Your search keyword '"Stephen C. Strom"' showing total 290 results

1. Effects of Pro-Inflammatory Cytokines on Hepatic Metabolism in Primary Human Hepatocytes

Author

Roberto Gramignoli, Aarati R. Ranade, Raman Venkataramanan, and Stephen C. Strom

Subjects

hepatocyte transplantation, inflammatory cytokines, hepatic functions, Biology (General), QH301-705.5, Chemistry, QD1-999

Abstract

Three decades of hepatocyte transplantation have confirmed such a cell-based approach as an adjunct or alternative treatment to solid organ transplantation. Donor cell survival and engraftment were indirectly measured by hepatospecific secretive or released metabolites, such as ammonia metabolism in urea cycle defects. In cases of sepsis or viral infection, ammonia levels can significantly and abruptly increase in these recipients, erroneously implying rejection. Pro-inflammatory cytokines associated with viral or bacterial infections are known to affect many liver functions, including drug-metabolizing enzymes and hepatic transport activities. We examined the influence of pro-inflammatory cytokines in primary human hepatocytes, isolated from both normal donors or patients with metabolic liver diseases. Different measures of hepatocyte functions, including ammonia metabolism and phase 1–3 metabolism, were performed. All the hepatic functions were profoundly and significantly suppressed after exposure to concentrations of from 0.1 to 10 ng/mL of different inflammatory cytokines, alone and in combination. Our data indicate that, like phase I metabolism, suppression of phase II/III and ammonia metabolism occurs in hepatocytes exposed to pro-inflammatory cytokines in the absence of cell death. Such inflammatory events do not necessarily indicate a rejection response or loss of the cell graft, and these systemic inflammatory signals should be carefully considered when the immunosuppressant regiment is reduced or relieved in a hepatocyte transplantation recipient in response to such alleged rejection.

Published

2022

2. Gene Editing Correction of a Urea Cycle Defect in Organoid Stem Cell Derived Hepatocyte-like Cells

Author

Mihaela Zabulica, Tomas Jakobsson, Francesco Ravaioli, Massoud Vosough, Roberto Gramignoli, Ewa Ellis, Olav Rooyackers, and Stephen C. Strom

Subjects

iPSC, hepatocytes, disease modelling, genome editing, CRISPR, urea cycle, Biology (General), QH301-705.5, Chemistry, QD1-999

Abstract

Urea cycle disorders are enzymopathies resulting from inherited deficiencies in any genes of the cycle. In severe cases, currently available therapies are marginally effective, with liver transplantation being the only definitive treatment. Donor liver availability can limit even this therapy. Identification of novel therapeutics for genetic-based liver diseases requires models that provide measurable hepatic functions and phenotypes. Advances in stem cell and genome editing technologies could provide models for the investigation of cell-based genetic diseases, as well as the platforms for drug discovery. This report demonstrates a practical, and widely applicable, approach that includes the successful reprogramming of somatic cells from a patient with a urea cycle defect, their genetic correction and differentiation into hepatic organoids, and the subsequent demonstration of genetic and phenotypic change in the edited cells consistent with the correction of the defect. While individually rare, there is a large number of other genetic-based liver diseases. The approach described here could be applied to a broad range and a large number of patients with these hepatic diseases where it could serve as an in vitro model, as well as identify successful strategies for corrective cell-based therapy.

Published

2021

3. Effects of Cryogenic Storage on Human Amnion Epithelial Cells

Author

Raghuraman C. Srinivasan, Stephen C. Strom, and Roberto Gramignoli

Subjects

placenta, amnion membrane, cell-based therapy, cryopreservation, cell transplant, Cytology, QH573-671

Abstract

Perinatal stem cells and epithelial cells isolated from full term amnion membrane, in particular, have attracted interest over the last decade, as a promising source of multipotent cells for cellular therapies. Human amnion epithelial cells (hAEC) have been used to treat monogenetic liver disease such as maple syrup urine disease or fibrosis of the liver in preclinical studies. In most studies xeno-transplants of hAEC were conducted without providing immunosuppression to recipients, reflecting the tolerogenic properties of hAEC. For many cell types, successful cryopreservation is critical for providing a readily available, off-the-shelf product. In this study, hAEC were isolated from full-term human placenta from 14 different donors, cryopreserved using a protocol and reagents commonly adopted for epithelial cell preservation. The cells were analyzed in terms of survival, recovery, and homogeneity, profiled for surface markers characteristic of epithelial, mesenchymal, endothelial, or hematopoietic cells. There were no significant differences observed in the percentage of cells with epithelial cell markers before and after cryopreservation. The relative proportion of stromal and hematopoietic cells was significantly reduced in hAEC preparations after cryopreservation. The expression of stem cell and immunomodulatory molecules were confirmed in the final product. Since multipotent cells are readily available from full-term placenta, this novel cell source might significantly increase the number of patients eligible to receive cellular therapies for liver and other diseases.

Published

2020

4. Potential Barriers to Human Hepatocyte Transplantation in MUP–uPARag2γC Mice

Author

Junji Komori, Aaron D. Deward, Roberto Gramignoli, Stephen C. Strom, Paulo Fontes, and Eric Lagasse PharmD, Ph.D.

Subjects

Medicine

Abstract

Primary human fetal and adult hepatocytes have been considered feasible donor cell sources for cell transplantation. We compared the engraftment efficiencies between adult human, fetal human, and adult porcine hepatocytes after transplantation into MUP–uPA tg(+/+) Rag2 -/- γC -/- mice. Transplantation of adult human hepatocytes yielded a 1,000-fold higher serum albumin level compared to transplantation of fetal human hepatocytes, while transplantation of adult porcine hepatocytes resulted in a 100-fold higher serum albumin level than adult human hepatocytes. These results suggest that adult liver cells are superior to fetal liver cells for transplantation, and caution should be applied if porcine hepatocytes are used for preclinical studies as a proof of concept for human hepatocytes.

Published

2014

5. Rapid and Sensitive Assessment of Human Hepatocyte Functions

Author

Roberto Gramignoli, Veysel Tahan, Kenneth Dorko, Raman Venkataramanan, Ira J. Fox, Ewa C. S. Ellis, Massoud Vosough, and Stephen C. Strom Ph.D.

Subjects

Medicine

Abstract

Transplantation of human hepatocytes (HTx) has gained recognition as a bridge to, or an alternative to, orthotopic liver transplantation for patients with acute liver failure or genetic defects in liver function. Although the quality of the hepatocytes used for cell transplantation is critical, no consensus exists on protocols to assess the function of hepatocytes prior to HTx. Application of this cell therapy in clinical practice could be aided by fast and reliable assays to evaluate the functional competence of isolated hepatocytes prior to clinical transplantation. Traditional assays for measuring metabolic functions in primary hepatocytes frequently involve highly technical equipment, time-consuming methods, and large numbers of cells. We describe a novel approach for the rapid assessment of the metabolic capabilities of human hepatocytes. This report details simple procedures to evaluate 11 endpoints from cells isolated from human liver that can be performed by a single operator within approximately 2 h of isolation. Longer term cultured hepatocytes were also analyzed to determine if the results from the 2-h tests were predictive of long-term hepatic function. The assays simultaneously measure five cytochrome P450 activities, one phase II activity, plating efficiency, and ammonia metabolism in addition to viability and cell yield. The assays require fewer than 20 million cells and can be completed using commonly available and inexpensive laboratory equipment. The protocol details methods that can be used in a time frame that would allow analysis of hepatic functions in freshly isolated hepatocytes prior to their use for clinical transplantation.

Published

2014

6. Hypothermic Storage of Human Hepatocytes for Transplantation

Author

Roberto Gramignoli, Kenneth Dorko, Veysel Tahan, Kristen J. Skvorak, Ewa Ellis, Carl Jorns, Bo-Goran Ericzon, Ira J. Fox, and Stephen C. Strom Ph.D.

Subjects

Medicine

Abstract

Transplantation of human hepatocytes is gaining recognition as a bridge or an alternative to orthotopic liver transplantation for patients with acute liver failure and genetic defects. Since most patients require multiple cell infusions over an extended period of time, we investigated hepatic functions in cells maintained in University of Wisconsin solution at 4°C up to 72 h. Eleven different assessments of hepatic viability and function were investigated both pre- and posthypothermic storage, including plating efficiency, caspase-3/7 activity, ammonia metabolism, and drug-metabolizing capacity of isolated hepatocytes. Long-term function, basal, and induced cytochrome P450 activities were measured after exposure to prototypical inducing agents. Cells from 47 different human liver specimens were analyzed. Viability significantly decreased in cells cold stored in UW solution, while apoptosis level and plating efficiency were not significantly different from fresh cells. Luminescent and fluorescent methods assessed phases I and II activities both pre- and post-24-72 h of cold preservation. A robust induction (up to 200-fold) of phase I enzymes was observed in cultured cells. Phase II and ammonia metabolism remained stable during hypothermic storage, although the inductive effect of culture on each metabolic activity was eventually lost. Using techniques that characterize 11 measurements of hepatic viability and function from plating efficiency, to ammonia metabolism, to phases I and II drug metabolism, it was determined that while viability decreased, the remaining viable cells in cold-stored suspensions retained critical hepatic functions for up to 48 h at levels not significantly different from those observed in freshly isolated cells.

Published

2014

7. Increased Reprogramming of Human Fetal Hepatocytes Compared with Adult Hepatocytes in Feeder-Free Conditions

Author

Marc C. Hansel, Roberto Gramignoli, William Blake, Julio Davila, Kristen Skvorak, Kenneth Dorko, Veysel Tahan, Brian R. Lee, Edgar Tafaleng, Jorge Guzman-Lepe, Alejandro Soto-Gutierrez, Ira J. Fox, and Stephen C. Strom

Subjects

Medicine

Abstract

Hepatocyte transplantation has been used to treat liver disease. The availability of cells for these procedures is quite limited. Human embryonic stem cells (hESCs) and induced pluripotent stem cells (hiPSCs) may be a useful source of hepatocytes for basic research and transplantation if efficient and effective differentiation protocols were developed and problems with tumorigenicity could be overcome. Recent evidence suggests that the cell of origin may affect hiPSC differentiation. Thus, hiPSCs generated from hepatocytes may differentiate back to hepatocytes more efficiently than hiPSCs from other cell types. We examined the efficiency of reprogramming adult and fetal human hepatocytes. The present studies report the generation of 40 hiPSC lines from primary human hepatocytes under feeder-free conditions. Of these, 37 hiPSC lines were generated from fetal hepatocytes, 2 hiPSC lines from normal hepatocytes, and 1 hiPSC line from hepatocytes of a patient with Crigler–Najjar syndrome, type 1. All lines were confirmed reprogrammed and expressed markers of pluripotency by gene expression, flow cytometry, immunocytochemistry, and teratoma formation. Fetal hepatocytes were reprogrammed at a frequency over 50-fold higher than adult hepatocytes. Adult hepatocytes were only reprogrammed with six factors, while fetal hepatocytes could be reprogrammed with three (OCT4, SOX2, NANOG) or four factors (OCT4, SOX2, NANOG, LIN28 or OCT4, SOX2, KLF4, C-MYC). The increased reprogramming efficiency of fetal cells was not due to increased transduction efficiency or vector toxicity. These studies confirm that hiPSCs can be generated from adult and fetal hepatocytes including those with genetic diseases. Fetal hepatocytes reprogram much more efficiently than adult hepatocytes, although both could serve as useful sources of hiPSC-derived hepatocytes for basic research or transplantation.

Published

2014

8. Development and Application of Purified Tissue Dissociation Enzyme Mixtures for Human Hepatocyte Isolation

Author

Roberto Gramignoli, Michael L. Green, Veysel Tahan, Kenneth Dorko, Kristen J. Skvorak, Fabio Marongiu, Wenchen Zao, Raman Venkataramanan, Ewa C. S. Ellis, David Geller, Andrew G. Breite, Francis E. Dwulet, Robert C. McCarthy, and Stephen C. Strom Ph.D.

Subjects

Medicine

Abstract

Human hepatocyte transplantation is gaining acceptance for the treatment of liver diseases. However, the reagents used to isolate hepatocytes from liver tissue are not standardized and show lot-to-lot variability in enzyme activity and endotoxin contamination. For clinical application, highly purified reagents are preferable to crude digest preparations. A purified tissue dissociating enzyme (TDE) preparation (CIzyme ™ purified enzymes) was developed based on the enzyme compositions found in a superior lot of collagenase previously used by our group for human hepatocyte isolation. The performance of this enzyme preparation was compared to collagenase type XI on 110 liver cases by assessing hepatocyte yield, viability, and seven other functional assays that included plating efficiency, basal and induced CYP450 activities, phase II conjugation activity, and ammonia metabolism. No statistically significant difference was observed between these TDEs when they were used to isolate hepatocytes from liver resections or organ donor tissue on 54 hepatocyte isolations with type XI enzyme and 56 isolations using CIzyme ™ . These results show that a highly purified and defined TDE preparation can be formulated that provides excellent performance with respect to viability, yield, and functional activity of the isolated cells. In addition to reproducible formulation, these purified enzyme products have only 2–3% of the endotoxin of crude enzyme preparations. These results show that purified enzymes such as CIzyme ™ will be a safe and effective for the isolation of human hepatocytes for clinical transplants.

Published

2012

9. Improving the Techniques for Human Hepatocyte Transplantation: Report from a Consensus Meeting in London

Author

Juliana Puppi, Stephen C. Strom, Robin D. Hughes, Sanjay Bansal, Jose V. Castell, Ibrahim Dagher, Ewa C. S. Ellis, Greg Nowak, Bo-Goran Ericzon, Ira J. Fox, M. José Gómez-Lechón, Chandan Guha, Sanjeev Gupta, Ragai R. Mitry, Kazuo Ohashi, Michael Ott, Lola M. Reid, Jayanta Roy-Chowdhury, Etienne Sokal, Anne Weber, and Anil Dhawan M.D., FRCPCH

Subjects

Medicine

Abstract

On September 6 and 7, 2009 a meeting was held in London to identify and discuss what are perceived to be current roadblocks to effective hepatocyte transplantation as it is currently practiced in the clinics and, where possible, to offer suggestions to overcome the blocks and improve the outcomes for this cellular therapy. Present were representatives of most of the active clinical hepatocyte transplant programs along with other scientists who have contributed substantial basic research to this field. Over the 2-day sessions based on the experience of the participants, numerous roadblocks or challenges were identified, including the source of cells for the transplants and problems with tracking cells following transplantation. Much of the discussion was focused on methods to improve engraftment and proliferation of donor cells posttransplantation. The group concluded that, for now, parenchymal hepatocytes isolated from donor livers remain the best cell source for transplantation. It was reported that investigations with other cell sources, including stem cells, were at the preclinical and early clinical stages. Numerous methods to modulate the immune reaction and vascular changes that accompany hepatocyte transplantation were proposed. It was agreed that, to obtain sufficient levels of repopulation of liver with donor cells in patients with metabolic liver disease, some form of liver preconditioning would likely be required to enhance the engraftment and/or proliferation of donor cells. It was reported that clinical protocols for preconditioning by hepatic irradiation, portal vein embolization, and surgical resection had been developed and that clinical studies using these protocols would be initiated in the near future. Participants concluded that sharing information between the groups, including standard information concerning the quality and function of the transplanted cells prior to transplantation, clinical information on outcomes, and standard preconditioning protocols, would help move the field forward and was encouraged.

Published

2012

10. Naive Rat Amnion-Derived Cell Transplantation Improved Left Ventricular Function and Reduced Myocardial Scar of Postinfarcted Heart

Author

Kazuro L. Fujimoto, Toshio Miki M.D., Ph.D., Li J. Liu, Ryotaro Hashizume, Stephen C. Strom, William R. Wagner, Bradley B. Keller, and Kimimasa Tobita

Subjects

Medicine

Abstract

Stem cells contained in the amniotic membrane may be useful for cellular repair of the damaged heart. Previously, we showed that amnion-derived cells (ADCs) express embryonic stem cell surface markers and pluripotent stem cell-specific transcription factor genes. These ADCs also possess the potential for mesoderm (cardiac) lineage differentiation. In the present study we investigated whether untreated naive ADC transplantation into the injured left ventricular (LV) myocardium is beneficial as a cell-based cardiac repair strategy in a rat model. ADCs were isolated from Lewis rat embryonic day 14 amniotic membranes. FACS analysis revealed that freshly isolated ADCs contained stage-specific embryonic antigen-1 (SSEA-1), Oct-4-positive cells, and mesenchymal stromal cells, while hematopoietic stem cell marker positive cells were absent. Reverse transcription-PCR revealed that naive ADCs expressed cardiac and vascular specific genes. We injected freshly isolated ADCs (2 × 10 6 cells suspended in PBS, ADC group) into acutely infarcted LV myocardium produced by proximal left coronary ligation. PBS was injected in postinfarction controls (PBS group). Cardiac function was assessed at 2 and 6 weeks after injection. ADC treatment attenuated LV dilatation and sustained LV contractile function at 2 and 6 weeks in comparison to PBS controls ( p < 0.05, ANOVA). LV peak systolic pressure and maximum dP/dt of ADC-treated heart were higher and LV end-diastolic pressure and negative dP/dt were lower than in PBS controls ( p < 0.05). Histological assessment revealed that infarcted myocardium of the ADC-treated group had less fibrosis, thicker ventricular walls, and increased capillary density ( p < 0.05). The fate of injected ADCs was confirmed using ADCs derived from EGFP(+) transgenic rats. Immunohistochemistry at 6 weeks revealed that EGFP(+) cells colocalized with von Willebrand factor, α-smooth muscle actin, or cardiac troponin-I. Our results suggest that naive ADCs are a potential cell source for cellular cardiomyoplasty.

Published

2009

11. Hepatocyte Transplantation: Clinical Experience and Potential for Future Use

Author

Stephen C. Strom, Paolo Bruzzone, Hongbo Cai, Ewa Ellis, Thomas Lehmann, Keitaro Mitamura, and Toshio Miki

Subjects

Medicine

Abstract

Hepatocyte transplantation has been proposed as a method to support patients with liver insufficiency. There are three main areas where the transplantation of isolated hepatocytes has been proposed and used for clinical therapy. Cell transplantation has been used: 1) for temporary metabolic support of patients in end-stage liver failure awaiting whole organ transplantation, 2) as a method to support liver function and facilitate regeneration of the native liver in cases of fulminant hepatic failure, and 3) in a manner similar to gene therapy, as a “cellular therapy” for patients with genetic defects in vital liver functions. We will briefly review the basic research that leads to clinical hepatocyte transplantation, the published clinical experience with this experimental technique, and some possible future uses of hepatocyte transplantation.

Published

2006

12. Isolated Hepatocyte Transplantation for Crigler-Najjar Syndrome Type 1

Author

Giovanni Ambrosino, Sergio Varotto, Stephen C. Strom, Graziella Guariso, Elisa Franchin, Diego Miotto, Luciana Caenazzo, Stefano Basso, Paolo Carraro, Maria Luisa Valente, Davide D'amico, Lucia Zancan, and Lorenzo D'antiga

Subjects

Medicine

Abstract

Crigler-Najjar syndrome type 1 (CN1) is an inherited disorder characterized by the absence of hepatic uridine diphosphoglucuronate glucuronosyltransferase (UDPGT), the enzyme responsible for the conjugation and excretion of bilirubin. We performed allogenic hepatocyte transplantation (AHT) in a child with CN1, aiming to improve bilirubin glucuronidation in this condition. A 9-year-old boy with CN1 was prepared with plasmapheresis and immunosuppression with prednisolone and tacrolimus. When a graft was made available, 7.5 × 109 hepatocytes were isolated and infused into the portal vein percutaneously. After 2 weeks phenobarbitone was added to promote the enzymatic activity of UDPGT of the transplanted hepatocytes. Nocturnal phototherapy was continued throughout the studied period. Total bilirubin was considered a reliable marker of allogenic cell function. There was no significant variation of vital signs nor complications during the infusion. Mean ± SD bilirubin level was 530 ± 38 μmol/L before and 359 ± 46 μmol/L after AHT (t-test, p < 0.001). However, the introduction of phenobarbitone was followed by a drop of tacrolimus level with increase of alanine aminotransferase (ALT) and increase of bilirubin. After standard treatment of cellular rejection bilirubin fell again but from then on it was maintained at a greater level. After discharge the patient experienced a further increase of bilirubin that returned to predischarge levels after readmission to the hospital. This was interpreted as poor compliance with phototherapy. Only partial correction of clinical jaundice and the poor tolerability to nocturnal phototherapy led the parents to refuse further hepatocyte infusions and request an orthotopic liver transplant. After 24 months the child is well, with good liver function on tacrolimus and prednisolone-based immunosuppression. Isolated AHT, though effective and safe, is not sufficient to correct CN1. Maintenance of adequate immunosuppression and family compliance are the main factors hampering the success of this procedure.

Published

2005

13. In Vitro Expansion of Human Hepatocytes is Restricted by Telomere-Dependent Replicative Aging

Author

Henning Wege, Michael S. Chui, Hai T. Le, Stephen C. Strom, and Mark A. Zern

Subjects

Medicine

Abstract

Currently, different techniques to expand human hepatocytes in vitro are being investigated to generate enough cells for liver-directed cell therapies. However, based on observations in fibroblasts and other cell types, telomere attrition limits the proliferative capacity of normal somatic cells. Therefore, we explored whether telomere-dependent replicative aging restricts the in vitro proliferation of human hepatocytes. Subpopulations of cells isolated from a neonatal liver and characterized as hepatocyte derived by RT-PCR and flow cytometry started to proliferate 5–7 days after plating and were termed proliferating human hepatocytes (PHH). Following retroviral-mediated transduction of the catalytic telomerase subunit, telomerase reverse transcriptase (hTERT), telomerase activity increased from almost undetectable levels to levels as high as in HepG2 and other telomerase-positive cell lines. As expected, untransduced PHH progressively lost telomeric repeats and arrested after 30–35 cell divisions with telomeres of less than 5 kilo bases. In comparison, telomerase-reconstituted PHH maintained elongated telomeres and continued to proliferate as shown by colorimetric assays and cell counts. In this study, telomere stabilization extended the proliferative capacity of in vitro proliferating human neonatal hepatocytes. Therefore, telomere attrition needs to be addressed when developing techniques to expand human hepatocytes.

Published

2003

14. Correction of a urea cycle defect after ex vivo gene editing of human hepatocytes

Author

Raghuraman C. Srinivasan, Carl Jorns, Anna Forslöw, Johannes Häberle, Burcu Bestas, Tanja Scherer, Mike Firth, Towe Jakobsson, Barry Rosen, Gabriella Allegri, Olav Rooyackers, Susanna Engberg, Christina Hammarstedt, Beat Thöny, Pinar Akcakaya, Marcello Maresca, Natalie Van Zuydam, Ewa Ellis, Nicole Rimann, Mihaela Zabulica, Stephen C. Strom, Tomas Jakobsson, Roberto Gramignoli, and Georgios Makris

Subjects

Adult, Male, Orotic acid, Urea cycle disorder, RNA Splicing, Mutant, Biology, Mice, 03 medical and health sciences, Liver disease, 0302 clinical medicine, Ammonia, Drug Discovery, Gene expression, Genetics, medicine, Animals, Humans, Child, Molecular Biology, Cells, Cultured, Ornithine Carbamoyltransferase, Ornithine transcarbamylase deficiency, Aged, 030304 developmental biology, Gene Editing, Orotic Acid, Pharmacology, 0303 health sciences, medicine.disease, Molecular biology, Introns, Ornithine Carbamoyltransferase Deficiency Disease, Disease Models, Animal, Gene Expression Regulation, 030220 oncology & carcinogenesis, Urea cycle, Mutation, Hepatocytes, Commentary, Molecular Medicine, Female, Ex vivo, medicine.drug

Abstract

Ornithine transcarbamylase deficiency (OTCD) is a monogenic disease of ammonia metabolism in hepatocytes. Severe disease is frequently treated by orthotopic liver transplantation. An attractive approach is the correction of a patient's own cells to regenerate the liver with gene-repaired hepatocytes. This study investigates the efficacy and safety of ex vivo correction of primary human hepatocytes. Hepatocytes isolated from an OTCD patient were genetically corrected ex vivo, through the deletion of a mutant intronic splicing site achieving editing efficiencies >60% and the restoration of the urea cycle in vitro. The corrected hepatocytes were transplanted into the liver of FRGN mice and repopulated to high levels (>80%). Animals transplanted and liver repopulated with genetically edited patient hepatocytes displayed normal ammonia, enhanced clearance of an ammonia challenge and OTC enzyme activity, as well as lower urinary orotic acid when compared to mice repopulated with unedited patient hepatocytes. Gene expression was shown to be similar between mice transplanted with unedited or edited patient hepatocytes. Finally, a genome-wide screening by performing CIRCLE-seq and deep sequencing of >70 potential off-targets revealed no unspecific editing. Overall analysis of disease phenotype, gene expression, and possible off-target editing indicated that the gene editing of a severe genetic liver disease was safe and effective.

Published

2021

15. Use of Amnion Epithelial Cells in Metabolic Liver Disorders

Author

Gramignoli, Roberto, primary, Marongiu, Fabio, additional, and Stephen C., Strom, additional

Published

2016

16. Insights From Liver‐Humanized Mice on Cholesterol Lipoprotein Metabolism and LXR‐Agonist Pharmacodynamics in Humans

Author

Mirko E, Minniti, Matteo, Pedrelli, Lise-Lotte, Vedin, Anne-Sophie, Delbès, Raphaël G P, Denis, Katariina, Öörni, Claudia, Sala, Chiara, Pirazzini, Divya, Thiagarajan, Harri J, Nurmi, Markus, Grompe, Kevin, Mills, Paolo, Garagnani, Ewa C S, Ellis, Stephen C, Strom, Serge H, Luquet, Elizabeth M, Wilson, John, Bial, Knut R, Steffensen, Paolo, Parini, Minniti ME, Pedrelli M, Vedin LL, Delbès AS, Denis RGP, Öörni K, Sala C, Pirazzini C, Thiagarajan D, Nurmi HJ, Grompe M, Mills K, Garagnani P, Ellis ECS, Strom SC, Luquet SH, Wilson EM, Bial J, Steffensen KR, Parini P, Karolinska Institutet [Stockholm], Department of Laboratory Medicine [Karolinska Institutet], Unité de Biologie Fonctionnelle et Adaptative (BFA (UMR_8251 / U1133)), Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS)-Université de Paris (UP), Wihuri Research Institute [Helsinki, Finland], University of Bologna, University of Helsinki, and University College of London [London] (UCL)

Subjects

Male, Mice, Knockout, Benzylamines, Lipoproteins, [SDV.MHEP.HEG]Life Sciences [q-bio]/Human health and pathology/Hépatology and Gastroenterology, Original Articles, [SDV.MHEP.EM]Life Sciences [q-bio]/Human health and pathology/Endocrinology and metabolism, Benzoates, LDL, Mice, Cholesterol, LDLR, Liver, Liver Biology/Pathobiology, CETP, Hepatocytes, hepatocyte, Animals, Humans, lipids (amino acids, peptides, and proteins), Original Article, translatability, APOB, Liver X Receptors

Abstract

International audience; Background and Aims; Genetically modified mice have been used extensively to study human disease. However, the data gained are not always translatable to humans because of major species differences. Liver‐humanized mice (LHM) are considered a promising model to study human hepatic and systemic metabolism. Therefore, we aimed to further explore their lipoprotein metabolism and to characterize key hepatic species‐related, physiological differences.Approach and Results: Fah−/−, Rag2−/−, and Il2rg−/− knockout mice on the nonobese diabetic (FRGN) background were repopulated with primary human hepatocytes from different donors. Cholesterol lipoprotein profiles of LHM showed a human‐like pattern, characterized by a high ratio of low‐density lipoprotein to high‐density lipoprotein, and dependency on the human donor. This pattern was determined by a higher level of apolipoprotein B100 in circulation, as a result of lower hepatic mRNA editing and low‐density lipoprotein receptor expression, and higher levels of circulating proprotein convertase subtilisin/kexin type 9. As a consequence, LHM lipoproteins bind to human aortic proteoglycans in a pattern similar to human lipoproteins. Unexpectedly, cholesteryl ester transfer protein was not required to determine the human‐like cholesterol lipoprotein profile. Moreover, LHM treated with GW3965 mimicked the negative lipid outcomes of the first human trial of liver X receptor stimulation (i.e., a dramatic increase of cholesterol and triglycerides in circulation). Innovatively, LHM allowed the characterization of these effects at a molecular level.Conclusions: LHM represent an interesting translatable model of human hepatic and lipoprotein metabolism. Because several metabolic parameters displayed donor dependency, LHM may also be used in studies for personalized medicine.

Published

2020

17. Evaluation of different routes of administration and biodistribution of human amnion epithelial cells in mice

Author

Kristina Kannisto, Raghuraman C. Srinivasan, Roberto Gramignoli, and Stephen C. Strom

Subjects

0301 basic medicine, Cancer Research, Pathology, medicine.medical_specialty, Biodistribution, Cell Transplantation, Placenta, Immunology, Cell, Spleen, Mice, 03 medical and health sciences, Liver disease, 0302 clinical medicine, Pregnancy, medicine, Animals, Humans, Immunology and Allergy, Amnion, Lung, Cells, Cultured, Genetics (clinical), Transplantation, Portal Vein, business.industry, Liver Diseases, Epithelial Cells, Cell Biology, medicine.disease, 030104 developmental biology, medicine.anatomical_structure, Liver, Oncology, Splenic Vein, 030220 oncology & carcinogenesis, Models, Animal, cardiovascular system, Female, business, Preclinical imaging

Abstract

Placenta is a non-controversial and promising source of cells for the treatment of several liver diseases. We previously reported that transplanted human amnion epithelial cells (hAECs) differentiate into hepatocyte-like cells, resulting in correction of mouse models of metabolic liver disease or acute hepatic failure. As part of preclinical safety studies, we investigated the distribution of hAECs using two routes of administration to efficiently deliver hAECs to the liver. Optical imaging is commonly used because it can provide fast, high-throughput, whole-body imaging, thus DiR-labeled hAECs were injected into immunodeficient mice, via the spleen or the tail vein. The cell distribution was monitored using an in vivo imaging system over the next 24 h. After splenic injection, the DiR signal was detected in liver and spleen at 1, 3 and 24 h post-transplant. The distribution was confirmed by analysis of human DNA content at 24 h post-transplant and human-specific cytokeratin 8/18 staining. Tail vein infusion resulted in cell engraftment mainly in the lungs, with minimal detection in the liver. Delivery of cells to the portal vein, via the spleen, resulted in efficient delivery of hAECs to the liver, with minimal, off-target distribution to lungs or other organs.

Published

2019

18. Targeting HSP90 with the small molecule inhibitor AUY922 (luminespib) as a treatment strategy against hepatocellular carcinoma

Author

Sarah Mongiovì, Roberto Gramignoli, Giuseppa Augello, Roberto Puleio, Melchiorre Cervello, Maria Rita Emma, James A. McCubrey, Giuseppe Montalto, Antonina Azzolina, Beatrice Belmonte, Stephen C. Strom, Alessandro Gulino, Antonella Cusimano, Giovanni Cassata, Augello, Giuseppa, Emma, Maria Rita, Cusimano, Antonella, Azzolina, Antonina, Mongiovì, Sarah, Puleio, Roberto, Cassata, Giovanni, Gulino, Alessandro, Belmonte, Beatrice, Gramignoli, Roberto, Strom, Stephen C, McCubrey, James A, Montalto, Giuseppe, and Cervello, Melchiorre

Subjects

p53, Male, Cancer Research, Cell, Transcriptome, 0302 clinical medicine, HCC, beta Catenin, Aged, 80 and over, Luminespib, AUY922, Liver Neoplasms, Hep G2 Cells, Sorafenib, Middle Aged, Up-Regulation, Gene Expression Regulation, Neoplastic, medicine.anatomical_structure, Oncology, Caspases, 030220 oncology & carcinogenesis, Hepatocellular carcinoma, Female, NUPR1, medicine.drug, Adult, Carcinoma, Hepatocellular, β-Catenin, Mice, Nude, Antineoplastic Agents, Small Molecule Libraries, 03 medical and health sciences, Downregulation and upregulation, In vivo, Cell Line, Tumor, medicine, HSP90, Animals, Humans, HSP90 Heat-Shock Proteins, Aged, Cell growth, business.industry, Mcl-1, Isoxazoles, Resorcinols, HCCS, medicine.disease, digestive system diseases, Mutation, Cancer research, business

Abstract

Hepatocellular carcinoma (HCC) is a highly malignant tumor that responds very poorly to existing therapies, most probably due to its extraordinary inter- and intra-tumor molecular heterogeneity. The modest therapeutic response to molecular targeted agents underlines the need for new therapeutic approaches for HCC. In our study, we took advantage of well-characterized human HCC cell lines, differing in transcriptomic subtypes, DNA mutation and amplification alterations, reflecting the heterogeneity of primary HCCs, to provide a preclinical evaluation of the specific heat shock protein 90 (HSP90) inhibitor AUY922 (luminespib). Indeed, HSP90 is highly expressed in different tumor types, but its role in hepatocarcinogenesis remains unclear. Here, we analyzed HSP90 expression in primary human HCC tissues and evaluated the antitumor effects of AUY922 in vitro as well as in vivo. HSP90 expression was significantly higher in HCC tissues than in cirrhotic peritumoral liver tissues. AUY922 treatment reduced the cell proliferation and viability of HCC cells in a dose-dependent manner, but did not do so for normal human primary hepatocytes. AUY922 treatment led to the upregulation of HSP70 and the simultaneous depletion of HSP90 client proteins. In addition, in a cell type-dependent manner, treatment induced either both caspase-dependent beta-catenin cleavage and the upregulation of p53, or Mcl-1 expression, or NUPR1 expression, which contributed to the increased efficacy of, or resistance to, treatment. Finally, in vivo AUY922 inhibited tumor growth in a xenograft model. In conclusion, HSP90 is a promising therapeutic target in HCC, and AUY922 could be a drug candidate for its treatment.

Published

2018

19. Effects of a liver APOEε4 ‐genotype on synaptic integrity, gliosis and insulin signaling in the brain

Author

Lander Foquet, Tore Bengtsson, Stephen C. Strom, Joan Benedicto Gras, Christina Hammarstedt, Andres de la Rosa, Yuan Fu, Guojun Bu, Kalicharan Patra, Andreas Giannisis, Ewa Ellis, Anna Edlund, Simon Moussaud, Greg Bial, Kristina Kannisto, Henrietta M. Nielsen, and Lur Agirrezabala Nieto

Subjects

medicine.medical_specialty, Epidemiology, Health Policy, Biology, Psychiatry and Mental health, Cellular and Molecular Neuroscience, Insulin receptor, Endocrinology, Developmental Neuroscience, Gliosis, Internal medicine, Genotype, medicine, biology.protein, Neurology (clinical), Geriatrics and Gerontology, medicine.symptom

Published

2020

20. Systemic modified messenger RNA for replacement therapy in alpha 1-antitrypsin deficiency

Author

Greg Nowak, Xuling Zhu, Marianne Eybye, Lisa M. Rice, Ahmad Karadagi, Andrea Frassetto, Ewa Ellis, Paolo Martini, Alex G. Cavedon, Helen Zemack, Stephen C. Strom, Rebecca A. White, Eleonora Guadagnin, and Carl Jorns

Subjects

Genetically modified mouse, congenital, hereditary, and neonatal diseases and abnormalities, medicine.medical_specialty, medicine.medical_treatment, Blotting, Western, lcsh:Medicine, Alpha (ethology), Enzyme-Linked Immunosorbent Assay, Liver transplantation, Article, Western blot, alpha 1-Antitrypsin Deficiency, Internal medicine, medicine, Animals, Humans, RNA, Messenger, lcsh:Science, Cells, Cultured, Liver diseases, Messenger RNA, Multidisciplinary, Alpha 1-antitrypsin deficiency, Protease, Molecular medicine, medicine.diagnostic_test, business.industry, lcsh:R, medicine.disease, Blot, Disease Models, Animal, Endocrinology, alpha 1-Antitrypsin, Nanoparticles, lcsh:Q, business

Abstract

Alpha 1-antitrypsin (AAT) deficiency arises from an inherited mutation in the SERPINA1 gene. The disease causes damage in the liver where the majority of the AAT protein is produced. Lack of functioning circulating AAT protein also causes uninhibited elastolytic activity in the lungs leading to AAT deficiency-related emphysema. The only therapy apart from liver transplantation is augmentation with human AAT protein pooled from sera, which is only reserved for patients with advanced lung disease caused by severe AAT deficiency. We tested modified mRNA encoding human AAT in primary human hepatocytes in culture, including hepatocytes from AAT deficient patients. Both expression and functional activity were investigated. Secreted AAT protein increased from 1,14 to 3,43 µg/ml in media from primary human hepatocytes following mRNA treatment as investigated by ELISA and western blot. The translated protein showed activity and protease inhibitory function as measured by elastase activity assay. Also, mRNA formulation in lipid nanoparticles was assessed for systemic delivery in both wild type mice and the NSG-PiZ transgenic mouse model of AAT deficiency. Systemic intravenous delivery of modified mRNA led to hepatic uptake and translation into a functioning protein in mice. These data support the use of systemic mRNA therapy as a potential treatment for AAT deficiency.

Published

2020

21. Aging and Caloric Restriction Modulate the DNA Methylation Profile of the Ribosomal RNA Locus in Human and Rat Liver

Author

Francesco Ravaioli, Paolo Garagnani, Fabio Marongiu, Miriam Capri, Roberto Gramignoli, Chiara Pirazzini, Noémie Gensous, Ewa Ellis, Claudio Franceschi, Maria Giulia Bacalini, Gianluca Storci, Stephen C. Strom, Ezio Laconi, Gensous N., Ravaioli F., Pirazzini C., Gramignoli R., Ellis E., Storci G., Capri M., Strom S., Laconi E., Franceschi C., Garagnani P., Marongiu F., and Bacalini M.G.

Subjects

0301 basic medicine, Male, Longevity, lcsh:TX341-641, Locus (genetics), Biology, liver, DNA, Ribosomal, Article, Epigenesis, Genetic, 03 medical and health sciences, 0302 clinical medicine, Downregulation and upregulation, Protein biosynthesis, Animals, Humans, Epigenetics, Promoter Regions, Genetic, Ribosomal DNA, Nutrition and Dietetics, DNA methylation, aging, Methylation, Ribosomal RNA, Molecular biology, 3. Good health, Rats, 030104 developmental biology, Genetic Loci, RNA, Ribosomal, caloric restriction, ribosomal RNA, lcsh:Nutrition. Foods and food supply, 030217 neurology & neurosurgery, Food Science

Abstract

A growing amount of evidence suggests that the downregulation of protein synthesis is an adaptive response during physiological aging, which positively contributes to longevity and can be modulated by nutritional interventions like caloric restriction (CR). The expression of ribosomal RNA (rRNA) is one of the main determinants of translational rate, and epigenetic modifications finely contribute to its regulation. Previous reports suggest that hypermethylation of ribosomal DNA (rDNA) locus occurs with aging, although with some species- and tissue- specificity. In the present study, we experimentally measured DNA methylation of three regions (the promoter, the 5&prime, of the 18S and the 5&prime, of 28S sequences) in the rDNA locus in liver tissues from rats at two, four, 10, and 18 months. We confirm previous findings, showing age-related hypermethylation, and describe, for the first time, that this gain in methylation also occurs in human hepatocytes. Furthermore, we show that age-related hypermethylation is enhanced in livers of rat upon CR at two and 10 months, and that at two months a trend towards the reduction of rRNA expression occurs. Collectively, our results suggest that CR modulates age-related regulation of methylation at the rDNA locus, thus providing an epigenetic readout of the pro-longevity effects of CR.

Published

2020

22. Differentiation of amniotic epithelial cells into various liver cell types and potential therapeutic applications

Author

Stephen C. Strom, Maura Fanti, Mônica Campos Serra, Fabio Marongiu, Erika Cadoni, and Roberto Gramignoli

Subjects

0301 basic medicine, Pathology, medicine.medical_specialty, Cell Transplantation, Cellular differentiation, Clinical uses of mesenchymal stem cells, Biology, Regenerative Medicine, Regenerative medicine, 03 medical and health sciences, 0302 clinical medicine, medicine, Animals, Humans, Amnion, Liver Diseases, Liver cell, Mesenchymal stem cell, Obstetrics and Gynecology, Cell Differentiation, Epithelial Cells, Amniotic stem cells, 030104 developmental biology, Liver, Reproductive Medicine, Amniotic epithelial cells, Cancer research, Stem cell, 030217 neurology & neurosurgery, Developmental Biology

Abstract

The aim of Regenerative Medicine is to replace or regenerate human cells, tissues or organs in order to restore normal function. Among all organs, the liver is endowed with remarkable regenerative capacity. Nonetheless, there are conditions in which this ability is impaired, and the use of isolated cells, including stem cells, is being considered as a possible therapeutic tool for the management of chronic hepatic disease. Placenta holds great promise for the field of regenerative medicine. It has long been used for the treatment of skin lesions and in ophthalmology, due to its ability to modulate inflammation and promote healing. More recently, cells isolated from the amniotic membrane are being considered as a possible resource for tissue regeneration, including in the context liver disease. Two cell types can be easily isolated from human amnion: epithelial cells (hAEC) and mesenchymal stromal cells (hAMSC). However only the first cell population has been demonstrated to be a possible source of proficient hepatic cells. This review will summarize current knowledge on the differentiation of hAEC into liver cells and their potential therapeutic application.

Published

2017

23. Oleocanthal exerts antitumor effects on human liver and colon cancer cells through ROS generation

Author

Antonella Cusimano, Antonina Azzolina, Giuseppe Montalto, Maria Rita Emma, Caterina Di Sano, Giuseppa Augello, Roberto Gramignoli, Melchiorre Cervello, Daniele Balasus, James A. McCubrey, Stephen C. Strom, Cusimano, A., Balasus, D., Azzolina, A., Augello, G., Emma, M., Di Sano, C., Gramignoli, R., Strom, S., Mccubrey, J., Montalto, G., and Cervello, M.

Subjects

0301 basic medicine, Cancer Research, Carcinoma, Hepatocellular, Hepatocellular carcinoma, Oleocanthal, Extra-virgin olive oil, Cell, Apoptosis, Cyclopentane Monoterpenes, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Phenols, medicine, Humans, Cyclooxygenase Inhibitors, Viability assay, Olive Oil, Caspase, Cell Proliferation, Aldehydes, biology, Cell growth, Liver Neoplasms, Apoptosi, Hep G2 Cells, Cell cycle, digestive system diseases, Colorectal carcinoma, 030104 developmental biology, medicine.anatomical_structure, Oncology, chemistry, Cell culture, 030220 oncology & carcinogenesis, Immunology, biology.protein, Cancer research, Reactive oxygen specie, Colorectal Neoplasms, Reactive Oxygen Species, DNA Damage

Abstract

The beneficial health properties of the Mediterranean diet are well recognized. The principle source of fat in Mediterranean diet is extra-virgin olive oil (EVOO). Oleocanthal (OC) is a naturally occurring minor phenolic compound isolated from EVOO, which has shown a potent anti-inflammatory activity, by means of its ability to inhibit the cyclooxygenase (COX) enzymes COX-1 and COX-2. A large body of evidence indicates that phenols exhibit anticancer activities. The aim of the present study was to evaluate the potential anticancer effects of OC in hepatocellular carcinoma (HCC) and colorectal carcinoma (CRC) models. A panel of human HCC (HepG2, Huh7, Hep3B and PLC/PRF/5) and CRC (HT29, SW480) cell lines was used. Cells were treated with OC, and cell viability and apoptosis were evaluated. Compared with classical commercially available COX inhibitors (ibuprofen, indomethacin, nimesulide), OC was more effective in inducing cell growth inhibition in HCC and CRC cells. Moreover, OC inhibited colony for mation and i nduced ap optosis, as confirmed by PARP cleavage, activation of caspases 3/7 and chromatin condensation. OC treatment in a dose dependent-manner induced expression of γH2AX, a marker of DNA damage, increased intracellular ROS production and caused mitochondrial depolarization. Moreover, the effects of OC were suppressed by the ROS scavenger N-acetyl-L-cysteine. Finally, OC was not toxic in primary normal human hepatocytes. In conclusion, OC treatment was found to exert a potent anticancer activity against HCC and CRC cells. Taken together, our findings provide preclinical support of the chemotherapeutic potential of EVOO against cancer.

Published

2017

24. Host conditioning and rejection monitoring in hepatocyte transplantation in humans

Author

Kyle Soltys, Kimberly Haberman, Chethan Ashokkumar, Jason V. Fong, Rachel Sada, George V. Mazariegos, Alexandra Dreyzin, Veysel Tahan, Sarangarajan Ranganathan, Donna B. Stolz, Ken Fukumitsu, Rakesh Sindhi, Chandan Guha, Kevin M. Baskin, Steven F. Dobrowolski, Rajavel Elango, Benjamin L. Shneider, Miguel Reyes-Múgica, Mubina Quader, John J. Crowley, Edgar N. Tafaleng, Kenneth Dorko, Roberto Gramignoli, Stephen C. Strom, Alejandro Soto Gutiérrez, Masaki Nagaya, Robert H. Squires, Jeffrey L. Platt, Ira J. Fox, Gerard Vockley, Taichiro Nishikawa, Marilia Cascalho, Jayanta Roy-Chowdhury, Melvin Deutsch, and Kentaro Setoyama

Subjects

Adult, Graft Rejection, Male, 0301 basic medicine, Pathology, medicine.medical_specialty, Transplantation Conditioning, Urea cycle disorder, Swine, medicine.medical_treatment, T cell, Transplantation, Heterologous, Human leukocyte antigen, Biology, Article, 03 medical and health sciences, 0302 clinical medicine, medicine, Animals, Humans, CD154, Hepatology, Liver Diseases, Immunosuppression, medicine.disease, Radiation therapy, Macaca fascicularis, surgical procedures, operative, 030104 developmental biology, medicine.anatomical_structure, Liver, Hepatocyte, Urea cycle, Immunology, Hepatocytes, Female, 030211 gastroenterology & hepatology

Abstract

Background & Aims Hepatocyte transplantation partially corrects genetic disorders and has been associated anecdotally with reversal of acute liver failure. Monitoring for graft function and rejection has been difficult, and has contributed to limited graft survival. Here we aimed to use preparative liver-directed radiation therapy, and continuous monitoring for possible rejection in an attempt to overcome these limitations. Methods Preparative hepatic irradiation was examined in non-human primates as a strategy to improve engraftment of donor hepatocytes, and was then applied in human subjects. T cell immune monitoring was also examined in human subjects to assess adequacy of immunosuppression. Results Porcine hepatocyte transplants engrafted and expanded to comprise up to 15% of irradiated segments in immunosuppressed monkeys preconditioned with 10Gy liver-directed irradiation. Two patients with urea cycle deficiencies had early graft loss following hepatocyte transplantation; retrospective immune monitoring suggested the need for additional immunosuppression. Preparative radiation, anti-lymphocyte induction, and frequent immune monitoring were instituted for hepatocyte transplantation in a 27year old female with classical phenylketonuria. Post-transplant liver biopsies demonstrated multiple small clusters of transplanted cells, multiple mitoses, and Ki67 + hepatocytes. Mean peripheral blood phenylalanine (PHE) level fell from pre-transplant levels of 1343±48μM (normal 30–119μM) to 854±25μM (treatment goal ≤360μM) after transplant (36% decrease; p Conclusions Radiation preconditioning and serial rejection risk assessment may produce better engraftment and long-term survival of transplanted hepatocytes. Hepatocyte xenografts engraft for a period of months in non-human primates and may provide effective therapy for patients with acute liver failure. Lay summary Hepatocyte transplantation can potentially be used to treat genetic liver disorders but its application in clinical practice has been impeded by inefficient hepatocyte engraftment and the inability to monitor rejection of transplanted liver cells. In this study, we first show in non-human primates that pretreatment of the host liver with radiation improves the engraftment of transplanted liver cells. We then used this knowledge in a series of clinical hepatocyte transplants in patients with genetic liver disorders to show that radiation pretreatment and rejection risk monitoring are safe and, if optimized, could improve engraftment and long-term survival of transplanted hepatocytes in patients.

Published

2017

25. Guide to the Assessment of Mature Liver Gene Expression in Stem Cell-Derived Hepatocytes

Author

Mihaela, Zabulica, Raghuraman C, Srinivasan, Massoud, Vosough, Christina, Hammarstedt, Tingting, Wu, Roberto, Gramignoli, Ewa, Ellis, Kristina, Kannisto, Alexandra, Collin de l'Hortet, Kazuki, Takeishi, Alejandro, Soto-Gutierrez, and Stephen C, Strom

Subjects

mature liver gene expression, Gene Expression Regulation, Liver, Original Research Reports, induced pluripotent stem cells, Gene Expression Profiling, hepatic differentiation, stem cell-derived hepatocytes, fetal liver gene expression, Hepatocytes, Humans, Cell Differentiation

Abstract

Differentiation of stem cells to hepatocyte-like cells (HLCs) holds great promise for basic research, drug and toxicological investigations, and clinical applications. There are currently no protocols for the production of HLCs from stem cells, such as embryonic stem cells or induced pluripotent stem cells, that produce fully mature hepatocytes with a wide range of mature hepatic functions. This report describes a standard method to assess the maturation of stem cell-derived HLCs with a moderately high-throughput format, by analysing liver gene expression by quantitative RT-qPCR. This method also provides a robust data set of the expression of 62 genes expressed in normal liver, generated from 17 fetal and 25 mature human livers, so that investigators can quickly and easily compare the expression of these genes in their stem cell-derived HLCs with the values obtained in authentic fetal and mature human liver. The simple methods described in this study will provide a quick and accurate assessment of the efficacy of a differentiation protocol and will help guide the optimization of differentiation conditions.

Published

2019

26. A liver-humanized mouse model of carbamoyl phosphate synthetase 1-deficiency

Author

Gabriella Allegri, Ahmad Karadagi, Jean-Marc Nuoffer, Raghuraman C. Srinivasan, Christina Hammarstedt, Ewa Ellis, Kristina Kannisto, Roberto Gramignoli, Johannes Häberle, Beat Thöny, Mihaela Zabulica, Tingting Wu, Ralph Fingerhut, Stephen C. Strom, Véronique Rüfenacht, University of Zurich, and Strom, Stephen C

Subjects

Male, 2716 Genetics (clinical), Carbamoyl-Phosphate Synthase I Deficiency Disease, Hydrolases, Mutant, Carbamoyl-Phosphate Synthase (Ammonia), Mice, Transgenic, 610 Medicine & health, medicine.disease_cause, Mice, 1311 Genetics, In vivo, medicine, Genetics, Animals, Humans, Genetics(clinical), Child, Gene, Cells, Cultured, Genetics (clinical), Mutation, Chemistry, Infant, Newborn, Infant, Metabolism, Middle Aged, Carbamoyl phosphate synthetase, Cell biology, Glutamine, Disease Models, Animal, Liver, Organ Specificity, 10036 Medical Clinic, Humanized mouse, Hepatocytes, Female

Abstract

A liver-humanized mouse model for CPS1-deficiency was generated by the high-level repopulation of the mouse liver with CPS1-deficient human hepatocytes. When compared with mice that are highly repopulated with CPS1-proficient human hepatocytes, mice that are repopulated with CPS1-deficient human hepatocytes exhibited characteristic symptoms of human CPS1 deficiency including an 80% reduction in CPS1 metabolic activity, delayed clearance of an ammonium chloride infusion, elevated glutamine and glutamate levels, and impaired metabolism of [15 N]ammonium chloride into urea, with no other obvious phenotypic differences. Because most metabolic liver diseases result from mutations that alter critical pathways in hepatocytes, a model that incorporates actual disease-affected, mutant human hepatocytes is useful for the investigation of the molecular, biochemical, and phenotypic differences induced by that mutation. The model is also expected to be useful for investigations of modified RNA, gene, and cellular and small molecule therapies for CPS1-deficiency. Liver-humanized models for this and other monogenic liver diseases afford the ability to assess the therapy on actual disease-affected human hepatocytes, in vivo, for long periods of time and will provide data that are highly relevant for investigations of the safety and efficacy of gene-editing technologies directed to human hepatocytes and the translation of gene-editing technology to the clinic.

Published

2019

27. Cell Therapy of Liver Disease

Author

Stephen C. Strom and Carl Jorns

Published

2019

28. Human amnion epithelial cells expressing HLA-G as novel cell-based treatment for liver disease

Author

Roberto Gramignoli and Stephen C. Strom

Subjects

0301 basic medicine, medicine.medical_treatment, Immunology, Cell- and Tissue-Based Therapy, Liver transplantation, Biology, Regenerative medicine, Cell therapy, 03 medical and health sciences, Immune Tolerance, medicine, Humans, Immunology and Allergy, Amnion, Induced pluripotent stem cell, HLA-G Antigens, Clinical Trials as Topic, Liver Diseases, Epithelial Cells, General Medicine, Liver regeneration, Liver Regeneration, Liver Transplantation, Adult Stem Cells, 030104 developmental biology, Liver, Amniotic epithelial cells, Hepatocytes, Female, Stem cell, Adult stem cell

Abstract

Despite routine liver transplantation and supporting medical therapies, thousands of patients currently wait for an organ and there is an unmet need for more refined and widely available regenerative strategies to treat liver diseases. Cell transplants attempt to maximize the potential for repair and/or regeneration in liver and other organs. Over 40years of laboratory pre-clinical research and 25years of clinical procedures have shown that certain liver diseases can be treated by the infusion of isolated cells (hepatocyte transplant). However, like organ transplants, hepatocyte transplant suffers from a paucity of tissues useful for cell production. Alternative sources have been investigated, yet with limited success. The tumorigenic potential of pluripotent stem cells together with their primitive level of hepatic differentiation, have limited the use of stem cell populations. Stem cell sources from human placenta, and the amnion tissue in particular are receiving renewed interest in the field of regenerative medicine. Unlike pluripotent stem cells, human amnion epithelial (AE) cells are easily available without ethical or religious concerns; they do not express telomerase and are not immortal or tumorigenic when transplanted. In addition, AE cells have been reported to express genes normally expressed in mature liver, when transplanted into the liver. Moreover, because of the possibility of an immune-privileged status related to their expression of HLA-G, it might be possible to transplant human AE cells without immunosuppression of the recipient.

Published

2016

29. Role of Chromatin Structural Changes in Regulating Human CYP3A Ontogeny

Author

Nicholas Giebel, Ronald N. Hines, Roberto Gramignoli, Ke Yan, Pippa Simpson, Kenneth Dorko, Stephen C. Strom, Jeffrey D Shadley, and D. Gail McCarver

Subjects

Adult, 0301 basic medicine, Histone-modifying enzymes, Transcription, Genetic, Protein Conformation, Pharmaceutical Science, Gestational Age, Gene Expression Regulation, Enzymologic, Chromatin remodeling, Special Section on Pediatric Drug Disposition and Pharmacokinetics, Histones, Structure-Activity Relationship, 03 medical and health sciences, 0302 clinical medicine, Cytochrome P-450 CYP3A, Humans, Child, Promoter Regions, Genetic, ChIA-PET, Aged, Aged, 80 and over, Pharmacology, Genetics, Regulation of gene expression, Binding Sites, biology, Age Factors, Gene Expression Regulation, Developmental, Infant, Middle Aged, Chromatin Assembly and Disassembly, Chromatin, 030104 developmental biology, Histone, Liver, Child, Preschool, Hepatocytes, biology.protein, Nucleic Acid Conformation, Chromatin immunoprecipitation, 030217 neurology & neurosurgery, Bivalent chromatin

Abstract

Variability in drug-metabolizing enzyme developmental trajectories contributes to interindividual differences in susceptibility to chemical toxicity and adverse drug reactions, particularly in the first years of life. Factors linked to these interindividual differences are largely unknown, but molecular mechanisms regulating ontogeny are likely involved. To evaluate chromatin structure dynamics as a likely contributing mechanism, age-dependent changes in modified and variant histone occupancy were evaluated within known CYP3A4 and 3A7 regulatory domains. Chromatin immunoprecipitation using fetal or postnatal human hepatocyte chromatin pools followed by quantitative polymerase chain reaction DNA amplification was used to determine relative chromatin occupancy by modified and variant histones. Chromatin structure representing a poised transcriptional state (bivalent chromatin), indicated by the occupancy by modified histones associated with both active and repressed transcription, was observed for CYP3A4 and most 3A7 regulatory regions in both postnatal and fetal livers. However, the CYP3A4 regulatory regions had significantly greater occupancy by modified histones associated with repressed transcription in the fetal liver. Conversely, some modified histones associated with active transcription exhibited greater occupancy in the postnatal liver. CYP3A7 regulatory regions also had significantly greater occupancy by modified histones associated with repressed transcription in the fetus. The observed occupancy by modified histones is consistent with chromatin structural dynamics contributing to CYP3A4 ontogeny, although the data are less conclusive regarding CYP3A7. Interpretation of the latter data may be confounded by cell-type heterogeneity in the fetal liver.

Published

2016

30. Ectonucleotidase Expression on Human Amnion Epithelial Cells: Adenosinergic Pathways and Dichotomic Effects on Immune Effector Cell Populations

Author

Alberto L. Horenstein, Roberto Gramignoli, Fabio Malavasi, Valeria Quarona, Angelo Corso Faini, Barbara Castella, Fabio Morandi, Raghuraman C. Srinivasan, and Stephen C. Strom

Subjects

Adenosine, Receptor, Adenosine A2A, Adenosine Deaminase, T cell, T-Lymphocytes, Immunology, Context (language use), CD38, Biology, Lymphocyte Activation, 03 medical and health sciences, 0302 clinical medicine, Mediator, medicine, Immunology and Allergy, Humans, Ectonucleotidase, Amnion, Receptor, Cells, Cultured, Cell Proliferation, B-Lymphocytes, Cell growth, Receptor, Adenosine A1, Purinergic receptor, Epithelial Cells, Cell biology, Killer Cells, Natural, medicine.anatomical_structure, cardiovascular system, Metabolic Networks and Pathways, 030215 immunology

Abstract

This study investigates the mechanism(s) underlying the immunoregulatory activities of placenta-derived human amnion epithelial cells (hAEC). The working hypothesis is that NAD+ and ATP, along with ectoenzymes involved in their metabolism, play a significant role in hAEC-mediated immune regulation. Proof of principle of the hypothesis was obtained by analyzing the interactions between hAEC and the main human leukocyte populations. The results obtained indicate that hAEC constitutively express a unique combination of functional ectoenzymes, driving the production of adenosine (ADO) via canonical (CD39, CD73) and alternative (CD38, CD203a/PC-1, CD73) pathways. Further, the picture is completed by the observation that hAEC express A1, A2a, and A2b ADO receptors as well as ADO deaminase, the enzyme involved in ADO catabolism. The contribution of the purinergic mediator to immunomodulation was confirmed by exposing in vitro different immune effector cells to the action of primary hAECs. B cells showed an enhanced proliferation and diminished spontaneous apoptosis when in contact with hAEC. T cell proliferation was partially inhibited by hAEC through ADO production, as confirmed by using specific ectoenzyme inhibitors. Further, hAEC induced an expansion of both T and B regulatory cells. Last, hAEC inhibited NK cell proliferation. However, the involvement of ADO-producing ectoenzymes is less apparent in this context. In conclusion, hAEC exert different in vitro immunoregulatory effects, per se, as a result of interactions with different populations of immune effector cells. These results support the view that hAEC are instrumental for regenerative medicine as well as in therapeutic applications for immune-related diseases.

Published

2018

31. Contributors

Author

Rachit Agarwal, Jon D. Ahlstrom, Rafiq Ahmad, Emilio I. Alarcon, Alejandro J. Almarza, Graça Almeida-Porada, Manuel Almeida, Melissa Alvarado-Velez, James M. Anderson, Judith Arcidiacono, Anthony Atala, Stephen F. Badylak, Wayne Balkan, Brian G. Ballios, Pedro M. Baptista, M. Douglas Baumann, Supinder S. Bedi, Ravi V. Bellamkonda, Nicole M. Bergmann, Helen M. Blau, Joel D. Boerckel, Andres M. Bratt-Leal, James C. Brown, Scott Brubaker, Isabelle Brunette, Gisele A. Calderon, Arnold I. Caplan, David G. Castner, Cynthia Chang, Aditya Chawla, Xuguang Chen, Paul Cohen, Michael J. Cooke, Joshua S. Copus, Vitor M. Correlo, Charles S. Cox, Abritee Dahl, Richard M. Day, Paolo De Coppi, Mahesh C. Dodla, Jennifer H. Elisseeff, Juliet A. Emamaullee, Adam Esa, Yunlan Fang, Heather J. Faust, John P. Fisher, Matthew B. Fisher, Elvis L. Francois, Andrés J. García, Svetlana Gavrilov, Dan Gazit, Zulma Gazit, Christopher V. Gemmiti, Gregory J. Gillispie, Sarah E. Gilpin, W.T. Godbey, Andrea Gray, Ronald M. Green, May Griffith, Robert E. Guldberg, Qiongyu Guo, Geoffrey C. Gurtner, Michael C. Hacker, Issa A. Hanna, Joshua M. Hare, Konstantinos E. Hatzistergos, Ralf-Peter Herber, Jöns Hilborn, H. David Humes, Joshua G. Hunsberger, Kenjiro Iwasa, John D. Jackson, Margaret L. Jackson, Hae Lin Jang, John A. Jansen, Josephine Johnston, Carl Jorns, Huijun Kang, David L. Kaplan, David S. Kaplan, Adam J. Katz, Matthew W. Kelley, Kelsey Kennedy, Ali Khademhosseini, Gilson Khang, Jinho Kim, Rachel H. Klein, Irina Klimanskaya, Paul S. Knoepfler, In Kap Ko, Yash M. Kolambkar, Jan Krieghoff, Nathan W. Kucko, Manoj Kumar, Joanne Kurtzberg, Anna Kwilas, Donald W. Landry, Mark T. Langhans, Robert Lanza, Giacomo Lanzoni, Sang Jin Lee, Sander C.G. Leeuwenburgh, Kam W. Leong, Rui Liang, Volha Liaudanskaya, Hang Lin, Michael T. Longaker, Hermann P. Lorenz, Jeanne F. Loring, Shi-Jiang Lu, Alberto Lue, Peter X. Ma, Renata S. Magalhaes, Serena Mandla, Clement D. Marshall, Manuela Martins-Green, Devon E. Mason, Jonquil R. Mau, Richard McFarland, Melissa K. McHale, James C. Melville, Jason R. Meyers, Antonios G. Mikos, Jordan S. Miller, Paul A. Mittermiller, Hideki Miyachi, Shinka Miyamoto, Nelson Monteiro, Alessandra L. Moore, Sara Morini, Philipp T. Moser, Vivek J. Mukhatyar, Mark Murdock, Aaron Nagiel, Gail K. Naughton, Allison Nauta, Javier Navarro, Jared M. Newton, Aparna Nori, Teruo Okano, Joaquim M. Oliveira, Harald C. Ott, Jagannath Padmanabhan, Kristin M. Page, Anil Kumar Pallickaveedu Rajan Asari, Virginia E. Papaioannou, Jihoon Park, Samantha L. Payne, Gadi Pelled, Andrew Pepper, Elumalai Perumal, Melissa Petreaca, Christopher J. Pino, Alessandro Pirosa, Iris Pla-Palacín, Marta Pokrywczynska, Christopher D. Porada, Blaise D. Porter, Milica Radisic, Kunal J. Rambhia, F. Raquel Maia, Buddy D. Ratner, A.H. Reddi, Rui L. Reis, Laura Ricles, Camillo Ricordi, Muhammad Rizwan, Rebecca Robinson, Melanie Rodrigues, Benjamin B. Rothrauff, Hooman Sadri-Ardekani, Pilar Sainz-Arnal, Rangarajan Sambathkumar, Natalia Sánchez-Romero, Michelle Scarritt, Christopher M. Schneider, Steven D. Schwartz, Sarah Selem, Trinidad Serrano-Aulló, A.M. James Shapiro, Dmitriy Sheyn, Tatsuya Shimizu, Toshiharu Shinoka, Molly S. Shoichet, Toshihiro Shoji, Thomas Shupe, Andrew G. Sikora, Fiona Simpson, Aleksander Skardal, Daniel Skuk, Brandon T. Smith, Jihee Sohn, Shay Soker, Estela Solanas, Jeong Eun Song, Disha Sood, David L. Stocum, Stephen C. Strom, Jessica M. Sun, Hironobu Takahashi, Jacques P. Tremblay, Nirmalya Tripathy, John W. Tse, Rocky S. Tuan, Catherine M. Verfaillie, Gordana Vunjak-Novakovic, William R. Wagner, Yanling Wang, Emma Watson, Jennifer L. West, David F. Williams, James K. Williams, Mark E. Wong, Savio L-Y. Woo, Fiona M. Wood, Lei Xu, Doron C. Yakubovich, Yafeng Yang, Michael J. Yaszemski, Pamela C. Yelick, Evelyn K.F. Yim, Carolyn Yong, James J. Yoo, Simon Young, Nora Yucel, Rachel L. Zacharias, Yuanyuan Zhang, Ai Zhang, Jin Zhang, and Yang Zhu

Published

2018

32. Molecular Aging of Human Liver: An Epigenetic/Transcriptomic Signature

Author

Cristina Giuliani, Maria Giulia Bacalini, Elena Marasco, Xiaoyuan Zhou, Roberto Gramignoli, Francesco Ravaioli, Noémie Gensous, Anna Maria Di Blasio, Daniel Remondini, Christine Nardini, Gastone Castellani, Ewa Ellis, Chiara Pirazzini, Gian Luca Grazi, Stephen C. Strom, Paolo Garagnani, Matteo Cescon, Davide Gentilini, Miriam Capri, Claudio Franceschi, Bacalini, Maria Giulia, Franceschi, Claudio, Gentilini, Davide, Ravaioli, Francesco, Zhou, Xiaoyuan, Remondini, Daniel, Pirazzini, Chiara, Giuliani, Cristina, Marasco, Elena, Gensous, Noémie, Di Blasio, Anna Maria, Ellis, Ewa, Gramignoli, Roberto, Castellani, Gastone, Capri, Miriam, Strom, Stephen, Nardini, Christine, Cescon, Matteo, Grazi, Gian Luca, and Garagnani, Paolo

Subjects

Adult, Male, 0301 basic medicine, Aging, Adolescent, Epigenetic clock, Liver cytology, Biopsy, medicine.medical_treatment, Computational biology, Liver transplantation, NO, Epigenesis, Genetic, Transcriptome, Young Adult, 03 medical and health sciences, medicine, Epigenetic Profile, LS2_8, Humans, Epigenetics, LS7_4, Aged, Aged, 80 and over, DNA methylation, business.industry, DNA methylation, Epigenetic clock, Epithelial-mesenchymal transition, Methylation, Middle Aged, Epithelial-mesenchymal transition, Tissue Donors, Liver Transplantation, 030104 developmental biology, Liver, CpG site, RNA, Female, Geriatrics and Gerontology, business

Abstract

The feasibility of liver transplantation from old healthy donors suggests that this organ is able to preserve its functionality during aging. To explore the biological basis of this phenomenon, we characterized the epigenetic profile of liver biopsies collected from 45 healthy liver donors ranging from 13 to 90 years old using the Infinium HumanMethylation450 BeadChip. The analysis indicates that a large remodeling in DNA methylation patterns occurs, with 8,823 age-associated differentially methylated CpG probes. Notably, these age-associated changes tended to level off after the age of 60, as confirmed by Horvath's clock. Using stringent selection criteria, we further identified a DNA methylation signature of aging liver including 75 genomic regions. We demonstrated that this signature is specific for liver compared to other tissues and that it is able to detect biological age-acceleration effects associated with obesity. Finally, we combined DNA methylation measurements with available expression data. Although the intersection between the two omic characterizations was low, both approaches suggested a previously unappreciated role of epithelial-mesenchymal transition and Wnt-signaling pathways in the aging of human liver.

Published

2018

33. Current status of hepatocyte xenotransplantation

Author

Stephen C. Strom, Raphael P. H. Meier, Philippe Morel, Leo Buhler, Henk-Jan Schuurman, and Nalu Navarro-Alvarez

Subjects

Swine, medicine.medical_treatment, Xenotransplantation, Transplantation, Heterologous, Porcine hepatocytes, Alcoholic hepatitis, Liver transplantation, medicine, Animals, Humans, Immunosuppression Therapy, Innate immunity, Physiologic species incompatibilities, Innate immune system, ddc:617, biology, business.industry, Immunosuppression, General Medicine, Liver Failure, Acute, medicine.disease, Immunity, Innate, Liver Transplantation, Clinical trial, medicine.anatomical_structure, Hepatocyte, Immunology, Hepatocytes, biology.protein, Animal models of liver failure, Surgery, Cell transplantation, Antibody, business, Acute liver failure

Abstract

The treatment of acute liver failure, a condition with high mortality, comprises optimal clinical care, and in severe cases liver transplantation. However, there are limitations in availability of organ donors. Hepatocyte transplantation is a promising alternative that could fill the medical need, in particular as the bridge to liver transplantation. Encapsulated porcine hepatocytes represent an unlimited source that could function as a bioreactor requiring minimal immunosuppression. Besides patients with acute liver failure, patients with alcoholic hepatitis who are unresponsive to a short course of corticosteroids are a target for hepatocyte transplantation. In this review we present an overview of the innate immune barriers in hepatocyte xenotransplantation, including the role of complement and natural antibodies; the role of phagocytic cells and ligands like CD47 in the regulation of phagocytic cells; and the role of Natural Killer cells. We present also some illustrations of physiological species incompatibilities in hepatocyte xenotransplantation, such as incompatibilities in the coagulation system. An overview of the methodology for cell microencapsulation is presented, followed by proof-of-concept studies in rodent and nonhuman primate models of fulminant liver failure: these studies document the efficacy of microencapsulated porcine hepatocytes which warrants progress towards clinical application. Lastly, we present an outline of a provisional clinical trial, that upon completion of preclinical work could start within the upcoming 2-3 years.

Published

2015

34. Amelioration of Hyperbilirubinemia in Gunn Rats after Transplantation of Human Induced Pluripotent Stem Cell-Derived Hepatocytes

Author

Yong Chen, Jayanta Roy-Chowdhury, Xia Wang, Tatyana Tchaikovskaya, Chan Jung Chang, Sanal Madhusudana Girija, Yanfeng Li, Bing Han, Stephen C. Strom, Eric E. Bouhassira, Krisztina Tar, Namita Roy-Chowdhury, Chandan Guha, Edgar N. Tafaleng, Wei Zhang, Yesim Avsar, Zsuzsanna Polgar, Vanessa Sauer, and Ira J. Fox

Subjects

medicine.medical_specialty, Glucuronosyltransferase, Crigler–Najjar syndrome, Bilirubin, Induced Pluripotent Stem Cells, Rats, Gunn, Cell- and Tissue-Based Therapy, Human skin, Biology, Biochemistry, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Report, Internal medicine, Genetics, medicine, Animals, Humans, Induced pluripotent stem cell, lcsh:QH301-705.5, Crigler-Najjar Syndrome, Hyperbilirubinemia, 030304 developmental biology, lcsh:R5-920, 0303 health sciences, Cell Biology, medicine.disease, Rats, 3. Good health, Transplantation, Endocrinology, lcsh:Biology (General), Liver, Liver Lobe, chemistry, Hepatocytes, biology.protein, 030211 gastroenterology & hepatology, Hepatocyte growth factor, lcsh:Medicine (General), Developmental Biology, medicine.drug

Abstract

Summary Hepatocyte transplantation has the potential to cure inherited liver diseases, but its application is impeded by a scarcity of donor livers. Therefore, we explored whether transplantation of hepatocyte-like cells (iHeps) differentiated from human induced pluripotent stem cells (iPSCs) could ameliorate inherited liver diseases. iPSCs reprogrammed from human skin fibroblasts were differentiated to iHeps, which were transplanted into livers of uridinediphosphoglucuronate glucuronosyltransferase-1 (UGT1A1)-deficient Gunn rats, a model of Crigler-Najjar syndrome 1 (CN1), where elevated unconjugated bilirubin causes brain injury and death. To promote iHep proliferation, 30% of the recipient liver was X-irradiated before transplantation, and hepatocyte growth factor was expressed. After transplantation, UGT1A1+ iHep clusters constituted 2.5%–7.5% of the preconditioned liver lobe. A decline of serum bilirubin by 30%–60% and biliary excretion of bilirubin glucuronides indicated that transplanted iHeps expressed UGT1A1 activity, a postnatal function of hepatocytes. Therefore, iHeps warrant further exploration as a renewable source of hepatocytes for treating inherited liver diseases., Highlights • Human skin fibroblast-derived iPSCs were differentiated to hepatocyte-like iHeps • iHeps were transplanted into Gunn rats, a model of Crigler-Najjar syndrome 1 • Engraftment of the iHeps in Gunn rat livers reduced serum bilirubin levels • iHeps may be potentially useful in treating liver-based metabolic disorders, Roy-Chowdhury and colleagues show that human iPSCs differentiated to hepatocyte-like iHep cells engraft into the liver of UGT1A1-deficient Gunn rats, a model of Crigler-Najjar syndrome 1, where hyperbilirubinemia causes brain injury and death. After iHep transplantation, serum bilirubin declined by 30%–60% and bilirubin glucuronides appeared in bile, indicating that the engrafted iHeps expressed UGT1A1, a postnatal hepatocyte function.

Published

2015

35. Rat-Derived Amniotic Epithelial Cells Differentiate into Mature Hepatocytes In Vivo with No Evidence of Cell Fusion

Author

Antonella Contini, Ezio Laconi, Fabio Marongiu, Stephen C. Strom, Maria Paola Serra, Marcella Sini, and Michela Marongiu

Subjects

Liver cytology, Biology, Dipeptidyl peptidase, Green fluorescent protein, Original Research Reports, Pregnancy, Placenta, medicine, Animals, Humans, Amnion, Cell fusion, Stem Cells, Cell Differentiation, Epithelial Cells, Cell Biology, Hematology, Molecular biology, Rats, Transplantation, medicine.anatomical_structure, Liver, Amniotic epithelial cells, Hepatocyte, Immunology, Hepatocytes, Female, Stem Cell Transplantation, Developmental Biology

Abstract

Amniotic epithelial cells (AEC) derived from human placenta represent a useful and noncontroversial source for liver-based regenerative medicine. Previous studies suggested that human- and rat-derived AEC differentiate into hepatocyte-like cells upon transplantation. In the retrorsine (RS) model of liver repopulation, clusters of donor-derived cells engrafted in the recipient liver and, importantly, showed characteristics of mature hepatocytes. The aim of the current study was to investigate the possible involvement of cell fusion in the emergence of hepatocyte clusters displaying a donor-specific phenotype. To this end, 4-week-old GFP(+)/DPP-IV(-) rats were treated with RS and then transplanted with undifferentiated AEC isolated from the placenta of DPP-IV(+) pregnant rats at 16-19 days of gestational age. Results indicated that clusters of donor-derived cells were dipeptidyl peptidase type IV (DPP-IV) positive, but did not express the green fluorescent protein (GFP), suggesting that rat amniotic epithelial cells (rAEC) did not fuse within the host parenchyma, as no colocalization of the two tags was observed. Moreover, rAEC-derived clusters expressed markers of mature hepatocytes (eg, albumin, cytochrome P450), but were negative for the expression of biliary/progenitor markers (eg, epithelial cell adhesion molecule [EpCAM]) and did not express the marker of preneoplastic hepatic nodules glutathione S-transferase P (GST-P). These results extend our previous findings on the potential of AEC to differentiate into mature hepatocytes and suggest that this process can occur in the absence of cell fusion with host-derived cells. These studies support the hypothesis that amnion-derived epithelial cells can be an effective cell source for the correction of liver disease.

Published

2015

36. Clinical Hepatocyte Transplantation: Practical Limits and Possible Solutions

Author

Stephen C. Strom, Raghuraman C. Srinivasan, Massoud Vosough, Roberto Gramignoli, and Kristina Kannisto

Subjects

Immunosuppression Therapy, medicine.medical_specialty, Liver Diseases, medicine.medical_treatment, Preservation, Biological, Clinical grade, Immunosuppression, Cell Separation, Biology, medicine.disease, Regenerative medicine, Transplantation, Human hepatocyte, Liver disease, Hepatocyte transplantation, Liver, Immunology, Hepatocytes, medicine, Cell separation, Humans, Surgery, Intensive care medicine

Abstract

Since the first human hepatocyte transplants (HTx) in 1992, clinical studies have clearly established proof of principle for this therapy as a treatment for patients with acquired or inherited liver disease. Although major accomplishments have been made, there are still some specific limitations to this technology, which, if overcome, could greatly enhance the efficacy and implementation of this therapy. Here, we describe what in our view are the most significant obstacles to the clinical application of HTx and review the solutions currently proposed. The obstacles of significance include the limited number and quality of liver tissues as a cell source, the lack of clinical grade reagents, quality control evaluation of hepatocytes prior to transplantation, hypothermic storage of cells prior to transplantation, preconditioning treatments to enhance engraftment and proliferation of donor cells, tracking or monitoring cells after transplantation, and the optimal immunosuppression protocols for transplant recipients.

Published

2015

37. Exogenous alpha 1-antitrypsin down-regulates SERPINA1 expression

Author

Greg Nowak, Helen Zemack, Ahmad Karadagi, Sabina Janciauskiene, Kristina Kannisto, Ewa Ellis, Sandeep Salipalli, Bo-Göran Ericzon, Stephen C. Strom, Knut Stokkeland, Lisa-Mari Mörk, Danny Jonigk, Carl Jorns, Helene Johansson, and Roberto Gramignoli

Subjects

0301 basic medicine, Male, Lipopolysaccharide, Pulmonology, lcsh:Medicine, Gene Expression, Endogeny, Biochemistry, chemistry.chemical_compound, 0302 clinical medicine, Animal Cells, Blood plasma, Gene expression, Medicine and Health Sciences, Public and Occupational Health, lcsh:Science, Cells, Cultured, Multidisciplinary, Protease Inhibitor Therapy, biology, Liver Diseases, Oncostatin M, Acute-phase protein, Middle Aged, Complementary DNA, Vaccination and Immunization, Immunohistochemistry, Nucleic acids, Liver, 030220 oncology & carcinogenesis, Child, Preschool, Female, Cellular Types, Anatomy, Research Article, Adult, medicine.medical_specialty, Adolescent, Forms of DNA, Chronic Obstructive Pulmonary Disease, Immunology, Antiretroviral Therapy, Down-Regulation, Surgical and Invasive Medical Procedures, Gastroenterology and Hepatology, Peripheral blood mononuclear cell, Polymorphism, Single Nucleotide, 03 medical and health sciences, Digestive System Procedures, Young Adult, Antiviral Therapy, Internal medicine, medicine, Genetics, Humans, RNA, Messenger, Emphysema, Transplantation, business.industry, lcsh:R, Biology and Life Sciences, Proteins, Acute Phase Proteins, Cell Biology, Organ Transplantation, DNA, Liver Transplantation, 030104 developmental biology, Endocrinology, chemistry, alpha 1-Antitrypsin, biology.protein, Hepatocytes, lcsh:Q, Preventive Medicine, business

Abstract

The main goal of the therapy with purified human plasma alpha1-antitrypsin (A1AT) is to increase A1AT levels and to prevent lungs from elastolytic activity in patients with PiZZ (Glu342Lys) A1AT deficiency-related emphysema. Potential hepatic gains of this therapy are unknown. Herein, we investigated the effect of A1AT therapy on SERPINA1 (gene encoding A1AT) expression. The expression of SERPINA1 was determined in A1AT or A1AT plus Oncostatin M (OSM) treated primary human hepatocytes isolated from liver tissues from A1AT deficient patients and control liver tissues. In addition, SERPINA1 mRNA was assessed in lung tissues from PiZZ emphysema patients with and without A1AT therapy, and in adherent human peripheral blood mononuclear cells (PBMC) isolated from healthy PiMM donors. In a dose-dependent manner purified A1AT lowered SERPINA1 expression in hepatocytes. This latter effect was more prominent in hepatocytes stimulated with OSM. Although it did not reach statistical significance (P = 0.0539)-analysis of lung tissues showed lower SERPINA1 expression in PiZZ emphysema patients receiving augmentation therapy relative to those without therapy. Finally, exogenously added purified A1AT (1mg/ml) reduced SERPINA1 expression in naive as well as in lipopolysaccharide (LPS)-stimulated human adherent PBMCs. Exogenous A1AT protein reduces its own endogenous expression. Hence, augmentation with native M-A1AT protein and a parallel reduction in expression of dysfunctional mutant Z-A1AT may be beneficial for PiZZ liver, and this motivates further studies.

Published

2017

38. Hypothermic Storage of Human Hepatocytes for Transplantation

Author

Kristen J. Skvorak, Ewa Ellis, Veysel Tahan, Bo-Göran Ericzon, Kenneth Dorko, Carl Jorns, Ira J. Fox, Stephen C. Strom, and Roberto Gramignoli

Subjects

Adult, Male, medicine.medical_specialty, Adenosine, Adolescent, Orthotopic liver transplantation, Cell Survival, Allopurinol, Organ Preservation Solutions, Biomedical Engineering, lcsh:Medicine, Cold storage, Biology, Bridge (interpersonal), Young Adult, Raffinose, Cytochrome P-450 Enzyme System, Ammonia, medicine, Humans, Insulin, Child, Cells, Cultured, Aged, Caspase 7, Cryopreservation, Transplantation, Caspase 3, lcsh:R, Liver failure, Infant, Cell Biology, Middle Aged, Glutathione, Surgery, Cold Temperature, Child, Preschool, Hepatocytes, Female

Abstract

Transplantation of human hepatocytes is gaining recognition as a bridge or an alternative to orthotopic liver transplantation for patients with acute liver failure and genetic defects. Since most patients require multiple cell infusions over an extended period of time, we investigated hepatic functions in cells maintained in University of Wisconsin solution at 4°C up to 72 h. Eleven different assessments of hepatic viability and function were investigated both pre- and posthypothermic storage, including plating efficiency, caspase-3/7 activity, ammonia metabolism, and drug-metabolizing capacity of isolated hepatocytes. Long-term function, basal, and induced cytochrome P450 activities were measured after exposure to prototypical inducing agents. Cells from 47 different human liver specimens were analyzed. Viability significantly decreased in cells cold stored in UW solution, while apoptosis level and plating efficiency were not significantly different from fresh cells. Luminescent and fluorescent methods assessed phases I and II activities both pre- and post-24-72 h of cold preservation. A robust induction (up to 200-fold) of phase I enzymes was observed in cultured cells. Phase II and ammonia metabolism remained stable during hypothermic storage, although the inductive effect of culture on each metabolic activity was eventually lost. Using techniques that characterize 11 measurements of hepatic viability and function from plating efficiency, to ammonia metabolism, to phases I and II drug metabolism, it was determined that while viability decreased, the remaining viable cells in cold-stored suspensions retained critical hepatic functions for up to 48 h at levels not significantly different from those observed in freshly isolated cells.

Published

2014

39. 63: CPS-1 Humanized Liver in FRGN Mouse as Model for Genetic Disorder

Author

Stephen C. Strom, Christina Hammerstadt, Raghuramanan Srinivasan, Mihaela Zabulica, and Roberto Gramignoli

Subjects

Genetics, Transplantation, Genetic disorder, medicine, Biology, medicine.disease

Published

2019

40. 42: Molecular Pathways in Support of Allogenic Human Amnion Epithelial Cell Transplantation for Liver Disease Without Immunosuppression

Author

Fabio Malavasi, Alberto L. Horenstein, Raghuramanan Srinivasan, Fabio Morandi, Roberto Gramignoli, and Stephen C. Strom

Subjects

Transplantation, Liver disease, medicine.anatomical_structure, Amnion, business.industry, medicine.medical_treatment, Cancer research, Medicine, Immunosuppression, business, medicine.disease, Epithelium

Published

2019

41. Cellular mechanism in support of allogenic human amnion epithelial cell transplantation without immunosuppression

Author

Fabio Morandi, Alberto L. Horenstein, Roberto Gramignoli, Raghuraman C. Srinivasan, Fabio Malavasi, Stephen C. Strom, and B. Strunz

Subjects

0301 basic medicine, Cancer Research, medicine.medical_treatment, Immunology, Human leukocyte antigen, Cell therapy, 03 medical and health sciences, 0302 clinical medicine, Immune system, Immunology and Allergy, Medicine, Genetics (clinical), Transplantation, business.industry, CD47, Immunosuppression, Cell Biology, Stem-cell therapy, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, cardiovascular system, Cancer research, Stem cell, business

Abstract

Background & Aim Placenta is a non-controversial and readily available source of stem cells for regenerative medicine. We previously reported that human amnion epithelial cells (hAEC) from term placenta are not tumorigenic, have immunomodulatory and anti-inflammatory properties and once transplanted differentiate into functional hepatocyte-like cells. In preclinical studies with immune-competent mice, hAEC engrafted and survived without administration of immunosuppressive drugs, resulting in correction of metabolic liver diseases or the reversal of acute liver failure. In clinical settings allogenic hAEC have been transplanted without immunosuppression. However, little or null is known about immunomodulatory cells, as hAEC. During the past years we studied and identified molecular pathways this novel stem cells has, driving immunoregulatory capacity. Methods, Results & Conclusion We performed a complete surface screening of hAEC, profiling all the molecules commonly described on other stem as well as somatic cells. Amnion characteristically lacks HLA class 2 expression and expresses both class 1a and non-polymorphic class 1b (responsible for maternal immune-toleration of the fetus). We quantified the level of expression of HLA-G and HLA-E molecules both as membrane-bound and soluble forms. Recently, purinergic mediators, hydrolyzed by plasma membrane nucleotidases, have also been identified to regulate immune cell response, thus we quantified the level of expression of all ecto-enzymes in hAEC preparations. Surprisingly, hAEC constitutively express all known ecto-enzymes. In addition, we proved constitutive expression of of CD47 (‘don't-eat-me’ signal) and complement system (CD55/CD59). Immunogenicity of the hAEC was confirmed on purified immune effector cells (T-, B- and NK-cells). Conclusions High level expression of ecto-enzymatic axis and non-canonical HLA molecules likely play a key role in immunological tolerance and long-term acceptance of the human xeno-cell graft in immunocompetent mice. The ability to treat the most common (liver) diseases with one stem cell therapy without the administration of immunosuppressive drugs could be a “game changer” and will greatly expand the number of patients who could receive cellular therapy. Based on their safety and the successful preclinical studies, approval was granted to begin banking of hAEC under cGMP condition at Karolinska Institutet, and to perform hAEC transplants on 10 patients with liver disease without immunosuppression.

Published

2019

42. Applying hydrodynamic pressure to efficiently generate induced pluripotent stem cells via reprogramming of centenarian skin fibroblasts

Author

Kristina Kannisto, Miriam Capri, Julie Piccand, Francesco Ravaioli, Paolo Garagnani, Claudio Franceschi, Mihaela Zabulica, Roberto Gramignoli, Stephen C. Strom, Marine R.-C. Kraus, Massoud Vosough, Vosough M., Ravaioli F., Zabulica M., Capri M., Garagnani P., Franceschi C., Piccand J., Kraus M.R.-C., Kannisto K., Gramignoli R., and Strom S.C.

Subjects

Adult, 0301 basic medicine, Somatic cell, Science, Genetic Vectors, Induced Pluripotent Stem Cells, Primary Cell Culture, Biology, Transfection, Sendai virus, Transplantation, Autologous, Viral vector, 03 medical and health sciences, Transduction (genetics), 0302 clinical medicine, Induced Pluripotent Stem Cells, Ageing, Pluripotency, Geriatrics, Humans, Cellular Reprogramming Techniques, Vector (molecular biology), Induced pluripotent stem cell, Cells, Cultured, Skin, Aged, 80 and over, Cloning, Multidisciplinary, Regeneration (biology), Age Factors, Infant, Newborn, Reproducibility of Results, Fibroblasts, Cellular Reprogramming, Skin Aging, 3. Good health, Cell biology, 030104 developmental biology, 030220 oncology & carcinogenesis, Hydrodynamics, Medicine, Reprogramming, Research Article

Abstract

Induced pluripotent stem cell (iPSC)-technology is an important platform in medicine and disease modeling. Physiological degeneration and disease onset are common occurrences in the aging population. iPSCs could offer regenerative medical options for age-related degeneration and disease in the elderly. However, reprogramming somatic cells from the elderly is inefficient when successful at all. Perhaps due to their low rates of replication in culture, traditional transduction and reprogramming approaches with centenarian fibroblasts met with little success. A simple and reproducible reprogramming process is reported here which enhances interactions of the cells with the viral vectors that leads to improved iPSC generation. The improved methods efficiently generates fully reprogrammed iPSC lines from 105–107 years old subjects in feeder-free conditions using an episomal, Sendai-Virus (SeV) reprogramming vector expressing four reprogramming factors. In conclusion, dermal fibroblasts from human subjects older than 100 years can be efficiently and reproducibly reprogrammed to fully pluripotent cells with minor modifications to the standard reprogramming procedures. Efficient generation of iPSCs from the elderly may provide a source of cells for the regeneration of tissues and organs with autologous cells as well as cellular models for the study of aging, longevity and age-related diseases.

Published

2019

43. FRI-448-Correction of a metabolic liver disease after ex vivo gene editing of defective human primary hepatocytes

Author

Olav Rooyackers, Stephen C. Strom, Johannes Häberle, Mihaela Zabulica, Gabriella Allegri, Tingting Wu, Beat Thöny, Christina Hammarstedt, and Raghuraman chittoor srinivasan

Subjects

Liver disease, Primary (chemistry), Hepatology, Genome editing, medicine, Cancer research, Biology, medicine.disease, Ex vivo

Published

2019

44. Mice With Human Livers

Author

Markus Grompe and Stephen C. Strom

Subjects

Regulation of gene expression, Liver injury, Severe combined immunodeficiency, Hepatology, Chimera, Liver Diseases, Transgene, Gastroenterology, Mice, Transgenic, Nod, Biology, medicine.disease, Disease Models, Animal, Mice, Chimera (genetics), medicine.anatomical_structure, Liver, Pharmaceutical Preparations, Hepatocyte, Immunology, Hepatocytes, medicine, Animals, Humans, Fumarylacetoacetate hydrolase

Abstract

Animal models are used to study many aspects of human disease and to test therapeutic interventions. However, some very important features of human biology cannot be replicated in animals, even in nonhuman primates or transgenic rodents engineered with human genes. Most human microbial pathogens do not infect animals and the metabolism of many xenobiotics is different between human beings and animals. The advent of transgenic immune-deficient mice has made it possible to generate chimeric animals harboring human tissues and cells, including hepatocytes. The liver plays a central role in many human-specific biological processes and mice with humanized livers can be used to model human metabolism, liver injury, gene regulation, drug toxicity, and hepatotropic infections.

Published

2013

45. Ritonavir and Efavirenz Significantly Alter the Metabolism of Erlotinib—an Observation in Primary Cultures of Human Hepatocytes That Is Relevant to HIV Patients with Cancer

Author

Susan M. Christner, Stephen C. Strom, Michelle A. Rudek, Jan H. Beumer, Venkateswaran C. Pillai, Robert A. Parise, Raman Venkataramanan, and Roberto Gramignoli

Subjects

Adult, Cyclopropanes, Male, Efavirenz, Anti-HIV Agents, CYP3A, Pharmaceutical Science, HIV Infections, Pharmacology, Biology, Erlotinib Hydrochloride, chemistry.chemical_compound, Neoplasms, medicine, Humans, Drug Interactions, heterocyclic compounds, neoplasms, Aged, Nucleic Acid Synthesis Inhibitors, Ritonavir, CYP3A4, virus diseases, Half-life, Articles, HIV Protease Inhibitors, Middle Aged, Benzoxazines, respiratory tract diseases, Ketoconazole, chemistry, 14-alpha Demethylase Inhibitors, Alkynes, Hepatocytes, Quinazolines, Female, Erlotinib, Rifampin, Half-Life, medicine.drug

Abstract

Erlotinib is approved for the treatment of non-small cell lung and pancreatic cancers, and is metabolized by CYP3A4. Inducers and inhibitors of CYP3A enzymes such as ritonavir and efavirenz, respectively, may be used as part of the highly active antiretroviral therapy drugs to treat patients with human immunodeficiency virus (HIV). When HIV patients with a malignancy need treatment with erlotinib, there is a potential of as-yet-undefined drug-drug interaction. We evaluated these interactions using human hepatocytes benchmarked against the interaction of erlotinib with ketoconazole and rifampin, the archetype cytochrome P450 inhibitor and inducer, respectively. Hepatocytes were treated with vehicle [0.1% dimethylsulfoxide, ritonavir (10 μM)], ketoconazole (10 μM), efavirenz (10 μM), or rifampin (10 μM) for 4 days. On day 5, erlotinib (5 μM) was incubated with the above agents for another 24-48 hours. Concentrations of erlotinib and O-desmethyl erlotinib were quantitated in collected samples (combined lysate and medium) using liquid chromatography and tandem mass spectrometry. The half-life (t(½)) of erlotinib increased from 10.6 ± 2.6 to 153 ± 80 and 23.9 ± 4.8 hours, respectively, upon treatment with ritonavir and ketoconazole. The apparent intrinsic clearance (C(Lint, app)) of erlotinib was lowered 16-fold by ritonavir and 1.9-fold by ketoconazole. Efavirenz and rifampin decreased t1/2 of erlotinib from 10.3 ± 1.1 to 5.0 ± 1.5 and 3.4 ± 0.2 hours, respectively. Efavirenz and rifampin increased the C(Lint, app) of erlotinib by 2.2- and 2-fold, respectively. Our results suggest that to achieve desired drug exposure, the clinically used dose (150 mg daily) of erlotinib may have to be significantly reduced (25 mg every other day) or increased (300 mg daily), respectively, when ritonavir or efavirenz is coadministered.

Published

2013

46. Genetic Variation in Aldo-Keto Reductase 1D1 (AKR1D1) Affects the Expression and Activity of Multiple Cytochrome P450s

Author

Erin G. Schuetz, Yiping Fan, Ranjit K. Thirumaran, Xia Yang, Kazuto Yasuda, Stephen C. Strom, and Amarjit S. Chaudhry

Subjects

Pharmacology, Regulation of gene expression, Untranslated region, Gene knockdown, Aldo-keto reductase, Pregnane X receptor, CYP3A4, Genetic Variation, Pharmaceutical Science, Articles, Hep G2 Cells, Biology, Polymorphism, Single Nucleotide, Molecular biology, Gene Expression Regulation, Enzymologic, Alternative Splicing, Cytochrome P-450 Enzyme System, Liver, Constitutive androstane receptor, Hepatocytes, Humans, Farnesoid X receptor, RNA, Messenger, Oxidoreductases

Abstract

Human liver gene regulatory (Bayesian) network analysis was previously used to identify a cytochrome P450 (P450) gene subnetwork with Aldo-keto reductase 1D1 (AKR1D1) as a key regulatory driver of this subnetwork. This study assessed the biologic importance of AKR1D1 [a key enzyme in the synthesis of bile acids, ligand activators of farnesoid X receptor (FXR), pregnane X receptor (PXR), and constitutive androstane receptor (CAR), known transcriptional regulators of P450s] to hepatic P450 expression. Overexpression of AKR1D1 in primary human hepatocytes led to increased expression of CYP3A4, CYP2C8, CYP2C9, CYP2C19, and CYP2B6. Conversely, AKR1D1 knockdown decreased expression of these P450s. We resequenced AKR1D1 from 98 donor livers and identified a 3'-untranslated region (UTR) (rs1872930) single nucleotide polymorphism (SNP) significantly associated with higher AKR1D1 mRNA expression. AKR1D1 3'-UTR-luciferase reporter studies showed that the variant allele resulted in higher luciferase activity, suggesting that the SNP increases AKR1D1 mRNA stability and/or translation efficiency. Consistent with AKR1D1's putative role as a driver of the P450 subnetwork, the AKR1D1 3'-UTR SNP was significantly associated with increased hepatic mRNA expression of multiple P450s (CYP3A4, CYP2C8, CYP2C9, CYP2C19, and CYP2B6) and CYP3A4, CYP2C8, CYP2C19, and CYP2B6 activities. After adjusting for multiple testing, the association remained significant for AKR1D1, CYP2C9, and CYP2C8 mRNA expression and CYP2C8 activity. These results provide new insights into the variation in expression and activity of P450s that can account for interindividual differences in drug metabolism/efficacy and adverse drug events. In conclusion, we provide the first experimental evidence supporting a role for AKR1D1 as a key genetic regulator of the P450 network.

Published

2013

47. A sensitive and specific CYP cocktail assay for the simultaneous assessment of human cytochrome P450 activities in primary cultures of human hepatocytes using LC–MS/MS

Author

Raman Venkataramanan, Steve N. Caritis, Stephen C. Strom, and Venkateswaran C. Pillai

Subjects

CYP2B6, Electrospray ionization, Clinical Biochemistry, Pharmaceutical Science, Mass spectrometry, Article, Analytical Chemistry, Cytochrome P-450 Enzyme System, Tandem Mass Spectrometry, Drug Discovery, medicine, Humans, Drug Interactions, Solid phase extraction, Cells, Cultured, Spectroscopy, Chromatography, CYP3A4, Chemistry, CYP1A2, Enzyme Activation, Pharmaceutical Preparations, Phenacetin, Chlorzoxazone, Hepatocytes, Chromatography, Liquid, medicine.drug

Abstract

A sensitive and specific CYP cocktail assay for simultaneous measurement of the activities of major human cytochrome P450 enzymes (CYP1A2 (phenacetin), CYP3A4/5 (midazolam), CYP2C9 (diclofenac), CYP2C19 (S-mephenytoin) and CYP2D6 (dextromethorphan)) in primary cultures of human hepatocytes, was developed and validated using liquid chromatography-tandem mass spectrometry (LC-MS/MS). Hepatocyte incubation medium was processed by a solid phase extraction (SPE) using Oasis SPE extraction cartridges prior to chromatography. The metabolites derived from each of the substrates were simultaneously quantitated using the corresponding stable isotope-labeled internal standards by a positive electrospray ionization mode using multiple reactions monitoring with a single eight minute run. The mean accuracy was in the range of 98-114%. The interday and intraday precision over the concentration ranges evaluated for all the analytes were lower than 15%, and 14%, respectively. All the generated metabolites were stable under the conditions used for sample analysis. Additionally, the interaction of a cocktail substrate on other CYP substrates was also analyzed. Due to substantial inter-substrate interaction, chlorzoxazone (CYP2E1) and bupropion (CYP2B6) were removed from the initial seven probes CYP cocktail assay. Therefore, the final CYP cocktail assay consisting of five probes provides a robust method to simultaneously measure activities of CYP1A2, CYP2C9, CYP2C19, CYP2D6 and CYP3A4/5 in primary cultures of human hepatocytes.

Published

2013

48. Treprostinil Improves Hepatic Cytochrome P450 Activity during Rat Liver Transplantation

Author

Junichi Yoshida, Noriko Murase, Raman Venkataramanan, Nisanne Ghonem, and Stephen C. Strom

Subjects

Pathology, medicine.medical_specialty, Hepatology, CYP3A, business.industry, Prostaglandin, Prostacyclin, Pharmacology, CYP2E1, Transplantation, chemistry.chemical_compound, surgical procedures, operative, chemistry, medicine, Original Article, Viaspan, business, Drug metabolism, medicine.drug, Treprostinil

Abstract

Background: Cytochrome P450 (CYP450) activity is an important indicator of liver graft function. CYP450 activity is altered by pro-inflammatory cytokines, which are associated with ischemia-reperfusion (I/R) injury during orthotopic liver transplantation (OLT). Treprostinil, an FDA-approved prostacyclin analog, ameliorated cold I/R injury during rat OLT. We hypothesized that treprostinil would improve CYP450 activity in liver graft during cold I/R injury post-OLT. Methods: OLT was performed in syngeneic male Lewis rats with 18 h graft preservation in cold UW solution. Donor and recipients received treprostinil (100 ng/kg/min) or matching placebo for 24 h before and up to 48 h post-OLT. Liver graft mRNA and protein expression of CYP450 isoforms were analyzed by qRT-PCR and Western blot analysis, respectively. The formation rates of 1-hydroxymidazolam and 6b-hydroxytestosterone, 6-hydroxychlorzoxazone, 2a- and 16a-hydroxytestosterone in liver graft microsomes served as markers for CYP3A, CYP2E1, and CYP2C11 activity, respectively, and were measured by LC–MS. Results: TreprostinilsignificantlydecreasedserumALTandASTlevelsat6–48hafterOLT,comparedtoplacebo.Theexpressions of TNFa and IFNg mRNA in the liver graft were significantly inhibited in the treprostinil-treated group at 1 h post-reperfusion. Treprostinil restored CYP2E1 protein expression to that of normal liver and significantly improved CYP3A activity to more than two-fold of placebo early post-OLT. Conclusions: Treprostinil significantly ameliorated hepatic injury, reduced expression of pro-inflammatory cytokines, and improved CYP450 activity in liver graft early post-OLT. These findings suggest that treprostinil has the potential to serve as a therapeutic optiontoprotectlivergraftfunctionagainstI/RinjuryduringclinicalOLT. (JCLINEXPHEPATOL2012;2:323–332)

Published

2012

49. Hepatocyte Transplantation in Special Populations: Clinical Use in Children

Author

Stephen C. Strom and Zahida Khan

Subjects

0301 basic medicine, medicine.medical_specialty, Special populations, Adolescent, Orthotopic liver transplantation, Cell Transplantation, Genetic enhancement, Regenerative medicine, Article, End Stage Liver Disease, 03 medical and health sciences, 0302 clinical medicine, Hepatocyte transplantation, medicine, Humans, Child, Intensive care medicine, business.industry, Whole liver, Infant, Liver Failure, Acute, Liver Transplantation, Transplantation, surgical procedures, operative, 030104 developmental biology, medicine.anatomical_structure, Child, Preschool, Hepatocyte, Immunology, Hepatocytes, 030211 gastroenterology & hepatology, business

Abstract

Orthotopic liver transplantation remains the only proven cure for end-stage liver failure. Despite significant advances in the field, the clinical demand for donor organs far outweighs the supply. Hepatocyte transplantation has been proposed as an alternative approach to whole liver transplant in select diseases. Several international centers have reported experimental trials of human hepatocyte transplantation in acute liver failure and liver-based metabolic disorders. This chapter provides an introduction to hepatocyte transplantation from both a technical and clinical perspective. We will also focus on the special needs of pediatric patients, since historically the majority of clinical hepatocyte transplants have involved infants and children.

Published

2016

50. Isolation of Human Amnion Epithelial Cells According to Current Good Manufacturing Procedures

Author

Raghuraman C. Srinivasan, Roberto Gramignoli, Kristina Kannisto, and Stephen C. Strom

Subjects

0301 basic medicine, Cell type, Placenta, Cell, Cell Separation, Biology, Regenerative medicine, Flow cytometry, Term placenta, 03 medical and health sciences, Pregnancy, medicine, Humans, Amnion, medicine.diagnostic_test, Epithelial Cells, Cell Biology, General Medicine, Flow Cytometry, Selective isolation, Cell biology, 030104 developmental biology, medicine.anatomical_structure, Immunology, cardiovascular system, Female, Developmental Biology

Abstract

Different cell types can be isolated from human placental tissues, and some have been reported to retain phenotypic plasticity and characteristics that make them a promising source of cells for regenerative medicine. Among these are human amnion epithelial cells (hAECs). Adoption of current good manufacturing practices (cGMP) and enhanced quality control is essential when isolating hAECs in order to deliver a safe and effective cellular product for clinical purposes. This unit describes a detailed protocol for selective isolation of hAECs from human term placenta with little to no contamination by other cell types. A method for characterizing the heterogeneity of the hAEC suspension is also provided. The resulting cell product will be useful for clinical as well as basic research applications. © 2016 by John Wiley & Sons, Inc.

Published

2016