Your search keyword '"Kelly McDaniel"' showing total 58 results

1. Rehabilitation through empowerment: adopting the consumer-participation model for treatment planning in mental health courts.

Author

Kelly, McDaniel M.

Subjects

Mental health courts -- Practice, Recidivism -- Prevention, Mental health services -- Models, Offender reintegration -- Models

Abstract

CONTENTS INTRODUCTION I. THE MENTAL HEALTH COURT SYSTEM A. The Goals and Successes of Mental Health Courts B. Mental Health Court Structure and Operation II. BARRIERS TO VOLUNTARINESS IN MENTAL [...]

Published

2015

2. Amelioration of Ductular Reaction by Stem Cell Derived Extracellular Vesicles in MDR2 Knockout Mice via Lethal‐7 microRNA

Author

Heather Francis, Shannon Glaser, Nan Wu, Demeng Chen, Tianhao Zhou, Sugeily Ramos-Lorenzo, Fanyin Meng, Pietro Invernizzi, Li Huang, Kelly McDaniel, Julie Venter, Gianfranco Alpini, Francesca Bernuzzi, Ludovica Ceci, Chaodong Wu, Keisaku Sato, Mcdaniel, K, Wu, N, Zhou, T, Huan, L, Sato, K, Venter, J, Ceci, L, Chen, D, Ramos-Lorenzo, S, Invernizzi, P, Bernuzzi, F, Wu, C, Francis, H, Glaser, S, Alpini, G, and Meng, F

Subjects

ductular reaction, Liver Cirrhosis, 0301 basic medicine, Cell signaling, ATP Binding Cassette Transporter, Subfamily B, liver stem cells, Cholangitis, Sclerosing, Liver Stem Cell, Real-Time Polymerase Chain Reaction, LIN28, Sensitivity and Specificity, Article, Cholangiocyte, Mice, Random Allocation, 03 medical and health sciences, 0302 clinical medicine, MED/12 - GASTROENTEROLOGIA, Risk Factors, Fibrosis, medicine, Animals, Humans, Secretion, Cells, Cultured, Mice, Knockout, Hepatology, Chemistry, Stem Cells, liver fibrosi, Cell Differentiation, Primary sclerosing cholangiti, medicine.disease, Cell biology, Disease Models, Animal, MicroRNAs, 030104 developmental biology, Hepatocytes, Hepatic stellate cell, Female, 030211 gastroenterology & hepatology, extracellular vesicle, Stem cell

Abstract

Cholangiopathies are diseases that affect cholangiocytes, the cells lining the biliary tract. Liver stem cells (LSCs) are able to differentiate into all cells of the liver and possibly influence the surrounding liver tissue by secretion of signaling molecules. One way in which cells can interact is through secretion of extracellular vesicles (EVs), which are small membrane-bound vesicles that contain proteins, microRNAs (miRNAs), and cytokines. We evaluated the contents of liver stem cell–derived EVs (LSCEVs), compared their miRNA contents to those of EVs isolated from hepatocytes, and evaluated the downstream targets of these miRNAs. We finally evaluated the crosstalk among LSCs, cholangiocytes, and human hepatic stellate cells (HSCs). We showed that LSCEVs were able to reduce ductular reaction and biliary fibrosis in multidrug resistance protein 2 (MDR2)(−/−) mice. Additionally, we showed that cholangiocyte growth was reduced and HSCs were deactivated in LSCEV-treated mice. Evaluation of LSCEV contents compared with EVs derived from hepatocytes showed a large increase in the miRNA, lethal-7 (let-7). Further evaluation of let-7 in MDR2(−/−) mice and human primary sclerosing cholangitis samples showed reduced levels of let-7 compared with controls. In liver tissues and isolated cholangiocytes, downstream targets of let-7 (identified by ingenuity pathway analysis), Lin28a (Lin28 homolog A), Lin28b (Lin28 homolog B), IL-13 (interleukin 13), NR1H4 (nuclear receptor subfamily 1 group H member 4) and NF-κB (nuclear factor kappa B), are elevated in MDR2(−/−) mice, but treatment with LSCEVs reduced levels of these mediators of ductular reaction and biliary fibrosis through the inhibition of NF-κB and IL-13 signaling pathways. Evaluation of crosstalk using cholangiocyte supernatants from LSCEV-treated cells on cultured HSCs showed that HSCs had reduced levels of fibrosis and increased senescence. CONCLUSION: Our studies indicate that LSCEVs could be a possible treatment for cholangiopathies or could be used for target validation for future therapies.

Published

2019

3. Mutterhunger : Der alles verzehrende Wunsch nach Liebe. Wie Frauen den Verlust von kindlicher Geborgenheit bewältigen und innere Stärke finden

Author

Kelly McDaniel and Kelly McDaniel

Abstract

Es fühlt sich an wie eine Bürde, die alles bestimmt: das unstillbare Bedürfnis nach Geliebtwerden, glücklose Beziehungen, exzessives Essen, der Drang nach Alkohol oder anderen Ersatzbefriedigungen, um die innere Leere zu füllen. Dahinter steckt eine tiefe Sehnsucht nach mütterlicher Liebe. Doch es gibt Wege aus dem Teufelskreis destruktiver Verhaltensweisen und orientierungsloser Suche in ein erfülltes Leben mit gesunden Beziehungen. Traumatherapeutin Kelly McDaniel zeigt, wie in der Kindheit versäumte Fürsorge, Schutz und Führung zurückgeholt werden können, die für die Entwicklung des Urvertrauens unerlässlich sind. Ihre eindringliche Botschaft: Damit Heilung geschehen kann, müssen wir zunächst benennen, was uns fehlt! Mit »Mutterhunger« gibt sie diesem Schmerz erstmals einen Namen und beleuchtet somit das mit Scham behaftete Gefühl von Bedürftigkeit. Von emotionalem Missbrauch bis zu schwerer Vernachlässigung – dieser Leitfaden liefert den Kompass, um den Kampf mit der Einsamkeit zu beenden und schrittweise neue Perspektiven zu schaffen. Auf wissenschaftlichen Erkenntnissen basierend schafft er Klarheit über das eigene unbewusste Bindungsverhalten und bietet therapeutische Werkzeuge wie Übungen zur Korrektur von falschen frühkindlichen Prägungen. »Ich las Mutterhunger wie eine heilige Schrift – jedes Wort enthüllte und beleuchtete mein tiefstes Inneres, von dem ich wusste, dass es da war, für das ich aber keinen Namen hatte.« - Nancy Levin, Autorin von Setting Boundaries Will Set You Free

Published

2024

4. Knockout of microRNA-21 attenuates alcoholic hepatitis through the VHL/NF-κB signaling pathway in hepatic stellate cells

Author

Li Huang, Chaodong Wu, Fanyin Meng, Heather Francis, Tami Annable, Kelly McDaniel, Gianfranco Alpini, Sugeily Ramos-Lorenzo, Demeng Chen, Nan Wu, Tianhao Zhou, and Shannon Glaser

Subjects

Liver Cirrhosis, 0301 basic medicine, Alcoholic liver disease, Physiology, medicine.medical_treatment, Down-Regulation, Alcoholic hepatitis, Inflammation, Mice, 03 medical and health sciences, Physiology (medical), microRNA, Hepatic Stellate Cells, medicine, Animals, Humans, Gene silencing, Cells, Cultured, Mice, Knockout, Liver injury, Hepatology, Hepatitis, Alcoholic, business.industry, Gastroenterology, medicine.disease, MicroRNAs, 030104 developmental biology, Cytokine, Gene Expression Regulation, Liver, Hepatic stellate cell, Cancer research, Cytokines, medicine.symptom, business, Research Article, Signal Transduction

Abstract

microRNA-21 (miRNA) is one of the most abundant miRNAs in chronic liver injuries including alcoholic liver injury. Previous studies have demonstrated that miR-21 plays a role in inflammation in the liver and functions in hepatic stellate cells (HSCs), which reside in the perisinusoidal space between sinusoidal endothelial cells and hepatocytes and regulate sinusoidal circulation. HSCs integrate cytokine-mediated inflammatory responses in the sinusoids and relay them to the liver parenchyma. Here, we showed that the activation of Von Hippel-Lindau (VHL) expression, by miR-21 knockout in vivo and anti-miR-21 or VHL overexpression in vitro, suppressed the production of proinflammatory cytokines, such as interleukin (IL)-6, monocyte chemoattractant protein-1, and IL-1β, in human HSCs during alcoholic liver injury. Sequence and functional analyses confirmed that miR-21 directly targeted the 3′-untranslated region of VHL. Immunofluorescence and real-time PCR analysis revealed that miR-21 depletion blocked NF-κB activation in human HSCs both in cultured HSCs as well as HSCs isolated from alcohol-related liver disease mice liver by laser capture microdissection. We also showed that conditioned medium from anti-miR-21-transfected HSCs suppressed human monocyte-derived THP-1 cell migration. Taken together, our study indicates that depletion of miR-21 may downregulate cytokine production in HSCs and macrophage chemotaxis during alcoholic liver injury and that the targeting of miR-21 may have therapeutic potential for preventing the progression of alcoholic liver diseases. NEW & NOTEWORTHY This study demonstrates that silencing microRNA-21 can inhibit cytokine production and inflammatory responses in human hepatic stellate cells during alcoholic liver injury and that the targeting of microR-21 in hepatic stellate cells may have therapeutic potential for prevention and treatment of alcoholic liver diseases.

Published

2018

5. Mother Hunger : How Adult Daughters Can Understand and Heal From Lost Nurturance, Protection, and Guidance

Author

Kelly McDaniel and Kelly McDaniel

Subjects

Self-actualization (Psychology) in women, Attachment behavior, Mothers and daughters

Abstract

An insatiable need for sex and love. Periods of overeating or starving. A pattern of unstable and painful relationships.Does this sound painfully familiar?Trauma counselor Kelly McDaniel has seen these traits over and over in clients who feel trapped in cycles of harmful behaviors-and are unable to stop.Many of us find ourselves stuck in unhealthy habits simply because we don't see a better way. With Mother Hunger, McDaniel helps women break the cycle of destructive behavior by taking a fresh look at childhood trauma and its lasting impact. In doing so, she destigmatizes the shame that comes with being under-mothered and misdiagnosed. McDaniel offers a healing path with powerful tools that include therapeutic interventions and lifestyle changes in service to healthy relationships.The constant search for mother love can be a lifelong emotional burden, but healing begins with knowing and naming what we are missing. McDaniel is the first clinician to identify Mother Hunger, which demystifies the search for love and provides the compass that each woman needs to end the struggle with achy, lonely emptiness, and come home to herself.

Published

2021

6. Knockdown of Hepatic Gonadotropin-Releasing Hormone by Vivo-Morpholino Decreases Liver Fibrosis in Multidrug Resistance Gene 2 Knockout Mice by Down-Regulation of miR-200b

Author

Shannon Glaser, Paolo Onori, Antonio Franchitto, Julie Venter, Fanyin Meng, Kelly McDaniel, Lindsey Kennedy, Gianfranco Alpini, Romina Mancinelli, Konstantina Kyritsi, Francesca Bernuzzi, Tianhao Zhou, Nan Wu, Heather Francis, Domenico Alvaro, Eugenio Gaudio, Pietro Invernizzi, Kyritsi, K, Meng, F, Zhou, T, Wu, N, Venter, J, Francis, H, Kennedy, L, Onori, P, Franchitto, A, Bernuzzi, F, Invernizzi, P, Mcdaniel, K, Mancinelli, R, Alvaro, D, Gaudio, E, Alpini, G, and Glaser, S

Subjects

Liver Cirrhosis, Male, 0301 basic medicine, Gonadotropin-releasing hormone, Morpholino, liver, cholangiocytes, hepatic gonadotropin-releasing hormone, Morpholinos, Gonadotropin-Releasing Hormone, Mice, Fibrosis, Mice, Knockout, Gene knockdown, Cholestasis, GNRHR, MicroRNA, Regular Article, Up-Regulation, Liver, Cholestasi, Knockout mouse, Disease Progression, Human, medicine.medical_specialty, ATP Binding Cassette Transporter, Subfamily B, Liver Cirrhosi, Down-Regulation, Biology, Cholangiocyte, Cell Line, Pathology and Forensic Medicine, 03 medical and health sciences, Internal medicine, Hepatic Stellate Cells, medicine, Animals, Humans, Cell Proliferation, Animal, P-Glycoprotein, medicine.disease, Hepatic Stellate Cell, Disease Models, Animal, MicroRNAs, 030104 developmental biology, Endocrinology, Gene Expression Regulation, Hepatic stellate cell, Hepatic fibrosis, Receptors, LHRH

Abstract

Hepatic fibrosis occurs during the progression of primary sclerosing cholangitis (PSC) and is characterized by accumulation of extracellular matrix proteins. Proliferating cholangiocytes and activated hepatic stellate cells (HSCs) participate in the promotion of liver fibrosis during cholestasis. Gonadotropin-releasing hormone (GnRH) is a trophic peptide hormone synthesized by hypothalamic neurons and the biliary epithelium and exerts its biological effects on cholangiocytes by interaction with the receptor subtype (GnRHR 1 ) expressed by cholangiocytes and HSCs. Previously, we demonstrated that administration of GnRH to normal rats increased intrahepatic biliary mass (IBDM) and hepatic fibrosis. Also, miR-200b is associated with the progression of hepatic fibrosis; however, the role of the GnRH/GnRHR 1 /miR-200b axis in the development of hepatic fibrosis in PSC is unknown. Herein, using the mouse model of PSC (multidrug resistance gene 2 knockout), the hepatic knockdown of GnRH decreased IBDM and liver fibrosis. In vivo and in vitro administration of GnRH increased the expression of miR-200b and fibrosis markers. The GnRH/GnRHR 1 axis and miR-200b were up-regulated in human PSC samples. Cetrorelix, a GnRHR 1 antagonist, inhibited the expression of fibrotic genes in vitro and decreased IBDM and hepatic fibrosis in vivo . Inhibition of miR-200b decreased the expression of fibrosis genes in vitro in cholangiocyte and HSC lines. Targeting the GnRH/GnRHR 1 /miR-200b axis may be key for the management of hepatic fibrosis during the progression of PSC.

Published

2017

7. Arene Dearomatization via Radical Hydroarylation

Author

Nathan Jui, David Vogt, Meredith Hughes, Kelly McDaniel, and Autumn Flynn

Abstract

A photocatalytic system for the dearomative hydroarylation of benzene derivatives has been developed. Using a combination of an organic photoredox catalyst and an amine reductant, this process operates through a reductive radical-polar crossover mechanism where aryl halide reduction triggers a regioselective cyclization event, giving rise to a range of complex spirocyclic cyclohexadienes. This light-driven protocol functions at room temperature in a green solvent system (aq. MeCN), without the need for precious metal-based catalysts or reagents, or the generation of stoichiometric metal byproducts.

Published

2019

8. Sa1502 PROMOTION OF M1 MACROPHAGE POLARIZATION AND DUCTULAR REACTION BY MICRORNA-34A DURING CHOLESTATIC LIVER INJURY

Author

Lixian Chen, Li Huang, Konstantina Kyritsi, Shannon Glaser, Kelly McDaniel, Nan Wu, Heather Francis, Fanyin Meng, Tianhao Zhou, Keisaku Sato, Chaodong Wu, Ludovica Ceci, Gianfranco Alpini, Zhihong Yang, and Suthat Liangpunsakul

Subjects

Liver injury, Promotion (rank), Hepatology, business.industry, MicroRNA 34a, media_common.quotation_subject, Gastroenterology, medicine, Macrophage polarization, Cancer research, medicine.disease, business, media_common

Published

2020

9. Expression of STING Is Increased in Liver Tissues from Patients With NAFLD and Promotes Macrophage-mediated Hepatic Inflammation and Fibrosis in Mice

Author

Yuqing Huo, Linda R. Knight, Shih Lung Woo, Ya Pei, Xiaoxian Qian, Michael A. Deveau, Jing Zhou, Xiaoqiu Xiao, Chaodong Wu, Yanming Chen, Xiangbai Chen, Heather Francis, Shannon Glaser, Qifu Li, Kelly McDaniel, Fanyin Meng, Xianjun Luo, Linqiang Ma, Xin Guo, Gianfranco Alpini, and Honggui Li

Subjects

Liver Cirrhosis, 0301 basic medicine, medicine.medical_specialty, Inflammation, Article, Hepatitis, 03 medical and health sciences, Mice, Fibrosis, Non-alcoholic Fatty Liver Disease, Internal medicine, Nonalcoholic fatty liver disease, medicine, Animals, Humans, Hepatology, business.industry, Macrophages, Fatty liver, Gastroenterology, Membrane Proteins, nutritional and metabolic diseases, medicine.disease, Immunity, Innate, eye diseases, Mice, Inbred C57BL, Sting, 030104 developmental biology, Endocrinology, Liver, Interferon Type I, Hepatic stellate cell, Tumor necrosis factor alpha, medicine.symptom, Steatosis, business

Abstract

Background & Aims Transmembrane protein 173 (TMEM173 or STING) signaling by macrophage activates the type I interferon-mediated innate immune response. The innate immune response contributes to hepatic steatosis and non-alcoholic fatty liver disease (NAFLD). We investigated whether STING regulates diet-induced in hepatic steatosis, inflammation, and liver fibrosis in mice. Methods Mice with disruption of Tmem173 (STINGgt) on a C57BL/6J background, mice without disruption of this gene (controls), and mice with disruption of Tmem173 only in myeloid cells were fed a standard chow diet, a high-fat diet (HFD; 60% fat calories), or a methionine- and choline-deficient diet (MCD). Liver tissues were collected and analyzed by histology and immunohistochemistry. Bone marrow cells were isolated from mice, differentiated into macrophages, and incubated with 5,6-dimethylxanthenone-4-acetic acid (DMXAA; an activator of STING) or cyclic guanosine monophosphate–adenosine monophosphate (cGAMP). Macrophages or their media were applied to mouse hepatocytes or human hepatic stellate cells (LX2) cells, which were analyzed for cytokine expression, protein phosphorylation, and fat deposition (by oil red O staining after incubation with palmitate). We obtained liver tissues from patients with and without NAFLD and analyzed these by immunohistochemistry. Results Non-parenchymal cells of liver tissues from patients with NAFLD had higher levels of STING than cells of liver tissues from patients without NAFLD. STINGgt mice and mice with disruption only in myeloid cells developed less severe hepatic steatosis, inflammation, and/or fibrosis after the HFD or MCD than control mice. Levels of phosphorylated c-Jun N-terminal kinase and p65 and mRNAs encoding tumor necrosis factor and interleukins 1B and 6 (markers of inflammation) were significantly lower in liver tissues from STINGgt mice vs control mice after the HFD or MCD. Transplantation of bone marrow cells from control mice to STINGgt mice restored the severity of steatosis and inflammation after the HFD. Macrophages from control, but not STINGgt, mice increased markers of inflammation in response to lipopolysaccharide and cGAMP. Hepatocytes and stellate cells cocultured with STINGgt macrophages in the presence of DMXAA or incubated with the medium collected from these macrophages had decreased fat deposition and markers of inflammation compared with hepatocytes or stellate cells incubated with control macrophages. Conclusions Levels of STING were increased in liver tissues from patients with NAFLD and mice with HFD-induced steatosis. In mice, loss of STING from macrophages decreased the severity of liver fibrosis and the inflammatory response. STING might be a therapeutic target for NAFLD.

Published

2018

10. Regulation of adipose tissue inflammation by adenosine 2A receptor in obese mice

Author

Ya Pei, Yuli Cai, Jing Zhou, Xiaoxian Qian, Tianshu Zeng, Honggui Li, Yanming Chen, Shannon Glaser, Xianjun Luo, Lulu Chen, Linqiang Ma, Chaodong Wu, Yuqing Huo, Fanyin Meng, Gianfranco Alpini, and Kelly McDaniel

Subjects

0301 basic medicine, Male, medicine.medical_specialty, Receptor, Adenosine A2A, Endocrinology, Diabetes and Metabolism, Adipose tissue macrophages, Palmitates, Adipose tissue, Inflammation, Diet, High-Fat, Weight Gain, Article, Proinflammatory cytokine, 03 medical and health sciences, 0302 clinical medicine, Endocrinology, Internal medicine, medicine, Macrophage, Animals, Obesity, Receptor, Adiposity, Chemistry, Macrophages, Interleukin, Mice, Inbred C57BL, 030104 developmental biology, Adipose Tissue, 030220 oncology & carcinogenesis, Hyperglycemia, Tumor necrosis factor alpha, Female, medicine.symptom, Insulin Resistance

Abstract

Adenosine 2A receptor (A2AR) exerts anti-inflammatory effects. However, the role of A2AR in obesity-associated adipose tissue inflammation remains to be elucidated. The present study examined the expression of A2AR in adipose tissue of mice with diet-induced obesity and determined the effect of A2AR disruption on the status of obesity-associated adipose tissue inflammation. WT C57BL/6J mice and A2AR-disrupted mice were fed a high-fat diet (HFD) for 12 weeks to induce obesity and adipose tissue inflammation. In vitro, bone marrow-derived macrophages from A2AR-disrupted mice and WT control mice were treated with palmitate and examined for macrophage proinflammatory activation. Compared with that of low-fat diet (LFD)-fed WT mice, A2AR expression in adipose tissue of HFD-fed WT mice was increased significantly and was present predominantly in adipose tissue macrophages. The increase in adipose tissue A2AR expression in HFD-fed mice was accompanied with increased phosphorylation states of c-Jun N-terminal kinase 1 p46 and nuclear factor kappa B p65 and mRNA levels of interleukin (Il)-1beta, Il6 and tumor necrosis factor alpha. In A2AR-disrupted mice, HFD feeding induced significant increases in adipose tissue inflammation, indicated by enhanced proinflammatory signaling and increased proinflammatory cytokine expression, and adipose tissue insulin resistance, indicated by a decrease in insulin-stimulated Akt phosphorylation relative to those in WT mice. Lastly, A2AR disruption enhanced palmitate-induced macrophage proinflammatory activation. Taken together, these results suggest that A2AR plays a protective role in obesity-associated adipose tissue inflammation, which is attributable to, in large part, A2AR suppression of macrophage proinflammatory activation.

Published

2018

11. Role of stem cells during diabetic liver injury

Author

Heather Francis, Tami Annable, Shannon Glaser, Ying Wan, Tianhao Zhou, Levine Phillip, Qiaobing Huang, Kelly McDaniel, Gianfranco Alpini, Yuyan Han, Nan Wu, Jessica Garner, and Fanyin Meng

Subjects

0301 basic medicine, non‐alcoholic fatty liver disease, liver diseases, medicine.medical_treatment, Type 2 diabetes, Review, Diabetes Complications, 03 medical and health sciences, 0302 clinical medicine, Insulin resistance, Diabetes mellitus, insulin resistance, medicine, Animals, Humans, Liver injury, diabetes, business.industry, Insulin, Stem Cells, Fatty liver, Cell Biology, medicine.disease, 3. Good health, 030104 developmental biology, medicine.anatomical_structure, Diabetes Mellitus, Type 2, Liver, 030220 oncology & carcinogenesis, Hepatocyte, Immunology, Hepatocytes, Molecular Medicine, Stem cell, business

Abstract

Diabetes mellitus is one of the most severe endocrine metabolic disorders in the world that has serious medical consequences with substantial impacts on the quality of life. Type 2 diabetes is one of the main causes of diabetic liver diseases with the most common being non‐alcoholic fatty liver disease. Several factors that may explain the mechanisms related to pathological and functional changes of diabetic liver injury include: insulin resistance, oxidative stress and endoplasmic reticulum stress. The realization that these factors are important in hepatocyte damage and lack of donor livers has led to studies concentrating on the role of stem cells (SCs) in the prevention and treatment of liver injury. Possible avenues that the application of SCs may improve liver injury include but are not limited to: the ability to differentiate into pancreatic β‐cells (insulin producing cells), the contribution for hepatocyte regeneration, regulation of lipogenesis, glucogenesis and anti‐inflammatory actions. Once further studies are performed to explore the underlying protective mechanisms of SCs and the advantages and disadvantages of its application, there will be a greater understand of the mechanism and therapeutic potential. In this review, we summarize the findings regarding the role of SCs in diabetic liver diseases.

Published

2015

12. Functional Role of Cellular Senescence in Biliary Injury

Author

Yuyan Han, Shannon Glaser, Kelly McDaniel, Phillip Levine, Morgan Quezada, Gianfranco Alpini, Fanyin Meng, Tianhao Zhou, Luke Meng, Emily Lin, and Heather Francis

Subjects

Senescence, Liver Cirrhosis, Biliary, Cell Cycle, Cholangitis, Sclerosing, Autophagy, Review, Biology, medicine.disease, Pathology and Forensic Medicine, Primary sclerosing cholangitis, Biliary injury, Primary biliary cirrhosis, Biliary Atresia, Biliary atresia, Immunology, medicine, Cancer research, Humans, Stem cell, Cell aging, Cellular Senescence

Abstract

Cellular senescence is a state of irreversible cell cycle arrest that has been involved in many gastrointestinal diseases, including human cholestatic liver disorders. Senescence may play a role in biliary atresia, primary sclerosing cholangitis, cellular rejection, and primary biliary cirrhosis, four liver diseases affecting cholangiocytes and the biliary system. In this review, we examine proposed mechanisms of senescence-related biliary diseases, including hypotheses associated with the senescence-associated phenotype, induction of senescence in nearby cells, and the depletion of stem cell subpopulations. Current evidence for the molecular mechanisms of senescence in the previously mentioned diseases is discussed in detail, with attention to recent advances on the role of pathways associated with senescence-associated phenotype, stress-induced senescence, telomere dysfunction, and autophagy.

Published

2015

13. Forkhead box A2 regulates biliary heterogeneity and senescence during cholestatic liver injury in mice‡

Author

Julie Venter, Heather Francis, Keisaku Sato, Ying Wan, Paolo Onori, Gianfranco Alpini, Qiaobing Huang, Tianhao Zhou, Nan Wu, Konstantina Kyritsi, Pietro Invernizzi, Fanyin Meng, Francesca Bernuzzi, Kelly McDaniel, Shannon Glaser, Eugenio Gaudio, Mcdaniel, K, Meng, F, Wu, N, Sato, K, Venter, J, Bernuzzi, F, Invernizzi, P, Zhou, T, Kyritsi, K, Wan, Y, Huang, Q, Onori, P, Francis, H, Gaudio, E, Glaser, S, and Alpini, G

Subjects

0301 basic medicine, Pathology, Aging, biliary heterogeneity, Cellular differentiation, Cell Communication, Mice, 0302 clinical medicine, Fibrosis, cellular senescence, Liver injury, Aged, 80 and over, Mice, Knockout, DNA methylation, Cholestasis, Middle Aged, Liver, Knockout mouse, primary sclerosing cholangiti, Hepatocyte Nuclear Factor 3-beta, 030211 gastroenterology & hepatology, Senescence, Adult, medicine.medical_specialty, Adolescent, Down-Regulation, hepatology, cholestatic liver injury, foxA2, Biology, Real-Time Polymerase Chain Reaction, digestive system, Article, Sampling Studies, Primary sclerosing cholangitis, 03 medical and health sciences, Genetic Heterogeneity, FoxA2, medicine, Hepatic Stellate Cells, Animals, Humans, Progenitor cell, Aged, Hepatology, medicine.disease, digestive system diseases, Disease Models, Animal, 030104 developmental biology, Gene Expression Regulation, Hepatic stellate cell, Hepatocytes, Bile Ducts

Abstract

Biliary-committed progenitor cells (small mouse cholangiocytes; SMCCs) from small bile ducts are more resistant to hepatobiliary injury than large mouse cholangiocytes (LGCCs) from large bile ducts. The definitive endoderm marker, forkhead box A2 (FoxA2), is the key transcriptional factor that regulates cell differentiation and tissue regeneration. Our aim was to characterize the translational role of FoxA2 during cholestatic liver injury. Messenger RNA expression in SMCCs and LGCCs was assessed by polymerase chain reaction (PCR) array analysis. Liver tissues and hepatic stellate cells (HSCs) from primary sclerosing cholangitis (PSC) and primary biliary cholangitis (PBC) patients were tested by real-time PCR for methylation, senescence, and fibrosis markers. Bile duct ligation (BDL) and multidrug resistance protein 2 (MDR2) knockout mice (MDR2-/-) were used as animal models of cholestatic liver injury with or without healthy transplanted large or small cholangiocytes. We demonstrated that FoxA2 was notably enhanced in murine liver progenitor cells and SMCCs and was silenced in human PSC and PBC liver tissues relative to respective controls that are correlated with the epigenetic methylation enzymes, DNA methyltransferase (DNMT) 1 and DNMT3B. Serum alanine aminotransferase and aspartate aminotransferase levels in nonobese diabetic/severe combined immunodeficiency mice engrafted with SMCCs post-BDL showed significant changes compared to vehicle-treated mice, along with improved liver fibrosis. Enhanced expression of FoxA2 was observed in BDL mouse liver after SMCC cell therapy. Furthermore, activation of fibrosis signaling pathways were observed in BDL/MDR2-/- mouse liver as well as in isolated HSCs by laser capture microdissection, and these signals were recovered along with reduced hepatic senescence and enhanced hepatic stellate cellular senescence after SMCC engraft. Conclusion: The definitive endoderm marker and the positive regulator of biliary development, FoxA2, mediates the therapeutic effect of biliary-committed progenitor cells during cholestatic liver injury.

Published

2017

14. Regulation of the Extrinsic Apoptotic Pathway by MicroRNA-21 in Alcoholic Liver Injury

Author

Phillip Levine, Fanyin Meng, Shannon Glaser, Li Huang, Tianhao Zhou, Heather Francis, Gianfranco Alpini, Yuyan Han, Fuquan Yang, Jennifer McCarra, Lindsey Kennedy, Xiuping Liu, Jia Ming Lai, Julie Venter, Kelly McDaniel, and Chang-Gong Liu

Subjects

STAT3 Transcription Factor, endocrine system, congenital, hereditary, and neonatal diseases and abnormalities, Alcoholic liver disease, endocrine system diseases, Apoptosis, Biochemistry, Fas ligand, Mice, microRNA, Hepatic Stellate Cells, medicine, Animals, Humans, STAT3, Liver Diseases, Alcoholic, Molecular Biology, Regulator gene, Liver injury, biology, Interleukin-6, nutritional and metabolic diseases, Cell Biology, medicine.disease, Molecular biology, Up-Regulation, Mice, Inbred C57BL, MicroRNAs, Real-time polymerase chain reaction, Liver, Cancer research, Hepatic stellate cell, biology.protein, Signal Transduction

Abstract

IL-6/Stat3 is associated with the regulation of transcription of key cellular regulatory genes (microRNAs) during different types of liver injury. This study evaluated the role of IL-6/Stat3 in regulating miRNA and miR-21 in alcoholic liver disease. By microarray, we identified that ethanol feeding significantly up-regulated 0.8% of known microRNAs in mouse liver compared with controls, including miR-21. Similarly, the treatment of normal human hepatocytes (N-Heps) and hepatic stellate cells (HSCs) with ethanol and IL-6 significantly increased miR-21 expression. Overexpression of miR-21 decreased ethanol-induced apoptosis in both N-Heps and HSCs. The expression level of miR-21 was significantly increased after Stat3 activation in N-Heps and HSCs, in support of the concept that the 5'-promoter region of miR-21 is regulated by Stat3. Using real time PCR, we confirmed that miR-21 activation is associated with ethanol-linked Stat3 binding of the miR-21 promoter. A combination of bioinformatics, PCR array, dual-luciferase reporter assay, and Western blot analysis revealed that Fas ligand (TNF superfamily, member 6) (FASLG) and death receptor 5 (DR5) are the direct targets of miR-21. Furthermore, inhibition of miR-21 by specific Vivo-Morpholino and knock-out of IL-6 in ethanol-treated mice also increased the expression of DR5 and FASLG in vivo during alcoholic liver injury. The identification of miR-21 as an important regulator of hepatic cell survival, transformation, and remodeling in vitro, as well as its upstream modulators and downstream targets, will provide insight into the involvement of altered miRNA expression in contributing to alcoholic liver disease progression and testing novel therapeutic approaches for human alcoholic liver diseases.

Published

2014

15. Molecular mechanisms of stem cell therapy in alcoholic liver disease

Author

Fanyin Meng, Phillip Levine, Gianfranco Alpini, Heather Francis, Lindsey Kennedy, and Kelly McDaniel

Subjects

Liver injury, Alcoholic liver disease, Hepatology, business.industry, medicine.medical_treatment, Mesenchymal stem cell, Hematopoietic Stem Cell Transplantation, Gastroenterology, Liver Stem Cell, Stem-cell therapy, Exosomes, Mesenchymal Stem Cell Transplantation, medicine.disease, Bioinformatics, Liver regeneration, Liver Regeneration, Cell therapy, Microvessels, Immunology, Hepatocytes, medicine, Humans, Stem cell, business, Liver Diseases, Alcoholic

Abstract

Alcoholic liver disease affects a great number of people worldwide. With limited therapeutic options, stem cell therapy offers significant potential for these patients. To date, a limited number of clinical trials have produced transient clinical responses to cell therapy in patients with alcoholic liver disease. Stem cell therapy to reorganize the postnatal liver is an important theme and mission for patients with chronic liver disorders including alcoholic liver injury. We therefore should redevelop the evidence of cell-based liver regeneration therapy, focusing on targets (disease, patient's status and hepatic function), materials (cells, cytokines and genes), and methodology (stem cell types and their derived microparticles, transplantation route, implantation technology and tissue engineering). In this review, we summarize the recent findings regarding the experimental and clinical use of mesenchymal and liver stem cells, focusing mainly on the treatment of alcoholic liver disorders and their relevance in the field of regenerative medicine, and advances on the role of microvesicles and exosomes in this process. We discuss new advances in stem cell therapy from liver regeneration to liver re-organization, which is involved in the recent progress of on-going clinical trials, basic research in stem cell therapy and liver regeneration, and updated exosomes/microvesicles recovery/repairing technology.

Published

2014

16. Overexpression of membrane metalloendopeptidase inhibits substance P stimulation of cholangiocarcinoma growth

Author

Kelly McDaniel, Syeda H. Afroze, Lindsey Kennedy, Shannon Glaser, Sharon DeMorrow, Micheleine Guerrier, Yuyan Han, Gianfranco Alpini, Laura Hargrove, Shanika Avila, Heather Francis, Debolina Ray, Holly Standeford, Julie Venter, Gabriel Frampton, Fanyin Meng, Matthew McMillin, and Morgan Quezada

Subjects

Male, Vascular Endothelial Growth Factor A, medicine.medical_specialty, Time Factors, Physiology, Mice, Nude, Substance P, Biology, Transfection, Gene Expression Regulation, Enzymologic, Cholangiocyte, Cholangiocarcinoma, Mice, Neurokinin-1 Receptor Antagonists, In vivo, Cell Line, Tumor, Proliferating Cell Nuclear Antigen, Physiology (medical), Internal medicine, parasitic diseases, medicine, Animals, Humans, Secretion, Autocrine signalling, Neprilysin, Cell Proliferation, Keratin-19, Mice, Inbred BALB C, Dose-Response Relationship, Drug, Hepatology, Cell growth, Gastroenterology, Receptors, Neurokinin-1, Xenograft Model Antitumor Assays, Molecular biology, Tumor Burden, Up-Regulation, Gene Expression Regulation, Neoplastic, Liver and Biliary Tract, Vascular endothelial growth factor A, Bile Ducts, Intrahepatic, Endocrinology, Bile Duct Neoplasms, Cell culture

Abstract

Substance P (SP) promotes cholangiocyte growth during cholestasis by activating its receptor, NK1R. SP is a proteolytic product of tachykinin (Tac1) and is deactivated by membrane metalloendopeptidase (MME). This study aimed to evaluate the functional role of SP in the regulation of cholangiocarcinoma (CCA) growth. NK1R, Tac1, and MME expression and SP secretion were assessed in human CCA cells and nonmalignant cholangiocytes. The proliferative effects of SP (in the absence/presence of the NK1R inhibitor, L-733,060) and of L-733,060 were evaluated. In vivo, the effect of L-733,060 treatment or MME overexpression on tumor growth was evaluated by using a xenograft model of CCA in nu/nu nude mice. The expression of Tac1, MME, NK1R, PCNA, CK-19, and VEGF-A was analyzed in the resulting tumors. Human CCA cell lines had increased expression of Tac1 and NK1R, along with reduced levels of MME compared with nonmalignant cholangiocytes, resulting in a subsequent increase in SP secretion. SP treatment increased CCA cell proliferation in vitro, which was blocked by L-733,060. Treatment with L-733,060 alone inhibited CCA proliferation in vitro and in vivo. Xenograft tumors derived from MME-overexpressed human Mz-ChA-1 CCA cells had a slower growth rate than those derived from control cells. Expression of PCNA, CK-19, and VEGF-A decreased, whereas MME expression increased in the xenograft tumors treated with L-733,060 or MME-overexpressed xenograft tumors compared with controls. The study suggests that SP secreted by CCA promotes CCA growth via autocrine pathway. Blockade of SP secretion and NK1R signaling may be important for the management of CCA.

Published

2014

17. The functional role of micro <scp>RNA</scp> s in alcoholic liver injury

Author

Heather Francis, Shannon Glaser, Leonardo Herrera, Kelly McDaniel, Yuyan Han, Emily Lin, Gianfranco Alpini, Tianhao Zhou, Phillip Levine, and Fanyin Meng

Subjects

Lipopolysaccharides, Alcoholic liver disease, LPS, Necrosis, Kupffer Cells, Reviews, Inflammation, Biology, Permeability, Hepatic Stellate Cells, medicine, alcoholic liver diseases, Humans, TLR4, Intestinal Mucosa, Liver Diseases, Alcoholic, Liver injury, Ethanol, Tumor Necrosis Factor-alpha, apoptosis, Cell Biology, medicine.disease, microRNAs, Intestines, Toll-Like Receptor 4, Gene Expression Regulation, Liver, TNF-α, Immunology, Hepatocytes, Hepatic stellate cell, Molecular Medicine, Tumor necrosis factor alpha, medicine.symptom, Steatohepatitis, Signal Transduction

Abstract

The function of microRNAs (miRNAs) during alcoholic liver disease (ALD) has recently become of great interest in biological research. Studies have shown that ALD associated miRNAs play a crucial role in the regulation of liver-inflammatory agents such as tumour necrosis factor-alpha (TNF-α), one of the key inflammatory agents responsible for liver fibrosis (liver scarring) and the critical contributor of alcoholic liver disease. Lipopolysaccharide (LPS), a component of the cell wall of gram-negative bacteria, is responsible for TNF-α release by Kupffer cells. miRNAs are the critical mediators of LPS signalling in Kupffer cells, hepatocytes and hepatic stellate cells. Certain miRNAs, in particular miR-155 and miR-21, show a positive correlation in up-regulation of LPS signalling when they are exposed to ethanol. ALD is related to enhanced gut permeability that allows the levels of LPS to increase, leads to increased secretion of TNF-α by the Kupffer cells and subsequently promotes alcoholic liver injury through specific miRNAs. Meanwhile, two of the most frequently dysregulated miRNAs in steatohepatitis, miR-122 and miR-34a are the critical mediators in ethanol/LPS activated survival signalling during ALD. In this review, we summarize recent findings regarding the experimental and clinical aspects of functions of specific microRNAs, focusing mainly on inflammation and cell survival after ethanol/LPS treatment, and advances on the role of circulating miRNAs in human alcoholic disorders.

Published

2014

18. Mo1436 – Regulation of Chemoresistance by Microrna-17-92 Cluster in Patient-Derived Cholangiocarcinoma Xenograft Tumors

Author

Shannon Glaser, Gianfranco Alpini, Nan Wu, Heather Francis, Tianhao Zhou, Scott Celinski, Li Huang, Fanyin Meng, Harshil Dhruv, and Kelly McDaniel

Subjects

Hepatology, microRNA, Gastroenterology, Cancer research, In patient, Biology, Disease cluster, Tumor xenograft

Published

2019

19. Su1023 – Regulation of Endothelial Progenitor Cell Function by Microrna in Cholestatic Liver Injury

Author

Nan Wu, Fanyin Meng, Heather Francis, Kelly McDaniel, Shannon Glaser, Tianhao Zhou, and Gianfranco Alpini

Subjects

Liver injury, Hepatology, business.industry, microRNA, Gastroenterology, medicine, Cancer research, medicine.disease, business, Endothelial progenitor cell, Function (biology)

Published

2019

20. Neuropeptide Y inhibits biliary hyperplasia of cholestatic rats by paracrine and autocrine mechanisms

Author

Gabriel Frampton, Fanyin Meng, Romina Mancinelli, Paolo Onori, Kelly McDaniel, Julie Venter, Dinorah Leyva-Illades, Gianfranco Alpini, Matthew A. Quinn, Shannon Glaser, Antonio Franchitto, Eugenio Gaudio, Hae Yong Pae, Heather Francis, and Sharon DeMorrow

Subjects

Male, medicine.medical_specialty, Physiology, proliferation, Paracrine Communication, Biology, Autocrine Communication, digestive system, neurotransmitters, Cell Line, Paracrine signalling, Proliferating Cell Nuclear Antigen, Physiology (medical), Internal medicine, mental disorders, medicine, Animals, Homeostasis, Neuropeptide Y, RNA, Messenger, Autocrine signalling, Receptor, Cell Proliferation, Cholestasis, Hyperplasia, Hepatology, biliary epithelium, Biliary hyperplasia, Gastroenterology, Neuropeptide Y receptor, Antibodies, Neutralizing, Rats, Inbred F344, humanities, Rats, Receptors, Neuropeptide Y, Liver and Biliary Tract, Bile Ducts, Intrahepatic, Endocrinology, cell cycle, Signal transduction, Signal Transduction

Abstract

Neuropeptide Y (NPY) exerts its functions through six subtypes of receptors (Y1–Y6). Biliary homeostasis is regulated by several factors through autocrine/paracrine signaling. NPY inhibits cholangiocarcinoma growth; however, no information exists regarding the autocrine/paracrine role of NPY on biliary hyperplasia during cholestasis. The aims of this study were to determine: 1) the expression of NPY and Y1–Y5 in cholangiocytes and 2) the paracrine/autocrine effects of NPY on cholangiocyte proliferation. Normal or bile duct ligation (BDL) rats were treated with NPY, neutralizing anti-NPY antibody, or vehicle for 7 days. NPY and NPY receptor (NPYR) expression was assessed in liver sections and isolated cholangiocytes. NPY secretion was assessed in serum and bile from normal and BDL rats, as well as supernatants from normal and BDL cholangiocytes and normal rat cholangiocyte cell line [intrahepatic normal cholangiocyte culture (NRICC)]. We evaluated intrahepatic bile ductal mass (IBDM) in liver sections and proliferation in cholangiocytes. With the use of NRICC, the effects of NPY or anti-NPY antibody on cholangiocyte proliferation were determined. The expression of NPY and all NPYR were increased after BDL. NPY levels were lower in serum and cholangiocyte supernatant from BDL compared with normal rats. NPY secretion from NRICC was detected at both the basolateral and apical domains. Chronic NPY treatment decreased proliferating cellular nuclear antigen (PCNA) expression and IBDM in BDL rats. Administration of anti-NPY antibody to BDL rats increased cholangiocyte proliferation and IBDM. NPY treatment of NRICC decreased PCNA expression and increased the cell cycle arrest, whereas treatment with anti-NPY antibody increased proliferation. Therapies targeting NPY-mediated signaling may prove beneficial for the treatment of cholangiopathies.

Published

2013

21. Utilities associated with subcutaneous injections and intravenous infusions for treatment of patients with bone metastases

Author

Janet E. Brown, Ze Cong, Ada Braun, Louis S. Matza, Alison Stopeck, Kate Van Brunt, Katia Tonkin, Karen Chung, and Kelly McDaniel

Subjects

medicine.medical_specialty, lcsh:R5-920, business.industry, Health Policy, Medicine (miscellaneous), Skeletal related events, Cancer, skeletal-related event, Intravenous Infusions, medicine.disease, Surgery, Subcutaneous injection, Patient Preference and Adherence, injection, Treatment modality, medicine, infusion, business, lcsh:Medicine (General), Pharmacology, Toxicology and Pharmaceutics (miscellaneous), Bisphosphonate treatment, Social Sciences (miscellaneous), Original Research

Abstract

Louis S Matza,1 Ze Cong,2 Karen Chung,2 Alison Stopeck,3 Katia Tonkin,4 Janet Brown,5 Ada Braun,2 Kate Van Brunt,6 Kelly McDaniel1 1Outcomes Research, United BioSource Corporation, Bethesda, MD, USA; 2Amgen, Inc, Thousand Oaks, CA, USA; 3Department of Medicine, University of Arizona, Tucson, AZ, USA; 4Department of Oncology, University of Alberta, Edmonton, Alberta, Canada; 5Leeds Institute of Molecular Medicine, St James University Hospital, Leeds, UK; 6formerly with Outcomes Research, United BioSource Corporation, Bethesda, MD, USA Introduction: Although cost-utility models are often used to estimate the value of treatments for metastatic cancer, limited information is available on the utility of common treatment modalities. Bisphosphonate treatment for bone metastases is frequently administered via intravenous infusion, while a newer treatment is administered as a subcutaneous injection. This study estimated the impact of these treatment modalities on health state preference. Methods: Participants from the UK general population completed time trade-off interviews to assess the utility of health state vignettes. Respondents first rated a health state representing cancer with bone metastases. Subsequent health states added descriptions of treatment modalities (ie, injection or infusion) to this basic health state. The two treatment modalities were presented with and without chemotherapy, and infusion characteristics were varied by duration (30 minutes or 2 hours) and renal monitoring. Results: A total of 121 participants completed the interviews (52.1% female, 76.9% white). Cancer with bone metastases had a mean utility of 0.40 on a standard utility scale (1 = full health; 0 = dead). The injection, 30-minute infusion, and 2-hour infusion had mean disutilities of −0.004, −0.02, and −0.04, respectively. The mean disutility of the 30-minute infusion was greater with renal monitoring than without. Chemotherapy was associated with substantial disutility (−0.17). When added to health states with chemotherapy, the mean disutilities of injection, 30-minute infusion, and 2-hour infusion were −0.02, −0.03, and −0.04, respectively. The disutility associated with injection was significantly lower than the disutility of the 30-minute and 2-hour infusions (P < 0.05), regardless of chemotherapy status. Conclusion: Respondents perceived an inconvenience with each type of treatment modality, but injections were preferred over infusions. The resulting utilities may be used in cost-utility models examining the value of treatments for the prevention of skeletal-related events in patients with bone metastases. Keywords: skeletal-related event, infusion, injection

Published

2013

22. Recent advances in the morphological and functional heterogeneity of the biliary epithelium

Author

Paolo Onori, Shannon Glaser, Antonio Franchitto, Guido Carpino, Marco Marzioni, Domenico Alvaro, Julie Venter, Heather Francis, Yuyan Han, Gianfranco Alpini, Fanyin Meng, Eugenio Gaudio, and Kelly McDaniel

Subjects

Biliary Tract Diseases, Apoptosis, camp, Biology, neurotransmitters, Epithelium, Article, General Biochemistry, Genetics and Molecular Biology, Gastrointestinal Hormones, bile ducts, gastrointestinal hormones, vegf, growth factors, In vivo, medicine, Animals, Humans, Biliary epithelium, Progenitor cell, Cell Proliferation, Cell growth, Stem Cells, Neuropeptides, Phenotype, Cell biology, medicine.anatomical_structure, Immunology, Bile Ducts, Stem cell, Hormone

Abstract

This review focuses on the recent advances related to the heterogeneity of different-sized bile ducts with regard to the morphological and phenotypical characteristics, and the differential secretory, apoptotic and proliferative responses of small and large cholangiocytes to gastrointestinal hormones/peptides, neuropeptides and toxins. We describe several in vivo and in vitro models used for evaluating biliary heterogeneity. Subsequently, we discuss the heterogeneous proliferative and apoptotic responses of small and large cholangiocytes to liver injury and the mechanisms regulating the differentiation of small into large (more differentiated) cholangiocytes. Following a discussion on the heterogeneity of stem/progenitor cells in the biliary epithelium, we outline the heterogeneity of bile ducts in human cholangiopathies. After a summary section, we discuss the future perspectives that will further advance the field of the functional heterogeneity of the biliary epithelium.

Published

2013

23. Lin28 and let-7: roles and regulation in liver diseases

Author

Chad Hall, Marco Marzioni, Terry C. Lairmore, Shannon Glaser, Gianfranco Alpini, Keisaku Sato, Kelly McDaniel, and Fanyin Meng

Subjects

0301 basic medicine, Cirrhosis, Physiology, Disease, Review, Biology, Primary sclerosing cholangitis, 03 medical and health sciences, Liver disease, Physiology (medical), medicine, Animals, Humans, Liver injury, Hepatitis, Hepatology, Liver Diseases, Cell Cycle, Gastroenterology, Cancer, RNA-Binding Proteins, medicine.disease, Liver regeneration, Liver Regeneration, MicroRNAs, 030104 developmental biology, Immunology, Cancer research, Signal Transduction

Abstract

The diagnosis and treatment of liver disease remain a major health concern worldwide because of the diverse etiologies of this disease. For this reason, new therapeutic targets are greatly needed to halt the progression of this damaging disease. Upon initiation of liver injury by viral infection, autoimmune disease or toxin, and/or hepatitis, chronic disease may develop, which can progress to cirrhosis, hepatocellular carcinoma (HCC), cholangiocarcinoma, liver failure, or death. The Lin28/lethal-7 (let-7) molecular switch has emerged as a central regulator of multiorgan injuries and cancer development. Lin28 is a stem cell marker vital to initiation or maintenance of a stem cell phenotype. Lin28 has not been extensively studied in the liver, despite its ability to induce tissue regeneration via reprogramming of oxidative enzymes in other tissues and its involvement with numerous upstream regulators and downstream targets in liver disease. Theoretically, overexpression of Lin28 in certain forms of liver disease could be a potential treatment that aids in liver regeneration. Alternatively, Lin28 has been implicated numerous times in the progression of diverse cancer types and is associated with increased severity of disease. In this case, Lin28 could be a potential inhibitory target to prevent malignant transformation in the liver. This review seeks to characterize the role of Lin28 in liver disease.

Published

2016

24. Stem Cell Derived Extracellular Vesicles Inhibits Liver Inflammation and Fibrosis in a Mouse Model of Primary Sclerosing Cholangitis

Author

Sugeily Ramos-Lorenzo, Konstantina Kyritsi, Keisaku Sato, Tianhao Zhou, Kelly McDaniel, Shannon Glaser, Julie Venter, Heather Francis, Nan Wu, Fanyin Meng, and Gianfranco Alpini

Subjects

Pathology, medicine.medical_specialty, Hepatology, business.industry, Gastroenterology, Inflammation, medicine.disease, Extracellular vesicles, Primary sclerosing cholangitis, Fibrosis, Medicine, medicine.symptom, Stem cell, business

Published

2017

25. The National Lung Screening Trial: Overview and Study Design

Author

Natalie Cunningham, Michael Khalili, John Waltz, Ralph Weiben, Deb Gurtner, Linda DeAlmeida, Sanjay Gupta, Sharon Maxfield, Crissy Kibic, Kathleen DeWitt, David DeMets, Walter Allen Bowman, Robert Epstein, Mia Burkhard, Stephen J. Swensen, Hattie Cromwell, Kianoush Rezai, Steadman Sankey, Lisa Scott Wasson, Rita Musanti, Tamim Malbari, Joy Ferola, Qimei He, Patty Trapnell, Melba Francis, Sam Quattlebaum, Joanice Thompson, Ana Birofka, Robin Griggs, Elizabeth Johnson, Margaret R. Spitz, Nicole Richardson, Yuting Liang, Lawrence G. Hutchins, Mirjana Tecmire, Lila Camara, James J. Navin, Eileen Frost, Diane Romano, Carrie Petkus, Eric J. Berns, Pei Jan P Lin, Steve D. Uttecht, Marian Acerra, Lawrence R. Ragard, Leo P. Lawler, Christopher M. Rogers, Alan Lee Goodwin, L. Ellen Martinusen, Melissa Ford, Michael T. Fisher, Beverly Powell, Cindy Lin, Jamie Downs, Brent Fodera, Bonita Wohlers, Michael Brangan, Peggy Bradley, Todd B. Burt, Susan Allen, Shiva Borgheian, Mingying Zeng, Thomas Riley, Danielle Gherardini, Steven Shiff, Olivia Campa, Wahied Gendi, Fang F. Xu, Ivana K. Kazda, Anne Chung, Briar Doi, Helen Price, Maria Vlachou, Alan Morgan, Simone Vuong, Pierre P. Massion, Darcy Watson, Debbie William, Esther Nakano, Karen Broski, David Creed, Melanie Bvorak, Lakisha Hawkins, Gladys Hino, Raymond Dauphinais, Michele Sallas, Helene Shiratori, Venus Brown, Denise Brooks, Heather Porter, Ilana F. Gareen, Tracy Lee, Melissa Cates, Kyle Turner, Tiffanie Hammond, Margaret Paquette, Lorraine Kerchum, Barbara Lewis, Douglas J. Reding, Thomas E. Hartman, Cathy Longden, Melissa Laron, Reza Abaya, Beborah Robertson, J W Semenkovich, Christine Holland, Hugh McGinley, Chani Montalbo, Karen Zubena, Vanessa Ralda, Adam C. Stein, Jennifer Ott, Lawrence M. Kotner, Jing Lee, Arnold Ssali, Michael Young, Quinn A. DeMordaunt, Linda V. White, Steve Dubinett, Pearl Chan, Roxana Phillips, Mallory Kolich, Brent B. Nelson, Phi Do, Jill Spivak, Angele LaFleur, Kesha Smith, Elayne Weslowsky, Patricia Nieters, Maurice LeBlanc, Satinder Singh, Lonna Matthews, Quentin McMullen, Karen Lappe, Sharon Longacre, Cindy Cobb, Jane A. Zehner, Michael Teepe, Pamela M. Marcus, Kathleen Bow, Wendy Francis, Mary Gemmel, Robert S. Fontana, Linda Jurjans, Barbara Ginther, Jonathan B. Clapp, Monica Richel, Scott F. Pickering, Brenda Edwards, Kendrick Looney, Randy Marshall, Roni Atkins, Danielle Wicks, Julie Peterson, Dcanna Cape, Albert J. Cook, Jerry Brekke, Louisa Turner, Larry Stoller, Mark B. Salerno, Bavid E. Midthun, Mark Delano, Minnetta Belyea, Deborah Greene, Jonathan Goldin, Terry Lewis, Virginia Fischer, Andrea Chapman, Shari Jordan, Deb Warren, Demetria Johnson, Rekha Khatri, Lisa Sirianni, Guillermo Geisse, Michael A. Fuchs, Kanya Kumbalasiri, Jeremy J. Erasmus, Vicki Shambaugh, Denise Boyles, Sarah Hallsky, Anna Nanovski, Jill Heinz, Mollie King, Kay Vydareny, Olga Soukhanova, Patricia Rueweler, Perry G. Pernicano, Regina Rendas-Baum, Phyllis Pirotte, Russell Harris, Neil Argyle, Miyoung Kim, June Krebsbach, Audrey Gallego, Sheila Wein, Mukesh F. Karwat, Karla Myra-Bloom, Pamela Byrnes, Mitchell D. Schnall, Hector Ahumada, Eric Sanchez, Donna DesMarais, Julie Maderitz, Cindy Lavergne, Lori Kirchoff, Patricia C. Sanders, Elizabeth Thielke, Michael Sullivan, Jennifer Gaegler, Janet Manual, Jennifer R. Heinz, Ray Zisumbo, Diane C. Strollo, Candace Mueller, Irene Mahon, Brenda Delfosse, Carolyn M. Johnson, William E. Grizzle, Merideth Stanley, Sylvan Green, Pamela Harvey, Lindsay Richardson, Brenda K. Brewer, Philip Costello, Deanna Zapolski, John Worrell, Jeffrey G. Schragin, David S. Alberts, Edward L. Korn, Tamara Owens, Hank Brastater, Kay Mathiesen-Viergutz, Mark Broschinsky, Paul W. Spirn, Grace Isaacs, John S. Waltz, Mitch Goodsitt, Christi Newton-Foster, Sharlene Snowden, Barbara Voight, Gail Bizer, Kathy McDonough, William Huynh, Eduard Van Stam, Robert A. Carlson, Mike Florzyk, Paula M. Jacobs, Joan Fuller, Mauren Grunenwald, Ann Bangerter, Jacksonville, Adriane Andersen, Tess Thompson, Kenneth Nowers, Stephanie Helwi, Martin J. Edelman, Emmanuel Omoba, Rubenia Flores, Kevin T. White, Patrick W. Wolfe, Michael Milacek, Sharon Gard, Brandon B. Bigby, Cynthia H. McCollough, Andrew Burnside, Sheryl L. Ogden, Maisha Pollard, Thomas K. Pilgram, Sydney Laster, Claudia J. Kasales, Bruce W. Turnbull, Cheri Haselhuhn, Laura N. Myers, Jean Jacobsen, Melissa Love, Gavin D. Watt, Cheryl Love, Gerald F. Abbott, Susanne Kozakowski, Jerry L. Montague, Cynthia Hill, Neil F. O'Donnell, Anna Sear, Thomas M. Beck, Jean Wegner, Chrispina Wray, Edward M. Brown, Louise Ledbetter, Karen Bellware, Julie Moody, Noel Bahr, Matthew T. Freedman, Thomas Hensley, John E. Madewell, Leanne Hadfield, David R. Maffitt, Lisa Cottrell, John J. Warner, Deborah Graham, Krystal Arnold, Alejandra Reyes, Kristin Lieberman, Derek Omori, Donna Garland, Mike Burek, Mel Johnson, Judith Harkins, Martha Fronheiser, M. Y. M. Chen, Dawn Simmons, Kathleen Voight, Aaron O. Bungum, Marianne Rice, Lakeshia Murray, Tami Krpata, Donna Sammons, Leslie Kmetty, Catherine Duda, Carissa Krzeczkowski, Anne Nguyen, Richard H. Lane, Cynthia Mack, Loren C. Macey, Eddy Wicklander, Kelly McDaniel, Sue Zahradka, Hassan Bourija, Cristina Farkas, Jincy George, Renae Kiffmeyer, Wendell Christie, Catherine Engartner, John Crump, Mimi Kim, Carol Steinberg, Reginald F. Munden, Deb Kirby, Jo Ann Stetz, Barbara O'Brien, Sally Tenorio, Laura Multerer, Carlotta McCalister-Cross, Jessica Silva-Gietzen, Tamara Saunders, Harvey Glazer, Cam Vashel, Maria Oh, Rodkise Estell, Steven M. Moore, Tara Riley, Grant Izmirlian, D. Claire Anderson, James Burner, Steven Peace, Phil Hoffman, Angela Del Pino, Brian Irons, Carlos Jamis-Dow, John K. Lawlor, Edward F. Patz, Jay Afiat, Amber Barrow, Bawn M. Beno, Melissa S. Fritz, Lynn Coppage, Scott J. Sheltra, Tim Swan, Jerry Bergen, Charlie Fenton, Eric Deaton, Marilyn J. Siegel, Korinna Vigeant, Kerry Engber, Sarah Merrill, Buddy Williams, Kimberly Stryker, Bradley S. Snyder, Christina Romo, Andrea Hugill, Michael J. O'Shea, Linda White, Gail Fellows, Yasmeen Hafeez, Joe Woodside, Shauna Dave Scholl, Philip C. Prorok, Sharon Carmen, Kelly Hatton, Steven V. Marx, Sooah Kim, Robert Kobistek, Dawn Thomas, Lea Momongan, Chris Steward, Kari Bohman, Holly Bradford, Bradley S. Sabloff, Phillip Peterson, William C. Black, Lisa Pineda, James G. Ravenel, Karen Taylor, Beverly Trombley, Mona N. Fouad, Amber McDonald, Lauren J. Ramsay, Lisa Harmon, Jeffrey Geiger, David L. Spizarny, Jeffrey S. Klein, Xizeng Wu, Heather Tumberlinson, Joy Espiritu, Gina Varner, Dawn Fuehrer, Eric A. Hoffman, Sheila Moesinger, Nina Wadhwa, Steve King, Patricia Lavernick, Paola Spicker, Timothy R. Church, Cheryl Whistle, Sheila Greenup, Patricia Fantuz, Stephanie Levi, Peter Balkin, Mary E. Johnson, Johanna Ziegler, Susan Hoffman, Kathy L. Clingan, Craig Kuhlka, Maria Marchese, Lawrence F Cohen, Cylen Javidan-Nejad, Wilbur A. Franklin, Kevin J. Leonard, Tim A. Parritt, Jade Quijano, Kathleen Poler, Jennifer Rosenbaum, Xiuli Zhang, Christine Brown, Terri David-Schlegel, Susan M. Peterson, James R. Jett, Kenneth W. Clark, Edward P. Gelmann, Arthur Migo, Patricia Fox, Lori Hamm, Janie McMahon, Darlene Guillette, Robert C. Young, Patty Beckmann, Jerome Jones, Nikki Jablonsky, Roberta Yoffie, Heather L. Bradley, Darlene Higgins, Francine L. Jacobson, Christine B. Berg, Mark Bramwitt, Constantine N. Petrochko, Karen Stokes, Jennifer Rowe, Kathy McKeeta-Frobeck, Brenda Sleasman, Courtney Bell, Dave Tripp, Saundra S. Buys, Susan Walsh, Jo Rean D. Sicks, Richard G. Barr, Kirk Midkiff, Tom Caldwell, Elisabeth A. Grady, Subbarao Inampudi, Marilyn Calulot, Paul A. Kvale, Alice DuChateau, Kathy Berreth, Ruth Holdener, Katie Kuenhold, Thomas E. Warfel, David P. Naidich, Mandie Leming, Fraser Wilton, Leanne Franceshelli, Kathleen McMurtrie, Elaine Bowman, Donald F. Bittner, Helen Kaemmerer, Merri Mullennix, Adelheid Lowery, Andrew Karellas, Jenny Hirschy, Kate Naughton, Ashley B. Long, Kristin M. Gerndt, Kathleen Young, Richard M. Schwartzstein, Wendy Smith, Joseph Aisner, Shane Ball, Kathleen Krach, Cathy Mueller, Virginia May, Christopher Blue, Marsha Lawrence, Ronald S. Kuzo, Colleen McGuire, Alisha Moore, Sara Cantrell, Christie Leary, Pamela Allen, Maryann Trotta, Clifford Caughman, Peggy J. Gocala, Brian Mullen, Janan Alkilidar, Maryann Duggan, Lin Mueller, Alesis Nieves, Fenghai Duan, Frederick Olson, Edwin G. Williams, Jo Ann Hall Sky, Grant Izmirilian, Peggy Joyce, Judy Preston, Cristine Juul, Julianne Falcone, Bruce Neilson, Fla Lisa Beagle, Beth Evans, Jamie Mood, Janet Bishop, Jean Tsukamoto, Vivien Gardner, Gillian Devereux, Minesh Patel, Sally Fraki, Celia Stolin, Ami Lyn Taplin, Stephenie Johnson, Saeed Matinkhah, Jenna Bradford, Sanjeev Bhalla, Charles Jackson, Julie Haglage, Darlene R. Fleming, Allie M. Bell, Paul A. Bunn, Gail Orvis, Andrew J. Bierhals, Julie Ngo, Belores K. Prudoehl, Elaine N. Daniel, Peggy Olson, Paul F. Pinsky, Glenna M. Fehrmann, Aras Acemgil, Andrea Hamilton-Foss, Leeta Grayson, Smita Patel, Scott Emerson, Carl J. Zylak, James R. Maxwell, Jennifer Fleischer, Suzanne Smith, Jacqueline R. Sheeran, Alan Williams, Scott Gaerte, John Fletcher, Sonya Clark, Nancy Gankiewicz, Stuart S. Sagel, Jason Spaulding, Nancy E. Hanson, Nicole Fields, Richard D. Nawfel, Dinakar Gopalakrishnan, Margaret Oechsli, Susan Wenmoth, Isabelle Forter, Elizabeth Morrell, Jessica Rider, Letitia Clark, Michael Woo, Cynthia A. Brown, Camille Mueller, Mark T. Dransfield, Lois M. Roberts, Anne Randall, Eduard J. Gamito, Carrie O'Brien, Carolyn Palazzolo, Julie Schach, Robert Falk, Melissa Hudson, Jennifer Garcia Livingston, Cynthia L. Andrist, Tammy Fox, Elliott Drake, Tanya Zeiger, Renee Metz, Kevin Thomas, Neha Kumar, Elizabeth Couch, Beborah Bay, Mei Hsiu Chen, Jason Bronfman, Philip Dennis, Deb Engelhard, Pamela McBride, Daniel Kimball, Amy Haas, Pamela M. Mazuerk, Marlea Osterhout, Venetia Cooke, Tina Taylor, Amy St.Claire, Joe Hughes, Becky McElsain, Beverly Brittain, Michele Adkinson, Paige Beck, Martha Maineiro, Paula R. Beerman, Jackie Seivert, Mary M. Pollock, Donald Corle, Tina Herron, Marcella Petruzzi, Natalie F. Scully, Kenneth A. Coleman, Jennifer Yang, Debra Loria, Wendy Moss, Alan Brisendine, Cheryl M. Lewis, Dalphany Blalock, Lonni Schultz, Douglas Bashford, Nora Szabo, David Shea, Amanda Devore, Karen Schleip, Judy Netzer, Barry Clot, Gerald M. Mulligan, Nancy E. Krieger Black, David Schultz, Jim Pool, Craig E. Leymaster, Kathryn Rabanal, Kay Bohn, Tara Berg, Marisol Furlong, Stacey Mitchell, Donna Biracree, Laura Jones, Cassie Olson, Robin Stewart, Jeremy Pierce, Marilyn Bruger, Valene Kennedy, Stephanie Davis, Colin O'Donnell, Glenn A. Tung, Shannon Wright, William Lake, Sharon Jones, Vincent Girardi, Brad Benjamin, Veenu Harjani, Drew A. Torigian, Kevin Edelman, Sue Frederickson, Paul E. Smart, Michelle Wann Haynes, D S Gierada, Glenn Fletcher, Rosalie Ronan, Patricia Ann Street, Eleace Eldridge-Smith, Lynly Wilcox, Cindy Lewis-Burke, La Tonja Davis, Rachel Black Thomas, Dawn Shone, Evangeline Griesemer, Tim Budd, Lindsey Dymond, Marlene Semansky, Amy Rueth, Constantine Gatsonis, Kay H. Vydareny, Usha Singh, Amy Lita Evangelista, Angelica C. Barrett, Bethany Pitino, Shirley Wachholz, Angela M. Williams, Sandra Fiarman, Karen Luttrop, David Chellini, Michael Bradley, Helen Fink, Aaron Zirbes, Roger Inatomi, Joon K. Lee, Heather Bishop Blake, Lisa Woodard, Craig Hritz, Sarah Neff, Aine Marie Kelly, Deborah Harbison, Baigalmaa Yondonsambuu, Amy Lloyd, Christine Gjertson, Erin Cunningham, Angelee Mean, June Morfit, Ping Hu, William Thomas, Jazman Brooke, Paul Marcus, Jeremy Gorelick, Erin Lange, William Stanford, Denise R. Aberle, Lena Glick, Annabelle Lee, Ian Malcomb, Deanna L. Miller, Mary Mesnard, Jacqueline Jackson, Jhenny Hernandez, Desiree E. Morgan, Howard I. Jolies, Jacquie Marietta, Teresa Lanning, Debra Rempinski, Amanda C. Davis, Karen Mathews Batton, Mahadevappa Mahesh, Erik Wilson, Deana Nelson, Sharan L. Campleman, William Manor, Julie Sears, Howard Mann, E. David Crawford, Carl Krinopol, Greg Gambill, Margo Cousins, Rex C. Yung, Sangeeta Tekchandani, Thomas Vahey, Ann D. McGinnis, Kimberly Nolan, Kaylene Crawford, Kelli P. Rockwell, Dana Roeshe, Fred W. Prior, Kari Ranae Kramer, Heidi Nordstrom, Frank Stahan, Shawn Sams, Cherie Baiton, Joy Tani, Thomas J. Watson, Angela Cosas, Diane Kowalik, Pritha Dalal, Ann Jolly, Jeanine Wade, Laura Bailey, Julie Varner, Glen K. Nyborg, Christopher Toyn, David Gemmel, Susanna N. Dyer, Laurie Amendolare, Mary Ellen Frebes, Judy Ho, Adele Perryman, John Keller, D. Sullivan, George Mahoney, Scott Cupp, Linda L. Welch, Peter Greenwald, Robert Sole, Marcello Grigolo, Caroline Chiles, Patricia Sheridan, Deborah M. Chewar, Vijayasri Narayanaswami, Susan Blackwell, Suzanne B. Lenz, Alphonso Dial, Melvin Tockman, Carolyn Hill, John Stubblefield, Catherine E. Smith, Judith Lobaugh, Rosa M. Medina, Jackie Meier, Nandita Bhattacharjee, Robert Tokarz, Lisa Clement, Nancy Caird, Cindy Masiejczyk, Patricia Shwarts, Laura Springhetti, Sandra Schornak-Curtis, Edwin F. Donnelly, Patricia Tesch, Laurie Rathmell, Pamela K. Woodard, Edward A. Sausville, David R. Pickens, Kylee Hansen, Paulette Williams, Barbara Ferris, Rachel L. McCall, Nicole M. Carmichael, Dawn Whistler, Ramachandra Chanapatna, Glynis Marsh, Mary Wiseman, Tony DeAngelis, L. Heather, Vicki Prayer, Robin Laura, Priscilla Bland, Gregory W. Gladish, Amy Garrett, Kelly McNulty, Daniel J. Pluta, Mylene T. Truong, Serelda Young, Crista Cimis, Gordon Jacob Sen, Rhonda Rosario, Anthony B. Miller, Edward Hunt, Juanita Helms, Jill K. Bronson, Jeff Yates, Ginette D. Turgeon, Bo Lu, Nancy Fredericks, Pam Senn, Ryan Pena, Hakan Sahin, Mary Lynn Steele, Jill E. Cordes, Noel Maddy, R. Adam DeBaugh, Hope Hooks, Zipporah Lewis, Robert L. Berger, Shani Harris, Natalie Gray, Jennifer Kasecamp, Elizabeth King, Jacinta Mattingly, Hrudaya Nath, Kathy Torrence, Christine Cole Johnson, Sara Mc Clellan, Kalin Albertsen, Kim Sprenger, Ryan Norton, Jody Wietharn Kristopher, Linda Warren, Byung Choi, Casey O'Quinn, Mark K. Haron, Chris J. Jennings, Karen Robinson, Joan Molton, Dorothy Hastings, Robert I. Garver, Christopher J. Cangelosi, Jeannette Lynch, Peter Ohan, Angela Campbell, Dawn Mead, Miriam Galbraith, Divine Hartwell, Natalya Portnov, Gene L. Colice, Andetta R. Hunsaker, Analisa Somoza, Todd Risa, Daniel C. Sullivan, Karthikeyan Meganathan, Tammy DeCoste, Peter Zamora, Richard M. Fagerstrom, Iiana Gareen, Phyllis J. Walters, Barbara L. Carter, Alem Mulugeta, Rob Bowman, Kavita Garg, Andrea Franco, Mary Adams Zafar Awan, Edward Reed Smith, Rachel Phillips, Michelle Aganon-Acheta, Fred R. Hirsch, Peter Jenkins, Pamela Taybus, Joy Knowles, Karen M. Horton, Cheryl Spoutz-Ryan, Sarah Landes, William G. Hocking, Laura B. Schroeder, Erini Makariou, Jered Sieren, Kaylene Evans, Erin Nekervis, Brenda Polding, Tonda Robinson, Joel L. Weissfeld, Terry J. Sackett, Michael F. McNitt-Gray, Leslie Dobson, Raymond Weatherby, Randell Kruger, Revathy B. Iyer, Mary Krisk, Anthony Levering, Susan Collins, Alison Schmidt, William M. Hanson, Patricia Schuler, Karen Glanz, Morgan Ford, Beatrice Trotman-Bickenson, Richard Guzman, Paul Koppel, Judith K. Amorosa, Meredith Slear, Dayna Love, Carol Vaughn, Kellyn Adams, Celeste Monje, Garry Morrison, Sherri Mesquita, Paul Cronin, Tony Blake, Constance Elbon-Copp, Robert A. Clark, Felix Mestas, Erich Allman, Armen Markarian, Cheryl Souza, Karen O’Toole, Elliot K. Fishman, Karen Augustine, Jane Hill, Bonnie Kwit, Ralph Drosten, Susan Foley, Stacy E. Smith, Angie Bailey, Jennifer Bishop Kaufmann, Shelly Meese, Phillip M. Boiselle, Howard Morrow, Thomas D. Hinke, Barry Edelstein, Erin Schuler, William C. Bailey, Donna Letizia, David S. Gierada, Frederick J. Larke, Robin Haverman, Sarah Baum, Sally Hurst, Richard L. Morin, Ben Dickstein, William Russell, J. Anthony Seibert, Sophia Sabina, Mary Alyce Riley, Michael A. Taylor, Katherine BeAngelis, Robert A. Hawkins, Fernando R. Gutierrez, Amie Welch, Heather Lancor, George Armah, James Blaine, Eric Henricks, Joel Dunnington, Carole Walker, Laura Motley, Melody Kolich, Bruce J. Hillman, David W. Sturges, Mindy Lofthouse, Amy Warren, Michael Black, Mark Kolich, Lisa A. Holloway, Shannon M. Pretzel, Susan Shannon, Yassminda Harts, Dallas Sorrel, Lance A. Yokochi, Diana Wisler, Arthur Sandy, Roberta Clune, Shirley Terrian, Shalonda Manning, Bradley Willcox, Thomas J. Payne, James L. Tatum, Dale Brawner, Sandy Morales, Rodolfo C. Morice, Amy Vieth, Emily Jewitt, Chelsea O'Carroll, Theresa C. McLoud, John E. Langenfeld, Chris H. Cagnon, Lisa B. Hinshaw, Gena Kucera, Helena R. Richter, Drew Torigian, June McSwain, Courtney Eysmans, Vinis Salazar, David Spizarny, Mary Kelly-Truran, Mark Whitty, Henry Albano, Connie L. Sathre, William R. Geiser, Barnett S. Kramer, Marianna Gustitis, Gordon C. Jones, Neil E. Caporaso, Timothy Welsh, Roger Tischner, Ana Maria Mendez, Dominick A. Antico, Cathy L. Bornhorst, Carla Chadwell, Stephanie Pawlak, Kelli M. West, Joe V. Selby, Randall Kruger, Jodi Hildestad, Elaine Freesmeier, Nicole Rivas, Andrew Goodman, Naima Vera-Gonzalez, Stuart Lutzker, Eric M. Hart, Melanie Yeh, Shane Sorrell, Deb Multerer, Sharon Jacoby, Debbie Gembala, Elizabeth Fleming, Myrle Johnson, Michael J. Flynn, Frank Tabrah, Martin L. Schwartz, Deanna Mandley, Brad Siga, Guillermo Marquez, Jeffrey Koford, Victoria Jenkins, Janice Pitts, Constantine A. Gatsonis, Natalie Baptiste, Edith M. Marom, Gina Sammons, Anne Burrough, Martha Ramirez, Jack Cahill, Carl Jaffe, Linda Heinrichs, Aura Cole, Paul Rust, Alon Coppens, Gregg Hamm, Lisa Conklin, Kathleen A. Robbins, Carleaner Williams, Gwen Chalom, Winston Sterling, Colleen Hudak, Lea Matous, Ella A. Kazerooni, Denise Kriescher, David A. Lynch, Liz Bolan, Jacob Wolf, Jonathan G. Goldin, Roberta Quinn, L. A. Schneider, Kathleen A. Murray, Erica Sturgeon, Jennifer Avrin, Michelle T. Biringer, Mark Hinson, Cynthia Reiners, Brian Chin, Amy Brunst, Ann M. Lambrecht, Katherine Lohmann, Jennifer Bacon, Ulander Giles, Diane Shepherd, William T. Corey, Timothy Cosgrove, Lana C. Walters, Nancy Kadish, Hilary C. Nosker, Christine D. Berg, Thomas Payne, Jackie Becker, Kanistha Sookpisal, Lyn Seguin, Todd R. Hazelton, Roy Adaniya, James Fisher, Annmarie Walsh, Shirleen Hyun, Laura Stark, Kenneth Hansen, Carolyn Nelson, Martin Tammemagi, Mary A. Wolfsberger, Barry H. Gross, Valentina Ortico, Marge Watry, Jeff Childs, Gabe Herron, Loretta Thorpe, Lisa Damon, Evanthia Papadopoulos, Denise Moline, Voula E. Christopoulos, John D. Minna, Tony Jones, Mitchell Machtay, Michael Plunkett, Melissa Laughren, Luis Zagarra, Adam Leming, Eda Ordonez, Chris Howell, Marissa Peters, Wendy Mosiman, Joanne Gerber, Alfonso Lorenzo, Barbara L. McComb, Laura Hill, Gale Christensen, Hanna Comer, Carmen Guzman, Kathy Taylor, Misty Oviatt, Malcolm King, Lily Stone, Rex Welsh, Bernadette Pennetta, Cristina Raver, Jan E. Hyder, Stephanie Clabo, Peggy Lau, Jacqueline Fearon, Patricia Pangburn, Pamela Dow, William K. Evans, Victor De Caravalho, Mike Wirth, Brooke Johnson, Meridith Blevins, Lisa H. Gren, Sharon L. Kurjan, James P. Evans, Kirk E. Smith, Donna King, John A. Worrell, Mindy S. Geisser, Philip F. Judy, Richard Barr, Sue Misko, Stanley R. Phillips, Jillian Nickel, Christine M. McKey, Joe Austin, Donna Hartfeil, Laura Young, Shovonna White, Alexis K. Potemkin, Anthony Boulos, Tawny Martin, Karen Kofka, Heather McLaughlin, Matthew K. Siemionko, Melissa Houston, Angela Lee Rowley, Adys Fernandez, Murray Backer, Jagdish Singh, Mary Weston, Nancy Payte, Charles Apgar, John K. Gohagan, Jeff Fairbanks, Wylie Burke, David Chi, Michael Nahill, Kevin DeMarco, Karen Patella, Beverly Rozanok, Carol M. Moser, Nicole Matetic Mac, Karen Boyle, Dinah Lorenzo, Elanor Adkins, Phyllis Olsson, Amanda M. Adams, Sujaya Rao, K.E. Jones, Polly Kay, D. Lynn Werner, John B. Weaver, Sally Anne Kopesec, Jennifer Frye, Victoria Chun, Cathy Francow, Cheri Whiton, Jo Ann Nevilles, Andrew Bodd, Barbara Galen, Sabrina Chen, Cindy Cyphert, Stephen M. Moore, Petra J. Lewis, Shanna Nichols, Mareie Walters, Thea Palmer Zimmerman, Warren B. Gefter, Peter Dubbs, Ann Reinert, Holly Washburn, Renee MacDonald, Boleyn R. Andrist, Dianalyn M. Evans, Marvin Flores, Tricia Adrales-Bentz, Claudine Isaacs, Regina C. MacDougall, Greg M. Silverman, Nichoie Cadez, Lynne Bradford, Rochelle Williams, Angela M. McLaughlin, Ellen Sandberg, Cheryl Crozier, Robert Mayer, Richard P. Remitz, Sheron Bube, Leroy Riley, Vish Iyer, Sophie Breer, Stephen Baylin, Anna Boyle, Shannon Williams, Kristen Keating, Martin M. Oken, Gerald L. Andriole, Bruce E. Hubler, Eric T. Goodman, David Engelhart, Bonna Au, Brianne Whittaker, Tricia Hoffa, Eng Brown, Tammy Wolfsohn, Denise L. Foster, Barry H. Cohen, Linda Galocy, Matthew T. Bee, Jacqueline Matuza, Leslie Henry, Katherine Meagher, Mona Fouad, Beth McLellan, Troy Cook, John Sheflin, Lilian Villaruz, Marcella Moore, Brandy Mack-Pipkin, Vanessa Graves, Ryan Weyls, William T. Herbick, Geoffrey McLennan, Lynn Hoese, Janise Webb, Terrie Kitchner, Michele Lee, Robert T. Greenlee, Charles C. Matthews, Nicole Spiese, Jeffrey Heffernon, Dianna D. Cody, Patricia Blair, Kathy Garrett, Michael A. Sullivan, and Loretta Granger

Subjects

Oncology, medicine.medical_specialty, business.industry, Mortality rate, medicine.disease, law.invention, Quality-adjusted life year, Randomized controlled trial, law, Internal medicine, medicine, Radiology, Nuclear Medicine and imaging, National Lung Screening Trial, Radiology, Overdiagnosis, business, Lung cancer, Lung cancer screening, Mass screening

Abstract

The National Lung Screening Trial (NLST) is a randomized multicenter study comparing low-dose helical computed tomography (CT) with chest radiography in the screening of older current and former heavy smokers for early detection of lung cancer, which is the leading cause of cancer-related death in the United States. Five-year survival rates approach 70% with surgical resection of stage IA disease; however, more than 75% of individuals have incurable locally advanced or metastatic disease, the latter having a 5-year survival of less than 5%. It is plausible that treatment should be more effective and the likelihood of death decreased if asymptomatic lung cancer is detected through screening early enough in its preclinical phase. For these reasons, there is intense interest and intuitive appeal in lung cancer screening with low-dose CT. The use of survival as the determinant of screening effectiveness is, however, confounded by the well-described biases of lead time, length, and overdiagnosis. Despite previous attempts, no test has been shown to reduce lung cancer mortality, an endpoint that circumvents screening biases and provides a definitive measure of benefit when assessed in a randomized controlled trial that enables comparison of mortality rates between screened individuals and a control group that does not undergo the screening intervention of interest. The NLST is such a trial. The rationale for and design of the NLST are presented.

Published

2011

26. Sa1453 - Secretin Knockout Reduces Liver Damage in Alcoholic Liver Disease

Author

Sugeily Ramos-Lorenzo, Kelly McDaniel, Thao Giang, Adrien Guillot, Shannon Glaser, Heather Francis, Bin Gao, Gianfranco Alpini, Nan Wu, Konstantina Kyritsi, Fanyin Meng, and Julie Venter

Subjects

medicine.medical_specialty, Alcoholic liver disease, Endocrinology, Hepatology, business.industry, Internal medicine, Gastroenterology, medicine, Liver damage, business, medicine.disease, Secretin

Published

2018

27. 245 - Liver Specific Deletion of Microrna-34A Alleviates Cellular Senescence and Liver Fibrosis During Experimental Cholestasis

Author

Kelly McDaniel, Sugeily Ramos-Lorenzo, Nan Wu, Shannon Glaser, Gianfranco Alpini, Tianhao Zhou, Heather Francis, and Fanyin Meng

Subjects

Hepatology, Cholestasis, MicroRNA 34a, business.industry, Liver fibrosis, Gastroenterology, Cancer research, medicine, Cellular senescence, medicine.disease, business

Published

2018

28. Sa1466 - Knockout of Microrna-21 Attenuates Alcoholic Hepatitis Through VHL/NF-KB Signaling Pathway

Author

Shannon Glaser, Nan Wu, Tianhao Zhou, Gianfranco Alpini, Heather Francis, Sugeily Ramos-Lorenzo, Fanyin Meng, Keisaku Sato, Lindsey Kennedy, and Kelly McDaniel

Subjects

Hepatology, NF-kB Signaling Pathway, microRNA, Gastroenterology, Cancer research, medicine, Alcoholic hepatitis, Biology, medicine.disease

Published

2018

29. Tu1619 Blockade of Substance P Receptor attenuates Cellular Senescence and Liver Fibrosis in the Mdr2−/− Mouse Model of Primary Sclerosing Cholangitis

Author

Heather Francis, Shannon Glaser, Tianhao Zhou, Fanyin Meng, Ying Wan, Kelly McDaniel, Nan Wu, Holly Standeford, Julie Venter, and Gianfranco Alpini

Subjects

Pathology, medicine.medical_specialty, Hepatology, business.industry, Liver fibrosis, Gastroenterology, medicine, Cellular senescence, medicine.disease, business, Substance-P Receptor, Blockade, Primary sclerosing cholangitis

Published

2016

30. 745 Inhibition of Hepatic Stellate Cell Activation by Stem Cell Derived Extracellular Vesicles and microRNAs During Cholestatic Liver Injury

Author

Lindsey Kennedy, Gianfranco Alpini, Kelly McDaniel, Tianhao Zhou, Heather Francis, Julie Venter, Fanyin Meng, Shannon Glaser, Ying Wan, and Nan Wu

Subjects

Liver injury, Hepatology, Chemistry, microRNA, Gastroenterology, Hepatic stellate cell, medicine, Stem cell, medicine.disease, Hepatic stellate cell activation, Extracellular vesicles, Cell biology

Published

2016

31. Characterization of Endothelial Dysfunction in Microrna-34A Knockout Mice with Alcoholic Liver Injury

Author

Tianhao Zhou, Ying Wan, Sugeily Ramos-Lorenzo, Gianfranco Alpini, Julie Venter, Heather Francis, Hidekazu Tsukamoto, Keisaku Sato, Nan Wu, Fanyin Meng, Kelly McDaniel, and Shannon Glaser

Subjects

Liver injury, Hepatology, business.industry, MicroRNA 34a, Knockout mouse, Gastroenterology, Cancer research, Medicine, Endothelial dysfunction, business, medicine.disease

Published

2017

32. The Secretin/Secretin Receptor Axis is Required for Inflammatory Cell-Cell Communication Via Extracellular Vesicles Between Cholangiocytes Treated with Lipopolysaccharide

Author

Tianhao Zhou, Gianfranco Alpini, Nan Wu, Kelly McDaniel, Julie Venter, Fanyin Meng, Keisaku Sato, and Shannon Glaser

Subjects

medicine.medical_specialty, Cell signaling, Hepatology, Lipopolysaccharide, Chemistry, Gastroenterology, Extracellular vesicles, Secretin, Cell biology, chemistry.chemical_compound, Endocrinology, Internal medicine, Inflammatory cell, medicine, Secretin receptor

Published

2017

33. Depletion of Microrna-21 Reduces Infiltration of Macrophages and Neutrophils in the Liver and Attenuates Inflammatory Cytokine Production in Liver Macrophages During Experimental Cholestatic Liver Injury

Author

Fanyin Meng, Heather Francis, Tianhao Zhou, Ying Wan, Lindsey Kennedy, Kelly McDaniel, Julie Venter, Keisaku Sato, Gianfranco Alpini, Shannon Glaser, and Sugeily Ramos-Lorenzo

Subjects

Liver injury, Pathology, medicine.medical_specialty, Cytokine, Hepatology, Chemistry, medicine.medical_treatment, microRNA, Gastroenterology, medicine, medicine.disease, Infiltration (medical)

Published

2017

34. Therapeutic actions of melatonin on gastrointestinal cancer development and progression

Author

Rachael, Glenister, Kelly, McDaniel, Heather, Francis, Julie, Venter, Kendal, Jensen, Giuseppina, Dusio, Eugenio, Gaudio, Shannon, Glaser, Fanyin, Meng, and Gianfranco, Alpini

Subjects

endocrine system, hormones, hormone substitutes, and hormone antagonists, Article

Abstract

Melatonin exerts a multitude of physiological functions including the regulation of the sleep cycle and circadian rhythm. Although the synthesis of melatonin in the pineal gland is regulated by changes in the light/dark cycle, the release of melatonin in the gastrointestinal tract is related to food consumption. Melatonin regulates antioxidative processes and it improves T-helper cell response by stimulating the production of specific cytokines. Melatonin is directly involved in preventing tumor initiation, promotion, and progression in a variety of cancers of the gastrointestinal tract including colorectal cancer, cholangiocarcinoma, hepatocarcinoma, and pancreatic carcinoma. This paper is a review of the literature regarding melatonin in the gastrointestinal tract and as a potential therapy for gastrointestinal cancers.

Published

2013

35. 287 Senescence of Activated Hepatic Stellate Cells Limits Liver Fibrosis During Alcoholic Liver Injury

Author

Kelly McDaniel, Julie Venter, Shannon Glaser, Haibo Bai, Nan Wu, Fanyin Meng, Heather Francis, Gianfranco Alpini, Ying Wan, and Tianhao Zhou

Subjects

Senescence, Liver injury, Pathology, medicine.medical_specialty, Hepatology, business.industry, Liver fibrosis, Gastroenterology, Hepatic stellate cell, Medicine, business, medicine.disease

Published

2016

36. 653 microRNA-34a Regulates Alcoholic Hepatitis Through SIRT1/NF-kappa;B Pathway

Author

Heather Francis, Tianhao Zhou, Julie Venter, Haibo Bai, Ying Wan, Nan Wu, Shannon Glaser, Fanyin Meng, Gianfranco Alpini, and Kelly McDaniel

Subjects

Hepatology, business.industry, MicroRNA 34a, Gastroenterology, Cancer research, Medicine, Alcoholic hepatitis, NFKB1, business, medicine.disease

Published

2016

37. Tu1618 Treatment of Biliary Injury With Small Cholangiocyte Therapy Decreases Stellate Cell Activation via Mediation of Cellular Senescence

Author

Nan Wu, Heather Francis, Gianfranco Alpini, Fanyin Meng, Shannon Glaser, Julie Venter, Tianhao Zhou, Ying Wan, and Kelly McDaniel

Subjects

medicine.medical_specialty, Hepatology, business.industry, Gastroenterology, Cellular senescence, Cholangiocyte, Biliary injury, Endocrinology, Internal medicine, Mediation, Hepatic stellate cell, medicine, Cancer research, business

Published

2016

38. PMS60 The Time Horizon Matters: Exploratory Results Varying the Time Horizon in Time Trade-Off and Standard Gamble Utility Elicitation

Author

M.K. Devine, Lee Bowman, David Feeny, Evan W Davies, Louis S. Matza, Joseph A. Johnston, Jessica B Jordan, Kelly McDaniel, and Kristina S. Boye

Subjects

Operations research, Health Policy, Economics, Public Health, Environmental and Occupational Health, Time horizon, Standard gamble, Utility elicitation, Time-trade-off

Published

2012

39. P1089 : Cellular senescence and lipopolysaccharide/toll-like receptor 4 signaling in alcoholic steatohepatitis

Author

Yuyan Han, Heather Francis, Kelly McDaniel, Fanyin Meng, and Gianfranco Alpini

Subjects

Toll-like receptor, chemistry.chemical_compound, Hepatology, Lipopolysaccharide, chemistry, Cellular senescence, Biology, Alcoholic steatohepatitis, Cell biology

Published

2015

40. Sa1718 C-Myc-Regulated Biliary Cellular Senescence and Functional Heterogeneity During Cholestatic Liver Injury

Author

Tami Annable, Debolina Ray, Kelly McDaniel, Shanika Avila, Ying Wan, Shannon Glaser, Nan Wu, Fanyin Meng, Heather Francis, Gianfranco Alpini, Yuyan Han, and Julie Venter

Subjects

Liver injury, Hepatology, Gastroenterology, Cancer research, medicine, Cellular senescence, Biology, medicine.disease

Published

2015

41. Sa1715 Regulation of Cellular Senescence by the microRNA-34a/p53 Axis During Alcoholic Liver Injury

Author

Heather Francis, Nan Wu, Shannon Glaser, Julie Venter, Tami Annable, Fanyin Meng, Ying Wan, Yuyan Han, Gianfranco Alpini, and Kelly McDaniel

Subjects

Liver injury, Hepatology, MicroRNA 34a, Gastroenterology, medicine, Cancer research, Cellular senescence, Biology, medicine.disease

Published

2015

42. 236 miR-34a Regulates Cellular Senescence in Activated Hepatic Stellate Cells During Alcohol Induced Hepatic Injury

Author

Yuyan Han, Julie Venter, Gianfranco Alpini, Shannon Glaser, Tami Annable, Kelly McDaniel, Fanyin Meng, Heather Francis, Ying Wan, and Nan Wu

Subjects

Hepatology, biology, urogenital system, Gastroenterology, Cellular senescence, Alcohol, medicine.disease, Molecular biology, chemistry.chemical_compound, nervous system, chemistry, Gene expression, Glial cell line-derived neurotrophic factor, biology.protein, medicine, Hepatic stellate cell, Steatosis, Gene

Abstract

A S L D A b st ra ct s GDNF suppresses expression of genes associated with hepatic steatosis Real-time PCR analyses of gene expression in liver from WT and GDNF Tg mice maintained on RD or HFD for 12 weeks. Plotted are means + SEM. *, P 5 mice per group.

Published

2015

43. 803 microRNA Regulation of Functional Heterogeneity in Human Cholangiocytes

Author

Ying Wan, Fanyin Meng, Yuyan Han, Debolina Ray, Shannon Glaser, Heather Francis, Shanika Avila, Kelly McDaniel, Julie Venter, Holly Standeford, and Gianfranco Alpini

Subjects

Hepatology, microRNA, Gastroenterology, Biology, Cell biology

Published

2015

44. Sa1720 Knockdown of microRNA-21 Reduces Biliary Hyperplasia and Liver Fibrosis in Cholestatic Bile Duct Ligated (BDL) Mice

Author

Heather Francis, Fanyin Meng, Yuyan Han, Laura Hargrove, Holly Standeford, Lindsey Kennedy, Gianfranco Alpini, Kelly McDaniel, and Julie Venter

Subjects

Gene knockdown, Pathology, medicine.medical_specialty, medicine.anatomical_structure, Hepatology, business.industry, Biliary hyperplasia, Bile duct, Liver fibrosis, microRNA, Gastroenterology, medicine, business

Published

2015

45. Sa1719 Dark Therapy Protects Mdr2−/- Mice From Cholestatic Liver Injury Through miR-34a Regulation of the p53/SIRT-1 Signaling Pathway

Author

Yuyan Han, Nan Wu, Fanyin Meng, Gianfranco Alpini, Debolina Ray, Julie Venter, Shannon Glaser, Kelly McDaniel, Holly Standeford, Shanika Avila, and Ying Wan

Subjects

Liver injury, Hepatology, Dark therapy, business.industry, Gastroenterology, Cancer research, Medicine, Signal transduction, business, medicine.disease

Published

2015

46. 698 Signal Transducer and Activator of Transcription (STAT)-3 Regulates MicroRNA Gene Expression in Alcoholic Steatohepatitis

Author

Julie Venter, Yuyan Han, Shannon Glaser, Fanyin Meng, Morgan Quezada, Heather Francis, Gianfranco Alpini, Kelly McDaniel, and Mena Milad

Subjects

Hepatology, Gastroenterology, MicroRNA Gene, STAT protein, Cancer research, Biology, STAT4, Alcoholic steatohepatitis, stat

Published

2014

47. Sa1700 Inhibition of the Substance P/Neurokinin 1 Receptor Signaling Axis Reduces Cholangiocarcinoma Growth In Vivo

Author

Matthew McMillin, Syeda H. Afroze, Gabriel Frampton, Holly Standeford, Fanyin Meng, Kelly McDaniel, Shannon Glaser, Sharon DeMorrow, Yuyan Han, Julie Venter, Laura Hargrove, Heather Francis, Micheleine Guerrier, Shanika Avila, and Gianfranco Alpini

Subjects

Liver injury, medicine.medical_specialty, Hepatology, Chemistry, Gastroenterology, Cholangiocyte proliferation, Substance P, medicine.disease, Cholangiocyte, chemistry.chemical_compound, Endocrinology, In vivo, Internal medicine, Tachykinin receptor 1, medicine, Phosphorylation, Galanin

Abstract

A S L D A b st ra ct s increase in circulating Galanin in the serum. Galanin immunoreactivity was observed in both cholangiocytes and hepatocytes, whereas GalR1 was found predominantly in cholangiocytes. Systemic treatment of rats with M617 increased both CK-19 expression and IBDM in both sham and BDL-treated animals. In vitro, treatment of the mouse cholangiocyte cell line with M617 increased ERK1/2 and RSK-1 activity. There was a concomitant increase in cholangiocyte proliferation after M617 treatment that could be blocked by pretreatment with inhibitors for ERK1/2 and RSK-1. Conclusions: Data presented here demonstrate a direct stimulatory role for Galanin on cholangiocyte proliferation under physiological (sham) and pathological (BDL) conditions via a mechanism involving the activation of ERK1/2 and subsequent phosphorylation of RSK-1. Targeting Galanin or GalR1 may prove a useful strategy to regulate biliary mass during cholestatic liver injury.

Published

2014

48. 646 Translational Control of the Circadian Rhythms by MicroRNA-34a in Human Cholangiocarcinoma

Author

Shannon Glaser, Fanyin Meng, Gianfranco Alpini, Yuyan Han, Heather Francis, Kelly McDaniel, and Julie Venter

Subjects

PER2, CLOCK, endocrine system, Hepatology, MicroRNA 34a, Cell growth, microRNA, Gastroenterology, Gene silencing, Cell cycle, Biology, Cell biology, PER1

Abstract

Background & aims: Disruption of circadian rhythm is associated with cancer development and progression. MicroRNAs (miRNAs) are a class of small noncoding RNAs that trigger mRNA translation, repression or degradation. Core clock genes are the molecular basis of circadian rhythms, which include BMAL1, CLOCK, Per1/2/3 and Cry1/2. We have previously demonstrated the downregulation of Per1 expression in human cholangiocarcinoma (CCA) that was predicted as the direct target of miR-34a. Thus, we aimed to evaluate the role of deregulated circadian rhythm and related microRNAs in CCA growth. Methods: Human intraand extrahepatic CCA cells and non-malignant (H69) human cholangiocytes were serum starved for 48 hr before stimulation with 50% serum for 2 hours. The 24-hour rhythmic expression of core clock genes, such as Per1,2/3, CLOCK, BMAL1 and Cry1/2 was evaluated in CCA and H69 cells by real-time PCR. To further evaluate the role of Per1, we overexpressed Per1 by transfecting the Mz-ChA-1 cells with Per1 cDNA and empty vector. In parallel, we also silenced miR-34a expression with lenti-miR-34a ZIP with relative controls. A stably overexpressing Per1 cell line and silencing of miR-34a were established, respectively. Then, wemeasured: (i) cell proliferation byMTS assays and PCNA immunoblots; (ii) cell cycle by BD Cycle test Plus reagent kit; (iii) apoptosis by Annexin V-PE apoptosis detection kit; and (iv) cell migration and invasion by commercially available kits. We utilized luciferase assay to demonstrate that Per1 act as a target of miR-34a. Results: The 24-hour rhythmical expression of Per1 was abolished in all CCA cell lines but not in H69 cells. The rhythmic expression of BMAL1, CLOCK, Per2/3, Cry1/2 was also lost in some of the CCA cell lines tested. After overexpression of Per1, the extrahepatic CCA cell line, Mz-ChA-1, showed: (i) reduced cell proliferation (by MTS assays and PCNA immunoblots); (ii) higher G0/G1 arrest and lower G2/M arrest; (iii) enhanced apoptosis; and (iv) decreased cell invasion and migration compared to control cells. Interestingly, miR-34a was rhythmically expressed in CCA cell lines and H69. The expression level of miR-34a was higher in CCA cell lines compared to H69. Moreover, the inhibition of miR-34a decreased proliferation, migration and invasion in CCA cell lines. Dual luciferase reporter assay demonstrated that miR-34a directly targets Per1. Summary and conclusions: Disruption of circadian rhythms, miR-34a and Per1 expression may contribute to the malignant phenotypes of human cholangiocarcinoma. Our findings suggest that modulation of miR-34a-dependent Per1 expression may represent a novel therapeutic approach for human CCA.

Published

2014

49. Tu1821 Regulation of the Extrinsic Apoptotic Pathway by MicroRNA-21 in Alcoholic Liver Injury

Author

Gianfranco Alpini, Julie Venter, Shannon Glaser, Kelly McDaniel, Fanyin Meng, Yuyan Han, Heather Francis, and Morgan Quezada

Subjects

Liver injury, Extrinsic apoptotic pathway, Hepatology, microRNA, Gastroenterology, medicine, Cancer research, Biology, medicine.disease

Published

2014

50. 473 Functional Role of Definitive Endoderm Marker FOXA2 in Biliary-Committed Progenitor Cells During Cholestatic Liver Injury

Author

Micheleine Guerrier, Heather Francis, Shannon Glaser, Gianfranco Alpini, Yuyan Han, Julie Venter, Kelly McDaniel, and Fanyin Meng

Subjects

Liver injury, Functional role, Pathology, medicine.medical_specialty, Hepatology, business.industry, Gastroenterology, Medicine, FOXA2, Progenitor cell, business, medicine.disease, Definitive endoderm

Published

2014