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512A AASLD ABSTRACTS HEPATOLOGY, October, 2015 Mitchell L. Shiffman - Advisory Committees or Review Panels: Merck, Gilead, Boehringer-Ingelheim, Bristol-Myers-Squibb, Abbvie, Janssen, Acchillion; Consulting: Roche/Genentech; Grant/Research Support: Merck, Gilead, Boehringer-Ingelheim, Bristol-Myers-Squibb, Abbvie, Beckman-Coulter, Achillion, Lumena, Intercept, Novartis, Gen-Probe; Speaking and Teaching: Roche/Genentech, Merck, Gilead, Abbvie, Janssen, Bayer Karel J. van Erpecum - Advisory Committees or Review Panels: Bristol Meyers Squibb, Abbvie, Janssen Cilag, Gilead Roya Hooshmand-Rad - Employment: Intercept pharmaceuticals Inc. Shawn Sheeron - Employment: Intercept Pharmaceuticals David Shapiro - Employment: Inttercept Pharmaceuticals; Management Position: Intercept Pharmaceuticals; Stock Shareholder: Intercept Pharmaceuticals The following authors have nothing to disclose: Giuseppe Mazzella, Pietro Invernizzi, Joost Drenth, Jaroslaw Regula, Annarosa Floreani, Velimir A. Luketic, Victor Vargas, Catherine Vincent, Bettina E. Hansen 610 Patients with Primary Biliary Cirrhosis Experience Progressive Bone Loss Over Time Beyond that Expected by Age and Despite Routine Clinical Care Aliya Gulamhusein 1 , Bryan McCauley 2 , Elizabeth J. Atkinson 2 , Brian D. Juran 1 , Erik M. Schlicht 1 , Mariza de Andrade 2 , Konstantinos Lazaridis 1 ; 1 Center for Basic Research in Digestive Diseases, Mayo Clinic, Rochester, Rochester, MN; 2 Health Science Research, Mayo Clinic, Rochester, MN Background and Aims: Osteopenia and osteoporosis are characterized by low bone mass and increased fracture risk. Previous reports suggest that patients with primary biliary cirrhosis (PBC) are at increased risk of osteoporosis with estimates varying between 15-50%, but study populations and testing approaches have been heterogeneous. Furthermore, the rate of bone loss in these patients is poorly understood. We sought to estimate the prevalence of low bone mass and characterize the change in bone mineral density (BMD) over time in a large cohort of patients with PBC. Methods: We identified patients recruited to the Mayo Clinic PBC Genetic Epidemiology Registry and Biorepository who had available dual X-ray absorptiometry (DXA) scans for assessment of BMD. Those with comorbid autoimmune hepatitis were excluded and data was censored at the time of liver transplant. Femoral neck (FN) BMD (g/cm 2 ) and T-score were used to assess bone loss. Per WHO criteria, osteopenia was defined as a T-score of < -1 but > -2.5 and osteoporosis as a T-score of ≤ -2.5. Linear mixed effects models were fit on subjects with multiple scans to estimate the changes in BMD over time using gender, age, and time since diagnosis as covariates. Results: 383 patients with 885 DXA scans were included. There were 813 scans on 348 women and 71 scans on 35 men. The median number of scans per subject was 2 (25%-75% IQR=1-3) and follow-up was over 9.2 years (25%-75% IQR=3.4-16.4). The prevalence of low bone mass (osteopenia or osteoporosis) in all patients aged
HEPATOLOGY, VOLUME 62, NUMBER 1 (SUPPL) AASLD ABSTRACTS 513A Disclosures: David Jones - Consulting: Intercept, Pfizer, Novartis; Speaking and Teaching: Falk, Shire The following authors have nothing to disclose: Claire Hardie, Kile J. Green, Sarah Pagan, Jessica K. Dyson, Lucy J. Walker, Laura Jopson, John G. Brain 612 Vitamin A deficiency promotes hepatic expansion of resident (Kupffer cells) and peripheral (Gr hi ) macrophages leading to excessive liver damage in rats with obstructive cholestasis Ali Saeed, Mark Hoekstra, Martijn O. Hoeke, Janette Heegsma, Han Moshage, Klaas Nico Faber; Department of Gastroenterology and Hepatology, University Medical Center Groningen, Groningen, University of Groningen, The Netherlands, Groningen, Netherlands Vitamin A deficiency (VAD) is associated with chronic liver diseases (CLD), including biliary atresia, primary biliary cirrhosis, primary sclerosing cholangitis and non-alcoholic fatty liver disease. Serum and/or hepatic retinol levels negatively correlate with disease progression. Previously, we found that VAD rats shown much more severe liver damage when exposed to bile duct ligation (BDL) compared to rats with sufficient vitamin A (VAS) levels, but the mechanisms involved remain unresolved so far. Vitamin A has potent anti-inflammatory properties and therefore we investigated its effect on resident (Kupffer cells) and peripheral (Gr hi ) macrophages in vitro and in vivo. Weaning male Wister rats were fed either a VAS or a VAD diet for 14-16 weeks, followed by BDL for 1, 2, 4, 7 days. One group subjected to 7-day BDL received retinyl-palmitate therapy. Liver damage marker were analysed in serum, and liver tissue was analysed with Q-PCR, Western blotting and immunohistochemistry. Primary rat Kupffer cells and THP-1 (human Leukemic monocyte cell line) cells were exposed to VAS and VAD conditions and cytokine expression was analysed by Q-PCR. CD68 (general macrophage marker) and CD11b (peripheral macrophages) positive cells were significantly increased in livers of VAD rats after 4- and 7-day BDL as compare to VAS-BDL control livers, and was associated with increased plasma γGT levels and expression of liver fibrosis makers, such as α-SMA and Collagen1A1. All these features were strongly suppressed in VAD-BDL rats receiving vitamin A therapy. In line, expression of the macrophage chemoattractant Ccl2 was significantly increased in VAD-BDL livers and suppressed by vitamin A therapy. VAD-BDL livers showed increased expression of proinflammatory and profibrotic markers, such as iNos, Tnf-α, Il-1, Il-6, Cox-2, Tgf-β and vitamin A therapy decreased this inflammatory response. In vitro, VAD (RPMI with lipid-stripped serum) caused an inflammatory polarization in primary Kupffer cells and PMA-activated-THP-1 cells as compare to control cells and increased the expression of inflammatory markers, including iNos, Tnf-α, Il-1, Il-6, Cox-2. The vitamin A metabolites, 9-cis retinoic acid and all trans retinoic acid, reduced expression of these inflammatory markers. In conclusion, vitamin A deficiency promotes hepatic macrophage expansion in obstructive cholestasis, which show an aggressive pro-inflammatory and pro-fibrotic phenotype that aggravates liver damage, but is effectively prevented by vitamin A supplementation. This study supports an direct role of vitamin A in preventing excessive liver damage in patients with chronic liver diseases. Disclosures: The following authors have nothing to disclose: Ali Saeed, Mark Hoekstra, Martijn O. Hoeke, Janette Heegsma, Han Moshage, Klaas Nico Faber 613 The Modulation of Co-stimulatory Molecules by Circulating Exosomes in Primary Biliary Cirrhosis Takashi Tomiyama 1,2 , Guo-Xiang Yang 1 , Ming Zhao 4 , Weici Zhang 1 , Hajime Tanaka 1,5 , Jing Wang 4 , Patrick S. Leung 1 , Kazuichi Okazaki 2 , Xiao-Song He 1 , Quiajin Lu 4 , Ross L. Coppel 3 , Christopher L. Bowlus 1 , M. Eric Gershwin 1 ; 1 Internal Medicine, University of California, Davis, CA; 2 Third Department of Internal Medicine, Division of Gastroenterology and Hepatology, Kansai Medical University, Osaka, Japan; 3 Department of Microbiology, Monash University, Melbourne, VIC, Australia; 4 Department of Dermatology, The Second Xiangya Hospital, Central South University, Hunan, China; 5 Department of Gastroenterology and Metabolism, Nagoya City University Graduate School of Medical Sciences, Nagoya, Japan Background: Exosomes are secreted intracellular microparticles that can induce antigen-specific immune responses and potentially trigger inflammation. The role of exosomes in autoimmunity has drawn significant attention because of their ability to modulate cell-to-cell communications in part by their ability to regulate cytokine and chemokine activation. However, the contribution of exosomes in autoimmune cholangitis has not been addressed. Herein, we studied the effect of exosomes from patients with primary biliary cirrhosis (PBC) and healthy controls (HCs) on cytokine production and co-stimulatory molecule expression in peripheral mononuclear cell populations. Further, we also determined the micro RNA (miRNA) profiles of circulating exosomes and verified with an independent cohort. Methods: Exosomes were purified from plasma from 28 patients with PBC and 25 HCs. Their effect on cytokine production and co-stimulatory molecule expression in mononuclear cell populations were examined using an ex vivo system. In addition, miR- NAs profile of the exosomes was measured by Agilent Human miRNA (8*60K) V19.0 microarray. miRNAs with a level of 2-fold or larger difference between groups were considered differentially expressed and verified using isolated exosomes from additional groups of PBC and HC using a Taqman PCR assay for individual miRNAs. Further, we examined whether the levels of these exosomal miRNAs correlated with severity of disease. Results: Our data showed that circulating exosomes from PBC are taken up by antigen presenting cells (APCs) and affect the expression of cell surface co-stimulatory molecules CD80, CD86 and CD40 on APCs. Circulating exosomes in PBC contain altered patterns of miRNA expression with 9 miR- NAs significantly up-regulated and another 9 miRNAs significantly down-regulated when compared to the HC. Conclusions: Exosomes significantly alter co-stimulatory molecule expression on antigen presenting cell populations and there were differences of miRNA expression in circulating exosomes in patients with PBC. The rigorous dissection of exosomes and their constituents is an important component for analysis to understand the nature of the pathogenic effects produced during the natural history of autoimmune cholangitis. Disclosures: Christopher L. Bowlus - Advisory Committees or Review Panels: Gilead Sciences, Inc; Grant/Research Support: Gilead Sciences, Inc, Intercept Pharmaceuticals, Bristol Meyers Squibb, Takeda, Lumena, Merck; Speaking and Teaching: Gilead Sciences, Inc The following authors have nothing to disclose: Takashi Tomiyama, Guo-Xiang Yang, Ming Zhao, Weici Zhang, Hajime Tanaka, Jing Wang, Patrick S. Leung, Kazuichi Okazaki, Xiao-Song He, Quiajin Lu, Ross L. Coppel, M. Eric Gershwin
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1312A AUTHOR INDEX HEPATOLOGY, Octo
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1366A CATEGORY INDEX HEPATOLOGY, Oc
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