Your search keyword '"JUP"' showing total 39 results

1. Combination of FLNC and JUP variants causing arrhythmogenic cardiomyopathy in an Iranian family with different clinical features

Author

Kasra Mehdizadeh, Mahdieh Soveizi, Amir Askarinejad, Amin Elahifar, Tannaz Masoumi, Amir Farjam Fazelifar, Sanaz Asadian, Majid Maleki, and Samira Kalayinia

Subjects

Arrhythmogenic cardiomyopathy, Arrhythmogenic left ventricular cardiomyopathy, FLNC, JUP, DES, Diseases of the circulatory (Cardiovascular) system, RC666-701

Abstract

Abstract Background Arrhythmogenic cardiomyopathy (ACM) characterized by progressive myocardial loss and replacement with fibro-fatty tissue is a major cause of sudden cardiac death (SCD). In particular, ACM with predominantly left ventricular involvement, known as arrhythmogenic left ventricular cardiomyopathy (ALVC), has a poor prognosis. Methods The proband underwent whole-exome sequencing (WES) to determine the etiology of ALVC. Family members were then analyzed using PCR and Sanger sequencing. Clinical evaluations including 12-lead ECG, transthoracic echocardiography, and cardiac MRI were performed for all available first-degree relatives. Results WES identified two variants in the FLNC (c.G3694A) and JUP (c.G1372A) genes, the combination of which results in ALVC and SCD. Conclusion The present study comprehensively investigates the involvement of two discovered variants of FLNC and JUP in the pathogenesis of ALVC. More study is necessary to elucidate the genetic factors involved in the etiology of ALVC.

Published

2024

2. Mycn ameliorates cardiac hypertrophy-induced heart failure in mice by mediating the USP2/JUP/Akt/β-catenin cascade

Author

Weinian Gao, Na Guo, Hongjiang Yan, Shuguang Zhao, Yongquan Sun, and Ziying Chen

Subjects

Cardiac hypertrophy, Heart failure, Mycn, USP2, JUP, Akt/β-catenin, Diseases of the circulatory (Cardiovascular) system, RC666-701

Abstract

Abstract Background Pathological cardiac hypertrophy is associated with cardiac dysfunction and is a key risk factor for heart failure and even sudden death. This study investigates the function of Mycn in cardiac hypertrophy and explores the interacting molecules. Methods A mouse model of cardiac hypertrophy was induced by isoproterenol (ISO). The cardiac dysfunction was assessed by the heart weight-to-body weight ratio (HW/BW), echocardiography assessment, pathological staining, biomarker detection, and cell apoptosis. Transcriptome alteration in cardiac hypertrophy was analyzed by bioinformatics analysis. Gain- or loss-of-function studies of MYCN proto-oncogene (Mycn), ubiquitin specific peptidase 2 (USP2), and junction plakoglobin (JUP) were performed. The biological functions of Mycn were further examined in ISO-treated cardiomyocytes. The molecular interactions were verified by luciferase assay or immunoprecipitation assays. Results Mycn was poorly expressed in ISO-treated mice, and its upregulation reduced HW/BW, cell surface area, oxidative stress, and inflammation while improving cardiac function of mice. It also reduced apoptosis of cardiomyocytes in mice and those in vitro induced by ISO. Mycn bound to the USP2 promoter to activate its transcription. USP2 overexpression exerted similar myocardial protective functions. It stabilized JUP protein by deubiquitination modification, which blocked the Akt/β-catenin pathway. Knockdown of JUP restored phosphorylation of Akt and β-catenin protein level, which negated the protective effects of USP2. Conclusion This study demonstrates that Mycn activates USP2 transcription, which mediates ubiquitination and protein stabilization of JUP, thus inactivating the Akt/β-catenin axis and alleviating cardiac hypertrophy-induced heart failure.

Published

2024

3. Combination of FLNC and JUP variants causing arrhythmogenic cardiomyopathy in an Iranian family with different clinical features

Author

Mehdizadeh, Kasra, Soveizi, Mahdieh, Askarinejad, Amir, Elahifar, Amin, Masoumi, Tannaz, Fazelifar, Amir Farjam, Asadian, Sanaz, Maleki, Majid, and Kalayinia, Samira

Published

2024

4. Mycn ameliorates cardiac hypertrophy-induced heart failure in mice by mediating the USP2/JUP/Akt/β-catenin cascade

Author

Gao, Weinian, Guo, Na, Yan, Hongjiang, Zhao, Shuguang, Sun, Yongquan, and Chen, Ziying

Published

2024

5. Downregulation of γ-Catenin by miR-195-5p Inhibits Colon Cancer Progression, Regulating Desmosome Function.

Author

Piccinno, Emanuele, Scalavino, Viviana, Labarile, Nicoletta, Bianco, Giusy, Savino, Maria Teresa, Armentano, Raffaele, Giannelli, Gianluigi, and Serino, Grazia

Subjects

*COLON cancer, *CANCER invasiveness, *INHIBITION of cellular proliferation, *DOWNREGULATION, *COLORECTAL cancer, *CATENINS

Abstract

Desmosomes are essential structures for ensuring tissue functions, and their deregulation is involved in the development of colorectal cancer (CRC). JUP (γ-catenin) is a desmosome adhesion component that also acts as a signaling hub, suggesting its potential involvement in CRC progression. In this context, we recently demonstrated that miR-195-5p regulated JUP and desmosome cadherins expression. In addition, miR-195-5p gain of function indirectly modulated the expression of key effectors of the Wnt pathway involved in JUP-dependent signaling. Here, our purpose was to demonstrate the aberrant expression of miR-195-5p and JUP in CRC patients and to functionally characterize the role of miR-195-5p in the regulation of desmosome function. First, we showed that miR-195-5p was downregulated in CRC tumors compared to adjacent normal tissue. Then, we demonstrated that JUP expression was significantly increased in CRC tissues compared to adjacent normal tissues. The effects of miR-195-5p on CRC progression were assessed using in vitro transient transfection experiments and in vivo miRNA administration. Increased miR-195-5p in colonic epithelial cells strongly inhibits cell proliferation, viability, and invasion via JUP. In vivo gain of function of miR-195-5p reduced the numbers and sizes of tumors and significantly ameliorated the histopathological changes typical of CRC. In conclusion, our findings indicate a potential pharmacological target based on miR-195-5p replacement as a new therapeutic approach in CRC. [ABSTRACT FROM AUTHOR]

Published

2024

6. miR-195-5p as Regulator of γ-Catenin and Desmosome Junctions in Colorectal Cancer.

Author

Piccinno, Emanuele, Scalavino, Viviana, Armentano, Raffaele, Giannelli, Gianluigi, and Serino, Grazia

Subjects

*COLORECTAL cancer, *CELL polarity, *CELLULAR control mechanisms, *CELL adhesion, *GENE expression, *TEMPOROPARIETAL junction, *WNT signal transduction, *CATENINS

Abstract

Desmosomes play a key role in the regulation of cell adhesion and signaling. Dysregulation of the desmosome complex is associated with the loss of epithelial cell polarity and disorganized tissue architecture typical of colorectal cancer (CRC). The aim of this study was to investigate and characterize the effect of miR-195-5p on desmosomal junction regulation in CRC. In detail, we proposed to investigate the deregulation of miR-195-5p and JUP, a gene target that encodes a desmosome component in CRC patients. JUP closely interacts with desmosomal cadherins, and downstream, it regulates several intracellular transduction factors. We restored the miR-195-5p levels by transient transfection in colonic epithelial cells to examine the effects of miR-195-5p on JUP mRNA and protein expression. The JUP regulation by miR-195-5p, in turn, determined a modulation of desmosome cadherins (Desmoglein 2 and Desmocollin 2). Furthermore, we focused on whether the miR-195-5p gain of function was also able to modulate the expression of key components of Wnt signaling, such as NLK, LEF1 and Cyclin D1. In conclusion, we have identified a novel mechanism controlled by miR-195-5p in the regulation of adhesive junctions, suggesting its potential clinical relevance for future miRNA-based therapy in CRC. [ABSTRACT FROM AUTHOR]

Published

2023

7. Extracellular vesicles of human diabetic retinopathy retinal tissue and urine of diabetic retinopathy patients are enriched for the junction plakoglo bin protein.

Author

Mighty, Jason, Rubio-Navarro, Alfonso, Cui Shi, Jing Zhou, Flores-Bellver, Miguel, Heissel, Søren, Onwumere, Onyekwere, Einbond, Linda, Gharbaran, Rajendra, Casper, Daniel S., Benito-Martin, Alberto, and Redenti, Stephen

Subjects

EXTRACELLULAR vesicles, DIABETIC retinopathy, PEOPLE with diabetes, RETINAL diseases, VISION disorders, URINE

Abstract

Introduction: Diabetic Retinopathy (DR) is a potentially blinding retinal disorder that develops through the pathogenesis of diabetes. The lack of disease predictors implies a poor prognosis with frequent irreversible retinal damage and vision loss. Extracellular Vesicles (EVs) present a novel opportunity for pre-symptomatic disease diagnosis and prognosis, both severely limited in DR. All biological fluids contain EVs, which are currently being studied as disease biomarkers. EV proteins derived from urine have emerged as potential noninvasive biomarkers. Methods: In this study, we isolated EVs from DR retinal tissue explants and from DR patients' urine, and characterized the vesicles, finding differences in particle number and size. Next, we performed proteomic analysis on human explanted DR retinal tissue conditioned media, DR retinal EVs and DR urinary EVs and compared to normal human retinal tissue, retinal EVs, and urinary EVs, respectively Results: Our system biology analysis of DR tissue and EV expression profiles revealed biological pathways related to cell-to-cell junctions, vesicle biology, and degranulation processes. Junction Plakoglobin (JUP), detected in DR tissue-derived EVs and DR urinary EVs, but not in controls, was revealed to be a central node in many identified pathogenic pathways. Proteomic results were validated by western blot. Urinary EVs obtained from healthy donors and diabetic patient without DR did not contain JUP. Conclusion: The absence of JUP in healthy urinary EVs provide the basis for development of a novel Diabetic Retinopathy biomarker, potentially facilitating diagnosis. [ABSTRACT FROM AUTHOR]

Published

2023

8. Extracellular vesicles of human diabetic retinopathy retinal tissue and urine of diabetic retinopathy patients are enriched for the junction plakoglo bin protein

Author

Jason Mighty, Alfonso Rubio-Navarro, Cui Shi, Jing Zhou, Miguel Flores-Bellver, Søren Heissel, Onyekwere Onwumere, Linda Einbond, Rajendra Gharbaran, Daniel S. Casper, Alberto Benito-Martin, and Stephen Redenti

Subjects

extracellular vesicle (EV), diabetic retinopathy, JUP, proteomics & bioinformatics, retina, urinary EVs, Diseases of the endocrine glands. Clinical endocrinology, RC648-665

Abstract

IntroductionDiabetic Retinopathy (DR) is a potentially blinding retinal disorder that develops through the pathogenesis of diabetes. The lack of disease predictors implies a poor prognosis with frequent irreversible retinal damage and vision loss. Extracellular Vesicles (EVs) present a novel opportunity for pre-symptomatic disease diagnosis and prognosis, both severely limited in DR. All biological fluids contain EVs, which are currently being studied as disease biomarkers. EV proteins derived from urine have emerged as potential noninvasive biomarkers.MethodsIn this study, we isolated EVs from DR retinal tissue explants and from DR patients’ urine, and characterized the vesicles, finding differences in particle number and size. Next, we performed proteomic analysis on human explanted DR retinal tissue conditioned media, DR retinal EVs and DR urinary EVs and compared to normal human retinal tissue, retinal EVs, and urinary EVs, respectivelyResultsOur system biology analysis of DR tissue and EV expression profiles revealed biological pathways related to cell-to-cell junctions, vesicle biology, and degranulation processes. Junction Plakoglobin (JUP), detected in DR tissue-derived EVs and DR urinary EVs, but not in controls, was revealed to be a central node in many identified pathogenic pathways. Proteomic results were validated by western blot. Urinary EVs obtained from healthy donors and diabetic patient without DR did not contain JUP.ConclusionThe absence of JUP in healthy urinary EVs provide the basis for development of a novel Diabetic Retinopathy biomarker, potentially facilitating diagnosis.

Published

2023

9. Politics of Constitutional Rightism and Musharraf’s Enlightened Moderation: An Estimate of JUP’s Endeavors on MMA’s Platform

Author

Dr. Mazher Hussain, Dr. Muhammad Mumtaz Ali Khan, and Mr. Imran Alam

Subjects

Constitutional, Rightism, JUP, MMA, Enlightened, Moderation, Islam, BP1-253

Abstract

The Jamm’iyyat Ulama-i-Pakistan (abbreviated hereafter as JUP), in 1990s onwards was headed by dynamic reliogio-political echelon Moulana Shah Ahmad Nurani who believed in ‘constitutional rightism’ and didn’t believe in extra-constitutional maneuvers in order to with the game of power politics. He ran his political affairs under some set principles and abided by with them throughout his political career. His religio-political dynamism during Musharraf regime was the last but ever-glorious episode of his political strife for the enforcement of Islamic socio-economic system to which he termed as Nizam-e-Mustafa. Under his dynamic leadership the religio-political alliance, Mutahidda Majlis-i-Amal, popularly called as the ‘MMA’ showed one of the unprecedented performances the religio-political right ever showed. Up till his death in 2003, The MMA showed no compromise on the set principles, but later things went different. Among other measures of General Musharraf, his policy of so-called moderation of the society on allegedly US command was taken by the religious right of the country as ‘Command Enlightened Moderation’, hence reaction was inevitable. It flocked under the banner of MMA and tried its level best to cope with it. The research in hand highlights this interesting epoch of the history of Pakistan..

Published

2022

10. Plakoglobin and High-Mobility Group Box 1 Mediate Intestinal Epithelial Cell Apoptosis Induced by Clostridioides difficile TcdB

Author

Yingxue Li, Wei Xu, Yutian Ren, Hung-Chi Cheung, Panpan Huang, Guneet Kaur, Chih-Jung Kuo, Sean P. McDonough, Susan L. Fubini, Stephen M. Lipkin, Xin Deng, Yung-Fu Chang, and Linfeng Huang

Subjects

C. difficile, TcdB, apoptosis, JUP, HMGB1, RNAi screen, Microbiology, QR1-502

Abstract

ABSTRACT Clostridioides difficile infection (CDI) is the leading cause of antibiotic-associated intestinal disease, resulting in severe diarrhea and fatal pseudomembranous colitis. TcdB, one of the essential virulence factors secreted by this bacterium, induces host cell apoptosis through a poorly understood mechanism. Here, we performed an RNA interference (RNAi) screen customized to Caco-2 cells, a cell line model of the intestinal epithelium, to discover host factors involved in TcdB-induced apoptosis. We identified plakoglobin, also known as junction plakoglobin (JUP) or γ-catenin, a member of the catenin family, as a novel host factor and a previously known cell death-related chromatin factor, high-mobility group box 1 (HMGB1). Disruption of those host factors by RNAi and CRISPR resulted in resistance of cells to TcdB-mediated and mitochondrion-dependent apoptosis. JUP was redistributed from adherens junctions to the mitochondria and colocalized with the antiapoptotic factor Bcl-XL. JUP proteins could permeabilize the mitochondrial membrane, resulting in the release of cytochrome c. Our results reveal a novel role of JUP in targeting the mitochondria to promote the mitochondrial apoptotic pathway. Treatment with glycyrrhizin, an HMGB1 inhibitor, resulted in significantly increased resistance to TcdB-induced epithelial damage in cultured cells and a mouse ligated colon loop model. These findings demonstrate the critical roles of JUP and HMGB1 in TcdB-induced epithelial cell apoptosis. IMPORTANCE Clostridioides difficile infection (CDI) is the leading cause of hospital-acquired diarrhea. Toxins, especially TcdB, cause epithelial cell apoptosis, but the underlying cell death mechanism is less clear. Through an apoptosis-focused RNAi screen using a bacterium-made small interfering (siRNA) library customized to a human colonic epithelial cell model, we found a novel host factor, plakoglobin (γ-catenin), as a key factor required for cell apoptosis induced by TcdB. Plakoglobin targets and permeabilizes mitochondria after stimulation by TcdB, demonstrating a hitherto underappreciated role of this catenin family member in the apoptosis of intestinal epithelial cells. We also found a previously known cell death-related chromatin factor, HMGB1, and explored the inhibition of HMGB1 for CDI therapy in vivo.

Published

2022

11. Effects of differential distributed-JUP on the malignancy of gastric cancer

Author

Yanlin Chen, Liping Yang, Yilu Qin, Shuiqing Liu, Yina Qiao, Xueying Wan, Huan Zeng, Xiaoli Tang, Manran Liu, and Yixuan Hou

Subjects

JUP, EGFR-AKT-GSK3β signaling, β-catenin stability, Gastric cancer, Medicine (General), R5-920, Science (General), Q1-390

Abstract

Introduction: JUP, a homologue of β-catenin, is a cell-cell junction protein involved in adhesion junction and desmosome composition. JUP may have a controversial role in different malignancies dependence of its competence with or collaboration with β-catenin as a transcription factor. Objective: In this study, we focused on the role of JUP in tumor progress and metastasis of GC. We investigated whether that the function of JUP is related to its cellular location in GC development process from epithelium-like, low malignant GC to advanced EMT-phenotypic GC. Conclusion: Gradual loss of membrane and/or cytoplasm JUP was closely correlated with GC malignancy and poor prognostics. Knockdown of JUP in epithelium-like GC cells causes EMT and promotes GC cell migration and invasion. Ectopic expression of wild JUP in malignant GC cells led to an attenuated malignant phenotype such as reduced cell invasive potential. In mechanism, loss of membrane and/or cytoplasm JUP abolished the restrain of JUP to EGFR at cell membrane and resulted in increased p-AKT levels and AKT/GSK3β/β-catenin signaling activity. In addition, nuclear JUP interacts with nuclear β-catenin and TCF4 and played a synergistic role with β-catenin in promoting TCF4 transcription and its downstream target MMP7 expression to fuel GC cell invasion.

Published

2021

12. Effects of differential distributed-JUP on the malignancy of gastric cancer.

Author

Chen, Yanlin, Yang, Liping, Qin, Yilu, Liu, Shuiqing, Qiao, Yina, Wan, Xueying, Zeng, Huan, Tang, Xiaoli, Liu, Manran, and Hou, Yixuan

Subjects

*STOMACH cancer, *EPIDERMAL growth factor receptors, *TRANSCRIPTION factors, *CELL migration, *FUEL cells

Abstract

JUP, a homologue of β-catenin, is a cell-cell junction protein involved in adhesion junction and desmosome composition. JUP may have a controversial role in different malignancies dependence of its competence with or collaboration with β-catenin as a transcription factor. In this study, we focused on the role of JUP in tumor progress and metastasis of GC. We investigated whether that the function of JUP is related to its cellular location in GC development process from epithelium-like, low malignant GC to advanced EMT-phenotypic GC. Gradual loss of membrane and/or cytoplasm JUP was closely correlated with GC malignancy and poor prognostics. Knockdown of JUP in epithelium-like GC cells causes EMT and promotes GC cell migration and invasion. Ectopic expression of wild JUP in malignant GC cells led to an attenuated malignant phenotype such as reduced cell invasive potential. In mechanism, loss of membrane and/or cytoplasm JUP abolished the restrain of JUP to EGFR at cell membrane and resulted in increased p-AKT levels and AKT/GSK3β/β-catenin signaling activity. In addition, nuclear JUP interacts with nuclear β-catenin and TCF4 and played a synergistic role with β-catenin in promoting TCF4 transcription and its downstream target MMP7 expression to fuel GC cell invasion. [ABSTRACT FROM AUTHOR]

Published

2021

13. Discovery of Digenic Mutation, KCNH2 c.1898A > C and JUP c.916dupA, in a Chinese Family with Long QT Syndrome via Whole-Exome Sequencing.

Author

Yafei Zhai, Jinxin Miao, Ying Peng, Guangming Fang, Chuchu Wang, Yaohe Wang, Xiaoyan Zhao, and Jianzeng Dong

Subjects

LONG QT syndrome, GENETIC mutation, ARRHYTHMIA, HEART diseases, INFLAMMATION

Abstract

Long QT syndrome (LQTS), which is caused by an ion channel-related gene mutation, is a malignant heart disease with a clinical course of a high incidence of ventricular fibrillation and sudden cardiac death in the young. Mutations in KCNH2 (which encodes potassium voltage-gated channel subfamily H member 2) are responsible for LQTS in many patients. Here we report the novel mutation c.1898A > C in KCNH2 in a Chinese family with LQTS through whole-exome sequencing. The c.916dupA mutation in JUP (which encodes junction plakoglobin) is also discovered. Mutations in JUP were found to be associated with arrhythmogenic right ventricular cardiomyopathy. The double mutation in the proband may help explain his severe clinical manifestations, such as sudden cardiac death at an early age. Sequencing for the proband's family members revealed that the KCNH2 mutation descends from his paternal line, while the mutation in JUP came from his maternal line. The data provided in this study may help expand the spectrum of LQTS-related KCNH2 mutations and add support to the genetic diagnosis and counseling of families affected by malignant arrhythmias. [ABSTRACT FROM AUTHOR]

Published

2020

14. Increased expression of plakoglobin is associated with upregulated MAPK and PI3K/AKT signalling pathways in early resectable pancreatic ductal adenocarcinoma.

Author

NWEKE, EKENE, NTWASA, MONDE, BRAND, MARTIN, DEVAR, JOHN, SMITH, MARTIN, and CANDY, GEOFFREY

Subjects

*EPIDERMAL growth factor receptors, *NOTCH signaling pathway, *RAS oncogenes, *ADENOCARCINOMA, *CELL adhesion

Abstract

Pancreatic ductal adenocarcinoma (PDAC) is one of the most lethal cancer types, and it is associated with a 5-year survival rate of <10% due to limited early detection methods and ineffective therapeutic options. Thus, an improved understanding of the mechanisms involved in the early stages of PDAC tumorigenesis is crucial in order to identify potential novel diagnostic and therapeutic targets. The most common signalling aberrations in PDAC occur in the Wnt/Notch signalling pathway, as well as within the epidermal growth factor receptor (EGFR) pathway and its associated ligands, EGF and transforming growth factor-β. In addition, the RAS family of oncogenes, which act downstream of EGFR, are found mutated in most pancreatic cancer samples. Plakoglobin, a component of the EGFR signalling pathway, serves an important role in normal cell adhesion; however, its role in PDAC is largely unknown. The present study used transcriptome sequencing and focussed proteome microarrays to identify dysregulated genes and proteins in PDAC. The presence of upregulated plakoglobin expression levels was identified as a distinguishing feature between the PDAC microenvironment and normal pancreatic tissue. Furthermore, plakoglobin was demonstrated to be associated with the differential upregulation of the PI3K/AKT and MAPK signalling pathways in the tumour microenvironment, which suggested that it may serve an important role in PDAC tumourigenesis. [ABSTRACT FROM AUTHOR]

Published

2020

15. Junction plakoglobin, a potential prognostic marker of oral squamous cell carcinoma, promotes proliferation, migration and invasion.

Author

Fang, Juan, Xiao, Li, Zhang, Qianyu, Peng, Yanshuang, Wang, Zhi, and Liu, Ying

Subjects

*SQUAMOUS cell carcinoma, *ORAL cancer, *BIOMARKERS, *CELL proliferation, *DISEASE progression, *CELL junctions, *CELL migration, *APOPTOSIS, *MOUTH tumors, *CELL physiology, *CELL motility, *RESEARCH funding, *CELL lines

Abstract

Background: Junction plakoglobin (JUP) is an important cell-cell junction protein. Recently, its deregulation has been correlated with the initiation and progression of various malignancies. Our aim was to investigate the expression of JUP in oral squamous cell carcinoma (OSCC) and its correlation with prognosis and to further study the effects of JUP on the proliferation, apoptosis, migration and invasion of OSCC cells.Methods: We detected JUP expression in 273 OSCC specimens using immunohistochemistry. We assessed the correlation of JUP expression with clinicopathologic parameters and patient survival by Cox regression. Then, expression levels of JUP in normal oral keratinocytes (NOKs) and OSCC cell lines were detected by Western blotting and quantitative real-time PCR (qPCR). Next, we used HSC3 cells to study the effect of JUP on tumor cell proliferation, apoptosis, migration, and invasion by using cell counting kit-8, flow cytometry, and transwell assays, respectively.Results: Cox regression showed that high expression of JUP was related to the poor prognosis of OSCC patients. Western blotting and qPCR assays showed that the expression level of JUP in OSCC cell lines was higher than that in NOKs. Overexpression of JUP promoted the proliferation, metastasis, and invasion of HSC3 cells and inhibited apoptosis, while the opposite was observed after JUP knockdown.Conclusion: This study initially revealed that JUP was overexpressed in OSCC, and that JUP promoted the proliferation, migration, and invasion of OSCC cells and inhibited apoptosis. Moreover, high expression of JUP could be used as a potential prognostic marker of OSCC. [ABSTRACT FROM AUTHOR]

Published

2020

16. Human Genetics of Cardiomyopathies

Author

Vermeer, Alexa M. C., Wilde, Arthur A. M., Christiaans, Imke, Rickert-Sperling, Silke, editor, Kelly, Robert G., editor, and Driscoll, David J., editor

Published

2016

17. Periodicities and Plasma Density Structure of Jupiter’s Dawnside Magnetosphere

Author

2463315, Ma, Xuanye, Schok, A.A., Delamere, P.A., Mino, B., Damiano, P.A., Zhang, B., Sciola, A., 2463315, Ma, Xuanye, Schok, A.A., Delamere, P.A., Mino, B., Damiano, P.A., Zhang, B., and Sciola, A.

Abstract

The ability to quantify variations in magnetic field topology and density within Jupiter’s magnetosphere is an important step in understanding the overall structure and dynamics. The Juno spacecraft has provided a rich data set in the dawnside magnetosphere. The recent Grid Agnostic MHD for Extended Research Applications (GAMERA) global simulation study by Zhang et al. (2021) showed a highly structured plasmadisc with closed magnetic field lines mapping between the outer dawn-tail flank and the high latitude polar region. To test these model predictions, we examined Juno’s magnetic field data and electron/energetic particle data to categorize portions of orbits 1-15 into one of three regions based on plasma confinement: the flux pileup region, the intermediate region, and the plasmadisc region. For each region we examined periodicities from magnetic field fluctuations and particle density fluctuations on the 1-10 hours time scale. Periodicities on this time scale could relate to internal (e.g. plasmadisc structure) or external processes (e.g. Kelvin-Helmholtz vortices). Similar analysis was performed on the GAMERA simulation with the data split into two regions, an outer (150 > R > 60) region and an inner (R < 60) region. Finally, using published density moments from Huscher et al. (2021) we compared the relative density variations of the Juno moments and the GAMERA simulation to further understand the overall structure and dynamics of the plasmadisc. The agreement between data and simulation supports the existence of such a highly structured plasmadisc.

Published

2023

18. Entre la proscripción y la construcción de una identidad: el peronismo universitario a inicios de los sesenta

Author

Julián Andrés Dércoli

Subjects

Peronismo, Universidad, 4161, JUP, Identidad, Communication. Mass media, P87-96

Abstract

La relación entre el peronismo y la universidad fue estudiada a partir de un conjunto de prejuicios que afirmaban su total antagonismo. Con el fin de poner en tela de juicio a los mismos, analizaremos el discurso sobre la universidad de la revista 4161; la misma se autodenominada órgano de la Juventud Universitaria Peronista y sus dos números aparecieron entre 1963 y 1964. A nuestro juicio, la relevancia de la revista radica en que fue una aparición temprana de un conjunto de universitarios dados a la tarea de construir una identidad universitaria peronista. La idea que guía nuestra pesquisa es que la revista ensaya un sincretismo que, partiendo del peronismo, busca converger con diversas corrientes como el reformismo o el marxismo. Este proceso es de vital importancia para dar cuenta de la posterior masividad que adquiere el peronismo en las universidades en la década del ´70 y, hacia el ´73 y cómo aquellas concepciones influyeron en los proyectos de reforma institucional de las universidades argentinas. Por este sendero, podemos pensar que 4161 fue el inicio de una cultura política universitaria del peronismo.

Published

2019

19. Identification of testicular cancer driver genes by a cross‐species comparative oncology approach.

Author

Sanchez, A., Xu, L., Pierce, J. L., Lafin, J. T., Abe, D., Bagrodia, A., Frazier, A. L., and Amatruda, J. F.

Subjects

*TESTIS tumors, *TESTICULAR cancer, *LABORATORY zebrafish, *GERM cell tumors, *CANCER genes, *TERATOCARCINOMA, *GENE expression profiling, *GERM cells

Abstract

Background: Germ cell tumors arise in the testis, ovary, or extragonadal locations and have a wide range of histopathological and clinical presentations. The relative lack of animal models of germ cell tumors has impeded functional assessment of candidate driver genes. Previously, we described the development of testicular germ cell tumors in zebrafish carrying a mutation in bmpr1bb, a BMP family receptor, and demonstrated that human germ cell tumors have defects in BMP signaling. Objective: To further credential the zebrafish model for studies of human germ cell tumor, and to elucidate conserved genetic programs underlying the development of germ cell tumor. Materials and Methods: We used genetic techniques to ablate the germ cell lineage in developing fish and tested tumors for loss‐of‐heterozygosity of the wild‐type allele of bmpr1bb. We performed comparative gene expression profiling of zebrafish and human germ cell tumors and carried out functional studies of selected genes. Results: Ablation of germ cells completely prevents testis tumor formation in the fish, definitively establishing the germ cell origin of the tumors. Germ cell tumors in bmpr1bb heterozygous mutants retain the wild‐type allele, indicating haploinsufficiency of bmpr1bb as the mechanism of tumor formation. Comparison of RNA‐Seq and microarray data from human and zebrafish germ cell tumors revealed a unique overlapping signature shared by the zebrafish tumors with human seminomas, yolk sac tumors, and embryonal carcinomas. The most highly conserved gene set in this cross‐species analysis included potential driver genes such as JUP, which we show to be essential for germ cell tumor cell growth. Conclusion: Our findings highlight the value of cross‐species comparative oncology for the identification of candidate human cancer genes. [ABSTRACT FROM AUTHOR]

Published

2019

20. Entre la proscripción y la construcción de una identidad: el peronismo universitario a inicios de los sesenta.

Author

Andrés Dércoli, Julián

Subjects

POLITICAL culture, PERONISM, PRESS, COLLEGE students

Abstract

Copyright of Question (1669-6581) is the property of Universidad Nacional de La Plata and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2019

21. Downregulation of γ-Catenin by miR-195-5p Inhibits Colon Cancer Progression, Regulating Desmosome Function.

Author

Piccinno E, Scalavino V, Labarile N, Bianco G, Savino MT, Armentano R, Giannelli G, and Serino G

Subjects

Humans, Desmosomes genetics, gamma Catenin, Down-Regulation genetics, Colonic Neoplasms genetics, MicroRNAs genetics

Abstract

Desmosomes are essential structures for ensuring tissue functions, and their deregulation is involved in the development of colorectal cancer (CRC). JUP (γ-catenin) is a desmosome adhesion component that also acts as a signaling hub, suggesting its potential involvement in CRC progression. In this context, we recently demonstrated that miR-195-5p regulated JUP and desmosome cadherins expression. In addition, miR-195-5p gain of function indirectly modulated the expression of key effectors of the Wnt pathway involved in JUP-dependent signaling. Here, our purpose was to demonstrate the aberrant expression of miR-195-5p and JUP in CRC patients and to functionally characterize the role of miR-195-5p in the regulation of desmosome function. First, we showed that miR-195-5p was downregulated in CRC tumors compared to adjacent normal tissue. Then, we demonstrated that JUP expression was significantly increased in CRC tissues compared to adjacent normal tissues. The effects of miR-195-5p on CRC progression were assessed using in vitro transient transfection experiments and in vivo miRNA administration. Increased miR-195-5p in colonic epithelial cells strongly inhibits cell proliferation, viability, and invasion via JUP. In vivo gain of function of miR-195-5p reduced the numbers and sizes of tumors and significantly ameliorated the histopathological changes typical of CRC. In conclusion, our findings indicate a potential pharmacological target based on miR-195-5p replacement as a new therapeutic approach in CRC.

Published

2023

22. Effects of differential distributed-JUP on the malignancy of gastric cancer

Author

Yina Qiao, Liping Yang, Yanlin Chen, Manran Liu, Xiaoli Tang, Xueying Wan, Yixuan Hou, Shuiqing Liu, Huan Zeng, and Yilu Qin

Subjects

0301 basic medicine, Cell, Article, 03 medical and health sciences, 0302 clinical medicine, medicine, JUP, lcsh:Science (General), Transcription factor, Protein kinase B, ComputingMethodologies_COMPUTERGRAPHICS, lcsh:R5-920, Gene knockdown, Multidisciplinary, Chemistry, Cell migration, TCF4, Cell biology, β-catenin stability, 030104 developmental biology, medicine.anatomical_structure, Cytoplasm, 030220 oncology & carcinogenesis, Ectopic expression, Gastric cancer, lcsh:Medicine (General), EGFR-AKT-GSK3β signaling, lcsh:Q1-390

Abstract

Graphical abstract, JUP, a homologue of β-catenin, is a cell-cell junction protein involved in adhesion junction and desmosome composition. JUP may have a controversial role in different malignancies dependence of its competence with or collaboration with β-catenin as a transcription factor. In this study, we reveal that the function of JUP is related to its cellular location in GC development process from epithelium-like, low malignant GC to advanced EMT-phenotypic GC. Gradual loss of membrane and/or cytoplasm JUP is closely correlated with GC malignancy and poor prognostics. Knockdown of JUP in epithelium-like GC cells causes EMT and promotes GC cell migration and invasion. Ectopic expression of wild JUP in malignant GC cells leads to an attenuated malignant phenotype such as reduced cell invasive potential. In mechanism, loss of membrane and/or cytoplasm JUP abolishes the restrain of JUP to EGFR at cell membrane and results in increased p-AKT levels and AKT/GSK3β/β-catenin signaling activity. In addition, nuclear JUP interacts with nuclear β-catenin and TCF4 and plays a synergistic role with β-catenin in promoting TCF4 transcription and its downstream target MMP7 expression to fuel GC cell invasion.

Published

2021

23. β-catenin coordinates with Jup and the TCF1/GATA6 axis to regulate human embryonic stem cell fate.

Author

Sun, Hongwei, Wang, Xiaohu, Liu, Kuisheng, Guo, Mengmeng, Zhang, Yan, Ying, Qi-Long, and Ye, Shoudong

Subjects

*CATENINS, *GATA proteins, *EMBRYONIC stem cells, *CELLULAR control mechanisms, *NEURAL circuitry

Abstract

β-catenin-mediated signaling has been extensively studied in regard to its role in the regulation of human embryonic stem cells (hESCs). However, the results are controversial and the mechanism by which β-catenin regulates the hESC fate remains unclear. Here, we report that β-catenin and γ-catenin are functionally redundant in mediating hESC adhesion and are required for embryoid body formation, but both genes are dispensable for hESC maintenance, as the undifferentiated state of β-catenin and γ-catenin double deficient hESCs can be maintained. Overexpression of β-catenin induces rapid hESC differentiation. Functional assays revealed that TCF1 plays a crucial role in hESC differentiation mediated by β-catenin. Forced expression of TCF1 , but not other LEF1/TCF family members, resulted in hESC differentiation towards the definitive endoderm. Conversely, knockdown of TCF1 or inhibition of the interaction between TCF1 and β-catenin delayed hESC exit from pluripotency. Furthermore, we demonstrated that GATA6 plays a predominant role in TCF1-mediated hESC differentiation. Knockdown of GATA6 completely eliminated the effect of TCF1, while forced expression of GATA6 induced hESC differentiation. Our data thus reveal more detailed mechanisms for β-catenin in regulating hESC fate decisions and will expand our understanding of the self-renewal and differentiation circuitry in hESCs. [ABSTRACT FROM AUTHOR]

Published

2017

24. Discovery of Digenic Mutation, KCNH2 c.1898A >C and JUP c.916dupA, in a Chinese Family with Long QT Syndrome via Whole-Exome Sequencing

Author

Guangming Fang, Ying Peng, Xiaoyan Zhao, Wang Chuchu, Yafei Zhai, Jinxin Miao, Yaohe Wang, and Jianzeng Dong

Subjects

0301 basic medicine, Genetics, congenital, hereditary, and neonatal diseases and abnormalities, digenic mutation, lcsh:Diseases of the circulatory (Cardiovascular) system, business.industry, Long QT syndrome, General Medicine, 030204 cardiovascular system & hematology, medicine.disease, long qt syndrome (lqts), 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, lcsh:RC666-701, Mutation (genetic algorithm), medicine, kcnh2, jup, cardiovascular diseases, Chinese family, business, Exome sequencing

Abstract

Long QT syndrome (LQTS), which is caused by an ion channel–related gene mutation, is a malignant heart disease with a clinical course of a high incidence of ventricular fibrillation and sudden cardiac death in the young. Mutations in KCNH2 (which encodes potassium voltage-gated channel subfamily H member 2) are responsible for LQTS in many patients. Here we report the novel mutation c.1898A>C in KCNH2 in a Chinese family with LQTS through whole-exome sequencing. The c.916dupA mutation in JUP (which encodes junction plakoglobin) is also discovered. Mutations in JUP were found to be associated with arrhythmogenic right ventricular cardiomyopathy. The double mutation in the proband may help explain his severe clinical manifestations, such as sudden cardiac death at an early age. Sequencing for the proband’s family members revealed that the KCNH2 mutation descends from his paternal line, while the mutation in JUP came from his maternal line. The data provided in this study may help expand the spectrum of LQTS-related KCNH2 mutations and add support to the genetic diagnosis and counseling of families affected by malignant arrhythmias.

Published

2020

25. Arrhythmogenic right ventricular cardiomyopathy in patients with biallelic JUP-associated skin fragility.

Author

Vahidnezhad, Hassan, Youssefian, Leila, Faghankhani, Masoomeh, Mozafari, Nikoo, Saeidian, Amir Hossein, Niaziorimi, Fatemeh, Abdollahimajd, Fahimeh, Sotoudeh, Soheila, Rajabi, Fateme, Mirsafaei, Liaosadat, Sani, Zahra Alizadeh, Liu, Lu, Guy, Alyson, Zeinali, Sirous, Kariminejad, Ariana, Ho, Reginald T, McGrath, John A, Uitto, Jouni, Vahidnezhad, Hassan, Youssefian, Leila, Faghankhani, Masoomeh, Mozafari, Nikoo, Saeidian, Amir Hossein, Niaziorimi, Fatemeh, Abdollahimajd, Fahimeh, Sotoudeh, Soheila, Rajabi, Fateme, Mirsafaei, Liaosadat, Sani, Zahra Alizadeh, Liu, Lu, Guy, Alyson, Zeinali, Sirous, Kariminejad, Ariana, Ho, Reginald T, McGrath, John A, and Uitto, Jouni

Abstract

Arrhythmogenic right ventricular cardiomyopathy (ARVC), with skin manifestations, has been associated with mutations in JUP encoding plakoglobin. Genotype-phenotype correlations regarding the penetrance of cardiac involvement, and age of onset have not been well established. We examined a cohort of 362 families with skin fragility to screen for genetic mutations with next-generation sequencing-based methods. In two unrelated families, a previously unreported biallelic mutation, JUP: c.201delC; p.Ser68Alafs*92, was disclosed. The consequences of this mutation were determined by expression profiling both at tissue and ultrastructural levels, and the patients were evaluated by cardiac and cutaneous work-up. Whole-transcriptome sequencing by RNA-Seq revealed JUP as the most down-regulated gene among 21 skin fragility-associated genes. Immunofluorescence showed the lack of plakoglobin in the epidermis. Two probands, 2.5 and 22-year-old, with the same homozygous mutation, allowed us to study the cross-sectional progression of cardiac involvements in relation to age. The older patient had anterior T wave inversions, prolonged terminal activation duration (TAD), and RV enlargement by echocardiogram, and together with JUP mutation met definite ARVC diagnosis. The younger patient had no evidence of cardiac disease, but met possible ARVC diagnosis with one major criterion (the JUP mutation). In conclusion, we identified the same biallelic homozygous JUP mutation in two unrelated families with skin fragility, but cardiac findings highlighted age-dependent penetrance of ARVC. Thus, young, phenotypically normal patients with biallelic JUP mutations should be monitored for development of ARVC.

Published

2020

26. Visualização de Tráfego Portuário em Tempo Real com Integração da JUP e do AIS.

Author

Santos, Jorge, Dias, Leonel, and Oliveira, Lino

Abstract

Copyright of CISTI (Iberian Conference on Information Systems & Technologies / Conferência Ibérica de Sistemas e Tecnologias de Informação) Proceedings is the property of Conferencia Iberica de Sistemas Tecnologia de Informacao and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2016

27. Novel founder mutation in French-Canadian families with Naxos disease.

Author

Marino, T. Cruz, Maranda, B., Leblanc, J., Pratte, A., Barabas, M., Dupéré, A., and Lévesque, S.

Subjects

*EXONS (Genetics)

Abstract

The article describes the cases of French-Canadian families with Naxos disease (NXD) linked to arrhythmogenic right ventricular cardiomyopathy (ARVC), palmoplantar keratoderma (PPK) and peculiar woolly hair. Other characteristics of the family members include homozygous mutation in the exon 5 of JUP gene, typical cutaneous and hair, and whites of French-Canadian descent. It is recommended that further studies are made to ascertain the cause of the genetic mutation in the heterozygous state.

Published

2017

28. A biological and pharmacological investigation of the unfolded protein response in models of breast cancer

Author

Leuzzi, Brian, Samali, Afshin, Gorman, Adrienne, and Horizon 2020

Subjects

Drug discovery, MYC, IRE1, Epithelial-mesenchymal transition, Breast cancer, IRE1 inhibitor, Unfolded Protein Response, KRAS, RIDD, JUP, Science and Engineering, Mesenchymal-epithelial transition, Natural Science, Oncogene

Abstract

Breast cancer is the most common malignancy in women worldwide. At the molecular level, breast cancer is a heterogeneous disease. For example, the claudin low subtype of breast cancer is characterised by epithelial-mesenchymal transition (EMT). EMT is a process by which epithelial cells lose cell-cell adhesion and their cell polarity, and gain migratory and invasive properties to become mesenchymal cells. The claudin-low subtype is also driven by specific oncogenes, such as MYC or KRAS. Both EMT and oncogene-driven tumorigenesis have been associated with the unfolded protein response (UPR). The UPR is a cellular stress response pathway which activates an adaptive mechanisms to overcome stress and restore endoplasmic reticulum (ER) homeostasis. The UPR comprises three signalling pathways which are activated by three transmembrane sensors of the ER: inositol requiring enzyme 1 (IRE1), protein kinase RNA‐activated (PKR)‐like ER kinase (PERK) and activating transcription factor 6 (ATF6). In breast cancer, IRE1, PERK and ATF6 contribute to cancer cell proliferation, drug resistance and EMT. Chapter III shows that the pharmacological block of IRE1 has no effect on EMT in breast cancer. The knockout of XBP1 was also not sufficient to induce an epithelial phenotype in the MDA-MB-231 claudin low breast cancer cell line. However, Chapter IV shows that plakoglobin, a component of the cell cell contacts, was down regulated by IRE1 in MDA-MB-231 cell line thus affecting cell migration and adhesion in an EMT independent manner. In Chapter V, the relationship between UPR and oncogenes in the regulation of apoptosis was also investigated by overexpressing the oncogenes MYC and KRASG12V in the MCF10A non-tumorigenic mammary epithelial cell line. We observed that the UPR was not activated by MYC and KRASG12V although these oncoproteins decreased cell viability and induced the activation of caspase-3. Finally, in Chapter VI, a cell free drug screening for IRE1 identified compound NUIG10 as a promising inhibitor of IRE1. Altogether, this thesis has evaluated and broadened our knowledge of the role that the UPR and more specifically IRE1 plays in breast cancer. 2024-12-15

Published

2020

29. Plakoglobin and High-Mobility Group Box 1 Mediate Intestinal Epithelial Cell Apoptosis Induced by Clostridioides difficile TcdB.

Author

Li Y, Xu W, Ren Y, Cheung HC, Huang P, Kaur G, Kuo CJ, McDonough SP, Fubini SL, Lipkin SM, Deng X, Chang YF, and Huang L

Subjects

Animals, Humans, Mice, Anti-Bacterial Agents pharmacology, Apoptosis, Bacterial Proteins metabolism, Caco-2 Cells, Chromatin, Clostridioides, Cytochromes c genetics, Diarrhea, Enterotoxins, Epithelial Cells metabolism, Glycyrrhizic Acid pharmacology, RNA, Small Interfering, Virulence Factors, Bacterial Toxins metabolism, Clostridioides difficile, Clostridium Infections microbiology, gamma Catenin genetics, HMGB1 Protein genetics

Abstract

Clostridioides difficile infection (CDI) is the leading cause of antibiotic-associated intestinal disease, resulting in severe diarrhea and fatal pseudomembranous colitis. TcdB, one of the essential virulence factors secreted by this bacterium, induces host cell apoptosis through a poorly understood mechanism. Here, we performed an RNA interference (RNAi) screen customized to Caco-2 cells, a cell line model of the intestinal epithelium, to discover host factors involved in TcdB-induced apoptosis. We identified plakoglobin, also known as junction plakoglobin (JUP) or γ-catenin, a member of the catenin family, as a novel host factor and a previously known cell death-related chromatin factor, high-mobility group box 1 (HMGB1). Disruption of those host factors by RNAi and CRISPR resulted in resistance of cells to TcdB-mediated and mitochondrion-dependent apoptosis. JUP was redistributed from adherens junctions to the mitochondria and colocalized with the antiapoptotic factor Bcl-X L . JUP proteins could permeabilize the mitochondrial membrane, resulting in the release of cytochrome c . Our results reveal a novel role of JUP in targeting the mitochondria to promote the mitochondrial apoptotic pathway. Treatment with glycyrrhizin, an HMGB1 inhibitor, resulted in significantly increased resistance to TcdB-induced epithelial damage in cultured cells and a mouse ligated colon loop model. These findings demonstrate the critical roles of JUP and HMGB1 in TcdB-induced epithelial cell apoptosis. IMPORTANCE Clostridioides difficile infection (CDI) is the leading cause of hospital-acquired diarrhea. Toxins, especially TcdB, cause epithelial cell apoptosis, but the underlying cell death mechanism is less clear. Through an apoptosis-focused RNAi screen using a bacterium-made small interfering (siRNA) library customized to a human colonic epithelial cell model, we found a novel host factor, plakoglobin (γ-catenin), as a key factor required for cell apoptosis induced by TcdB. Plakoglobin targets and permeabilizes mitochondria after stimulation by TcdB, demonstrating a hitherto underappreciated role of this catenin family member in the apoptosis of intestinal epithelial cells. We also found a previously known cell death-related chromatin factor, HMGB1, and explored the inhibition of HMGB1 for CDI therapy in vivo .

Published

2022

30. ICAT promotes colorectal cancer metastasis via binding to JUP and activating the NF-κB signaling pathway.

Author

Wang Z, Hu J, Chen J, Zhang J, Li W, Tian Y, Liu H, and Yang X

Subjects

Adaptor Proteins, Signal Transducing, Biomarkers, Cell Line, Tumor, Cell Proliferation, Gene Expression Regulation, Neoplastic, Humans, NF-kappa B metabolism, Neoplasm Metastasis, TCF Transcription Factors metabolism, Wnt Signaling Pathway, gamma Catenin metabolism, Colorectal Neoplasms pathology, beta Catenin genetics, beta Catenin metabolism

Abstract

Background: The inhibitor of β-catenin and T-cell factor (ICAT) is a direct negative regulator of the canonical Wnt signaling pathway, which is an attractive therapeutic target for colorectal cancer (CRC). Accumulating evidence suggests that ICAT interacts with other proteins to exert additional functions, which are not yet fully elucidated., Methods: The overexpression of ICAT of CRC cells was conducted by lentivirus infection and plasmids transfection and verified by quantitative real-time reverse transcription-polymerase chain reaction (real-time RT-PCR) and Western blotting. The effect of ICAT on the mobility of CRC cells was assessed by wound healing assay and transwell assay in vitro and lung metastasis in vivo. New candidate ICAT-interacting proteins were explored and verified using the STRING database, silver staining, co-immunoprecipitation mass spectrometry analysis (Co-IP/MS), and immunofluorescence (IF) staining analysis., Result: Inhibitor of β-catenin and T-cell factor overexpression promoted in vitro cell migration and invasion and tumor metastasis in vivo. Co-IP/MS analysis and STRING database analyses revealed that junction plakoglobin (JUP), a homolog of β-catenin, was involved in a novel protein interaction with ICAT. Furthermore, JUP downregulation impaired ICAT-induced migration and invasion of CRC cells. In addition, ICAT overexpression activated the NF-κB signaling pathway, which led to enhanced CRC cell migration and invasion., Conclusion: Inhibitor of β-catenin and T-cell factor promoted CRC cell migration and invasion by interacting with JUP and the NF-κB signaling pathway. Thus, ICAT could be considered a protein diagnostic biomarker for predicting the metastatic ability of CRC., (© 2022 The Authors. Journal of Clinical Laboratory Analysis published by Wiley Periodicals LLC.)

Published

2022

31. Investigating the role of IRE1α RNase activity in breast cancer

Author

McGrath, Eoghan Patrick, Samali, Afshin, Irish Research Council, and Horizon 2020

Subjects

Unfolded protein response, Breast cancer, therapy resistance, Unfolded Protein Response in Breast Cancer, JUP, IRE1, Cell Migration, ER stress, Natural Sciences, Biochemistry

Abstract

Metastatic, drug resistant disease poses the greatest threat to the survival of breast cancer patients. Thus, elucidating and targeting mechanisms which govern this phenotype is a primary goal of the breast cancer field. Breast cancers manipulate cellular stress pathways to gain a survival advantage and fuel their growth. The unfolded protein response (UPR) is a major cell stress pathway responsible for the genesis and growth of many breast cancers. The most evolutionarily conserved transducer of the unfolded protein response is a protein called inositol-requiring enzyme 1 (IRE1), which is an important player in both luminal and basal-like breast cancers. Pro-tumour roles of IRE1 are mediated through its endoribonuclease (RNase) domain which has two functions, X-box binding protein 1 (XBP1) splicing and regulated IRE1-dependent decay (RIDD). In this thesis we have determined that the IRE1 RNase is particularly active in triple negative breast cancer (TNBC), a subtype with a poor prognosis and limited treatment options. We have discovered novel targets of the IRE1 RNase domain, namely C-X-C motif chemokine ligand 1 (CXCL1) which we have shown to govern a drug-resistant and stem cell-like phenotype. We also identified the first RIDD substrate in breast cancer (junction plakoglobin (JUP)) and found that its degradation by IRE1 may promote migration of TNBC cells. We employed MKC8866, a small molecule with clinical potential, to show that both of these processes can be blocked. This work highlights the promise of targeting IRE1 in the clinic to prolong and improve the lives of breast cancer patients. 2022-12-17

Published

2018

32. Importância das características dos Sistemas Comunitários Portuários (PCS – Port Community Systems) no desempenho dos portos

Author

Salvador, Antonia de Sena Pedro and Caldeirinha, Vítor

Subjects

Sistemas Portuários Comunitários, PCS, Características, Performance, characteristics, Port Community System, JUP, Desempenho

Abstract

Dissertaça o apresentada para cumprimento dos requisitos necessa rios a obtença o do grau de Mestre em Ciências Empresariais- Ramo Gestão Logística Este estudo tem como propósito avaliar a importância das suas características dos sistemas comunitários portuários (PCS – Port Community Systems) para o desempenho dos portos e das economias, ou seja, determinar em que medida as características específicas dos sistemas comunitários portuários influenciam o seu desempenho. Em termos concretos, visa determinar em que medida as características específicas da Janela Única Portuária portuguesa influenciam o seu desempenho, com impacto no desempenho dos portos portugueses. Foi utilizada a metodologia de análise estatística com o SPSS, correlação entre variáveis e do caso de estudo. A amostra inclui 15 observações, recolhidas em outubro de 2017, em Portugal, com recurso a inquérito sobre a importância dos fatores (escala Likert5), para o caso geral dos PCS e para o caso de estudo da JUP. Conclui-se que as variáveis obtidas a partir da literatura definem as características importantes dos sistemas comunitários portuários e das suas medidas de desempenho e que as características dos sistemas comunitários portuários determinam o seu desempenho. The purpose of this study is to evaluate the importance of Port Community Systems (PCS) and their characteristics for the performance of ports and economies, that means, determine in what measure the specific characteristics of Port Community Systems determine their performance. In concrete terms, aims to determine in what measure the specific characteristics of Port Single Window Portuguese influence their performance, with an impact on the performance of Portuguese ports. A methodology of statistical analysis was used with the SPSS, correlation between variables and of the case study. The sample includes 15 observations, collected in October of 2017, in Portugal, with recourse to a survey about the importance of the factors (Likert5 scale) for the general case of PCS and for the JUP case study. Concludes that the variables obtained from the literature define the important characteristics of Port Community Systems and its performance measures, and that the characteristics of the Port Community Systems determine their performance.

Published

2017

33. Between proscription and the building of an identity: peronism in university in the early sixties

Author

Julián Andrés Dércoli

Subjects

Universidad, Peronismo, Political science, JUP, Comunicación Social, General Agricultural and Biological Sciences, Humanities, Identidad, lcsh:P87-96, lcsh:Communication. Mass media

Abstract

La relación entre el peronismo y la universidad fue estudiada a partir de un conjunto de prejuicios que afirmaban su total antagonismo. Con el fin de poner en tela de juicio a los mismos, analizaremos el discurso sobre la universidad de la revista 4161; la misma se autodenominada órgano de la Juventud Universitaria Peronista y sus dos números aparecieron entre 1963 y 1964. A nuestro juicio, la relevancia de la revista radica en que fueuna aparición temprana de un conjunto de universitarios dados a la tarea de construir una identidad universitaria peronista. La idea que guía nuestra pesquisaes que la revista ensaya un sincretismo que, partiendo del peronismo, busca converger con diversas corrientes como el reformismo o el marxismo. Este proceso es de vital importancia para dar cuenta de la posterior masividad que adquiere el peronismo en las universidades en la década del 70 y, hacia 1973 y cómo aquellas concepciones influyeron en los proyectos de reforma institucional de las universidades argentinas. Por este sendero, podemos pensar que 4161 fue el inicio de una cultura política universitaria del peronismo., The relationship between Peronism and University has been studied on the basis of the prejudice that upheldtheir mutual antagonism. With de purpose of challenging this prejudice, we shall analyse the discourse about university in 4161 magazine. 4161 designated itself as the news media of the University Peronist Youth (JUP for its acronym in Spanish), andits two issues were released between 1963 and 1964. From our point of view, the relevance of this magazine is based on the fact that it meant the early appearance of a group of university students aiming at building a peronist university identity. The leading idea of our research is that the magazine attempts at a syncretism that, based on peronism, looks at converging with other identities, such as reformism or marxism. This process is crucial to understand the subsequent popularity that peronism gains inthe university world in the seventies and towards 1973, as well as its influence in the projects of institutional reform during this period. Along the same lines, we might affirm that 4161 meant the beginning of the university political culture of peronism., Facultad de Periodismo y Comunicación Social

Published

2019

34. JUP/plakoglobin is regulated by salt-inducible kinase 2, and is required for insulin-induced signalling and glucose uptake in adipocytes.

Author

Negoita, Florentina, Vavakova, Magdalena, Säll, Johanna, Laurencikiene, Jurga, and Göransson, Olga

Subjects

*INSULIN regulation, *ADIPOSE tissues, *ADHERENS junctions, *CELL communication, *GLUCOSE, *MUSCLE cells, *INSULIN, *INSULIN receptors

Abstract

Salt-inducible kinase 2 (SIK2) is abundant in adipocytes, but downregulated in adipose tissue from individuals with obesity and insulin resistance. Moreover, SIK isoforms are required for normal insulin signalling and glucose uptake in adipocytes, but the underlying molecular mechanisms are currently not known. The adherens junction protein JUP, also termed plakoglobin or γ-catenin, has recently been reported to promote insulin signalling in muscle cells. The objective of this study was to analyse if JUP is required for insulin signalling in adipocytes and the underlying molecular mechanisms of this regulation. Co-expression of SIK2 and JUP mRNA levels in adipose tissue from a human cohort was analysed. siRNA silencing and/or pharmacological inhibition of SIK2, JUP, class IIa HDACs and CRTC2 was employed in 3T3-L1- and primary rat adipocytes. JUP protein expression was analysed by western blot and mRNA levels by qPCR. Insulin signalling was evaluated by western blot as levels of phosphorylated PKB/Akt and AS160, and by monitoring the uptake of 3H-2-deoxyglucose. mRNA expression of SIK2 correlated with that of JUP in human adipose tissue. SIK2 inhibition or silencing resulted in downregulation of JUP mRNA and protein expression in 3T3-L1- and in primary rat adipocytes. Moreover, JUP silencing reduced the expression of PKB and the downstream substrate AS160, and consequently attenuated activity in the insulin signalling pathway, including insulin-induced glucose uptake. The known SIK2 substrates CRTC2 and class IIa HDACs were found to play a role in the SIK-mediated regulation of JUP expression. These findings identify JUP as a novel player in the regulation of insulin sensitivity in adipocytes, and suggest that changes in JUP expression could contribute to the effect of SIK2 on insulin signalling in these cells. • JUP/plakoglobin is decreased after SIK2 inhibition in adipocytes. • JUP silencing results in diminished insulin signalling and glucose uptake. • CRTCs are likely involved in SIK2-mediated JUP downregulation. • JUP is a novel molecular target downstream SIK2 in adipocytes. [ABSTRACT FROM AUTHOR]

Published

2020

35. The Juventud Universitaria Peronista in the Memories of the Reformist and Marxist student militancy of UBA, 1973-1976

Author

Millán, Mariano Ignacio

Subjects

Izquierda Universitaria, CIENCIAS SOCIALES, purl.org/becyt/ford/5 [https], Otras Sociología, Movimiento Estudiantil, JUP, Reformismo Universitario, purl.org/becyt/ford/5.4 [https], Sociología

Abstract

Recorremos aquí las memorias de la militancia estudiantil reformista y marxista de la UBA acerca de la Juventud Universitaria Peronista entre 1973 y 1976. Analizamos 15 testimonios orales de activistas de diversas organizaciones, en los que encontramos cuatro tópicos centrales: la JUP era una fuerza de formación reciente, con escasa trayectoria y conocimiento del medio universitario; esta agrupación carecía de un proyecto universitario consistente; tenía relaciones conflictivas con sus aliados y, con el pasaje de Montoneros a la clandestinidad, se agudizaron las tensiones con las otras agrupaciones de la UBA. In this paper we visit the memories of the reformist and marxist student activism of the UBA about the Juventud Universitaria Peronista between 1973 and 1976. We analyzed 15 oral testimonies of activists from various organizations and found four main topics: the JUP was a organization of recent formation, with little experience and knowledge of the university environment; this group lacked a consistent university project; the JUP had conflictive relations with its allies and, with the passage of Montoneros to clandestinity, the tensions with the other militant groupings of the UBA were exacerbated. Fil: Millán, Mariano Ignacio. Consejo Nacional de Investigaciones Científicas y Técnicas. Oficina de Coordinación Administrativa Saavedra 15. Instituto de Historia Argentina y Americana "Dr. Emilio Ravignani". Universidad de Buenos Aires. Facultad de Filosofía y Letras. Instituto de Historia Argentina y Americana "Dr. Emilio Ravignani"; Argentina

Published

2016

36. Effects of differential distributed-JUP on the malignancy of gastric cancer.

Author

Chen Y, Yang L, Qin Y, Liu S, Qiao Y, Wan X, Zeng H, Tang X, Liu M, and Hou Y

Abstract

JUP, a homologue of β-catenin, is a cell-cell junction protein involved in adhesion junction and desmosome composition. JUP may have a controversial role in different malignancies dependence of its competence with or collaboration with β-catenin as a transcription factor. In this study, we reveal that the function of JUP is related to its cellular location in GC development process from epithelium-like, low malignant GC to advanced EMT-phenotypic GC. Gradual loss of membrane and/or cytoplasm JUP is closely correlated with GC malignancy and poor prognostics. Knockdown of JUP in epithelium-like GC cells causes EMT and promotes GC cell migration and invasion. Ectopic expression of wild JUP in malignant GC cells leads to an attenuated malignant phenotype such as reduced cell invasive potential. In mechanism, loss of membrane and/or cytoplasm JUP abolishes the restrain of JUP to EGFR at cell membrane and results in increased p-AKT levels and AKT/GSK3β/β-catenin signaling activity. In addition, nuclear JUP interacts with nuclear β-catenin and TCF4 and plays a synergistic role with β-catenin in promoting TCF4 transcription and its downstream target MMP7 expression to fuel GC cell invasion., Competing Interests: The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (© 2020 The Authors. Published by Elsevier B.V. on behalf of Cairo University.)

Published

2020

37. A Genetic Variants Database for Arrhythmogenic Right Ventricular Dysplasia/Cardiomyopathy

Author

Hennie Bikker, J. Peter van Tintelen, Paul A. van der Zwaag, Robert M.W. Hofstra, Roselie Jongbloed, Jan D. H. Jongbloed, Maarten P. van den Berg, Jasper J. van der Smagt, Cardiovascular Centre (CVC), Amsterdam Cardiovascular Sciences, Amsterdam Gastroenterology Endocrinology Metabolism, Other Research, Human Genetics, and Other departments

Subjects

medicine.medical_specialty, Cardiomyopathy, EARLY-ONSET, PLAKOGLOBIN NAXOS-DISEASE, RECESSIVE MUTATION, LONG ARM, heart disease, Biology, computer.software_genre, Sudden death, Models, Biological, DSG2, PKP2, PALMOPLANTAR KERATODERMA, MOLECULAR-GENETICS, SUDDEN-DEATH, TGFB3, Molecular genetics, DSC2, TP63, Databases, Genetic, Genetics, medicine, Missense mutation, Humans, JUP, PLAKOPHILIN-2 MUTATIONS, DSP, Genetics (clinical), Arrhythmogenic Right Ventricular Dysplasia, database, Internet, TMEM43, Database, Genetic Variation, medicine.disease, DILATED CARDIOMYOPATHY, Arrhythmogenic right ventricular dysplasia, WOOLLY HAIR, Leiden Open Variation Database, computer, cardiomyopathy

Abstract

Arrhythmogenic right ventricular dysplasia/cardiomyopathy (ARVD/C) is a hereditary cardiomyopathy characterized by fibrofatty replacement of cardiomyocytes, ventricular tachyarrhythmias and sudden death. ARVD/C is mainly caused by mutations in genes encoding desmosomal proteins. However, the pathogenicity of variants is not always clear. Therefore, we created an online database (www.arvcdatabase.info), providing information on variants in ARVD/C-associated genes. We searched the literature using ARVD/C and its underlying genes as search terms. From the selected papers and our unpublished data, we collected details on the type of mutation and information provided at the protein level. A "details page" contains clinical data and references. To aid the interpretation of missense mutations, we provide data from in silico prediction methods. In May 2009 the database contained 481 variants in eight genes. A total of 144 variants are considered pathogenic, 73 are unknown/unclassified, and 264 have no known pathogenicity. The database was converted into the Leiden Open Variation Database (LOVD) format, a gene-centered collection of DNA variations. The ARVD/C database will be useful for both researchers and clinicians. It can be searched to determine if variants have been published and whether they are considered pathogenic. External users are invited to add information to improve the quantity and quality of the data entered. Hum Mutat 30:1278-1283, 2009. (C) 2009 Wiley-Liss, Inc.

Published

2009

38. University struggles and student conflict in UBA during the rectory of Rodolfo Puiggrós (june – october 1973)

Author

Millán, Mariano Ignacio

Subjects

CIENCIAS SOCIALES, Rodolfo Puiggrós, Universidad de Buenos Aires, purl.org/becyt/ford/5 [https], Otras Sociología, Student movement, JUP, Reformismo universitario, Movimiento estudiantil, purl.org/becyt/ford/5.4 [https], Sociología, Universitarian reformism

Abstract

En este artículo analizamos el conflicto estudiantil y universitario en la UBA durante el rectorado de Rodolfo Puiggrós, entre junio y principios de octubre de 1973. Realizamos una periodización de los enfrentamientos distinguiendo centralmente los grupos que chocaron y los complejos procesos para la formación de alianzas. Mostramos los bríos y las dificultades para la composición de fuerzas en la izquierda, así como la emergencia de articulaciones de centro y de derechas de creciente importancia. Nuestra periodización tiene tres grandes cortes, signados por el avance de estos sectores: la llamada Masacre de Ezeiza, el día 20 de junio de 1973; el final del gobierno de Héctor Cámpora, el 13 de julio y la renuncia de Rodolfo Puiggrós, el 1 de octubre del mismo año. In this article we analyze student’s and university conflicts in UBA during the rectory of Rodolfo Puiggrós between June and early October 1973. We make a periodization of the struggles, marking the groups that clashed and the complex process of forming alliances. We show the vigor and the difficulties for the composition of forces on the left wing, and the emergence of increasingly important political forces from center and right wing. Our periodization has three major sections, marked by strengthening of conservative forces: the so calledEzeiza massacre, on June 20th, 1973; the end of the government of Hector Cámpora, on July 13th and Rodolfo Puiggrós´s resignation on October 1st of that year. Fil: Millán, Mariano Ignacio. Consejo Nacional de Investigaciones Científicas y Técnicas. Oficina de Coordinación Administrativa Saavedra 15. Instituto de Historia Argentina y Americana ; Argentina

Published

2015

39. Caractérisation clinique et moléculaire de nouvelles translocations chromosomiques ciblant le gène RUNX1 dans les leucémies aiguës de l’adulte

Author

Giguere, Amelie and Hébert, Josée

Subjects

leucémie aiguë, RUNX1, CEBPA, JUP, acute leukemia, NHEJ

Abstract

La leucémie aiguë myéloïde est une hémopathie maligne génétiquement hétérogène caractérisée par de fréquents réarrangements impliquant la bande chromosomique 21q22 et le gène RUNX1. Dans ce groupe d’anomalies, les translocations t(8;21)(q22;q22) et t(3;21)(q26;q22), associées respectivement à un pronostic favorable et défavorable, sont les mieux étudiées. Or, plus de la moitié des réarrangements ciblant RUNX1 ne sont toujours pas caractérisés au niveau clinique et moléculaire. Les principaux objectifs de cette thèse sont de caractériser quatre nouvelles translocations ciblant RUNX1 et d’étudier la dérégulation transcriptionnelle associée à ces anomalies au niveau de cibles plus spécifiques ayant un rôle dans l’auto-renouvellement ou dans la différenciation hématopoïétique. À l’aide des techniques de cytogénétique et de biologie moléculaire, deux nouveaux partenaires de RUNX1, soit CLCA2 et SV2B, ont été identifiés au sein des t(1;21)(p22.3;q22) et t(15;21)(q26.1;q22) et la récurrence des partenaires USP42 et TRPS1 a été démontrée suite à l’étude des t(7;21)(p22.1;q22) et t(8;21)(q23.3;q22). Ce travail a permis de confirmer l’existence de divers modes de dérégulation de RUNX1 dans les leucémies aiguës. L’expression présumée de protéines chimériques et/ou d’isoformes tronquées de RUNX1, un dosage aberrant des transcrits de RUNX1 et la surexpression des gènes partenaires sont des conséquences révélées par l’étude de ces fusions. Le séquençage et l’analyse des jonctions génomiques des fusions récurrentes RUNX1-USP42/USP42-RUNX1 et RUNX1-TRPS1/TRPS1-RUNX1 ont démontré la présence de signatures moléculaires caractéristiques du mode de recombinaison non-homologue de type NHEJ. En raison de la structure et de la composition différente des jonctions, l’implication de composantes distinctes du mécanisme NHEJ a été proposée. Enfin, des analyses par PCR quantitative en temps réel nous ont permis de démontrer l’existence de cibles de dérégulation partagées par les fusions récurrentes et plus rares de RUNX1. Nous avons démontré que CEBPA est moins exprimé dans la majorité des spécimens étudiés présentant une fusion de RUNX1 par rapport aux spécimens avec un caryotype normal alors que JUP, une composante effectrice de la voie Wnt, est plutôt surexprimé. Malgré l’activation transcriptionnelle de JUP dans l’ensemble de ces spécimens, certaines cibles de la voie Wnt telles que CCND1 et MYC sont différemment exprimées dans ces cellules, appuyant l’hétérogénéité décrite dans ce groupe de leucémies. Malgré l’implication de partenaires variés, nos données d’expression démontrent que les chimères et les protéines tronquées de RUNX1 partagent des cibles communes d’activation et de répression transcriptionnelle et établissent, pour la première fois, des évidences moléculaires suggérant l’existence de similitudes entre la fusion récurrente RUNX1-RUNX1T1 et quatre fusions plus rares de RUNX1. Puisque des rechutes surviennent fréquemment dans ce groupe génétique, l’inhibition de JUP pourrait être une option thérapeutique intéressante et ceci est appuyé par les bénéfices observés lors de l’inhibition de la voie Wnt dans d’autres groupes génétiques de leucémies aiguës., Acute myeloid leukemia (AML) is a genetically heterogeneous disease characterized by frequent rearrangements of the RUNX1 gene located at chromosomal band 21q22. In this subtype of leukemias, t(8;21)(q22;q22) and t(3;21)(q26;q22) translocations are among the most studied rearrangements, being respectively associated with a favourable and poor prognosis. However, approximately half of RUNX1 translocations remain uncharacterized at the clinical and molecular levels at the present time. The main objectives of this thesis are to characterize four novel RUNX1 translocations in adult patients with acute leukemias and to study the expression profiles of specific transcriptional targets of RUNX1 fusions involved in self-renewal or differentiation of hematopoietic cells. Using molecular techniques, we identified CLCA2 and SV2B genes as novel fusion partners of RUNX1 in t(1;21)(p22;q22) and t(15;21)(q26;q22) translocations. We also described the recurrence of the USP42 and TRPS1 genes involved in t(7;21)(p22;q22) and t(8;21)(q23.3;q22) translocations. Chimeric fusion proteins, truncated isoforms of RUNX1, alteration of RUNX1 transcripts expression and overexpression of the fusion partner were possible outcomes of these various fusions, thus demonstrating the diversity of RUNX1 alterations in acute leukemias. Genomic breakpoints of the recurrent RUNX1-UPS42/USP42-RUNX1 and RUNX1-TRPS1/TRPS1-RUNX1 fusions were cloned and analyzed revealing typical signatures of the non-homologous end joining recombination mechanism at fusion junctions. Since variation in the structure and composition of these junctions was observed, we proposed that distinct cellular machineries would be involved in the genesis of these abnormalities. Quantitative real-time PCR was performed on primary leukemic cells expressing these rare RUNX1 fusions. We demonstrated, for the first time, that similar downregulation of CEBPA and upregulation of JUP, an effector of the Wnt pathway, are detected in most samples studied presenting either recurrent or rare RUNX1 fusions. Despite an overexpression of JUP detected in each RUNX1 positive sample studied, other targets of the Wnt pathway like CCND1 and MYC genes were differently expressed in these cells, thus confirming the heterogeneity of this group of leukemias. Our expression data show that similar transcriptional targets, activated or repressed, are detected in cells expressing either chimeric or truncated RUNX1 proteins and establish the first molecular evidences suggesting that the recurrent RUNX1-RUNX1T1 and four rare RUNX1 fusions share common molecular deregulations. As relapse frequently occurs in RUNX1 positive leukemias, JUP overexpression could be of particular interest with regard to targeted-therapy, as demonstrated by previous work showing potential benefits of inhibiting the Wnt pathway in other genetic groups of acute leukemias.

Published

2012