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1. Soluble urokinase plasminogen activator receptor levels predict survival in patients with portal hypertension undergoing TIPS

Author

Loosen, Sven H., Benz, Fabian, Mohr, Raphael, Reuken, Philipp A., Wirtz, Theresa H., Junker, Lioba, Jansen, Christian, Meyer, Carsten, Praktiknjo, Michael, Wree, Alexander, Reißing, Johanna, Demir, Münevver, Gu, Wenyi, Vucur, Mihael, Schierwagen, Robert, Stallmach, Andreas, Kunstein, Anselm, Bode, Johannes, Trautwein, Christian, Tacke, Frank, Luedde, Tom, Bruns, Tony, Trebicka, Jonel, and Roderburg, Christoph

Published
2024
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2. A global research priority agenda to advance public health responses to fatty liver disease

Author

Lazarus, Jeffrey V., Mark, Henry E., Allen, Alina M., Arab, Juan Pablo, Carrieri, Patrizia, Noureddin, Mazen, Alazawi, William, Alkhouri, Naim, Alqahtani, Saleh A., Arrese, Marco, Bataller, Ramon, Berg, Thomas, Brennan, Paul N., Burra, Patrizia, Castro-Narro, Graciela E., Cortez-Pinto, Helena, Cusi, Kenneth, Dedes, Nikos, Duseja, Ajay, Francque, Sven M., Hagström, Hannes, Huang, Terry T-K., Wajcman, Dana Ivancovsky, Kautz, Achim, Kopka, Christopher J., Krag, Aleksander, Miller, Veronica, Newsome, Philip N., Rinella, Mary E., Romero, Diana, Sarin, Shiv Kumar, Silva, Marcelo, Spearman, C. Wendy, Tsochatzis, Emmanuel A., Valenti, Luca, Villota-Rivas, Marcela, Zelber-Sagi, Shira, Schattenberg, Jörn M., Wong, Vincent Wai-Sun, Younossi, Zobair M., Aberg, Fredrik, Adams, Leon, Al-Naamani, Khalid, Albadawy, Reda M., Alexa, Zinaida, Allison, Michael, Alnaser, Faisal A., Alswat, Khalid, Alvares-da-Silva, Mario Reis, Alvaro, Domenico, Alves-Bezerra, Michele, Andrade, Raul J., Anstee, Quentin M., Awuku, Yaw Asante, Baatarkhuu, Oidov, Baffy, Gyorgy, Bakieva, Shokhista, Bansal, Meena B., Barouki, Robert, Batterham, Rachel L., Behling, Cynthia, Belfort-DeAguiar, Renata, Berzigotti, Annalisa, Betel, Michael, Bianco, Cristiana, Bosi, Emanuele, Boursier, Jerome, Brunt, Elizabeth M., Bugianesi, Elisabetta, Byrne, Christopher J., Cabrera Cabrejos, Maria Cecilia, Caldwell, Stephen, Carr, Rotonya, Castellanos Fernández, Marlen Ivón, Castera, Laurent, Castillo-López, Maria Gabriela, Caussy, Cyrielle, Cerda-Reyes, Eira, Ceriello, Antonio, Chan, Wah- Kheong, Chang, Yoosoo, Charatcharoenwitthaya, Phunchai, Chavez-Tapia, Norberto, Chung, Raymond T., Colombo, Massimo, Coppell, Kirsten, Cotrim, Helma P., Craxi, Antonio, Crespo, Javier, Dassanayake, Anuradha, Davidson, Nicholas O., De Knegt, Robert, de Ledinghen, Victor, Demir, Münevver, Desalegn, Hailemichael, Diago, Moises, Dillon, John F., Dimmig, Bruce, Dirac, M. Ashworth, Dirchwolf, Melisa, Dufour, Jean-François, Dvorak, Karel, Ekstedt, Mattias, El-Kassas, Mohamed, Elsanousi, Osama M., Elsharkawy, Ahmed M., Elwakil, Reda, Eskridge, Wayne, Eslam, Mohammed, Esmat, Gamal, Fan, Jian- Gao, Ferraz, Maria Lucia, Flisiak, Robert, Fortin, Davide, Fouad, Yasser, Freidman, Scott L., Fuchs, Michael, Gadano, Adrian, Gastaldelli, Amalia, Geerts, Anja, Geier, Andreas, George, Jacob, Gerber, Lynn H., Ghazinyan, Hasmik, Gheorghe, Liana, Kile, Denise Giangola, Girala, Marcos, Boon Bee, George Goh, Goossens, Nicolas, Graupera, Isabel, Grønbæk, Henning, Hamid, Saeed, Hebditch, Vanessa, Henry, Zachary, Hickman, Ingrid J., Hobbs, L. Ansley, Hocking, Samantha L., Hofmann, Wolf Peter, Idilman, Ramazan, Iruzubieta, Paula, Isaacs, Scott, Isakov, Vasily A., Ismail, Mona H., Jamal, Mohammad H., Jarvis, Helen, Jepsen, Peter, Jornayvaz, François, Sudhamshu, K.C., Kakizaki, Satoru, Karpen, Saul, Kawaguchi, Takumi, Keating, Shelley E., Khader, Yousef, Kim, Seung Up, Kim, Won, Kleiner, David E., Koek, Ger, Joseph Komas, Narcisse Patrice, Kondili, Loreta A., Koot, Bart G., Korenjak, Marko, Kotsiliti, Eleni, Koulla, Yiannoula, Kugelmas, Carina, Kugelmas, Marcelo, Labidi, Asma, Lange, Naomi F., Lavine, Joel E., Lazo, Mariana, Leite, Nathalie, Lin, Han-Chieh, Lkhagvaa, Undram, Long, Michelle T., Lopez-Jaramillo, Patricio, Lozano, Adelina, Macedo, Maria Paula, Malekzadeh, Reza, Marchesini, Giulio, Marciano, Sebastian, Martinez, Kim, Martínez Vázquez, Sophia E., Mateva, Lyudmila, Mato, José M., Nlombi, Charles Mbendi, McCary, Alexis Gorden, McIntyre, Jeff, McKee, Martin, Mendive, Juan M., Mikolasevic, Ivana, Miller, Pamela S., Milovanovic, Tamara, Milton, Terri, Moreno-Alcantar, Rosalba, Morgan, Timothy R., Motala, Ayesha, Muris, Jean, Musso, Carla, Nava-González, Edna J., Negro, Francesco, Nersesov, Alexander V., Neuschwander-Tetri, Brent A., Nikolova, Dafina, Norris, Suzanne, Novak, Katja, Ocama, Ponsiano, Ong, Janus P., Ong-Go, Arlinking, Onyekwere, Charles, Padilla, Martin, Pais, Raluca, Pan, Calvin, Panduro, Arturo, Panigrahi, Manas K., Papatheodoridis, Georgios, Paruk, Imran, Patel, Keyur, Gonçalves, Carlos Penha, Figueroa, Marlene Pérez, Pérez-Escobar, Juanita, Pericàs, Juan M., Perseghin, Gianluca, Pessoa, Mário Guimarães, Petta, Salvatore, Marques Souza de Oliveira, Claudia Pinto, Prabhakaran, Dorairaj, Pyrsopoulous, Nikolaos, Rabiee, Atoosa, Ramji, Alnoor, Ratziu, Vlad, Ravendhran, Natarajan, Ray, Katrina, Roden, Michael, Romeo, Stefano, Romero-Gómez, Manuel, Rotman, Yaron, Rouabhia, Samir, Rowe, Ian A., Sadirova, Shakhlo, Alkhatry, Maryam Salem, Salupere, Riina, Satapathy, Sanjaya K., Schwimmer, Jeffrey B., Sebastiani, Giada, Seim, Lynn, Seki, Yosuke, Serme, Abdel Karim, Shapiro, David, Sharvadze, Lali, Shaw, Jonathan E., Shawa, Isaac Thom, Shenoy, Thrivikrama, Shibolet, Oren, Shimakawa, Yusuke, Shubrook, Jay H., Singh, Shivaram Prasad, Sinkala, Edford, Skladany, Lubomir, Skrypnyk, Igor, Song, Myeong Jun, Sookoian, Silvia, Sridharan, Kannan, Stefan, Norbert, Stine, Jonathan G., Stratakis, Nikolaos, Sheriff, Dhastagir Sultan, Sundaram, Shikha S., Svegliati-Baroni, Gianluca, Swain, Mark G., Tacke, Frank, Taheri, Shahrad, Tan, Soek-Siam, Tapper, Elliot B., Targher, Giovanni, Tcaciuc, Eugen, Thiele, Maja, Tiniakos, Dina, Tolmane, Ieva, Torre, Aldo, Torres, Esther A., Treeprasertsuk, Sombat, Trenell, Michael, Turcan, Svetlana, Turcanu, Adela, Valantinas, Jonas, van Kleef, Laurens A., Velarde Ruiz Velasco, Jose Antonio, Vesterhus, Mette, Vilar-Gomez, Eduardo, Waked, Imam, Wattacheril, Julia, Wedemeyer, Heiner, Wilkins, Fonda, Willemse, José, Wong, Robert J., Yilmaz, Yusuf, Yki-Järvinen, Hannele, Yu, Ming-Lung, Yumuk, Volkan, Zeybel, Müjdat, Zheng, Kenneth I., Zheng, Ming-Hua, and Huang, Terry T.-K.

Published
2023
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3. Treating hepatitis D with bulevirtide – Real-world experience from 114 patients

Author

Dietz-Fricke, Christopher, Tacke, Frank, Zöllner, Caroline, Demir, Münevver, Schmidt, Hartmut H., Schramm, Christoph, Willuweit, Katharina, Lange, Christian M., Weber, Sabine, Denk, Gerald, Berg, Christoph P., Grottenthaler, Julia M., Merle, Uta, Olkus, Alexander, Zeuzem, Stefan, Sprinzl, Kathrin, Berg, Thomas, van Bömmel, Florian, Wiegand, Johannes, Herta, Toni, Seufferlein, Thomas, Zizer, Eugen, Dikopoulos, Nektarios, Thimme, Robert, Neumann-Haefelin, Christoph, Galle, Peter R., Sprinzl, Martin, Lohse, Ansgar W., Schulze zur Wiesch, Julian, Kempski, Jan, Geier, Andreas, Reiter, Florian P., Schlevogt, Bernhard, Gödiker, Juliana, Hofmann, Wolf Peter, Buggisch, Peter, Kahlhöfer, Julia, Port, Kerstin, Maasoumy, Benjamin, Cornberg, Markus, Wedemeyer, Heiner, and Deterding, Katja

Published
2023
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4. Natürlicher Verlauf

Author

Demir, Münevver, Steffen, Hans-Michael, Geier, Andreas, editor, Canbay, Ali, editor, and Lammert, Frank, editor

Published
2022
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7. Norursodeoxycholic acid versus placebo in the treatment of non-alcoholic fatty liver disease: a double-blind, randomised, placebo-controlled, phase 2 dose-finding trial

Author

Vogel, Wolfgang, Aigner, Elmar, Datz, Christian, Tilg, Herbert, Gerken, Guido, Rust, Christian, Cordes, Hans-Jörg, Steib, Christian, Pathil-Warth, Anita, Prinz, MD, Christian, Lammert, Frank, Antoni, Christoph, Klausmann, Gerhard, Häussinger, Dieter, Zipprich, Alexander, Traussnigg, Stefan, Schattenberg, Jörn M, Demir, Münevver, Wiegand, Johannes, Geier, Andreas, Teuber, Gerlinde, Hofmann, Wolf Peter, Kremer, Andreas E, Spreda, Frank, Kluwe, Johannes, Petersen, Jörg, Boettler, Tobias, Rainer, Florian, Halilbasic, Emina, Greinwald, Roland, Pröls, Markus, Manns, Michael P, Fickert, Peter, and Trauner, Michael

Published
2019
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10. Cenicriviroc for the treatment of COVID-19: first interim results of a randomised, placebo-controlled, investigator-initiated, double-blind phase II trial

Author

Kurth, Florian, Helbig, Elisa T., Lippert, Lena J., Thibeault, Charlotte, Barbone, Gianluca, Eckart, Marius A., Kluge, Martin, Puengel, Tobias, Demir, Münevver, Röhle, Robert, Keller, Theresa, Ruwwe-Glösenkamp, Christoph, Witzenrath, Martin, Suttorp, Norbert, von Kalle, Christof, Sander, Leif E., Jochum, Christoph, and Tacke, Frank

Published
2023
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13. SAT-135 Soluble urokinase plasminogen activator receptor (suPAR) levels predict survival in patients with portal hypertension undergoing TIPS

Author

Loosen, Sven H., Benz, Fabian, Mohr, Raphael, Reuken, Philipp, Hildegard Wirtz, Theresa, Gu, Wenyi, Junker, Lioba, Jansen, Christian, Meyer, Carsten, Praktiknjo, Michael, Wree, Alexander, Reissing, Johanna, Demir, Münevver, Vucur, Mihael, Schierwagen, Robert, Stallmach, Andreas, Kunstein, Anselm, Bode, Johannes, Trautwein, Christian, Tacke, Frank, Luedde, Tom, Bruns, Tony, Trebicka, Jonel, and Roderburg, Christoph

Published
2024
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15. Uncontrolled hypertension: A neglected risk in patients with NAFLD

Author

Kasper, Philipp, Martin, Anna, zu Schwabedissen, Albrecht Meyer, Scherdel, Julia, Lang, Sonja, Goeser, Tobias, Demir, Muenevver, Steffen, Hans-Michael, Kasper, Philipp, Martin, Anna, zu Schwabedissen, Albrecht Meyer, Scherdel, Julia, Lang, Sonja, Goeser, Tobias, Demir, Muenevver, and Steffen, Hans-Michael

Published
2022

16. Management of Dyslipidemia in Patients with Non-Alcoholic Fatty Liver Disease

Author

Martin, Anna, Lang, Sonja, Goeser, Tobias, Demir, Muenevver, Steffen, Hans-Michael, Kasper, Philipp, Martin, Anna, Lang, Sonja, Goeser, Tobias, Demir, Muenevver, Steffen, Hans-Michael, and Kasper, Philipp

Abstract

Purpose of Review Patients with non-alcoholic fatty liver disease (NAFLD), often considered as the hepatic manifestation of the metabolic syndrome, represent a population at high cardiovascular risk and frequently suffer from atherogenic dyslipidemia. This article reviews the pathogenic interrelationship between NAFLD and dyslipidemia, elucidates underlying pathophysiological mechanisms and focuses on management approaches for dyslipidemic patients with NAFLD. Recent Findings Atherogenic dyslipidemia in patients with NAFLD results from hepatic and peripheral insulin resistance along with associated alterations of hepatic glucose and lipoprotein metabolism, gut dysbiosis, and genetic factors. Since atherogenic dyslipidemia and NAFLD share a bi-directional relationship and are both major driving forces of atherosclerotic cardiovascular disease (ASCVD) development, early detection and adequate treatment are warranted. Thus, integrative screening and management programs are urgently needed. A stepwise approach for dyslipidemic patients with NAFLD includes (i) characterization of dyslipidemia phenotype, (ii) individual risk stratification, (iii) definition of treatment targets, (iv) lifestyle modification, and (v) pharmacotherapy if indicated.

Published
2022

17. Dietary omega-6/omega-3 ratio is not associated with gut microbiota composition and disease severity in patients with nonalcoholic fatty liver disease

Author

Heinzer, Kathrin, Lang, Sonja, Farowski, Fedja, Wisplinghoff, Hilmar, Vehreschild, Maria J. G. T., Martin, Anna, Nowag, Angela, Kretzschmar, Anne, Scholz, Claus Juergen, Roderburg, Christoph, Mohr, Raphael, Tacke, Frank, Kasper, Philipp, Goeser, Tobias, Steffen, Hans -Michael, Demir, Muenevver, Heinzer, Kathrin, Lang, Sonja, Farowski, Fedja, Wisplinghoff, Hilmar, Vehreschild, Maria J. G. T., Martin, Anna, Nowag, Angela, Kretzschmar, Anne, Scholz, Claus Juergen, Roderburg, Christoph, Mohr, Raphael, Tacke, Frank, Kasper, Philipp, Goeser, Tobias, Steffen, Hans -Michael, and Demir, Muenevver

Abstract

In this cross-sectional study, we hypothesized that a high dietary ratio of omega-6 (n-6) to omega-3 (n-3) fatty acids could be associated with an altered gut bacterial composition and with the disease severity in patients with nonalcoholic fatty liver disease (NAFLD). A total of 101 NAFLD patients were included in the study, of which 63 underwent a liver biopsy. All 101 patients completed a 14-day food and activity record. Ebispro 2016 professional software was used to calculate individual macronutrients and micronutrients consumed. Patients were grouped into 3 quantiles (Q) according to a low (Q1: < 6.1, n = 34), moderate (Q2: 6.1-7.8, n = 33), or high (Q3: > 7.8, n = 34) dietary n-6/n-3 ratio. Stool samples were analyzed using 16S rRNA gene sequencing. Spearman correlation coefficients and principal coordinate analysis were used to detect differences in the bacterial composition of the gut microbiota. The me-dian dietary n-6/n-3 ratio of all patients was 6.7 (range, 3.1-14.9). No significant associations between the dietary n-6/n-3 ratio and the gut microbiota composition or disease severity were observed. However, the abundance of specific bacteria such as Catenibacterium or Lacto-bacillus ruminis were found to be positively correlated and the abundance of Clostridium were negatively correlated with dietary n-6 fatty acid intake. The results indicate that a high di-etary n-6/n-3 ratio is probably not a highly relevant factor in the pathogenesis of human NAFLD. Further studies are needed to clarify the importance of interactions between gut bacterial taxa and n-6 fatty acids in the pathophysiology of NAFLD.(c) 2022 Elsevier Inc. All rights reserved.

Published
2022

22. List of contributors

Author

Adeyanyu, Adeyemi A., Ahmad, Saghir, Ajani, Clement K., Ali, Murtaza, Ali, Tahira Mohsin, Ariyantoro, Achmad Ridwan, Ayofemi Olalekan, Adeyeye Samuel, Bassey, Anthony P., Bassey, Edidiong J., Bhavaniramya, Sundaresan, Bobade, Hanuman, Butt, Natasha Abbas, Chin, Nyuk L., Demir, Münevver, Esua, Okon J., Guo, Zebin, Haider, Salman, Hegde, Sanjay Vinayak, Hussain, Nisar, Idrishi, Rubeka, Jaganmohan, R., Kajla, Priyanka, Kalpanadevi, Chinnusamy, Karthiayani, Kaur, Ramandeep, Kaur, Sukhpreet, Khurana, Savi, Kumari, Parveen, Kırboğa, Kevser Kübra, Liu, Honglin, Liu, Lu, Manzoor, Arshied, Mondragón-Cortéz, Pedro, Morales-Hernández, Norma, Muhammad, Dimas Rahadian Aji, Okonkwo, Clinton E., Olagunju, Aderonke Ibidunni, Oluwajuyitan, Timilehin David, Omoba, Olufunmilayo Sade, S., Padma Ishwarya, Pareek, Vanya, Prieto-Vázquez del Mercado, Pavel Alejandro, Ramar, Vanajothi, Rangan, Latha, Rasmi, Yousef, Roshini, Deepika, Sachdev, Poonam A., Shaikh, Faiza, Shaikh, Marium, Shelke, Rahul G., Singh, Rajendra Pratap, Singha, Siddhartha, Surendra Babu, A., Tekin, Burcu, Vishnupriya, Selvaraju, Yudhistira, Bara, Yulviatun, Anastriyani, Zeng, Xin-An, and Zheng, Baodong

Published
2024
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24. Combined analysis of gut microbiota, diet and PNPLA3 polymorphism in biopsy-proven non-alcoholic fatty liver disease

Author

Lang, Sonja, Martin, Anna, Zhang, Xinlian, Farowski, Fedja, Wisplinghoff, Hilmar, J. G. T. Vehreschild, Maria, Krawczyk, Marcin, Nowag, Angela, Kretzschmar, Anne, Scholz, Claus, Kasper, Philipp, Roderburg, Christoph, Mohr, Raphael, Lammert, Frank, Tacke, Frank, Schnabl, Bernd, Goeser, Tobias, Steffen, Hans-Michael, Demir, Muenevver, Lang, Sonja, Martin, Anna, Zhang, Xinlian, Farowski, Fedja, Wisplinghoff, Hilmar, J. G. T. Vehreschild, Maria, Krawczyk, Marcin, Nowag, Angela, Kretzschmar, Anne, Scholz, Claus, Kasper, Philipp, Roderburg, Christoph, Mohr, Raphael, Lammert, Frank, Tacke, Frank, Schnabl, Bernd, Goeser, Tobias, Steffen, Hans-Michael, and Demir, Muenevver

Abstract

Background and aims Non-alcoholic fatty liver disease (NAFLD) is a global health burden. Risk factors for disease severity include older age, increased body mass index (BMI), diabetes, genetic variants, dietary factors and gut microbiota alterations. However, the interdependence of these factors and their individual impact on disease severity remain unknown. Methods In this cross-sectional study, we performed 16S gene sequencing using fecal samples, collected dietary intake, PNPLA3 gene variants and clinical and liver histology parameters in a well-described cohort of 180 NAFLD patients. Principal component analyses were used for dimensionality reduction of dietary and microbiota data. Simple and multiple stepwise ordinal regression analyses were performed. Results Complete data were available for 57 NAFLD patients. In the simple regression analysis, features associated with the metabolic syndrome had the highest importance regarding liver disease severity. In the multiple regression analysis, BMI was the most important factor associated with the fibrosis stage (OR per kg/m(2): 1.23, 95% CI 1.10-1.37, P < .001). The PNPLA3 risk allele had the strongest association with the histological grade of steatosis (OR 5.32, 95% CI 1.56-18.11, P = .007), followed by specific dietary patterns. Low abundances of Faecalibacterium, Bacteroides and Prevotella and high abundances of Gemmiger were associated with the degree of inflammation, ballooning and stages of fibrosis, even after taking other cofactors into account. Conclusions BMI had the strongest association with histological fibrosis, but PNPLA3 gene variants, gut bacterial features and dietary factors were all associated with different histology features, which underscore the multifactorial pathogenesis of NAFLD.

Published
2021

25. Maternal Exercise Mediates Hepatic Metabolic Programming via Activation of AMPK-PGC1 alpha Axis in the Offspring of Obese Mothers

Author

Kasper, Philipp, Breuer, Saida, Hoffmann, Thorben, Vohlen, Christina, Janoschek, Ruth, Schmitz, Lisa, Appel, Sarah, Fink, Gregor, Huenseler, Christoph, Quaas, Alexander, Demir, Muenevver, Lang, Sonja, Steffen, Hans-Michael, Martin, Anna, Schramm, Christoph, Buerger, Martin, Mahabir, Esther, Goeser, Tobias, Doetsch, Joerg, Hucklenbruch-Rother, Eva, Bae-Gartz, Inga, Kasper, Philipp, Breuer, Saida, Hoffmann, Thorben, Vohlen, Christina, Janoschek, Ruth, Schmitz, Lisa, Appel, Sarah, Fink, Gregor, Huenseler, Christoph, Quaas, Alexander, Demir, Muenevver, Lang, Sonja, Steffen, Hans-Michael, Martin, Anna, Schramm, Christoph, Buerger, Martin, Mahabir, Esther, Goeser, Tobias, Doetsch, Joerg, Hucklenbruch-Rother, Eva, and Bae-Gartz, Inga

Abstract

Maternal obesity is associated with an increased risk of hepatic metabolic dysfunction for both mother and offspring and targeted interventions to address this growing metabolic disease burden are urgently needed. This study investigates whether maternal exercise (ME) could reverse the detrimental effects of hepatic metabolic dysfunction in obese dams and their offspring while focusing on the AMP-activated protein kinase (AMPK), representing a key regulator of hepatic metabolism. In a mouse model of maternal western-style-diet (WSD)-induced obesity, we established an exercise intervention of voluntary wheel-running before and during pregnancy and analyzed its effects on hepatic energy metabolism during developmental organ programming. ME prevented WSD-induced hepatic steatosis in obese dams by alterations of key hepatic metabolic processes, including activation of hepatic ss-oxidation and inhibition of lipogenesis following increased AMPK and peroxisome-proliferator-activated-receptor-gamma-coactivator-1 alpha (PGC-1 alpha)-signaling. Offspring of exercised dams exhibited a comparable hepatic metabolic signature to their mothers with increased AMPK-PGC1 alpha-activity and beneficial changes in hepatic lipid metabolism and were protected from WSD-induced adipose tissue accumulation and hepatic steatosis in later life. In conclusion, this study demonstrates that ME provides a promising strategy to improve the metabolic health of both obese mothers and their offspring and highlights AMPK as a potential metabolic target for therapeutic interventions.

Published
2021

26. Hypertension in NAFLD: An uncontrolled burden

Author

Kasper, Philipp, Martin, Anna, Lang, Sonja, Demir, Muenevver, Steffen, Hans-Michael, Kasper, Philipp, Martin, Anna, Lang, Sonja, Demir, Muenevver, and Steffen, Hans-Michael

Published
2021

28. Serum levels of bone sialoprotein correlate with portal pressure in patients with liver cirrhosis

Author

Benz, Fabian, Bogen, Andreas, Praktiknjo, Michael, Jansen, Christian, Meyer, Carsten, Wree, Alexander, Demir, Muenevver, Loosen, Sven, Vucur, Mihael, Schierwagen, Robert, Tacke, Frank, Trebicka, Jonel, Roderburg, Christoph, and Strnad, Pavel

Subjects
Adult, Liver Cirrhosis, Male, Patients, Science, Gastroenterology and Hepatology, Biochemistry, Severity of Illness Index, Veins, stomatognathic system, Hypertension, Portal, Medicine and Health Sciences, Humans, Integrin-Binding Sialoprotein, ddc:610, Portal Veins, Aged, Retrospective Studies, Portal Vein, Liver Diseases, Biology and Life Sciences, Ascites, Portal Hypertension, Middle Aged, Prognosis, Portal Pressure, Health Care, Cirrhosis, Cardiovascular Anatomy, Disease Progression, Medicine, Blood Vessels, Female, Anatomy, Biomarkers, Research Article
Abstract

PLOS ONE 15(4), e0231701 (2020). doi:10.1371/journal.pone.0231701, Published by PLOS, San Francisco, California, US

Published
2020

29. SAT-156 - Improvements in ALT levels during Bulevirtide treatment for hepatitis D are seen regardless of virologic response

Author

Dietz-Fricke, Christopher, Tacke, Frank, Zöllner, Caroline, Demir, Münevver, Schmidt, Hartmut, Schramm, Christoph, Willuweit, Katharina, Lange, Christian M., Weber, Sabine, Denk, Gerald, Berg, Christoph, Grottenthaler, Julia, Merle, Uta, Olkus, Alexander, Zeuzem, Stefan, Sprinzl, Kathrin, Berg, Thomas, van Bömmel, Florian, Wiegand, Johannes, Herta, Toni, Seufferlein, Thomas, Zizer, Eugen, Dikopoulos, Nektarios, Thimme, Robert, Neumann-Haefelin, Christoph, Galle, Peter, Sprinzl, Martin, Lohse, Ansgar W., Kempski, Jan, zur Wiesch, Julian Schulze, Geier, Andreas, Reiter, Florian P, Schlevogt, Bernhard, Goediker, Juliana, Hofmann, Wolf Peter, Buggisch, Peter, Kahlhöfer, Julia, Port, Kerstin, Maasoumy, Benjamin, Cornberg, Markus, Wedemeyer, Heiner, and Deterding, Katja

Published
2023
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31. Cytolysin-positive Enterococcus faecalis is not increased in patients with non-alcoholic steatohepatitis

Author

Lang, Sonja, Demir, Muenevver, Duan, Yi, Martin, Anna, Schnabl, Bernd, Lang, Sonja, Demir, Muenevver, Duan, Yi, Martin, Anna, and Schnabl, Bernd

Abstract

Several studies show associations between gut bacterial dysbiosis and chronic liver diseases, but causative mechanisms are largely unclear. We recently identified cytolysin, a bacterial exotoxin expressed and secreted by Enterococcus faecalis to cause liver damage in the setting of alcohol-related liver disease. Cytolysin was increased and highly correlated with liver disease severity and mortality in alcoholic hepatitis patients. In this study, we investigated if faecal cytolysin-positivity can be linked to non-alcoholic fatty liver disease, a highly prevalent disease where new biomarkers and treatment targets are urgently needed. In contrast to what we observed in alcoholic hepatitis, only seven out of 96 non-alcoholic fatty liver disease patients were cytolysin-positive, and these patients did not have increased liver disease activity compared with cytolysin-negative patients. These results indicate that the association of cytolysin carriage with worse clinical outcome might be specific for alcoholic hepatitis.

Published
2020

32. High Protein Intake Is Associated With Histological Disease Activity in Patients With NAFLD

Author

Lang, Sonja, Martin, Anna, Farowski, Fedja, Wisplinghoff, Hilmar, Vehreschild, Maria J. G. T., Liu, Jinyuan, Krawczyk, Marcin, Nowag, Angela, Kretzschmar, Anne, Herweg, Jens, Schnabl, Bernd, Tu, Xin M., Lammert, Frank, Goeser, Tobias, Tacke, Frank, Heinzer, Kathrin, Kasper, Philipp, Steffen, Hans-Michael, Demir, Muenevver, Lang, Sonja, Martin, Anna, Farowski, Fedja, Wisplinghoff, Hilmar, Vehreschild, Maria J. G. T., Liu, Jinyuan, Krawczyk, Marcin, Nowag, Angela, Kretzschmar, Anne, Herweg, Jens, Schnabl, Bernd, Tu, Xin M., Lammert, Frank, Goeser, Tobias, Tacke, Frank, Heinzer, Kathrin, Kasper, Philipp, Steffen, Hans-Michael, and Demir, Muenevver

Abstract

Overconsumption of carbohydrates and lipids are well known to cause nonalcoholic fatty liver disease (NAFLD), while the role of nutritional protein intake is less clear. In Western diet, meat and other animal products are the main protein source, with varying concentrations of specific amino acids. Whether the amount or composition of protein intake is associated with a higher risk for disease severity has not yet been examined. In this study, we investigated associations of dietary components with histological disease activity by analyzing detailed 14-day food records in a cohort of 61 patients with biopsy-proven NAFLD. Furthermore, we used 16S ribosomal RNA gene sequencing to detect associations with different abundances of the gut microbiota with dietary patterns. Patients with definite nonalcoholic steatohepatitis (NAFLD activity score of 5-8 on liver biopsy) had a significantly higher daily relative intake of protein compared with patients with a NAFLD activity score of 0-4 (18.0% vs. 15.8% of daily protein-based calories, P = 0.018). After adjustment for several potentially confounding factors, a higher protein intake (>= 17.3% of daily protein-based calories) remained associated with definite nonalcoholic steatohepatitis, with an odds ratio of 5.09 (95% confidence interval 1.22-21.25, P = 0.026). This association was driven primarily by serine, glycine, arginine, proline, phenylalanine, and methionine. A higher protein intake correlated with a lower Bacteroides abundance and an altered abundance of several other bacterial taxa. Conclusion: A high protein intake was independently associated with more active and severe histological disease activity in patients with NAFLD. Further studies are needed to investigate the potential harmful role of dietary amino acids on NAFLD, with special attention to meat as their major source.

Published
2020

33. Phenotyping non-alcoholic fatty liver disease by the gut microbiota: Ready for prime time?

Author

Demir, Muenevver, Lang, Sonja, Martin, Anna, Farowski, Fedja, Wisplinghoff, Hilmar, Vehreschild, Maria J. G. T., Krawczyk, Marcin, Nowag, Angela, Scholz, Claus Jurgen, Kretzschmar, Anne, Roderburg, Christoph, Lammert, Frank, Goeser, Tobias, Kasper, Philipp, Steffen, Hans-Michael, Demir, Muenevver, Lang, Sonja, Martin, Anna, Farowski, Fedja, Wisplinghoff, Hilmar, Vehreschild, Maria J. G. T., Krawczyk, Marcin, Nowag, Angela, Scholz, Claus Jurgen, Kretzschmar, Anne, Roderburg, Christoph, Lammert, Frank, Goeser, Tobias, Kasper, Philipp, and Steffen, Hans-Michael

Abstract

Background and Aim Several studies observed alterations in the gut microbiota in patients with non-alcoholic fatty liver disease (NAFLD). However, analyzed patient populations and methods strongly differ among these studies. The aim of this study was to prove the reproducibility of published results and to provide a detailed overview of all findings in our NAFLD cohort using next generation sequencing methods. Methods The individual taxonomic microbiota composition of fecal samples from 90 NAFLD patients and 21 healthy controls was analyzed using 16S rRNA gene sequencing. Study participants were grouped according to their disease stage and compared regarding their gut microbiota composition. Studies were identified from PubMed listed publications, and the results were compared with the findings in our cohort. Results Results from 13 identified studies were compared with our data. A decreased abundance of the Bacteroidetes and Ruminococcaceae as well as an increased abundance of Lactobacillaceae and Veillonellaceae and Dorea were the most frequently reported changes among NAFLD patients in 4/13, 5/13, 4/13, 2/13, and 3/13 studies, respectively. Even though these alterations in the gut microbiota composition were also observed in our patient cohort, the majority of published differences could not be reproduced, neither in our own nor in other NAFLD cohort studies. Conclusion Despite repeatedly reproduced abundance patterns of specific bacteria, the heterogeneous study results did not reveal a consistent disease specific gut microbiota signature. Further prospective studies with homogenous patient cohorts and standardized methods are necessary to phenotype NAFLD by the gut microbiota.

Published
2020

34. Prediction of advanced fibrosis in non-alcoholic fatty liver disease using gut microbiota-based approaches compared with simple non-invasive tools

Author

Lang, Sonja, Farowski, Fedja, Martin, Anna, Wisplinghoff, Hilmar, Vehreschild, Maria J. G. T., Krawczyk, Marcin, Nowag, Angela, Kretzschmar, Anne, Scholz, Claus, Kasper, Philipp, Roderburg, Christoph, Lammert, Frank, Goeser, Tobias, Steffen, Hans-Michael, Demir, Muenevver, Lang, Sonja, Farowski, Fedja, Martin, Anna, Wisplinghoff, Hilmar, Vehreschild, Maria J. G. T., Krawczyk, Marcin, Nowag, Angela, Kretzschmar, Anne, Scholz, Claus, Kasper, Philipp, Roderburg, Christoph, Lammert, Frank, Goeser, Tobias, Steffen, Hans-Michael, and Demir, Muenevver

Abstract

Liver fibrosis is the major determinant of liver related complications in patients with non-alcoholic fatty liver disease (NAFLD). A gut microbiota signature has been explored to predict advanced fibrosis in NAFLD patients. The aim of this study was to validate and compare the diagnostic performance of gut microbiota-based approaches to simple non-invasive tools for the prediction of advanced fibrosis in NAFLD. 16S rRNA gene sequencing was performed in a cohort of 83 biopsy-proven NAFLD patients and 13 patients with non-invasively diagnosed NAFLD-cirrhosis. Random Forest models based on clinical data and sequencing results were compared with transient elastography, the NAFLD fibrosis score (NFS) and FIB-4 index. A Random Forest model containing clinical features and bacterial taxa achieved an area under the curve (AUC) of 0.87 which was only marginally superior to a model without microbiota features (AUC 0.85). The model that aimed to validate a published algorithm achieved an AUC of 0.71. AUC's for NFS and FIB-4 index were 0.86 and 0.85. Transient elastography performed best with an AUC of 0.93. Gut microbiota signatures might help to predict advanced fibrosis in NAFLD. However, transient elastography achieved the best diagnostic performance for the detection of NAFLD patients at risk for disease progression.

Published
2020

35. Maternal exercise conveys protection against NAFLD in the offspring via hepatic metabolic programming

Author

Bae-Gartz, Inga, Kasper, Philipp, Grossmann, Nora, Breuer, Saida, Janoschek, Ruth, Kretschmer, Tobias, Appel, Sarah, Schmitz, Lisa, Vohlen, Christina, Quaas, Alexander, Schweiger, Michal R., Grimm, Christina, Fischer, Axel, Ferrari, Nina, Graf, Christine, Frese, Christian K., Lang, Sonja, Demir, Muenevver, Schramm, Christoph, Fink, Gregor, Goeser, Tobias, Doetsch, Joerg, Hucklenbruch-Rother, Eva, Bae-Gartz, Inga, Kasper, Philipp, Grossmann, Nora, Breuer, Saida, Janoschek, Ruth, Kretschmer, Tobias, Appel, Sarah, Schmitz, Lisa, Vohlen, Christina, Quaas, Alexander, Schweiger, Michal R., Grimm, Christina, Fischer, Axel, Ferrari, Nina, Graf, Christine, Frese, Christian K., Lang, Sonja, Demir, Muenevver, Schramm, Christoph, Fink, Gregor, Goeser, Tobias, Doetsch, Joerg, and Hucklenbruch-Rother, Eva

Abstract

Maternal exercise (ME) during pregnancy has been shown to improve metabolic health in offspring and confers protection against the development of non-alcoholic fatty liver disease (NAFLD). However, its underlying mechanism are still poorly understood, and it remains unclear whether protective effects on hepatic metabolism are already seen in the offspring early life. This study aimed at determining the effects of ME during pregnancy on offspring body composition and development of NAFLD while focusing on proteomic-based analysis of the hepatic energy metabolism during developmental organ programming in early life. Under an obesogenic high-fat diet (HFD), male offspring of exercised C57BL/6J-mouse dams were protected from body weight gain and NAFLD in adulthood (postnatal day (P) 112). This was associated with a significant activation of hepatic AMP-activated protein kinase (AMPK), peroxisome proliferator-activated receptor alpha (PPAR alpha) and PPAR coactivator-1 alpha (PGC1 alpha) signaling with reduced hepatic lipogenesis and increased hepatic beta-oxidation at organ programming peak in early life (P21). Concomitant proteomic analysis revealed a characteristic hepatic expression pattern in offspring as a result of ME with the most prominent impact on Cholesterol 7 alpha-hydroxylase (CYP7A1). Thus, ME may offer protection against offspring HFD-induced NAFLD by shaping hepatic proteomics signature and metabolism in early life. The results highlight the potential of exercise during pregnancy for preventing the early origins of NAFLD.

Published
2020

36. Circulating levels of microRNA193a-5p predict outcome in early stage hepatocellular carcinoma

Author

Loosen, Sven H., Wirtz, Theresa H., Roy, Sanchari, Vucur, Mihael, Castoldi, Mirco, Schneider, Anne T., Koppe, Christiane, Ulmer, Tom F., Roeth, Anjali A., Bednarsch, Jan, Alizai, Patrick H., Paffenholz, Pia, Demir, Muenevver, Trautwein, Christian, Tacke, Frank, Neumann, Ulf P., Roderburg, Christoph, Luedde, Tom, Loosen, Sven H., Wirtz, Theresa H., Roy, Sanchari, Vucur, Mihael, Castoldi, Mirco, Schneider, Anne T., Koppe, Christiane, Ulmer, Tom F., Roeth, Anjali A., Bednarsch, Jan, Alizai, Patrick H., Paffenholz, Pia, Demir, Muenevver, Trautwein, Christian, Tacke, Frank, Neumann, Ulf P., Roderburg, Christoph, and Luedde, Tom

Abstract

While tumor resection and liver transplantation (LT) represent potentially curative therapeutic options for patients with early-stage hepatocellular carcinoma (HCC), the identification of the ideal surgical candidates has remained challenging. Just recently, miRNA-193a-5p was described as a tumor suppressor in murine and human HCC but only little is known about circulating miRNA-193a-5p in HCC patients. Here, we evaluated serum levels of miR-193a-5p by qPCR in 41 HCC patients undergoing tumor resection (n = 33) or LT (n = 8) and 20 controls. Circulating relative miR-193a-5p levels were significantly elevated in HCC patients compared to healthy controls. While relative miR-193a-5p levels were comparable between patients of different underlying disease etiology and tumor size, high relative miR-193a-5p levels were predictive for the patients' postoperative outcome, which was confirmed in uni- and multivariate Cox-regression analysis. As such, HCC patients with a preoperative relative miR-193a-5p level above the ideal cut-off value (3.57) had a median overall survival (OS) of only 451 days compared to 1158 days in patients with a relative miR-193a-5p level below this cut-off value. Our data support a novel function of miR-193a-5p as a biomarker in early-stage HCC patients that might help to identify the best surgical candidates in terms of postoperative outcome.

Published
2020

37. Intestinal Virome Signature Associated With Severity of Nonalcoholic Fatty Liver Disease

Author

Lang, Sonja, Demir, Muenevver, Martin, Anna, Jiang, Lu, Zhang, Xinlian, Duan, Yi, Gao, Bei, Wisplinghoff, Hilmar, Kasper, Philipp, Roderburg, Christoph, Tacke, Frank, Steffen, Hans-Michael, Goeser, Tobias, Abraldes, Juan G., Tu, Xin M., Loomba, Rohit, Starkel, Peter, Pride, David, Fouts, Derrick E., Schnabl, Bernd, Lang, Sonja, Demir, Muenevver, Martin, Anna, Jiang, Lu, Zhang, Xinlian, Duan, Yi, Gao, Bei, Wisplinghoff, Hilmar, Kasper, Philipp, Roderburg, Christoph, Tacke, Frank, Steffen, Hans-Michael, Goeser, Tobias, Abraldes, Juan G., Tu, Xin M., Loomba, Rohit, Starkel, Peter, Pride, David, Fouts, Derrick E., and Schnabl, Bernd

Abstract

BACKGROUND & AIMS: Alterations in the gut microbiome have been associated with the severity of nonalcoholic fatty liver disease (NAFLD). Previous studies focused exclusively on the bacteria in the microbiome; we investigated changes in the viral microbiome (virome) in patients with NAFLD. METHODS: In a prospective, cross-sectional, observational study, we extracted RNA and DNA virus-like particles from fecal samples from 73 patients with NAFLD: 29 patients had an NAFLD Activity Score (NAS) of 0-4, 44 patients had an NAS of 5-8 or liver cirrhosis (LCI), 37 patients had F0-F1 fibrosis, and 36 patients had F2-F4 fibrosis. As controls, 9 individuals without liver disease and 13 patients with mild primary biliary chol-angitis were included in the analysis. We performed shotgun metagenomic sequencing of virus-like particles. RESULTS: Patients with NAFLD and NAS 5-8/LCI had a significant decrease in intestinal viral diversity compared with patients with NAFLD and NAS 0-4 or control individuals. The presence of more advanced NAFLD was associated with a significant reduction in the proportion of bacteriophages compared with other intestinal viruses. Using multivariate logistic regression analysis with leave-1-out cross validation, we developed a model, including a viral diversity index and simple clinical variables, that identified patients with NAS 5- 8/LCI with an area under the curve of 0.95 (95% confidence interval, 0.91-0.99) and F2-F4 fibrosis with an area under the curve of 0.88 (95% confidence interval, 0.80-0.95). Addition of data on viral diversity significantly improved multivariate models, including those based on only clinical parameters or bacterial diversity. CONCLUSIONS: In a study of fecal viromes from patients with NAFLD and control individuals, we associated histologic markers of NAFLD severity with significant decreases in viral diversity and proportion of bacteriophages. We developed a model based on fecal viral diversity and clinical data that identifie

Published
2020

38. Hepatocellular carcinoma surveillance with liver imaging is not associated with improved survival

Author

Lang, Sonja, Martin, Anna, Kasper, Philipp, Schramm, Christoph, Kuetting, Fabian, Goeser, Tobias, Steffen, Hans-Michael, Demir, Muenevver, Lang, Sonja, Martin, Anna, Kasper, Philipp, Schramm, Christoph, Kuetting, Fabian, Goeser, Tobias, Steffen, Hans-Michael, and Demir, Muenevver

Abstract

Objective: International guidelines recommend hepatocellular carcinoma (HCC) surveillance with ultrasound in high-risk patients with chronic liver diseases. However, there is low-strength evidence about the effects on mortality. The aim of our study was to assess the impact of surveillance on the clinical course and survival of HCC patients seen at a tertiary referral center in Germany. Material and methods: We retrospectively evaluated the data of 401 HCC patients, who presented to our clinic between 1997 and 2015. Two groups were compared regarding patient and disease outcomes: one group included patients who received at least two ultrasound examinations for surveillance purposes prior to first diagnosis (n = 111). The other group consisted of patients with HCC at first presentation without foregoing HCC surveillance (n = 290). Results: Median follow-up in the surveillance group was 76 months (range 4-310 months). Patients in the surveillance group had smaller median tumor sizes (3.5 cm vs. 4.5 cm; p < .001), fulfilled more often Milan criteria (64% vs. 42%; p < .001) and received more often liver transplantation (27% vs. 9%, p < .001) when compared with the non-surveillance group. However, HCC surveillance was not associated with an improved survival (14 months in the surveillance group vs. 12 months in the non-surveillance group, p = .375), hazard ratio regarding overall mortality for the surveillance group: 0.80 (95% CI: 0.62-1.04, p = .09). Conclusions: HCC surveillance with ultrasound led to the detection of earlier disease stages but was not significantly associated with improved survival. Further prospective and long-term studies are needed to clarify benefits and harms of HCC surveillance programs on mortality.

Published
2020

40. Serum levels of bone sialoprotein correlate with portal pressure in patients with liver cirrhosis

Author

Benz, Fabian, primary, Bogen, Andreas, additional, Praktiknjo, Michael, additional, Jansen, Christian, additional, Meyer, Carsten, additional, Wree, Alexander, additional, Demir, Muenevver, additional, Loosen, Sven, additional, Vucur, Mihael, additional, Schierwagen, Robert, additional, Tacke, Frank, additional, Trebicka, Jonel, additional, and Roderburg, Christoph, additional

Published
2020
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42. Heterozygous carriage of the alpha1-antitrypsin Pi*Z variant increases the risk to develop liver cirrhosis

Author

Strnad, Pavel, Buch, Stephan, Hamesch, Karim, Fischer, Janett, Rosendahl, Jonas, Schmelz, Renate, Brueckner, Stefan, Brosch, Mario, Heimes, Carolin V., Woditsch, Vivien, Scholten, David, Nischalke, Hans Dieter, Janciauskiene, Sabina, Mandorfer, Mattias, Trauner, Michael, Way, Michael J., McQuillin, Andrew, Reichert, Matthias C., Krawczyk, Marcin, Casper, Markus, Lammert, Frank, von Schoenfels, Witigo, Hinz, Sebastian, Burmeister, Greta, Hellerbrand, Claus, Teufel, Andreas, Feldman, Alexandra, Schattenberg, Joern M., Bantel, Heike, Pathil, Anita, Demir, Muenevver, Kluwe, Johannes, Boettler, Tobias, Ridinger, Monika, Wodarz, Norbert, Soyka, Michael, Rietschel, Marcella, Kiefer, Falk, Weber, Thomas, Marhenke, Silke, Vogel, Arndt, Hinrichsen, Holger, Canbay, Ali, Schlattjan, Martin, Sosnowsky, Katharina, Sarrazin, Christoph, von Felden, Johann, Geier, Andreas, Deltenre, Pierre, Sipos, Bence, Schafmayer, Clemens, Nothnagel, Michael, Aigner, Elmar, Datz, Christian, Stickel, Felix, Morgan, Marsha Yvonne, Hampe, Jochen, Berg, Thomas, Trautwein, Christian, Strnad, Pavel, Buch, Stephan, Hamesch, Karim, Fischer, Janett, Rosendahl, Jonas, Schmelz, Renate, Brueckner, Stefan, Brosch, Mario, Heimes, Carolin V., Woditsch, Vivien, Scholten, David, Nischalke, Hans Dieter, Janciauskiene, Sabina, Mandorfer, Mattias, Trauner, Michael, Way, Michael J., McQuillin, Andrew, Reichert, Matthias C., Krawczyk, Marcin, Casper, Markus, Lammert, Frank, von Schoenfels, Witigo, Hinz, Sebastian, Burmeister, Greta, Hellerbrand, Claus, Teufel, Andreas, Feldman, Alexandra, Schattenberg, Joern M., Bantel, Heike, Pathil, Anita, Demir, Muenevver, Kluwe, Johannes, Boettler, Tobias, Ridinger, Monika, Wodarz, Norbert, Soyka, Michael, Rietschel, Marcella, Kiefer, Falk, Weber, Thomas, Marhenke, Silke, Vogel, Arndt, Hinrichsen, Holger, Canbay, Ali, Schlattjan, Martin, Sosnowsky, Katharina, Sarrazin, Christoph, von Felden, Johann, Geier, Andreas, Deltenre, Pierre, Sipos, Bence, Schafmayer, Clemens, Nothnagel, Michael, Aigner, Elmar, Datz, Christian, Stickel, Felix, Morgan, Marsha Yvonne, Hampe, Jochen, Berg, Thomas, and Trautwein, Christian

Abstract

Objective Homozygous alpha1-antitrypsin (AAT) deficiency increases the risk for developing cirrhosis, whereas the relevance of heterozygous carriage remains unclear. Hence, we evaluated the impact of the two most relevant AAT variants (' Pi* Z' and ' Pi* S'), present in up to 10% of Caucasians, on subjects with non-alcoholic fatty liver disease (NAFLD) or alcohol misuse. Design We analysed multicentric case-control cohorts consisting of 1184 people with biopsy-proven NAFLD and of 2462 people with chronic alcohol misuse, both cohorts comprising cases with cirrhosis and controls without cirrhosis. Genotyping for the Pi* Z and Pi* S variants was performed. Results T he Pi* Z variant presented in 13.8% of patients with cirrhotic NAFLD but only in 2.4% of counterparts without liver fibrosis (p< 0.0001). Accordingly, the Pi* Z variant increased the risk of NAFLD subjects to develop cirrhosis (adjusted OR=7.3 (95% CI 2.2 to 24.8)). Likewise, the Pi* Z variant presented in 6.2% of alcohol misusers with cirrhosis but only in 2.2% of alcohol misusers without significant liver injury (p< 0.0001). Correspondingly, alcohol misusers carrying the Pi* Z variant were prone to develop cirrhosis (adjusted OR=5.8 (95% CI 2.9 to 11.7)). In contrast, the Pi* S variant was not associated with NAFLDrelated cirrhosis and only borderline with alcohol-related cirrhosis (adjusted OR=1.47 (95% CI 0.99 to 2.19)). Conclusion T he Pi* Z variant is the hitherto strongest single nucleotide polymorphism-based risk factor for cirrhosis in NAFLD and alcohol misuse, whereas the Pi* S variant confers only a weak risk in alcohol misusers. As 2%-4% of Caucasians are Pi* Z carriers, this finding should be considered in genetic counselling of affected individuals.

Published
2019

44. FIB-4 Is a Potential Tool for Hepatocellular Carcinoma Risk Stratification in Ethnically Diverse Chronic Hepatitis B Patients When Using Specific Cutoff Values

Author

Kuetting, Fabian, Lang, Sonja, Schramm, Christoph, Kasper, Philipp, Goeser, Tobias, Steffen, Hans-Michael, Demir, Muenevver, Kuetting, Fabian, Lang, Sonja, Schramm, Christoph, Kasper, Philipp, Goeser, Tobias, Steffen, Hans-Michael, and Demir, Muenevver

Abstract

Background: In a previous publication, a FIB-4 cutoff value of >= 1.25, which had been determined in an Asian population, did not allow reliable prediction of the development of hepatocellular carcinoma (HCC) in a patient collective with chronic hepatitis B (CHB) of predominantly non-Asian descent. Objectives: Here, we aimed to validate the modified FIB-4 cutoff values as a means of stratifying the HCC risk in a non-Asian cohort seen at an outpatient university hospital liver unit in Germany. Methods: We retrospectively analyzed 350 adult patients with CHB infection. We recorded demographics, laboratory parameters, results from liver imaging, serological hepatitis B markers, antiviral treatment, and histology. We separated patients into two groups based on individual FIB-4 levels. We, then, analyzed the patients' hazard ratios for HCC and adjusted it for sex, age, antiviral medication, duration of CHB infection, body mass index, alcohol consumption, and type 2 diabetes. An additional sub-analysis was performed by including only non-cirrhotic patients to determine the validity of the proposed cutoffs in that cohort. Results: The median duration of follow-up was 8.9 years with a range of 1- 21.3 years. Our patients were 65% males. In comparison with patients that had a low FIB-4 (< 0.3635), those with elevated FIB-4 (>= 0.3635) had an HCC incidence hazard ratio of 11.67 (95% confidence interval (CI): 2.73 - 49.96; P = 0.001) and an adjusted hazard ratio of 7.90 (95% CI: 1.58 - 39.39; P = 0.012). Elevated FIB-4 non-cirrhotic patients had a hazard ratio (HR) of 15.88 (95% CI: 2.04 - 123.20) for HCC incidence (P < 0.0001) and an adjusted HR of 11.99 (95% CI:1.36 -105.72) (P = 0.001). Conclusions: A FIB-4 value of < 0.3635 appears to be a clinical indicator for a low likelihood of HCC incidence in non-Asian patients with CHB with or without cirrhosis. Further studies in patients of diverse descent are necessary to prove its utility as a clinical tool in this setting.

Published
2019

45. Could inherited predisposition drive non-obese fatty liver disease? Results from German tertiary referral centers

Author

Krawczyk, Marcin, Bantel, Heike, Rau, Monika, Schattenberg, Joern M., Gruenhage, Frank, Pathil, Anita, Demir, Muenevver, Kluwe, Johannes, Boettler, Tobias, Weber, Susanne N., Geier, Andreas, Lammert, Frank, Krawczyk, Marcin, Bantel, Heike, Rau, Monika, Schattenberg, Joern M., Gruenhage, Frank, Pathil, Anita, Demir, Muenevver, Kluwe, Johannes, Boettler, Tobias, Weber, Susanne N., Geier, Andreas, and Lammert, Frank

Abstract

Non-alcoholic fatty liver disease (NAFLD) is frequent among obese individuals with metabolic syndrome. Variants PNPLA3 p.I148M, TM6SF2 p.E167K and MBOAT7 rs641738 are associated with higher liver fat contents. Here we analyzed 63 biopsied non-obese, non-diabetic patients with NAFLD (39 men, age: 20-72 years) recruited within the German NAFLD CSG program. The frequencies of the PNPLA3, TM6SF2 and MBOAT7 polymorphisms were compared with the remaining patients in the NAFLD CSG cohort and with a control population (n = 174). Serum CK18-M30 was measured by ELISA. In non-obese NAFLD patients, the frequency of the PNPLA3 p.I148M allele (74.6%), but not of the TM6SF2 or MBOAT7 polymorphisms, was significantly (P < 0.05) higher as compared to the other patients in the NAFLD CSG cohort (54.9%) or controls (40.2%). The presence of the minor PNPLA3 p.I148M risk allele increased the risk of developing NAFLD (OR = 3.29, P < 0.001) and was associated with higher steatosis, fibrosis, and serum CK18-M30 levels (all P < 0.05). According to the population attributable fraction (PAF), 49.8% of NAFLD cases could be eliminated if the PNPLA3 mutation was absent. The MBOAT7 polymorphism was more frequent (P = 0.019) in patients with severe hepatic steatosis. In conclusion, PNPLA3, and to a lesser extent, MBOAT7 variants are associated with NAFLD risk and modulate liver injury in non-obese patients without diabetes.

Published
2018

47. Self‐limited HBV infection of the recipient does not reactivate after liver transplantation: Observations from a 30‐year liver transplant program.

Author

Ossami Saidy, R.R., Demir, Muenevver, Nibbe, Pauline, Dobrindt, Eva‐Maria, Oellinger, Robert, Schoening, Wenzel, Pratschke, Johann, and Eurich, Dennis

Subjects
*LIVER transplantation, *HEPATITIS associated antigen, *HEPATITIS B, *HEPATITIS C
Abstract

Background: A self‐limited hepatitis B infection can reactivate in patients under immunosuppression or chemotherapy (reappearance of hepatitis B surface antigen (HBsAg) or HBV‐DNA). Exact circumstances of HBV reactivation in patients undergoing liver transplantation (LT) for end‐stage liver diseases (ESLD) unrelated to HBV are unknown, and recommendations on HBV prophylaxis remain unclear. Patients and methods: Among 1273 liver transplants, 168 patients with a self‐limited HBV hepatitis B infection prior to LT were identified from our prospective liver transplant database. Patients with underlying chronic HBV infection and recipients of an anti‐HBc‐positive liver were not included in the analysis. Demographic, laboratory, serological, and virological data were analyzed retrospectively. Appearance of HBsAg or HBV‐DNA was defined as reactivation. Results: The median follow‐up after LT was 12.0 years (0.6‐30.7 years). The rate of HBV reactivation was 0% independent of antiviral prophylaxis (n = 7; 4.2%), the etiology of ESLD, hepatitis C treatment, or the anti‐HBs concentration. The overall patient survival with a history of a self‐limited HBV infection before LT did not significantly differ from the rest of the cohort. Conclusion: Antiviral treatment with nucleos(t)ide analogues post‐liver transplantation in order to prevent HBV reactivation in patients with a resolved self‐limited hepatitis B infection prior to LT seems to be omittable since the main viral reservoir is removed by the hepatectomy. These findings may clarify the current uncertainty in the recommendations regarding the risk of HBV reactivation in patients with self‐limited hepatitis B prior to LT. [ABSTRACT FROM AUTHOR]

Published
2021
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48. Heterozygous carriage of the alpha1-antitrypsin Pi*Z variant increases the risk to develop liver cirrhosis

Author

Strnad, Pavel, primary, Buch, Stephan, additional, Hamesch, Karim, additional, Fischer, Janett, additional, Rosendahl, Jonas, additional, Schmelz, Renate, additional, Brueckner, Stefan, additional, Brosch, Mario, additional, Heimes, Carolin V, additional, Woditsch, Vivien, additional, Scholten, David, additional, Nischalke, Hans Dieter, additional, Janciauskiene, Sabina, additional, Mandorfer, Mattias, additional, Trauner, Michael, additional, Way, Michael J, additional, McQuillin, Andrew, additional, Reichert, Matthias C, additional, Krawczyk, Marcin, additional, Casper, Markus, additional, Lammert, Frank, additional, Braun, Felix, additional, von Schönfels, Witigo, additional, Hinz, Sebastian, additional, Burmeister, Greta, additional, Hellerbrand, Claus, additional, Teufel, Andreas, additional, Feldman, Alexandra, additional, Schattenberg, Joern M, additional, Bantel, Heike, additional, Pathil, Anita, additional, Demir, Muenevver, additional, Kluwe, Johannes, additional, Boettler, Tobias, additional, Ridinger, Monika, additional, Wodarz, Norbert, additional, Soyka, Michael, additional, Rietschel, Marcella, additional, Kiefer, Falk, additional, Weber, Thomas, additional, Marhenke, Silke, additional, Vogel, Arndt, additional, Hinrichsen, Holger, additional, Canbay, Ali, additional, Schlattjan, Martin, additional, Sosnowsky, Katharina, additional, Sarrazin, Christoph, additional, von Felden, Johann, additional, Geier, Andreas, additional, Deltenre, Pierre, additional, Sipos, Bence, additional, Schafmayer, Clemens, additional, Nothnagel, Michael, additional, Aigner, Elmar, additional, Datz, Christian, additional, Stickel, Felix, additional, Morgan, Marsha Yvonne, additional, Hampe, Jochen, additional, Berg, Thomas, additional, and Trautwein, Christian, additional

Published
2018
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49. Insufficient evidence of benefit regarding mortality due to albumin substitution in HCC-free cirrhotic patients undergoing large volume paracentesis

Author

Kuetting, Fabian, Schubert, Jens, Franklin, Jeremy, Bowe, Andrea, Hoffmann, Vera, Demir, Muenevver, Pelc, Agnes, Nierhoff, Dirk, Toex, Ulrich, Steffen, Hans-Michael, Kuetting, Fabian, Schubert, Jens, Franklin, Jeremy, Bowe, Andrea, Hoffmann, Vera, Demir, Muenevver, Pelc, Agnes, Nierhoff, Dirk, Toex, Ulrich, and Steffen, Hans-Michael

Abstract

BackgroundCurrent guidelines for clinical practice recommend the infusion of human albumin after large volume paracentesis. After inspecting the current evidence behind this recommendation, we decided to conduct a systematic review and meta-analysis in order to address the effect of albumin on mortality and morbidity in the context of large volume paracentesis. MethodsWe performed a comprehensive search of large databases and abstract books of conference proceedings up to March 15th 2016 for randomized controlled trials, testing the infusion of human albumin against alternatives (vs no treatment, vs plasma expanders; vs vasoconstrictors) in HCC-free patients suffering from cirrhosis. We analyzed these trials with regard to mortality, changes in plasma renin activity (PRA), hyponatremia, renal impairment, recurrence of ascites with consequential re-admission into hospital and additional complications. We employed trial sequential analysis in order to calculate the number of patients required in controlled trials to be able to determine a statistically significant advantage of the administration of one agent over another with regard to mortality. ResultsWe were able to include 21 trials totaling 1277 patients. While the administration of albumin prevents a rise in PRA as well as hyponatremia, no improvement in strong clinical endpoints such as mortality could be demonstrated. Trial sequential analysis showed that at least 1550 additional patients need to be recruited into RCTs and analyzed with regard to this question in order to detect or disprove a 25% mortality effect. ConclusionsThere is insufficient evidence that the infusion of albumin after LVP significantly lowers mortality in HCC-free patients with advanced liver disease.

Published
2017

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