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1. Results of Fabry Disease Screening in Male Pre-End Stage Renal Disease Patients with Unknown Etiology Found Through the Platform of a Chronic Kidney Disease Education Program in a Northern Taiwan Medical Center

Author

Cheng-Jui Lin, Yin-Hsiu Chien, Thung-S. Lai, Hong-Mou Shih, Yi-Chou Chen, Chi-Feng Pan, Han-Hsiang Chen, Wuh-Liang Hwu, and Chih-Jen Wu

Subjects
Fabry disease, Chronic kidney disease, High-risk screening, Dermatology, RL1-803, Diseases of the circulatory (Cardiovascular) system, RC666-701, Diseases of the genitourinary system. Urology, RC870-923
Abstract

Background/Aims: Fabry disease (FD), a rare x-lined genetic disorder is a cause of renal deterioration. The phenotype of FD is highly variable and nonspecific, and correct diagnosis has always been delayed. We aimed to explore the prevalence and clinical presentation of FD in this high-risk male population in a Northern Taiwan medical center. Methods: This is the first study to survey the incidence of FD in this high-risk population through the platform of a chronic kidney disease (CKD) education program in Asia. A total of 1,012 male patients with unknown CKD causes were screened using an assay of alpha-galactosidase A activity (α-Gal A) by dried blood spots (DBS). A final GLA gene analysis was also done for those with low enzyme activity. Results: We identified two new patients with classic FD and four patients with late-onset FD. One novel GLA mutation with c.413 G>A was found in one classic FD patient (index 5). The prevalence of FD is about 0.59 % (6 in 1,012) in the high-risk population group with CKD. The clinical symptoms of FD patients are nonspecific except in those with various degrees of renal failure. Those patients’ correct diagnosis was delayed, taking years and even decades. Three patients received enzyme replacement therapy and one started regular hemodialysis due to persistent renal function deterioration. Another two patients were found from family screening through a new index. In addition, a false negative result occurred in one patient who was proved to have FD by his kidney pathology as determined by this screening. Conclusion: FD is not such as rare a disease and its prevalence is greater in this high-risk male population. Clinicians need to be aware that FD should be included in the differential diagnosis in CKD with unknown etiology.

Published
2018
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7. HLA‐DQ genotype and biochemical characterization of anti‐transglutaminase 2 antibodies in patients with type 1 diabetes mellitus in Taiwan

Author

Yi‐Wen Yang, Thung-S. Lai, Wei-Hsin Ting, Yann-Jinn Lee, Fu-Sung Lo, Chiung-Ling Lin, Wen-Shan Lin, Yu-Ting Hsieh, Chi-Yu Huang, Cheng-Jui Lin, and Chen‐Chung Chu

Subjects
Male, 0301 basic medicine, Adolescent, Genotype, Tissue transglutaminase, Taiwan, Human leukocyte antigen, Biochemistry, Gliadin, 03 medical and health sciences, 0302 clinical medicine, GTP-Binding Proteins, HLA-DQ Antigens, HLA-DQ, Genetics, Humans, Medicine, Protein Glutamine gamma Glutamyltransferase 2, Child, Molecular Biology, Autoantibodies, Type 1 diabetes, Transglutaminases, biology, business.industry, Autoantibody, Endothelial Cells, Infant, nutritional and metabolic diseases, medicine.disease, Immunoglobulin A, Celiac Disease, Diabetes Mellitus, Type 1, 030104 developmental biology, Epitope mapping, Child, Preschool, Immunology, biology.protein, Female, Antibody, business, 030217 neurology & neurosurgery, Biotechnology
Abstract

Human Leukocyte Antigen (HLA)-DQ2 and HLA-DQ8 are genetic risk factors for Type 1 Diabetes Mellitus (T1DM) and Celiac disease (CD) in Caucasians, but their association with Taiwanese Han population is unknown. We screened 532 Taiwanese T1DM patients for CD biomarkers including anti-tissue transglutaminase (TGM2), anti-gliadin and anti-neoepitope antibodies (Abs), sequencing DQB1 genotypes, and characterized the TGM2 Abs. We report that 3.76% of Taiwanese patients had TGM2-Abs and all had no CD's symptoms. In contrast to Caucasian's CD patients, DQ2/DQ8 only constituted ~4/5 of TGM2-Abs positive patients, while the other ~1/5 patients belonged to different HLA genotypes. Either anti-gliadin or anti-neoepitope Abs coexisted with ~3/4 of TGM2-Abs positive patients that were likely due to gluten-ingestion, while the cause of TGM2-Abs production for other ~1/4 of patients was unknown. Purified anti-TGM2 IgA (TGA) and anti-TGM2 IgG (TGG) could bind on endothelial cells surface, recognized native better than denatured forms of TGM2, and TGA inhibited TGM2's transamidation activity by up to 80% but TGG had no effects. Epitope mapping of all TGM2-Abs positive sera demonstrated that TGM2-Abs had heterogeneity in specificities. This is the first study on the differences between Taiwanese Han group and Caucasian in HLA genotypes and properties of TGM2-Abs.

Published
2020
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9. Mechanisms of Sorafenib Resistance in HCC Culture Relate to the Impaired Membrane Expression of Organic Cation Transporter 1 (OCT1)

Author

Chava S, Ekmen N, Ferraris P, Aydin Y, Moroz K, Wu T, Thung SN, and Dash S

Subjects
hepatocellular carcinoma (hcc), sorafenib, sorafenib resistance (sr), organic cation transporter-1 (oct1)., Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282
Abstract

Srinivas Chava,1 Nergiz Ekmen,2 Pauline Ferraris,1 Yucel Aydin,2 Krzysztof Moroz,1 Tong Wu,1 Swan N Thung,3 Srikanta Dash1,2,4 1Department of Pathology and Laboratory Medicine, Tulane University Health Sciences Center, New Orleans, LA, USA; 2Department of Gastroenterology and Hepatology, Tulane University Health Sciences Center, New Orleans, LA, USA; 3Department of Pathology, Icahn School of Medicine at Mount Sinai, New York, NY, USA; 4Southeast Louisiana Veterans Health Care System, New Orleans, LA, USACorrespondence: Srikanta Dash, Department of Pathology and Laboratory Medicine, Tulane University Health Sciences Center, 1430 Tulane Avenue, New Orleans, LA, 70112, USA, Tel +1 504-988-2519, Fax +1 504-988-7389, Email sdash@tulane.eduIntroduction: Sorafenib, an FDA-approved drug for advanced hepatocellular carcinoma (HCC) treatment, encounters resistance in many patients. Deciphering the mechanisms underlying sorafenib resistance is crucial for devising alternative strategies to overcome it.Aim: This study aimed to investigate sorafenib resistance mechanisms using a diverse panel of HCC cell lines.Methods: HCC cell lines were subjected to continuous sorafenib treatment, and stable cell lines (Huh 7.5 and Huh 7PX) exhibiting sustained growth in its presence were isolated. The investigation of drug resistance mechanisms involved a comparative analysis of drug-targeted signal transduction pathways (EGFR/RAF/MEK/ERK/Cyclin D), sorafenib uptake, and membrane expression of the drug uptake transporter.Results: HCC cell lines (Huh 7.5 and Huh 7PX) with a higher IC50 (10μM) displayed a more frequent development of sorafenib resistance compared to those with a lower IC50 (2– 4.8μM), indicating a potential impact of IC50 variation on initial treatment response. Our findings reveal that activated overexpression of Raf1 kinases and impaired sorafenib uptake, mediated by reduced membrane expression of organic cation transporter-1 (OCT1), contribute to sorafenib resistance in HCC cultures. Stable expression of the drug transporter OCT1 through cDNA transfection or adenoviral delivery of OCT1 mRNA increased sorafenib uptake and successfully overcame sorafenib resistance. Additionally, consistent with sorafenib resistance in HCC cultures, cirrhotic liver-associated human HCC tumors often exhibited impaired membrane expression of OCT1 and OCT3.Conclusion: Intrinsic differences among HCC cell clones, affecting sorafenib sensitivity at the expression level of Raf kinases, drug uptake, and OCT1 transporters, were identified. This study underscores the potential of HCC tumor targeted OCT1 expression to enhance sorafenib treatment response.Keywords: hepatocellular carcinoma, HCC, cholangiocarcinoma, CCA, tyrosine kinase inhibitors, TKI, organic cation transporter-1, OCT1, organic cation transporter-3, OCT3, sorafenib resistance cell lines, SR huh 7

Published
2024

10. Macroscopic Characterization of Hepatocellular Carcinoma: An Underexploited Source of Prognostic Factors

Author

Gonvers S, Martins-Filho SN, Hirayama A, Calderaro J, Phillips R, Uldry E, Demartines N, Melloul E, Park YN, Paradis V, Thung SN, Alves V, Sempoux C, and Labgaa I

Subjects
liver cancer, hcc, prognostication, gross, survival, recurrence, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282
Abstract

Stéphanie Gonvers,1,2 Sebastiao N Martins-Filho,3 André Hirayama,4 Julien Calderaro,5 Rebecca Phillips,3 Emilie Uldry,1,2 Nicolas Demartines,1,2 Emmanuel Melloul,1,2 Young Nyun Park,6 Valérie Paradis,7 Swan N Thung,8 Venancio Alves,4 Christine Sempoux,2,9 Ismail Labgaa1,2 1Department of Visceral Surgery, Lausanne University Hospital (CHUV), Lausanne, Switzerland; 2Faculty of Biology & Medicine (FBM), University of Lausanne (UNIL), Lausanne, Switzerland; 3Department of Laboratory Medicine and Pathology, University of Alberta, Edmonton, Alberta, Canada; 4Department of Pathology, Faculdade de Medicina FMUSP, Universidade de Sao Paulo, Sao Paulo, Brazil; 5Department of Pathology, APHP, Henri Mondor University Hospital, Creteil, Val-de-Marne, France; 6Department of Pathology, Severance Hospital, Yonsei University College of Medicine, Seoul, Republic of Korea; 7Department of Pathology, APHP, Beaujon University Hospital, Clichy, France; 8Department of Pathology, Molecular and Cell Based Medicine, Icahn School of Medicine at Mount Sinai, New York, NY, USA; 9Department of Pathology, Lausanne University Hospital (CHUV), Lausanne, SwitzerlandCorrespondence: Ismail Labgaa, Department of Visceral Surgery, University Hospital of Lausanne (CHUV), Rue du Bugnon 46, CH-1011, Lausanne, Switzerland, Tel +41 0 79 556 68 47, Email ismail.labgaa@chuv.chAbstract: The macroscopic appearance of a tumor such as hepatocellular carcinoma (HCC) may be defined as its phenotype which is de facto dictated by its genotype. Therefore, macroscopic characteristics of HCC are unlikely random but rather reflect genomic traits of cancer, presumably acting as a valuable source of information that can be retrieved and exploited to infer prognosis. This review aims to provide a comprehensive overview of the available data on the prognostic value of macroscopic characterization in HCC. A total of 57 studies meeting eligible criteria were identified, including patients undergoing liver resection (LR; 47 studies, 83%) or liver transplant (LT; 9 studies, 16%). The following macroscopic variables were investigated: tumor size (n = 42 studies), number of nodules (n = 28), vascular invasion (n = 24), bile duct invasion (n = 6), growth pattern (n = 15), resection margin (n = 11), tumor location (n = 6), capsule (n = 2) and satellite (n = 1). Although the selected studies provided insightful data with notable prognostic performances, a lack of standardization and substantial gaps were noted in the report and the analysis of gross findings. This topic remains incompletely covered. While the available studies underscored the value of macroscopic variables in HCC prognostication, important lacks were also observed. Macroscopic characterization of HCC is likely an underexploited source of prognostic factors that must be actively explored by future multidisciplinary research. Keywords: liver cancer, HCC, prognostication, gross, survival, recurrence

Published
2024

17. HLA‐DQ genotype and biochemical characterization of anti‐transglutaminase 2 antibodies in patients with type 1 diabetes mellitus in Taiwan

Author

Lee, Yann‐Jinn, primary, Ting, Wei‐Hsin, additional, Yang, Yi‐Wen, additional, Lin, Cheng‐Jui, additional, Hsieh, Yu‐Ting, additional, Huang, Chi‐Yu, additional, Lo, Fu‐Sung, additional, Chu, Chen‐Chung, additional, Lin, Chiung‐Ling, additional, Lin, Wen‐Shan, additional, and Lai, Thung‐S., additional

Published
2020
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18. The role of indoxyl sulfate in renal anemia in patients with chronic kidney disease

Author

Cheng Yi Chen, Hung I. Yeh, Pei Chen Wu, Hsuan Liang Liu, Cheng Jui Lin, Fang Ju Sun, Chih Jen Wu, Chih-Kuang Chuang, Thung S. Lai, Han Hsiang Chen, and Chih-Sheng Lin

Subjects
Gerontology, Nephrology, medicine.medical_specialty, 030232 urology & nephrology, 030204 cardiovascular system & hematology, 03 medical and health sciences, 0302 clinical medicine, Negatively associated, Renal anemia, Internal medicine, hemic and lymphatic diseases, medicine, In patient, indoxyl sulfate, business.industry, University hospital, medicine.disease, Oncology, Erythropoietin, Indoxyl Sulfate, erythropoietin, business, chronic kidney disease, Kidney disease, medicine.drug, Research Paper, renal anemia
Abstract

// Chih-Jen Wu 1, 2, 3 , Cheng-Yi Chen 1, 8, 11 , Thung-S. Lai 4 , Pei-Chen Wu 1 , Chih-Kuang Chuang 5, 6, 7 , Fang-Ju Sun 8, 9 , Hsuan-Liang Liu 5 , Han-Hsiang Chen 1, 8 , Hung-I. Yeh 10 , Chih-Sheng Lin 11 and Cheng-Jui Lin 1, 5, 8 1 Division of Nephrology, Department of Internal Medicine, Mackay Memorial Hospital, Mackay Medical College ,Taipei, Taiwan 2 Department of Medical Research, China Medical University Hospital, China Medical University, Taichung, Taiwan 3 Graduate Institute of Medical Sciences and Department of Pharmacology, School of Medicine, College of Medicine, Taipei Medical University, Taipei, Taiwan 4 Graduate Institute of Biomedical Science, Mackay Medical College, New Taipei City, Taiwan 5 Institute of Biotechnology, National Taipei University of Technology, Taipei, Taiwan 6 Division of Genetics and Metabolism, Department of Medical Research, Mackay Memorial Hospital, Taipei, Taiwan 7 College of Medicine, Fu-Jen Catholic University, Taipei, Taiwan 8 Mackay Junior College of Medicine, Nursing and Management, Taipei, Taiwan 9 Department of Medical Research, Mackay Memorial Hospital, Taipei, Taiwan 10 Department of Medicine, Mackay Medical College, New Taipei City, Taiwan 11 Department of Biological Science and Technology, National Chaio Tung University, Hsinchu, Taiwan Correspondence to: Cheng-Jui Lin, email: lincj@mmh.org.tw Keywords: indoxyl sulfate, chronic kidney disease, erythropoietin, renal anemia Received: April 27, 2017 Accepted: May 29, 2017 Published: June 28, 2017 ABSTRACT Renal anemia is a common complication in patients with advanced chronic kidney disease. In vitro studies have shown that indoxyl sulfate decreases erythropoietin production. Whether this effect is seen in vivo remains unclear. Our goal was to explore the role of indoxyl sulfate in renal anemia. We found serum indoxyl sulfate levels are significantly and negatively associated with erythropoietin levels in human. A multiple stepwise linear regression analyses after adjustment for other independent parameters revealed that free indoxyl sulfate, and total indoxyl sulfate were significantly associated with erythropoietin levels. In animal studies, erythropoietin gene and protein expression were markedly inhibited in rats with chronic kidney disease; however, this effect was significantly reversed by lowering serum indoxyl sulfate with AST-120. Indoxyl sulfate may also inhibit erythropoietin expression in animal models with chronic kidney disease. These findings further support the role of indoxyl sulfate in the development of renal anemia.

Published
2017

19. Tissue transglutaminase TG2 and mitochondrial function and dysfunction

Author

Cheng-Jui Lin, Thung-S. Lai, Yu-Ting Wu, and Chih-Jen Wu

Subjects
0301 basic medicine, Epithelial-Mesenchymal Transition, Tissue transglutaminase, Mitochondrial disease, Cell, Respiratory chain, Autoimmunity, Mitochondrion, medicine.disease_cause, Gene Expression Regulation, Enzymologic, 03 medical and health sciences, Alzheimer Disease, GTP-Binding Proteins, medicine, Animals, Humans, Protein Glutamine gamma Glutamyltransferase 2, chemistry.chemical_classification, Wound Healing, Reactive oxygen species, Transglutaminases, 030102 biochemistry & molecular biology, biology, Cytochrome c, fungi, food and beverages, Neurodegenerative Diseases, Parkinson Disease, medicine.disease, Mitochondria, Cell biology, Huntington Disease, medicine.anatomical_structure, chemistry, biology.protein, Oxidative stress
Abstract

Mitochondria are the cell's power plant to satisfy the energy demands. However, dysfunctional mitochondria can cause overproduction of reactive oxygen species (ROS), oxidative stress, and alteration of calcium homeostasis, which are the hallmarks of mitochondrial diseases. Under prolong oxidative stress, repeated cytosolic calcium elevations even only transiently, can lead to activation of some enzymes. One calcium-activated enzyme with demonstrated pathophysiological important in mitochondrial disease is tissue transglutaminase (TG2). TG2 is known as a post-translational modification (PTM) enzyme that is induced by oxidative stress. Compared to other types of PTMs, the physiological significance of TG2 mediated PTM is just beginning to be understood. Once activated, TG2 can modulate transcription, inactivate metabolic enzymes, and cause aggregation of critical proteins. Recent data indicate that TG2's activity not only can modulate the assembly of respiratory chain complexes but can also modulate the transcription of critical genes including PGC-1alpha and cytochrome C that are important for function and biogenesis of mitochondria. Here, we summarize dysfunctional mitochondria in diseases such as in neurodegenerative disorders can modulate TG2's activity and function. TG2 is also important for normal function of mitochondria.

Published
2017
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21. ASS1 Overexpression: A Hallmark of Sonic Hedgehog Hepatocellular Adenomas; Recommendations for Clinical Practice

Author

Sala, M., Gonzales, D., Leste-Lasserre, T., Dugot-Senant, N., Paradis, V., Di Tommaso, S., Dupuy, J.W., Pitard, V., Dourthe, C., Sciarra, A., Sempoux, C., Ferrell, L.D., Clouston, A.D., Miller, G., Yeh, M.M., Thung, S., Gouw, ASH, Quaglia, A., Han, J., Huan, J., Fan, C., Crawford, J., Nakanuma, Y., Harada, K., le Bail, B., Castain, C., Frulio, N., Trillaud, H., Possenti, L., Blanc, J.F., Chiche, L., Laurent, C., Balabaud, C., Bioulac-Sage, P., Raymond, A.A., Saltel, F., and Groningen Institute for Organ Transplantation (GIOT)

Subjects
PCR, MARKERS, MOLECULAR CLASSIFICATION, RISK-FACTORS, MANAGEMENT, lcsh:Diseases of the digestive system. Gastroenterology, Original Article, Original Articles, lcsh:RC799-869, TRANSFORMATION
Abstract

Until recently, 10% of hepatocellular adenomas (HCAs) remained unclassified (UHCA). Among the UHCAs, the sonic hedgehog HCA (shHCA) was defined by focal deletions that fuse the promoter of Inhibin beta E chain with GLI1. Prostaglandin D2 synthase was proposed as immunomarker. In parallel, our previous work using proteomic analysis showed that most UHCAs constitute a homogeneous subtype associated with overexpression of argininosuccinate synthase (ASS1). To clarify the use of ASS1 in the HCA classification and avoid misinterpretations of the immunohistochemical staining, the aims of this work were to study (1) the link between shHCA and ASS1 overexpression and (2) the clinical relevance of ASS1 overexpression for diagnosis. Molecular, proteomic, and immunohistochemical analyses were performed in UHCA cases of the Bordeaux series. The clinico‐pathological features, including ASS1 immunohistochemical labeling, were analyzed on a large international series of 67 cases. ASS1 overexpression and the shHCA subgroup were superimposed in 15 cases studied by molecular analysis, establishing ASS1 overexpression as a hallmark of shHCA. Moreover, the ASS1 immunomarker was better than prostaglandin D2 synthase and only found positive in 7 of 22 shHCAs. Of the 67 UHCA cases, 58 (85.3%) overexpressed ASS1, four cases were ASS1 negative, and in five cases ASS1 was noncontributory. Proteomic analysis performed in the case of doubtful interpretation of ASS1 overexpression, especially on biopsies, can be a support to interpret such cases. ASS1 overexpression is a specific hallmark of shHCA known to be at high risk of bleeding. Therefore, ASS1 is an additional tool for HCA classification and clinical diagnosis., ShHCA is a new HCA subgroup with a high risk of bleeding with PTGDS and ASS1 proposed as immunomarkers, with conflicting results and interpretations in the literature. By molecular, proteomic, and immunohistochemistry analyses, we established that ASS1 overexpression was a specific hallmark of shHCA. Having shown that PTGDS was not a good marker, we demonstrated, using a large cohort of UHCAs, the sensitivity of ASS1 immunomarker and its clinical relevance. Therefore, ASS1 is an additional tool for HCA classification, clinical diagnosis of shHCA, and appropriate management.

Published
2019

22. Histology of portal vascular changes associated with idiopathic non-cirrhotic portal hypertension: nomenclature and definition

Author

Guido, M., Alves, VAF, Balabaud, C., Bathal, P.S., Bioulac-Sage, P., Colombari, R., Crawford, J.M., Dhillon, A.P., Ferrell, L.D., Gill, R.M., Hytiroglou, P., Nakanuma, Y., Paradis, V., Quaglia, A., Rautou, P.E., Theise, N.D., Thung, S., Tsui, WMS, Sempoux, C., Snover, D., van Leeuwen, D.J., and International Liver Pathology Study Group

Subjects
Humans, Hypertension, Portal/pathology, Liver/pathology, idiopathic non-cirrhotic portal hypertension, liver vascular lesions, obliterative portal venopathy, phlebosclerosis
Abstract

Idiopathic non-cirrhotic portal hypertension (INCPH) is a rare vascular liver disease that has attracted new interest in recent years. It is characterised by clinical signs of portal hypertension in the absence of cirrhosis or severe fibrosis and any known cause of portal hypertension. As much uncertainty exists about INCPH pathophysiology, and no definite diagnostic tests are available, liver biopsy is an essential tool for achieving a definite diagnosis. Unfortunately, the histological diagnosis of INCPH is not always straightforward, as the characteristic lesions are unevenly distributed, vary greatly in their severity, are often very subtle, and are not all necessarily present in a single case. Furthermore, specifically for the characteristic portal vessel changes observed in INCPH, the terminology and definition are ambiguous, which adds complexity to the already complex clinicopathological scenario. An international study group of liver pathologists and hepatologists pursued a consensus on nomenclature for the portal vascular lesions of INCPH. Such standardisation may assist pathologists in the recognition of such lesions, and will possibly facilitate further advancement in this field.

Published
2019

25. cHCC-CCA: Consensus terminology for primary liver carcinomas with both hepatocytic and cholangiocytic differentation

Author

Brunt, E, Aishima, S, Clavien, PA, Fowler, K, Goodman, Z, Gores, G, Gouw, A, Kagen, A, Klimstra, D, Komuta, M, Kondo, F, Miksad, R, Nakano, M, Nakanuma, Y, Ng, I, Paradis, V, Nyun Park, Y, Quaglia, A, Roncalli, M, Roskams, T, Sakamoto, M, Saxena, R, Sempoux, C, Sirlin, C, Stueck, A, Thung, S, Tsui, WMS, Wang, XW, Wee, A, Yano, H, Yeh, M, Zen, Y, and Zucman-Rossi, J

Abstract

© 2018 by the American Association for the Study of Liver Diseases. Primary liver carcinomas with both hepatocytic and cholangiocytic differentiation have been referred to as “combined (or mixed) hepatocellular-cholangiocarcinoma.” These tumors, although described over 100 years ago, have attracted greater attention recently because of interest in possible stem cell origin and perhaps because of greater frequency and clinical recognition. Currently, because of a lack of common terminology in the literature, effective treatment and predictable outcome data have been challenging to accrue. This article represents a consensus document from an international community of pathologists, radiologists, and clinicians who have studied and reported on these tumors and recommends a working terminology for diagnostic and research approaches for further study and evaluation. Conclusion: It is recommended that diagnosis is based on routine histopathology with hematoxylin and eosin (H&E); immunostains are supportive, but not essential for diagnosis. (Hepatology 2018;68:113-126).

Published
2018
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27. Endothelial cell-surface tissue transglutaminase inhibits neutrophil adhesion by binding and releasing nitric oxide

Author

Zishan A. Haroon, Mark W. Dewhirst, Charles S. Greenberg, Y. L. Juang, Thung S. Lai, Robert A. Lindberg, Alfred Hausladen, Hua Lin Zhou, and Jonathan S. Stamler

Subjects
0301 basic medicine, Endothelium, Neutrophil adhesion, Tissue transglutaminase, Neutrophils, lcsh:Medicine, Nitric Oxide, Article, Nitric oxide, 03 medical and health sciences, chemistry.chemical_compound, GTP-Binding Proteins, medicine, Cell Adhesion, Human Umbilical Vein Endothelial Cells, Humans, Protein Glutamine gamma Glutamyltransferase 2, lcsh:Science, Multidisciplinary, Transglutaminases, 030102 biochemistry & molecular biology, biology, Chemistry, lcsh:R, Cell biology, Endothelial stem cell, 030104 developmental biology, Membrane, medicine.anatomical_structure, biology.protein, lcsh:Q, Tumor necrosis factor alpha, Cysteine
Abstract

Nitric oxide (NO) produced by endothelial cells in response to cytokines displays anti-inflammatory activity by preventing the adherence, migration and activation of neutrophils. The molecular mechanism by which NO operates at the blood-endothelium interface to exert anti-inflammatory properties is largely unknown. Here we show that on endothelial surfaces, NO is associated with the sulfhydryl-rich protein tissue transglutaminase (TG2), thereby endowing the membrane surfaces with anti-inflammatory properties. We find that tumor necrosis factor-α-stimulated neutrophil adherence is opposed by TG2 molecules that are bound to the endothelial surface. Alkylation of cysteine residues in TG2 or inhibition of endothelial NO synthesis renders the surface-bound TG2 inactive, whereas specific, high affinity binding of S-nitrosylated TG2 (SNO-TG2) to endothelial surfaces restores the anti-inflammatory properties of the endothelium, and reconstitutes the activity of endothelial-derived NO. We also show that SNO-TG2 is present in healthy tissues and that it forms on the membranes of shear-activated endothelial cells. Thus, the anti-inflammatory mechanism that prevents neutrophils from adhering to endothelial cells is identified with TG2 S-nitrosylation at the endothelial cell-blood interface.

Published
2017

28. Correction: The role of indoxyl sulfate in renal anemia in patients with chronic kidney disease

Author

Han-Hsiang Chen, Pei-Chen Wu, Chih-Sheng Lin, Hsuan Liang Liu, Chih-Jen Wu, Hung-I. Yeh, Cheng-Yi Chen, Fang-Ju Sun, Cheng-Jui Lin, Thung-S. Lai, and Chih-Kuang Chuang

Subjects
medicine.medical_specialty, business.industry, Correction, medicine.disease, Gastroenterology, Text mining, Oncology, Renal anemia, Internal medicine, medicine, Indoxyl Sulfate, In patient, business, Kidney disease
Abstract

Renal anemia is a common complication in patients with advanced chronic kidney disease.

Published
2019
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29. Integrative molecular classification of extrahepatic cholangiocarcinoma

Author

Montal, R., primary, Leow, W.Q., additional, Montironi, C., additional, Bassaganyas, L., additional, Moeini, A., additional, Sia, D., additional, Pinyol, R., additional, Cabellos, L., additional, Peix, J., additional, Maeda, M., additional, Tabrizian, P., additional, Minguez, B., additional, Pawlik, T., additional, Labgaa, I., additional, Roberts, L., additional, Sole, M., additional, Fiel, M.I., additional, Thung, S., additional, Roayaie, S., additional, Villanueva, A., additional, Schwartz, M., additional, and Llovet, J.M., additional

Published
2018
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30. Results of Fabry Disease Screening in Male Pre-End Stage Renal Disease Patients with Unknown Etiology Found Through the Platform of a Chronic Kidney Disease Education Program in a Northern Taiwan Medical Center

Author

Lin, Cheng-Jui, primary, Chien, Yin-Hsiu, additional, Lai, Thung-S., additional, Shih, Hong-Mou, additional, Chen, Yi-Chou, additional, Pan, Chi-Feng, additional, Chen, Han-Hsiang, additional, Hwu, Wuh-Liang, additional, and Wu, Chih-Jen, additional

Published
2018
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34. Molecular characterization of the immune class of hepatocellular carcinoma

Author

Martinez-Quętglas, I., primary, Sia, D., additional, Jiao, Y., additional, Kuchuck, O., additional, Martin, C.V., additional, De Moura, M.C., additional, Putra, J., additional, Camprecios, G., additional, Thung, S., additional, Mazzaferro, V., additional, Esteller, M., additional, Villanueva, A., additional, and Llovet, J.M., additional

Published
2017
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36. 2016 Comprehensive Update of the Banff Working Group on Liver Allograft Pathology: Introduction of Antibody-Mediated Rejection.

Author

UCL - SSS/IREC/CHEX - Pôle de chirgurgie expérimentale et transplantation, UCL - (SLuc) Service de chirurgie et transplantation abdominale, Demetris, A J, Bellamy, C, Hübscher, S G, O'Leary, J, Randhawa, P S, Feng, S, Neil, D, Colvin, R B, McCaughan, G, Fung, J J, Del Bello, A, Reinholt, F P, Haga, H, Adeyi, O, Czaja, A J, Schiano, T, Fiel, M I, Smith, M L, Sebagh, M, Tanigawa, R Y, Yilmaz, F, Alexander, G, Baiocchi, L, Balasubramanian, M, Batal, I, Bhan, A K, Bucuvalas, J, Cerski, C T S, Charlotte, F, de Vera, M E, ElMonayeri, M, Fontes, P, Furth, E E, Gouw, A S H, Hafezi-Bakhtiari, S, Hart, J, Honsova, E, Ismail, W, Itoh, T, Jhala, N C, Khettry, U, Klintmalm, G B, Knechtle, S, Koshiba, T, Kozlowski, T, Lassman, C R, Lerut, Jan, Levitsky, J, Licini, L, Liotta, R, Mazariegos, G, Minervini, M I, Misdraji, J, Mohanakumar, T, Mölne, J, Nasser, I, Neuberger, J, O'Neil, M, Pappo, O, Petrovic, L, Ruiz, P, Sağol, Ö, Sanchez Fueyo, A, Sasatomi, E, Shaked, A, Shiller, M, Shimizu, T, Sis, B, Sonzogni, A, Stevenson, H L, Thung, S N, Tisone, G, Tsamandas, A C, Wernerson, A, Wu, T, Zeevi, A, Zen, Y, UCL - SSS/IREC/CHEX - Pôle de chirgurgie expérimentale et transplantation, UCL - (SLuc) Service de chirurgie et transplantation abdominale, Demetris, A J, Bellamy, C, Hübscher, S G, O'Leary, J, Randhawa, P S, Feng, S, Neil, D, Colvin, R B, McCaughan, G, Fung, J J, Del Bello, A, Reinholt, F P, Haga, H, Adeyi, O, Czaja, A J, Schiano, T, Fiel, M I, Smith, M L, Sebagh, M, Tanigawa, R Y, Yilmaz, F, Alexander, G, Baiocchi, L, Balasubramanian, M, Batal, I, Bhan, A K, Bucuvalas, J, Cerski, C T S, Charlotte, F, de Vera, M E, ElMonayeri, M, Fontes, P, Furth, E E, Gouw, A S H, Hafezi-Bakhtiari, S, Hart, J, Honsova, E, Ismail, W, Itoh, T, Jhala, N C, Khettry, U, Klintmalm, G B, Knechtle, S, Koshiba, T, Kozlowski, T, Lassman, C R, Lerut, Jan, Levitsky, J, Licini, L, Liotta, R, Mazariegos, G, Minervini, M I, Misdraji, J, Mohanakumar, T, Mölne, J, Nasser, I, Neuberger, J, O'Neil, M, Pappo, O, Petrovic, L, Ruiz, P, Sağol, Ö, Sanchez Fueyo, A, Sasatomi, E, Shaked, A, Shiller, M, Shimizu, T, Sis, B, Sonzogni, A, Stevenson, H L, Thung, S N, Tisone, G, Tsamandas, A C, Wernerson, A, Wu, T, Zeevi, A, and Zen, Y

Abstract

The Banff Working Group on Liver Allograft Pathology reviewed and discussed literature evidence regarding antibody-mediated liver allograft rejection at the 11th (Paris, France, June 5-10, 2011), 12th (Comandatuba, Brazil, August 19-23, 2013), and 13th (Vancouver, British Columbia, Canada, October 5-10, 2015) meetings of the Banff Conference on Allograft Pathology. Discussion continued online. The primary goal was to introduce guidelines and consensus criteria for the diagnosis of liver allograft antibody-mediated rejection and provide a comprehensive update of all Banff Schema recommendations. Included are new recommendations for complement component 4d tissue staining and interpretation, staging liver allograft fibrosis, and findings related to immunosuppression minimization. In an effort to create a single reference document, previous unchanged criteria are also included.

Published
2016

37. Strategies for a Successful Anatomic Pathology Subspecialty Workgroup: The 26-Year Collaboration of 'The Elves'

Author

Scheuer, PJ, Alves, V, Balabaud, C, Bardadin, K, Bhathal, P, Bioulac-Sage, P-E, Colombari, R, Crawford, JM, Dhillon, AP, Ferrell, LD, Guido, M, Hytiroglou, P, Nakanuma, Y, Portmann, B, Paradis, V, Quaglia, A, Rode, J, Snover, D, Theise, ND, Thung, S, Tsui, W, van Leeuwen, D, Scheuer, PJ, Alves, V, Balabaud, C, Bardadin, K, Bhathal, P, Bioulac-Sage, P-E, Colombari, R, Crawford, JM, Dhillon, AP, Ferrell, LD, Guido, M, Hytiroglou, P, Nakanuma, Y, Portmann, B, Paradis, V, Quaglia, A, Rode, J, Snover, D, Theise, ND, Thung, S, Tsui, W, and van Leeuwen, D

Abstract

From 1990 to present, 14 liver pathologists and 2 clinical hepatologists from 9 countries have met annually to hold thematic 2.5-day meetings centered on case-based discussion. The goal of these meetings has been to identify gaps in knowledge in our field and fuel scholarly effort to address these gaps. The founding principles were worldwide representation, good representation of women, compatibility of participants, commitment to stable membership and regular attendance, mutual education and friendship, and free exchange of ideas. A summary report of the 2.5-day meeting constituted an enduring document that captured the free flow of ideas discussed. These ideas were open to all participants for the pursuit of scholarship back at their home institutions. However, any idea borne out of an Elves meeting merits open invitation for other Elves to participate in, using established standards for meaningful coauthorship. Over 26 consecutive meetings (1990-2015), themes covered the breadth of liver pathology. With retirement of 2 individuals, resignation of 3, and death of 1, six new members were nominated and voted into membership. Over these same 26 years, active members published 2025 articles indexed in PubMEd Central under the topic "liver;" 3% of these articles represented collaborations between members. This international group represents a successful model in a subspecialty of anatomic pathology for open exchange of ideas, mutual education, and generation of topics worthy of scholarly investigation. We conclude that a self-selected group of subspecialty pathologists can meet successfully over 26 years, maintain a high state of engagement through each annual meeting, self-renew as a result of retirement or resignation, and provide a creative stimulus for highly productive academic careers.

Published
2016

38. Site-directed Mutagenesis of the Calcium-binding Site of Blood Coagulation Factor XIIIa

Author

Thomas F. Slaughter, Keith A. Peoples, Thung-S. Lai, and Charles S. Greenberg

Subjects
Models, Molecular, Protein Conformation, Stereochemistry, Molecular Sequence Data, chemistry.chemical_element, Calcium, Crystallography, X-Ray, Biochemistry, Thrombin, Protein structure, Aspartic acid, Escherichia coli, medicine, Amino Acid Sequence, Binding site, Site-directed mutagenesis, Molecular Biology, Alanine, Binding Sites, Transglutaminases, Chemistry, Cell Biology, Recombinant Proteins, Cross-Linking Reagents, Mutagenesis, Site-Directed, Factor XIIIa, Sequence Alignment, Protein Binding, medicine.drug
Abstract

Blood coagulation factor XIIIa is a calcium-dependent enzyme that covalently ligates fibrin molecules during blood coagulation. X-ray crystallography studies identified a major calcium-binding site involving Asp(438), Ala(457), Glu(485), and Glu(490). We mutated two glutamic acid residues (Glu(485) and Glu(490)) and three aspartic acid residues (Asp(472), Asp(476), and Asp(479)) that are in close proximity. Alanine substitution mutants of these residues were constructed, expressed, and purified from Escherichia coli. The K(act) values for calcium ions increased by 3-, 8-, and 21-fold for E485A, E490A, and E485A,E490A, respectively. In addition, susceptibility to proteolysis was increased by 4-, 9-, and 10-fold for E485A, E490A, and E485A,E490A, respectively. Aspartic acids 472, 476, and 479 are not involved directly in calcium binding since the K(act) values were not changed by mutagenesis. However, Asp(476) and Asp(479) are involved in regulating the conformation for exposure of the secondary thrombin cleavage site. This study provides biochemical evidence that Glu(485) and Glu(490) are Ca(2+)-binding ligands that regulate catalysis. The binding of calcium ion to this site protects the molecule from proteolysis. Furthermore, Asp(476) and Asp(479) play a role in modulating calcium-dependent conformational changes that cause factor XIIIa to switch from a protease-sensitive to a protease-resistant molecule.

Published
1999
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41. Histaminylation of fibrinogen by tissue transglutaminase-2 (TGM-2): potential role in modulating inflammation

Author

Charles S. Greenberg and Thung-S. Lai

Subjects
Tissue transglutaminase, Clinical Biochemistry, Inflammation, Fibrinogen, Biochemistry, Fibrin, chemistry.chemical_compound, GTP-Binding Proteins, medicine, Human Umbilical Vein Endothelial Cells, Humans, Platelet, Protein Glutamine gamma Glutamyltransferase 2, Transglutaminases, biology, Chemistry, Organic Chemistry, Recombinant Proteins, Endothelial stem cell, biology.protein, medicine.symptom, Wound healing, Histamine, medicine.drug
Abstract

Plasma fibrinogen plays an important role in hemostasis and inflammation. Fibrinogen is converted to fibrin to impede blood loss and serves as the provisional matrix that aids wound healing. Fibrinogen also binds to cytokine activated endothelial cells and promotes the binding and migration of leukocytes into tissues during inflammation. Tissue transglutaminase (TGM-2) released from injured cells could cross-link fibrinogen to form multivalent complexes that could promote adhesion of platelets and vascular cells to endothelium. Histamine released by mast cells is a potent biogenic amine that promotes inflammation. The covalent attachment of histamine to proteins (histaminylation) by TGM-2 could modify local inflammatory reactions. We investigated TGM-2 crosslinking of several biogenic amines (serotonin, histamine, dopamine and noradrenaline) to fibrinogen. We identified histaminylation of fibrinogen by TGM-2 as a preferred reaction in solid and solution phase transglutaminase assays. Histamine caused a concentration-dependent inhibition of fibrinogen cross-linking by TGM-2. Fibrinogen that was not TGM-2 crosslinked bound to unactivated endothelial cells with low affinity. However, the binding was increased by sevenfold when fibrinogen was cross-linked by TGM-2. Histaminylation of fibrinogen also inhibited TGM-2 crosslinking of fibrinogen and the binding to un-activated HUVEC cells by 75–90 %. In summary, the histaminylation of fibrinogen by TGM-2 could play a role in modifying inflammation by sequestering free histamine and by inhibiting TGM-2 crosslinking of fibrinogen.

Published
2013

42. An evaluation of fetal heart rate characteristics associated with neonatal encephalopathy: a case-control study.

Author

Frey, H. A., Liu, X., Lynch, C. D., Musindi, W., Samuels, P., Rood, K. M., Thung, S. F., Bakk, J. M., Cheng, W., and Landon, M. B.

Subjects
FETAL heart, FETAL heart rate, HEPATIC encephalopathy, LOGISTIC regression analysis, GESTATIONAL age, BRAIN diseases, COMPARATIVE studies, FETAL heart rate monitoring, NEONATAL diseases, RESEARCH methodology, MEDICAL cooperation, MULTIVARIATE analysis, RESEARCH, RESEARCH funding, EVALUATION research, RETROSPECTIVE studies, CASE-control method, ODDS ratio
Abstract

Objective: We sought to identify fetal heart rate (FHR) characteristics that are associated with neonatal encephalopathy (NE).Design: Retrospective case-control study.Setting: A single medical centre in Shanghai, China, 2006-2015.Sample: Women delivering a singleton, non-anomalous infant at ≥36 weeks' gestation diagnosed with NE (cases, n = 109) were compared with a group of women with unaffected infants (controls, n = 233).Methods: Two physicians blinded to the outcome independently reviewed FHR tracings during the last 30 minutes of tracing prior to delivery. FHR characteristics were compared in the two groups and multivariable logistic regression was used to adjust for confounding.Main Outcome Measures: Adjusted odds ratio (aOR) and 95% confidence interval (CI) for the presence of specific FHR categories and characteristics.Results: Category II FHR tracings were observed in 89% of women prior to delivery and were not independently associated with NE. Notably, a category III FHR was observed in 17.4% of women in the NE group compared with 0.9% of women in the control group (aOR 44.99, 95% CI 7.23-279.97). Bradycardia, minimal/absent variability, late decelerations and prolonged decelerations were independently associated with NE, whereas accelerations were protective. Similar findings were found when the cases were limited to NE with arterial cord pH <7.1 and in a subgroup analysis of women with category II tracings.Conclusions: Category III tracings, while infrequent, are not uncommon prior to delivery among fetuses who develop NE. In contrast, most FHR tracings are category II prior to delivery; however, individual FHR characteristics within this category are associated with NE.Funding: This research was supported by the Interdisciplinary Programme of Shanghai Jiao Tong University.Tweetable Abstract: Category III tracings are not uncommon prior to delivery among fetuses who develop neonatal encephalopathy. [ABSTRACT FROM AUTHOR]

Published
2018
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43. C-terminal Deletion of Human Tissue Transglutaminase Enhances Magnesium-dependent GTP/ATPase Activity

Author

Thung S. Lai, Charles S. Greenberg, Celine M. Koropchak, Thomas F. Slaughter, and Zishan A. Haroon

Subjects
GTP', Tissue transglutaminase, Recombinant Fusion Proteins, Mutant, GTPase, Biology, Biochemistry, Structure-Activity Relationship, ATP hydrolysis, Humans, Magnesium, Enzyme kinetics, Molecular Biology, Glutathione Transferase, Adenosine Triphosphatases, Transglutaminases, Factor XIII, C-terminus, Wild type, Cell Biology, Nucleoside-Triphosphatase, Molecular biology, Adenosine Monophosphate, Acid Anhydride Hydrolases, Adenosine Diphosphate, Kinetics, Mutagenesis, Site-Directed, biology.protein, Guanosine Triphosphate
Abstract

Tissue transglutaminase (tTG) exhibits a magnesium-dependent GTP/ATPase activity that is involved in the regulation of the cell cycle and cell receptor signaling. The portion of the molecule involved in GTP/ATP hydrolysis is unknown. We expressed and purified a series of C-terminal truncation mutants of human tTG as glutathione S-transferase fusion proteins (DeltaS538, DeltaE447, DeltaP345, DeltaC290, DeltaV228, and DeltaF185) to determine the effect on GTP/ATPase activity. The truncation of the C terminus did not change significantly the apparent Km value for either GTP or ATP. In contrast, the Kcat value for GTP was increased by 4.6- and 3-fold for the DeltaS538 and DeltaE447 mutants, respectively. The DeltaP345 mutant had the highest hydrolysis activity with a 34-fold increase. The hydrolysis activity then declined to 8.1-, 8.7-, and 1. 9-fold for the DeltaC290, DeltaV228, and DeltaF185 mutants, respectively. The Kcat for ATP changed in parallel with the GTPase results. Thin layer chromatography analysis of the hydrolysis reaction products revealed that ATP was rapidly converted to ADP followed by a much slower conversion of ADP to AMP when incubated with wild type tTG or the DeltaP345 mutant. There was a substantial decrease in the calcium-dependent TGase activity when the last 149 amino acid residues were deleted from the C terminus. Less than 5% of the TGase activity was detected for the DeltaS538 and DeltaE447 mutants. In conclusion, we have located the ATP and GTP hydrolytic domain to amino acid residues 1-185. The C terminus functions to inhibit the expression of endogenous GTP/ATPase activity of tTG, and the potential role of the C terminus in modulating this activity is discussed.

Published
1996
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47. Human tissue transglutaminase is inhibited by pharmacologic and chemical acetylation

Author

Thung S, Lai, Christopher, Davies, and Charles S, Greenberg

Subjects
Models, Molecular, Transglutaminases, Aspirin, Molecular Structure, GTP-Binding Proteins, Humans, Succinimides, Acetylation, Protein Glutamine gamma Glutamyltransferase 2, Acetates, Enzyme Inhibitors, Article, Protein Structure, Tertiary
Abstract

Human tissue transglutaminase (TGM2) is implicated in the pathogenesis of several neurodegenerative disorders including Alzheimer's, Parkinson's and expanded polyglutamine (polyQ) diseases. TGM2 promotes formation of soluble and insoluble high molecular weight aggregates by catalyzing a covalent linkage between peptide-bound Q residues in polyQ proteins and a peptide-bound Lys residue. Therapeutic approaches to modulate the activity of TGM2 are needed to proceed with studies to test the efficacy of TGM2 inhibition in disease processes. We investigated whether acetylation of Lys-residues by sulfosuccinimidyl acetate (SNA) or aspirin (ASA) would alter the crosslinking activity of TGM2. Acetylation by either SNA and/or ASA resulted in a loss of90% of crosslinking activity. The Lys residues that were critical for inhibition were identified by mass spectrometry as Lys(444), Lys(468), and Lys(663). Hence, acetylation of Lys-residues may modulate the enzymatic function of TGM2 in vivo and offer a novel approach to treatment of TGM2 mediated disorders.

Published
2009

49. Identification of two GTP-independent alternatively spliced forms of tissue transglutaminase in human leukocytes, vascular smooth muscle, and endothelial cells

Author

Yusha Liu, Weidong Li, Thung-S. Lai, and Charles S. Greenberg

Subjects
Gene isoform, Intracellular Fluid, Umbilical Veins, Vascular smooth muscle, GTP', Tissue transglutaminase, Molecular Sequence Data, HL-60 Cells, Biology, Biochemistry, Article, Gene Expression Regulation, Enzymologic, Muscle, Smooth, Vascular, Cell Line, GTP-binding protein regulators, GTP-Binding Proteins, Genetics, Leukocytes, Humans, Protein Glutamine gamma Glutamyltransferase 2, Amino Acid Sequence, Molecular Biology, Aorta, Transglutaminases, Alternative splicing, HEK 293 cells, Endothelial Cells, Transfection, Molecular biology, Isoenzymes, Alternative Splicing, biology.protein, Guanosine Triphosphate, Biotechnology
Abstract

Tissue transglutaminase (tTG) is a multifunctional enzyme with transglutaminase crosslinking (TGase), GTP binding, and hydrolysis activities that play a role in many different disorders. We identified, characterized, and investigated the function and stability of two alternatively spliced forms of tTG using biochemical, cellular, and molecular biological approaches. Using a human aortic vascular smooth muscle cells (VSMC) cDNA library, we identified two cDNAs encoding C-terminal truncated forms, tTGV1 and tTGV2. tTGV1,2 mRNAs were synthesized by a rare splicing event using alternate splice sites within exons 12 and 13 of the tTG gene, respectively. Quantitative PCR and immunoblotting demonstrated that there was unique expression and localization of tTGV1,2 compared with tTG in human umbilical vein endothelial cells (HUVECs), VSMC, and leukocytes. The loss of C-terminal 52 amino acid residues (AAs) in tTGV1,2 altered GTP binding, enhanced GTP hydrolysis, rendered the variants insensitive to GTP inhibition, and resulted in

Published
2007

50. Abstract 5192: TGM-2 mediated downregulation of fibronectin during TGFb-induced epithelial-mesenchymal transition in lung cancer NCI-H358 cells

Author

Charles S. Greenberg, Thung S. Lai, Robert M. Gemmill, Harry A. Drabkin, and Pin-Tsen Lin

Subjects
A549 cell, Cancer Research, biology, Chemistry, Tissue transglutaminase, Mesenchymal stem cell, Cancer, medicine.disease, Metastasis, Fibronectin, Oncology, Downregulation and upregulation, biology.protein, medicine, Cancer research, Epithelial–mesenchymal transition
Abstract

The epithelial to mesenchymal transition (EMT), which converts epithelial cells into an elongated, motile, and invasive phenotype, is considered to be a critical step in the dissemination of tumor cells. During EMT, the loss of E-cadherin (ECad) and upregulation of N-cadherin (NCad) or fibronectin (FN) have been most frequently described. FN binds integrin Alpha5 and is known for its upregulation in aggressive tumor cells. In addition, FN binds tissue transglutaminase (TGM-2) with high affinity (∼in nM) and plays a role in TGM-2 secretion. TGM-2, a multifunctional enzyme with transamidation or crosslinking, and GTP/ATP binding activities, is up-regulated in various malignant diseases, including lung cancer. In breast, cervical and ovarian cancers, TGM-2 has been shown to play a role in chemotherapy resistance and tumor metastasis during induction of EMT. TGM-2 overexpression results in the loss of epithelial features, up-regulation of mesenchymal markers, increased migration and invasion, and up-regulation of transcriptional repressors (e.g., ZEB1/2, Snail) known to mediate the EMT process. However, most of these studies were performed in aggressive tumor cells. In this study, we investigated the role of TGM-2 in TGFbeta-induced EMT process using NSCLC H358 cells. H358 cells express high levels of epithelial genes and are relatively resistant to TGFbeta induced EMT when compared to A549 cells. Particularly, H358 expresses barely detectable TGM-2 and FN. To investigate the role of TGM-2 during TGFbeta induced EMT, we constructed three isogenic cell lines with doxycycline (Dox)-inducible TGM-2 or C277A (an inactive mutant of TGM-2 with no transamidating activity) using InVitrogen's Flp-in TRex system. We found continuing treatment of 10 ng/ml TGFbeta for 6 days inducing H358 flp-in (vector control) cells to mescenchymal phenotype as demonstrated by the disappearance of Ecad, and the increased expression of NCad and FN. Under the same condition, Dox inducible TGM-2 and C277A facilitate the disappearance of Ecad, and Occludin and the appearance of Ncad. However, the expression of FN was undetectable in H358/TGM-2 and H358/C277A cells. As a result, H358/TGM-2 and H358/C277A remained localized and failed to migrate as demonstrated by a scratch wound healing assay. Seahorse mitochondria stress assay also demonstrated H358/TGM-2 and H358/C277A utilize more oxidative phosphorylation pathway than glycolytic pathway when compared with H358/flp-in, an indication of shifting cells to more normal phenotype. In summary, overexpression of TGM-2 (or inactive C277A mutant) inhibited the expression of FN and resulted in a less migratory H358 cells. Our results demonstrated that the role of TGM-2 during EMT in less aggressive epithelial cells such as H358 is different from its role in promoting EMT in other aggressive tumor cell; the suppression of FN might be a critical factor. Note: This abstract was not presented at the meeting. Citation Format: Thung S. Lai, Pin-Tsen Lin, Charles S. Greenberg, Harry A. Drabkin, Robert Gemmill. TGM-2 mediated downregulation of fibronectin during TGFb-induced epithelial-mesenchymal transition in lung cancer NCI-H358 cells. [abstract]. In: Proceedings of the 106th Annual Meeting of the American Association for Cancer Research; 2015 Apr 18-22; Philadelphia, PA. Philadelphia (PA): AACR; Cancer Res 2015;75(15 Suppl):Abstract nr 5192. doi:10.1158/1538-7445.AM2015-5192

Published
2015
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