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1. Loss of liver function in chronic liver disease: An identity crisis

Author

Berasain, C. (Carmen), Arechederra, M. (María), Argemí, J. (Josepmaria), Fernández-Barrena, M.G. (Maite G.), and Avila, M.A. (Matías Antonio)

Subjects
Hepatocellular differentiation, Molecular therapies, mRNA splicing factors, Chronic liver disease, Transcriptional reprogramming, Transcription factors
Abstract

Adult hepatocyte identity is constructed throughout embryonic development and fine-tuned after birth. A multinodular network of transcription factors, along with pre-mRNA splicing regulators, define the transcriptome, which encodes the proteins needed to perform the complex metabolic and secretory functions of the mature liver. Transient hepatocellular dedifferentiation can occur as part of the regenerative mechanisms triggered in response to acute liver injury. However, persistent downregulation of key identity genes is now accepted as a strong determinant of organ dysfunction in chronic liver disease, a major global health burden. Therefore, the identification of core transcription factors and splicing regulators that preserve hepatocellular phenotype, and a thorough understanding of how these networks become disrupted in diseased hepatocytes, is of high clinical relevance. In this context, we review the key players in liver differentiation and discuss in detail critical factors, such as HNF4α, whose impairment mediates the breakdown of liver function. Moreover, we present compelling experimental evidence demonstrating that restoration of core transcription factor expression in a chronically injured liver can reset hepatocellular identity, improve function and ameliorate structural abnormalities. The possibility of correcting the phenotype of severely damaged and malfunctional livers may reveal new therapeutic opportunities for individuals with cirrhosis and advanced liver disease.

Published
2023

2. SLU7: a new hub of gene expression regulation-from epigenetics to protein stability in health and disease

Author

Gárate-Rascón, M. (María), Recalde, M. (Miriam), Rojo-González, C. (Carla), García-Fernández-de-Barrena, M. (Maite), Avila, M.A. (Matías Antonio), Arechederra, M. (María), and Berasain, C. (Carmen)

Subjects
Genomic stability, Differentiation, Epigenetics, Gene expression, Cell cycle, Stress, Liver pathophysiology, Transcription, Alternative splicing, Cancer
Abstract

SLU7 (Splicing factor synergistic lethal with U5 snRNA 7) was first identified as a splicing factor necessary for the correct selection of 3 ' splice sites, strongly impacting on the diversity of gene transcripts in a cell. More recent studies have uncovered new and non-redundant roles of SLU7 as an integrative hub of different levels of gene expression regulation, including epigenetic DNA remodeling, modulation of transcription and protein stability. Here we review those findings, the multiple factors and mechanisms implicated as well as the cellular functions affected. For instance, SLU7 is essential to secure liver differentiation, genome integrity acting at different levels and a correct cell cycle progression. Accordingly, the aberrant expression of SLU7 could be associated with human diseases including cancer, although strikingly, it is an essential survival factor for cancer cells. Finally, we discuss the implications of SLU7 in pathophysiology, with particular emphasis on the progression of liver disease and its possible role as a therapeutic target in human cancer.

Published
2022

3. Activation of the unfolded protein response (UPR) is associated with cholangiocellular injury, fibrosis and carcinogenesis in an experimental model of fibropolycystic liver disease

Author

Chen, C. (Chaobo), Wu, H. (Hanghang), Ye, H. (Hui), Tortajada, A. (Agustín), Rodriguez-Perales, S. (Sandra), Torres-Ruiz, R. (Raúl), Vidal, A. (August), Peligros, M.I. (María Isabel), Reissing, J. (Johanna), Bruns, T. (Tony), Zheng, K. (Kang), Mohamed, M.R. (Mohamed Ramadan), Lujambio, A. (Amaya), Iraburu-Elizalde, M.J. (María José), Colyn, L. (Leticia), Latasa, M.U. (María Ujué), Arechederra, M. (María), Fernández-Barrena, M.G. (Maite G.), Berasain, C. (Carmen), Vaquero, J. (Javier), Bañares, R. (Rafael), Nelson, L.J. (Leonard J.), Trautwein, C. (Christian), Davis, R.J. (Roger J.), Martínez-Naves, E. (Eduardo), Nevzorova, Y. (Yulia), Villanueva, A. (Alberto), Avila, M.A. (Matías Antonio), and Cubero, F.J. (Francisco Javier)

Subjects
c-Jun N-terminal kinases (JNK), Cholangiocarcinoma (CCA), CM272, Endoplasmic reticulum (ER), Stressthioacetamide (TAA), Fibropolycystic liver disease
Abstract

Polycystic liver disease (PLD) is a group of rare disorders that result from structural changes in the biliary tree development in the liver. In the present work, we studied alterations in molecular mechanisms and signaling pathways that might be responsible for these pathologies. We found that activation of the unfolded protein response, a process that occurs in response to an accumulation of unfolded or misfolded proteins in the lumen of the endoplasmic reticulum, as well as the scarring of the liver tissue, contribute to the pathogenesis of PLD and the development of cancer. As a preclinical animal model we have used mutant mice of a specific signaling pathway, the c-Jun N-terminal kinase 1/2 (Jnk1/2). These mice resemble a perfect model for the study of PLD and early cancer development.

Published
2022

5. Epigenetic Mechanisms in Gastric Cancer: Potential New Therapeutic Opportunities

Author

Canale, M. (Matteo), Casadei-Gardini, A. (Andrea), Ulivi, P. (Paola), Arechederra, M. (María), Berasain, C. (Carmen), Lollini, P.L. (Pier-Luigi), Fernández-Barrena, M.G. (Maite G.), Avila, M.A. (Matías Antonio), Canale M., Casadei-Gardini A., Ulivi P., Arechederra M., Berasain C., Lollini P.-L., Fernandez-Barrena M.G., Avila M.A., Canale, M., Casadei Gardini, A., Ulivi, P., Arechederra, M., Berasain, C., Lollini, P. -L., Fernandez-Barrena, M. G., and Avila, M. A.

Subjects
Epigenetic therapie, Epigenetic therapies, Epigenetic mechanisms, gastric cancer, Stomach, epigenetic mechanisms, Review, DNA Methylation, Epigenesis, Genetic, epigenetic therapies, Gene Expression Regulation, Neoplastic, lcsh:Chemistry, lcsh:Biology (General), lcsh:QD1-999, Stomach Neoplasms, Epigenetic mechanism, Humans, Gastric cancer, lcsh:QH301-705.5
Abstract

Gastric cancer (GC) is one of the deadliest malignancies worldwide. Complex disease heterogeneity, late diagnosis, and suboptimal therapies result in the poor prognosis of patients. Besides genetic alterations and environmental factors, it has been demonstrated that alterations of the epigenetic machinery guide cancer onset and progression, representing a hallmark of gastric malignancies. Moreover, epigenetic mechanisms undergo an intricate crosstalk, and distinct epigenomic profiles can be shaped under different microenvironmental contexts. In this scenario, targeting epigenetic mechanisms could be an interesting therapeutic strategy to overcome gastric cancer heterogeneity, and the efforts conducted to date are delivering promising results. In this review, we summarize the key epigenetic events involved in gastric cancer development. We conclude with a discussion of new promising epigenetic strategies for gastric cancer treatment.

Published
2020

6. Recent advances in alcohol-related liver disease (ALD): summary of a Gut roundtable meeting

Author

Avila, M.A. (Matías Antonio), Dufour, J.F. (Jean-Francois), Gerbes, A. (Alexander), Zoulim, F. (Fabien), Bataller, R. (Ramón), Burra, P. (Patrizia), Cortez-Pinto, H. (Helena), Gao, B. (Bin), Gilmore, I. (Ian), Mathurin, P. (Philippe), Moreno, C. (Christophe), Poznyak, V. (Vladimir), Schnabl, B. (Bernd), Szabo, G. (Gyongyi), Thiele, M. (Maja), and Thursz, M.R. (Mark R.)

Subjects
Alcohol use disorder, Alcohol-related liver disease, Steatosis, Cirrhosis, The gut-liver axis, Acute on chronic liver failure, Alcohol consumption, Alcoholic hepatitis, Fibrosis, Liver transplant, Animal modelsTherapeutic targets
Abstract

Alcohol-related liver disease (ALD), which includes a range of disorders of different severity and is one of the most prevalent types of liver disease worldwide, has recently regained increased attention. Among other reasons, the realisation that any alcohol intake, regardless of type of beverage represents a health risk, and the new therapeutic strategies tested in recently published or undergoing clinical trials spur scientific interest in this area. In April 2019, Gut convened a round table panel of experts during the European Association for the Study of the Liver (EASL) International Liver Congress (ILC) in Vienna to discuss critical and up-to-date issues and clinical trial data regarding ALD, its epidemiology, diagnosis, management, pathomechanisms, possible future treatments and prevention. This paper summarises the discussion and its conclusions.

Published
2020

7. Epigenetics in liver fibrosis: could HDACs be a therapeutic target?

Author

Claveria-Cabello, A. (Alex), Colyn, L. (Leticia), Arechederra, M. (María), Urman, J.M. (Jesús M.), Berasain, C. (Carmen), Avila, M.A. (Matías Antonio), and Fernández-Barrena, M.G. (Maite G.)

Subjects
Histone deacetylases, Liver fibrosis, Precision medicine, Epigenetics
Abstract

Chronic liver diseases (CLD) represent a worldwide health problem. While CLDs may have diverse etiologies, a common pathogenic denominator is the presence of liver fibrosis. Cirrhosis, the end-stage of CLD, is characterized by extensive fibrosis and is markedly associated with the development of hepatocellular carcinoma. The most important event in hepatic fibrogenesis is the activation of hepatic stellate cells (HSC) following liver injury. Activated HSCs acquire a myofibroblast-like phenotype becoming proliferative, fibrogenic, and contractile cells. While transient activation of HSCs is part of the physiological mechanisms of tissue repair, protracted activation of a wound healing reaction leads to organ fibrosis. The phenotypic changes of activated HSCs involve epigenetic mechanisms mediated by non-coding RNAs (ncRNA) as well as by changes in DNA methylation and histone modifications. During CLD these epigenetic mechanisms become deregulated, with alterations in the expression and activity of epigenetic modulators. Here we provide an overview of the epigenetic alterations involved in fibrogenic HSCs transdifferentiation with particular focus on histones acetylation changes. We also discuss recent studies supporting the promising therapeutic potential of histone deacetylase inhibitors in liver fibrosis.

Published
2020

8. Loss of c-Jun N-terminal kinase 1 and 2 function in liver epithelial cells triggers biliary hyperproliferation resembling cholangiocarcinoma

Author

Cubero, F.J. (Francisco Javier), Mohamed, M.R. (Mohamed Ramadan), Woitok, M.M. (Marius Maximilian), Zhao, G. (Gang), Hatting, M. (Maximilian), Nevzorova, Y. (Yulia), Chen, C. (Chaobo), Haybaeck, J. (Johannes), Bruin, A. (Alain) de, Avila, M.A. (Matías Antonio), Boekschoten, M.V. (Mark V.), Davis, R.J. (Roger J.), and Trautwein, C. (Christian)

Subjects
Cholangiocarcinoma, c-Jun N-terminal kinases, Therapeutic potential, Cell-type-specific role
Abstract

Targeted inhibition of the c-Jun N-terminal kinases ( JNKs) has shown therapeutic potential in intrahepatic cholangiocarcinoma (CCA)-related tumorigenesis. However, the cell-type-specific role and mechanisms triggered by JNK in liver parenchymal cells during CCA remain largely unknown. Here, we aimed to investigate the relevance of JNK1 and JNK2 function in hepatocytes in two different models of experimental carcinogenesis, the dethylnitrosamine (DEN) model and in nuclear factor kappa B essential modulator (NEMO)hepatocyte-specific knockout (Δhepa) mice, focusing on liver damage, cell death, compensatory proliferation, fibrogenesis, and tumor development. Moreover, regulation of essential genes was assessed by reverse transcription polymerase chain reaction, immunoblottings, and immunostainings. Additionally, specific Jnk2 inhibition in hepatocytes of NEMOΔhepa/JNK1Δhepa mice was performed using small interfering (si) RNA (siJnk2) nanodelivery. Finally, active signaling pathways were blocked using specific inhibitors. Compound deletion of Jnk1 and Jnk2 in hepatocytes diminished hepatocellular carcinoma (HCC) in both the DEN model and in NEMOΔhepa mice but in contrast caused massive proliferation of the biliary ducts. Indeed, Jnk1/2 deficiency in hepatocytes of NEMOΔhepa (NEMOΔhepa/JNKΔhepa) animals caused elevated fibrosis, increased apoptosis, increased compensatory proliferation, and elevated inflammatory cytokines expression but reduced HCC. Furthermore, siJnk2 treatment in NEMOΔhepa/JNK1Δhepa mice recapitulated the phenotype of NEMOΔhepa/JNKΔhepa mice. Next, we sought to investigate the impact of molecular pathways in response to compound JNK deficiency in NEMOΔhepa mice. We found that NEMOΔhepa/JNKΔhepa livers exhibited overexpression of the interleukin-6/signal transducer and activator of transcription 3 pathway in addition to epidermal growth factor receptor (EGFR)-rapidly accelerated fibrosarcoma (Raf )-mitogen-activated protein kinase kinase (MEK)-extracellular signal-regulated kinase (ERK) cascade. The functional relevance was tested by administering lapatinib, which is a dual tyrosine kinase inhibitor of erythroblastic oncogene B-2 (ErbB2) and EGFR signaling, to NEMOΔhepa/JNKΔhepa mice. Lapatinib effectively inhibited cystogenesis, improved transaminases, and effectively blocked EGFR-Raf-MEK-ERK signaling. Conclusion: We define a novel function of JNK1/2 in cholangiocyte hyperproliferation. This opens new therapeutic avenues devised to inhibit pathways of cholangiocarcinogenesis.

Published
2020

9. Hepatocellular carcinoma: updates in pathogenesis, detection and treatment

Author

Martinez-Chantar, M.L. (María Luz), Avila, M.A. (Matías Antonio), and Lu, S.C. (Shelly C.)

Subjects
Immune checkpoint inhibitors, Risk factors, Liquid biopsy, Hepatocellular carcinoma, Molecular mechanisms, Multikinase inhibitors, Early diagnosis
Abstract

Hepatocellular carcinoma (HCC) is the most frequent primary liver cancer and the second most common cause of cancer mortality worldwide [1]. The prognosis of HCC patients is very poor. The rates of HCC incidence and mortality are almost equivalent [2] and have increased across most countries over the past three decades [3]. HCC development is closely associated with the presence of chronic liver disease and cirrhosis, albeit the risk factors underlying this condition vary geographically. Hepatitis B virus (HBV) infection and aflatoxin B1 exposure are predominant risk factors in Asia and Africa, while hepatitis C virus (HCV) infection and alcohol consumption are the main risk factors in Europe, the USA and Japan [3,4,5]. Non-alcoholic fatty liver disease (NAFLD) is currently the most prevalent liver disease worldwide, and approximately 60% of biopsied NAFLD patients have non-alcoholic steatohepatitis (NASH) [3]. Importantly, patients with NASH are at high risk of developing HCC even without presenting established cirrhosis [6]. With widespread HBV vaccination and the advent of direct-acting antiviral drugs for HCV infection, NAFLD and associated conditions such as diabetes and obesity are emerging as major global risk factors for HCC. In view of the dismal prognosis of HCC patients, implementing preventive strategies would be an ideal approach to quell the incidence of the disease. Obvious interventions include advocating HBV vaccination in endemic regions, achieving HCV eradication with direct-acting antivirals, promoting healthy nutrition and weight reduction, improving diabetes control, and avoiding excessive alcohol consumption. Still, the implementation of these measures is not always feasible.

Published
2020

10. Dual Pharmacological Targeting of HDACs and PDE5 Inhibits Liver Disease Progression in a Mouse Model of Biliary Inflammation and Fibrosis

Author

Claveria-Cabello, A. (Alex), Colyn, L. (Leticia), Uriarte, I. (Iker), Latasa, M.U. (María Ujué), Arechederra, M. (María), Herranz, J.M. (José M.), Alvarez-Asiain, L. (Laura), Urman, J.M. (Jesús M.), Martinez-Chantar, M.L. (María Luz), Banales, J.M. (Jesús M.), Sangro, B. (Bruno), Rombouts, K. (Krista), Oyarzabal, J. (Julen), Marin, J.J.G (Jose J.G.), Berasain, C. (Carmen), Avila, M.A. (Matías Antonio), and García-Fernández-de-Barrena, M. (Maite)

Subjects
cGMP, Histone deacetylases, HDAC inhibitor, Liver fibrosis, Precision medicine, Phosphodiesterase inhibitor, Hepatobiliary carcinogenesis
Abstract

Liver fibrosis, a common hallmark of chronic liver disease (CLD), is characterized by the accumulation of extracellular matrix secreted by activated hepatic fibroblasts and stellate cells (HSC). Fibrogenesis involves multiple cellular and molecular processes and is intimately linked to chronic hepatic inflammation. Importantly, it has been shown to promote the loss of liver function and liver carcinogenesis. No effective therapies for liver fibrosis are currently available. We examined the anti-fibrogenic potential of a new drug (CM414) that simultaneously inhibits histone deacetylases (HDACs), more precisely HDAC1, 2, and 3 (Class I) and HDAC6 (Class II) and stimulates the cyclic guanosine monophosphate (cGMP)-protein kinase G (PKG) pathway activity through phosphodiesterase 5 (PDE5) inhibition, two mechanisms independently involved in liver fibrosis. To this end, we treated Mdr2-KO mice, a clinically relevant model of liver inflammation and fibrosis, with our dual HDAC/PDE5 inhibitor CM414. We observed a decrease in the expression of fibrogenic markers and collagen deposition, together with a marked reduction in inflammation. No signs of hepatic or systemic toxicity were recorded. Mechanistic studies in cultured human HSC and cholangiocytes (LX2 and H69 cell lines, respectively) demonstrated that CM414 inhibited pro-fibrogenic and inflammatory responses, including those triggered by transforming growth factor β (TGFβ). Our study supports the notion that simultaneous targeting of pro-inflammatory and fibrogenic mechanisms controlled by HDACs and PDE5 with a single molecule, such as CM414, can be a new disease-modifying strategy.

Published
2020

11. A novel serum metabolomic profile for the differential diagnosis of distal cholangiocarcinoma and pancreatic ductal adenocarcinoma

Author

Macias, R. (Rocío), Muñoz-Bellvis, L. (Luis), Sánchez-Martín, A. (Anabel), Arretxe, A. (Anere), Martínez-Arranz, I. (Ibon), Lapitz, A. (Ainhoa), Gutiérrez, M.L. (María Laura), Lacasta, A. (Adelaida), Alonso, C. (Cristina), González, L.M. (Luis M.), Avila, M.A. (Matías Antonio), Martinez-Chantar, M.L. (María Luz), Castro, R.E. (Rui E.), Bujanda, L. (Luis), Banales, J.M. (Jesús M.), and Marin, J.J.G (Jose J.G.)

Subjects
Tumor non-invasive biomarker, Metabolites, Differential diagnosis, Pancreatic cancer, Biliary cancer
Abstract

The diagnosis of adenocarcinomas located in the pancreas head, i.e., distal cholangiocarcinoma (dCCA) and pancreatic ductal adenocarcinoma (PDAC), constitutes a clinical challenge because they share many symptoms, are not easily distinguishable using imaging techniques and accurate biomarkers are not available. Searching for biomarkers with potential usefulness in the differential diagnosis of these tumors, we have determined serum metabolomic profiles in healthy controls and patients with dCCA, PDAC or benign pancreatic diseases (BPD). Ultra-high-performance liquid chromatography coupled to mass spectrometry (UHPLC-MS) analysis was performed in serum samples from dCCA (n = 34), PDAC (n = 38), BPD (n = 42) and control (n = 25) individuals, divided into discovery and validation cohorts. This approach permitted 484 metabolites to be determined, mainly lipids and amino acids. The analysis of the results led to the proposal of a logistic regression model able to discriminate patients with dCCA and PDAC (AUC value of 0.888) based on the combination of serum levels of nine metabolites (acylcarnitine AC(16:0), ceramide Cer(d18:1/24:0), phosphatidylcholines PC(20:0/0:0) and PC(O-16:0/20:3), lysophosphatidylcholines PC(20:0/0:0) and PC(0:0/20:0), lysophosphatidylethanolamine PE(P-18:2/0:0), and sphingomyelins SM(d18:2/22:0) and SM(d18:2/23:0)) and CA 19-9. In conclusion, we propose a novel specific panel of serum metabolites that can help in the differential diagnosis of dCCA and PDAC. Further validation of their clinical usefulness in prospective studies is required.

Published
2020

12. Targeting CCL2/CCR2 in tumor-infiltrating macrophages: a tool emerging out of the box against hepatocellular carcinoma

Author

Avila, M.A. (Matías Antonio) and Berasain, C. (Carmen)

Subjects
Cancer-related mortality, Hepatocellular carcinoma (HCC), Liver tumor, neoplasms, digestive system diseases
Abstract

Hepatocellular carcinoma (HCC) is the most frequent primary liver tumor and a leading cause of cancer-related mortality. Unfortunately, the majority of HCC patients present with advanced disease, when locoregional curative strategies are no longer applicable. On the other hand, early, HCCs proved to be resistant to conventional chemotherapies, and drugs targeting specific growth factor signaling pathways tested over the past decade have not succeeded in clinical trials. The molecular heterogeneity of HCCs and the lack of biomarker-based patient stratification strategies may underlie the failure of most of these trials. HCCs usually develop on a background of chronic liver injury and regeneration, inflammation, and fibrosis, features that promote tumor hypervascularity, the other histologic hallmark of this neoplasia. Indeed, the fibrotic and immune microenvironment plays a key role in pathogenic angiogenesis and HCC development and progression. This tenet is supported not only by experimental evidence, but also by the fact that the only therapeutic agents showing clinical efficacy in advanced HCC are those directed toward the interaction of HCC with its microenvironment (ie, anti-angiogenic multikinase inhibitors such as sorafenib, and immune checkpoint inhibitors such as antibodies targeting programmed cell death receptor 1 and its ligand).

Published
2019

13. Causes of hOCT1-dependent cholangiocarcinoma resistance to sorafenib and sensitization by tumor-selective gene therapy

Author

Lozano, E. (Elisa), Macias, R. (Rocío), Monte, M.J. (María J.), Asensio, M. (Maitane), Carmen, S. (Sofia) del, Sanchez-Vicente, L. (Laura), Alonso-Peña, M. (Marta), Al-Abdulla, R. (Ruba), Munoz-Garrido, P. (Patricia), Satriano, L. (Letizia), O’Rourke, C.J. (Colm J.), Banales, J.M. (Jesús M.), Avila, M.A. (Matías Antonio), Martinez-Chantar, M.L. (María Luz), Andersen, J.B. (Jesper B.), Briz, O. (Oscar), and Marin, J.J.G (Jose J.G.)

Subjects
Mechanisms of chemoresistance, Multi-tyrosine, Cholangiocarcinoma (CCA), Several cancers
Abstract

Although the multi-tyrosine kinase inhibitor sorafenib is useful in the treatment of several cancers, cholangiocarcinoma (CCA) is refractory to this drug. Among other mechanisms of chemoresistance, impaired uptake through human organic cation transporter type 1 (hOCT1) (gene SLC22A1) has been suggested. Here we have investigated the events accounting for this phenotypic characteristic and have evaluated the interest of selective gene therapy strategies to overcome this limitation. Gene expression and DNA methylation of SLC22A1 were analyzed using intrahepatic (iCCA) and extrahepatic (eCCA) biopsies (Copenhagen and Salamanca cohorts; n = 132) and The Cancer Genome Atlas (TCGA)-CHOL (n = 36). Decreased hOCT1 mRNA correlated with hypermethylation status of the SLC22A1 promoter. Treatment of CCA cells with decitabine (demethylating agent) or butyrate (histone deacetylase inhibitor) restored hOCT1 expression and increased sorafenib uptake. MicroRNAs able to induce hOCT1 mRNA decay were analyzed in paired samples of TCGA-CHOL (n = 9) and Copenhagen (n = 57) cohorts. Consistent up-regulation in tumor tissue was found for miR-141 and miR-330. High proportion of aberrant hOCT1 mRNA splicing in CCA was also seen. Lentiviral-mediated transduction of eCCA (EGI-1 and TFK-1) and iCCA (HuCCT1) cells with hOCT1 enhanced sorafenib uptake and cytotoxic effects. In chemically induced CCA in rats, reduced rOct1 expression was accompanied by impaired sorafenib uptake. In xenograft models of eCCA cells implanted in mouse liver, poor response to sorafenib was observed. However, tumor growth was markedly reduced by cotreatment with sorafenib and adenoviral vectors encoding hOCT1 under the control of the BIRC5 promoter, a gene highly up-regulated in CCA. Conclusion: The reason for impaired hOCT1-mediated sorafenib uptake by CCA is multifactorial. Gene therapy capable of selectively inducing hOCT1 in tumor cells can be considered a potentially useful chemosensitization strategy to improve the response of CCA to sorafenib.

Published
2019

14. Dual targeting of histone methyltransferase G9a and DNMT1 for the treatment of experimental hepatocellular carcinoma

Author

Bárcena-Varela, M. (Marina), Avila, M.A. (Matías Antonio), and García-Fernández-de-Barrena, M. (Maite)

Subjects
Biología celular, Ciencias de la Salud::Microbiología y biología molecular [Materias Investigacion], Patología experimental, Ciencias de la Salud::Oncología [Materias Investigacion]
Abstract

Las modificaciones epigenéticas, como la metilación del ADN e histonas, cooperan funcionalmente para fomentar el crecimiento tumoral, incluido el carcinoma hepatocelular (HCC). La inhibición farmacológica de estos mecanismos puede abrir nuevas vías terapéuticas. El objetivo del trabajo desarrollado en la presente tesis doctoral fue determinar la eficacia terapéutica y el potencial mecanismo de acción de nuevos inhibidores duales de la histona-metiltransferasa G9a y la ADN-metiltransferasa 1 (DNMT1) en células HCC humanas y su interferencia con células fibrogénicas. Estos inhibidores han sido desarrollados en la propia Institución y sujetos a patente (EPOPatent application #14-382230.2-1462). La expresión de G9a y DNMT1, junto con la de su adaptador molecular UHRF1, se midió en muestras de HCC humanas (n = 268), tejidos peritumorales (n = 154) y líneas células de HCC (n = 32). Se evaluó el efecto de la inhibición individual y combinada de G9a y DNMT1 en el crecimiento de células HCC mediante enfoques farmacológicos y genéticos. La actividad de nuestro compuesto principal, CM-272, se examinó en células HCC bajo normoxia e hipoxia, células estelares hepáticas humanas y células LX2, y tumores de xenoinjerto formados por células HCC o células HCC + LX2 combinadas. Encontramos una sobreexpresión significativa y correlativa de G9a, DNMT1 y UHRF1 en HCC en asociación con un mal pronóstico. La inhibición farmacológica independiente de G9a y DNMT1 redujo sinérgicamente el crecimiento de las células HCC. CM-272 inhibió potentemente la proliferación de células HCC y LX2, y detuvo el crecimiento del tumor en xenoinjertos de HCC y HCC combinadas con LX2. CM-272 impidió la adaptación metabólica de las células HCC a la hipoxia, e indujo un fenotipo diferenciado en las células HCC y fibrogénicas. La expresión del gen supresor de tumores metabólicos fructosa-1,6-bifosfatasa (FBP1), reprimido epigenéticamente en el HCC, fue restaurada por CM-272. Como conclusión del trabajo, la inhibición combinada de G9a / DNMT1 con compuestos como CM-272 es una estrategia prometedora para el tratamiento del HCC. Nuestros hallazgos también subrayan el potencial de la terapia de diferenciación en el HCC.

Published
2018

15. Estudio del papel del FGF15/19 en la respuesta a la dieta rica en grasa. Desarrollo de una nueva molécula hepatoprotectora y pro-regenerativa basada en el FGF19

Author

Álvarez-Sola, G. (Gloria), Avila, M.A. (Matías Antonio), and Uriarte, I. (Iker)

Subjects
Ciencias de la vida::Citología, biología celular [Materias Investigacion], Ciencias de la vida::Biología [Materias Investigacion]
Abstract

Los objetivos de esta tesis doctoral son: 1) Evaluar el papel del FGF15/19 endógeno en respuesta a la administración de una dieta rica en grasa. 2) Desarrollar una nueva proteína basada en la fusión del FGF19 y la ApoA-I que aumente la vida media y el tropismo hepático. 3) Evaluar la actividad biológica de la nueva proteína de fusión, así como su posible aplicación en modelos experimentales en los que la regeneración hepática esté impedida.

Published
2018

16. Post-translational deregulation of YAP1 is genetically controlled in rat liver cancer and determines the fate and stem-like behavior of the human disease

Author

Simile, M.M. (María M.), Latte, G. (Gavinella), Demartis, M.I. (María I.), Brozzetti, S. (Stefania), Calvisi, D.F. (Diego F.), Porcu, A. (Alberto), Feo, C.F. (Claudio F.), Seddaiu, M.A. (María A.), Daino, L. (Lucia), Berasain, C. (Carmen), Tomasi, M.L. (María L.), Avila, M.A. (Matías Antonio), Feo, F. (Francesco), and Pascale, R.M. (Rosa M.)

Subjects
Hepatocarcinogenesis, Progression, Yap targets, Stem cells, Gene expression profile, neoplasms, digestive system diseases
Abstract

Previous studies showed that YAP1 is over-expressed in hepatocellular carcinoma (HCC). Here we observed higher expression of Yap1/Ctgf axis in dysplastic nodules and HCC chemically-induced in F344 rats, genetically susceptible to hepatocarcinogenesis, than in lesions induced in resistant BN rats. In BN rats, highest increase in Yap1- tyr357, p73 phosphorylation and Caspase 3 cleavage occurred. In human HCCs with poorer prognosis (< 3 years survival after partial liver resection, HCCP), levels of YAP1, CTGF, 14–3–3, and TEAD proteins, and YAP1-14-3-3 and YAP1-TEAD complexes were higher than in HCCs with better outcome (> 3 years survival; HCCB). In the latter, higher levels of phosphorylated YAP1-ser127, YAP1-tyr357 and p73, YAP1 ubiquitination, and Caspase 3 cleavage occurred. Expression of stemness markers NANOG, OCT-3/4, and CD133 were highest in HCCP and correlated with YAP1 and YAP1-TEAD levels. In HepG2, Huh7, and Hep3B cells, forced YAP1 over-expression led to stem cell markers expression and increased cell viability, whereas inhibition of YAP1 expression by specific siRNA, or transfection of mutant YAP1 which does not bind to TEAD, induced opposite alterations. These changes were associated, in Huh7 cells transfected with YAP1 or YAP1 siRNA, with stimulation or inhibition of cell migration and invasivity, respectively. Furthermore, transcriptome analysis showed that YAP1 transfection in Huh7 cells induces over-expression of genes involved in tumor stemness. In conclusion, Yap1 post-translational modifications favoring its ubiquitination and apoptosis characterize HCC with better prognosis, whereas conditions favoring the formation of YAP1-TEAD complexes are associated with aggressiveness and acquisition of stemness features by HCC cells.

Published
2016

17. Función de la metaloproteasa de matriz 10 (MMP10) en la regeneración hepática y la carcinogénesis

Author

García-Irigoyen, O. (Oihane), Berasain, C. (Carmen), and Avila, M.A. (Matías Antonio)

Subjects
Biología molecular, Biología celular
Abstract

Upon tissue injury, the liver mounts a potent reparative and regenerative response. This wound-healing response involves a transitory substitution of damaged hepatic parenchyma by extracellular matrix (ECM) that subsequently needs to be removed when liver tissue is regenerated. A role for proteases, including matrix metalloproteinases (MMPs), in this process is increasingly recognized, acting as regulatory molecules by the selective proteolytic activation of growth factors and cell surface receptors in addition to their ability to degrade ECM constituents. Moreover, MMPs also have been demonstrated to participate in cancer by promoting a protumorigenic microenvironment. We have evaluated the hepatic expression and function of MMP10 (stromelysin-2) in mouse models of liver wound-healing and regeneration, in human hepatocellular carcinoma (HCC) and in diethylnitrosamine (DEN)-induced mouse hepatocarcinogenesis. The role of MMP10 was evaluated by comparing the response of wild type (MMP10+/+) and MMP10-deficient (MMP10-/-) mice to the different experimental models. Mouse MMP10 hepatic expression was readily induced in different injury and regeneration models: two-thirds partial hepatectomy (PH), bile duct ligation (BDL) and carbon tetrachloride (CCl4) acute administration. MMP10 protein was detected in hepatocytes, cholangiocytes and macrophages. MMP10 was also induced in human and murine HCC tissues and cells. In cultured liver epithelial cells, MMP10 expression was additively induced by transforming growth factor-β and epidermal growth factor receptor ligands. TLR4 ligands also stimulated its expression in macrophages. Lack of MMP10 resulted in increased liver injury and fibrogenesis, impaired resolution of necrotic areas and defective turnover of fibrin(ogen) and fibronectin upon PH, BDL and CCl4 administration. On the other hand, in the DEN model, MMP10-/- mice showed less HCC incidence, smaller histological lesions, reduced tumor vascularization, and less lung metastases. Importantly, expression of the protumorigenic C-X-C chemokine receptor 4 (CXCR4) was reduced in those mice. A MMP10 overexpressing human HCC cell line was generated. These HCC cells had increased CXCR4 expression and showed enhanced migratory capacity, and the pharmacological inhibition of CXCR4 reduced MMP10-stimulated cell migration. MMP10 expression in HCC cells was induced by hypoxia and the CXCR4 ligand stroma-derived factor 1 (SDF1), through the ERK1/2 pathway, involving an activator protein 1 site in MMP10 gene promoter. Conclusions: MMP10 expression is induced during mouse liver injury and participates in the hepatic wound-healing response, where the profibrinolytic activity of MMP10 may be essential in this hepatoprotective role. In contrast, MMP10 contributes to HCC development, participating in tumor angiogenesis, growth, and dissemination. We identified a new reciprocal crosstalk between MMP10 and the CXCR4/SDF1 axis contributing to HCC progression and metastasis.

Published
2015

18. Estudio del papel fisiopatológico de Slu7 en el hígado

Author

Elizalde, M. (María), Berasain, C. (Carmen), and Avila, M.A. (Matías Antonio)

Subjects
Oncología clínica, Procesos metabólicos, Ciencias de la vida [Materias Investigacion], Bioquímica molecular, Metabolismo humano
Abstract

A precise equilibrium between cellular differentiation and proliferation is fundamental for tissue homeostasis. Maintaining this balance is particularly important for the liver, a highly differentiated organ with systemic metabolic functions that is endowed with unparalleled regenerative potential. Carcinogenesis in the liver develops as the result of hepatocellular de-differentiation and uncontrolled proliferation. Here, we identified SLU7, which encodes a pre-mRNA splicing regulator that is inhibited in hepatocarcinoma, as a pivotal gene for hepatocellular homeostasis. SLU7 knockdown in human liver cells and mouse liver resulted in profound changes in pre-mRNA splicing and gene expression, leading to impaired glucose and lipid metabolism, refractoriness to key metabolic hormones, and reversion to a fetal-like gene expression pattern. Additionally, loss of SLU7 also increased hepatocellular proliferation and induced a switch to a tumor-like glycolytic phenotype. Slu7 governed the splicing and/or expression of multiple genes essential for hepatocellular differentiation, including serine/arginine-rich splicing factor 3 (Srsf3) and hepatocyte nuclear factor 4α (Hnf4α), and was critical for cAMP-regulated gene transcription. Together, out data indicate that SLU7 is central regulator of hepatocyte identity and quiescence.

Published
2014

19. Methylthioadenosine (MTA) inhibits melanoma cell proliferation and in vivo tumor growth

Author

Andreu-Perez, P. (Pedro), Hernandez-Losa, J. (Javier), Moline, T. (Teresa), Gil, R. (Rosa), Grueso, J. (Judit), Pujol, A. (Anna), Cortes, J. (Javier), Avila, M.A. (Matías Antonio), and Recio, J.A. (Juan A.)

Subjects
Cell Proliferation/drug effects, Skin Neoplasms/drug therapy, Melanoma/drug therapy, Adenosine/pharmacology, neoplasms, Antineoplastic Agents/pharmacology, Thionucleosides/pharmacology
Abstract

BACKGROUND: Melanoma is the most deadly form of skin cancer without effective treatment. Methylthioadenosine (MTA) is a naturally occurring nucleoside with differential effects on normal and transformed cells. MTA has been widely demonstrated to promote anti-proliferative and pro-apoptotic responses in different cell types. In this study we have assessed the therapeutic potential of MTA in melanoma treatment. METHODS: To investigate the therapeutic potential of MTA we performed in vitro proliferation and viability assays using six different mouse and human melanoma cell lines wild type for RAS and BRAF or harboring different mutations in RAS pathway. We also have tested its therapeutic capabilities in vivo in a xenograft mouse melanoma model and using variety of molecular techniques and tissue culture we investigated its anti-proliferative and pro-apoptotic properties. RESULTS: In vitro experiments showed that MTA treatment inhibited melanoma cell proliferation and viability in a dose dependent manner, where BRAF mutant melanoma cell lines appear to be more sensitive. Importantly, MTA was effective inhibiting in vivo tumor growth. The molecular analysis of tumor samples and in vitro experiments indicated that MTA induces cytostatic rather than pro-apoptotic effects inhibiting the phosphorylation of Akt and S6 ribosomal protein and inducing the down-regulation of cyclin D1. CONCLUSIONS: MTA inhibits melanoma cell proliferation and in vivo tumor growth particularly in BRAF mutant melanoma cells. These data reveal a naturally occurring drug potentially useful for melanoma treatment.

Published
2010

20. Oral methylthioadenosine administration attenuates fibrosis and chronic liver disease progression in Mdr2-/- mice

Author

Latasa, M.U. (María Ujué), Gil-Puig, C. (Carmen), García-Fernández-de-Barrena, M. (Maite), Rodriguez-Ortigosa, C.M. (Carlos M.), Banales, J.M. (Jesús M.), Urtasun, R. (Raquel), Goñi, S. (Saioa), Mendez, M. (Miriam), Arcelus, S. (Sara), Juanarena, N. (Nerea), Recio, J.A. (Juan A.), Lotersztajn, S. (Sophie), Prieto, J. (Jesús), Berasain, C. (Carmen), Corrales, F.J. (Fernando José), Lecanda, J. (Jon), and Avila, M.A. (Matías Antonio)

Subjects
P-Glycoproteins/genetics, Thionucleosides/administration & dosage, Liver Diseases/genetics, Liver Diseases/pathology, Adenosine/analogs & derivatives, Fibrosis/drug therapy
Abstract

BACKGROUND: Inflammation and fibrogenesis are directly related to chronic liver disease progression, including hepatocellular carcinoma (HCC) development. Currently there are few therapeutic options available to inhibit liver fibrosis. We have evaluated the hepatoprotective and anti-fibrotic potential of orally-administered 5'-methylthioadenosine (MTA) in Mdr2(-/-) mice, a clinically relevant model of sclerosing cholangitis and spontaneous biliary fibrosis, followed at later stages by HCC development. METHODOLOGY: MTA was administered daily by gavage to wild type and Mdr2(-/-) mice for three weeks. MTA anti-inflammatory and anti-fibrotic effects and potential mechanisms of action were examined in the liver of Mdr2(-/-) mice with ongoing fibrogenesis and in cultured liver fibrogenic cells (myofibroblasts). PRINCIPAL FINDINGS: MTA treatment reduced hepatomegaly and liver injury. α-Smooth muscle actin immunoreactivity and collagen deposition were also significantly decreased. Inflammatory infiltrate, the expression of the cytokines IL6 and Mcp-1, pro-fibrogenic factors like TGFβ2 and tenascin-C, as well as pro-fibrogenic intracellular signalling pathways were reduced by MTA in vivo. MTA inhibited the activation and proliferation of isolated myofibroblasts and down-regulated cyclin D1 gene expression at the transcriptional level. The expression of JunD, a key transcription factor in liver fibrogenesis, was also reduced by MTA in activated myofibroblasts. CONCLUSIONS/SIGNIFICANCE: Oral MTA administration was well tolerated and proved its efficacy in reducing liver inflammation and fibrosis. MTA may have multiple molecular and cellular targets. These include the inhibition of inflammatory and pro-fibrogenic cytokines, as well as the attenuation of myofibroblast activation and proliferation. Downregulation of JunD and cyclin D1 expression in myofibroblasts may be important regarding the mechanism of action of MTA. This compound could be a good candidate to be tested for the treatment of (biliary) liver fibrosis.

Published
2010

21. Influence of impaired liver methionine metabolism on the development of vascular disease and inflammation

Author

Avila, M.A. (Matías Antonio), Berasain, C. (Carmen), Prieto, J. (Jesús), Mato, J.M. (José María), Ruiz Garcia-Trevijano, E. (Elena), and Corrales, F.J. (Fernando José)

Subjects
Inflammation, Methionine, s-Adenosylhomocysteine, Liver, Cirrhosis, s-Adenosylmethionine, Homocysteine, Methylation
Abstract

Methionine (Met) metabolism involves the sequential formation of S-adenosylmethionine (SAM, the main biological methyl donor), S-adenosylhomocysteine (SAH) and homocysteine (Hcy). Hcy can be remethylated to Met or catabolized through the trans-sulfuration pathway. In mammals, as much as 48% of Met metabolism and up to 85% of all transmethylation reactions occur in the liver. These figures underscore the central role played by this organ in Met metabolism. Maintaining the homeostasis of this metabolic cycle has proved to be essential for the preservation of liver function up to the point of preventing its neoplastic transformation. However, an adequate hepatic metabolism of Met is not only important for the liver parenchymal cell. Evidence has accumulated over the past few years supporting the involvement of Met-derived metabolites in the triggering or attenuation of pathological processes with systemic implications. This is best illustrated by the fact that a deteriorated liver function has emerged as a major factor in the development of hyperhomocysteinemia. Elevated plasma levels of Hcy have been related to several disorders including cardiovascular and cerebrovascular diseases. On the other end, liver damage also leads to deficient SAM synthesis. Among the consequences of impaired SAM synthesis in liver tissue are the enhanced production of pro-inflammatory cytokines and mediators. In this review, we will address the mechanisms and consequences of abnormal Met metabolism in liver injury, the systemic implications of such impairment and finally the potential therapeutic interventions.

Published
2005

22. Methylthioadenosine

Author

Avila, M.A. (Matías Antonio), Ruiz Garcia-Trevijano, E. (Elena), Lu, S.C. (Shelly C.), Corrales, F.J. (Fernando José), and Mato, J.M. (José María)

Subjects
Methylthioadenosine, S-adenosylmethionine, MTAP
Abstract

5'-Methylthioadenosine (MTA) is a naturally occurring sulfur-containing nucleoside present in all mammalian tissues. MTA is produced from S-adenosylmethionine mainly through the polyamine biosynthetic pathway, where it behaves as a powerful inhibitory product. This compound is metabolized solely by MTA-phosphorylase, to yield 5-methylthioribose-1-phosphate and adenine, a crucial step in the methionine and purine salvage pathways, respectively. Abundant evidence has accumulated over time suggesting that MTA can affect cellular processes in many ways. MTA has been shown to influence numerous critical responses of the cell including regulation of gene expression, proliferation, differentiation and apoptosis. Although most of these responses have been observed at the pharmacological level, their specificity makes it tempting to speculate that endogenous MTA could play a regulatory role in the cell. Finally, observations carried out in models of liver damage and cancer demonstrate a therapeutic potential for MTA that deserves further consideration.

Published
2004

23. 5'-methylthioadenosine modulates the inflammatory response to endotoxin in mice and in rat hepatocytes

Author

Hevia, H. (Henar), Varela-Rey, M. (Marta), Corrales, F.J. (Fernando José), Berasain, C. (Carmen), Martinez-Chantar, M.L. (María Luz), Latasa, M.U. (María Ujué), Lu, S.C. (Shelly C.), Mato, J.M. (José María), Ruiz Garcia-Trevijano, E. (Elena), and Avila, M.A. (Matías Antonio)

Subjects
Thionucleosides/pharmacokinetics, Shock, Septic/drug therapy, Hepatocytes/immunology, Deoxyadenosines/pharmacokinetics, Anti-Inflammatory Agents/pharmacology, Hepatocytes/drug effects, Lipopolysaccharides/pharmacology
Abstract

5'-methylthioadenosine (MTA) is a nucleoside generated from S-adenosylmethionine (AdoMet) during polyamine synthesis. Recent evidence indicates that AdoMet modulates in vivo the production of inflammatory mediators. We have evaluated the anti-inflammatory properties of MTA in bacterial lipopolysaccharide (LPS) challenged mice, murine macrophage RAW 264.7 cells, and isolated rat hepatocytes treated with pro-inflammatory cytokines. MTA administration completely prevented LPS-induced lethality. The life-sparing effect of MTA was accompanied by the suppression of circulating tumor necrosis factor-alpha (TNF-alpha), inducible NO synthase (iNOS) expression, and by the stimulation of IL-10 synthesis. These responses to MTA were also observed in LPS-treated RAW 264.7 cells. MTA prevented the transcriptional activation of iNOS by pro-inflammatory cytokines in isolated hepatocytes, and the induction of cyclooxygenase 2 (COX2) in RAW 264.7 cells. MTA inhibited the activation of p38 mitogen-activated protein kinase (MAPK), c-jun phosphorylation, inhibitor kappa B alpha (IkappaBalpha) degradation, and nuclear factor kappaB (NFkappaB) activation, all of which are signaling pathways related to the generation of inflammatory mediators. These effects were independent of the metabolic conversion of MTA into AdoMet and the potential interaction of MTA with the cAMP signaling pathway, central to the anti-inflammatory actions of its structural analog adenosine. In conclusion, these observations demonstrate novel immunomodulatory properties for MTA that may be of value in the management of inflammatory diseases.

Published
2004

24. L-methionine availability regulates expression of the methionine adenosyltransferase 2A gene in human hepatocarcinoma cells: role of S-adenosylmethionine

Author

Martinez-Chantar, M.L. (María Luz), Latasa, M.U. (María Ujué), Varela-Rey, M. (Marta), Lu, S.C. (Shelly C.), Ruiz Garcia-Trevijano, E. (Elena), Mato, J.M. (José María), and Avila, M.A. (Matías Antonio)

Subjects
Liver Neoplasms/metabolism, S-Adenosylmethionine/physiology, Methionine Adenosyltransferase/genetics, Methionine/metabolism, Carcinoma, Hepatocellular/metabolism
Abstract

In mammals, methionine adenosyltransferase (MAT), the enzyme responsible for S-adenosylmethionine (AdoMet) synthesis, is encoded by two genes, MAT1A and MAT2A. In liver, MAT1A expression is associated with high AdoMet levels and a differentiated phenotype, whereas MAT2A expression is associated with lower AdoMet levels and a dedifferentiated phenotype. In the current study, we examined regulation of MAT2A gene expression by l-methionine availability using HepG2 cells. In l-methionine-deficient cells, MAT2A gene expression is rapidly induced, and methionine adenosyltransferase activity is increased. Restoration of l-methionine rapidly down-regulates MAT2A mRNA levels; for this effect, l-methionine needs to be converted into AdoMet. This novel action of AdoMet is not mediated through a methyl transfer reaction. MAT2A gene expression was also regulated by 5'-methylthioadenosine, but this was dependent on 5'-methylthioadenosine conversion to methionine through the salvage pathway. The transcription rate of the MAT2A gene remained unchanged during l-methionine starvation; however, its mRNA half-life was significantly increased (from 100 min to more than 3 h). The effect of l-methionine withdrawal on MAT2A mRNA stabilization requires both gene transcription and protein synthesis. We conclude that MAT2A gene expression is modulated as an adaptive response of the cell to l-methionine availability through its conversion to AdoMet.

Published
2003

25. NO, SNO and low O2

Author

Mato, J.M. (José María), Avila, M.A. (Matías Antonio), and Corrales, F.J. (Fernando José)

Subjects
Signal Transduction/physiology, Hemoglobins/metabolism, Nitric Oxide/metabolism, Oxygen/metabolism
Published
2001

26. Specific interaction of methionine adenosyltransferase with free radicals

Author

Avila, M.A. (Matías Antonio), Corrales, F.J. (Fernando José), Ruiz, F.A. (Félix A.), Sanchez-Gongora, E. (E.), Mingorance, J. (J.), Carretero, M.V. (M. Victoria), and Mato, J.M. (José María)

Subjects
Oxidative Stress/physiology, Methionine Adenosyltransferase/metabolism, Glutathione/metabolism
Abstract

Although free radicals have been traditionally implicated in cell injury, and associated to pathophysiological processes, recent data implicate them in cell signaling events. Free radicals are naturally occurring oxygen-,nitrogen-and sulfur-derived species with an unpaired electron, such as superoxide, hydroxyl radical or nitric oxide. In order to assess the role of free radicals in cell signaling, we have studies the modulator effect of oxygen and nitrogen active species on liver methionine adenosyltransferase (MAT), a key metabolic enzyme. The presence of 10 cysteine residues per subunit, makes liver MAT a sensitive target for oxidation/nitrosylation. Here we show that purified MAT from rat liver is nitrosylated and oxidized in vitro. Incubation with H202 or the NO donor S-nitrosylated GSH (GSNO), diminish MAT activity in a dose-and time-dependent manner. Furthermore, the inactivation derived from both oxidation and nitrosylation, was reverted by GSH. MAT inactivation originates on the specific and covalent modification of the sulphydryl group of cysteine residue 121. We also studied how free radicals modulate MAT activity in vivo. It was previously shown that MAT activity is strongly dependent on cellular GSH levels. Generation of oxygen and nitrogen active species in rats by injection of LPS, induced a decrease of liver MAT activity. This effect might derive from nitrosylation and/or oxidation of the enzyme. Modulation of liver MAT by NO is further supported by the inactivation of this enzyme observed in experimental models in which NO is produced; such as the administration of NO donors to rats and in hepatocytes cultured in hypoxia, a condition that induces the expression of the inducible nitric oxide synthase (iNOS). Oxidation also controls liver MAT activity in a cell environment as shown in CHO cells stably transfected with rat liver MAT cDNA upon addition of H2O2 to the culture medium. This effect depends upon the generation of the hydroxyl radical. On the basis of the metabolic implications of liver MAT, together with the structural features accounting for the sensitivity of this enzyme to active oxygen and nitrogen species, we propose that modulation of MAT by these agents could be a mechanism to regulate the consumption of ATP in the liver, and thus preserve cellular viability under different stress conditions.

Published
1998

27. New therapies for hepatocellular carcinoma

Author

Avila, M.A. (Matías Antonio)

Subjects
Hepatocellular carcinoma, Molecular targets, New therapies
Abstract

Hepatocellular carcinoma (HCC), one of the most common cancers worldwide, is often diagnosed at an advanced stage when most potentially curative therapies such as resection, transplantation or percutaneous and transarterial interventions are of limited efficacy. The fact that HCC is resistant to conventional chemotherapy, and is rarely amenable to radiotherapy, leaves this disease with no effective therapeutic options and a very poor prognosis. Therefore, the development of more effective therapeutic tools and strategies is much needed. HCCs are phenotypically and genetically heterogeneous tumors that commonly emerge on a background of chronic liver disease. However, in spite of this heterogeneity recent insights into the biology of HCC suggest that certain signaling pathways and molecular alterations are likely to play essential roles in HCC development by promoting cell growth and survival. The identification of such mechanisms may open new avenues for the prevention and treatment of HCC through the development of targeted therapies. In this review we will describe the new potential therapeutic targets and clinical developments that have emerged from progress in the knowledge of HCC biology, In addition, recent advances in gene therapy and combined cell and gene therapy, together with new radiotherapy techniques and immunotherapy in patients with HCC will be discussed.

Published
2006

28. S-Adenosylmethionine revisited: its essential role in the regulation of liver function

Author

Avila, M.A. (Matías Antonio)

Subjects
S -Adenosylmethionine, Liver damage, Cirrhosis, Hepatocarcinoma, Gene expression
Abstract

Dietary methionine is mainly metabolized in the liver where it is converted into S-adenosylmethionine (AdoMet), the main biologic methyl donor. This reaction is catalyzed by methionine adenosyltransferase I/III (MAT I/III), the product of MAT1A gene, which is exclusively expressed in this organ. It was first observed that serum methionine levels were elevated in experimental models of liver damage and in liver cirrhosis in human beings. Results of further studies showed that this pathological alteration was due to reduced MAT1A gene expression and MAT I/III enzyme inactivation associated with liver injury. Synthesis of AdoMet is essential to all cells in the organism, but it is in the liver where most of the methylation reactions take place. The central role played by AdoMet in cellular function, together with the observation that AdoMet administration reduces liver damage caused by different agents and improves survival of alcohol-dependent patients with cirrhosis, led us to propose that alterations in methionine metabolism could play a role in the onset of liver disease and not just be a consequence of it. In the present work, we review the recent findings that support this hypothesis and highlight the mechanisms behind the hepatoprotective role of AdoMet.

Published
2002

29. Reduced mRNA abundance of the main enzymes involved in methionine metabolism in human liver cirrhosis and hepatocellular carcinoma

Author

Avila, M.A. (Matías Antonio)

Subjects
Cirrhosis, DNA methylation, Hepatocarcinema, Liver, Methionine
Abstract

BACKGROUND/AIMS: It has been known for at least 50 years that alterations in methionine metabolism occur in human liver cirrhosis. However, the molecular basis of this alteration is not completely understood. In order to gain more insight into the mechanisms behind this condition, mRNA levels of methionine adenosyltransferase (MAT1A), glycine methyltransferase (GNMT), methionine synthase (MS), betaine homocysteine methyltransferase (BHMT) and cystathionine beta-synthase (CBS) were examined in 26 cirrhotic livers, five hepatocellular carcinoma (HCC) tissues and ten control livers. METHODS: The expression of the above-mentioned genes was determined by quantitative RT-PCR analysis. Methylation of MAT1A promoter was assessed by methylation-sensitive restriction enzyme digestion of genomic DNA. RESULTS: When compared to normal livers MAT1A, GNMT, BHMT, CBS and MS mRNA contents were significantly reduced in liver cirrhosis. Interestingly, MAT1A promoter was hypermethylated in the cirrhotic liver. HCC tissues also showed decreased mRNA levels of these enzymes. CONCLUSIONS: These findings establish that the abundance of the mRNA of the main genes involved in methionine metabolism is markedly reduced in human cirrhosis and HCC. Hypermethylation of MAT1A promoter could participate in its reduced expression in cirrhosis. These observations help to explain the hypermethioninemia, hyperhomocysteinemia and reduced hepatic glutathione content observed in cirrhosis.

Published
2000

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