology, QH573-671

Abstract

Abstract The functions of macrophages are governed by distinct polarization phenotypes, which can be categorized as either anti-tumor/M1 type or pro-tumor/M2 type. Glycosylation is known to play a crucial role in various cellular processes, but its influence on macrophage polarization is not well-studied. In this study, we observed a significant decrease in bisecting GlcNAc during M0-M1 polarization, and impaired bisecting GlcNAc was found to drive M0-M1 polarization. Using a glycoproteomics strategy, we identified Lgals3bp as a specific glycoprotein carrying bisecting GlcNAc. A high level of bisecting GlcNAc modification facilitated the degradation of Lgals3bp, while a low level of bisecting GlcNAc stabilized Lgals3bp. Elevated levels of Lgals3bp promoted M1 polarization through the activation of the NF-кB pathway. Conversely, the activated NF-кB pathway significantly repressed the transcription of MGAT3, leading to reduced levels of bisecting GlcNAc modification on Lgals3bp. Overall, our study highlights the impact of glycosylation on macrophage polarization and suggests the potential of engineered macrophages via glycosylated modification. Video Abstract

Published

2024

6. Impaired bisecting GlcNAc reprogrammed M1 polarization of macrophage.

Author

He, Xin, Wang, Bowen, Deng, Wenli, Cao, Jinhua, Tan, Zengqi, Li, Xiang, and Guan, Feng

Subjects

*MACROPHAGES, *GLYCOSYLATION, *GLYCOCALYX

Abstract

The functions of macrophages are governed by distinct polarization phenotypes, which can be categorized as either anti-tumor/M1 type or pro-tumor/M2 type. Glycosylation is known to play a crucial role in various cellular processes, but its influence on macrophage polarization is not well-studied. In this study, we observed a significant decrease in bisecting GlcNAc during M0-M1 polarization, and impaired bisecting GlcNAc was found to drive M0-M1 polarization. Using a glycoproteomics strategy, we identified Lgals3bp as a specific glycoprotein carrying bisecting GlcNAc. A high level of bisecting GlcNAc modification facilitated the degradation of Lgals3bp, while a low level of bisecting GlcNAc stabilized Lgals3bp. Elevated levels of Lgals3bp promoted M1 polarization through the activation of the NF-кB pathway. Conversely, the activated NF-кB pathway significantly repressed the transcription of MGAT3, leading to reduced levels of bisecting GlcNAc modification on Lgals3bp. Overall, our study highlights the impact of glycosylation on macrophage polarization and suggests the potential of engineered macrophages via glycosylated modification. 2x6vCQx7YpKy5jGV-ci9bT Video Abstract [ABSTRACT FROM AUTHOR]

Published

2024

7. Extracellular LGALS3BP: a potential disease marker and actionable target for antibody–drug conjugate therapy in glioblastoma

Author

Beatrice Dufrusine, Emily Capone, Sara Ponziani, Rossano Lattanzio, Paola Lanuti, Francesco Giansanti, Vincenzo De Laurenzi, Stefano Iacobelli, Rodolfo Ippoliti, Annunziato Mangiola, Gianluca Trevisi, and Gianluca Sala

Subjects

antibody–drug conjugates, extracellular vesicles, glioblastoma, LGALS3BP, liquid biopsy, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Glioblastoma multiforme (GBM) is a lethal disease characterized by an overall survival of about 1 year, making it one of the most aggressive tumours, with very limited therapeutic possibilities. Specific biomarkers for early diagnosis as well as innovative therapeutic strategies are urgently needed to improve the management of this deadly disease. In this work, we demonstrated that vesicular galectin‐3‐binding protein (LGALS3BP), a glycosylated protein overexpressed in a variety of human malignancies, is a potential GBM disease marker and can be efficiently targeted by a specific antibody–drug conjugate (ADC). Immunohistochemical analysis on patient tissues showed that LGALS3BP is highly expressed in GBM and, compared with healthy donors, the amount of vesicular but not total circulating protein is increased. Moreover, analysis of plasma‐derived extracellular vesicles from mice harbouring human GBM revealed that LGALS3BP can be used for liquid biopsy as a marker of disease. Finally, an ADC targeting LGALS3BP, named 1959‐sss/DM4, specifically accumulates in tumour tissue, producing a potent and dose‐dependent antitumor activity. In conclusion, our work provides evidence that vesicular LGALS3BP is a potential novel GBM diagnostic biomarker and therapeutic target deserving further preclinical and clinical validation.

Published

2023

8. 90K/LGALS3BP expression is upregulated in COVID-19 but may not restrict SARS-CoV-2 infection.

Author

Bosquillon de Jarcy, Laure, Akbil, Bengisu, Mhlekude, Baxolele, Leyens, Johanna, Postmus, Dylan, Harnisch, Greta, Jansen, Jenny, Schmidt, Marie L., Aigner, Annette, Pott, Fabian, Chua, Robert Lorenz, Krist, Lilian, Gentile, Roberta, Mühlemann, Barbara, Jones, Terence C., Niemeyer, Daniela, Fricke, Julia, Keil, Thomas, Pischon, Tobias, and Janke, Jürgen

Subjects

*GENE expression, *SARS-CoV-2, *COVID-19, *BLOOD proteins, *EXTRACELLULAR space

Abstract

Glycoprotein 90K, encoded by the interferon-stimulated gene LGALS3BP, displays broad antiviral activity. It reduces HIV-1 infectivity by interfering with Env maturation and virion incorporation, and increases survival of Influenza A virus-infected mice via antiviral innate immune signaling. Its antiviral potential in SARS-CoV-2 infection remains largely unknown. Here, we analyzed the expression of 90K/LGALS3BP in 44 hospitalized COVID-19 patients at multiple levels. We quantified 90K protein concentrations in serum and PBMCs as well as LGALS3BP mRNA levels. Complementary, we analyzed two single cell RNA-sequencing datasets for expression of LGALS3BP in respiratory specimens and PBMCs from COVID-19 patients. Finally, we analyzed the potential of 90K to interfere with SARS-CoV-2 infection of HEK293T/ACE2, Calu-3 and Caco-2 cells using authentic virus. 90K protein serum concentrations were significantly elevated in COVID-19 patients compared to uninfected sex- and age-matched controls. Furthermore, PBMC-associated concentrations of 90K protein were overall reduced by SARS-CoV-2 infection in vivo, suggesting enhanced secretion into the extracellular space. Mining of published PBMC scRNA-seq datasets uncovered monocyte-specific induction of LGALS3BP mRNA expression in COVID-19 patients. In functional assays, neither 90K overexpression in susceptible cell lines nor exogenous addition of purified 90K consistently inhibited SARS-CoV-2 infection. Our data suggests that 90K/LGALS3BP contributes to the global type I IFN response during SARS-CoV-2 infection in vivo without displaying detectable antiviral properties in vitro. [ABSTRACT FROM AUTHOR]

Published

2023

9. Extracellular LGALS3BP: a potential disease marker and actionable target for antibody–drug conjugate therapy in glioblastoma.

Author

Dufrusine, Beatrice, Capone, Emily, Ponziani, Sara, Lattanzio, Rossano, Lanuti, Paola, Giansanti, Francesco, De Laurenzi, Vincenzo, Iacobelli, Stefano, Ippoliti, Rodolfo, Mangiola, Annunziato, Trevisi, Gianluca, and Sala, Gianluca

Abstract

Glioblastoma multiforme (GBM) is a lethal disease characterized by an overall survival of about 1 year, making it one of the most aggressive tumours, with very limited therapeutic possibilities. Specific biomarkers for early diagnosis as well as innovative therapeutic strategies are urgently needed to improve the management of this deadly disease. In this work, we demonstrated that vesicular galectin‐3‐binding protein (LGALS3BP), a glycosylated protein overexpressed in a variety of human malignancies, is a potential GBM disease marker and can be efficiently targeted by a specific antibody–drug conjugate (ADC). Immunohistochemical analysis on patient tissues showed that LGALS3BP is highly expressed in GBM and, compared with healthy donors, the amount of vesicular but not total circulating protein is increased. Moreover, analysis of plasma‐derived extracellular vesicles from mice harbouring human GBM revealed that LGALS3BP can be used for liquid biopsy as a marker of disease. Finally, an ADC targeting LGALS3BP, named 1959‐sss/DM4, specifically accumulates in tumour tissue, producing a potent and dose‐dependent antitumor activity. In conclusion, our work provides evidence that vesicular LGALS3BP is a potential novel GBM diagnostic biomarker and therapeutic target deserving further preclinical and clinical validation. [ABSTRACT FROM AUTHOR]

Published

2023

10. Circular RNA circARHGEF28 inhibited the progression of prostate cancer via the miR‐671‐5p/LGALS3BP/NF‐κB axis.

Author

Guo, Kaixuan, Shi, Juanyi, Tang, Zhuang, Lai, Cong, Liu, Cheng, Li, Kuiqing, Li, Zhuohang, and Xu, Kewei

Abstract

Circular RNAs (circRNAs) play crucial roles in various biological processes, including prostate cancer (PCa). However, the precise roles and mechanism of circRNAs are complicated. Hence, we studied the function of a circRNA that might be involved in the progression of PCa. In this study, we found that circARHGEF28 was frequently downregulated in PCa tissues and cell lines. Furthermore, gain‐ and loss‐of function experiments in vitro showed that circARHGEF28 inhibited proliferation, migration, and invasion of PCa. Additionally, circARHGEF28 suppressed PCa progression in vivo. Bioinformatics analysis and RNA pull‐down and capture assay found that circARHGEF28 sponged miR‐671‐5p in PCa cells. Importantly, qRT‐PCR and dual luciferase assays found that Lectin galactoside‐binding soluble 3 binding protein (LGALS3BP) was downstream of miR‐671‐5p, and western blot analysis further confirmed that LGALS3BP negatively regulated the nuclear factor kappa‐B (NF‐κB) pathway. These results demonstrated that circARHGEF28 abolished the degradation of LGALS3BP by sponging miR‐671‐5p, thus blocking the activation of the NF‐κB pathway. Our findings revealed that circARHGEF28/miR‐671‐5p/LGALS3BP/NF‐κB may be an important axis that regulates PCa progression. [ABSTRACT FROM AUTHOR]

Published

2023

11. Investigation of conceptus stimulated gene expression in buffalo peripheral blood mononuclear cells as potential diagnostic markers of early pregnancy.

Author

Sharma, Paramjeet, Choudhary, Ratan Kumar, Ratta, Navdeep Singh, and Singh, Sikh Tejinder

Subjects

MONONUCLEAR leukocytes, DECIDUA, GENE expression, ANIMAL herds, PREGNANCY in animals, PREGNANCY, DAIRY cattle

Abstract

Exploration of novel strategies for early pregnancy diagnosis is pivotal in enhancing the reproductive potential and monetary gains from dairy herds. In buffalo, the trophectoderm cells of the elongating conceptus secrete interferon-tau that stimulates the transcription of various genes in peripheral blood mononuclear cells (PBMC) during the peri-implantation period. We explored the differential expression of classical (ISG15) and novel (LGALS3BP and CD9) early pregnancy markers in PBMC of buffaloes during various stages of pregnancy. Natural heat was detected in buffaloes by assessing the vaginal fluid, and artificial insemination (AI) was done. Whole blood was collected from the jugular vein in EDTA-containing vacutainers for PBMC isolation before AI (0-day) and 20, 25 and 40 d post-AI. On day 40, transrectal ultrasonography examination was performed to confirm pregnancy. The inseminated non-pregnant animals served as control. Total RNA was extracted using the TRIzol method. The temporal abundance of ISG15, LGALS3BP and CD9 genes in PBMC was compared between pregnant and non-pregnant groups (n = 9 per group) using real time-qPCR. Results showed transcripts of ISG15 and LGALS3BP were more abundant at 20 d in the pregnant group compared to the 0 d and 20 d values of the non-pregnant group. However, due to variability in expression, threshold (Ct) cycle of RT-qPCR alone could not distinguish pregnant and non-pregnant animals. In conclusion, ISG15 and LGALS3BP transcripts abundance in PBMCs are potential candidate biomarkers for early prediction of buffalo pregnancy 20-days post-AI, but further work is required to allow the development of a reliable new methodology. [ABSTRACT FROM AUTHOR]

Published

2023

12. 90 K increased delivery efficiency of extracellular vesicles through mediating internalization.

Author

Zhu, Guiquan, Yang, Fan, Wei, Hongxuan, Meng, Wanrong, Gan, Jianguo, Wang, Linlin, He, Chuanshi, Lu, Shun, Cao, Bangrong, Luo, Huaichao, Han, Bo, and Li, Ling

Subjects

*MYELOID-derived suppressor cells, *EXTRACELLULAR vesicles, *REGULATORY T cells, *ENDOCYTOSIS, *SUPPRESSOR cells, *INTEGRINS, *HEAD & neck cancer

Abstract

Using mass spectrometry-based high-throughput proteomics, we identified a membrane protein on extracellular vesicles (EVs), 90 K, which predicts poor overall survival of patients with head and neck cancer. 90 K levels in serum EVs could serve as an independent factor for poor prognosis of patients with head and neck cancer. Pre-treatment of immune competent mice with tumor-derived EVs (TDEs) elicited an immune-suppressive microenvironment for tumor cells, which was regulated by 90 K. The immunosuppressive function of TDE-90 K depends on the presence of myeloid derived suppressor cells (MDSCs) rather than regulatory T cells. The immune regulatory role of TDEs on MDSCs depends on miR-21 which is encapsulated in TDEs. Moreover, 90 K is required for the internalization of TDE cargo though interacting with integrin-β1 and anti-siglec-9 rather than directly affecting the immune function of MDSCs. 90 K modification of γδT cell-derived EVs (γδTEVs) could increase the delivery efficiency and therapeutic effect of PD-L1 siRNA by γδTEVs. We concluded that as a secreted protein modulating cell-cell and cell-matrix interactions, 90 K can be carried by TDEs to mediate the internalization and delivery of TDEs cargo by recipient cells. This function of 90 K could be utilized to improve the efficiency of EV-based drug delivery. [Display omitted] • Increased 90 K levels in serum extracellular vesicles predicts poor survival of patients with head and neck cancer. • 90 K-enriched tumor-derived extracellular vesicles inhibited anti-tumor immunity through myeloid derived suppressor cells. • 90 K-mediated delivery of miR-21 by TDEs contributed to immunosuppression of myeloid derived suppressor cells. • Integrin-β1 and Siglec-9 mediate 90 K-induced tumor-derived extracellular vesicle internalization. • 90 K modification optimized γδTEV-based delivery of PD-L1 siRNA by γδT cell-derived vesicles. [ABSTRACT FROM AUTHOR]

Published

2023

13. Galectin 3-binding protein (LGALS3BP) depletion attenuates hepatic fibrosis by reducing transforming growth factor-β1 (TGF-β1) availability and inhibits hepatocarcinogenesis.

Author

Kim DH, Sung M, Park MS, Sun EG, Yoon S, Yoo KH, Radhakrishnan K, Jung SY, Bae WK, Cho SH, and Chung IJ

Subjects

Animals, Female, Humans, Male, Mice, Antigens, Neoplasm metabolism, Antigens, Neoplasm genetics, Carcinogenesis genetics, Carcinogenesis metabolism, Carrier Proteins metabolism, Carrier Proteins genetics, Mice, Inbred C57BL, Mice, Knockout, Signal Transduction, Transforming Growth Factor beta1 metabolism, Transforming Growth Factor beta1 genetics, Carcinoma, Hepatocellular metabolism, Carcinoma, Hepatocellular genetics, Carcinoma, Hepatocellular pathology, Liver Cirrhosis metabolism, Liver Cirrhosis genetics, Liver Cirrhosis pathology, Liver Neoplasms metabolism, Liver Neoplasms genetics, Liver Neoplasms pathology

Abstract

Background: Increased Galectin 3-binding protein (LGALS3BP) serum levels have been used to assess hepatic fibrosis stages and the severity of hepatocellular carcinoma (HCC). Considering the crucial role of transforming growth factor-β1 (TGF-β1) in the emergence of these diseases, the present study tested the hypothesis that LGALS3BP regulates the TGF-β1 signaling pathway., Methods: The expression levels of LGALS3BP and TGFB1 were analyzed in patients with metabolic dysfunction-associated steatohepatitis (MASH) and HCC. Multiple omics techniques, such as RNA-sequencing, transposase-accessible chromatin-sequencing assay, and liquid chromatography-tandem mass spectrometry proteomics, were used to identify the regulatory mechanisms for the LGALS3BP-TGF-β1 axis. The effects of altered TGF-β1 signaling by LGALS3BP were investigated in conditional LGALS3BP-knockin and LGALS3BP-knockout mice., Results: In patients with MASH and HCC, the levels of LGALS3BP and TGFB1 exhibited positive correlations. Stimulation of LGALS3BP by the inflammatory cytokine interferon α in HCC cells or ectopic overexpression of LGALS3BP in hepatocytes promoted the expression levels of TGFB1. Aggravated fibrosis was observed in the livers of hepatocyte-specific LGALS3BP-knockin mice, with increased TGFB1 levels. LGALS3BP directly bound to and assembled integrin αV, an integral mediator required for releasing active TGF-β1 from extracellular latent complex with the rearranged F-actin cytoskeleton. The released TGF-β1 activated JunB transcription factor, which in turn promoted the TGF-β1 positive feedback loop. LGALS3BP deletion in the hepatocytes downregulated TGF-β1 signaling and CCl 4 induced fibrosis. Moreover, LGALS3BP depletion hindered hepatocarcinogenesis by limiting the availability of fibrogenic TGF-β1., Conclusion: LGALS3BP plays a crucial role in hepatic fibrosis and carcinogenesis by controlling the TGF-β1 signaling pathway, making it a promising therapeutic target in TGF-β1-related diseases., (© 2024 The Author(s). Cancer Communications published by John Wiley & Sons Australia, Ltd on behalf of Sun Yat‐sen University Cancer Center.)

Published

2024

14. LGALS3BP: A Potential Plasma Biomarker Associated with Diagnosis and Prognosis in Patients with Sepsis

Author

Luo M, Zhang Q, Hu Y, Sun C, Sheng Y, and Deng C

Subjects

lgals3bp, sepsis, plasma biomarker, dia, elisa, Infectious and parasitic diseases, RC109-216

Abstract

Meiyan Luo,1– 3 Qian Zhang,1– 3 Yingchun Hu,4 Changfeng Sun,1– 3 Yunjian Sheng,1– 3 Cunliang Deng1– 3 1Department of Infectious Diseases, The Affiliated Hospital of Southwest Medical University, Louzhou, 646000, People’s Republic of China; 2Department of Tuberculosis, The Affiliated Hospital of Southwest Medical University, Louzhou, 646000, People’s Republic of China; 3Infection and Immunity Laboratory,The Affiliated Hospital of Southwest Medical University, Louzhou, 646000, People’s Republic of China; 4Department of Emergency, The Affiliated Hospital of Southwest Medical University, Louzhou, 646000, People’s Republic of ChinaCorrespondence: Cunliang DengDepartment of Infectious Diseases, The Affiliated Hospital of Southwest Medical University, No. 25 Taiping Street, Louzhou, 646000, People’s Republic of ChinaEmail dengcunl64@vip.sina.comPurpose: This study aimed to screen differentially expressed proteins (DEPs) in plasma of patients with sepsis through data-independent acquisition (DIA) and enzyme-linked immunosorbent assays (ELISAs), and provide convenient and accurate serum markers for determining the condition of septic patients.Methods: A total of 53 septic patients and 16 normal controls who were admitted to the Affiliated Hospital of Southwest Medical University between January 2019 and December 2020 were enrolled in this study; 6 specimens from the normal group and 15 from the sepsis group were randomly selected for DIA-based quantitative proteomic analysis. The acquired data were subjected to Gene Ontology (GO) and Kyoto Encyclopedia of Genes and Genomes (KEGG) analysis, and a protein-protein interaction (PPI) network was constructed to screen potential markers. The selected proteins were further verified through ELISAs. The differences between control and sepsis groups and between survivors and non-survivors were analysed. Receiver operating characteristic (ROC) curves were drawn to explore their diagnostic value and prognostic efficacy.Results: A total of 149 DEPs were identified by bioinformatics methods. The analyses showed that these proteins are mainly involved in biological processes such as cell movement, stress response, cell proliferation, and immune response. Functional pathway analysis showed that they are mainly involved in leukocyte transendothelial migration, protein synthesis and processing, and various bacterial infections. LGALS3BP was selected as a potential plasma biomarker and further verified through an ELISA. Its level in septic patients was significantly higher than that in normal controls, and its level in non-survivors was also higher than that in survivors. The ROC curves suggested its great diagnostic efficacy and prognostic ability in sepsis.Conclusion: LGALS3BP levels were significantly different between the normal and sepsis groups; it has good diagnostic value in sepsis, and is related to patient prognosis; thus, it might be a biomarker for sepsis.Keywords: LGALS3BP, sepsis, plasma biomarker, DIA, ELISA

Published

2021

15. Aberrant expression of LGALS3BP drives an unfavorable prognosis and more aggressive in HCC via regulating PI3K/AKT signaling.

Author

Liu, Yang, Liang, Lei, Li, Jian, Pang, Tao, Zhang, Shu Hong, and Xia, Zhang Yong

Subjects

PI3K/AKT pathway, PROGNOSIS, PHOSPHATIDYLINOSITOL 3-kinases, HEPATOCELLULAR carcinoma, CELL growth

Abstract

Lectin galactoside-binding soluble 3-binding protein (LGALS3BP) is associated with cancer metastasis and is a promising prognostic marker in neoplasms. In hepatocellular carcinoma (HCC), the prognostic impact and pro-metastatic function of LGALS3BP remain unclear. This study evaluated the endogenous LGALS3BP expression in HCC tissue and its association with prognosis. LGALS3BP protein levels were significantly elevated in clinical HCC tissues and cell lines. Increased LGALS3BP expression was closely associated with disease progression in HCC patients, and they also exhibited an unfavorable prognosis. Furthermore, the knockdown of LGALS3BP inhibited the growth, migration, and invasion of HCC cells in vitro. In mice xenografts, silencing LGALS3BP significantly inhibited tumor cell growth in vivo. Mechanically, upon LGALS3BP depletion, the tumor-suppressive function was dependent on inactivating Phosphatidylinositol 3-kinase (PI3K)/V-akt murine thymoma viral oncogene homolog (AKT) signaling pathway. Collectively, these findings suggest that LGALS3BP employs a pro-tumorigenic function in HCC and may be a promising HCC prognostic marker. • LGALS3BP is dramatically elevated in clinical hepatocellular carcinoma (HCC) tissues as well as cell lines. • Higher LGALS3BP expression causes to an unfavorable prognosis. • Knockdown of LGALS3BP suppresses HCC cell growth in vitro and in vitro. • LGALS3BP exerts a pro-tumorigenic function in HCC via regulating PI3K/AKT signaling. [ABSTRACT FROM AUTHOR]

Published

2024

16. Osteosarcoma exocytosis of soluble LGALS3BP mediates macrophages toward a tumoricidal phenotype.

Author

Li, Jing, Zhao, Chenguang, Li, Yuhuan, Wen, Junxiang, Wang, Shuang, Wang, Difan, Dong, Hui, Wang, Dong, Zhao, Yonglin, Wang, Xiaohui, He, Xijing, and Qin, Jie

Subjects

*MACROPHAGES, *OSTEOSARCOMA, *EXOCYTOSIS, *TUMOR microenvironment, *PHENOTYPES, *RESEARCH, *ANIMAL experimentation, *RESEARCH methodology, *CELL physiology, *APOPTOSIS, *MEDICAL cooperation, *EVALUATION research, *COMPARATIVE studies, *CELL lines, *MICE

Abstract

This study aimed to elucidate the interactions between osteosarcoma (OS) and M1 macrophages infiltrated into the tumor microenvironment and to explore the underlying mechanisms whereby M1 macrophages influence the growth of OS, so that novel treatments of OS can be developed. A transwell co-culture system, an indirect conditioned medium culture system and two orthotopic bearing OS models were established to assess for the interplay between M1 macrophages and OS. We found that the co-culture of M1 macrophages with OS cells significantly inhibited the growth of the tumor cells by inducing apoptosis. Furthermore, HSPA1L secreted by M1 macrophages exerted this anti-tumor effect through the IRAK1 and IRAK4 pathways. LGALS3BP secreted by OS cells bound to the ligand LGALS3 on M1 macrophages and thereby induced the secretion of Hspa11 via Akt phosphorylation. In vivo experiments demonstrated that the culture supernatant of OS-stimulated M1 macrophages significantly inhibited the growth of OS, whereas silencing Lgals3bp promoted the progression of OS. In conclusion, OS modifies the phenotype of tumor-associated macrophages (TAMs) and thereby influences the apoptosis of OS cells through soluble factors. The modulation of TAMs may be a promising and effective therapeutic approach in OS. [ABSTRACT FROM AUTHOR]

Published

2022

17. MZT2A promotes NSCLC viability and invasion by increasing Akt phosphorylation via the MOZART2 domain.

Author

Wang, Huanxi, Jiang, Xizi, Cheng, Yu, Ren, Hongjiu, Hu, Yujiao, Zhang, Yao, Su, Hongbo, Zou, Zifang, Wang, Qiongzi, Liu, Zongang, Zhang, Jiameng, and Qiu, Xueshan

Abstract

Mitotic spindle organizing protein 2A (MZT2A) is localized at the centrosome and regulates microtubule nucleation activity in cells. This study assessed the role of MZT2A in non–small‐cell lung cancer (NSCLC). Differential MZT2A expression was bioinformatically assessed using TCGA database, the GEPIA database, and Kaplan‐Meier survival data to determine the association between MZT2A expression and NSCLC prognosis. Furthermore, NSCLC tissue specimens were evaluated by immunohistochemistry. MZT2A was overexpressed or knocked down in NSCLC cells using cDNA and siRNA, respectively. The cells were subjected to various assays and treated with the selective Akt inhibitor LY294002 or co‐transfected with galectin‐3‐binding protein (LGALS3BP) siRNA. MZT2A mRNA and protein levels were upregulated in NSCLC lesions and MTZ2A expression was associated with poor NSCLC prognosis. MZT2A protein was also highly expressed in NSCLC cells compared with the expression in normal bronchial cells. MZT2A expression promoted NSCLC cell viability and invasion, whereas MTZ2A siRNA had the opposite effect on NSCLC cells in vitro. At the protein level, MZT2A induced Akt phosphorylation, promoting NSCLC proliferation and invasion (but the selective Akt inhibitor blocked these effects) through upregulation of LGALS3BP via the MTZ2A MOZART2 domain, whereas LGALS3BP siRNA suppressed MTZ2A activity in NSCLC cells. The limited in vivo experiments confirmed the in vitro data. In conclusion, MZT2A exhibits oncogenic activity by activating LGALS3BP and Akt in NSCLC. Future studies will assess MTZ2A as a biomarker to predict NSCLC prognosis or as a target in the control of NSCLC progression. [ABSTRACT FROM AUTHOR]

Published

2021

18. Increased LGALS3 expression independently predicts shorter overall survival in patients with the proneural subtype of glioblastoma

Author

Xia He, Sunfu Zhang, Junchen Chen, and Dekang Li

Subjects

glioblastoma, LGALS3, LGALS3BP, proneural subtype, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract In the current study, we tried to study the expression of LGALS3 and LGALS3BP, their potential as prognostic markers and the possible genetic/epigenetic mechanisms underlying their dysregulation in different subtypes of glioblastoma (GBM). An in silico retrospective study was performed using large online databases. Results showed that LGALS3 and LGALS3BP were upregulated at both RNA and protein levels in GBM tissue and were generally associated with shorter overall survival (OS) in GBM patients. However, in subgroup analysis, we only found the association in proneural subtype. The copy number alterations did not necessarily lead to LGALS3/LGALS3BP dysregulation. In the proneural subtype of GBM patients, hypermethylation of the two CpG sites (cg19099850 and cg17403875) was associated with significantly lower expression of LGALS3. In univariate and multivariate analysis, LGALS3 expression independently predicted shorter OS in the proneural subtype of GBM (HR: 1.487, 95% CI: 1.229‐1.798, P

Published

2019

19. Anti-LGALS3BP antibody-drug conjugate treatment induces durable and potent antitumor response in a preclinical model of adenoid cystic carcinoma.

Author

Capone, Emily, Perrotti, Vittoria, Cela, Ilaria, Lattanzio, Rossano, Togni, Lucrezia, Rubini, Corrado, Caponio, Vito Carlo Alberto, Lo Muzio, Lorenzo, Colasante, Martina, Giansanti, Francesco, Ippoliti, Rodolfo, Iacobelli, Stefano, Wick, Michael J., Spardy Burr, Nicole, and Sala, Gianluca

Subjects

*ANTIBODY-drug conjugates, *ADENOID cystic carcinoma, *ANIMAL models in research, *SALIVARY glands, *GENE expression, *IMMUNOHISTOCHEMISTRY

Abstract

• ACC presents high risk for recurrence and refractoriness to anti-cancer treatments. • LGALS3BP is largely expressed in ACC patients. • LGALS3BP is a potential target for ADC therapy in ACC. Adenoid cystic carcinoma (ACC) is a rare type of cancer that typically arises from glandular tissues, most commonly in the salivary glands. Although relatively rare, it represents a serious clinical issue as the management of the disease is highly complex being the only therapeutic options represented by invasive surgery and/or radiotherapy. In the present study, we have explored the potential of galectin-3 binding protein (LGALS3BP) as a novel target for antibody-drug conjugate (ADC) therapy in ACC. RNAseq was conducted on a panel of 10 ACC patient-derived xenografts (PDX)s tissues and 6 normal salivary glands to analyze LGALS3BP gene expression. Protein expression was assessed in ACC PDX and primary tumor tissues using immunohistochemistry. Anti-LGALS3BP ADC named 1959-sss/DM4, was tested in high LGALS3BP expressing ACC PDX model ST1502B. RNAseq analysis revealed that LGALS3BP expression was highly expressed in ACC PDX tissues compared to normal salivary gland tissues. As evaluated by immunohistochemical analysis, LGALS3BP protein was found to be heterogeneously expressed in 10 ACC PDX and in tumor tissues derived from a cohort of 37 ACC patients. Further, treatment with 1959-sss/DM4 ADC led to durable tumor growth inhibition (TGI) in 100% of animals without observed toxicity. Our study provides strong evidence that LGALS3BP is a promising therapeutic target for ACC, warranting further expedited preclinical and clinical investigation. [ABSTRACT FROM AUTHOR]

Published

2024

20. LGALS3BP is a novel and potential biomarker in clear cell renal cell carcinoma.

Author

Li L, Qin S, Tan H, and Zhou J

Subjects

Humans, Fibroblast Growth Factor 2 metabolism, Kidney pathology, Biomarkers, Tumor genetics, Biomarkers, Tumor metabolism, Cell Line, Tumor, Prognosis, Gene Expression Regulation, Neoplastic, Antigens, Neoplasm genetics, Antigens, Neoplasm metabolism, Carcinoma, Renal Cell pathology, Kidney Neoplasms pathology, Carcinoma genetics

Abstract

Clear cell renal cell carcinoma (ccRCC) is the most common solid renal tumor. Therefore, it is necessary to explore the related tumor markers. LGALS3BP (galectin 3 binding protein) is a multifunctional glycoprotein implicated in immunity and cancer. Some studies have shown that LGALS3BP promotes the occurrence and development of tumors. However, their exact role in renal tumorigenesis remains unclear. Our study used a webserver to explore the mRNA expression and clinical features of LGALS3BP in ccRCC. Survival analysis showed that patients with high LGALS3BP expression had significantly worse OS and DFS than those with low LGALS3BP expression. LGALS3BP expression is significantly related to B cells, CD4+ T cells, macrophages, neutrophils, and dendritic cells. Furthermore, we determined that LGALS3BP is significantly associated with angiogenesis, stemness and proliferation in renal cancer. Three phenotypes may be associated with a poor prognosis. Genes related to proliferation, angiogenesis and stemness were derived from a Venn diagram of FGF2. FGF2 is negatively correlated with proliferation and positively correlated with angiogenesis. Finally, we screened for drugs that may have potential therapeutic value for ccRCC. The PCR results showed that the expression of LGALS3BP in the normal cell line was lower than that in the tumor cell lines. After LGALS3BP knockdown, the proliferation of 769-P and 786-O cells decreased. The present findings show that LGALS3BP is critical for ccRCC cell proliferation and may be a potential target and biomarker for ccRCC.

Published

2024

21. Extracellular <scp>LGALS3BP</scp> : a potential disease marker and actionable target for antibody–drug conjugate therapy in glioblastoma

Author

Beatrice Dufrusine, Emily Capone, Sara Ponziani, Rossano Lattanzio, Paola Lanuti, Francesco Giansanti, Vincenzo De Laurenzi, Stefano Iacobelli, Rodolfo Ippoliti, Annunziato Mangiola, Gianluca Trevisi, and Gianluca Sala

Subjects

Cancer Research, liquid biopsy, Oncology, glioblastoma, Genetics, LGALS3BP, antibody-drug conjugates, Molecular Medicine, Antibody-Drug Conjugates, Glioblastoma, extracellular vesicles, General Medicine

Published

2023

22. Increased LGALS3 expression independently predicts shorter overall survival in patients with the proneural subtype of glioblastoma.

Author

He, Xia, Zhang, Sunfu, Chen, Junchen, and Li, Dekang

Subjects

*GENETIC markers, *ONLINE databases, *GENETIC regulation, *GLIOBLASTOMA multiforme, *UNIVARIATE analysis, *MULTIVARIATE analysis

Abstract

In the current study, we tried to study the expression of LGALS3 and LGALS3BP, their potential as prognostic markers and the possible genetic/epigenetic mechanisms underlying their dysregulation in different subtypes of glioblastoma (GBM). An in silico retrospective study was performed using large online databases. Results showed that LGALS3 and LGALS3BP were upregulated at both RNA and protein levels in GBM tissue and were generally associated with shorter overall survival (OS) in GBM patients. However, in subgroup analysis, we only found the association in proneural subtype. The copy number alterations did not necessarily lead to LGALS3/LGALS3BP dysregulation. In the proneural subtype of GBM patients, hypermethylation of the two CpG sites (cg19099850 and cg17403875) was associated with significantly lower expression of LGALS3. In univariate and multivariate analysis, LGALS3 expression independently predicted shorter OS in the proneural subtype of GBM (HR: 1.487, 95% CI: 1.229‐1.798, P < 0.001), after adjustment of age, gender, IDH1 mutations, temozolomide chemotherapy, radiotherapy and LGALS3BP expression. In comparison, LGALS3BP lost the prognostic value in multivariate analysis. Based on these findings, we infer that LGALS3 expression serves as an independent biomarker of shorter OS in the proneural subtype of GBM, the expression of which might be regulated in an epigenetic manner. [ABSTRACT FROM AUTHOR]

Published

2019

23. Size-exclusion chromatography as a stand-alone methodology identifies novel markers in mass spectrometry analyses of plasma-derived vesicles from healthy individuals

Author

Armando de Menezes-Neto, María José Fidalgo Sáez, Inés Lozano-Ramos, Joan Segui-Barber, Lorena Martin-Jaular, Josep M. Estanyol Ullate, Carmen Fernandez-Becerra, Francesc E. Borrás, and Hernando A. del Portillo

Subjects

exosomes, low infrastructure settings, CD5L, LGALS3BP, comparative analysis, plasma-derived exosomes, mass spectrometry, Cytology, QH573-671

Abstract

Plasma-derived vesicles hold a promising potential for use in biomedical applications. Two major challenges, however, hinder their implementation into translational tools: (a) the incomplete characterization of the protein composition of plasma-derived vesicles, in the size range of exosomes, as mass spectrometric analysis of plasma sub-components is recognizably troublesome and (b) the limited reach of vesicle-based studies in settings where the infrastructural demand of ultracentrifugation, the most widely used isolation/purification methodology, is not available. In this study, we have addressed both challenges by carrying-out mass spectrometry (MS) analyses of plasma-derived vesicles, in the size range of exosomes, from healthy donors obtained by 2 alternative methodologies: size-exclusion chromatography (SEC) on sepharose columns and Exo-Spin™. No exosome markers, as opposed to the most abundant plasma proteins, were detected by Exo-Spin™. In contrast, exosomal markers were present in the early fractions of SEC where the most abundant plasma proteins have been largely excluded. Noticeably, after a cross-comparative analysis of all published studies using MS to characterize plasma-derived exosomes from healthy individuals, we also observed a paucity of “classical exosome markers.” Independent of the isolation method, however, we consistently identified 2 proteins, CD5 antigen-like (CD5L) and galectin-3-binding protein (LGALS3BP), whose presence was validated by a bead-exosome FACS assay. Altogether, our results support the use of SEC as a stand-alone methodology to obtain preparations of extracellular vesicles, in the size range of exosomes, from plasma and suggest the use of CD5L and LGALS3BP as more suitable markers of plasma-derived vesicles in MS.

Published

2015

24. Lysosomal proteomics reveals mechanisms of neuronal apoE4associated lysosomal dysfunction.

Author

Krogsaeter EK, McKetney J, Marquez A, Cakir Z, Stevenson E, Jang GM, Rao A, Zhou A, Huang Y, Krogan NJ, and Swaney DL

Abstract

ApoE4 is the primary risk factor for Alzheimer's Disease. While apoE is primarily expressed by astrocytes, AD pathology including endosomal abnormalities and mitochondrial dysfunction first occurs in neurons. Lysosomes are poised at the convergence point between these features. We find that apoE4-expressing cells exhibit lysosomal alkalinization, reduced lysosomal proteolysis, and impaired mitophagy. To identify driving factors for this lysosomal dysfunction, we performed quantitative lysosomal proteome profiling. This revealed that apoE4 expression results in lysosomal depletion of Lgals3bp and accumulation of Tmed5 in both Neuro-2a cells and postmitotic human neurons. Modulating the expression of both proteins affected lysosomal function, with Tmed5 knockdown rescuing lysosomal alkalinization in apoE4 cells, and Lgals3bp knockdown causing lysosomal alkalinization and reduced lysosomal density in apoE3 cells. Taken together, our work reveals that apoE4 exerts gain-of-toxicity by alkalinizing the lysosomal lumen, pinpointing lysosomal Tmed5 accumulation and Lgals3bp depletion as apoE4-associated drivers for this phenotype., Competing Interests: Yadong Huang is a co-founder and scientific advisory board member of GABAeron. The Krogan Laboratory has received research support from Vir Biotechnology, F. Hoffmann-La Roche, and Rezo Therapeutics. Nevan J. Krogan has previously held financially compensated consulting agreements with the Icahn School of Medicine at Mount Sinai, New York, and Twist Bioscience Corp. He currently has financially compensated consulting agreements with Maze Therapeutics, Interline Therapeutics, Rezo Therapeutics, and GEn1E Lifesciences, Inc. He is on the Board of Directors of Rezo Therapeutics and is a shareholder in Tenaya Therapeutics, Maze Therapeutics, Rezo Therapeutics, and Interline Therapeutics. Danielle L. Swaney has financially compensated consulting agreements with Maze Therapeutics and Rezo Therapeutics. The other authors declare no competing interests.

Published

2023

25. Galectin‐3‐binding protein: A multitask glycoprotein with innate immunity functions in viral and bacterial infections.

Author

Loimaranta, Vuokko, Hepojoki, Jussi, Laaksoaho, Olli, and Pulliainen, Arto T.

Subjects

GALECTINS, CARRIER proteins, GLYCOPROTEINS, NEOPLASTIC cell transformation, DOUBLE-stranded RNA

Abstract

Abstract: Galectin‐3‐binding protein (Gal‐3BP) is a ubiquitous and multifunctional secreted glycoprotein originally identified and mainly studied in the context of neoplastic transformation and cancer progression. However, Gal‐3BP expression is induced in viral infection and by a multitude of molecules that either mimic or are characteristic for an ongoing inflammation and microbial infection, such as IFN‐α, IFN‐β, IFN‐γ, TNF‐α, poly(I:C), dsRNA, and dsDNA. Furthermore, Gal‐3BP belongs to the scavenger receptor cysteine‐rich (SRCR) domain‐containing protein family, by virtue of its N‐terminal SRCR domain. The SRCR domain is found in soluble or membrane‐associated innate immunity‐related proteins and is implicated in self‐nonself discrimination. This review summarizes the current knowledge of structural features of Gal‐3BP and its proposed intracellular and extracellular innate immunity functions with special emphasis on viral and bacterial infections. [ABSTRACT FROM AUTHOR]

Published

2018

26. Glycoprotein 90K Promotes E-Cadherin Degradation in a Cell Density-Dependent Manner via Dissociation of E-Cadherin-p120-Catenin Complex.

Author

So-Yeon Park, Somy Yoon, Eun Gene Sun, Rui Zhou, Bae, Jeong A., Young-Woo Seo, Jung-Il Chae, Man-Jeong Paik, Hyung-Ho Ha, Hangun Kim, and Kyung Keun Kim

Subjects

*GLYCOPROTEINS, *CANCER prognosis, *METASTASIS, *ADHERENS junctions, *CADHERINS, *CELL adhesion, *CELL motility, *CANCER patients

Abstract

Glycoprotein 90K (also known as LGALS3BP or Mac-2BP) is a tumor-associated protein, and high 90K levels are associated with poor prognosis in some cancers. To clarify the role of 90K as an indicator for poor prognosis and metastasis in epithelial cancers, the present study investigated the effect of 90K on an adherens junctional protein, E-cadherin, which is frequently absent or downregulated in human epithelial cancers. Treatment of certain cancer cells with 90K significantly reduced E-cadherin levels in a cell-population-dependent manner, and these cells showed decreases in cell adhesion and increases in invasive cell motility. Mechanistically, 90K-induced E-cadherin downregulation occurred via ubiquitination-mediated proteasomal degradation. 90K interacted with the E-cadherin-p120-catenin complex and induced its dissociation, altering the phosphorylation status of p120-catenin, whereas it did not associate with β-catenin. In subconfluent cells, 90K decreased membrane-localized p120-catenin and the membrane fraction of the p120-catenin. Particularly, 90K-induced E-cadherin downregulation was diminished in p120-catenin knocked-down cells. Taken together, 90K upregulation promotes the dissociation of the E-cadherin-p120-catenin complex, leading to E-cadherin proteasomal degradation, and thereby destabilizing adherens junctions in less confluent tumor cells. Our results provide a potential mechanism to explain the poor prognosis of cancer patients with high serum 90K levels. [ABSTRACT FROM AUTHOR]

Published

2017

27. 90K predicts the prognosis of glioma patients and enhances tumor lysate-pulsed DC vaccine for immunotherapy of GBM in vitro

Author

Xin Chen and Yu Zeng

Subjects

Aging, medicine.medical_treatment, Malignancy, Cancer Vaccines, DC vaccine, 90K, Antigens, Neoplasm, Glioma, medicine, Biomarkers, Tumor, Cytotoxic T cell, LGALS3BP, Humans, business.industry, Brain Neoplasms, Cell Biology, Immunotherapy, Dendritic cell, Dendritic Cells, medicine.disease, Prognosis, CTL, Apoptosis, Cancer research, Biomarker (medicine), business, Research Paper

Abstract

Objectives: This study aimed to investigate the relationship between 90K expression with glioma malignancy and prognosis. Additionally, the enhancement effect of 90K in the Dendritic cell (DC) vaccine for Immunotherapy of glioblastoma (GBM) was evaluated in vitro. Methods: The expression of 90K protein in glioma tissues was detected by western blot. The relationship between the 90K expression and the tumor grade as well as the prognosis of patients was further analyzed by mining TCGA and CGGA database. The concentration of IL-12p70 and IL-10 was detected by ELISA. T lymphocyte proliferation and lethal effect of cytotoxic T cell (CTL) were detected by CCK-8. Results: The expression of 90K was significantly higher in glioma than normal tissue and increased with tumor grade (P< 0.05). Higher 90K expression was observed in IDH wildtype glioma than IDH mutant and predicted worse overall survival for glioma patients. The concentration of IL-12p70 and IFN-γ was the highest in the Apoptosis U251-90K-DC group, in which group the ability to kill U251 cells by CTL was also the strongest. Conclusion: 90K was a useful biomarker for glioma malignancy and patient prognosis. The appearance of 90K enhanced the effect of Apoptosis U251-DC vaccine for immunotherapy of GBM.

Published

2021

28. Shoc2-tranduced ERK1/2 motility signals — Novel insights from functional genomics.

Author

Jeoung, Myoungkun, Jang, Eun Ryoung, Liu, Jinpeng, Wang, Chi, Rouchka, Eric C., Li, Xiaohong, and Galperin, Emilia

Subjects

*CELLULAR signal transduction, *EXTRACELLULAR signal-regulated kinases, *FUNCTIONAL genomics, *CELL determination, *SCAFFOLD proteins, *GROWTH factors

Abstract

The extracellular signal-regulated kinase 1 and 2 (ERK1/2) pathway plays a central role in defining various cellular fates. Scaffold proteins modulating ERK1/2 activity control growth factor signals transduced by the pathway. Here, we analyzed signals transduced by Shoc2, a critical positive modulator of ERK1/2 activity. We found that loss of Shoc2 results in impaired cell motility and delays cell attachment. As ERKs control cellular fates by stimulating transcriptional response, we hypothesized that the mechanisms underlying changes in cell adhesion could be revealed by assessing the changes in transcription of Shoc2-depleted cells. Using quantitative RNA-seq analysis, we identified 853 differentially expressed transcripts. Characterization of the differentially expressed genes showed that Shoc2 regulates the pathway at several levels, including expression of genes controlling cell motility, adhesion, crosstalk with the transforming growth factor beta (TGFβ) pathway, and expression of transcription factors. To understand the mechanisms underlying delayed attachment of cells depleted of Shoc2, changes in expression of the protein of extracellular matrix (lectin galactoside-binding soluble 3-binding protein; LGALS3BP) were functionally analyzed. We demonstrated that delayed adhesion of the Shoc2-depleted cells is a result of attenuated expression and secretion of LGALS3BP. Together our results suggest that Shoc2 regulates cell motility by modulating ERK1/2 signals to cell adhesion. [ABSTRACT FROM AUTHOR]

Published

2016

29. LGALS3BP: A Potential Plasma Biomarker Associated with Diagnosis and Prognosis in Patients with Sepsis

Author

Cunliang Deng, Meiyan Luo, Yun-Jian Sheng, Qian Zhang, Yingchun Hu, and Changfeng Sun

Subjects

Pharmacology, Oncology, medicine.medical_specialty, Receiver operating characteristic, business.industry, plasma biomarker, medicine.disease, Normal group, Fight-or-flight response, Sepsis, sepsis, Infectious Diseases, Immune system, Infection and Drug Resistance, Internal medicine, medicine, DIA, Biomarker (medicine), LGALS3BP, Pharmacology (medical), In patient, ELISA, KEGG, business, Original Research

Abstract

Meiyan Luo,1– 3 Qian Zhang,1– 3 Yingchun Hu,4 Changfeng Sun,1– 3 Yunjian Sheng,1– 3 Cunliang Deng1– 3 1Department of Infectious Diseases, The Affiliated Hospital of Southwest Medical University, Louzhou, 646000, People’s Republic of China; 2Department of Tuberculosis, The Affiliated Hospital of Southwest Medical University, Louzhou, 646000, People’s Republic of China; 3Infection and Immunity Laboratory,The Affiliated Hospital of Southwest Medical University, Louzhou, 646000, People’s Republic of China; 4Department of Emergency, The Affiliated Hospital of Southwest Medical University, Louzhou, 646000, People’s Republic of ChinaCorrespondence: Cunliang DengDepartment of Infectious Diseases, The Affiliated Hospital of Southwest Medical University, No. 25 Taiping Street, Louzhou, 646000, People’s Republic of ChinaEmail dengcunl64@vip.sina.comPurpose: This study aimed to screen differentially expressed proteins (DEPs) in plasma of patients with sepsis through data-independent acquisition (DIA) and enzyme-linked immunosorbent assays (ELISAs), and provide convenient and accurate serum markers for determining the condition of septic patients.Methods: A total of 53 septic patients and 16 normal controls who were admitted to the Affiliated Hospital of Southwest Medical University between January 2019 and December 2020 were enrolled in this study; 6 specimens from the normal group and 15 from the sepsis group were randomly selected for DIA-based quantitative proteomic analysis. The acquired data were subjected to Gene Ontology (GO) and Kyoto Encyclopedia of Genes and Genomes (KEGG) analysis, and a protein-protein interaction (PPI) network was constructed to screen potential markers. The selected proteins were further verified through ELISAs. The differences between control and sepsis groups and between survivors and non-survivors were analysed. Receiver operating characteristic (ROC) curves were drawn to explore their diagnostic value and prognostic efficacy.Results: A total of 149 DEPs were identified by bioinformatics methods. The analyses showed that these proteins are mainly involved in biological processes such as cell movement, stress response, cell proliferation, and immune response. Functional pathway analysis showed that they are mainly involved in leukocyte transendothelial migration, protein synthesis and processing, and various bacterial infections. LGALS3BP was selected as a potential plasma biomarker and further verified through an ELISA. Its level in septic patients was significantly higher than that in normal controls, and its level in non-survivors was also higher than that in survivors. The ROC curves suggested its great diagnostic efficacy and prognostic ability in sepsis.Conclusion: LGALS3BP levels were significantly different between the normal and sepsis groups; it has good diagnostic value in sepsis, and is related to patient prognosis; thus, it might be a biomarker for sepsis.Keywords: LGALS3BP, sepsis, plasma biomarker, DIA, ELISA

Published

2021

30. MZT2A promotes NSCLC viability and invasion by increasing Akt phosphorylation via the MOZART2 domain

Author

Hongjiu Ren, Xueshan Qiu, Qiongzi Wang, Jiameng Zhang, Zifang Zou, Xizi Jiang, Zongang Liu, Yu Cheng, Hongbo Su, Yujiao Hu, Yao Zhang, and Huanxi Wang

Subjects

0301 basic medicine, Cancer Research, Lung Neoplasms, Cell Survival, Carcinogenesis, NSCLC, 03 medical and health sciences, chemistry.chemical_compound, Mice, 0302 clinical medicine, Downregulation and upregulation, Protein Domains, In vivo, Antigens, Neoplasm, Carcinoma, Non-Small-Cell Lung, Cell Line, Tumor, medicine, Biomarkers, Tumor, Animals, Humans, LGALS3BP, LY294002, Neoplasm Invasiveness, Phosphorylation, Lung cancer, Protein kinase B, neoplasms, Messenger RNA, Akt, General Medicine, Original Articles, medicine.disease, Prognosis, In vitro, respiratory tract diseases, Gene Expression Regulation, Neoplastic, 030104 developmental biology, Oncology, chemistry, 030220 oncology & carcinogenesis, Cancer research, Immunohistochemistry, MZT2A, Original Article, Microtubule-Associated Proteins, Proto-Oncogene Proteins c-akt, Signal Transduction

Abstract

Mitotic spindle organizing protein 2A (MZT2A) is localized at the centrosome and regulates microtubule nucleation activity in cells. This study assessed the role of MZT2A in non–small‐cell lung cancer (NSCLC). Differential MZT2A expression was bioinformatically assessed using TCGA database, the GEPIA database, and Kaplan‐Meier survival data to determine the association between MZT2A expression and NSCLC prognosis. Furthermore, NSCLC tissue specimens were evaluated by immunohistochemistry. MZT2A was overexpressed or knocked down in NSCLC cells using cDNA and siRNA, respectively. The cells were subjected to various assays and treated with the selective Akt inhibitor LY294002 or co‐transfected with galectin‐3‐binding protein (LGALS3BP) siRNA. MZT2A mRNA and protein levels were upregulated in NSCLC lesions and MTZ2A expression was associated with poor NSCLC prognosis. MZT2A protein was also highly expressed in NSCLC cells compared with the expression in normal bronchial cells. MZT2A expression promoted NSCLC cell viability and invasion, whereas MTZ2A siRNA had the opposite effect on NSCLC cells in vitro. At the protein level, MZT2A induced Akt phosphorylation, promoting NSCLC proliferation and invasion (but the selective Akt inhibitor blocked these effects) through upregulation of LGALS3BP via the MTZ2A MOZART2 domain, whereas LGALS3BP siRNA suppressed MTZ2A activity in NSCLC cells. The limited in vivo experiments confirmed the in vitro data. In conclusion, MZT2A exhibits oncogenic activity by activating LGALS3BP and Akt in NSCLC. Future studies will assess MTZ2A as a biomarker to predict NSCLC prognosis or as a target in the control of NSCLC progression., MZT2A induced Akt phosphorylation, promoting NSCLC proliferation and invasion through the upregulation of LGALS3BP via the MTZ2A MOZART2 domain. Future studies will assess MTZ2A as a biomarker to predict NSCLC prognosis or as a target to control NSCLC progression

Published

2021

31. Prognostic relevance of LGALS3BP in human colorectal carcinoma.

Author

Piccolo, Enza, Tinari, Nicola, D'Addario, Domenica, Rossi, Cosmo, Iacobelli, Valentina, Sorda, Rossana La, Lattanzio, Rossano, D'Egidio, Maurizia, Di Risio, Annalisa, Piantelli, Mauro, Natali, Pier Giorgio, and Iacobelli, Stefano

Subjects

*ANTINEOPLASTIC agents, *COLON cancer, *UBIQUITINATION, *CANCER invasiveness, *CELL culture

Abstract

Background: A previous report has shown that LGALS3BP (also known as 90K or Mac-2 BP) has antitumor activity in colorectal cancer (CRC) via suppression of Wnt signalling with a novel mechanism of ISGylation-dependent ubiquitination of β-catenin. The role of LGALS3BP in CRC prognosis was investigated. Methods: The role of LGALS3BP on CRC progression and clinical prognosis was analyzed by combining cell cultures, in vitro assays, and immunohistochemistry. Results: Silencing of LGALS3BP in HCT-116 human colon cancer cells resulted in enhanced β-catenin expression that was reversed by addition of human recombinant LGALS3BP. Moreover, intra-tumor delivery of LGALS3BP reduced tumor growth of xenografts originating from LGALS3BP-silenced HCT-116 cells. Finally, in a series of 196 CRC patients, LGALS3BP expression in tumor tissue associated with clinical outcome. Patients with high LGALS3BP expression had lower risk of relapse and a longer overall survival time than those with low LGALS3BP expression. Multivariate analyses confirmed LGALS3BP expression status as the only independent prognostic factor of survival. Conclusions: These results provide evidence that low expression of LGALS3BP participates in malignant progression of CRC and implicates poor prognosis, highlighting its augmentation as a potential therapeutic approach. [ABSTRACT FROM AUTHOR]

Published

2015

32. Size-exclusion chromatography as a stand-alone methodology identifies novel markers in mass spectrometry analyses of plasma-derived vesicles from healthy individuals.

Author

de Menezes-Neto, Armando, Sáez, María José Fidalgo, Lozano-Ramos, Inés, Segui-Barber, Joan, Martin-Jaular, Lorena, Ullate, Josep M. Estanyol, Fernandez-Becerra, Carmen, Borrás, Francesc E., and del Portillo, Hernando A.

Abstract

Plasma-derived vesicles hold a promising potential for use in biomedical applications. Two major challenges, however, hinder their implementation into translational tools: (a) the incomplete characterization of the protein composition of plasma-derived vesicles, in the size range of exosomes, as mass spectrometric analysis of plasma sub-components is recognizably troublesome and (b) the limited reach of vesicle-based studies in settings where the infrastructural demand of ultracentrifugation, the most widely used isolation/purification methodology, is not available. In this study, we have addressed both challenges by carrying-out mass spectrometry (MS) analyses of plasma-derived vesicles, in the size range of exosomes, from healthy donors obtained by 2 alternative methodologies: size-exclusion chromatography (SEC) on sepharose columns and Exo-Spin™. No exosome markers, as opposed to the most abundant plasma proteins, were detected by Exo-Spin™. In contrast, exosomal markers were present in the early fractions of SEC where the most abundant plasma proteins have been largely excluded. Noticeably, after a cross-comparative analysis of all published studies using MS to characterize plasma-derived exosomes from healthy individuals, we also observed a paucity of “classical exosome markers.” Independent of the isolation method, however, we consistently identified 2 proteins, CD5 antigen-like (CD5L) and galectin-3-binding protein (LGALS3BP), whose presence was validated by a bead-exosome FACS assay. Altogether, our results support the use of SEC as a stand-alone methodology to obtain preparations of extracellular vesicles, in the size range of exosomes, from plasma and suggest the use of CD5L and LGALS3BP as more suitable markers of plasma-derived vesicles in MS. [ABSTRACT FROM AUTHOR]

Published

2015

33. Proteins and Molecular Pathways Relevant for the Malignant Properties of Tumor-Initiating Pancreatic Cancer Cells

Author

Lisa Samonig, Andrea Loipetzberger, Constantin Blöchl, Marc Rurik, Oliver Kohlbacher, Fritz Aberger, and Christian G. Huber

Subjects

Proteomics, cancer stem cells, Proteome, Mice, Nude, differential proteome analysis, Article, MRP14, Cell Line, Tumor, Animals, Humans, LGALS3BP, RNA, Messenger, S100A8, lcsh:QH301-705.5, S100A9, MRP8, Principal Component Analysis, functional assays, tumor grafting model, Reproducibility of Results, Xenograft Model Antitumor Assays, Neoplasm Proteins, Gene Expression Regulation, Neoplastic, Pancreatic Neoplasms, lcsh:Biology (General), MAC-2-BP, Neoplastic Stem Cells, TICs, CSCs, S100 proteins, Signal Transduction

Abstract

Cancer stem cells (CSCs), a small subset of the tumor bulk with highly malignant properties, are deemed responsible for tumor initiation, growth, metastasis, and relapse. In order to reveal molecular markers and determinants of their tumor-initiating properties, we enriched rare stem-like pancreatic tumor-initiating cells (TICs) by harnessing their clonogenic growth capacity in three-dimensional multicellular spheroid cultures. We compared pancreatic TICs isolated from three-dimensional tumor spheroid cultures with nontumor-initiating cells (non-TICs) enriched in planar cultures. Employing differential proteomics (PTX), we identified more than 400 proteins with significantly different expression in pancreatic TICs and the non-TIC population. By combining the unbiased PTX with mRNA expression analysis and literature-based predictions of pro-malignant functions, we nominated the two calcium-binding proteins S100A8 (MRP8) and S100A9 (MRP14) as well as galactin-3-binding protein LGALS3BP (MAC-2-BP) as putative determinants of pancreatic TICs. In silico pathway analysis followed by candidate-based RNA interference mediated loss-of-function analysis revealed a critical role of S100A8, S100A9, and LGALS3BP as molecular determinants of TIC proliferation, migration, and in vivo tumor growth. Our study highlights the power of combining unbiased proteomics with focused gene expression and functional analyses for the identification of novel key regulators of TICs, an approach that warrants further application to identify proteins and pathways amenable to drug targeting.

Published

2020

34. Cells / Proteins and Molecular Pathways Relevant for the malignant properties of tumor‐initiating pancreatic cancer cells

Subjects

cancer stem cells, MRP8, functional assays, tumor grafting model, differential proteome analysis, proteomics, MRP14, MAC-2-BP, TICs, CSCs, LGALS3BP, S100A8, S100 proteins, S100A9

Abstract

Cancer stem cells (CSCs), a small subset of the tumor bulk with highly malignant properties, are deemed responsible for tumor initiation, growth, metastasis, and relapse. In order to reveal molecular markers and determinants of their tumor-initiating properties, we enriched rare stem-like pancreatic tumor-initiating cells (TICs) by harnessing their clonogenic growth capacity in three-dimensional multicellular spheroid cultures. We compared pancreatic TICs isolated from three-dimensional tumor spheroid cultures with nontumor-initiating cells (non-TICs) enriched in planar cultures. Employing differential proteomics (PTX), we identified more than 400 proteins with significantly different expression in pancreatic TICs and the non-TIC population. By combining the unbiased PTX with mRNA expression analysis and literature-based predictions of pro-malignant functions, we nominated the two calcium-binding proteins S100A8 (MRP8) and S100A9 (MRP14) as well as galactin-3-binding protein LGALS3BP (MAC-2-BP) as putative determinants of pancreatic TICs. In silico pathway analysis followed by candidate-based RNA interference mediated loss-of-function analysis revealed a critical role of S100A8, S100A9, and LGALS3BP as molecular determinants of TIC proliferation, migration, and in vivo tumor growth. Our study highlights the power of combining unbiased proteomics with focused gene expression and functional analyses for the identification of novel key regulators of TICs, an approach that warrants further application to identify proteins and pathways amenable to drug targeting.

Published

2020

35. Maldevelopment of dermal lymphatics in Wnt5a-knockout-mice.

Author

Buttler, Kerstin, Becker, Jürgen, Pukrop, Tobias, and Wilting, Jörg

Subjects

*LYMPHATICS, *KNOCKOUT mice, *LABORATORY mice, *ENDOTHELIAL cells, *WNT proteins, *ACETYLCHOLINE

Abstract

Abstract: Maintenance of tissue homeostasis and immune surveillance are important functions of the lymphatic vascular system. Lymphatic vessels are lined by lymphatic endothelial cells (LECs). By gene micro-array expression studies we recently compared human lymphangioma-derived LECs with umbilical vein endothelial cells (HUVECs). Here, we followed up on these studies. Besides well-known LEC markers, we observed regulation of molecules involved in immune regulation, acetylcholine degradation and platelet regulation. Moreover we identified differentially expressed WNT pathway components, which play important roles in the morphogenesis of various organs, including the blood vascular system. WNT signaling has not yet been addressed in lymphangiogenesis. We found high expression of FZD3, FZD5 and DKK2 mRNA in HUVECs, and WNT5A in LECs. The latter was verified in normal skin-derived LECs. With immunohistological methods we detected WNT5A in LECs, as well as ROR1, ROR2 and RYK in both LECs and HUVECs. In the human, mutations of WNT5A or its receptor ROR2 cause the Robinow syndrome. These patients show multiple developmental defects including the cardio-vascular system. We studied Wnt5a-knockout (ko) mouse embryos at day 18.5. We show that the number of dermal lymphatic capillaries is significantly lower in Wnt5a-null-mice. However, the mean size of individual lymphatics and the LEC number per vessel are greater. In sum, the total area covered by lymphatics and the total number of LECs are not significantly altered. The reduced number of lymphatic capillaries indicates a sprouting defect rather than a proliferation defect in the dermis of Wnt5a-ko-mice, and identifies Wnt5a as a regulator of lymphangiogenesis. [Copyright &y& Elsevier]

Published

2013

36. LGALS3BP, lectin galactoside-binding soluble 3 binding protein, induces vascular endothelial growth factor in human breast cancer cells and promotes angiogenesis.

Author

Piccolo, Enza, Tinari, Nicola, Semeraro, Daniela, Traini, Sara, Fichera, Imma, Cumashi, Albana, Sorda, Rossana, Spinella, Francesca, Bagnato, Anna, Lattanzio, Rossano, D'Egidio, Maurizia, Risio, Annalisa, Stampolidis, Pavlos, Piantelli, Mauro, Natoli, Clara, Ullrich, Axel, and Iacobelli, Stefano

Subjects

*BREAST cancer diagnosis, *GALACTOSIDES, *CARRIER proteins, *CANCER invasiveness, *BLOOD vessels, *FIBRONECTINS, *LECTINS

Abstract

Elevated serum or tissue levels of lectin galactoside-binding soluble 3 binding protein (LGALS3BP) have been associated with short survival and development of metastasis in a variety of human cancers. However, the role of LGALS3BP, particularly in the context of tumor-host relationships, is still missing. Here, we show that LGALS3BP knockdown in MDA-MB-231 human breast cancer cells leads to a decreased adhesion to fibronectin, a reduced transendothelial migration and, more importantly, a reduced expression of vascular endothelial growth factor (VEGF). Production of VEGF, that was restored by exposure of silenced cells to recombinant LGALS3BP, required an intact PI3k/Akt signaling. Furthermore, we show that LGALS3BP was able to directly stimulate HUVEC tubulogenesis in a VEGF-independent, galectin-3-dependent manner. Immunohistochemical analysis of human breast cancer tissues revealed a correlation among LGALS3BP expression, VEGF expression, and blood vessel density. We propose that in addition to its prometastatic role, LGALS3BP secreted by breast cancer cells functions critically as a pro-angiogenic factor through a dual mechanism, i.e by induction of tumor VEGF and stimulation of endothelial cell tubulogenesis. [ABSTRACT FROM AUTHOR]

Published

2013

37. Identification and validation of differentially expressed proteins in epithelial ovarian cancers using quantitative proteomics

Author

Haiteng Deng, Jiatong Xu, Yuling Chen, Guangming Cao, Chongdong Liu, Zhenyu Zhang, and Hong Qu

Subjects

0301 basic medicine, epithelial ovarian cancer, Proteomics, Pathology, Time Factors, Carcinoma, Ovarian Epithelial, 0302 clinical medicine, LGALS3BP, Carbon-Nitrogen Ligases, Neoplasms, Glandular and Epithelial, Ovarian Neoplasms, CLIC1, therapeutic target, Cell cycle, Tumor Burden, Blot, Gene Expression Regulation, Neoplastic, Oncology, 030220 oncology & carcinogenesis, Biosynthetic process, Immunohistochemistry, Female, RNA Interference, medicine.drug, Research Paper, Signal Transduction, medicine.medical_specialty, Cytidine Triphosphate, Quantitative proteomics, Mice, Nude, Antineoplastic Agents, Biology, Transfection, 03 medical and health sciences, Antigens, Neoplasm, Chloride Channels, Predictive Value of Tests, Cell Line, Tumor, medicine, Biomarkers, Tumor, Animals, Humans, Cell Proliferation, Glycoproteins, Cisplatin, Dose-Response Relationship, Drug, Reproducibility of Results, Hydrogen Peroxide, medicine.disease, G1 Phase Cell Cycle Checkpoints, Oxidative Stress, 030104 developmental biology, Drug Resistance, Neoplasm, Cancer research, Ovarian cancer, Carrier Proteins

Abstract

// Hong Qu 1, * , Yuling Chen 2, 3, * , Guangming Cao 1 , Chongdong Liu 1 , Jiatong Xu 3 , Haiteng Deng 3 , Zhenyu Zhang 1 1 Department of Obstetrics & Gynecology, Beijing Chao-yang Hospital Affiliated to Capital Medical University, Beijing, China 2 Tsinghua University-Peking University Joint Center for Life Sciences, Beijing, China 3 MOE Key Laboratory of Bioinformatics, School of Life Sciences, Tsinghua University, Beijing, China * These authors have contributed equally to this work Correspondence to: Zhenyu Zhang, email: zhenyuzhang2000@163.com Haiteng Deng, email: dht@mail.tsinghua.edu.cn Keywords: proteomics, epithelial ovarian cancer, CLIC1, LGALS3BP, therapeutic target Received: May 02, 2016 Accepted: October 19, 2016 Published: November 4, 2016 ABSTRACT Ovarian cancer is the most lethal gynecological malignant tumor because of its high recurrence rate. In the present work, in order to find new therapeutic targets, we identified 8480 proteins in thirteen pairs of ovarian cancer tissues and normal ovary tissues through quantitative proteomics. 498 proteins were found to be differentially expressed in ovarian cancer, which involved in various cellular processes, including metabolism, response to stimulus and biosynthetic process. The expression levels of chloride intracellular channel protein 1 (CLIC1) and lectin galactoside-binding soluble 3 binding protein (LGALS3BP) in epithelial ovarian cancer tissues were significantly higher than those in normal ovary tissues as confirmed by western blotting and immunohistochemistry. The knockdown of CLIC1 in A2780 cell line downregulated expression of CTPS1, leading to the decrease of CTP and an arrest of cell cycle G1 phase, which results into a slower proliferation. CLIC1-knockdown can also slow down the tumor growth in vivo. Besides, CLIC1-knockdown cells showed an increased sensitivity to hydrogen peroxide and cisplatin, suggesting that CLIC1 was involved in regulation of redox and drug resistance in ovarian cancer cells. These results indicate CLIC1 promotes tumorgenesis, and is a potential therapeutic target in epithelial ovarian cancer treatment.

Published

2016

38. LGALS3BP/Gal-3 promotes osteogenic differentiation of human periodontal ligament stem cells.

Author

Zhang, Lingpeng, Huang, Yanfei, Lou, Huiquan, Gong, Xuetao, Ouyang, Qian, and Yu, Hongbin

Subjects

*PERIODONTAL ligament, *STEM cells, *ALKALINE phosphatase, *SOX2 protein, *PROTEIN expression

Abstract

• Expression of LGALS3BP and Gal-3 is increased in hPDLSCs induced by osteogenic differentiation. • Recombinant Gal-3 promotes osteogenic differentiation of hPDLSCs. • Knockdown of Gal-3 suppresses the osteogenic differentiation and osteogenesis ability of hPDLSCs. To identify the role of LGALS3BP/Gal-3 in the process of human periodontal ligament stem cells (hPDLSCs) differentiating into osteoblasts. IP-WB experiments were carried out to examine the binding of LGALS3BP and Gal-3. Western blot was performed to detect the expressions of LGALS3BP and Gal-3 in hPDLSCs with or without osteogenic differentiation inducement. The expressions of differentiation-related Oct4, Sox2 and Runx2 were also detected by western blot. Alkaline Phosphatase (ALP) Assay Kit was used to measure ALP activity in hPDLSCs. The mineralization ability of hPDLSCs was observed by staining with Alizarin Red S solution. LGALS3BP bound with Gal-3 in hPDLSCs, and the expression of LGALS3BP and Gal-3 was improved after osteogenic differentiation of hPDLSCs. Recombinant GAL-3 promoted the expression of differentiation-related proteins Oct4 and Sox2 and Runx2 in osteogenic differentiation-induced hPDLSCs. Recombinant GAL-3 also promoted the differentiation of osteogenesis-induced hPDLSCs. Furthermore, LGALS3BP had a facilitating effect on differentiation-related protein expression, while it could be reversed by shGal-3. LGALS3BP also promoted osteogenic capacity of hPDLSCs, and shGal-3 could reverse this effect. LGALS3BP binds to Gal-3, producing a promoting effect on the osteogenic differentiation of human periodontal ligament stem cells. [ABSTRACT FROM AUTHOR]

Published

2021

39. Targeting Vesicular LGALS3BP by an Antibody-Drug Conjugate as Novel Therapeutic Strategy for Neuroblastoma

Author

Vincenzo De Laurenzi, Manuela Iezzi, Fabio Pastorino, Rodolfo Ippoliti, Rossano Lattanzio, Stefano Iacobelli, Enza Piccolo, Valeria Panella, Sara Ponziani, Michele Sallese, Mirco Ponzoni, Cosmo Rossi, Giulia Di Vittorio, Francesco Giansanti, Arturo Sala, Gianluca Sala, Daniela D'Agostino, Valentina Iacobelli, Sandra Bibbò, Alessia Lamolinara, Emily Capone, and Roberta Gentile

Subjects

0301 basic medicine, Cancer Research, Antibody-drug conjugate, Stromal cell, medicine.medical_treatment, lcsh:RC254-282, Article, Targeted therapy, neuroblastoma, 03 medical and health sciences, 0302 clinical medicine, Antibody-Drug Conjugates (ADC)s, LGALS3BP, targeted therapy, Neuroblastoma, Medicine, Therapeutic strategy, Tumor microenvironment, business.industry, Cancer, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, medicine.disease, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Cancer research, business, Conjugate

Abstract

Simple Summary Antibody Drug Conjugates are an emerging class of biopharmaceuticals that have seen an impressive increase of attention in the field of cancer therapy. Here, we describe the therapeutic activity of 1959-sss/DM3, a non-internalizing ADC targeting LGALS3BP, a secreted, extracellular vesicles-associated protein expressed by the majority of human cancers, including neuroblastoma. We show that 1959-sss/DM3 treatment can cure mice with established neuroblastoma tumours in pseudometastatic, orthotopic and Patient Derived Xenograft models. Abstract Neuroblastoma is the most common extra-cranial solid tumor in infants and children, which accounts for approximately 15% of all cancer-related deaths in the pediatric population. New therapeutic modalities are urgently needed. Antibody-Drug Conjugates (ADC)s-based therapy has been proposed as potential strategy to treat this pediatric malignancy. LGALS3BP is a highly glycosylated protein involved in tumor growth and progression. Studies have shown that LGALS3BP is enriched in extracellular vesicles (EV)s derived by most neuroblastoma cells, where it plays a critical role in preparing a favorable tumor microenvironment (TME) through direct cross talk between cancer and stroma cells. Here, we describe the development of a non-internalizing LGALS3BP ADC, named 1959-sss/DM3, which selectively targets LGALS3BP expressing neuroblastoma. 1959-sss/DM3 mediated potent therapeutic activity in different types of neuroblastoma models. Notably, we found that treatments were well tolerated at efficacious doses that were fully curative. These results offer preclinical proof-of-concept for an ADC targeting exosomal LGALS3BP approach for neuroblastomas.

Published

2020

40. Increased LGALS3 expression independently predicts shorter overall survival in patients with the proneural subtype of glioblastoma

Author

Dekang Li, Junchen Chen, Xia He, and Sunfu Zhang

Subjects

0301 basic medicine, Oncology, Male, Cancer Research, Galectin 3, 0302 clinical medicine, LGALS3BP, Promoter Regions, Genetic, Original Research, Brain Neoplasms, Blood Proteins, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Prognosis, Isocitrate Dehydrogenase, Up-Regulation, Gene Expression Regulation, Neoplastic, CpG site, 030220 oncology & carcinogenesis, DNA methylation, Biomarker (medicine), Female, proneural subtype, medicine.drug, medicine.medical_specialty, IDH1, In silico, Galectins, Subgroup analysis, Biology, lcsh:RC254-282, 03 medical and health sciences, Antigens, Neoplasm, Internal medicine, medicine, Biomarkers, Tumor, Humans, Radiology, Nuclear Medicine and imaging, Computer Simulation, Epigenetics, Retrospective Studies, LGALS3, Temozolomide, Gene Expression Profiling, glioblastoma, Clinical Cancer Research, DNA Methylation, Survival Analysis, 030104 developmental biology, CpG Islands

Abstract

In the current study, we tried to study the expression of LGALS3 and LGALS3BP, their potential as prognostic markers and the possible genetic/epigenetic mechanisms underlying their dysregulation in different subtypes of glioblastoma (GBM). An in silico retrospective study was performed using large online databases. Results showed that LGALS3 and LGALS3BP were upregulated at both RNA and protein levels in GBM tissue and were generally associated with shorter overall survival (OS) in GBM patients. However, in subgroup analysis, we only found the association in proneural subtype. The copy number alterations did not necessarily lead to LGALS3/LGALS3BP dysregulation. In the proneural subtype of GBM patients, hypermethylation of the two CpG sites (cg19099850 and cg17403875) was associated with significantly lower expression of LGALS3. In univariate and multivariate analysis, LGALS3 expression independently predicted shorter OS in the proneural subtype of GBM (HR: 1.487, 95% CI: 1.229‐1.798, P

Published

2018

41. LGALS3BP, lectin galactoside-binding soluble 3 binding protein, promotes oncogenic cellular events impeded by antibody intervention

Author

Stampolidis, P, Ullrich, A, and Iacobelli, S

Published

2015

42. Molecular and Functional Characterization of the Galectin-3-Binding Protein LGALS3BP in Cancer and Centrosome Biology

Author

Schade, Sophia

Subjects

centrosome, LGALS3BP, cancer

Abstract

The centrosome acts as the main microtubule-organizing centre in eukaryotic cells. Besides its function in microtubule nucleation it is further implicated in integrating cellular signalling pathways that are essential for cell cycle progression or the response to DNA damage, for instance. In cancer, numerical and structural centrosome aberrations are frequently detected where they contribute to chromosomal instability. Seeking for factors that are functionally relevant for these centrosomal abnormalities, our group established a protein-protein interaction network among centrosomal and cell cycle-regulatory proteins using TAP-MS analysis. Thereby, LGALS3BP, which is deregulated in cancer, was revealed to interact with centrosomal components. The subcellular localization of LGALS3BP to centrosomes and in particular to the proximal part of centrioles was validated by several approaches in this study. LGALS3BP has been previously reported as a secreted glycoprotein with extracellular functions. The present study, however, provides striking evidence that LGALS3BP is involved in the maintenance of centrosome integrity: LGALS3BP upregulation caused centrosome hypertrophy, while depletion led to an accumulation of defective centriolar structures. Supportingly, LGALS3BP deregulation correlated with centrosome abnormalities in certain prostate as well as breast cancer cell lines. Importantly, two rescue experiments revealed a reversion of these phenotypes towards control cells upon restoration of normal LGALS3BP levels. Furthermore, the presence of both LGALS3BP and its interaction partner C-Nap1 was found to be crucial for cell proliferation and viability as simultaneous loss of these proteins caused aneuploidy and apoptosis. An in vitro kinase assay on LGALS3BP peptides revealed AKT1, CHK1 and CHK2 as candidate kinases, which suggests an implication of LGALS3BP in AKT signalling downstream events and DNA damage response. Together, these findings asked for mechanisms that regulate LGALS3BP expression and reasons for its deregulation in cancer. The present study revealed BRD4 as a positive regulator of LGALS3BP gene expression and as a mediator of INFγ-induced LGALS3BP upregulation. Additionally, EZH2 was found responsible for silencing LGALS3BP gene expression in prostate cancer as EZH2 depletion in a respective prostate cancer cell line led to re-expression of LGALS3BP. BRD4 and EZH2 are deregulated in various cancer types, which might explain LGALS3BP deregulation and centrosome aberrations. This study represents the first characterization of intracellular LGALS3BP maintaining centrosome integrity and function. The new insights into LGALS3BP transcriptional regulation now provide opportunities to study if epigenetic therapies targeting LGALS3BP could counteract centrosome aberration in cancer., Das Zentrosom stellt das wesentliche Mikrotubuli-organisierende Zentrum in eukaryotischen Zellen dar. Neben seiner Funktion bei der Mikrotubulinukleation ist es beteiligt an der Integration von zellulären Signaltransduktionswegen, welche beispielsweise für das Fortschreiten des Zellzyklus sowie für die Antwort auf DNS-Schäden wichtig sind. Numerische und strukturelle Aberrationen des Zentrosoms treten sehr häufig während der Krebsentstehung auf und tragen zur Ausbildung von chromosomaler Instabilität bei. Um funktionell relevante Faktoren für diese zentrosomalen Anomalien zu identifizieren, wurde von unserer Arbeitsgruppe ein Proteininteraktionsnetzwerk mittels TAP-MS-Analyse etabliert, welches sich um zentrosomale und Zellzyklus-regulierende Proteine aufbaut. Hierbei wurde LGALS3BP, ein in Krebs dereguliertes Protein, entdeckt, welches mit anderen zentrosomalen Proteinen interagierte. Es konnte durch mehrere Methoden gezeigt werden, dass LGALS3BP am Zentrosom lokalisiert und zwar insbesondere am proximalen Teil der Zentriolen. Zuvor wurde LGALS3BP als ein sekretiertes Glykoprotein mit extrazellulären Funktionen beschrieben. Diese Studie jedoch belegt, dass LGALS3BP auch an der Aufrechterhaltung zentrosomaler Integrität beteiligt ist. Eine Hochregulation von LGALS3BP führte zu zentrosomaler Hypertrophie, wohingegen eine Verminderung von LGALS3BP eine Akkumulation fehlerhafter zentriolärer Strukturen bewirkte. Diese Ergebnisse korrelieren positiv mit LGALS3BP-Fehlexpression und zentrosomalen Aberrationen in verschiedenen Prostata- und Brustkrebszelllinien. Zudem konnte durch die Wiederherstellung normaler LGALS3BP-Expression in zwei Experimenten der jeweilige zentrosomale Phänotyp rückgängig gemacht werden. Es wurde außerdem gezeigt, dass LGALS3BP zusammen mit seinem Interaktionspartner C-Nap1 für die Zellproliferation und -lebensfähigkeit benötigt wird, da das Herunterregulieren beider Proteine zu Aneuploidie und Apoptose führte. Des Weiteren wurden die Kinasen AKT1, CHK1 und CHK2 über eine in vitro Phosphorylierungs-Analyse an LGALS3BP-Peptiden identifiziert, was darauf hindeutet, dass LGALS3BP in AKT-Signalwegen und in Antwortmechanismen auf DNS-Schäden involviert sein könnte. Aufgrund dieser Ergebnisse stellte sich die Frage nach Möglichkeiten der transkriptionellen Regulation von LGALS3BP und nach den Ursachen dessen Deregulierung in Krebs. In dieser Studie VIIZusammenfassung wurde BRD4 als ein positiver Regulator der LGALS3BP-Genexpression ermittelt, welcher auch als Mediator der INFγ-Antwort von LGALS3BP agierte. Zudem wurde EZH2 für die LGALS3BP-Genstilllegung in Prostatakrebs verantwortlich gefunden, da eine Verminderung von EZH2 zur Reexpression von LGALS3BP in einer entsprechenden Prostatakrebszelllinie führte. In verschiedenen Krebsarten werden BRD4 und EZH2 häufig fehlexprimiert, was auch die LGALS3BP-Deregulation und somit die zentrosomalen Anomalien erklären könnte. Die vorliegende Arbeit stellt die erste Charakterisierung von intrazellulärem LGALS3BP dar, welches zentrosomale Integrität und Funktion aufrechterhält. Die neuen Einblicke in die transkriptionelle Regulation von LGALS3BP erlauben es nun experimentell zu ergründen, ob auf LGALS3BP gerichtete epigenetische Therapien Auswirkungen auf die Krebsentwicklung haben und die möglicherweise ursächlichen zentrosomalen Anomalitäten reduzieren.

Published

2017

43. Targeting Vesicular LGALS3BP by an Antibody-Drug Conjugate as Novel Therapeutic Strategy for Neuroblastoma.

Author

Capone, Emily, Lamolinara, Alessia, Pastorino, Fabio, Gentile, Roberta, Ponziani, Sara, Di Vittorio, Giulia, D'Agostino, Daniela, Bibbò, Sandra, Rossi, Cosmo, Piccolo, Enza, Iacobelli, Valentina, Lattanzio, Rossano, Panella, Valeria, Sallese, Michele, De Laurenzi, Vincenzo, Giansanti, Francesco, Sala, Arturo, Iezzi, Manuela, Ponzoni, Mirco, and Ippoliti, Rodolfo

Subjects

*THERAPEUTIC use of monoclonal antibodies, *CELL proliferation, *ANIMAL experimentation, *CELL differentiation, *EXTRACELLULAR space, *GENE expression, *MICE, *NEUROBLASTOMA, *TREATMENT effectiveness

Abstract

Simple Summary: Antibody Drug Conjugates are an emerging class of biopharmaceuticals that have seen an impressive increase of attention in the field of cancer therapy. Here, we describe the therapeutic activity of 1959-sss/DM3, a non-internalizing ADC targeting LGALS3BP, a secreted, extracellular vesicles-associated protein expressed by the majority of human cancers, including neuroblastoma. We show that 1959-sss/DM3 treatment can cure mice with established neuroblastoma tumours in pseudometastatic, orthotopic and Patient Derived Xenograft models. Neuroblastoma is the most common extra-cranial solid tumor in infants and children, which accounts for approximately 15% of all cancer-related deaths in the pediatric population. New therapeutic modalities are urgently needed. Antibody-Drug Conjugates (ADC)s-based therapy has been proposed as potential strategy to treat this pediatric malignancy. LGALS3BP is a highly glycosylated protein involved in tumor growth and progression. Studies have shown that LGALS3BP is enriched in extracellular vesicles (EV)s derived by most neuroblastoma cells, where it plays a critical role in preparing a favorable tumor microenvironment (TME) through direct cross talk between cancer and stroma cells. Here, we describe the development of a non-internalizing LGALS3BP ADC, named 1959-sss/DM3, which selectively targets LGALS3BP expressing neuroblastoma. 1959-sss/DM3 mediated potent therapeutic activity in different types of neuroblastoma models. Notably, we found that treatments were well tolerated at efficacious doses that were fully curative. These results offer preclinical proof-of-concept for an ADC targeting exosomal LGALS3BP approach for neuroblastomas. [ABSTRACT FROM AUTHOR]

Published

2020

44. Proteins and Molecular Pathways Relevant for the Malignant Properties of Tumor-Initiating Pancreatic Cancer Cells.

Author

Samonig, Lisa, Loipetzberger, Andrea, Blöchl, Constantin, Rurik, Marc, Kohlbacher, Oliver, Aberger, Fritz, and Huber, Christian G.

Subjects

*PANCREATIC cancer, *CANCER cells, *CALCIUM-binding proteins, *PROTEINS, *RNA interference, *PROTEOMICS, *CANCER cell culture, *CANCER stem cells

Abstract

Cancer stem cells (CSCs), a small subset of the tumor bulk with highly malignant properties, are deemed responsible for tumor initiation, growth, metastasis, and relapse. In order to reveal molecular markers and determinants of their tumor-initiating properties, we enriched rare stem-like pancreatic tumor-initiating cells (TICs) by harnessing their clonogenic growth capacity in three-dimensional multicellular spheroid cultures. We compared pancreatic TICs isolated from three-dimensional tumor spheroid cultures with nontumor-initiating cells (non-TICs) enriched in planar cultures. Employing differential proteomics (PTX), we identified more than 400 proteins with significantly different expression in pancreatic TICs and the non-TIC population. By combining the unbiased PTX with mRNA expression analysis and literature-based predictions of pro-malignant functions, we nominated the two calcium-binding proteins S100A8 (MRP8) and S100A9 (MRP14) as well as galactin-3-binding protein LGALS3BP (MAC-2-BP) as putative determinants of pancreatic TICs. In silico pathway analysis followed by candidate-based RNA interference mediated loss-of-function analysis revealed a critical role of S100A8, S100A9, and LGALS3BP as molecular determinants of TIC proliferation, migration, and in vivo tumor growth. Our study highlights the power of combining unbiased proteomics with focused gene expression and functional analyses for the identification of novel key regulators of TICs, an approach that warrants further application to identify proteins and pathways amenable to drug targeting. [ABSTRACT FROM AUTHOR]

Published

2020

45. 90K predicts the prognosis of glioma patients and enhances tumor lysate-pulsed DC vaccine for immunotherapy of GBM in vitro .

Author

Zeng Y and Chen X

Subjects

Cancer Vaccines immunology, Humans, Immunotherapy, Prognosis, Antigens, Neoplasm metabolism, Biomarkers, Tumor metabolism, Brain Neoplasms pathology, Cancer Vaccines pharmacology, Dendritic Cells immunology, Glioma pathology

Abstract

Objectives: This study aimed to investigate the relationship between 90K expression with glioma malignancy and prognosis. Additionally, the enhancement effect of 90K in the Dendritic cell (DC) vaccine for Immunotherapy of glioblastoma (GBM) was evaluated in vitro ., Methods: The expression of 90K protein in glioma tissues was detected by western blot. The relationship between the 90K expression and the tumor grade as well as the prognosis of patients was further analyzed by mining TCGA and CGGA database. The concentration of IL-12p70 and IL-10 was detected by ELISA. T lymphocyte proliferation and lethal effect of cytotoxic T cell (CTL) were detected by CCK-8., Results: The expression of 90K was significantly higher in glioma than normal tissue and increased with tumor grade (P< 0.05). Higher 90K expression was observed in IDH wildtype glioma than IDH mutant and predicted worse overall survival for glioma patients. The concentration of IL-12p70 and IFN-γ was the highest in the Apoptosis U251-90K-DC group, in which group the ability to kill U251 cells by CTL was also the strongest., Conclusion: 90K was a useful biomarker for glioma malignancy and patient prognosis. The appearance of 90K enhanced the effect of Apoptosis U251-DC vaccine for immunotherapy of GBM.

Published

2021

46. Maldevelopment of dermal lymphatics in Wnt5a-knockout-mice

Author

Kerstin Buttler, Jürgen C. Becker, Jörg Wilting, and Tobias Pukrop

Subjects

Male, FABP4, Mice, ENTPD1, LGALS3BP, Lymphangiogenesis, Wnt Signaling Pathway, ROR1, Tissue homeostasis, Cells, Cultured, Skin, Mice, Knockout, Wnt signaling pathway, Cell biology, WNT5A, Lymphatic Endothelium, medicine.anatomical_structure, Lymphatic system, Knockout mouse, embryonic structures, Intercellular Signaling Peptides and Proteins, government.form_of_government, Biology, Receptor Tyrosine Kinase-like Orphan Receptors, Wnt-5a Protein, FDZ3, Dermis, medicine, Human Umbilical Vein Endothelial Cells, Animals, Humans, Lymphatic endothelial cell, Molecular Biology, Cell Proliferation, Lymphatic Vessels, RYK, Lymphangioma, DKK2, fungi, Infant, Cell Biology, Embryo, Mammalian, Frizzled Receptors, Wnt Proteins, body regions, Case-Control Studies, Immunology, Mutation, government, AChE, sense organs, Transcriptome, Biomarkers, Developmental Biology

Abstract

Maintenance of tissue homeostasis and immune surveillance are important functions of the lymphatic vascular system. Lymphatic vessels are lined by lymphatic endothelial cells (LECs). By gene micro-array expression studies we recently compared human lymphangioma-derived LECs with umbilical vein endothelial cells (HUVECs). Here, we followed up on these studies. Besides well-known LEC markers, we observed regulation of molecules involved in immune regulation, acetylcholine degradation and platelet regulation. Moreover we identified differentially expressed WNT pathway components, which play important roles in the morphogenesis of various organs, including the blood vascular system. WNT signaling has not yet been addressed in lymphangiogenesis. We found high expression of FZD3, FZD5 and DKK2 mRNA in HUVECs, and WNT5A in LECs. The latter was verified in normal skin-derived LECs. With immunohistological methods we detected WNT5A in LECs, as well as ROR1, ROR2 and RYK in both LECs and HUVECs. In the human, mutations of WNT5A or its receptor ROR2 cause the Robinow syndrome. These patients show multiple developmental defects including the cardio-vascular system. We studied Wnt5a-knockout (ko) mouse embryos at day 18.5. We show that the number of dermal lymphatic capillaries is significantly lower in Wnt5a-null-mice. However, the mean size of individual lymphatics and the LEC number per vessel are greater. In sum, the total area covered by lymphatics and the total number of LECs are not significantly altered. The reduced number of lymphatic capillaries indicates a sprouting defect rather than a proliferation defect in the dermis of Wnt5a-ko-mice, and identifies Wnt5a as a regulator of lymphangiogenesis.

Published

2013

47. Glycoprotein 90K Promotes E-Cadherin Degradation in a Cell Density-Dependent Manner via Dissociation of E-Cadherin–p120-Catenin Complex

Author

Hyung-Ho Ha, Jung-Il Chae, Somy Yoon, So-Yeon Park, Man-Jeong Paik, Jeong A Bae, Eun Gene Sun, Kyung Keun Kim, Young-Woo Seo, Rui Zhou, and Hangun Kim

Subjects

Male, 0301 basic medicine, Delta Catenin, Cell Count, adherens junction, Metastasis, lcsh:Chemistry, 0302 clinical medicine, Neoplasms, LGALS3BP, Mac-2BP, Phosphorylation, lcsh:QH301-705.5, Spectroscopy, chemistry.chemical_classification, Catenins, General Medicine, Cadherins, Prognosis, 90K glycoprotein, E-cadherin, p120-catenin, Computer Science Applications, Cell biology, Gene Expression Regulation, Neoplastic, 030220 oncology & carcinogenesis, MCF-7 Cells, Female, Down-Regulation, Motility, Article, Catalysis, Inorganic Chemistry, Adherens junction, 03 medical and health sciences, Downregulation and upregulation, Antigens, CD, Antigens, Neoplasm, Cell Line, Tumor, Biomarkers, Tumor, Cell Adhesion, medicine, Humans, Neoplasm Invasiveness, Physical and Theoretical Chemistry, Molecular Biology, Glycoproteins, Cadherin, Cell Membrane, Organic Chemistry, medicine.disease, HEK293 Cells, 030104 developmental biology, lcsh:Biology (General), lcsh:QD1-999, chemistry, Proteolysis, Cancer cell, Caco-2 Cells, Carrier Proteins, Glycoprotein

Abstract

Glycoprotein 90K (also known as LGALS3BP or Mac-2BP) is a tumor-associated protein, and high 90K levels are associated with poor prognosis in some cancers. To clarify the role of 90K as an indicator for poor prognosis and metastasis in epithelial cancers, the present study investigated the effect of 90K on an adherens junctional protein, E-cadherin, which is frequently absent or downregulated in human epithelial cancers. Treatment of certain cancer cells with 90K significantly reduced E-cadherin levels in a cell-population-dependent manner, and these cells showed decreases in cell adhesion and increases in invasive cell motility. Mechanistically, 90K-induced E-cadherin downregulation occurred via ubiquitination-mediated proteasomal degradation. 90K interacted with the E-cadherin–p120-catenin complex and induced its dissociation, altering the phosphorylation status of p120-catenin, whereas it did not associate with β-catenin. In subconfluent cells, 90K decreased membrane-localized p120-catenin and the membrane fraction of the p120-catenin. Particularly, 90K-induced E-cadherin downregulation was diminished in p120-catenin knocked-down cells. Taken together, 90K upregulation promotes the dissociation of the E-cadherin–p120-catenin complex, leading to E-cadherin proteasomal degradation, and thereby destabilizing adherens junctions in less confluent tumor cells. Our results provide a potential mechanism to explain the poor prognosis of cancer patients with high serum 90K levels.

Published

2017

48. Increased LGALS3BP promotes proliferation and migration of oral squamous cell carcinoma via PI3K/AKT pathway.

Author

Zhang, Xiaoxin, Ding, Haoyue, Lu, Zhanyi, Ding, Liang, Song, Yuxian, Jing, Yue, Hu, Qingang, Dong, Yingchun, and Ni, Yanhong

Subjects

*SQUAMOUS cell carcinoma, *IMMUNOSTAINING, *PROTEIN binding, *CANCER invasiveness, *CELL migration

Abstract

Previous studies showed that lectin galactoside-binding soluble 3 binding protein (LGALS3BP) is an important participant in tumor progression. However, its prognostic value and functional mechanism in oral squamous cell carcinoma (OSCC) are still unclear. In this study, we analyzed LGALS3BP expression in OSCC tissues via Oncomine databases and immunohistochemical staining. LGALS3BP was significantly up-regulated in OSCC tumor tissues. IHC analysis showed that LGALS3BP was predominantly expressed in tumor cells and correlated with poor clinical characteristics. In addition, high LGALS3BP expression predicted poor clinical outcomes and multivariate analysis revealed that LGALS3BP expression was as an independent prognostic factor for OS, DFS and RFS (p <.0001, p =.002, p =.002). Mechanically, LGALS3BP regulated OSCC proliferation and migration via PI3K/AKT pathways, which was abrogated by PI3K inhibitor LY294002 in a dose-dependent manner. Our results suggested that LGALS3BP could be served as a novel independent prognostic factor as well as a potential therapeutic target for OSCC treatment. Unlabelled Image • LGALS3BP is overexpressed in OSCC and correlated with poor clinical characteristics. • LGALS3BP is an independent prognostic factor for OS, DFS and RFS. • LGALS3BP promoted OSCC cell proliferation and migration via PI3K/AKT pathways. [ABSTRACT FROM AUTHOR]

Published

2019

49. Size-exclusion chromatography as a stand-alone methodology identifies novel markers in mass spectrometry analyses of plasma-derived vesicles from healthy individuals

Author

Lorena Martin-Jaular, María José Fidalgo Sáez, Josep Maria Estanyol i Ullate, Armando de Menezes-Neto, Inés Lozano-Ramos, Carmen Fernandez-Becerra, Joan Segui-Barber, Hernando A. del Portillo, Francesc E. Borràs, and AM-N is a recipient of a postdoctoral fellowship from CNPq, Conselho Nacional de Desenvolvimento Científico e Tecnologico – Brasil. Work in the HAP laboratory is funded by the European Community’s Seventh Framework Programme and by the Ministerio Español

Subjects

Histology, comparative analysis, low infrastructure settings, Size-exclusion chromatography, exosomes, Mass spectrometry, Bioinformatics, Exosome, Sepharose, CD5L, Medicine, LGALS3BP, Original Research Article, lcsh:QH573-671, mass spectrometry, lcsh:Cytology, business.industry, Vesicle, Cell Biology, Blood proteins, Microvesicles, Biochemistry, Ultracentrifuge, business, plasma-derived exosomes

Abstract

Plasma-derived vesicles hold a promising potential for use in biomedical applications. Two major challenges, however, hinder their implementation into translational tools: (a) the incomplete characterization of the protein composition of plasma-derived vesicles, in the size range of exosomes, as mass spectrometric analysis of plasma sub-components is recognizably troublesome and (b) the limited reach of vesicle-based studies in settings where the infrastructural demand of ultracentrifugation, the most widely used isolation/purification methodology, is not available. In this study, we have addressed both challenges by carrying-out mass spectrometry (MS) analyses of plasma-derived vesicles, in the size range of exosomes, from healthy donors obtained by 2 alternative methodologies: size-exclusion chromatography (SEC) on sepharose columns and Exo-Spin™. No exosome markers, as opposed to the most abundant plasma proteins, were detected by Exo-Spin™. In contrast, exosomal markers were present in the early fractions of SEC where the most abundant plasma proteins have been largely excluded. Noticeably, after a cross-comparative analysis of all published studies using MS to characterize plasma-derived exosomes from healthy individuals, we also observed a paucity of “classical exosome markers.” Independent of the isolation method, however, we consistently identified 2 proteins, CD5 antigen-like (CD5L) and galectin-3-binding protein (LGALS3BP), whose presence was validated by a bead-exosome FACS assay. Altogether, our results support the use of SEC as a stand-alone methodology to obtain preparations of extracellular vesicles, in the size range of exosomes, from plasma and suggest the use of CD5L and LGALS3BP as more suitable markers of plasma-derived vesicles in MS. Keywords : exosomes; low infrastructure settings; CD5L; LGALS3BP; comparative analysis; plasma-derived exosomes; mass spectrometry (Published: 6 July 2015) Citation: Journal of Extracellular Vesicles 2015, 4 : 27378 - http://dx.doi.org/10.3402/jev.v4.27378 SUPPLEMENTARY MATERIAL : To access the supplementary material to this article, please see Supplementary files under ‘Article Tools’.

Published

2015

50. Regulation von Ras-Zielgenen durch DNA-Methylierung und Histon-modifizierende Mechanismen

Author

Weißhaupt, Karen Roselind

Subjects

Clusterin, Loxl2, Lgals3bp, Lox, 600 Technik, Medizin, angewandte Wissenschaften::610 Medizin und Gesundheit, Methylation, Mmp2, Thbs1, Fstl1, Acetylierung, Timp2, Ras

Abstract

In der vorliegenden Arbeit wurde der Einfluss von Methylierung und Acetylierung auf die Expression von insgesamt acht Ras-abhängig regulierten Genen in den Rattenfibroblasten 208F (immortal) und FE-8 (Hras-Onkogen transformiert) untersucht. Alle Gene sind Zielgene des Raf/MEK/ERK-Signalwegs in den FE-8 Zellen und werden durch einen aktivierten Signalweg supprimiert. Durch pharmakologische Hemmung des Signalwegs werden diese Gene aufreguliert. Clusterin, Loxl2, Mmp2, Thbs1, Timp2 und Lgals3bp wurden zusätzlich durch das demethylierende Agens 5-Aza-CdR in den Ras-transformierten FE-8 Zellen aufreguliert. Anders als in den Vorversuchen wies Fstl1 keine Regulierung und Lox sogar eine weitere Suppression unter 5-Aza-CdR auf. Inhibition der Histondeacetylasen durch TSA führte zu einer Aufregulierung von Clusterin, Loxl2, Mmp2, Thbs1 und Timp2. Lox und Lgals3bp zeigten eine Suppression unter TSA, Fstl1 keine Expressionsänderung. siRNA gegen DNMT1 hatte eine Reexpression von Clusterin und Mmp2 in den FE-8 Zellen zur Folge, die übrigen Gene wurden nicht analysiert. Diese Experimente lassen epigenetische Mechanismen in der Inaktivierung dieser Gene nach Ras-Transformation vermuten. Für das Gen Clusterin konnte tatsächlich eine methylierungsabhängige Regulation nachgewiesen werden [Lund et al., 2006]. Die Gene Loxl2, Mmp2, Timp2, Thbs1 und Lgals3bp werden zumindest indirekt reguliert. Für Timp2 und Lgals3bp kann ein räumlicher Effekt auf der DNA mit übergeordneten regulatorischen Elementen für eine epigenetische Regulation postuliert werden: beide Gene liegen auf dem Chromosom 10q32.3, zwischen ihren Transkriptionsstartpunkten befinden sich keine weiteren kodierenden Regionen. Der Mechanismus der Ras-abhängigen Methylierung ist unklar, jedoch stellt DNMT1 ein mögliches Schlüsselenzym dar. Für einige der untersuchten Gene ist bereits eine Beteiligung an der Transformation oder der Tumorgenese bekannt. Weitere Grundlagenforschung ist notwendig, um die komplexen Mechanismen der Genregulation (in Tumorzellen) aufzudecken., Within the current thesis, the influence of DNA methylation and histone deacetylation onto the expression of eight Ras-dependent regulated genes was investigated in immortalized (208F) and Hras-transformed (FE-8) rat fibroblasts. All genes are target genes of the Raf/MEK/ERK-signal transduction pathway in FE-8 cells and are suppressed through an activated pathway. Upon pharmacological inhibition of the pathway, the genes get re-expressed. Clusterin, Loxl2, Mmp2, Thbs1, Timp2 and Lgals3bp also became upregulated in the Hras-transformed cells upon treatment with the demethylating agent 5-Aza- CdR. In contrast to preliminary investigations, Fstl1 was not upregulated and Lox was even further suppressed by 5-Aza-CdR. Inhibition of Histon deacetylases by Trichostatin A resulted in an upregulation of Clusterin, Loxl2, Mmp2, Thbs1 and Timp2. The expression of Lox and Lgals3bp was suppressed; the expression of Fstl1 was not influenced. siRNA against DNMT1 in the Hras-transformed cells resulted in a re-expression of Clusterin and Mmp2, the other genes were not analysed. These experiments suggest an involvement of epigenetic mechanisms in the suppression of genes following Ras transformation. For the Clusterin gene, a methylation-dependent regulation could indeed be proven [Lund et al., 2006], while Loxl2, Mmp2, Thbs1 and Timp2 are likely to be regulated indirectly via DNA methylation. A territorial effect on DNA with higher-ranking regulatory elements mediating an epigenetic regulation was postulated for Timp2 and Lgals3bp: both genes are located on chromosome 10q32.3 with no other coding regions in between. The mechanism of RAS-dependent epigenetic regulation is unclear, however DNMT1 must be discussed as one of the key enzymes. An involvement in transformation or tumour genesis is already known for most of the genes investigated. Further research is necessary to reveal the complex mechanisms of gene regulation (in tumour cells).

Published

2010